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Persons using assistive technology might not be able to fully access information in this file. For assistance, please send e-mail to: mmwrq@cdc.gov. Type 508 Accommodation and the title of the report in the subject line of e-mail. Update: Vaccine Side Effects, Adverse Reactions, Contraindications, and Precautions Recommendations of the Advisory Committee on Immunization Practices (ACIP)Summary This report provides updated information concerning the potential adverse events associated with vaccination for hepatitis B, poliomyelitis, measles, mumps, diphtheria, tetanus, and pertussis. This information incorporates findings from a series of recent literature reviews, conducted by an expert committee at the Institute of Medicine (IOM), of all evidence regarding the possible adverse consequences of vaccines administered to children. This report contains modifications to the previously published recommendations of the Advisory Committee on Immunization Practices (ACIP) and is based on an ACIP review of the IOM findings and new research on vaccine safety. In addition, this report incorporates information contained in the "Recommendations of the Advisory Committee on Immunization Practices: Use of Vaccines and Immune Globulins in Persons with Altered Immunocompetence" (MMWR 1993;42{No. RR-4}) and the "General Recommendations on Immunization: Recommendations of the Advisory Committee on Immunization Practices (ACIP)" (MMWR 1994;43{No. RR-1}). Major changes to the previous recommendations are highlighted within the text, and specific information concerning the following vaccines and the possible adverse events associated with their administration are included: hepatitis B vaccine and anaphylaxis; measles vaccine and a) thrombocytopenia and b) possible risk for death resulting from anaphylaxis or disseminated disease in immunocompromised persons; diphtheria and tetanus toxoids and pertussis vaccine (DTP) and chronic encephalopathy; and tetanus-toxoid-containing vaccines and a) Guillain-Barre syndrome, b) brachial neuritis, and c) possible risk for death resulting from anaphylaxis. These modifications will be incorporated into more comprehensive ACIP recommendations for each vaccine when such statements are revised. Also included in this report are interim recommendations concerning the use of measles and mumps vaccines in
INTRODUCTION Immunization has enabled the global eradication of smallpox (1), the elimination of poliomyelitis from the Western hemisphere (2), and major reductions in the incidence of other vaccine-preventable diseases in the United States (Table_1). However, although immunization has successfully reduced the incidence of vaccine-preventable diseases, vaccination can cause both minor and, rarely, serious side effects. Public awareness of and controversy about vaccine safety has increased, primarily because increases in vaccine coverage resulted in an increased number of adverse events that occurred after vaccination. Such adverse events include both true reactions to vaccine and events coincidental to, but not caused by, vaccination. Despite concerns about vaccine safety, vaccination is safer than accepting the risks for the diseases these vaccines prevent. Unless a disease has been eradicated (e.g., smallpox), failure to vaccinate increases the risks to both the individual and society. In response to concerns about vaccine safety, the National Childhood Vaccine Injury Act of 1986 established a no-fault compensation process for persons possibly injured by selected vaccines (3). The Act also mandated that the Institute of Medicine * (IOM) review scientific and other evidence regarding the possible adverse consequences of vaccines administered to children. IOM constituted an expert committee to review all available information on these vaccine adverse events; such information included epidemiologic studies, case series, individual case reports, and testimonials. To derive their conclusions, the IOM committee members created five categories of causality to describe the relationships between the vaccines and specific adverse events. The first IOM review examined certain events occurring after administration of pertussis and rubella vaccines (Table_2) (4). The second IOM review examined events occurring after administration of all other vaccines usually administered during childhood (i.e., diphtheria and tetanus toxoids and measles, mumps, hepatitis B, Haemophilus influenzae type b {Hib}, and poliovirus vaccines) (Table_3) (5). Two other IOM committees have met since the findings of the second review were published. These two committees have published their findings concerning both the diphtheria and tetanus toxoids and pertussis vaccine (DTP) and chronic nervous system dysfunction (Figure_1) (6) and research strategies for vaccine-associated adverse events (7). The Advisory Committee on Immunization Practices (ACIP) recently reviewed the findings of the IOM committees and modified the previously published ACIP recommendations to ensure consistency with IOM conclusions. These recommendations, which are included in this report, update all previously published ACIP recommendations pertaining to the precautions, contraindications, side effects, and adverse reactions ** associated with specific vaccines. ACIP accepted the IOM conclusions for almost all vaccine adverse events; the few exceptions generally occurred because new information that was available to ACIP had not been available when the IOM committees published their recommendations. These exceptions included a) oral poliovirus vaccine (OPV) and Guillain-Barre syndrome (GBS), b) tetanus-toxoid- containing vaccines and GBS, and c) DTP and chronic nervous system dysfunction. In addition, this report incorporates information contained in the "Recommendations of the Advisory Committee on Immunization Practices: Use of Vaccines and Immune Globulins in Persons with Altered Immunocompetence" (MMWR 1993; 42{No. RR-4}) and the "General Recommendations on Immunization: Recommendations of the Advisory Committee on Immunization Practices (ACIP)" (MMWR 1994;43{No. RR-1}). To facilitate recognition of the new recommendations in this report, all major changes that are being made to the previously published ACIP statements are highlighted within the text. These changes include information on the following vaccines and the possible adverse events associated with their administration:
The modifications contained in this report, and possibly other changes as new information becomes available, will be incorporated into more comprehensive ACIP recommendations for each vaccine when such statements are revised. HEPATITIS B VACCINE The following recommendations concerning adverse events associated with hepatitis B vaccination update those applicable sections in "Hepatitis B Virus: A Comprehensive Strategy for Eliminating Transmission in the United States Through Universal Childhood Vaccination -- Recommendations of the Immunization Practices Advisory Committee (ACIP)" (MMWR 1991;40{No. RR-13}). Vaccine Side Effects and Adverse Reactions Hepatitis B vaccines are safe to administer to adults and children. More than an estimated 10 million adults and 2 million infants and children have been vaccinated in the United States, and at least 12 million children have been vaccinated worldwide. Vaccine-Associated Side Effects Pain at the injection site (3%-29%) and a temperature greater than 37.7 C (1%-6%) have been among the most frequently reported side effects among adults and children receiving vaccine (8-12). In placebo-controlled studies, these side effects were reported no more frequently among vaccinees than among persons receiving a placebo (11,12). Among children receiving both hepatitis B vaccine and DTP, these mild side effects have been observed no more frequently than among children receiving only DTP. The recommendation to begin hepatitis B vaccination soon after birth has raised the concern that a substantial number of infants will require an extensive medical evaluation for elevated temperatures secondary to hepatitis B vaccination. Several population-based studies to evaluate this possibility are in progress. Adverse Events In the United States, surveillance of adverse reactions indicated a possible association between GBS and receipt of the first dose of plasma-derived hepatitis B vaccine (CDC, unpublished data; 13). However, an estimated 2.5 million adults received one or more doses of recombinant hepatitis B vaccine during 1986-1990, and available data concerning these vaccinees do not indicate an association between receipt of recombinant vaccine and GBS (CDC, unpublished data). Based on reports to the Vaccine Adverse Events Reporting System (VAERS), the estimated incidence rate of anaphylaxis among vaccine recipients is low (i.e., approximately one event per 600,000 vaccine doses distributed). Two of these adverse events occurred in children (CDC, unpublished data). In addition, only one case of anaphylaxis occurred among 100,763 children ages 10-11 years who had been vaccinated with recombinant vaccine in British Columbia (D. Scheifele, unpublished data), and no adverse events were reported among 166,757 children who had been vaccinated with plasma-derived vaccine in New Zealand (5). Although none of the persons who developed anaphylaxis died, this adverse event can be fatal; in addition, hepatitis B vaccine can -- in rare instances -- cause a life-threatening hypersensitivity reaction in some persons (5). Therefore, subsequent vaccination with hepatitis B vaccine is contraindicated for persons who have previously had an anaphylactic response to a dose of this vaccine. Large-scale hepatitis B immunization programs for infants in Alaska, New Zealand, and Taiwan have not established an association between vaccination and the occurrence of other severe adverse events, including seizures and GBS (B. McMahon and A. Milne, unpublished data; 14). However, systematic surveillance for adverse reactions in these populations has been limited, and only a minimal number of children have received recombinant vaccine. Any presumed risk for adverse events that might be causally associated with hepatitis B vaccination must be balanced with the expected risk for hepatitis B virus (HBV)-related liver disease. Currently, an estimated 2,000-5,000 persons in each U.S. birth cohort will die as a result of HBV-related liver disease because of the 5% lifetime risk for HBV infection. As hepatitis B vaccine is introduced for routine vaccination of infants, surveillance for vaccine-associated adverse events will continue to be an important part of the program despite the current record of safety. Any adverse event suspected to be associated with hepatitis B vaccination should be reported to VAERS. VAERS forms can be obtained by calling (800) 822-7967. POLIOMYELITIS PREVENTION The following recommendations concerning adverse events associated with poliomyelitis vaccination update those applicable sections in "Poliomyelitis Prevention: Recommendation of the Immunization Practices Advisory Committee (ACIP)" (MMWR 1982;31:22-6,31-4) and "Poliomyelitis Prevention: Enhanced-Potency Inactivated Poliomyelitis Vaccine -- Supplementary Statement" (MMWR 1987;36:795-8). Precautions and Contraindications Pregnancy Although no conclusive evidence documents the adverse effects of OPV or inactivated poliovirus vaccine (IPV) in pregnant women and their developing fetuses, vaccination of pregnant women should be avoided. However, if immediate protection against poliomyelitis is necessary, OPV or IPV can be given. Immunodeficiency Persons who have congenitally acquired immune-deficiency diseases (e.g., combined immunodeficiency, hypogammaglobulinemia, and agammaglobulinemia) should not be given OPV because of their substantially increased risk for vaccine-associated disease. Furthermore, persons who have altered immune status resulting from acquired conditions (e.g., human immunodeficiency virus {HIV} infection, leukemia, lymphoma, or generalized malignancy) or who have immune systems compromised by therapy (e.g., treatment with corticosteroids, alkylating drugs, antimetabolites, or radiation) should not receive OPV because of the theoretical risk for paralytic disease. IPV -- and not OPV -- should be used to vaccinate immunodeficient persons and their household contacts. Many immunosuppressed persons are already immune to polioviruses because of previous vaccination or exposure to wild-type virus when they were immunocompetent. Although such persons should not receive OPV, their risk for paralytic disease may be less than that of persons who have congenitally acquired immunodeficiency. Although a protective immune response to IPV in the immunodeficient patient cannot be ensured, the vaccine is safe and some protection may result from its administration. If a household contact of an immunodeficient person is vaccinated inadvertently with OPV, the OPV recipient should avoid close physical contact with the immunodeficient person for approximately 4-6 weeks after vaccination (i.e., during the period of maximum excretion of vaccine virus). If such contact cannot be avoided, rigorous hygiene and hand washing after contact with feces (e.g., after diaper changing) and avoidance of contact with saliva (e.g., by not sharing eating utensils or food) should be practiced. These practices are an acceptable, but probably less effective, alternative than refraining from contact. Because immunodeficiency is possible in other children born to a family in which one child is immunodeficient, OPV should not be administered to a member of such a house-hold until the immune status of the recipient and other children in the family is documented. Adverse Reactions OPV In rare instances, administration of OPV has been associated with paralytic poliomyelitis in healthy recipients and their contacts. Very rarely, OPV has caused fatal paralytic poliomyelitis in immunocompromised persons (5). Other than efforts for identifying persons with immune-deficiency conditions, no procedures are currently available to identify persons likely to experience such adverse reactions. Although the risk of vaccine-associated paralysis is extremely small for vaccinees and their susceptible, close, personal contacts, they should be informed of this risk. Available data do not indicate a measurable increased risk for GBS after receipt of OPV. Initial reports (at the time of IOM review) of two studies conducted in Finland suggested that OPV might cause GBS. These studies identified an apparent increased incidence of GBS that was temporally associated with mass OPV vaccination of children and adults who had previously received IPV (15,16). Since the IOM review, a reanalysis of the data derived from the studies conducted in Finland and an analysis of an observational study conducted in the United States have not demonstrated a causal relationship between OPV and GBS in infants (17). Because OPV contains trace amounts of streptomycin, bacitracin, and neomycin, its use is contraindicated in persons who have previously had an anaphylactic reaction to OPV or to these antibiotics. IPV No serious side effects of currently available IPV have been documented. Since IPV contains trace amounts of streptomycin and neomycin, there is a possibility of hypersensitivity reactions in individuals sensitive to these antibiotics. MEASLES PREVENTION The following recommendations concerning adverse events associated with measles vaccination update those applicable sections in "Measles Prevention: Recommendations of the Immunization Practices Advisory Committee" (MMWR 1989; 38{No. S-9}), and they apply regardless of whether the vaccine is administered as a single antigen or as a component of measles-rubella (MR) or measles-mumps-rubella (MMR) vaccine. Information concerning adverse events associated with the mumps component of MMR vaccine is reviewed later in this document (see Mumps Prevention), and information concerning the rubella component is located in the previously published ACIP statement for rubella (18). Side Effects and Adverse Reactions More than 240 million doses of measles vaccine were distributed in the United States from 1963 through 1993. The vaccine has an excellent record of safety. From 5% to 15% of vaccinees may develop a temperature of greater than or equal to 103 F ( greater than or equal to 39.4 C) beginning 5-12 days after vaccination and usually lasting several days (19). Most persons with fever are otherwise asymptomatic. Transient rashes have been reported for approximately 5% of vaccinees. Central nervous system (CNS) conditions, including encephalitis and encephalopathy, have been reported with a frequency of less than one per million doses administered. The incidence of encephalitis or encephalopathy after measles vaccination of healthy children is lower than the observed incidence of encephalitis of unknown etiology. This finding suggests that the reported severe neurologic disorders temporally associated with measles vaccination were not caused by the vaccine. These adverse events should be anticipated only in susceptible vaccinees and do not appear to be age-related. After revaccination, most reactions should be expected to occur only among the small proportion of persons who failed to respond to the first dose. Personal and Family History of Convulsions As with the administration of any agent that can produce fever, some children may have a febrile seizure. Although children with a personal or family history of seizures are at increased risk for developing idiopathic epilepsy, febrile seizures following vaccinations do not in themselves increase the probability of subsequent epilepsy or other neurologic disorders. Most convulsions following measles vaccination are simple febrile seizures, and they affect children without known risk factors. An increased risk of these convulsions may occur among children with a prior history of convulsions or those with a history of convulsions in first-degree family members (i.e., siblings or parents) (20). Although the precise risk cannot be determined, it appears to be low. In developing vaccination recommendations for these children, ACIP considered a number of factors, including risks from measles disease, the large proportion (5%-7%) of children with a personal or family history of convulsions, and the fact that convulsions following measles vaccine are uncommon. Studies conducted to date have not established an association between MMR vaccination and the development of a residual seizure disorder (5). ACIP concluded that the benefits of vaccinating these children greatly outweigh the risks. They should be vaccinated just as children without such histories. Because the period for developing vaccine-induced fever occurs approximately 5-12 days after vaccination, prevention of febrile seizures is difficult. Prophylaxis with antipyretics has been suggested as one alternative, but these agents may not be effective if given after the onset of fever. To be effective, such agents would have to be initiated before the expected onset of fever and continued for 5-7 days. However, parents should be alert to the occurrence of fever after vaccination and should treat their children appropriately. Children who are being treated with anticonvulsants should continue to take them after measles vaccination. Because protective levels of most currently available anticonvulsant drugs (e.g., phenobarbital) are not achieved for some time after therapy is initiated, prophylactic use of these drugs does not seem feasible. The parents of children who have either a personal or family history of seizures should be advised of the small increased risk of seizures following measles vaccination. In particular, they should be told in advance what to do in the unlikely event that a seizure occurs. The permanent medical record should document that the small risk of postimmunization seizures and the benefits of vaccination have been discussed. Subacute Sclerosing Panencephalitis (SSPE) Measles vaccine significantly reduces the likelihood of developing SSPE, as evidenced by the near elimination of SSPE cases after widespread measles vaccination began. SSPE has been reported rarely in children who do not have a history of natural measles infection but who have received measles vaccine. The available evidence suggests that at least some of these children may have had an unidentified measles infection before vaccination and that the SSPE probably resulted from the natural measles infection. The administration of live measles vaccine does not increase the risk for SSPE, regardless of whether the vaccinee has had measles infection or has previously received live measles vaccine (5,21). Thrombocytopenia Surveillance of adverse reactions in the United States and other countries indicates that MMR vaccine can, in rare circumstances, cause clinically apparent thrombocytopenia within the 2 months after vaccination. In prospective studies, the reported incidence of clinically apparent thrombocytopenia after MMR vaccination ranged from one case per 30,000 vaccinated children in Finland (22) and Great Britain (23) to one case per 40,000 in Sweden, with a temporal clustering of cases occurring 2-3 weeks after vaccination (24). With passive surveillance, the reported incidence was approximately one case per 100,000 vaccine doses distributed in Canada and France (25), and approximately one case per 1 million doses distributed in the United States (26). The clinical course of these cases was usually transient and benign, although hemorrhage occurred rarely (26). Furthermore, the risk for thrombocytopenia during rubella or measles infection is much greater than the risk after vaccination. Of 30,000 school-children in one Pennsylvania county who had been infected with rubella during the 1963-64 measles epidemic, 10 children developed thrombocytopenic purpura (incidence: one case per 3,000 children) (27). Based on case reports, the risk for thrombocytopenia may be higher for persons who previously have had idiopathic thrombocytopenic purpura, particularly for those who had thrombocytopenic purpura after an earlier dose of MMR vaccine (5,28,29). Revaccination Risks There is no evidence of an increased risk for adverse reactions after administration of live measles vaccine to persons who are already immune to measles as a result of either previous vaccination or natural disease. Precautions and Contraindications Pregnancy Live measles vaccine, when given as a component of MR or MMR, should not be given to women known to be pregnant or who are considering becoming pregnant within the next 3 months. Women who are given monovalent measles vaccine should not become pregnant for at least 30 days after vaccination. This precaution is based on the theoretical risk of fetal infection, although no evidence substantiates this theoretical risk. Considering the importance of protecting adolescents and young adults against measles, asking women if they are pregnant, excluding those who are, and explaining the theoretical risks to the others before vaccination are sufficient precautions. Febrile Illness The decision to administer or delay vaccination because of a current or recent febrile illness depends largely on the cause of the illness and the severity of symptoms. Minor illnesses, such as a mild upper-respiratory infection with or without low-grade fever, are not contraindications for vaccination. For persons whose compliance with medical care cannot be assured, every opportunity should be taken to provide appropriate vaccinations. Children with moderate or severe febrile illnesses can be vaccinated as soon as they have recovered from the acute phase of the illness. This wait avoids superimposing adverse effects of vaccination on the underlying illness or mistakenly attributing a manifestation of the underlying illness to the vaccine. Performing routine physical examinations or measuring temperatures are not prerequisites for vaccinating infants and children who appear to be in good health. Asking the parent or guardian if the child is ill, postponing vaccination for children with moderate or severe febrile illnesses, and vaccinating those without contraindications are appropriate procedures in childhood immunization programs. Allergic Reactions Hypersensitivity reactions rarely occur after the administration of MMR or any of its component vaccines. Most of these reactions are minor and consist of a wheal and flare or urticaria at the injection site. Immediate, anaphylactic reactions to MMR or its component vaccines are extremely rare. Although greater than 70 million doses of MMR vaccine have been distributed in the United States since VAERS was implemented in 1990, only 33 cases of anaphylactic reactions that occurred after MMR vaccination have been reported. Furthermore, only 11 of these cases a) occurred immediately after vaccination and b) occurred in persons who had symptoms consistent with anaphylaxis (CDC, unpublished data). In the past, persons who had a history of anaphylactic reactions (i.e., hives, swelling of the mouth or throat, difficulty breathing, hypotension, and shock) following egg ingestion were considered to be at increased risk for serious reactions after receipt of measles-containing vaccines, which are produced in chick embryo fibroblasts. Protocols requiring caution were developed for skin testing and vaccinating persons who had had anaphylactic reactions after egg ingestion (30-34). However, the predictive value of such skin testing and the need for special protocols when vaccinating egg-allergic persons with measles-containing vaccines is uncertain. The results of recent studies suggest that anaphylactic reactions to measles-containing vaccines are not associated with hypersensitivity to egg antigens but with some other component of the vaccines. The risk for serious allergic reaction to these vaccines in egg-allergic patients is extremely low, and skin testing is not necessarily predictive of vaccine hypersensitivity (35-37). Therefore, ACIP is re-evaluating whether skin testing and the use of special protocols are routinely necessary when administering MMR or other measles-containing vaccines to persons who have a history of anaphylactic-like reactions after egg ingestion. MMR and its component vaccines contain hydrolyzed gelatin as a stabilizer. The literature contains a single case report of a person with an anaphylactic sensitivity to gelatin who had an anaphylactic reaction after receipt of the MMR vaccine licensed in the United States (38). Similar cases have occurred in Japan (39). Therefore, ACIP is currently considering recommendations for vaccination of persons who have had an anaphylactic reaction to gelatin or gelatin-containing products. In the meantime, such persons should be vaccinated with MMR and its component vaccines with extreme caution. MMR vaccine and its component vaccines contain trace amounts of neomycin. Although the amount present is less than that usually used for a skin test to determine hypersensitivity, persons who have experienced anaphylactic reactions to neomycin should not be given these vaccines. Most often, neomycin allergy is manifested by contact dermatitis rather than anaphylaxis. A history of contact dermatitis to neomycin is not a contraindication to receiving measles vaccine. Live measles virus vaccine does not contain penicillin. Thrombocytopenia Children who have a history of thrombocytopenic purpura or thrombocytopenia may be at increased risk for developing clinically significant thrombocytopenia after MMR vaccination. The decision to vaccinate should depend on the benefits of immunity to measles, mumps, and rubella and the risks for recurrence or exacerbation of thrombocytopenia after vaccination or during natural infections with measles or rubella. The benefits of immunization are usually greater than the potential risks, and administration of MMR vaccine is justified -- particularly with regard to the even greater risk for thrombocytopenia after measles or rubella disease. However, avoiding a subsequent dose might be prudent if the previous episode of thrombocytopenia occurred in close temporal proximity to (i.e., within 6 weeks after) the previous vaccination. Serologic evidence of measles immunity in such persons may be sought in lieu of MMR vaccination. Recent Administration of Immune Globulins Previous recommendations, based on data from persons who received low doses of immune globulin preparations, stated that MMR and its individual component vaccines could be administered as early as 6 weeks to 3 months after administration of immune globulins (40,41). However, recent evidence suggests that high doses of immune globulins can inhibit the immune response to measles vaccine for more than 3 months (42,43). Administration of immune globulins also can inhibit the response to rubella vaccine (42). The effect of immune globulin preparations on the response to mumps vaccine is unknown, but commercial immune globulin preparations contain antibodies to these viruses. Blood (e.g., whole blood, packed red blood cells, and plasma) and other antibody-containing blood products (e.g., immune globulin; specific immune globulins; and immune globulin, intravenous {IGIV}) can diminish the immune response to MMR or its individual component vaccines. Therefore, after an immune globulin preparation is received, these vaccines should not be administered before the recommended interval (Table_4) and (Table_5). However, the postpartum vaccination of rubella-susceptible women with the rubella or MMR vaccine should not be delayed because anti-Rho(D) IG (human) or any other blood product was received during the last trimester of pregnancy or at delivery. These women should be vaccinated immediately after delivery and, if possible, tested at least 3 months later to ensure immunity to rubella and, if necessary, to measles. If administration of an immune globulin preparation becomes necessary because of imminent exposure to disease, MMR or its component vaccines can be administered simultaneously with the immune globulin preparation, although vaccine-induced immunity might be compromised. The vaccine should be administered at a site remote from that chosen for the immune globulin inoculation. Unless serologic testing indicates that specific antibodies have been produced, vaccination should be repeated after the recommended interval (Table_4) and (Table_5). If administration of an immune globulin preparation becomes necessary after MMR or its individual component vaccines have been administered, interference can occur. Usually, vaccine virus replication and stimulation of immunity will occur 1-2 weeks after vaccination. Thus, if the interval between administration of any of these vaccines and subsequent administration of an immune globulin preparation is less than 14 days, vaccination should be repeated after the recommended interval (Table_4) and (Table_5), unless serologic testing indicates that antibodies were produced. Altered Immunocompetence Non-HIV-Infected Persons. Replication of vaccine viruses can be enhanced in persons with immune-deficiency diseases and in persons with immunosuppression, as occurs with leukemia, lymphoma, generalized malignancy, or therapy with alkylating agents, antimetabolites, radiation, or large doses of corticosteroids. Evidence based on case reports has linked measles vaccine and measles infection to subsequent death in some severely immunocompromised children. Of the greater than 200 million doses of measles vaccine administered in the United States, fewer than five such deaths have been reported (5). Patients who have such conditions or are undergoing such therapies (excluding most HIV-infected patients) should not be given live measles virus vaccine. Patients with leukemia in remission who have not received chemotherapy for at least 3 months may receive live-virus vaccines. The exact amount of systemically absorbed corticosteroids and the duration of administration needed to suppress the immune system of an otherwise healthy child are not well defined. Most experts agree that steroid therapy usually does not contraindicate administration of live virus vaccine when it is short term (i.e., less than 2 weeks); low to moderate dose; long-term, alternate-day treatment with short-acting preparations; maintenance physiologic doses (replacement therapy); or administered topically (skin or eyes), by aerosol, or by intra-articular, bursal, or tendon injection (44). Although of recent theoretical concern, no evidence of increased severe reactions to live vaccines has been reported among persons receiving steroid therapy by aerosol, and such therapy is not in itself a reason to delay vaccination. The immunosuppressive effects of steroid treatment vary, but many clinicians consider a dose equivalent to either 2 mg/kg of body weight or a total of 20 mg per day of prednisone as sufficiently immunosuppressive to raise concern about the safety of vaccination with live virus vaccines (44). Corticosteroids used in greater than physiologic doses also can reduce the immune response to vaccines. Physicians should wait at least 3 months after discontinuation of therapy before administering a live-virus vaccine to patients who have received high systemically absorbed doses of corticosteroids for greater than or equal to 2 weeks. HIV-Infected Persons. Because of the increased risk for severe complications associated with measles infection and the absence of serious adverse events after measles vaccination among HIV-infected persons (41,45), ACIP has recommended that MMR vaccine be administered to all asymptomatic HIV-infected persons and that MMR vaccine be considered for administration to all symptomatic HIV-infected persons who would otherwise be eligible for measles vaccine -- even though the immune response may be attenuated in such persons (41,44,45). There is a theoretical risk for an increase (probably transient) in HIV viral load following MMR vaccination because such effects have been observed with other vaccines (46,47). Because of the recently reported case of pneumonitis in a measles vaccinee who had an advanced case of acquired immunodeficiency syndrome (AIDS) (48) and because of other evidence indicating a diminished antibody response to measles vaccination among severely immunocompromised persons (49), ACIP is re-evaluating the recommendations for vaccination of severely immunocompromised HIV-infected persons. In the interim, it may be prudent to withhold MMR or other measles-containing vaccines from HIV-infected persons with evidence of severe immunosuppression, defined as either a) CD4+ T-lymphocyte counts less than 750 for children ages less than 12 months, less than 500 for children ages 1-5 years, or less than 200 for persons ages greater than or equal to 6 years; or b) CD4+ T-lymphocytes constituting less than 15% of total lymphocytes for children ages less than 13 years or less than 14% for persons ages greater than or equal to 13 years (50,51). ACIP continues to recommend MMR for HIV-infected persons without evidence of measles immunity (47) who are not severely immunocompromised (50,51). Severely immunocompromised and other symptomatic HIV-infected patients who are exposed to measles should receive immune globulin (IG), regardless of prior vaccination status (44). In addition, health-care providers should weigh the risks and benefits of measles vaccination or IG prophylaxis for severely immunocompromised HIV-infected patients who are at risk for measles exposure because of outbreaks or international travel. Because the immunologic response to both live and killed antigen vaccines may decrease as HIV disease progresses (44,52), vaccination early in the course of HIV infection may be more likely to induce an immune response. Therefore, HIV-infected infants without severe immunosuppression should routinely receive MMR as soon as possible upon reaching their first birthday. Evaluation and testing of asymptomatic persons to identify HIV infection are not necessary before deciding to administer MMR or other measles-containing vaccine (44). Management of Patients with Contraindications to Measles Vaccine If immediate protection against measles is required for persons with contraindications to measles vaccination, passive immunization with IG, 0.25 mL/kg (0.11 mL/lb) of body weight (maximum dose=15 mL), should be given as soon as possible after known exposure. Exposed symptomatic HIV-infected and other immunocompromised persons should receive IG regardless of their previous vaccination status; however, IG in usual doses may not be effective in such patients. For immunocompromised persons, the recommended dose is 0.5 mL/kg of body weight if IG is administered intramuscularly (maximum dose=15 mL). This corresponds to a dose of protein of approximately 82.5 mg/kg (maximum dose=2,475 mg). Intramuscular IG may not be needed if a patient with HIV infection is receiving 100-400 mg/kg IGIV at regular intervals and the last dose was given within 3 weeks of exposure to measles. Because the amounts of protein administered are similar, high-dose IGIV may be as effective as IG given intramuscularly. However, no data are available concerning the effectiveness of IGIV in preventing measles. Simultaneous Administration of Vaccines In general, simultaneous administration of the most widely used live and inactivated vaccines does not impair antibody responses or increase rates of adverse reactions (53). The administration of MMR vaccine yields results similar to the administration of individual measles, mumps, and rubella vaccines at different sites or at different times. Vaccines recommended for administration at 12-15 months of age can be administered at either one or two visits. There are equivalent antibody responses and no clinically significant increases in the frequency of adverse events when DTP, MMR, and OPV (or IPV) vaccines and H. influenzae type b conjugate vaccine (HbCV) are administered either simultaneously at different sites or at separate times. If a child might not be brought back for future vaccinations, all vaccines (including DTP {or DTaP}, OPV {or IPV}, MMR, varicella, HbCV, and hepatitis B vaccines) may be administered simultaneously, as appropriate to the child's age and previous vaccination status. MUMPS PREVENTION The following recommendations concerning adverse events associated with mumps vaccination update those applicable sections in "Mumps Prevention" (MMWR 1989;38:388-92,397-400), and they apply regardless of whether the vaccine is administered as a single antigen or as a component of MR or MMR vaccine. Information concerning adverse events associated with the measles component of MMR vaccine is reviewed earlier in this document (see Measles Prevention), and information concerning the rubella component is located in the previously published ACIP statement for rubella (18). Adverse Effects of Vaccine Use In field trials before licensure, illnesses did not occur more often in vaccinees than in unvaccinated controls (54). Reports of illnesses following mumps vaccination have mainly been episodes of parotitis and low-grade fever. Allergic reactions including rash, pruritus, and purpura have been temporally associated with mumps vaccination but are uncommon and usually mild and of brief duration. The reported occurrence of encephalitis within 30 days of receipt of a mumps-containing vaccine (0.4 per million doses) is not greater than the observed background incidence rate of CNS dysfunction in the normal population. Aseptic meningitis has been epidemiologically associated with receipt of the vaccine containing the Urabe strain of mumps virus, but not with the vaccine containing the Jeryl Lynn strain, the latter of which is used in vaccine distributed in the United States (5). During 1988-1992, 15 sentinel surveillance laboratories in the United Kingdom identified 13 aseptic meningitis cases that had occurred within 15-35 days after vaccination with the Urabe strain (i.e., 91 cases per 1 million doses distributed) (55). No vaccine-associated aseptic meningitis cases have been reported since 1992, when only the Jeryl Lynn strain has been used (23). Febrile seizures also have been infrequently reported. However, no evidence suggests that mumps vaccine causes residual seizure disorder (5). Although sensorineural deafness following mumps vaccination has been reported rarely, the data are inadequate to distinguish vaccine from nonvaccine causation. No association has been established between mumps vaccination and pancreatic damage or subsequent development of diabetes mellitus (5). Contraindications to Vaccine Use Pregnancy Although mumps vaccine virus has been shown to infect the placenta and fetus (56), there is no evidence that it causes congenital malformations in humans. However, because of the theoretical risk of fetal damage, it is prudent to avoid giving live virus vaccine to pregnant women. Live mumps vaccine, when combined with rubella vaccine, should not be administered to women known to be pregnant or who are considering becoming pregnant within the next 3 months. Women vaccinated with monovalent mumps vaccine should avoid becoming pregnant for 30 days after the vaccination. Routine precautions for vaccinating postpubertal women include asking if they are or may be pregnant, excluding those who say they are, and explaining the theoretical risk to those who plan to receive the vaccine. Vaccination during pregnancy should not be considered an indication for termination of pregnancy. However, the final decision about interruption of pregnancy must rest with the individual patient and her physician. Severe Febrile Illness Vaccine administration should not be postponed because of minor or intercurrent febrile illnesses, such as mild upper respiratory infections. However, vaccination of persons with severe febrile illnesses should generally be deferred until they have recovered from the acute phase of the illness. Allergic Reactions Hypersensitivity reactions rarely occur after the administration of MMR or any of its component vaccines. Most of these reactions are minor and consist of a wheal and flare or urticaria at the injection site. Immediate, anaphylactic reactions to MMR or its component vaccines are extremely rare. Although greater than 70 million doses of MMR vaccine have been distributed in the United States since VAERS was implemented in 1990, only 33 cases of anaphylactic reactions that occurred after MMR vaccination have been reported. Furthermore, only 11 of these cases a) occurred immediately after vaccination and b) occurred in persons who had symptoms consistent with anaphylaxis (CDC, unpublished data). In the past, persons who had a history of anaphylactic reactions (i.e., hives, swelling of the mouth or throat, difficulty breathing, hypotension, and shock) following egg ingestion were considered to be at increased risk for serious reactions after receipt of mumps-containing vaccines, which are produced in chick embryo fibroblasts. Protocols requiring caution were developed for skin testing and vaccinating persons who had had anaphylactic reactions after egg ingestion (30-34). However, the predictive value of such skin testing and the need for special protocols when vaccinating egg-allergic persons with mumps-containing vaccines is uncertain. The results of recent studies suggest that anaphylactic reactions to mumps-containing vaccines are not associated with hypersensitivity to egg antigens but with some other component of the vaccines. The risk for serious allergic reaction to these vaccines in egg-allergic patients is extremely low, and skin testing is not necessarily predictive of vaccine hypersensitivity (35-37). Therefore, ACIP is re-evaluating whether skin testing and the use of special protocols are routinely necessary when administering mumps-containing vaccines to persons who have a history of anaphylactic-like reactions after egg ingestion. MMR and its component vaccines contain hydrolyzed gelatin as a stabilizer. The literature contains a single case report of a person with an anaphylactic sensitivity to gelatin who had an anaphylactic reaction after receipt of the MMR vaccine licensed in the United States (38). Similar cases have occurred in Japan (39). Therefore, ACIP is currently considering recommendations for vaccination of persons who have had an anaphylactic reaction to gelatin or gelatin-containing products. In the meantime, such persons should be vaccinated with MMR or other mumps vaccines with extreme caution. Since mumps vaccine contains trace amounts of neomycin (25 ug), persons who have experienced anaphylactic reactions to topically or systemically administered neomycin should not receive mumps vaccine. Most often, neomycin allergy is manifested as a contact dermatitis, which is a delayed-type (cell-mediated) immune response, rather than anaphylaxis. In such persons, the adverse reaction, if any, to 25 ug of neomycin in the vaccine would be an erythematous, pruritic nodule or papule at the site of injection after 48-96 hours. A history of contact dermatitis to neomycin is not a contraindication to receiving mumps vaccine. Live mumps virus vaccine does not contain penicillin. Recent Injection of Immune Globulin The effect of immune globulin preparations on the response to mumps vaccine is unknown, but commercial immune globulin preparations contain mumps antibodies. Therefore, monovalent mumps or rubella-mumps vaccine should be given at least 2 weeks before the administration of an immune globulin preparation or deferred until approximately 3 months after the administration of an immune globulin preparation. For suggested time intervals between administration of immune globulin preparations and vaccines containing live measles virus, refer to (Table_5). Altered Immunocompetence In theory, replication of the mumps vaccine virus may be potentiated in patients with immune deficiency diseases and by the suppressed immune responses that occur with leukemia, lymphoma, or generalized malignancy or with therapy with corticosteroids, alkylating drugs, antimetabolites, or radiation. In general, patients with such conditions should not be given live mumps virus vaccine. Because vaccinated persons do not transmit mumps vaccine virus, the risk of mumps exposure for those patients may be reduced by vaccinating their close susceptible contacts. An exception to these general recommendations is in persons infected with HIV; asymptomatic HIV-infected children should receive MMR as soon as possible upon reaching their first birthday (44), and MMR vaccine should be considered for all symptomatic HIV-infected children who do not have evidence of severe immunosuppression (see Measles Prevention, Altered Immunocompetence). Patients with leukemia in remission whose chemotherapy has been terminated for at least 3 months may also receive live mumps virus vaccine. Most experts agree that steroid therapy usually does not contraindicate administration of live virus vaccine when it is short term (i.e., less than 2 weeks); low to moderate dose; long-term, alternate-day treatment with short-acting preparations; maintenance physiologic doses (replacement therapy); or administered topically (skin or eyes), by aerosol, or by intraarticular, bursal, or tendon injection (44). However, mumps vaccine should be avoided if systemic immunosuppressive levels are reached by prolonged, extensive, topical application. DTP The following recommendations concerning adverse events associated with DTP vaccination update those applicable sections in "Diphtheria, Tetanus, and Pertussis: Recommendations for Vaccine Use and Other Preventive Measures -- Recommendations of the Immunization Practices Advisory Committee (ACIP)" (MMWR 1991;40{No. RR-10}). Side Effects and Adverse Reactions Following DTP Vaccination Local reactions (generally erythema and induration with or without tenderness) are common after the administration of vaccines containing diphtheria, tetanus, or pertussis antigens. Occasionally, a nodule may be palpable at the injection site of adsorbed products for several weeks. Sterile abscesses at the injection site have been reported rarely (6-10 events per million doses of DTP). Mild systemic reactions such as fever, drowsiness, fretfulness, and anorexia occur frequently. These reactions are substantially more common following the administration of DTP than of DT, but they are self-limited and can be safely managed with symptomatic treatment. Acetaminophen is frequently given by physicians to lessen fever and irritability associated with DTP vaccination, and it may be useful in preventing seizures among febrile-convulsion-prone children. However, fever that does not begin until greater than or equal to 24 hours after vaccination or persists for more than 24 hours after vaccination should not be assumed to be due to DTP vaccination. These new or persistent fevers should be evaluated for other causes so that treatment is not delayed for serious conditions such as otitis media or meningitis. Moderate-to-severe systemic events include high fever (i.e., temperature of greater than or equal to 40.5 C {greater than or equal to 105 F}); persistent, inconsolable crying lasting greater than or equal to 3 hours; collapse (hypotonic-hyporesponsive episode); or short-lived convulsions (usually febrile). These events occur infrequently. These events appear to be without sequelae (57-59). Other more severe neurologic events, such as a prolonged convulsion or encephalopathy, although rare, have been reported in temporal association with DTP administration. Approximate rates for the occurrence of adverse events following receipt of DTP (regardless of dose number in the series or age of the child) are shown in (Table_6) (60,61). The frequencies of local reactions and fever are substantially higher with increasing numbers of doses of DTP, while other mild-to-moderate systemic reactions (e.g., fretfulness, vomiting) are substantially less frequent (59-61). Concern about the possible role of pertussis vaccine in causing neurologic reactions has been present since the earliest days of vaccine use. Rare but serious acute neurologic illnesses, including encephalitis/encephalopathy and prolonged convulsions, have been anecdotally reported following receipt of whole-cell pertussis vaccine given as DTP (62,63). Whether pertussis vaccine causes or is only coincidentally related to such illnesses or reveals an inevitable event has been difficult to determine conclusively for the following reasons: a) serious acute neurologic illnesses often occur or become manifest among children during the first year of life irrespective of vaccination; b) there is no specific clinical sign, pathologic finding, or laboratory test which can determine whether the illness is caused by the DTP; c) it may be difficult to determine with certainty whether infants less than 6 months of age are neurologically normal, which complicates assessment of whether vaccinees were already neurologically impaired before receiving DTP; and d) because these events are exceedingly rare, appropriately designed large studies are needed to address the question. Despite these methodologic difficulties, the National Childhood Encephalopathy Study (NCES) and other controlled epidemiologic studies have provided evidence that DTP can cause acute encephalopathy (64-68). This adverse event occurs rarely, with an estimated risk of zero to 10.5 episodes per million DTP vaccinations (68). A detailed follow-up of the NCES indicated that children who had had a serious acute neurologic illness after DTP administration were significantly more likely than children in the control group to have chronic nervous system dysfunction 10 years later. These children with chronic nervous system dysfunction were more likely than children in the control group to have received DTP within 7 days of onset of the original serious acute neurologic illness (i.e., 12 {3.3%} of 367 children vs. six {0.8%} of 723 children) (69). After reviewing the follow-up data, IOM concluded that the NCES provided evidence of an association between DTP and chronic nervous system dysfunction in children who had had a serious acute neurologic illness after vaccination with DTP. The committee proposed three possible explanations for this association. First, the acute neurologic illness and subsequent chronic nervous system dysfunction might have been caused by DTP. Second, DTP might trigger an acute neurologic illness and subsequent chronic nervous system dysfunction in children who have underlying brain or metabolic abnormalities. Such children might experience similar chronic dysfunction in the absence of DTP vaccination if other stimuli (e.g., fever or infection) are present. Third, DTP might cause an acute neurologic illness in children who have underlying brain or metabolic abnormalities that would inevitably have led to chronic nervous system dysfunction even if the acute neurologic illness had not developed (6). IOM concluded that the NCES data do not support one explanation over another. According to IOM, the balance of evidence was consistent with a causal relationship between DTP and some forms of chronic nervous system disorders in children who had developed an acute neurologic disorder after receiving DTP. However, IOM also concluded that the results were insufficient to determine whether DTP increases the overall risk for chronic nervous system dysfunction in children. A subcommittee of the National Vaccine Advisory Committee (NVAC) also reviewed the study and concluded that the results were insufficient to determine whether DTP administration before the acute neurologic event influenced the potential for neurologic dysfunction 10 years later (Ad hoc Subcommittee of the NVAC, unpublished data, 1994). ACIP concurs with this evaluation. Although the NCES examined and reported risk for the 7 days after DTP vaccination, the increased risk for serious acute neurologic illness occurred primarily during the first 3 days after DTP administration (64). Thus, if an association between DTP and chronic encephalopathy exists, the risk is primarily in the first 3 days after DTP vaccination. Among a subset of children who were participating in the NCES and who had infantile spasms, both DTP and DT vaccination appeared either to precipitate early manifestations of the condition or to lead to its identification by parents (70). IOM reviewed this and other studies and concluded that neither vaccine causes the illness (71,72). Sudden infant death syndrome (SIDS) is listed on death certificates as the cause of death for 5,000-6,000 infants (ages 0-364 days) each year in the United States. Because the peak incidence of SIDS for infants occurs at 2-4 months of age, many instances of a close temporal relation between SIDS and receipt of DTP are to be expected by simple chance. Only one methodologically rigorous study has suggested that DTP vaccination might cause SIDS (73). A total of four deaths were reported within 3 days of DTP vaccination, compared with 1.36 expected deaths. However, these deaths were unusual in that three of the four occurred within a 13-month interval during the 12-year study. These four children also tended to be vaccinated at older ages than their controls, suggesting that they might have had other unrecognized risk factors for SIDS independent of vaccination. In contrast, DTP vaccination was not associated with SIDS in several larger studies performed in the past decade (62,74-76). In addition, none of three studies that examined unexpected deaths among infants not classified as SIDS found an association with DTP vaccination (73,75,76). IOM reviewed these studies and concluded that the available information does not establish a causal relationship between DTP and SIDS (4). IOM concluded recently that no available evidence indicates that DTP might cause transverse myelitis, other more subtle neurologic disorders (e.g., hyperactivity, learning disorders, and infantile autism), and progressive degenerative conditions of the CNS (4). Furthermore, one study indicated that children who received pertussis vaccine exhibited fewer school problems than those who did not, even after adjustment for socioeconomic status (77). Recent data suggest that infants and young children who have ever had convulsions (febrile or afebrile) or who have immediate family members with such histories are more likely to have seizures following DTP vaccination than those without such histories (78,79). For those with a family history of seizures, the increased risks of seizures occurring within 3 days of receipt of DTP or 4-28 days following receipt of DTP are identical, suggesting that these histories are nonspecific risk factors and are unrelated to DTP vaccination (79). Rarely, immediate anaphylactic reactions (i.e., swelling of the mouth, breathing difficulty, hypotension, or shock) have been reported after receipt of preparations containing diphtheria, tetanus, and/or pertussis antigens. However, no deaths caused by anaphylaxis following DTP vaccination have been reported to CDC since the inception of vaccine-adverse-events reporting in 1978, a period during which more than 80 million doses of publicly purchased DTP vaccine were administered. While substantial underreporting exists in this passive surveillance system, the severity of anaphylaxis and its immediacy following vaccination suggest that such events are likely to be reported. Although no causal relation to any specific component of DTP has been established, the occurrence of true anaphylaxis usually contraindicates further doses of any one of these components. Rashes that are macular, papular, petechial, or urticarial and appear hours or days after a dose of DTP are frequently antigen-antibody reactions of little consequence or are due to other causes, such as viral illnesses, and are unlikely to recur following subsequent injections (80,81). In addition, there is no evidence for a causal relation between DTP vaccination and hemolytic anemia or thrombocytopenic purpura. Precautions and Contraindications General Considerations The decision to administer or delay DTP vaccination because of a current or recent febrile illness depends largely on the severity of the symptoms and their etiology. Although a moderate or severe febrile illness is sufficient reason to postpone vaccination, minor illnesses such as mild upper-respiratory infections with or without low-grade fever are not contraindications. If ongoing medical care cannot be assured, taking every opportunity to provide appropriate vaccinations is particularly important. Children with moderate or severe illnesses with or without fever can receive DTP as soon as they have recovered. Waiting a short period before administering DTP avoids superimposing the adverse effects of the vaccination on the underlying illness or mistakenly attributing a manifestation of the underlying illness to vaccination. Routine physical examinations or temperature measurements are not prerequisites for vaccinating infants and children who appear to be in good health. Appropriate immunization practice includes asking the parent or guardian if the child is ill, postponing DTP vaccination for those with moderate or severe acute illnesses, and vaccinating those without contraindications or precautionary circumstances. When an infant or child returns for the next dose of DTP, the parent should always be questioned about any adverse events that might have occurred following the previous dose. A history of prematurity generally is not a reason to defer vaccination (82-84). Preterm infants should be vaccinated according to their chronological age from birth. Immunosuppressive therapies -- including irradiation, antimetabolites, alkylating agents, cytotoxic drugs, and corticosteroids (used in greater than physiologic doses) -- may reduce the immune response to vaccines. Short-term (less than 2-week) corticosteroid therapy or intra-articular, bursal, or tendon injections with corticosteroids should not be immunosuppressive. Although no specific studies with pertussis vaccine are available, if immunosuppressive therapy will be discontinued shortly, it is reasonable to defer vaccination until the patient has been off therapy for 1 month; otherwise, the patient should be vaccinated while still on therapy (85). Special Considerations for Preparations Containing Pertussis Vaccine Precautions and contraindications guidelines that were previously published regarding the use of pertussis vaccine were based on three assumptions about the risks for adverse events associated with pertussis vaccination: a) that the vaccine on rare occasions caused acute encephalopathy resulting in permanent brain damage; b) that pertussis vaccine aggravated preexisting CNS disease; and c) that certain nonencephalitic reactions are predictive of more severe reactions with subsequent doses (86). In addition, children from whom pertussis vaccine was withheld were thought to be well protected by herd immunity, a belief that is no longer valid. The current revised ACIP recommendations reflect better understanding of the risks associated not only with pertussis vaccine but also with pertussis disease. Contraindications If any of the following events occur in temporal relationship to the administration of DTP, further vaccination with DTP is contraindicated (Table_7):
Precautions If any of the following events occur in temporal relation to receipt of DTP, the decision to give subsequent doses of vaccine containing the pertussis component should be carefully considered (Table_7). Although these events were considered absolute contraindications in previous ACIP recommendations, there may be circumstances, such as a high incidence of pertussis, in which the potential benefits outweigh possible risks, particularly because these events are not associated with permanent sequelae (86). The following events were previously considered contraindications and are now considered precautions:
Vaccination of infants and young children who have underlying neurologic disorders Infants and children with recognized, possible, or potential underlying neurologic conditions present a unique problem. They seem to be at increased risk for the appearance of manifestations of the underlying neurologic disorder within 2-3 days after vaccination. However, more prolonged manifestations or increased progression of the disorder or exacerbation of the disorder as a result of DTP vaccination have not been recognized (94). In addition, most neurologic conditions in infancy and young childhood are associated with evolving, changing neurological findings. Functional abnormalities are often unmasked by progressive neurologic development. Thus, confusion over the interpretation of progressive neurologic signs may arise when DTP vaccination or any other therapeutic or preventive measure is carried out. Protection against diphtheria, tetanus, and pertussis is as important for children with neurologic disabilities as for other children. Such protection may be even more important for neurologically disabled children. They often receive custodial care or attend special schools where the risk of pertussis is greater because DTP vaccination is avoided for fear of adverse reactions. Also, if pertussis affects a neurologically disabled child who has difficulty in handling secretions and in cooperating with symptomatic care, it may aggravate preexisting neurologic problems because of anoxia, intracerebral hemorrhages, and other manifestations of the disease. Whether and when to administer DTP to children with proven or suspected underlying neurologic disorders must be decided on an individual basis. Important considerations include the current local incidence of pertussis, the near absence of diphtheria in the United States, and the low risk of infection with Clostridium tetani. On the basis of these considerations and the nature of the child's disorder, the following approaches are recommended:
Vaccination of infants and young children who have a family history of convulsion or other CNS disorder A family history of convulsions or other CNS disorder is not a contraindication to pertussis vaccination (95). Acetaminophen should be given at the time of DTP vaccination and every 4 hours for 24 hours to reduce the possibility of postvaccination fever (92,93). Preparations Containing Diphtheria Toxoid and Tetanus Toxoid The only contraindication to tetanus and diphtheria toxoids is a history of a neurologic or severe hypersensitivity reaction following a previous dose. Vaccination with tetanus and diphtheria toxoids is not known to be associated with an increased risk of convulsions. Local side effects alone do not preclude continued use. If an anaphylactic reaction to a previous dose of tetanus toxoid is suspected, intradermal skin testing with appropriately diluted tetanus toxoid may be useful before a decision is made to discontinue tetanus toxoid vaccination (86). In one study, 94 of 95 persons with histories of anaphylactic symptoms following a previous dose of tetanus toxoid were nonreactive following intradermal testing and tolerated further tetanus toxoid challenge without incident (86). One person had erythema and induration immediately following skin testing, but tolerated a full IM dose without adverse effects. Mild, nonspecific skin-test reactivity to tetanus toxoid, particularly if used undiluted, appears to be fairly common. Most vaccinees develop inconsequential cutaneous delayed hypersensitivity to the toxoid. Although very rare, severe hypersensitivity reactions may occur after receipt of tetanus-toxoid-containing vaccines; these reactions can be life-threatening (5). Persons who experienced Arthus-type hypersensitivity reactions or a temperature of greater than 103 F ( greater than 39.4 C) following a prior dose of tetanus toxoid usually have high serum tetanus antitoxin levels and should not be given even emergency doses of Td more frequently than every 10 years, even if they have a wound that is neither clean nor minor. If a contraindication to using tetanus-toxoid-containing preparations exists for a person who has not completed a primary series of tetanus toxoid immunization and that person has a wound that is neither clean nor minor, only passive immunization should be given using tetanus IG (TIG). On the basis of a) a report of a 42-year-old man who had GBS on three separate occasions after receipt of tetanus toxoid and b) evidence that a vaccine-induced immunologic response can cause GBS, IOM concluded that tetanus-toxoid-containing vaccines can trigger the onset of GBS in adults. GBS can be a life-threatening disease. Persons who have a history of GBS associated with a particular vaccine may be at increased risk for recurrent GBS after subsequent doses of that vaccine (5). However, in a study in which an estimated 1.2 million doses of tetanus-containing toxoid were administered to persons greater than 18 years of age, two cases of GBS were expected by chance alone during the 6 weeks after vaccination, and only one case was reported (CDC, unpublished data). This finding suggests that the risk for GBS after administration of tetanus toxoid is extremely low. No increased risk for GBS has been observed with the use of DTP in children. In a study of 0.7 million children of preschool-ages who were vaccinated with DTP during a 7-year period, three cases of GBS were expected by chance alone during the 6 weeks after vaccination, and only two cases were reported (17). Because tetanus vaccination has been associated rarely with recurrence of GBS, the decision to administer additional doses of tetanus-toxoid-containing vaccine to persons who have had GBS within 6 weeks after receiving tetanus toxoid should be based on the benefits of subsequent vaccination and the risk for recurrence of GBS. For example, vaccination is usually justified for children whose primary immunization schedules are incomplete (i.e., fewer than three doses have been received); but routine booster vaccination probably is not indicated for adults who have received three or more doses. Vaccination with tetanus-toxoid-containing vaccines has been associated with brachial neuritis in adult vaccinees, with a relative risk of 5-10 in comparison with the population-based background incidence and a 1-month attributable incidence of approximately one-half to one case per 100,000 recipients of tetanus toxoid (5). Although no evidence exists that tetanus and diphtheria toxoids are teratogenic, waiting until the second trimester of pregnancy to administer Td is a reasonable precaution for minimizing any concern about the theoretical possibility of such reactions. Misconceptions Concerning Contraindications to DTP Some health-care providers inappropriately consider certain conditions or circumstances as contraindications to DTP vaccination. These include the following:
References
+------------------------------------------------------------------- --+ | Erratum: Vol. 45, No. RR-12 | | =========================== | | SOURCE: MMWR 46(10) DATE: Mar 14, 1997 | | | | In the MMWR Recommendations and Reports entitled "Update: | | Vaccine Side Effects, Adverse Reactions, Contraindications, and | | Precautions -- Recommendations of the Advisory Committee on | | Immunization Practices (ACIP)," the first complete paragraph on | | page 10 should read: "OPV should not be administered to persons | | who have experienced an anaphylactic reaction to a previous dose | | of OPV." The next paragraph should read: "IPV should not be | | administered to persons who have experienced a) an anaphylactic | | reaction following a previous dose of IPV or b) an anaphylactic | | reaction to streptomycin, polymyxin B, or neomycin." | +------------------------------------------------------------------- --+ Table_1 Note: To print large tables and graphs users may have to change their printer settings to landscape and use a small font size. TABLE 1. The maximum number of cases of specified vaccine-preventable diseases ever reported for a calendar year compared with the number of cases of disease and vaccine adverse events reported for 1995 -- United States =================================================================================================== Maximum no. reported Year(s) Reported Percentage cases during maximum no. no. cases change in Category prevaccine era cases reported during 1995 * morbidity ------------------------------------------------------------------------------------------------- Disease Congenital rubella syndrome 20,000 + 1964-65 7 (-99.96) Diphtheria 206,939 1921 0 (-99.99) Invasive Haemophilus influenzae 20,000 + 1984 1,164 (-94.18) Measles 894,134 1941 309 (-99.97) Mumps 152,209 1968 840 (-99.45) Pertussis 265,269 1934 4,315 (-98.37) Poliomyelitis (wild) 21,269 1952 0 (-99.99) Rubella 57,686 1969 146 (-99.75) Tetanus 601 1948 34 (-97.82) Vaccine adverse events & 0 10,594 ------------------------------------------------------------------------------------------------- * Provisional totals. + Estimated because national reporting did not exist in the prevaccine era. & Total number reported to the Vaccine Adverse Events Reporting System (VAERS). =================================================================================================== Return to top. Table_2 Note: To print large tables and graphs users may have to change their printer settings to landscape and use a small font size. TABLE 2. Summarized conclusions of evidence regarding the possible association between specific adverse effects and receipt of diphtheria and tetanus toxoids and pertussis vaccine (DTP) * and RA 27/3 measles-mumps-rubella (MMR) + vaccine, by determination of causality -- Institute of Medicine, 1991 & =================================================================================================== Adverse event reviewed Conclusion, by determination ---------------------------------------------------------- of casuality DTP vaccine RA 27/3 MMR ------------------------------------------------------------------------------------------------ 1. No evidence was available to Autism None establish a causal relationship 2. Inadequate evidence to accept Aseptic meningitis Radiculoneuritis and or reject a causal relationship Chronic neurologic damage @ other neuropathies Erythema multiforme or other rash Thrombocytopenic Guillain-Barre syndrome purpura Hemolytic anemia Juvenile diabetes Learning disabilities and attention-deficit disorder Peripheral mononeuropathy Thrombocytopenia 3. Evidence favored rejection of a Infantile spasms None causal relationship Hypsarrythmia Reye syndrome Sudden infant death syndrome 4. Evidence favored acceptance of Acute encephalopathy ** Chronic arthritis a causal relationship Shock and unusual shock-like state 5. Evidence established a causal Anaphylaxis Acute arthritis relationship Protracted, inconsolable crying ------------------------------------------------------------------------------------------------ * The evidence only differentiated between components of DTP in the event of protracted, inconsolable crying, for which the evidence specifically implicated the pertussis vaccine component. + Trivalent MMR vaccine containing the RA 27/3 rubella strain. & This table is an adaptation of a table published previously by the Institute of Medicine (IOM) (4), an independent research organization chartered by the National Academy of Sciences. The National Childhood Vaccine Injury Act of 1986 mandated that IOM review scientific and other evidence (e.g., epidemiologic studies, case series, individual case reports, and testimonials) regarding the possible adverse consequences of vaccines administered to children. IOM constituted an expert committee to review and summarize all available information; this committee created five categories of causality to describe the relationships between the vaccines and specific adverse events. @ IOM reviewed this adverse event again in 1994 (5). ** Defined in the controlled studies that were reviewed as encephalopathy, encephalitis, or encephalomyelitis. =================================================================================================== Return to top. Table_3 Note: To print large tables and graphs users may have to change their printer settings to landscape and use a small font size. TABLE 3. Summarized conclusions of evidence regarding the possible association between specific adverse effects and receipt of childhood vaccines, by determination of causality -- Institute of Medicine, 1994 * =================================================================================================================================================================== Haemophilus influenzae DT/Td/Tetanus toxoid + Measles vaccine & Mumps vaccine & OPV/IPV @ Hepatitis B vaccine type b (Hib) vaccine -------------------------------------------------------------------------------------------------------------------------------------------------- 1. No evidence was available to establish a causal relationship None None Neuropathy Transverse myelitis None None Residual seizure (IPV) disorder Thrombocytopenia (IPV) Anaphylaxis (IPV) 2. Inadequate evidence to accept or reject a causal relationship Residual seizure Encephalopathy Encephalopathy Transverse myelitis Guillain-Barre Guillain-Barre syndrome disorder other than Subacute sclerosing Aseptic meningitis (OPV) syndrome Transverse myelitis infantile spasms panencephalitis Sensorineural Guillain-Barre Demyelinating Thrombocytopenia Demyelinating Residual seizure deafness (MMR) syndrome (IPV) diseases of the Anaphylaxis diseases of the disorder Insulin-dependent Death from SIDS ++ central nervous Death from SIDS ++ central nervous Sensorineural diabetes mellitus system system deafness (MMR) Sterility Arthritis Mononeuropathy Optic neuritis Thrombocytopenia Death from SIDS ++ Arthritis Transverse myelitis Anaphylaxis ** Erythema multiforme Guillain-Barre syndrome Thrombocytopenia Insulin-dependent diabetes mellitus 3. Evidence favored rejection of a causal relationship Encephalopathy && None None None None Early onset Hib disease Infantile spasms (conjugate vaccines) (DT only) @@ Death from SIDS (DT only) @@ *** 4. Evidence favored acceptance of a causal relationship Guillain-Barre Anaphylaxis ** None Guillain-Barre None Early-onset Hib disease syndrome +++ &&& syndrome (OPV) &&& in children ages Brachial neuritis +++ >= 18 mos whose first Hib vaccination was with unconjugated PRP vaccine 5. Evidence established a causal relationship Anaphylaxis +++ Thrombocytopenia None Poliomyelitis in Anaphylaxis None (MMR) recipient or contact Anaphylaxis (MMR) ** (OPV) Death from measles- Death from polio- vaccine-strain viral vaccine-strain viral infection ++ @@@ infection ++ @@@ -------------------------------------------------------------------------------------------------------------------------------------------------- * This table is an adaptation of a table published previously by the Institute of Medicine (IOM) (5), an independent research organization chartered by the National Academy of Sciences. The National Childhood Vaccine Injury Act of 1986 mandated that IOM review scientific and other evidence (e.g., epidemiologic studies, case series, individual case reports, and testimonials) regarding the possible adverse consequences of vaccines administered to children. IOM constituted an expert committee to review and summarize all available information; this committee created five categories of causality to describe the relationships between the vaccines and specific adverse events. + DT=diphtheria and tetanus toxoids for pediatric use; Td=diphtheria and tetanus toxoids for adult use. & If the data derived from studies of a monovalent preparation, then the causal relationship also extended to multivalent preparations. If the data derived exclusively from studies of the measles-mumps-rubella (MMR) vaccine, the vaccine is specified parenthetically in italics. In the absence of data concerning the monovalent preparation, the causal relationship determined for the multivalent preparations did not extend to the monovalent components. @ For some adverse events, the IOM committee was charged with assessing the causal relationship between the adverse event and only oral poliovirus vaccine (OPV) (i.e., for poliomyelitis) or only inactivated poliovirus vaccine (IPV) (i.e., for anaphylaxis and thrombocytopenia). If the conclusions for the two vaccines differed for the other adverse events, the vaccine to which the adverse event applied is specified parenthetically in italics. ** The evidence used to establish a causal relationship for anaphylaxis applies to MMR vaccine. The evidence regarding monovalent measles vaccine favored acceptance of a causal relationship, but this evidence was less convincing than that for MMR vaccine because of either incomplete documentation of symptoms or the possible attenuation of symptoms by medical intervention. ++ This table lists weight-of-evidence determinations only for deaths that were classified as sudden infant death syndrome (SIDS) and deaths that were a consequence of vaccine-strain viral infection. However, if the evidence favored the acceptance of (or established) a causal relationship between a vaccine and a possibly fatal adverse event, then the evidence also favored the acceptance of (or established) a causal relationship between the vaccine and death from the adverse event. Direct evidence regarding death in association with a vaccine-associated adverse event was limited to a) Td and Guillain-Barre syndrome, b) tetanus toxoid and anaphylaxis, and c) OPV and poliomyelitis. && The evidence derived from studies of DT. If the evidence favored rejection of a causal relationship between DT and encephalopathy, then the evidence also favored rejection of a causal relationship between Td and tetanus toxoid and encephalopathy. @@ Infantile spasms and SIDS occur only in an age group that is administered DT but not Td or tetanus toxoid. *** The evidence derived primarily from studies of DTP, although the evidence also favored rejection of a causal relationship between DT and SIDS. +++ The evidence derived from studies of tetanus toxoid. If the evidence favored acceptance of (or established) a causal relationship between tetanus toxoid and an adverse event, then the evidence also favored acceptance of (or established) a causal relationship between DT and Td and the adverse event. &&& This conclusion differs from the information contained in the ACIP recommendations because of new information that became available after IOM published this table. @@@ Deaths occurred primarily among persons known to be immunocompromised. =================================================================================================================================================================== Return to top. Figure_1 Return to top. Table_4 Note: To print large tables and graphs users may have to change their printer settings to landscape and use a small font size. TABLE 4. Guidelines for spacing the administration of immune globulin preparations * and vaccines containing live measles, mumps, or rubella virus =================================================================================================================================== Simultaneous administration º Nonsimultaneous administration ---------------------------------------------------------------------+-------------------------------------------------------- º Immunobiologic administered Recommended Immunobiologic Recommended minimum interval º ---------------------------------- minimum interval combination between doses º First Second between doses ---------------------------------------------------------------------+-------------------------------------------------------- Immune globulin Should generally not be administered º Immune globulin Vaccine Dose related + and vaccine simultaneously. + If simultaneous administration º of measles-mumps-rubella {MMR}, º Vaccine Immune globulin 2 weeks measles-rubella, and monovalent measles º vaccine is unavoidable, administer at different º sites and revaccinate or test for seroconversion º after the recommended interval (Table 5). º ------------------------------------------------------------------------------------------------------------------------------ * Blood products containing large amounts of immune globulin (such as serum immune globulin, specific immune globulins {e.g., TIG and HBIG}, intravenous immune globulin {IGIV}, whole blood, packed red cells, plasma, and platelet products). + The duration of interference of immune globulin preparations with the immune response to the measles component of the MMR, measles-rubella, and monovalent measles vaccine is dose-related (Table 5). =================================================================================================================================== Return to top. Table_5 Note: To print large tables and graphs users may have to change their printer settings to landscape and use a small font size. TABLE 5. Suggested intervals between administration of immune globulin prep- arations for various indications and vaccines containing live measles virus * ================================================================================================= Time interval (mos) before measles Indication Dose (including mg IgG/kg) vaccination ---------------------------------------------------------------------------------------- Tetanus (TIG) prophylaxis 250 units (10 mg IgG/kg) IM 3 Hepatitis A (IG) prophylaxis Contact prophylaxis 0.02 mL/kg (3.3 mg IgG/kg) IM 3 International travel 0.06 mL/kg (10 mg IgG/kg) IM 3 Hepatitis B prophylaxis (HBIG) 0.06 mL/kg (10 mg IgG/kg) IM 3 Rabies immune globulin (HRIG) 20 IU/kg (22 mg IgG/kg) IM 4 Varicella prophylaxis (VZIG) 125 units/10 kg 5 (20-40 mg IgG/kg) IM (maximum 625 units) Measles prophylaxis (IG) Standard (i.e., nonimmunocompromised contact) 0.25 mL/kg (40 mg IgG/kg) IM 5 Immunocompromised contact 0.50 mL/kg (80 mg IgG/kg) IM 6 Blood transfusion: Red blood cells (RBCs), washed 10 mL/kg (negligible IgG/kg) IV 0 RBCs, adenine-saline added 10 mL/kg (10 mg IgG/kg) IV 3 Packed RBCs (Hct 65%) + 10 mL/kg (60 mg IgG/kg) IV 6 Whole blood cells (Hct 35%-50%) + 10 mL/kg (80-100 mg IgG/kg) IV 6 Plasma/platelet products 10 mL/kg (160 mg IgG/kg) IV 7 Replacement therapy for immune deficiencies 300-400 mg/kg IV & (as IGIV) 8 Treatment of: Immune thrombocytopenic purpura @ 400 mg/kg IV (as IGIV) 8 Immune thrombocytopenic purpura @ 1,000 mg/kg IV (as IGIV) 10 Kawasaki disease 2 g/kg IV (as IGIV) 11 ---------------------------------------------------------------------------------------- * This table is not intended for determining the correct indications and dosage for the use of immune globulin preparations. Unvaccinated persons may not be fully protected against measles during the entire suggested time interval, and additional doses of immune globulin and/or measles vaccine may be indicated after measles exposure. The concentration of measles antibody in a particular immune globulin preparation can vary by lot. The rate of antibody clearance after receipt of an immune globulin preparation also can vary. The recommended time intervals are extrapolated from an estimated half-life of 30 days for passively acquired antibody and an observed interference with the immune response to measles vaccine for 5 months after a dose of 80 mg IgG/kg (42). + Assumes a serum IgG concentration of 16 mg/mL. & Measles vaccination is recommended for most HIV-infected children who do not have evidence of severe immunosuppression, but it is contraindicated for patients who have congenital dis- orders of the immune system. @ Formerly referred to as idiopathic thrombocytopenic purpura. ================================================================================================= Return to top. Table_6 Note: To print large tables and graphs users may have to change their printer settings to landscape and use a small font size. TABLE 6. Adverse events * occurring within 48 hours after vaccination with diphtheria and tetanus toxoids and pertussis vaccine (DTP) ======================================================================================= Event Frequency of event + ----------------------------------------------------------------------------- Local reaction - Pain 1 per 2 doses - Swelling 2 per 5 doses - Redness 1 per 3 doses Systemic reaction - Fever >=100.4 F (>=38 C) 1 per 2 doses - Fretfulness 1 per 2 doses - Drowsiness 1 per 3 doses - Anorexia 1 per 5 doses - Vomiting 1 per 15 doses - Persistent, inconsolable crying (i.e., for >=3 hrs) 1 per 100 doses - Fever >=105 F (>=40.5 C) 1 per 330 doses - Collapse (hypotonic-hyporesponsive episode) 1 per 1,750 doses - Convulsions (with or without fever) 1 per 1,750 doses ----------------------------------------------------------------------------- * Adapted from Cody CL, Baraff LJ, Cherry JD, et al., 1981 (60). + Rate per total number of doses, regardless of dose number in DTP series. ======================================================================================= Return to top. Table_7 Note: To print large tables and graphs users may have to change their printer settings to landscape and use a small font size. TABLE 7. Contraindications and precautions to subsequent vaccination with diphtheria and tetanus toxoids and pertussis vaccine (DTP) ============================================================================================== Classification/Response to DTP vaccination -------------------------------------------------------------------------------------------- Contraindications - An immediate anaphylactic reaction. - Encephalopathy occurring within 7 days after vaccination. Precautions - Fever >=105 F (>=40.5 C) that is not attributed to another identifiable cause occurring within 48 hours after vaccination. - Collapse or shock-like state (i.e., a hypotonic-hyporesponsive episdode) occurring within 48 hours after vaccination. - Persistent, inconsolable crying lasting >=3 hours and occurring within 48 hours after vaccination. - Convulsions with or without fever occurring within 3 days after vaccination. -------------------------------------------------------------------------------------------- ============================================================================================== Return to top. Disclaimer All MMWR HTML versions of articles are electronic conversions from ASCII text into HTML. This conversion may have resulted in character translation or format errors in the HTML version. Users should not rely on this HTML document, but are referred to the electronic PDF version and/or the original MMWR paper copy for the official text, figures, and tables. An original paper copy of this issue can be obtained from the Superintendent of Documents, U.S. Government Printing Office (GPO), Washington, DC 20402-9371; telephone: (202) 512-1800. Contact GPO for current prices. **Questions or messages regarding errors in formatting should be addressed to mmwrq@cdc.gov.Page converted: 09/19/98 |
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