About
CDC vaccine recommendations are developed using an explicit evidence-based method based on the Grading of Recommendations, Assessment, Development and Evaluation (GRADE) approach.
Introduction
On October 21, 2021, the ACIP recommended use of 20-valent pneumococcal conjugate vaccine (PCV20 [Prevnar 20, Wyeth Pharmaceuticals LLC, a subsidiary of Pfizer Inc.]) alone or 15-valent pneumococcal conjugate vaccine (PCV15 [Vaxneuvance, Merck Sharp & Dohme Corp.]) in series with 23-valent pneumococcal polysaccharide vaccine (PPSV23) [Pneumovax23, Merck Sharp & Dohme Corp Inc.]) for all adults aged ≥65 years, and for adults aged 19–64 years with certain underlying medical conditions or other risk factors*, who have not previously received a pneumococcal conjugate vaccine or whose previous vaccination history is unknown. A systematic review and Grading of Recommendations, Assessment, Development and Evaluation (GRADE) approach was employed to guide ACIP’s deliberations regarding use of these vaccines.
Introduction Footnote
*Alcoholism, chronic heart/liver/lung disease, chronic renal failure, cigarette smoking, cochlear implant, congenital or acquired asplenia, CSF leak, diabetes mellitus, generalized malignancy, HIV, Hodgkin disease, immunodeficiency, iatrogenic immunosuppression, leukemia, lymphoma, multiple myeloma, nephrotic syndrome, solid organ transplants, or sickle cell disease or other hemoglobinopathies.
Methods
A systematic literature search was completed to review all available evidence on the immunogenicity and safety of PCV15 and PCV20 among age groups for which the vaccines were approved. Since only immunogenicity and safety data were available for PCV15 or PCV20, the search included PCV13 and PPSV23 efficacy or effectiveness studies to help interpret PCV15 and PCV20 immunogenicity study findings. Literature search for evidence on both PCV15 and PCV20 was done simultaneously given the similarities in the policy questions and given that use of both PCV15 and PCV20 were considered by the ACIP simultaneously. GRADE assessment was performed for PCV15 and PCV20 studies only. As a basis for the GRADE analysis, the policy question consisting of the population, intervention, comparison, and outcomes of interest was defined (Table 1).
Table 1. Policy Question and PICO
- Vaccine-type invasive pneumococcal disease, vaccine-type non-bacteremic pneumococcal pneumonia, and vaccine-type pneumococcal mortality
- Serious adverse events following immunization
Table 2. Outcomes and Rankings
| Outcome | Importance* | Included in evidence profile |
|---|---|---|
| Vaccine-type invasive pneumococcal disease | Critical | Yes |
| Vaccine-type non-bacteremic pneumococcal pneumonia | Critical | Yes |
| Vaccine-type pneumococcal mortality | Critical | Yes |
| Serious adverse events following immunization | Critical | Yes |
Table 2. Footnote
*Three options: 1. Critical; 2. Important but not critical; 3. Not important for decision making
We leveraged a systematic review presented to the World Health Organization Strategic Advisory Group of Experts (SAGE) meeting in October 2020, which included literature up to March 20191. To identify literature published during April 2019 to February 2021, we searched Pubmed, Medline, Embase, CINAHL, Scopus, Epistemonikos and Cochrane library databases. The search terms are included in the appendix I. Search results were supplemented by an updated Pubmed search using “V114*”, “PCV15”, “PCV20”. Unpublished data were provided by the vaccine manufacturers.
Studies were included if they presented primary data on PCV15 use in series with PPSV23 in adults aged ≥18 years. Of the 2,499 titles screened for WHO SAGE and 923 titles screened for the updated review in 2021, 3 unpublished PCV15 studies were included in the GRADE analysis234. Characteristics of these studies are presented in Table 2. Beneficial and harmful outcomes for the GRADE assessment were selected by the ACIP Pneumococcal Vaccine Work Group calls and via an email survey in which Work Group members were asked to rank the relative importance of each outcome. Vaccine-type invasive pneumococcal disease, vaccine-type non-bacteremic pneumococcal pneumonia, vaccine-type pneumococcal mortality, and serious adverse events (SAEs) following immunization were deemed to be critical outcomes (Table 2).
Methods Footnote
*V114 is the name used for Merck’s investigational 15-valent pneumococcal conjugate vaccine candidate
Table 3a. Summary of Studies Reporting Immunogenicity
| Study | Age or other characteristic of importance | N intervention | N comparison | Comparator vaccine | OPA GMT Ratios* (serotype) | Absolute difference in % seroresponders† (serotype) |
Interpretation | Study limitations (Risk of Bias) |
|---|---|---|---|---|---|---|---|---|
| V114-017 | Native Americans or adults with chronic medical conditions‡ aged 18-49 years th | GMT: 830-844 %seroresponders: 742-831 th |
GMT: 276-283 %seroresponders: 247-279 th |
PCV13 + PPSV23th (6-month interval between vaccines; 1-month post PPSV23) | 0.88 (4) to 1.42 (18C)th | -6.7 (6A) to 6.0 (14) th | GMT ratios
% seroresponders
|
Not seriousth |
| V114-018 | Adults ≥18 years of age with HIVth | GMT: 118-123 %seroresponders: 102-119 th |
GMT: 113-117 %seroresponders: 105-113 th |
PCV13 + PPSV23th (8-week interval between vaccines; 1-month post PPSV23) | 0.89 (6A) to 1.52 (5)th | -2.0 (3) to 15.0 (19F) th | GMT ratios
% seroresponders
|
Not seriousth |
| V114-016 | Adults ≥50 years of age th | GMT: 320-321 %seroresponders: 243-273th |
GMT: 322-323 %seroresponders:245-272th |
PCV13 + PPSV23th (12-month interval between vaccines; 1-month post PPSV23) | 1.03 (19F) to 1.38 (1)th | -1 (5) to 9.1 (1)th | GMT ratios
% serorespondersth
|
Not seriousth |
Table 3a. Footnotes
GMR=geometric mean ratio, GMT=geometric mean titers, OPA=opsonophagocytic activity, PCV13=13-valent pneumococcal conjugate vaccine, PCV15=15-valent pneumococcal conjugate vaccine, PPSV23=23-valent pneumococcal polysaccharide vaccine
*Ratio calculated as [GMT (PCV15)] / [GMT (comparator vaccine)]. Range of GMT ratios for 13 serotypes common to PCV13 and PCV15 is shown
†Seroresponse: subjects with >=4-fold rise in OPA GMT titer 30 days post-vaccination compared to pre-vaccination. Range is shown for the 13 serotypes shared between PCV13 and PCV15.
‡Chronic heart/liver/lung disease, cigarette smoking, diabetes mellitus
Table 3b. Summary of Studies Reporting Safety
| Study | Age or other characteristic of importance | N intervention | N comparison | Comparator vaccine | Absolute % difference (% SAE PCV15 – % SAE comparator) | N related to vaccine | Study limitations (Risk of Bias) |
|---|---|---|---|---|---|---|---|
| V114-017 | Native Americans or adults with chronic medical conditions* aged 18-49 years of age | 1036 | 345 | PCV13 + PPSV23 (1-month observation period post-PPSV23) | -0.6 | 0 | Not serious |
| V114-018 | Adults ≥18 years of age with HIV | 150 | 148 | PCV13 + PPSV23 (4-month observation period post-PPSV23) | -2.8 | 0 | Not serious |
| V114-016 | Adults ≥50 years of age | 298 | 302 | PCV13 + PPSV23 (1-month observation period post-PPSV23) | -0.4 | 0 | Not serious |
Table 3b. Footnotes
PCV13=13-valent pneumococcal conjugate vaccine, PCV20=20-valent pneumococcal conjugate vaccine, PPSV23=23-valent pneumococcal polysaccharide vaccine, SAE=serious adverse events
Table 4. GRADE Summary of Findings Table
| Certainty assessment | Number of patients | Results | Certainty | Importance | ||||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|
| № of studies (reference) | Study design | Risk of bias | Inconsistency | Indirectness | Imprecision | Other considerations | Intervention | Comparison | Relative effect | Absolute effect | ||
| Vaccine effectiveness (Vaccine-type invasive pneumococcal disease, Vaccine-type non-bacteremic pneumococcal pneumonia, Vaccine-type pneumococcal mortality) | ||||||||||||
| 3 (2-4) | Randomized studies | Not serious | Not serious | Serious*,† | Not serious | Not serious | 1611 | 854 | PCV15+PPSV23 had higher immune responses vs. PCV13+PPSV23 for 9–13 PCV13 serotypes (GMT) or 5–11 PCV13 serotypes (% seroresponders) across studies. | 2 | Critical | |
| Serious adverse events | ||||||||||||
| 3 (2-4) | Randomized studies | Not serious | Not serious | Not serious† | Serious‡ | Not serious | 0/1484 | 0/795 | non estimable | — | 2 | Critical |
Table 4. Footnotes
GMT=geometric mean titers, PCV13=13-valent pneumococcal conjugate vaccine, PCV15=15-valent pneumococcal conjugate vaccine, PPSV23=23-valent pneumococcal polysaccharide vaccine, SAE=serious adverse events
*These are all immunogenicity studies and there are no correlates of protection
†V114-017: population was Immunocompetent adults 18-49 years of age at risk of pneumococcal disease; V114-018: population was adults ≥18 years of age with HIV; similar responses observed compared to general population
‡No vaccine-related serious adverse events reported
Table 5: Summary of Evidence for Outcomes of Interest
| Outcome | Importance | Included in evidence profile | Certainty |
|---|---|---|---|
| Vaccine-type invasive pneumococcal disease | Critical | Yes | 2, moderate |
| Vaccine-type non-bacteremic pneumococcal pneumonia | Critical | Yes | 2, moderate |
| Vaccine-type pneumococcal mortality | Critical | Yes | 2, moderate |
| Serious adverse events following immunization | Critical | Yes | 2, moderate |
Summary
The evidence type for use of PCV15 in series with PPSV23 in adults aged ≥65 years was determined to be 2 (moderate certainty of evidence). The ACIP reviewed the results of both GRADE analysis and the Evidence to Recommendations (EtR) framework in June 2021. An updated EtR table was shared with the ACIP in September 2021. In October 2021, the ACIP recommended use of PCV15 in series with PPSV23 for all adults aged ≥65 years who have not previously received a pneumococcal conjugate vaccine or whose previous vaccination history is unknown.
Appendix I. Search Strategy
| Database | Strategy | Run Date | Records |
|---|---|---|---|
| Medline (OVID) |
1. streptococcus pneumoniae/ 2. (pneumococcal or pneumococci or “streptococcus pneumonie” or “streptococcus pneumoniae” or “s pneumoniae”).tw,kf. 3. 1 or 2 4. vaccination/ or immunization/ or Vaccines, Conjugate/ 5. (vaccine? or vaccination? or immunisation or immunization).tw,kf. 6. 4 or 5 7. Pneumococcal Vaccines/ 8. (heptavalent or “7 valent” or “7valent” or “pcv 7” or pcv7* or “10 valent” or “10valent” or pcv10 or “pcv 10” or “13valent” or “13 valent” or pcv13 or “pcv 13” or ppv23 or “ppv 23” or “23 valent” or “23valent”).tw,kf. 9. 7 or 8 10. (3 and 6) 11. 10 or 9 12. comparative effectiveness research/ or treatment outcome/ or Vaccine Potency/ 13. (efficacy or effectiveness or effects or “immune response” or impact or “treatment outcome”).tw,kf. 14. 12 or 13 15. adult/ or aged/ or “aged, 80 and over”/ or frail elderly/ 16. (adult? or elderly or elderlies).tw,kf. 17. 15 or 16 18. 11 and 14 and 17 19. (201904* OR 201905* OR 201906* OR 201907* OR 201908* OR 201909* OR 201910* OR 201911* OR 201912* OR 2020* OR 2021*).ed,ep,yr,dp,dt. 20. 17 and 18 |
02/18/2021 | 351 |
| Embase (OVID) 1988- |
1. Streptococcus pneumoniae/ 2. (pneumococcal or pneumococci or “streptococcus pneumonie” or “streptococcus pneumoniae” or “s pneumoniae”).tw,kw. 3. 1 or 2 4. vaccination/ or immunization/ or vaccine/ 5. (vaccine? or vaccination? or immunisation or immunization).tw,kw. 6. 4 or 5 7. Pneumococcus vaccine/ 8. (heptavalent or “7 valent” or “7valent” or “pcv 7” or pcv7* or “10 valent” or “10valent” or pcv10 or “pcv 10” or “13valent” or “13 valent” or pcv13 or “pcv 13” or ppv23 or “ppv 23” or “23 valent” or “23valent”).tw,kw. 9. 7 or 8 10. 3 and 6 11. 9 OR 10 12. comparative effectiveness/ or treatment outcome/ 13. (efficacy or effectiveness or effects or “immune response” or impact or “treatment outcome”).tw,kw. 14. 12 or 13 15. aged/ or adult/ or aged hospital patient/ or frail elderly/ or institutionalized elderly/ or very elderly/ 16. (adult? or elderly or elderlies).tw,kw. 17. 15 or 16 18. 11 and 14 and 17 19. (201904* OR 201905* OR 201906* OR 201907* OR 201908* OR 201909* OR 201910* OR 201911* OR 201912* OR 2020* OR 2021*).dc 20. limit 19 to (conference abstracts or embase) |
02/18/2021 | 521
– = |
| Cochrane Library | ( ( (pneumococcal or pneumococci or “streptococcus pneumonie” or “streptococcus pneumoniae” or “s pneumoniae”):ti,ab AND ([mh Vaccines] OR [mh Immunization] OR (vaccine# or vaccination# or immunisation or immunization):ti,ab) ) OR (MH “Pneumococcal Vaccine”) OR TI (heptavalent or “7 valent” or “7valent” or “pcv 7” or pcv7* or “10 valent” or “10valent” or pcv10 or “pcv 10” or “13valent” or “13 valent” or pcv13 or “pcv 13” or ppv23 or “ppv 23” or “23 valent” or “23valent”) OR AB (heptavalent or “7 valent” or “7valent” or “pcv 7” or pcv7* or “10 valent” or “10valent” or pcv10 or “pcv 10” or “13valent” or “13 valent” or pcv13 or “pcv 13” or ppv23 or “ppv 23” or “23 valent” or “23valent”) ) AND[mh “Treatment Outcomes”] OR (efficacy or effectiveness or effects or “immune response” or impact or “treatment outcome”):ti,abAND[mh Adult] OR [mh Aged+] OR (adult# or elderly or elderlies):ti,ab |
02/18/2021 | 56
– = |
| CINAHL (EbscoHost) |
( (TI (pneumococcal or pneumococci or “streptococcus pneumonie” or “streptococcus pneumoniae” or “s pneumoniae”) OR AB (pneumococcal or pneumococci or “streptococcus pneumonie” or “streptococcus pneumoniae” or “s pneumoniae”)) AND ((MH “Vaccines”) OR (MH “Immunization”) OR TI (vaccine# or vaccination# or immunisation or immunization) OR AB (vaccine# or vaccination# or immunisation or immunization)) OR (MH “Pneumococcal Vaccine”) OR TI (heptavalent or “7 valent” or “7valent” or “pcv 7” or pcv7* or “10 valent” or “10valent” or pcv10 or “pcv 10” or “13valent” or “13 valent” or pcv13 or “pcv 13” or ppv23 or “ppv 23” or “23 valent” or “23valent”) OR AB (heptavalent or “7 valent” or “7valent” or “pcv 7” or pcv7* or “10 valent” or “10valent” or pcv10 or “pcv 10” or “13valent” or “13 valent” or pcv13 or “pcv 13” or ppv23 or “ppv 23” or “23 valent” or “23valent”) ) AND (MH “Treatment Outcomes”) OR TI (efficacy or effectiveness or effects or “immune response” or impact or “treatment outcome”) OR AB (efficacy or effectiveness or effects or “immune response” or impact or “treatment outcome”) AND ((MH “Adult”) OR (MH “Aged+”) OR TI (adult# or elderly or elderlies) OR AB (adult# or elderly or elderlies))Limiters – Published Date: 20190401-20210218; Exclude MEDLINE records |
02/18/2021 | 43
– = |
| Scopus (for WOS) |
(TITLE-ABS-KEY(“heptavalent” or “7 valent” or “7valent” or “pcv 7” or pcv7* or “10 valent” or “10valent” or “pcv10” or “pcv 10” or “13valent” or “13 valent” or “pcv13” or “pcv 13” or “ppv23” or “ppv 23” or “23 valent” or “23valent”) OR (TITLE-ABS-KEY(“vaccine$” or “vaccination$” or “immunisation” or “immunization”) AND TITLE-ABS-KEY(“pneumococcal” or “pneumococci” or “streptococcus pneumonie” or “streptococcus pneumoniae” or “s pneumoniae”))) AND TITLE-ABS-KEY(“adult$” or “elderly” or “elderlies”) AND TITLE-ABS-KEY(“efficacy” or “effectiveness” or “effects” or “immune response” or “impact” or “treatment outcome”)
Limit April 2019 – |
02/18/2021 | 458
– = |
| Epistemonikos | Search 1: (pneumococcal OR pneumococci OR “streptococcus pneumonie” OR “streptococcus pneumoniae” OR “s pneumoniae”) AND (vaccine* OR vaccination* OR immunisation OR immunization) AND (efficacy OR effectiveness OR effects OR “immune response” OR impact OR “treatment outcome”) AND (adult* OR elderly OR elderlies) – limited to 2019-2021Search 2: (heptavalent OR “7 valent” OR “7valent” OR “pcv 7” OR pcv7* OR “10 valent” OR “10valent” OR pcv10 OR “pcv 10” OR “13valent” OR “13 valent” OR pcv13 OR “pcv 13” OR ppv23 OR “ppv 23” OR “23 valent” OR “23valent”) AND (efficacy OR effectiveness OR effects OR “immune response” OR impact OR “treatment outcome”) AND (adult* OR elderly OR elderlies) – limited to 2019-2021 |
02/18/2021 | 19 + 10
– = |
Appendix II. Studies Included in the Review of Evidence
| Study | Study design | Country (or more detail, if needed) | Age (range) | Total population | N Intervention | N comparison | Outcomes | Funding source |
|---|---|---|---|---|---|---|---|---|
| V114-017 | Phase III randomized controlled trial | US | Native Americans or adults with chronic medical conditions* aged 18-49 years | 1381 | 1035 | 346 | Immunogenicity, Safety |
Merck |
| V114-018 | Phase III randomized controlled trial | US | Adults ≥18 years of age with HIV | 298 | 150 | 148 | Immunogenicity, Safety |
Merck |
| V114-016 | Phase III randomized controlled trial | US | Adults ≥50 years of age | 627 | 325 | 302 | Immunogenicity, Safety |
Merck |
Appendix II Footnote
*Chronic heart/liver/lung disease, cigarette smoking, diabetes mellitus
View the complete list of GRADE evidence tables
- World Health Organization. Strategic Advisory Group of Experts on Immunization 5-7 October 2020. 2020 [cited 2021 July 28]; Available from: https://terrance.who.int/mediacentre/data/sage/SAGE_eYB_October_2020.pdf?ua=1.
- A Study to Evaluate the Safety, Tolerability, and Immunogenicity of V114 Followed by PNEUMOVAX™23 in Adults at Increased Risk for Pneumococcal Disease (V114-017/PNEU-DAY). . Available from: https://ClinicalTrials.gov/show/NCT03547167.
- Safety and Immunogenicity of V114 in Healthy Adults (V114-019/PNEU-AGE). https://ClinicalTrials.gov/show/NCT03950622.
- A Study to Evaluate the Safety, Tolerability, and Immunogenicity of V114 Followed by PNEUMOVAX™23 in Adults Infected With Human Immunodeficiency Virus (HIV) (V114-018). https://ClinicalTrials.gov/show/NCT03480802.