Characteristics and Adverse Events of Patients for Whom Nifurtimox Was Released Through CDC-Sponsored Investigational New Drug Program for Treatment of Chagas Disease — United States, 2001–2021

Chagas disease, or American trypanosomiasis, is caused by the parasite Trypanosoma cruzi. Chagas disease is endemic in rural areas of Latin America, but T. cruzi, triatomine vectors, infected mammalian reservoir hosts, and rare cases of autochthonous vector borne transmission have been reported in the United States (1). Possible modes of transmission include the following: vector borne via skin or mucosal contact with feces of infected triatomine bugs, congenital, blood transfusion, organ transplantation, or laboratory accident. Chagas disease can be treated with benznidazole (commercially available since May 14, 2018) or nifurtimox (2). Before January 25, 2021, nifurtimox (Lampit) had been exclusively available through CDC under an Institutional Review Board–approved Investigational New Drug (IND) treatment protocol, at which time it became reasonably accessible to health care providers outside of the program. This report summarizes CDC Drug Service reports for selected characteristics of and adverse events reported by 336 patients for whom nifurtimox was requested under the CDC IND program during January 1, 2001–January 25, 2021. Of the 336 patients, 34.2% resided in California. Median age of patients was 37 years (range = 1–78 years). Most patients were aged ≥18 (91.8%; 305 of 332) and Hispanic (93.2%; 290 of 311). Among the patients with available information, 91.4% (222 of 243) reported an adverse event. Among those with information about the severity of their adverse events, 20.5% reported a severe event. start highlightOn August 6, 2020, the Food and Drug Administration (FDA) announced approval of a nifurtimox product, Lampit (Bayer), for treatment of Chagas disease in patients aged <18 years weighing ≥5.5 lbs (≥2.5 kg).end highlight Lampit became commercially available during October 2020. Physicians should take frequency of adverse events into consideration when prescribing nifurtimox and counseling patients.

Patient characteristics and reported adverse events were recorded for the purpose of drug release under the CDC program. The information was provided by the physicians who requested nifurtimox to treat their patients and monitored the patients during and after treatment. Age groups were created based on Chagas disease treatment recommendations (1). Data were excluded for releases made under FDA individual IND authorizations, separate from the CDC protocol. In some situations, the process for release of nifurtimox was initiated but never finalized; data from those incomplete requests were also excluded. If multiple releases of the drug were for treatment of the same patient, the associated data were combined. The prevalence of patient characteristics, reported adverse events, and severity of adverse events are reported. Fisher’s exact test was used to assess statistical significance (p<0.05). All analyses were performed using R (version 4.0.2; R Foundation) and QGIS (version 3.10; QGIS Association). This activity was reviewed by CDC and was conducted consistent with applicable federal law and CDC policy.*

From January 1, 2001, until patient enrollment was discontinued on January 25, 2021, CDC released nifurtimox under the IND for treatment of 336 patients, 22 (6.5%) of whom did not start treatment. Patients for whom information was available but who did not begin treatment did not differ substantially from the group as a whole. The state with the highest number of patients for whom drug was released was California (115; 34.2%) followed by New York (29; 8.6%) (Figure). The median age of 332 patients with reported age was 37 years (range = 1–78 years), with 27 (8.1%) aged <18 years, 246 (74.1%) aged 18–50 years, and 59 (17.8%) aged >50 years. Among the 27 patients aged <18 years, five were aged <15 years.

Approximately one half of patients were female (58.9%; 196 of 333) and most identified as Hispanic (93.2%; 290 of 311). Among 315 patients reporting country of exposure,^† the three most commonly reported countries were El Salvador (109; 34.6%), Mexico (99; 31.4%), and Bolivia (37; 11.7%) (Table 1).

Information on adverse events was available for 243 (77.4%) of the 314 persons who started treatment; among those, 222 (91.4%) reported at least one adverse event; a total of 1,155 adverse events were reported. The median number of adverse events reported per person was four (range = 0–17). Most adverse events were reported for the following categories: gastrointestinal (68.7%), neurologic (60.5%), and constitutional (46.5%). The most common adverse events reported were nausea (50.6%), anorexia (46.1%), weight loss (35.0%), headache (33.3%), and abdominal pain (23.1%) (Table 2). At least 90% of patients aged <18, 18–50, and >50 years reported adverse events. There was no statistically significant difference between the percentage of females and males reporting adverse events (93.6% and 88.2%, respectively; p = 0.17).

Information on severity of adverse events was available for 210 (94.6%) persons who reported an adverse event and 1,042 (90.2%) adverse events. Among those 1,042 events, 680 (65.3%) were described as mild, 254 (24.4%) as moderate, and 108 (10.4%) as severe. Forty-three patients reported a severe adverse event; the most frequent were depression (22.6%), peripheral neuropathy (18.5%), paresthesia (17.9%), and dizziness/vertigo (17.2%) (Table 2). The percentage of patients with at least one adverse event classified as severe was higher among patients aged >50 years (31.8%) than among those aged 18–50 years (18.1%; odds ratio = 2.1; p = 0.06). Two (13.3%) adolescents, both aged 17 years, reported severe adverse events. The percentage of females and males reporting severe adverse events was similar (22.0% and 17.4%, respectively; p = 0.48).

Corresponding author: Andrew Abbott, aabbott@cdc.gov, 404-718-1216.

¹Epidemic Intelligence Service, CDC; ²Division of Parasitic Diseases and Malaria, Center for Global Health, CDC.

References

1. Bern C, Montgomery SP, Herwaldt BL, et al. Evaluation and treatment of Chagas disease in the United States: a systematic review. JAMA 2007;298:2171–81. https://doi.org/10.1001/jama.298.18.2171 PMID:18000201
2. Herwaldt BL, Dougherty CP, Allen CK, et al. Characteristics of patients for whom benznidazole was released through the CDC-sponsored Investigational New Drug Program for Treatment of Chagas Disease—United States, 2011–2018. MMWR Morb Mortal Wkly Rep 2018;67:803–5. https://doi.org/10.15585/mmwr.mm6729a3 PMID:30048425
3. Berenstein AJ, Falk N, Moscatelli G, et al. Adverse events associated with nifurtimox treatment for Chagas disease in children and adults. Antimicrob Agents Chemother 2021;65:e01135-20. https://doi.org/10.1128/AAC.01135-20 PMID:33168612
4. Jackson Y, Alirol E, Getaz L, Wolff H, Combescure C, Chappuis F. Tolerance and safety of nifurtimox in patients with chronic Chagas disease. Clin Infect Dis 2010;51:e69–75. https://doi.org/10.1086/656917 PMID:20932171
5. Olivera MJ, Cucunubá ZM, Álvarez CA, Nicholls RS. Safety profile of nifurtimox and treatment interruption for chronic Chagas disease in Colombian adults. Am J Trop Med Hyg 2015;93:1224–30. https://doi.org/10.4269/ajtmh.15-0256 PMID:26392162
6. Forsyth CJ, Hernandez S, Olmedo W, et al. Safety profile of nifurtimox for treatment of Chagas disease in the United States. Clin Infect Dis 2016;63:1056–62. https://doi.org/10.1093/cid/ciw477 PMID:27432838
7. Murcia L, Carrilero B, Albajar Viñas P, Segovia M. Nifurtimox chemotherapy: collateral effects in treated Trypanosoma cruzi infected patients. Rev Esp Quimioter 2012;25:74–5. PMID:22488545
8. Altcheh J, Castro L, Dib JC, et al.; CHICO Study Group. Prospective, historically controlled study to evaluate the efficacy and safety of a new paediatric formulation of nifurtimox in children aged 0 to 17 years with Chagas disease one year after treatment (CHICO). PLoS Negl Trop Dis 2021;15:e0008912. https://doi.org/10.1371/journal.pntd.0008912 PMID:33412557
9. Meymandi SK, Forsyth CJ, Soverow J, et al. Prevalence of Chagas disease in the Latin American-born population of Los Angeles. Clin Infect Dis 2017;64:1182–8. https://doi.org/10.1093/cid/cix064 PMID:28329123
10. Bern C, Montgomery SP. An estimate of the burden of Chagas disease in the United States. Clin Infect Dis 2009;49:e52–4. https://doi.org/10.1086/605091 PMID:19640226

FIGURE. Number of nifurtimox releases for treatment of Chagas disease for 336 unique patients, by state — United States, 2001–2021.

Abbreviation: DC = District of Columbia.

Abbreviation: NA = not applicable.
* Patients might have had more than one country of exposure.

Abbreviation: NA = not applicable.
* Patients could have both severe and nonsevere adverse events in each category, therefore not calculated.
^† None reported as severe.
^§ Other includes abdominal discomfort (three), abnormal taste (three), dry mouth (three), hepatitis (two), dysphagia (one), and constipation (one).
^¶ Other includes confusion (three), seizure (two), excessive blinking (one), forgetfulness (one), leg weakness (one), poor balance (one), and stuttering (one).
** Other includes chills (two), hot flashes (two), diaphoresis (one), and irritation (one).
^†† Other includes crying spells (two), hallucinations (two), morbid thoughts (one), and nightmares (one).
^§§ Other includes whole body pain (two), back pain (two), and leg cramps (one).
^¶¶ Other includes flushing (two), dry skin (one), hair loss (one), and jaundice (one).
*** Other includes syncope (one), affliction from the heart (one), and high blood pressure (one).
^††† Miscellaneous includes urinary symptoms (four), sexual dysfunction (three), cough (three), shortness of breath (three), hypoglycemia (three), facial swelling (two), hypersensitivity pneumonitis (one), itchy eyes (one), left-sided neck vein throbbing (one), runny nose (one), elevated alanine aminotransferase (one), and eosinophilia (one).