PLoS ONE (Jan 2020)

IMRAS-A clinical trial of mosquito-bite immunization with live, radiation-attenuated P. falciparum sporozoites: Impact of immunization parameters on protective efficacy and generation of a repository of immunologic reagents.

  • Bradley Hickey,
  • Nimfa Teneza-Mora,
  • Joanne Lumsden,
  • Sharina Reyes,
  • Martha Sedegah,
  • Lindsey Garver,
  • Michael R Hollingdale,
  • Jo Glenna Banania,
  • Harini Ganeshan,
  • Megan Dowler,
  • Anatalio Reyes,
  • Cindy Tamminga,
  • Alexandra Singer,
  • Alicia Simmons,
  • Maria Belmonte,
  • Arnel Belmonte,
  • Jun Huang,
  • Sandra Inoue,
  • Rachel Velasco,
  • Steve Abot,
  • Carlos S Vasquez,
  • Ivelese Guzman,
  • Mimi Wong,
  • Patrick Twomey,
  • Mariusz Wojnarski,
  • James Moon,
  • Yolanda Alcorta,
  • Santina Maiolatesi,
  • Michele Spring,
  • Silas Davidson,
  • Sidhartha Chaudhury,
  • Eileen Villasante,
  • Thomas L Richie,
  • Judith E Epstein

DOI
https://doi.org/10.1371/journal.pone.0233840
Journal volume & issue
Vol. 15, no. 6
p. e0233840

Abstract

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BackgroundImmunization with radiation-attenuated sporozoites (RAS) by mosquito bite provides >90% sterile protection against Plasmodium falciparum (Pf) malaria in humans. RAS invade hepatocytes but do not replicate. CD8+ T cells recognizing parasite-derived peptides on the surface of infected hepatocytes are likely the primary protective mechanism. We conducted a randomized clinical trial of RAS immunization to assess safety, to achieve 50% vaccine efficacy (VE) against controlled human malaria infection (CHMI), and to generate reagents from protected and non-protected subjects for future identification of protective immune mechanisms and antigens.MethodsTwo cohorts (Cohort 1 and Cohort 2) of healthy, malaria-naïve, non-pregnant adults age 18-50 received five monthly immunizations with infected (true-immunized, n = 21) or non-infected (mock-immunized, n = 5) mosquito bites and underwent homologous CHMI at 3 weeks. Immunization parameters were selected for 50% protection based on prior clinical data. Leukapheresis was done to collect plasma and peripheral blood mononuclear cells.ResultsAdverse event rates were similar in true- and mock-immunized subjects. Two true- and two mock-immunized subjects developed large local reactions likely caused by mosquito salivary gland antigens. In Cohort 1, 11 subjects received 810-1235 infected bites; 6/11 (55%) were protected against CHMI vs. 0/3 mock-immunized and 0/6 infectivity controls (VE 55%). In Cohort 2, 10 subjects received 839-1131 infected bites with a higher first dose and a reduced fifth dose; 9/10 (90%) were protected vs. 0/2 mock-immunized and 0/6 controls (VE 90%). Three/3 (100%) protected subjects administered three booster immunizations were protected against repeat CHMI vs. 0/6 controls (VE 100%). Cohort 2 uniquely showed a significant rise in IFN-γ responses after the third and fifth immunizations and higher antibody responses to CSP.ConclusionsPfRAS were generally safe and well tolerated. Cohort 2 had a higher first dose, reduced final dose, higher antibody responses to CSP and significant rise of IFN-γ responses after the third and fifth immunizations. Whether any of these factors contributed to increased protection in Cohort 2 requires further investigation. A cryobank of sera and cells from protected and non-protected individuals was generated for future immunological studies and antigen discovery.Trial registrationClinicalTrials.gov NCT01994525.