1. Multi-Dose Priming Regimens of PfSPZ Vaccine: Safety and Efficacy against Controlled Human Malaria Infection in Equatoguinean Adults
- Author
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Said Abdallah Jongo, L. W. Preston Church, Vicente Urbano Nsue Ndong Nchama, Ali Hamad, Raul Chuquiyauri, Kamaka Ramadhani Kassim, Thabit Athuman, Anna Deal, KC Natasha, Ali Mtoro, Maxmillian Mpina, Elizabeth Nyakarungu, Gertrudis Owono Bidjimi, Marta Alene Owono, Escolástica Raquel Mansogo Mayé, Martín Eká Ondó Mangue, Genaro Nsué Nguema Okomo, Beltrán Ekuá Ntutumu Pasialo, Dolores Mbang Ondó Mandumbi, María-Silvia A. López Mikue, Fortunata Lobede Mochomuemue, Mariano Obiang Obono, Juan Carlos Momo Besahá, José Raso Bijeri, Gabriel Mbá Abegue, Yolanda Rimoy Veri, Ines Toichoa Bela, Federico Comsil Chochi, José Enrique Lima Sánchez, Vanessa Pencelli, Griselda Gayozo, José Antonio Esono Mbá Nlang, Tobias Schindler, Eric R. James, Yonas Abebe, Laurence Lemiale, Thomas C. Stabler, Tooba Murshedkar, Mei-Chun Chen, Christopher Schwabe, Josea Ratsirarson, Matilde Riloha Rivas, Mitoha Ondo’o Ayekaba, Diosdado Vicente Nsué Milang, Carlos Cortés Falla, Wonder P. Phiri, Guillermo A. García, Carl D. Maas, Bonifacio Manguire Nlavo, Marcel Tanner, Peter F. Billingsley, B. Kim Lee Sim, Claudia Daubenberger, Stephen L. Hoffman, Salim Abdulla, and Thomas L. Richie
- Subjects
Infectious Diseases ,Virology ,Parasitology - Abstract
Plasmodium falciparum sporozoite (PfSPZ) Vaccine is composed of radiation-attenuated, aseptic, purified cryopreserved PfSPZ. Multiple clinical trials empirically assessing two to six doses have shown multi-dose priming (two to four doses the first week) to be optimal for protection in both 4- and 16-week regimens. In this randomized, double-blind, normal saline (NS) placebo-controlled trial, four groups (G) of 18- to 32-year-old Equatoguineans received multi-dose priming regimens with or without a delayed final dose at 4 or 16 weeks. The regimens were G1: days 1, 3, 5, 7, and 113; G2: days 1, 3, 5, and 7; G3: days 1, 3, 5, 7, and 29; and G4: days 1, 8, and 29. All doses were 9 × 105 PfSPZ. Tolerability, safety, immunogenicity, and vaccine efficacy (VE) against homologous controlled human malaria infection (CHMI) 6–7 weeks after vaccination were assessed to down-select the best regimen. All four regimens were safe and well tolerated, with no significant differences in adverse events (AEs) between vaccinees (N = 84) and NS controls (N = 20) or between regimens. Out of 19 controls, 13 developed Pf parasitemia by quantitative polymerase chain reaction (qPCR) after CHMI. Only the vaccine regimen administered on study days 1, 8, and 29 gave significant protection (7/21 vaccinees versus 13/19 controls infected, VE 51.3%, P = 0.03, Barnard’s test, two-tailed). There were no significant differences in antibodies against Pf circumsporozoite protein (PfCSP), a major SPZ antigen, between protected and nonprotected vaccinees or controls pre-CHMI. The six controls not developing Pf parasitemia had significantly higher antibodies to blood stage antigens Pf exported protein 1 (PfEXP1) and Pf merozoite surface protein 1 (PfMSP1) than the controls who developed parasitemia, suggesting naturally acquired immunity against Pf limited infections in controls. This study identified a safe, protective, 4-week, multi-dose prime vaccination regimen for assessment in future trials of PfSPZ Vaccine.
- Published
- 2021