PfSPZ-CVac efficacy against malaria increases from 0% to 75% when administered in the absence of erythrocyte stage parasitemia: A randomized, placebo-controlled trial with controlled human malaria infection

PfSPZ-CVac efficacy against malaria increases from 0% to 75% when administered in the absence of erythrocyte stage parasitemia: A randomized, placebo-controlled trial with controlled human malaria infection

PfSPZ-CVac combines 'PfSPZ Challenge', which consists of infectious Plasmodium falciparum sporozoites (PfSPZ), with concurrent antimalarial chemoprophylaxis. In a previously-published PfSPZ-CVac study, three doses of 5.12x10.sup.4 PfSPZ-CVac given 28 days apart had 100% vaccine efficacy (V...

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Veröffentlicht in:PLoS pathogens 2021-05, Vol.17 (5), p.e1009594-e1009594
Hauptverfasser: Murphy, Sean C, Deye, Gregory A, Sim, B. Kim Lee, Galbiati, Shirley, Kennedy, Jessie K, Cohen, Kristen W, Chakravarty, Sumana, K. C., Natasha, Abebe, Yonas, James, Eric R, Kublin, James G, Hoffman, Stephen L, Richie, Thomas L, Jackson, Lisa A
Format: Artikel
Sprache:eng
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Adverse events
Alanine
Alanine transaminase
Alkaline phosphatase
Aspartate aminotransferase
Bilirubin
Biology and Life Sciences
Blood
Creatinine
Development and progression
Dosage and administration
Erythrocytes
Evaluation
Hemoglobin
Immune response
Immune response (cell-mediated)
Immune response (humoral)
Immune system
Injections
Leukocytes
Life cycles
Malaria
Malaria vaccine
Medicine and Health Sciences
Parasitemia
Parasites
Pharmacokinetics
Placebos
Potassium
Prevention
Red blood cells
Replication
Research and Analysis Methods
Risk factors
Schedules
Sporozoites
Testing
Vaccination
Vaccine efficacy
Vaccines
Vector-borne diseases
White blood cells
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Zusammenfassung:PfSPZ-CVac combines 'PfSPZ Challenge', which consists of infectious Plasmodium falciparum sporozoites (PfSPZ), with concurrent antimalarial chemoprophylaxis. In a previously-published PfSPZ-CVac study, three doses of 5.12x10.sup.4 PfSPZ-CVac given 28 days apart had 100% vaccine efficacy (VE) against controlled human malaria infection (CHMI) 10 weeks after the last immunization, while the same dose given as three injections five days apart had 63% VE. Here, we conducted a dose escalation trial of similarly condensed schedules. Of the groups proceeding to CHMI, the first study group received three direct venous inoculations (DVIs) of a dose of 5.12x10.sup.4 PfSPZ-CVac seven days apart and the next full dose group received three DVIs of a higher dose of 1.024x10.sup.5 PfSPZ-CVac five days apart. CHMI (3.2x10.sup.3 PfSPZ Challenge) was performed by DVI 10 weeks after the last vaccination. In both CHMI groups, transient parasitemia occurred starting seven days after each vaccination. For the seven-day interval group, the second and third vaccinations were therefore administered coincident with parasitemia from the prior vaccination. Parasitemia was associated with systemic symptoms which were severe in 25% of subjects. VE in the seven-day group was 0% (7/7 infected) and in the higher-dose, five-day group was 75% (2/8 infected). Thus, the same dose of PfSPZ-CVac previously associated with 63% VE when given on a five-day schedule in the prior study had zero VE here when given on a seven-day schedule, while a double dose given on a five-day schedule here achieved 75% VE. The relative contributions of the five-day schedule and/or the higher dose to improved VE warrant further investigation. It is notable that administration of PfSPZ-CVac on a schedule where vaccine administration coincided with blood-stage parasitemia was associated with an absence of sterile protective immunity.
ISSN:1553-7374
1553-7366
1553-7374
DOI:10.1371/journal.ppat.1009594