Lessons learnt from the first controlled human malaria infection study conducted in Nairobi, Kenya

Susanne H. Hodgson; Elizabeth Juma; Amina Salim; Charles Magiri; Daniel Njenga; Sassy Molyneux; Patricia Njuguna; Ken Awuondo; Brett Lowe; Peter F. Billingsley; Andrew O. Cole; Caroline Ogwang; Faith Osier; Roma Chilengi; Stephen L. Hoffman; Simon J. Draper; Bernhards Ogutu; Kevin Marsh

doi:10.1186/s12936-015-0671-x

Lessons learnt from the first controlled human malaria infection study conducted in Nairobi, Kenya

Susanne H. Hodgson, Elizabeth Juma, Amina Salim, Charles Magiri, Daniel Njenga, Sassy Molyneux, Patricia Njuguna, Ken Awuondo, Brett Lowe, Peter F. Billingsley, Andrew O. Cole, Caroline Ogwang, Faith Osier, Roma Chilengi, Stephen L. Hoffman, Simon J. Draper, Bernhards Ogutu, Kevin Marsh

Research output: Contribution to journal › Article › peer-review

56 Citations (Scopus)

Abstract

Background: Controlled human malaria infection (CHMI) studies, in which healthy volunteers are infected with Plasmodium falciparum to assess the efficacy of novel malaria vaccines and drugs, have become a vital tool to accelerate vaccine and drug development. CHMI studies provide a cost-effective and expeditious way to circumvent the use of large-scale field efficacy studies to deselect intervention candidates. However, to date few modern CHMI studies have been performed in malaria-endemic countries. Methods: An open-label, randomized pilot CHMI study was conducted using aseptic, purified, cryopreserved, infectious P. falciparum sporozoites (SPZ) (Sanaria® PfSPZ Challenge) administered intramuscularly (IM) to healthy Kenyan adults (n∈=∈28) with varying degrees of prior exposure to P. falciparum. The purpose of the study was to establish the PfSPZ Challenge CHMI model in a Kenyan setting with the aim of increasing the international capacity for efficacy testing of malaria vaccines and drugs, and allowing earlier assessment of efficacy in a population for which interventions are being developed. This was part of the EDCTP-funded capacity development of the CHMI platform in Africa. Discussion: This paper discusses in detail lessons learnt from conducting the first CHMI study in Kenya. Issues pertinent to the African setting, including community sensitization, consent and recruitment are considered. Detailed reasoning regarding the study design (for example, dose and route of administration of PfSPZ Challenge, criteria for grouping volunteers according to prior exposure to malaria and duration of follow-up post CHMI) are given and changes other centres may want to consider for future studies are suggested. Conclusions: Performing CHMI studies in an African setting presents unique but surmountable challenges and offers great opportunity for acceleration of malaria vaccine and drug development. The reflections in this paper aim to aid other centres and partners intending to use the CHMI model in Africa.

Original language	English
Article number	182
Journal	Malaria Journal
Volume	14
Issue number	1
DOIs	https://doi.org/10.1186/s12936-015-0671-x
Publication status	Published - 28 Apr 2015
Externally published	Yes

Keywords

African
Challenge
CHMI
Drug
Kenya
Lessons
Malaria
PfSPZ Challenge
Plasmodium falciparum
Vaccine

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1186/s12936-015-0671-xLicence: CC BY

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Hodgson, S. H., Juma, E., Salim, A., Magiri, C., Njenga, D., Molyneux, S., Njuguna, P., Awuondo, K., Lowe, B., Billingsley, P. F., Cole, A. O., Ogwang, C., Osier, F., Chilengi, R., Hoffman, S. L., Draper, S. J., Ogutu, B., & Marsh, K. (2015). Lessons learnt from the first controlled human malaria infection study conducted in Nairobi, Kenya. Malaria Journal, 14(1), Article 182. https://doi.org/10.1186/s12936-015-0671-x

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abstract = "Background: Controlled human malaria infection (CHMI) studies, in which healthy volunteers are infected with Plasmodium falciparum to assess the efficacy of novel malaria vaccines and drugs, have become a vital tool to accelerate vaccine and drug development. CHMI studies provide a cost-effective and expeditious way to circumvent the use of large-scale field efficacy studies to deselect intervention candidates. However, to date few modern CHMI studies have been performed in malaria-endemic countries. Methods: An open-label, randomized pilot CHMI study was conducted using aseptic, purified, cryopreserved, infectious P. falciparum sporozoites (SPZ) (Sanaria{\textregistered} PfSPZ Challenge) administered intramuscularly (IM) to healthy Kenyan adults (n∈=∈28) with varying degrees of prior exposure to P. falciparum. The purpose of the study was to establish the PfSPZ Challenge CHMI model in a Kenyan setting with the aim of increasing the international capacity for efficacy testing of malaria vaccines and drugs, and allowing earlier assessment of efficacy in a population for which interventions are being developed. This was part of the EDCTP-funded capacity development of the CHMI platform in Africa. Discussion: This paper discusses in detail lessons learnt from conducting the first CHMI study in Kenya. Issues pertinent to the African setting, including community sensitization, consent and recruitment are considered. Detailed reasoning regarding the study design (for example, dose and route of administration of PfSPZ Challenge, criteria for grouping volunteers according to prior exposure to malaria and duration of follow-up post CHMI) are given and changes other centres may want to consider for future studies are suggested. Conclusions: Performing CHMI studies in an African setting presents unique but surmountable challenges and offers great opportunity for acceleration of malaria vaccine and drug development. The reflections in this paper aim to aid other centres and partners intending to use the CHMI model in Africa.",

keywords = "African, Challenge, CHMI, Drug, Kenya, Lessons, Malaria, PfSPZ Challenge, Plasmodium falciparum, Vaccine",

author = "Hodgson, \{Susanne H.\} and Elizabeth Juma and Amina Salim and Charles Magiri and Daniel Njenga and Sassy Molyneux and Patricia Njuguna and Ken Awuondo and Brett Lowe and Billingsley, \{Peter F.\} and Cole, \{Andrew O.\} and Caroline Ogwang and Faith Osier and Roma Chilengi and Hoffman, \{Stephen L.\} and Draper, \{Simon J.\} and Bernhards Ogutu and Kevin Marsh",

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Hodgson, SH, Juma, E, Salim, A, Magiri, C, Njenga, D, Molyneux, S, Njuguna, P, Awuondo, K, Lowe, B, Billingsley, PF, Cole, AO, Ogwang, C, Osier, F, Chilengi, R, Hoffman, SL, Draper, SJ, Ogutu, B & Marsh, K 2015, 'Lessons learnt from the first controlled human malaria infection study conducted in Nairobi, Kenya', Malaria Journal, vol. 14, no. 1, 182. https://doi.org/10.1186/s12936-015-0671-x

TY - JOUR

T1 - Lessons learnt from the first controlled human malaria infection study conducted in Nairobi, Kenya

AU - Hodgson, Susanne H.

AU - Juma, Elizabeth

AU - Salim, Amina

AU - Magiri, Charles

AU - Njenga, Daniel

AU - Molyneux, Sassy

AU - Njuguna, Patricia

AU - Awuondo, Ken

AU - Lowe, Brett

AU - Billingsley, Peter F.

AU - Cole, Andrew O.

AU - Ogwang, Caroline

AU - Osier, Faith

AU - Chilengi, Roma

AU - Hoffman, Stephen L.

AU - Draper, Simon J.

AU - Ogutu, Bernhards

AU - Marsh, Kevin

PY - 2015/4/28

Y1 - 2015/4/28

N2 - Background: Controlled human malaria infection (CHMI) studies, in which healthy volunteers are infected with Plasmodium falciparum to assess the efficacy of novel malaria vaccines and drugs, have become a vital tool to accelerate vaccine and drug development. CHMI studies provide a cost-effective and expeditious way to circumvent the use of large-scale field efficacy studies to deselect intervention candidates. However, to date few modern CHMI studies have been performed in malaria-endemic countries. Methods: An open-label, randomized pilot CHMI study was conducted using aseptic, purified, cryopreserved, infectious P. falciparum sporozoites (SPZ) (Sanaria® PfSPZ Challenge) administered intramuscularly (IM) to healthy Kenyan adults (n∈=∈28) with varying degrees of prior exposure to P. falciparum. The purpose of the study was to establish the PfSPZ Challenge CHMI model in a Kenyan setting with the aim of increasing the international capacity for efficacy testing of malaria vaccines and drugs, and allowing earlier assessment of efficacy in a population for which interventions are being developed. This was part of the EDCTP-funded capacity development of the CHMI platform in Africa. Discussion: This paper discusses in detail lessons learnt from conducting the first CHMI study in Kenya. Issues pertinent to the African setting, including community sensitization, consent and recruitment are considered. Detailed reasoning regarding the study design (for example, dose and route of administration of PfSPZ Challenge, criteria for grouping volunteers according to prior exposure to malaria and duration of follow-up post CHMI) are given and changes other centres may want to consider for future studies are suggested. Conclusions: Performing CHMI studies in an African setting presents unique but surmountable challenges and offers great opportunity for acceleration of malaria vaccine and drug development. The reflections in this paper aim to aid other centres and partners intending to use the CHMI model in Africa.

AB - Background: Controlled human malaria infection (CHMI) studies, in which healthy volunteers are infected with Plasmodium falciparum to assess the efficacy of novel malaria vaccines and drugs, have become a vital tool to accelerate vaccine and drug development. CHMI studies provide a cost-effective and expeditious way to circumvent the use of large-scale field efficacy studies to deselect intervention candidates. However, to date few modern CHMI studies have been performed in malaria-endemic countries. Methods: An open-label, randomized pilot CHMI study was conducted using aseptic, purified, cryopreserved, infectious P. falciparum sporozoites (SPZ) (Sanaria® PfSPZ Challenge) administered intramuscularly (IM) to healthy Kenyan adults (n∈=∈28) with varying degrees of prior exposure to P. falciparum. The purpose of the study was to establish the PfSPZ Challenge CHMI model in a Kenyan setting with the aim of increasing the international capacity for efficacy testing of malaria vaccines and drugs, and allowing earlier assessment of efficacy in a population for which interventions are being developed. This was part of the EDCTP-funded capacity development of the CHMI platform in Africa. Discussion: This paper discusses in detail lessons learnt from conducting the first CHMI study in Kenya. Issues pertinent to the African setting, including community sensitization, consent and recruitment are considered. Detailed reasoning regarding the study design (for example, dose and route of administration of PfSPZ Challenge, criteria for grouping volunteers according to prior exposure to malaria and duration of follow-up post CHMI) are given and changes other centres may want to consider for future studies are suggested. Conclusions: Performing CHMI studies in an African setting presents unique but surmountable challenges and offers great opportunity for acceleration of malaria vaccine and drug development. The reflections in this paper aim to aid other centres and partners intending to use the CHMI model in Africa.

KW - African

KW - Challenge

KW - CHMI

KW - Drug

KW - Kenya

KW - Lessons

KW - Malaria

KW - PfSPZ Challenge

KW - Plasmodium falciparum

KW - Vaccine

U2 - 10.1186/s12936-015-0671-x

DO - 10.1186/s12936-015-0671-x

M3 - Article

SN - 1475-2875

VL - 14

JO - Malaria Journal

JF - Malaria Journal

IS - 1

M1 - 182

ER -

Lessons learnt from the first controlled human malaria infection study conducted in Nairobi, Kenya

Abstract

Keywords

UN SDGs

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