Sydney Johnson scite author profile

Sydney Johnson

3Publications

13Citation Statements Received

81Citation Statements Given

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Affiliations

McMaster University, Lewisham and Greenwich NHS Trust

Publications

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Clinical trials to assess adjuvant therapeutics for severe malaria

Varo

Erice

Johnson

et al. 2020

Malar J

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Despite potent anti-malarial treatment, mortality rates associated with severe falciparum malaria remain high. To attempt to improve outcome, several trials have assessed a variety of potential adjunctive therapeutics, however none to date has been shown to be beneficial. This may be due, at least partly, to the therapeutics chosen and clinical trial design used. Here, we highlight three themes that could facilitate the choice and evaluation of putative adjuvant interventions for severe malaria, paving the way for their assessment in randomized controlled trials. Most clinical trials of adjunctive therapeutics to date have been underpowered due to the large number of participants required to reach mortality endpoints, rendering these study designs challenging and expensive to conduct. These limitations may be mitigated by the use of risk-stratification of participants and application of surrogate endpoints. Appropriate surrogate endpoints include direct measures of pathways causally involved in the pathobiology of severe and fatal malaria, including markers of host immune and endothelial activation and microcirculatory dysfunction. We propose using circulating markers of these pathways to identify high-risk participants that would be most likely to benefit from adjunctive therapy, and further by adopting these biomarkers as surrogate endpoints; moreover, choosing interventions that target deleterious host immune responses that directly contribute to microcirculatory dysfunction, multi-organ dysfunction and death; and, finally, prioritizing where possible, drugs that act on these pathways that are already approved by the FDA, or other regulators, for other indications, and are known to be safe in target populations, including children. An emerging understanding of the critical role of the host response in severe malaria pathogenesis may facilitate both clinical trial design and the search of effective adjunctive therapeutics.

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Recent Methods in Antimalarial Susceptibility Testing

Co¹,

Johnson²,

Murthy³

et al. 2010

AIAMC

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G611(P) Subsidized malaria prophylaxis for children: is it useful?

Pelly

Jewell

Lawrence

et al. 2020

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Conclusion This pilot study may suggest the presence of sufficient pertussis seroimmunity rates in the studied mothers-neonates pair. Still, there were some failures in immune acquisition probably due to waning of immunity with age. Transplacental passage of pertussis antibodies may not confer similar seroimmunity to pertussis in neonates as in mothers. Wider scale studies would allow better insight into the pertussis immune status of the females in the child bearing period in our country and hence the need for booster immunization during pregnancy.

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Sydney Johnson

Clinical trials to assess adjuvant therapeutics for severe malaria

Recent Methods in Antimalarial Susceptibility Testing

G611(P) Subsidized malaria prophylaxis for children: is it useful?

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