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Beyond Blood Smears: Qualification of Plasmodium 18S rRNA as a Biomarker for Controlled Human Malaria Infections

18S rRNA is a biomarker that provides an alternative to thick blood smears in controlled human malaria infection (CHMI) trials. We reviewed data from CHMI trials at non-endemic sites that used blood smears and Plasmodium 18S rRNA/rDNA biomarker nucleic acid tests (NATs) for time to positivity. We va...

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Autores principales: Seilie, Annette M., Chang, Ming, Hanron, Amelia E., Billman, Zachary P., Stone, Brad C., Zhou, Kevin, Olsen, Tayla M., Daza, Glenda, Ortega, Jose, Cruz, Kurtis R., Smith, Nahum, Healy, Sara A., Neal, Jillian, Wallis, Carolyn K., Shelton, Lisa, Mankowski, Tracie (VonGoedert), Wong-Madden, Sharon, Mikolajczak, Sebastian A., Vaughan, Ashley M., Kappe, Stefan H. I., Fishbaugher, Matt, Betz, Will, Kennedy, Mark, Hume, Jen C. C., Talley, Angela K., Hoffman, Stephen L., Chakravarty, Sumana, Sim, B. Kim Lee, Richie, Thomas L., Wald, Anna, Plowe, Christopher V., Lyke, Kirsten E., Adams, Matthew, Fahle, Gary A., Cowan, Elliot P., Duffy, Patrick E., Kublin, James G., Murphy, Sean C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The American Society of Tropical Medicine and Hygiene 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6553913/
https://www.ncbi.nlm.nih.gov/pubmed/31017084
http://dx.doi.org/10.4269/ajtmh.19-0094
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author Seilie, Annette M.
Chang, Ming
Hanron, Amelia E.
Billman, Zachary P.
Stone, Brad C.
Zhou, Kevin
Olsen, Tayla M.
Daza, Glenda
Ortega, Jose
Cruz, Kurtis R.
Smith, Nahum
Healy, Sara A.
Neal, Jillian
Wallis, Carolyn K.
Shelton, Lisa
Mankowski, Tracie (VonGoedert)
Wong-Madden, Sharon
Mikolajczak, Sebastian A.
Vaughan, Ashley M.
Kappe, Stefan H. I.
Fishbaugher, Matt
Betz, Will
Kennedy, Mark
Hume, Jen C. C.
Talley, Angela K.
Hoffman, Stephen L.
Chakravarty, Sumana
Sim, B. Kim Lee
Richie, Thomas L.
Wald, Anna
Plowe, Christopher V.
Lyke, Kirsten E.
Adams, Matthew
Fahle, Gary A.
Cowan, Elliot P.
Duffy, Patrick E.
Kublin, James G.
Murphy, Sean C.
author_facet Seilie, Annette M.
Chang, Ming
Hanron, Amelia E.
Billman, Zachary P.
Stone, Brad C.
Zhou, Kevin
Olsen, Tayla M.
Daza, Glenda
Ortega, Jose
Cruz, Kurtis R.
Smith, Nahum
Healy, Sara A.
Neal, Jillian
Wallis, Carolyn K.
Shelton, Lisa
Mankowski, Tracie (VonGoedert)
Wong-Madden, Sharon
Mikolajczak, Sebastian A.
Vaughan, Ashley M.
Kappe, Stefan H. I.
Fishbaugher, Matt
Betz, Will
Kennedy, Mark
Hume, Jen C. C.
Talley, Angela K.
Hoffman, Stephen L.
Chakravarty, Sumana
Sim, B. Kim Lee
Richie, Thomas L.
Wald, Anna
Plowe, Christopher V.
Lyke, Kirsten E.
Adams, Matthew
Fahle, Gary A.
Cowan, Elliot P.
Duffy, Patrick E.
Kublin, James G.
Murphy, Sean C.
author_sort Seilie, Annette M.
collection PubMed
description 18S rRNA is a biomarker that provides an alternative to thick blood smears in controlled human malaria infection (CHMI) trials. We reviewed data from CHMI trials at non-endemic sites that used blood smears and Plasmodium 18S rRNA/rDNA biomarker nucleic acid tests (NATs) for time to positivity. We validated a multiplex quantitative reverse transcription–polymerase chain reaction (qRT-PCR) for Plasmodium 18S rRNA, prospectively compared blood smears and qRT-PCR for three trials, and modeled treatment effects at different biomarker-defined parasite densities to assess the impact on infection detection, symptom reduction, and measured intervention efficacy. Literature review demonstrated accelerated NAT-based infection detection compared with blood smears (mean acceleration: 3.2–3.6 days). For prospectively tested trials, the validated Plasmodium 18S rRNA qRT-PCR positivity was earlier (7.6 days; 95% CI: 7.1–8.1 days) than blood smears (11.0 days; 95% CI: 10.3–11.8 days) and significantly preceded the onset of grade 2 malaria-related symptoms (12.2 days; 95% CI: 10.6–13.3 days). Discrepant analysis showed that the risk of a blood smear–positive, biomarker-negative result was negligible. Data modeling predicted that treatment triggered by specific biomarker-defined thresholds can differentiate complete, partial, and non-protective outcomes and eliminate many grade 2 and most grade 3 malaria-related symptoms post-CHMI. Plasmodium 18S rRNA is a sensitive and specific biomarker that can justifiably replace blood smears for infection detection in CHMI trials in non-endemic settings. This study led to biomarker qualification through the U.S. Food and Drug Administration for use in CHMI studies at non-endemic sites, which will facilitate biomarker use for the qualified context of use in drug and vaccine trials.
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spelling pubmed-65539132019-06-26 Beyond Blood Smears: Qualification of Plasmodium 18S rRNA as a Biomarker for Controlled Human Malaria Infections Seilie, Annette M. Chang, Ming Hanron, Amelia E. Billman, Zachary P. Stone, Brad C. Zhou, Kevin Olsen, Tayla M. Daza, Glenda Ortega, Jose Cruz, Kurtis R. Smith, Nahum Healy, Sara A. Neal, Jillian Wallis, Carolyn K. Shelton, Lisa Mankowski, Tracie (VonGoedert) Wong-Madden, Sharon Mikolajczak, Sebastian A. Vaughan, Ashley M. Kappe, Stefan H. I. Fishbaugher, Matt Betz, Will Kennedy, Mark Hume, Jen C. C. Talley, Angela K. Hoffman, Stephen L. Chakravarty, Sumana Sim, B. Kim Lee Richie, Thomas L. Wald, Anna Plowe, Christopher V. Lyke, Kirsten E. Adams, Matthew Fahle, Gary A. Cowan, Elliot P. Duffy, Patrick E. Kublin, James G. Murphy, Sean C. Am J Trop Med Hyg Articles 18S rRNA is a biomarker that provides an alternative to thick blood smears in controlled human malaria infection (CHMI) trials. We reviewed data from CHMI trials at non-endemic sites that used blood smears and Plasmodium 18S rRNA/rDNA biomarker nucleic acid tests (NATs) for time to positivity. We validated a multiplex quantitative reverse transcription–polymerase chain reaction (qRT-PCR) for Plasmodium 18S rRNA, prospectively compared blood smears and qRT-PCR for three trials, and modeled treatment effects at different biomarker-defined parasite densities to assess the impact on infection detection, symptom reduction, and measured intervention efficacy. Literature review demonstrated accelerated NAT-based infection detection compared with blood smears (mean acceleration: 3.2–3.6 days). For prospectively tested trials, the validated Plasmodium 18S rRNA qRT-PCR positivity was earlier (7.6 days; 95% CI: 7.1–8.1 days) than blood smears (11.0 days; 95% CI: 10.3–11.8 days) and significantly preceded the onset of grade 2 malaria-related symptoms (12.2 days; 95% CI: 10.6–13.3 days). Discrepant analysis showed that the risk of a blood smear–positive, biomarker-negative result was negligible. Data modeling predicted that treatment triggered by specific biomarker-defined thresholds can differentiate complete, partial, and non-protective outcomes and eliminate many grade 2 and most grade 3 malaria-related symptoms post-CHMI. Plasmodium 18S rRNA is a sensitive and specific biomarker that can justifiably replace blood smears for infection detection in CHMI trials in non-endemic settings. This study led to biomarker qualification through the U.S. Food and Drug Administration for use in CHMI studies at non-endemic sites, which will facilitate biomarker use for the qualified context of use in drug and vaccine trials. The American Society of Tropical Medicine and Hygiene 2019-06 2019-04-22 /pmc/articles/PMC6553913/ /pubmed/31017084 http://dx.doi.org/10.4269/ajtmh.19-0094 Text en © The American Society of Tropical Medicine and Hygiene This is an open-access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Articles
Seilie, Annette M.
Chang, Ming
Hanron, Amelia E.
Billman, Zachary P.
Stone, Brad C.
Zhou, Kevin
Olsen, Tayla M.
Daza, Glenda
Ortega, Jose
Cruz, Kurtis R.
Smith, Nahum
Healy, Sara A.
Neal, Jillian
Wallis, Carolyn K.
Shelton, Lisa
Mankowski, Tracie (VonGoedert)
Wong-Madden, Sharon
Mikolajczak, Sebastian A.
Vaughan, Ashley M.
Kappe, Stefan H. I.
Fishbaugher, Matt
Betz, Will
Kennedy, Mark
Hume, Jen C. C.
Talley, Angela K.
Hoffman, Stephen L.
Chakravarty, Sumana
Sim, B. Kim Lee
Richie, Thomas L.
Wald, Anna
Plowe, Christopher V.
Lyke, Kirsten E.
Adams, Matthew
Fahle, Gary A.
Cowan, Elliot P.
Duffy, Patrick E.
Kublin, James G.
Murphy, Sean C.
Beyond Blood Smears: Qualification of Plasmodium 18S rRNA as a Biomarker for Controlled Human Malaria Infections
title Beyond Blood Smears: Qualification of Plasmodium 18S rRNA as a Biomarker for Controlled Human Malaria Infections
title_full Beyond Blood Smears: Qualification of Plasmodium 18S rRNA as a Biomarker for Controlled Human Malaria Infections
title_fullStr Beyond Blood Smears: Qualification of Plasmodium 18S rRNA as a Biomarker for Controlled Human Malaria Infections
title_full_unstemmed Beyond Blood Smears: Qualification of Plasmodium 18S rRNA as a Biomarker for Controlled Human Malaria Infections
title_short Beyond Blood Smears: Qualification of Plasmodium 18S rRNA as a Biomarker for Controlled Human Malaria Infections
title_sort beyond blood smears: qualification of plasmodium 18s rrna as a biomarker for controlled human malaria infections
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6553913/
https://www.ncbi.nlm.nih.gov/pubmed/31017084
http://dx.doi.org/10.4269/ajtmh.19-0094
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