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Malaria in pregnancy alters L-arginine bioavailability and placental vascular development

Reducing adverse birth outcomes due to malaria in pregnancy (MIP) is a global health priority. However, there are few safe and effective interventions. L-arginine is an essential amino acid in pregnancy and an immediate precursor in the biosynthesis of nitric oxide (NO), but there are limited data o...

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Autores principales: McDonald, Chloe R., Cahill, Lindsay S., Gamble, Joel L., Elphinstone, Robyn, Gazdzinski, Lisa M., Zhong, Kathleen J. Y., Philson, Adrienne C., Madanitsa, Mwayiwawo, Kalilani-Phiri, Linda, Mwapasa, Victor, ter Kuile, Feiko O., Sled, John G., Conroy, Andrea L., Kain, Kevin C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Association for the Advancement of Science 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6510298/
https://www.ncbi.nlm.nih.gov/pubmed/29514999
http://dx.doi.org/10.1126/scitranslmed.aan6007
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author McDonald, Chloe R.
Cahill, Lindsay S.
Gamble, Joel L.
Elphinstone, Robyn
Gazdzinski, Lisa M.
Zhong, Kathleen J. Y.
Philson, Adrienne C.
Madanitsa, Mwayiwawo
Kalilani-Phiri, Linda
Mwapasa, Victor
ter Kuile, Feiko O.
Sled, John G.
Conroy, Andrea L.
Kain, Kevin C.
author_facet McDonald, Chloe R.
Cahill, Lindsay S.
Gamble, Joel L.
Elphinstone, Robyn
Gazdzinski, Lisa M.
Zhong, Kathleen J. Y.
Philson, Adrienne C.
Madanitsa, Mwayiwawo
Kalilani-Phiri, Linda
Mwapasa, Victor
ter Kuile, Feiko O.
Sled, John G.
Conroy, Andrea L.
Kain, Kevin C.
author_sort McDonald, Chloe R.
collection PubMed
description Reducing adverse birth outcomes due to malaria in pregnancy (MIP) is a global health priority. However, there are few safe and effective interventions. L-arginine is an essential amino acid in pregnancy and an immediate precursor in the biosynthesis of nitric oxide (NO), but there are limited data on the impact of MIP on NO biogenesis. We hypothesized that hypoarginemia contributes to the pathophysiology of MIP and that L-arginine supplementation would improve birth outcomes. In a prospective study of pregnant Malawian women, we show that MIP was associated with lower concentrations of L- arginine and higher concentrations of endogenous inhibitors of NO biosynthesis, asymmetric and symmetric dimethylarginine, which were associated with adverse birth outcomes. In a model of experimental MIP, L-arginine supplementation in dams improved birth outcomes (decreased stillbirth and increased birth weight) compared with controls. The mechanism of action was via normalized angiogenic pathways and enhanced placental vascular development, as visualized by placental microcomputerized tomography imaging. These data define a role for dysregulation of NO biosynthetic pathways in the pathogenesis of MIP and support the evaluation of interventions to enhance L-arginine bioavailability as strategies to improve birth outcomes.
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spelling pubmed-65102982019-05-30 Malaria in pregnancy alters L-arginine bioavailability and placental vascular development McDonald, Chloe R. Cahill, Lindsay S. Gamble, Joel L. Elphinstone, Robyn Gazdzinski, Lisa M. Zhong, Kathleen J. Y. Philson, Adrienne C. Madanitsa, Mwayiwawo Kalilani-Phiri, Linda Mwapasa, Victor ter Kuile, Feiko O. Sled, John G. Conroy, Andrea L. Kain, Kevin C. Sci Transl Med Malaria Reducing adverse birth outcomes due to malaria in pregnancy (MIP) is a global health priority. However, there are few safe and effective interventions. L-arginine is an essential amino acid in pregnancy and an immediate precursor in the biosynthesis of nitric oxide (NO), but there are limited data on the impact of MIP on NO biogenesis. We hypothesized that hypoarginemia contributes to the pathophysiology of MIP and that L-arginine supplementation would improve birth outcomes. In a prospective study of pregnant Malawian women, we show that MIP was associated with lower concentrations of L- arginine and higher concentrations of endogenous inhibitors of NO biosynthesis, asymmetric and symmetric dimethylarginine, which were associated with adverse birth outcomes. In a model of experimental MIP, L-arginine supplementation in dams improved birth outcomes (decreased stillbirth and increased birth weight) compared with controls. The mechanism of action was via normalized angiogenic pathways and enhanced placental vascular development, as visualized by placental microcomputerized tomography imaging. These data define a role for dysregulation of NO biosynthetic pathways in the pathogenesis of MIP and support the evaluation of interventions to enhance L-arginine bioavailability as strategies to improve birth outcomes. American Association for the Advancement of Science 2018-03-07 2018 /pmc/articles/PMC6510298/ /pubmed/29514999 http://dx.doi.org/10.1126/scitranslmed.aan6007 Text en © 2018 The Authors, some rights reserved http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution license, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Malaria
McDonald, Chloe R.
Cahill, Lindsay S.
Gamble, Joel L.
Elphinstone, Robyn
Gazdzinski, Lisa M.
Zhong, Kathleen J. Y.
Philson, Adrienne C.
Madanitsa, Mwayiwawo
Kalilani-Phiri, Linda
Mwapasa, Victor
ter Kuile, Feiko O.
Sled, John G.
Conroy, Andrea L.
Kain, Kevin C.
Malaria in pregnancy alters L-arginine bioavailability and placental vascular development
title Malaria in pregnancy alters L-arginine bioavailability and placental vascular development
title_full Malaria in pregnancy alters L-arginine bioavailability and placental vascular development
title_fullStr Malaria in pregnancy alters L-arginine bioavailability and placental vascular development
title_full_unstemmed Malaria in pregnancy alters L-arginine bioavailability and placental vascular development
title_short Malaria in pregnancy alters L-arginine bioavailability and placental vascular development
title_sort malaria in pregnancy alters l-arginine bioavailability and placental vascular development
topic Malaria
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6510298/
https://www.ncbi.nlm.nih.gov/pubmed/29514999
http://dx.doi.org/10.1126/scitranslmed.aan6007
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