Author
Listed:
- Mariya B. Shapiro
(Oregon Health & Science University)
- Tracy Cheever
(Oregon Health & Science University)
- Delphine C. Malherbe
(Oregon Health & Science University
University of Texas Medical Branch)
- Shilpi Pandey
(Oregon Health & Science University)
- Jason Reed
(Oregon Health & Science University)
- Eun Sung Yang
(Vaccine Research Center, NIAID/NIH)
- Keyun Wang
(Vaccine Research Center, NIAID/NIH)
- Amarendra Pegu
(Vaccine Research Center, NIAID/NIH)
- Xuejun Chen
(Vaccine Research Center, NIAID/NIH)
- Don Siess
(Oregon Health & Science University)
- David Burke
(Oregon Health & Science University)
- Heidi Henderson
(Oregon Health & Science University)
- Rebecca Lewinsohn
(Oregon Health & Science University)
- Miranda Fischer
(Oregon Health & Science University)
- Jeffrey J. Stanton
(Oregon Health & Science University)
- Michael K. Axthelm
(Oregon Health & Science University)
- Christoph Kahl
(Oregon Health & Science University
Atara Biotherapeutics)
- Byung Park
(Oregon Health & Science University)
- Anne D. Lewis
(Oregon Health & Science University)
- Jonah B. Sacha
(Oregon Health & Science University
Oregon Health & Science University
Oregon Health & Science University)
- John R. Mascola
(Vaccine Research Center, NIAID/NIH)
- Ann J. Hessell
(Oregon Health & Science University)
- Nancy L. Haigwood
(Oregon Health & Science University
Oregon Health & Science University)
Abstract
Vertical transmission accounts for most human immunodeficiency virus (HIV) infection in children, and treatments for newborns are needed to abrogate infection or limit disease progression. We showed previously that short-term broadly neutralizing antibody (bNAb) therapy given 24 h after oral exposure cleared simian-human immunodeficiency virus (SHIV) in a macaque model of perinatal infection. Here, we report that all infants given either a single dose of bNAbs at 30 h, or a 21-day triple-drug ART regimen at 48 h, are aviremic with almost no virus in tissues. In contrast, bNAb treatment beginning at 48 h leads to tight control without adaptive immune responses in half of animals. We conclude that both bNAbs and ART mediate effective post-exposure prophylaxis in infant macaques within 30–48 h of oral SHIV exposure. Our findings suggest that optimizing the treatment regimen may extend the window of opportunity for preventing perinatal HIV infection when treatment is delayed.
Suggested Citation
Mariya B. Shapiro & Tracy Cheever & Delphine C. Malherbe & Shilpi Pandey & Jason Reed & Eun Sung Yang & Keyun Wang & Amarendra Pegu & Xuejun Chen & Don Siess & David Burke & Heidi Henderson & Rebecca , 2020.
"Single-dose bNAb cocktail or abbreviated ART post-exposure regimens achieve tight SHIV control without adaptive immunity,"
Nature Communications, Nature, vol. 11(1), pages 1-13, December.
Handle:
RePEc:nat:natcom:v:11:y:2020:i:1:d:10.1038_s41467-019-13972-y
DOI: 10.1038/s41467-019-13972-y
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Citations
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Cited by:
- Joana Dias & Giulia Fabozzi & Slim Fourati & Xuejun Chen & Cuiping Liu & David R. Ambrozak & Amy Ransier & Farida Laboune & Jianfei Hu & Wei Shi & Kylie March & Anna A. Maximova & Stephen D. Schmidt &, 2024.
"Administration of anti-HIV-1 broadly neutralizing monoclonal antibodies with increased affinity to Fcγ receptors during acute SHIVAD8-EO infection,"
Nature Communications, Nature, vol. 15(1), pages 1-18, December.
- Xiaolei Wang & Eunice Vincent & Summer Siddiqui & Katherine Turnbull & Hong Lu & Robert Blair & Xueling Wu & Meagan Watkins & Widade Ziani & Jiasheng Shao & Lara A. Doyle-Meyers & Kasi E. Russell-Lodr, 2022.
"Early treatment regimens achieve sustained virologic remission in infant macaques infected with SIV at birth,"
Nature Communications, Nature, vol. 13(1), pages 1-12, December.
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