Origin and evolution of HIV-1 in breast milk determined by single-genome amplification and sequencing.

Salazar-Gonzalez, JF; Salazar, MG; Learn, GH; Fouda, GG; Kang, HH; Mahlokozera, T; Wilks, AB; Lovingood, RV; Stacey, A; Kalilani, L; Meshnick, SR; Borrow, P; Montefiori, DC; Denny, TN; Letvin, NL; Shaw, GM; Hahn, BH; Permar, SR; A0167854, Center for HIV AIDS Vaccine Immunology

Origin and evolution of HIV-1 in breast milk determined by single-genome amplification and sequencing.

dc.contributor.author	Salazar-Gonzalez, JF
dc.contributor.author	Salazar, MG
dc.contributor.author	Learn, GH
dc.contributor.author	Fouda, GG
dc.contributor.author	Kang, HH
dc.contributor.author	Mahlokozera, T
dc.contributor.author	Wilks, AB
dc.contributor.author	Lovingood, RV
dc.contributor.author	Stacey, A
dc.contributor.author	Kalilani, L
dc.contributor.author	Meshnick, SR
dc.contributor.author	Borrow, P
dc.contributor.author	Montefiori, DC
dc.contributor.author	Denny, TN
dc.contributor.author	Letvin, NL
dc.contributor.author	Shaw, GM
dc.contributor.author	Hahn, BH
dc.contributor.author	Permar, SR
dc.contributor.author	A0167854, Center for HIV AIDS Vaccine Immunology
dc.coverage.spatial	United States
dc.date.accessioned	2017-06-02T12:49:10Z
dc.date.available	2017-06-02T12:49:10Z
dc.date.issued	2011-03
dc.description.abstract	HIV transmission via breastfeeding accounts for a considerable proportion of infant HIV acquisition. However, the origin and evolution of the virus population in breast milk, the likely reservoir of transmitted virus variants, are not well characterized. In this study, HIV envelope (env) genes were sequenced from virus variants amplified by single-genome amplification from plasmas and milk of 12 chronically HIV-infected, lactating Malawian women. Maximum likelihood trees and statistical tests of compartmentalization revealed interspersion of plasma and milk HIV env sequences in the majority of subjects, indicating limited or no compartmentalization of milk virus variants. However, phylogenetic tree analysis further revealed monotypic virus variants that were significantly more frequent in milk (median proportion of identical viruses, 29.5%; range, 0 to 61%) than in plasma (median proportion of identical viruses, 0%; range, 0 to 26%) (P = 0.002), suggesting local virus replication in the breast milk compartment. Moreover, clonally amplified virus env genes in milk produced functional virus Envs that were all CCR5 tropic. Milk and plasma virus Envs had similar predicted phenotypes and neutralization sensitivities to broadly neutralizing antibodies in both transmitting and nontransmitting mothers. Finally, phylogenetic comparison of longitudinal milk and plasma virus env sequences revealed synchronous virus evolution and new clonal amplification of evolved virus env genes in milk. The limited compartmentalization and the clonal amplification of evolving, functional viruses in milk indicate continual seeding of the mammary gland by blood virus variants, followed by transient local replication of these variants in the breast milk compartment.
dc.identifier	https://www.ncbi.nlm.nih.gov/pubmed/21191008
dc.identifier	JVI.02316-10
dc.identifier.eissn	1098-5514
dc.identifier.uri	https://hdl.handle.net/10161/14740
dc.language	eng
dc.publisher	American Society for Microbiology
dc.relation.ispartof	J Virol
dc.relation.isversionof	10.1128/JVI.02316-10
dc.subject	Cluster Analysis
dc.subject	Evolution, Molecular
dc.subject	Female
dc.subject	Genetic Variation
dc.subject	HIV Infections
dc.subject	HIV-1
dc.subject	Humans
dc.subject	Infant
dc.subject	Infant, Newborn
dc.subject	Malawi
dc.subject	Milk, Human
dc.subject	Molecular Sequence Data
dc.subject	Phylogeny
dc.subject	Plasma
dc.subject	Pregnancy
dc.subject	RNA, Viral
dc.subject	Receptors, CCR5
dc.subject	Receptors, HIV
dc.subject	Sequence Analysis, DNA
dc.subject	Sequence Homology
dc.subject	Viral Tropism
dc.subject	env Gene Products, Human Immunodeficiency Virus
dc.title	Origin and evolution of HIV-1 in breast milk determined by single-genome amplification and sequencing.
dc.type	Journal article
duke.contributor.orcid	Montefiori, DC\|0000-0003-0856-6319
pubs.author-url	https://www.ncbi.nlm.nih.gov/pubmed/21191008
pubs.begin-page	2751
pubs.end-page	2763
pubs.issue	6
pubs.organisational-group	Basic Science Departments
pubs.organisational-group	Clinical Science Departments
pubs.organisational-group	Duke
pubs.organisational-group	Duke Human Vaccine Institute
pubs.organisational-group	Immunology
pubs.organisational-group	Institutes and Centers
pubs.organisational-group	Medicine
pubs.organisational-group	Medicine, Duke Human Vaccine Institute
pubs.organisational-group	Molecular Genetics and Microbiology
pubs.organisational-group	Pediatrics
pubs.organisational-group	Pediatrics, Infectious Diseases
pubs.organisational-group	School of Medicine
pubs.organisational-group	Surgery
pubs.organisational-group	Surgery, Surgical Sciences
pubs.publication-status	Published
pubs.volume	85

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