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Phenotypic properties of transmitted founder HIV-1

Authors :
Beatrice H. Hahn
Lara Zajic
Bhavna Hora
George M. Shaw
Julie M. Decker
Amit Kumar
Haitao Ding
Jennifer Hopper
Christina Ochsenbauer
Anthony P. West
Robert W. Doms
John C. Kappes
Feng Gao
Shilpa S. Iyer
Thomas N. Denny
Barton F. Haynes
Mark Muldoon
Nina Bhardwaj
Hannah J. Barbian
Hui Li
Nicholas F. Parrish
James Theiler
Fangping Cai
Erica H. Parrish
Elena E. Giorgi
Anna Berg
Persephone Borrow
Pamela J. Bjorkman
Bette T. Korber
Craig B. Wilen
Meagan O’Brien
Rachel P. Galimidi
Source :
Proceedings of the National Academy of Sciences. 110:6626-6633
Publication Year :
2013
Publisher :
Proceedings of the National Academy of Sciences, 2013.

Abstract

Defining the virus–host interactions responsible for HIV-1 transmission, including the phenotypic requirements of viruses capable of establishing de novo infections, could be important for AIDS vaccine development. Previous analyses have failed to identify phenotypic properties other than chemokine receptor 5 (CCR5) and CD4+ T-cell tropism that are preferentially associated with viral transmission. However, most of these studies were limited to examining envelope (Env) function in the context of pseudoviruses. Here, we generated infectious molecular clones of transmitted founder (TF; n = 27) and chronic control (CC; n = 14) viruses of subtypes B ( n = 18) and C ( n = 23) and compared their phenotypic properties in assays specifically designed to probe the earliest stages of HIV-1 infection. We found that TF virions were 1.7-fold more infectious ( P = 0.049) and contained 1.9-fold more Env per particle ( P = 0.048) compared with CC viruses. TF viruses were also captured by monocyte-derived dendritic cells 1.7-fold more efficiently ( P = 0.035) and more readily transferred to CD4+ T cells ( P = 0.025). In primary CD4+ T cells, TF and CC viruses replicated with comparable kinetics; however, when propagated in the presence of IFN-α, TF viruses replicated to higher titers than CC viruses. This difference was significant for subtype B ( P = 0.000013) but not subtype C ( P = 0.53) viruses, possibly reflecting demographic differences of the respective patient cohorts. Together, these data indicate that TF viruses are enriched for higher Env content, enhanced cell-free infectivity, improved dendritic cell interaction, and relative IFN-α resistance. These viral properties, which likely act in concert, should be considered in the development and testing of AIDS vaccines.

Details

ISSN :
10916490 and 00278424
Volume :
110
Database :
OpenAIRE
Journal :
Proceedings of the National Academy of Sciences
Accession number :
edsair.doi.dedup.....86e08d5133b8c1182703192f2399d14c
Full Text :
https://doi.org/10.1073/pnas.1304288110