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Functional conservation and coherence of HIV-1 subtype A Vpu alleles.


ABSTRACT: Functional studies of HIV-1 proteins are normally conducted using lab adapted strains of HIV-1. The extent of those functions in clinical strains is sometimes unknown. In this study, we amplified and sequenced HIV-1 Vpu from 10 Iranian patients infected with HIV-1. Phylogenetic analysis indicated that the Vpu alleles were closely related to the CRF35_AD from Iran and subtype A Vpu. We addressed some of the well-established functions of the HIV-1 Vpu, as well as some of its recently reported functions. Ability of the clinical strains of subtype A Vpu alleles for downregulation of CD4 was similar to that of the lab adapted NL4.3 Vpu. Majority of the subtype A Vpu alleles performed stronger than NL4.3 Vpu for downregulation of SNAT1. The Vpu alleles differentially induced downregulation of HLA-C, ranging from no effect to 88% downregulation of surface HLA-C. Downregulation of tetherin and enhancement of virus release was similar for the subtype A Vpu alleles and NL4.3. Subtype A Vpu alleles were more potent when compared with NL4.3 for inhibition of NF-?B activation. Our study shows that subtype A Vpu alleles exert the classical functions of HIV-1 Vpu.

SUBMITTER: Romani B 

PROVIDER: S-EPMC5357900 | biostudies-literature | 2017 Mar

REPOSITORIES: biostudies-literature

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Functional conservation and coherence of HIV-1 subtype A Vpu alleles.

Romani Bizhan B   Kavyanifard Amirarsalan A   Allahbakhshi Elham E  

Scientific reports 20170320


Functional studies of HIV-1 proteins are normally conducted using lab adapted strains of HIV-1. The extent of those functions in clinical strains is sometimes unknown. In this study, we amplified and sequenced HIV-1 Vpu from 10 Iranian patients infected with HIV-1. Phylogenetic analysis indicated that the Vpu alleles were closely related to the CRF35_AD from Iran and subtype A Vpu. We addressed some of the well-established functions of the HIV-1 Vpu, as well as some of its recently reported func  ...[more]

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2019-02-05 | GSE117655 | GEO