Proteomic profiling of SupT1 cells reveal modulation of host proteins by HIV-1 Nef variants.

Proteomic profiling of SupT1 cells reveal modulation of host proteins by HIV-1 Nef variants.

Nef is an accessory viral protein that promotes HIV-1 replication, facilitating alterations in cellular pathways via multiple protein-protein interactions. The advent of proteomics has expanded the focus on better identification of novel molecular pathways regulating disease progression. In this stu...

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Main Authors: Reshu Saxena, Sudipti Gupta, Kavita Singh, Kalyan Mitra, Anil Kumar Tripathi, Raj Kamal Tripathi
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2015-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4395413?pdf=render
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spelling doaj-6d3171a8b9cb419fbe959f5fa11fe7e92020-11-24T21:56:45ZengPublic Library of Science (PLoS)PLoS ONE1932-62032015-01-01104e012299410.1371/journal.pone.0122994Proteomic profiling of SupT1 cells reveal modulation of host proteins by HIV-1 Nef variants.Reshu SaxenaSudipti GuptaKavita SinghKalyan MitraAnil Kumar TripathiRaj Kamal TripathiNef is an accessory viral protein that promotes HIV-1 replication, facilitating alterations in cellular pathways via multiple protein-protein interactions. The advent of proteomics has expanded the focus on better identification of novel molecular pathways regulating disease progression. In this study, nef was sequenced from randomly selected patients, however, sequence variability identified did not elicited any specific mutation that could have segregated HIV-1 patients in different stages of disease progression. To explore the difference in Nef functionality based on sequence variability we used proteomics approach. Proteomic profiling was done to compare the effect of Nef variants in host cell protein expression. 2DGE in control and Nef transfected SupT1 cells demonstrated several differentially expressed proteins. Fourteen protein spots were detected with more than 1.5 fold difference. Significant down regulation was seen in six unique protein spots in the Nef treated cells. Proteins were identified as Cyclophilin A, EIF5A-1 isoform B, Rho GDI 1 isoform a, VDAC1, OTUB1 and α-enolase isoform 1 (ENO1) through LC-MS/MS. The differential expression of the 6 proteins was analyzed by Real time PCR, Western blotting and Immunofluorescence studies with two Nef variants (RP14 and RP01) in SupT1 cells. There was contrasting difference between the effect of these Nef variants upon the expression of these six proteins. Downregulation of α-enolase (ENO1), VDAC1 and OTUB1 was more significant by Nef RP01 whereas Cyclophilin A and RhoGDI were found to be more downregulated by Nef RP14. This difference in Nef variants upon host protein expression was also studied through a site directed mutant of Nef RP01 (55AAAAAAA61) and the effect was found to be reversed. Deciphering the role of these proteins mediated by Nef variants will open a new avenue of research in understanding Nef mediated pathogenesis. Overall study determines modulation of cellular protein expression in T cells by HIV-1 Nef variants.http://europepmc.org/articles/PMC4395413?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Reshu Saxena
Sudipti Gupta
Kavita Singh
Kalyan Mitra
Anil Kumar Tripathi
Raj Kamal Tripathi
spellingShingle Reshu Saxena
Sudipti Gupta
Kavita Singh
Kalyan Mitra
Anil Kumar Tripathi
Raj Kamal Tripathi
Proteomic profiling of SupT1 cells reveal modulation of host proteins by HIV-1 Nef variants.
PLoS ONE
author_facet Reshu Saxena
Sudipti Gupta
Kavita Singh
Kalyan Mitra
Anil Kumar Tripathi
Raj Kamal Tripathi
author_sort Reshu Saxena
title Proteomic profiling of SupT1 cells reveal modulation of host proteins by HIV-1 Nef variants.
title_short Proteomic profiling of SupT1 cells reveal modulation of host proteins by HIV-1 Nef variants.
title_full Proteomic profiling of SupT1 cells reveal modulation of host proteins by HIV-1 Nef variants.
title_fullStr Proteomic profiling of SupT1 cells reveal modulation of host proteins by HIV-1 Nef variants.
title_full_unstemmed Proteomic profiling of SupT1 cells reveal modulation of host proteins by HIV-1 Nef variants.
title_sort proteomic profiling of supt1 cells reveal modulation of host proteins by hiv-1 nef variants.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2015-01-01
description Nef is an accessory viral protein that promotes HIV-1 replication, facilitating alterations in cellular pathways via multiple protein-protein interactions. The advent of proteomics has expanded the focus on better identification of novel molecular pathways regulating disease progression. In this study, nef was sequenced from randomly selected patients, however, sequence variability identified did not elicited any specific mutation that could have segregated HIV-1 patients in different stages of disease progression. To explore the difference in Nef functionality based on sequence variability we used proteomics approach. Proteomic profiling was done to compare the effect of Nef variants in host cell protein expression. 2DGE in control and Nef transfected SupT1 cells demonstrated several differentially expressed proteins. Fourteen protein spots were detected with more than 1.5 fold difference. Significant down regulation was seen in six unique protein spots in the Nef treated cells. Proteins were identified as Cyclophilin A, EIF5A-1 isoform B, Rho GDI 1 isoform a, VDAC1, OTUB1 and α-enolase isoform 1 (ENO1) through LC-MS/MS. The differential expression of the 6 proteins was analyzed by Real time PCR, Western blotting and Immunofluorescence studies with two Nef variants (RP14 and RP01) in SupT1 cells. There was contrasting difference between the effect of these Nef variants upon the expression of these six proteins. Downregulation of α-enolase (ENO1), VDAC1 and OTUB1 was more significant by Nef RP01 whereas Cyclophilin A and RhoGDI were found to be more downregulated by Nef RP14. This difference in Nef variants upon host protein expression was also studied through a site directed mutant of Nef RP01 (55AAAAAAA61) and the effect was found to be reversed. Deciphering the role of these proteins mediated by Nef variants will open a new avenue of research in understanding Nef mediated pathogenesis. Overall study determines modulation of cellular protein expression in T cells by HIV-1 Nef variants.
url http://europepmc.org/articles/PMC4395413?pdf=render
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