Please use this identifier to cite or link to this item: http://hdl.handle.net/123456789/1004
Title: Impact of Genetic Variations in HIV-1 Tat on LTR-Mediated Transcription via TAR RNA Interaction
Authors: Banerjea, Akhil C
Ronsard, Larance
Ganguli, Nilanjana
Singh, Vivek K.
Mohankumar, Kumaravel
Rai, Tripti
Sridharan, Subhashree
Pajaniradje, Sankar
Kumar, Binod
Rai, Devesh
Chaudhuri, Suhnrita
Coumar, Mohane S.
Ramachandran, Vishnampettai G.
Issue Date: Apr-2017
Publisher: Frontiers Media S.A
Abstract: HIV-1 evades host defense through mutations and recombination events, generating numerous variants in an infected patient. These variants with an undiminished virulence can multiply rapidly in order to progress to AIDS. One of the targets to intervene in HIV-1 replication is the trans-activator of transcription (Tat), a major regulatory protein that transactivates the long terminal repeat promoter through its interaction with trans-activation response (TAR) RNA. In this study, HIV-1 infected patients (n = 120) from North India revealed Ser46Phe (20%) and Ser61Arg (2%) mutations in the Tat variants with a strong interaction toward TAR leading to enhanced transactivation activities. Molecular dynamics simulation data verified that the variants with this mutation had a higher binding affinity for TAR than both the wild-type Tat and other variants that lacked Ser46Phe and Ser61Arg. Other mutations in Tat conferred varying affinities for TAR interaction leading to differential transactivation abilities. This is the first report from North India with a clinical validation of CD4 counts to demonstrate the influence of Tat genetic variations affecting the stability of Tat and its interaction with TAR. This study highlights the co-evolution pattern of Tat and predominant nucleotides for Tat activity, facilitating the identification of genetic determinants for the attenuation of viral gene expression.
URI: http://hdl.handle.net/123456789/1004
Appears in Collections:Virology- II, Publications

Files in This Item:
File Description SizeFormat 
fmicb-08-00706 (1).pdf2.61 MBAdobe PDFView/Open    Request a copy


Items in DSpace are protected by copyright, with all rights reserved, unless otherwise indicated.