نتایج جستجو برای: hiv 1 pr

تعداد نتایج: 2909370  

Journal: :The Journal of general virology 2007
Tamás Sperka Gabriella Miklóssy Yunfeng Tie Péter Bagossi Gábor Zahuczky Péter Boross Krisztina Matúz Robert W Harrison Irene T Weber József Tözsér

Bovine leukemia virus (BLV) is a valuable model system for understanding human T-lymphotropic virus 1 (HTLV-1); the availability of an infectious BLV clone, together with animal-model systems, will help to explore anti-HTLV-1 strategies. Nevertheless, the specificity and inhibitor sensitivity of the BLV protease (PR) have not been characterized in detail. To facilitate such studies, a molecular...

2004
R. A. Broglia G. Tiana D. Provasi F. Simona L. Sutto F. Vasile M. Zanotti

Being HIV–1–PR an essential enzyme in the viral life cycle, its inhibition can control AIDS. Because the folding of single domain proteins, like HIV–1–PR is controlled by local elementary structures (LES, folding units stabilized by strongly interacting, highly conserved amino acids) which have evolved over myriads of generations to recognize and strongly attract each other so as to make the pr...

2014
Esther Torrecilla Teresa Llácer Delicado África Holguín

BACKGROUND Polymorphisms at cleavage sites (CS) can influence Gag and Pol proteins processing by the viral protease (PR), restore viral fitness and influence the virological outcome of specific antiretroviral drugs. However, data of HIV-1 variant-associated CS variability is scarce. METHODS In this descriptive research, we examine the effect of HIV-1 variants on CS conservation using all 9,02...

Journal: :Journal of virology 2008
Milan Kozísek Klára Grantz Sasková Pavlína Rezácová Jirí Brynda Noortje M van Maarseveen Dorien De Jong Charles A Boucher Ron M Kagan Monique Nijhuis Jan Konvalinka

While the selection of amino acid insertions in human immunodeficiency virus (HIV) reverse transcriptase (RT) is a known mechanism of resistance against RT inhibitors, very few reports on the selection of insertions in the protease (PR) coding region have been published. It is still unclear whether these insertions impact protease inhibitor (PI) resistance and/or viral replication capacity. We ...

Journal: :Journal of virology 1988
H G Kräusslich H Schneider G Zybarth C A Carter E Wimmer

We expressed the gag and proteinase regions of human immunodeficiency virus (HIV) type 1 by transcription and translation in vitro. A synthetic RNA spanning the gag and pro domains gave primarily the unprocessed capsid precursor pr53. Efficient cleavage of this precursor was observed when the gag and pro domains were placed in the same translational reading frame, yielding equimolar amounts of ...

Journal: :Journal of virology 2010
Abdul A Waheed Sherimay D Ablan Raymond C Sowder James D Roser Carl P Schaffner Elena Chertova Eric O Freed

We previously reported that human immunodeficiency virus type 1 (HIV-1) develops resistance to the cholesterol-binding compound amphotericin B methyl ester (AME) by acquiring mutations (P203L and S205L) in the cytoplasmic tail of the transmembrane envelope glycoprotein gp41 that create cleavage sites for the viral protease (PR). In the present study, we observed that a PR inhibitor-resistant (P...

Journal: :Journal of clinical virology : the official publication of the Pan American Society for Clinical Virology 2009
João Pereira-Vaz Vitor Duque Luís Trindade José Saraiva-da-Cunha António Meliço-Silvestre

BACKGROUND Amino acids insertions in the protease (PR) coding region have been reported in protease inhibitors (PIs) treatment-naïve and experienced HIV-1 infected individuals ranging from 0.1% to 4.55% and have been rarely found in non-B HIV-1 subtype strains. OBJECTIVES To investigate the presence of amino acid insertions in the PR coding region in sequences from treatment-naïve HIV-1 infec...

2016
Rosemberg O. Soares Pedro H.M. Torres Manuela L. da Silva Pedro G. Pascutti

The data described here supports the research article "Unraveling HIV Protease Flaps Dynamics by Constant pH Molecular Dynamics Simulations" (Soares et al., 2016) [1]. The data involves both standard Molecular Dynamics (MD) and Constant pH Molecular Dynamics (CpHMD) to elucidate the effect of protonation states of catalytic dyad on the HIV-PR conformation. The data obtained from MD simulation d...

Journal: :The Journal of biological chemistry 2001
C Dash M Rao

The active site cleft of the HIV-1 protease (PR) is bound by two identical conformationally mobile loops known as flaps, which are important for substrate binding and catalysis. The present article reports, for the first time, an HIV-1 PR inhibitor, ATBI, from an extremophilic Bacillus sp. The inhibitor is found to be a hydrophilic peptide with Mr of 1147, and an amino acid sequence of Ala-Gly-...

2015
Sonald Duclair Archana Gautam Andrew Ellington Vinayaka R Prasad

HIV-1 aspartyl protease (PR) plays a key role in virion morphogenesis, underscoring the effectiveness of protease inhibitors (PI). Despite their utility, side effects and drug-resistance remains a problem. We report the development of RNA aptamers as inhibitors of HIV-1 PR for potential use in anti-HIV gene therapy. Employing Systematic Evolution of Ligands by Exponential Enrichment (SELEX), we...

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