HIV-1逆转录酶β8-αE环上第154位带正电荷的侧链是形成稳定三元复合物所必需的。

A positively charged side chain at position 154 on the beta8-alphaE loop of HIV-1 RT is required for stable ternary complex formation.

作者信息

Sharma Bechan, Kaushik Neerja, Upadhyay Alok, Tripathi Snehlata, Singh Kamalendra, Pandey Virendra N

机构信息

Department of Biochemistry and Molecular Biology, Center for the Study of Emerging and Re-Emerging Pathogens, University of Medicine and Dentistry of New Jersey, New Jersey Medical School, 185 South Orange Avenue, Newark, NJ 07103, USA.

出版信息

Nucleic Acids Res. 2003 Sep 1;31(17):5167-74. doi: 10.1093/nar/gkg708.

DOI:10.1093/nar/gkg708

PMID:12930968

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC212807/

Abstract

Lys154 is the only positively charged residue located in the VLPQGWK motif on the beta8-alphaE loop at the junction of the fingers and palm subdomains of human immunodeficiency virus type 1 reverse transcriptase (HIV-1 RT). Some of the conserved residues in this motif are critical for RT function, while others have been shown to confer nucleoside drug resistance and fidelity to the enzyme. In order to understand the functional implication of this positively charged residue, we carried out site-directed mutagenesis at position 154 and biochemically characterized the mutant enzymes. Mutants carrying negatively charged side chains (K154D and K154E) were severely impaired in their polymerase function, while those with hydrophobic side chains (K154A and K154I) were moderately affected. Analysis of the binary complexes formed by these mutants revealed that all the mutant derivatives retained their ability to form an enzyme template primer (E-TP) binary complex similar to the wild-type enzyme. In contrast, their ability to form stable E-TP-dNTP ternary complexes varied greatly and was dependent on the nature of the side chain at position 154. The conservative Lys-->Arg mutant was not affected in its ability to form a stable ternary complex, while those carrying non-polar or negatively charged side chains were significantly impaired. The apparent K(d [dNTP]) values for these non-conservative mutants were approximately 16- to 400-fold higher than the wild-type enzyme, indicating that a positively charged side chain at position 154 may be required for efficient formation of a stable ternary complex. Interestingly, all the mutant derivatives of Lys154 were completely resistant to a nucleoside analog inhibitor, 3'-dideoxy 3'-thiacytidine (3TC), implying that Lys154 may play a role in conferring 3TC sensitivity to HIV-1 RT. These findings are discussed in the context of the binary and ternary complex crystal structures of HIV-1 RT.

摘要

赖氨酸154是位于人免疫缺陷病毒1型逆转录酶（HIV-1 RT）指状结构域和掌状结构域交界处β8-αE环上VLPQGWK基序中的唯一带正电荷残基。该基序中的一些保守残基对逆转录酶功能至关重要，而其他一些残基已被证明赋予该酶核苷类药物抗性和保真度。为了了解这个带正电荷残基的功能意义，我们在第154位进行了定点诱变，并对突变酶进行了生化特性分析。携带带负电荷侧链的突变体（K154D和K154E）的聚合酶功能严重受损，而带有疏水侧链的突变体（K154A和K154I）受到中度影响。对这些突变体形成的二元复合物的分析表明，所有突变衍生物都保留了与野生型酶类似的形成酶模板引物（E-TP）二元复合物的能力。相比之下，它们形成稳定的E-TP-dNTP三元复合物的能力差异很大，并且取决于第154位侧链的性质。保守的赖氨酸→精氨酸突变体形成稳定三元复合物的能力未受影响，而携带非极性或带负电荷侧链的突变体则明显受损。这些非保守突变体的表观K（d [dNTP]）值比野生型酶高约16至400倍，表明第154位的带正电荷侧链可能是有效形成稳定三元复合物所必需的。有趣的是，赖氨酸154的所有突变衍生物对核苷类似物抑制剂3'-双脱氧3'-硫代胞苷（3TC）完全耐药，这意味着赖氨酸154可能在赋予HIV-1 RT对3TC敏感性方面发挥作用。将结合HIV-1 RT的二元和三元复合物晶体结构对这些发现进行讨论。