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The M184V Mutation in the Reverse Transcriptase of Human Immunodeficiency Virus Type 1 Impairs Rescue of Chain-Terminated DNA Synthesis

机译:人类免疫缺陷病毒1型逆转录酶中的M184V突变削弱了链终止DNA合成的救援。

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摘要

Nucleoside analog chain terminators such as 3′-azido-3′-deoxythymidine (AZT) and 2′,3′-dideoxy-3′-thiacytidine (3TC) represent an important class of drugs that are used in the clinic to inhibit the reverse transcriptase (RT) of human immunodeficiency virus type 1. Recent data have suggested that mutant enzymes associated with AZT resistance are capable of removing the chain-terminating residue with much greater efficiency than wild-type RT and this may, in turn, facilitate rescue of DNA synthesis; these experiments were performed using physiological concentrations of pyrophosphate or nucleoside triphosphates, respectively. The present study demonstrates that the M184V mutation, which confers high-level resistance to 3TC, can severely compromise the removal of chain-terminating nucleotides. Pyrophosphorolysis on 3TC-terminated primer strands was not detectable with M184V-containing, as opposed to wild-type, RT, and rescue of AZT-terminated DNA synthesis was significantly decreased with the former enzyme. Thus, mutated RTs associated with resistance to AZT and 3TC possess opposing, and therefore incompatible, phenotypes in this regard. These results are consistent with tissue culture and clinical data showing sustained antiviral effects of AZT in the context of viruses that contain the M184V mutation in the RT-encoding gene.
机译:核苷类似物链终止剂,例如3'-叠氮基3'-脱氧胸苷(AZT)和2',3'-二脱氧-3'-硫代胞苷(3TC)代表了一类重要的药物,可用于临床抑制逆转1型人类免疫缺陷病毒的转录酶(RT)。最新数据表明,与AZT抗性相关的突变酶能够以比野生型RT高得多的效率去除链终止残基,这反过来可能有助于拯救DNA合成;这些实验分别使用生理浓度的焦磷酸盐或三磷酸核苷进行。本研究表明赋予M3V高水平抗性的M184V突变会严重损害链终止核苷酸的去除。与野生型RT相比,含M184V不能检测3TC终止引物链上的焦磷酸解,而前一种酶显着降低了AZT终止DNA合成的拯救。因此,在这方面,与AZT和3TC抗性相关的突变RT具有相反的表型,因此具有不相容的表型。这些结果与组织培养和临床数据一致,临床数据表明AZT在RT编码基因中包含M184V突变的病毒中具有持续的抗病毒作用。

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