首页> 美国卫生研究院文献>Antimicrobial Agents and Chemotherapy >Correlation of Phenotypic Zidovudine Resistance with Mutational Patterns in the Reverse Transcriptase of Human Immunodeficiency Virus Type 1: Interpretation of Established Mutations and Characterization of New Polymorphisms at Codons 208 211 and 214
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Correlation of Phenotypic Zidovudine Resistance with Mutational Patterns in the Reverse Transcriptase of Human Immunodeficiency Virus Type 1: Interpretation of Established Mutations and Characterization of New Polymorphisms at Codons 208 211 and 214

机译:表型齐多夫定耐药性与人类免疫缺陷病毒1型逆转录酶中突变模式的相关性:解释已建立的突变并鉴定208、211和214号密码子的新多态性。

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摘要

Zidovudine resistance (ZDV-R) is associated with classic genotypic changes at codons 41, 67, 70, 210, 215, and 219 of the human immunodeficiency virus type 1 (HIV-1) reverse transcriptase (RT) gene as well as with the multinucleoside resistance (MNR) complexes (Q151M MNR complex; 6-bp insertion/A62V complex). In addition, enhanced resistance to ZDV in the context of the classic ZDV mutations plus the M184V mutation has been associated with additional mutations at positions 208, 211, 214, and 333. In this study we investigated phenotypic ZDV-R determined by a recombinant virus assay (Antivirogram; Virco) in 223 clinical samples in relation to the above genotypic changes. 150 out of 223 clinical samples had the M184V mutation. Phenotypic ZDV-R ranged from 0.3- to 5,338-fold. Sixteen samples (15 with high ZDV-R ranging from 90- to 3,571-fold) contained MNR-associated patterns. Analysis of classic mutational patterns broadly demonstrated increasing ZDV-R with increasing number of ZDV mutations. A comparable correlation was obtained when ZDV-R was analyzed only relative to the T215Y/F mutation. Site-directed mutagenesis experiments investigating the influence of the additional mutations H208Y, R211K, and L214F on ZDV-R resulted in a 7.4- or 21-fold increase in ZDV-R when the R211K/L214F or H208Y/R211K/L214F mutations, respectively, were added to a highly ZDV-R virus. In the clinical sample data set we analyzed, the combination of R211K/L214F appeared most frequently. The H208Y change was detected only in highly ZDV-R viruses, whereas the G333E/D change was distributed equally. All changes were independent of the M184V mutation. A 2.4- or 8-fold increase in ZDV-R was observed in the clinical samples with high ZDV-R containing the R211K/L214F or H208Y/R211K/L214F mutations, respectively. We have shown that the combination of the additional mutations H208Y, R211K, and L214F in HIV-1 RT may influence ZDV-R and should be considered when assessing ZDV-R.
机译:齐多夫定耐药性(ZDV-R)与人类免疫缺陷病毒1型(HIV-1)逆转录酶(RT)基因第41、67、70、210、215和219位密码子的经典基因型变化以及与多核苷抗性(MNR)复合物(Q151M MNR复合物; 6 bp插入/ A62V复合物)。此外,在经典ZDV突变加上M184V突变的情况下,对ZDV的增强抵抗力与位置208、211、214和333处的其他突变相关。在这项研究中,我们研究了由重组病毒确定的表型ZDV-R与上述基因型变化相关的223种临床样品中的抗病毒检测(Antivirogram; Virco)。 223个临床样本中有150个具有M184V突变。表型ZDV-R的范围是0.3到5,338倍。 16个样本(其中15个具有高ZDV-R,从90到3,571倍不等)包含MNR相关模式。经典突变模式的分析广泛表明,随着ZDV突变数量的增加,ZDV-R也随之增加。当仅相对于T215Y / F突变分析ZDV-R时,获得了可比的相关性。定点诱变实验研究另外的突变H208Y,R211K和L214F对ZDV-R的影响,当分别为R211K / L214F或H208Y / R211K / L214F突变时,导致ZDV-R增加7.4或21倍,被添加到高度ZDV-R病毒中。在我们分析的临床样本数据集中,R211K / L214F的组合出现频率最高。仅在高度ZDV-R病毒中检测到H208Y变化,而G333E / D变化平均分布。所有变化均独立于M184V突变。在高ZDV-R的临床样品中,分别含有R211K / L214F或H208Y / R211K / L214F突变的ZDV-R的ZDV-R升高了2.4倍或8倍。我们已经表明,HIV-1 RT中其他突变H208Y,R211K和L214F的组合可能会影响ZDV-R,因此在评估ZDV-R时应予以考虑。

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