依法韦仑联合治疗失败患者HIV-1突变

《依法韦仑联合治疗失败患者HIV-1突变》

来源专题：艾滋病防治
编译者： 李越
发布时间：2005-04-17
Efavirenz is a potent and selective nonnucleoside inhibitor of human immunodeficiency virus type 1 (HIV-1) reverse transcriptase (RT). Nucleotide sequence analyses of the protease and RT genes (coding region for amino acids 1 to 229) of multiple cloned HIV-1 genomes from virus found in the plasma of patients in phase II clinical studies of efavirenz combination therapy were undertaken in order to identify the spectrum of mutations in plasma-borne HIV-1 associated with virological treatment failure. A K103N substitution was the HIV-1 RT gene mutation most frequently observed among plasma samples from patients for whom combination therapy including efavirenz failed, occurring in at least 90% of cases of efavirenz-indinavir or efavirenz-zidovudine (ZDV)-lamivudine (3TC) treatment failure. V108I and P225H mutations were observed frequently, predominantly in viral genomes that also contained other nonnucleoside RT inhibitor (NNRTI) resistance mutations. L100I, K101E, K101Q, Y188H, Y188L, G190S, G190A, and G190E mutations were also observed. V106A, Y181C, and Y188C mutations, which have been associated with high levels of resistance to other NNRTIs, were rare in the patient samples in this study, both before and after exposure to efavirenz. The spectrum of mutations observed in cases of virological treatment failure was similar for patients initially dosed with efavirenz at 200, 400, or 600 mg once a day and for patients treated with efavirenz in combination with indinavir, stavudine, or ZDV-3TC. The proportion of patients carrying NNRTI resistance mutations, usually K103N, increased dramatically at the time of initial viral load rebound in cases of treatment failure after exposure to efavirenz. Viruses with multiple, linked NNRTI mutations, especially K103N-V108I and K103N-P225H double mutants, accumulated more slowly following the emergence of K103N mutant viruses.

展开更多
原文来源：http://www.pubmedcentral.gov/articlerender.fcgi?tool=pmcentrez&artid=90088

7浏览量

0点赞

原文链接

相关报告

《经输血感染的HIV/AIDS患者HIV-1耐药基因突变研究》
- 来源专题：艾滋病防治
- 编译者：李越
- 发布时间：2013-05-28
- 目的研究经输血感染的HIV-1遗传基因突变特征,分析其对抗HIV药物的耐药性。方法经输血感染HIV-1的患者37例,从血浆提取HIV-1 RNA,运用RT-PCR和巢式聚合酶链反应(nested-PCR)扩增HIV-1 pol区基因片段,并对电泳阳性的目的片段进行测序,将结果提交到http://HIVdb.stanford.edu,分析HIV-1的耐药突变情况。结果 37例患者中共20例发生耐药突变,其中19例为病毒学或免疫学失败。3例患者在治疗过程中发生了蛋白酶抑制剂(PIs)位点突变,主要位点突变为V32AV,但未引发PIs耐药。有23例患者发生了反转录酶编码区基因突变,包括M184V、TAMs、Q151M复合体、K103N、Y181C等,其中20例HIV-1遗传基因的突变不同程度地导致了反转录酶抑制剂(RTIs)耐药,发生率为54.1%(20/37)。结论经血液感染HIV-1患者在参加抗病毒治疗后耐药发生率较高,应适时进行耐药监测,及时更新治疗方案。更多还原
  
  展开更多
28浏览量

0点赞

收藏

原文链接
《云南地区123例艾滋病抗病毒治疗失败患者的HIV-1基因耐药突变位点分析》
- 来源专题：艾滋病防治
- 编译者：李越
- 发布时间：2013-05-28
- 目的探讨云南地区抗病毒治疗失败的艾滋病患者中HIV-1基因耐药突变位点间的差异.方法 2009年8月至2011年1月,选择151例云南省HIV/AIDS抗病毒治疗失败患者作为监测对象,进行横断面调查.用RT-PCR方法扩增HIV-1 pol区基因,所得扩增片段进行测序后提交斯坦福大学HIV耐药数据库分析耐药突变发生情况.对所得到的HIV-1耐药基因突变频率和位点与HIV/AIDS患者的性别、民族、感染途径和亚型进行统计学处理分析,采用x2检验或Fisher精确概率法进行统计学检验.结果 151例患者中有123例患者的样本扩增成功,共获得123例患者蛋白酶区和逆转录酶区的基因扩增片段.RT区主要耐药位点是M184(72.4％,89/123),其次是K103(47.2％,58/123),其余依次为G190(34.1％,42/123)、Y181 (29.3％,36/123)、T215(26.0％,32/123)、K101(17.1％,21/123)、D67 (15.4％,19/123).突变位点V75、A62、M230在女性中比男性发生率高(x2=7.001,6.975,5.446,P均＜0.05)；在汉族人群中,变异位点T215、K70、T69比其他少数民族发生率高(x2 =5.290,4.060,3.860,P均＜0.05)；位点M41在少数民族中并未出现；在性接触感染途径人群中针对NRTI的突变位点T215、T69比在静脉吸毒人群中发生率高(x2=10.431,7.952,P均＜0.05),V75在静脉吸毒人群中并未出现；在针对NNRTI的耐药位点中,G190在静脉吸毒人群比性接触感染途径人群间发生率高(x2=6.669,P＜0.05),M230在静脉吸毒人群中并未出现；不同亚型中突变位点V75、T69、M230在CRF01_AE亚型人群中比在B亚型中发生率高,而L74在CRF01_AE亚型中并未出现.结论 HIV基因耐药突变是导致云南德宏、个旧、文山、玉溪等地区AIDS患者抗病毒治疗失败的主要原因.结果分析显示这些耐药突变位点的发生在民族、性别、传播途径及亚型不同的患者中存在着显著差异.
  
  展开更多
32浏览量

0点赞

收藏

原文链接

《依法韦仑联合治疗失败患者HIV-1突变》

《经输血感染的HIV/AIDS患者HIV-1耐药基因突变研究》

《云南地区123例艾滋病抗病毒治疗失败患者的HIV-1基因耐药突变位点分析》