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首页> 外文期刊>AIDS Research and Human Retroviruses >Short communication: High natural polymorphism in the gag gene cleavage sites of non-B HIV type 1 isolates from gabon
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Short communication: High natural polymorphism in the gag gene cleavage sites of non-B HIV type 1 isolates from gabon

机译:简短交流:来自加蓬的非B型HIV 1型分离株的gag基因切割位点具有很高的自然多态性

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The main goal of the present study was to determine the frequency of substitutions in the cleavage sites (CS) of gag gene among non-B HIV-1 isolates from Gabon. Fifty plasma specimens, collected in 2010-2011, from HIV-1-infected patients failing first-line antiretroviral (ARV) regimens (constituted of two nucleoside reverse transcriptase inhibitors+one nonnucleoside reverse transcriptase inhibitor) (n=38) and from HIV-1-infected individuals untreated with ARV (n=12) were analyzed in the gag and gag-pol cleavage sites. Compared to HXB2 reference sequence, the total median number of substitutions in gag and gag-pol CS was 10 (range, 5-18). The cleavage site p2/NC was the most variable of the four gag CS with 100% (50/50) isolates carrying at least 1 substitution (range, 1-9). The two gag-pol TFP/p6pol and p6pol/PR CS sites were also highly variable (at least one substitution, 50/50, 100% in both cases). Substitutions at position G381 (p2/NC), L449 (p1/p6gag), and K444 (TFP/p6pol) were significantly more frequent in CRF02-AG strains, compared to other non-B strains (30.4% vs. 3.7%, p=0.03; 87.0% vs. 59.3%, p=0.03; and 91.3% vs. 59.3%, p=0.01, respectively). Other non-B subtypes were significantly more likely to harbor substitutions at position N487 (p6 pol) (70.4%) than CRF02-AG (39.1%) (p=0.02). In Gabon, gag and gag-pol cleavage sites were highly polymorphic in protease inhibitor-naive patients harboring non-B HIV-1 strains. In sub-Saharan Africa, further studies are definitively required to better understand the impact of gag mutations among subjects receiving second-line LPV/r-containing regimens (monotherapy or triple combinations).
机译:本研究的主要目标是确定加蓬非B HIV-1分离株中gag基因切割位点(CS)的取代频率。在2010-2011年期间,从一线抗逆转录病毒(ARV)方案失败的HIV-1感染患者(由两种核苷逆转录酶抑制剂+一种非核苷逆转录酶抑制剂组成)(n = 38)和HIV-在gag和gag-pol裂解位点分析未经ARV治疗的1感染个体(n = 12)。与HXB2参考序列相比,gag和gag-pol CS中取代的总中位数为10(范围5-18)。裂解位点p2 / NC是四个gag CS中变化最大的,带有至少1个取代(范围1-9)的100%(50/50)分离株。两个gag-pol TFP / p6pol和p6pol / PR CS位点也高度可变(在两种情况下,至少一个取代,分别为50 / 50、100%)。与其他非B菌株相比,CRF02-AG菌株中G381(p2 / NC),L449(p1 / p6gag)和K444(TFP / p6pol)位置的取代显着更高(30.4%vs. 3.7%,p = 0.03;分别为87.0%和59.3%,p = 0.03; 91.3%和59.3%,p = 0.01)。与CRF02-AG(39.1%)(p = 0.02)相比,其他非B亚型在N487位(p6 pol)(70.4%)具有更高的替代可能性。在加蓬,gag和gag-pol切割位点在携带非B HIV-1菌株的未使用蛋白酶抑制剂的患者中高度多态。在撒哈拉以南非洲地区,需要进一步研究以更好地了解gag突变对接受二线LPV / r疗法(单一疗法或三联疗法)的受试者的影响。

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