Sa-Filho Dercy J, Costa Luciana J, de Oliveira Carlos F, Guimarães Ana Paula C, Accetturi Conceição A, Tanuri Amilcar, Diaz Ricardo S
Retrovirology Laboratory, Federal University of São Paulo, R. Pedro de Toledo 781, 16 andar Vila Clementino, São Paulo, SP 04039-032, Brazil.
J Clin Virol. 2003 Oct;28(2):186-202. doi: 10.1016/s1386-6532(03)00007-6.
Protease inhibitors (PI) are an important HIV-1 treatment tool. The HIV-1 genetic diversity as a result of antiretroviral exposure is a potential barrier to successful antiretroviral therapy.
To describe the impact of the selective pressure of the PI Indinavir in the protease region of the pol gene of HIV-1.
We have examined the extent of protease sequence heterogeneity in previously antiretroviral drug naive HIV-1 infected individuals receiving Indinavir as monotherapy for at least 48 weeks.
Analysis based on the consensus of this group of sequences showed regions with higher and lower polymorphism. The degree of genetic variation was greater in regions less critical for the structure and function of the enzyme. To investigate the selective pressure imposed by drug therapy, we have analyzed the rate of synonymous (ds) and nonsynonymous (dn) substitutions. The three critical regions for enzyme activity showed ds/dn ratio >1. whereas other regions had ds/dn ratio <1. The detected amino acid mutations had a trend to be conservative, thus maintaining the physical chemical amino acid characteristics. Phylogenetic analysis established the presence of subtype B (n=38), subtype F (n=9), and B/F recombinants within the protease region of pol gene (n=3). More prevalent detected mutations, thought to contribute to antiretroviral resistance, were L63P (42%), L10I (35%), M36I (30%), V82A/T/F (26%).
A great deal of predicted cross-resistance between PIs was observed. Out of the 50 individuals, 34% were considered to have major mutations to Indinavir, and 66% had minor or no mutations to Indinavir. Viral loads were significantly higher among patients with major mutations, compared with patients minor/no mutations, although no differences in the CD4 counts were found. The viral load at baseline and nadir (week 4) was able to predict the group of individuals with greater chances of selecting drug resistance related mutations.
蛋白酶抑制剂(PI)是治疗HIV-1的重要工具。抗逆转录病毒治疗导致的HIV-1基因多样性是抗逆转录病毒疗法成功的潜在障碍。
描述PI茚地那韦的选择压力对HIV-1 pol基因蛋白酶区域的影响。
我们检测了先前未接受过抗逆转录病毒药物治疗、接受茚地那韦单药治疗至少48周的HIV-1感染者蛋白酶序列的异质性程度。
基于这组序列的共识进行分析,发现了多态性较高和较低的区域。在对酶的结构和功能不太关键的区域,遗传变异程度更大。为了研究药物治疗施加的选择压力,我们分析了同义(ds)和非同义(dn)替换率。酶活性的三个关键区域显示ds/dn比率>1,而其他区域ds/dn比率<1。检测到的氨基酸突变倾向于保守,从而保持氨基酸的物理化学特性。系统发育分析确定在pol基因的蛋白酶区域存在B亚型(n = 38)、F亚型(n = 9)和B/F重组体(n = 3)。检测到的更常见的突变,被认为与抗逆转录病毒耐药性有关,包括L63P(42%)、L10I(35%)、M36I(30%)、V82A/T/F(26%)。
观察到PI之间存在大量预测的交叉耐药性。在50名个体中,34%被认为对茚地那韦有主要突变,66%对茚地那韦有轻微突变或无突变。与有轻微/无突变的患者相比,有主要突变的患者病毒载量显著更高,尽管CD4细胞计数没有差异。基线和最低点(第4周)的病毒载量能够预测更有可能选择耐药相关突变的个体组。
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