首页> 美国卫生研究院文献>Journal of Virology >Demented and nondemented patients with AIDS differ in brain-derived human immunodeficiency virus type 1 envelope sequences.
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Demented and nondemented patients with AIDS differ in brain-derived human immunodeficiency virus type 1 envelope sequences.

机译:痴呆和非痴呆的AIDS患者在脑源性人类免疫缺陷病毒1型包膜序列方面有所不同。

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摘要

Human immunodeficiency virus (HIV) dementia is a common clinical syndrome of uncertain pathogenesis in patients with AIDS. In several animal models of retrovirus-induced brain disease, specific viral envelope sequences have been found to influence the occurrence of central nervous system disease. Therefore, to search for unique envelope sequences correlated with HIV dementia, we studied 22 HIV-infected patients who were neurologically assessed premortem and classified into demented (HIVD) (n = 14) and nondemented (ND) (n = 8) groups. Using DNA from autopsied brain and spleen, we amplified, cloned, and sequenced a 430-nucleotide region including the V3 loop and flanking regions. All brain-derived clones in both clinical groups showed marked homology to the macrophage-tropic consensus sequence within the V3 loop. Two amino acid positions within (position 305) and outside (position 329) the V3 region showed significant divergence between the two clinical groups. At position 305, a histidine was predominant in the HIVD group and was not observed in the ND group, but a proline was predominant in the ND group and was not observed in the HIVD group. Similarly, at position 329, a leucine was predominant in the HIVD group but rarely observed in the ND group, whereas an isoleucine was predominant in the ND group at this position. In addition, the HIVD group had 21 amino acid residues at specific positions that were unique relative to the ND group, whereas only 2 residues at specific positions were unique to the ND group. These data suggest that distinct HIV envelope sequences are associated with the clinical expression of HIV dementia.
机译:人类免疫缺陷病毒(HIV)痴呆症是AIDS患者发病机理不确定的常见临床综合征。在逆转录病毒引起的脑疾病的几种动物模型中,已经发现特定的病毒包膜序列会影响中枢神经系统疾病的发生。因此,为了搜索与HIV痴呆症相关的独特包膜序列,我们研究了22名经过HIV感染的患者,这些患者经过神经学评估为死前,分为痴呆(HIVD)(n = 14)和非痴呆(ND)(n = 8)组。使用来自尸体解剖的大脑和脾脏的DNA,我们扩增,克隆并测序了430个核苷酸的区域,包括V3环和侧翼区域。两个临床组中所有脑源性克隆均与V3环内的巨噬细胞嗜性共有序列具有明显的同源性。 V3区内部(位置305)和外部(位置329)的两个氨基酸位置在两个临床组之间显示出显着差异。在第305位,组氨酸在HIVD组中占主导地位,而在ND组中未发现,但脯氨酸在ND组中占主导地位,而在HIVD组中未发现。类似地,在位置329处,亮氨酸在HIVD组中占优势,但在ND组中很少观察到,而在该位置的ND组中异亮氨酸占主导。此外,HIVD组在特定位置具有21个氨基酸残基,相对于ND组是唯一的,而在特定位置只有2个残基对于ND组是唯一的。这些数据表明,不同的HIV包膜序列与HIV痴呆的临床表达有关。

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