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来自印度、乌干达和南非的非 B 亚型 HIV-1 共受体嗜性的流行病学和临床相关性。

The epidemiology and clinical correlates of HIV-1 co-receptor tropism in non-subtype B infections from India, Uganda and South Africa.

机构信息

Pfizer Inc., New York, NY 10017, USA.

出版信息

J Int AIDS Soc. 2012 Jan 26;15(1):2. doi: 10.1186/1758-2652-15-2.

Abstract

BACKGROUND

The introduction of C-C chemokine receptor type-5 (CCR5) antagonists as antiretroviral therapy has led to the need to study HIV co-receptor tropism in different HIV-1 subtypes and geographical locations. This study was undertaken to evaluate HIV-1 co-receptor tropism in the developing world where non-B subtypes predominate, in order to assess the therapeutic and prophylactic potential of CCR5 antagonists in these regions.

METHODS

HIV-1-infected patients were recruited into this prospective, cross-sectional, epidemiologic study from HIV clinics in South Africa, Uganda and India. Patients were infected with subtypes C (South Africa, India) or A or D (Uganda). HIV-1 subtype and co-receptor tropism were determined and analyzed with disease characteristics, including viral load and CD4(+) and CD8(+) T cell counts.

RESULTS

CCR5-tropic (R5) HIV-1 was detected in 96% of treatment-naïve (TN) and treatment-experienced (TE) patients in India, 71% of TE South African patients, and 86% (subtype A/A1) and 71% (subtype D) of TN and TE Ugandan patients. Dual/mixed-tropic HIV-1 was found in 4% of Indian, 25% of South African and 13% (subtype A/A1) and 29% (subtype D) of Ugandan patients. Prior antiretroviral treatment was associated with decreased R5 tropism; however, this decrease was less in subtype C from India (TE: 94%, TN: 97%) than in subtypes A (TE: 59%; TN: 91%) and D (TE: 30%; TN: 79%). R5 virus infection in all three subtypes correlated with higher CD4(+) count.

CONCLUSIONS

R5 HIV-1 was predominant in TN individuals with HIV-1 subtypes C, A, and D and TE individuals with subtypes C and A. Higher CD4(+) count correlated with R5 prevalence, while treatment experience was associated with increased non-R5 infection in all subtypes.

摘要

背景

C-C 趋化因子受体 5(CCR5)拮抗剂作为抗逆转录病毒疗法的引入,导致需要在不同的 HIV-1 亚型和地理位置研究 HIV 辅助受体嗜性。本研究旨在评估在非 B 亚型占主导地位的发展中国家的 HIV-1 辅助受体嗜性,以评估 CCR5 拮抗剂在这些地区的治疗和预防潜力。

方法

从南非、乌干达和印度的 HIV 诊所招募了这项前瞻性、横断面、流行病学研究的 HIV-1 感染患者。患者感染的亚型为 C(南非、印度)或 A 或 D(乌干达)。确定了 HIV-1 亚型和辅助受体嗜性,并与疾病特征(包括病毒载量以及 CD4+和 CD8+T 细胞计数)进行了分析。

结果

在印度,96%的初治(TN)和治疗经验(TE)患者、71%的南非 TE 患者以及 86%(亚型 A/A1)和 71%(亚型 D)的 TN 和 TE 乌干达患者检测到 CCR5 嗜性(R5)HIV-1。在印度发现 4%的双重/混合嗜性 HIV-1,南非 25%的双重/混合嗜性 HIV-1,乌干达 13%(亚型 A/A1)和 29%(亚型 D)的双重/混合嗜性 HIV-1。先前的抗逆转录病毒治疗与 R5 嗜性降低相关;然而,与 A 型(TE:59%;TN:91%)和 D 型(TE:30%;TN:79%)相比,来自印度的 C 型(TE:94%;TN:97%)的降低幅度较小。所有三种亚型的 R5 病毒感染均与较高的 CD4+计数相关。

结论

在 HIV-1 亚型 C、A 和 D 的 TN 个体和 HIV-1 亚型 C 和 A 的 TE 个体中,R5 HIV-1 占主导地位。较高的 CD4+计数与 R5 流行相关,而治疗经验与所有亚型中非 R5 感染的增加相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ade6/3298508/b4c9971c0a82/1758-2652-15-2-1.jpg

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