MT-2嗜性和CCR-5基因型强烈影响HIV-1感染个体的疾病进展。

MT-2 tropism and CCR-5 genotype strongly influence disease progression in HIV-1-infected individuals.

作者信息

Bratt G, Leandersson A C, Albert J, Sandström E, Wahren B

机构信息

Gay Men's Health Clinic, Department of Dermatovenereology, Söder Hospital, Stockholm, Sweden.

出版信息

AIDS. 1998 May 7;12(7):729-36. doi: 10.1097/00002030-199807000-00009.

DOI:10.1097/00002030-199807000-00009

PMID:9619804

Abstract

BACKGROUND

The beta-chemokine receptor CCR-5 is the coreceptor for cellular entry by non-syncytium-inducing (NSI) HIV-1 strains that dominate early in infection. A 32 base-pair deletion (delta32) in the CCR-5 gene renders this coreceptor non-functional. Heterozygosity for this deletion [delta32/wild-type (wt)] is associated with slow disease progression. The purpose of this study was to document the combined impact on HIV-1 disease progression of the CCR-5 genotype and the biological phenotype of HIV-1.

METHODS

In a cross-sectional study of 258 HIV-1-infected Swedish individuals, the CCR-5 genotype (wt/wt or delta32/wt) was determined by polymerase chain reaction and the biological phenotype [NSI or syncytium-inducing (SI)] of virus isolates was determined in the MT-2 cell assay. Clinical status, HIV-1 RNA levels in plasma, CD4+ lymphocyte counts, and rate of CD4+ lymphocyte decline, based on retrospective analysis of CD4+ lymphocyte counts, were also recorded. None of the individuals were treated with protease inhibitors.

RESULTS

The prevalence of the delta32/wt genotype was 23%. Subjects with the delta32/wt CCR-5 genotype more often carried SI virus than subjects with the wt/wt genotype (49 versus 35%; P=0.067), but there were no differences between the two groups in prevalence of AIDS, viral load, CD4+ lymphocyte count or CD4+ slope. NSI virus isolates were found in 159 (62%) out of 258 individuals. Individuals with NSI had lower prevalence of AIDS (39 versus 19%; P < 0.01), higher CD4+ lymphocyte counts (289+/-188 x 10(6)/l versus 153+/-162 x 10(6)/l; P=0.001), lower viral loads (median, 4.45 log10 versus 4.91 log10 copies/ml; P < 0.01) and a lower prevalence of the delta32/wt genotype (19 versus 29%; P=0.067) compared with individuals with SI virus. When the material was further subdivided, subjects with the delta32/wt genotype and SI virus had the highest prevalence of AIDS (P < 0.001), lowest CD4+ lymphocyte count (P=0.0001) and highest viral load (P=0.023) whereas the opposite was true for subjects with the delta32/wt genotype and NSI virus. A significantly higher proportion of subjects with NSI virus with delta32/wt and wt/wt CCR-5 genotype had been immunized with recombinant gp160.

CONCLUSION

In summary, the delta32/wt CCR-5 genotype has a protective effect against HIV-1 disease progression that appears to be limited to individuals carrying HIV-1 variants with NSI phenotype. Immunization with recombinant gp160 tended to reduce the frequency of SI phenotypes.

摘要

背景

β-趋化因子受体CCR-5是在感染早期占主导地位的非合胞体诱导型（NSI）HIV-1毒株进入细胞的共受体。CCR-5基因中的32个碱基对缺失（Δ32）使该共受体失去功能。这种缺失的杂合性[Δ32/野生型（wt）]与疾病进展缓慢有关。本研究的目的是记录CCR-5基因型和HIV-1生物学表型对HIV-1疾病进展的综合影响。

方法

在一项对258名感染HIV-1的瑞典个体的横断面研究中，通过聚合酶链反应确定CCR-5基因型（wt/wt或Δ32/wt），并在MT-2细胞试验中确定病毒分离株的生物学表型[NSI或合胞体诱导型（SI）]。还记录了临床状态、血浆中HIV-1 RNA水平、CD4+淋巴细胞计数以及基于CD4+淋巴细胞计数回顾性分析的CD4+淋巴细胞下降率。所有个体均未接受蛋白酶抑制剂治疗。

结果

Δ32/wt基因型的患病率为23%。与wt/wt基因型的受试者相比，携带Δ32/wt CCR-5基因型的受试者更常携带SI病毒（49%对35%；P=0.067），但两组在艾滋病患病率、病毒载量、CD4+淋巴细胞计数或CD4+斜率方面没有差异。在258名个体中有159名（62%）检测到NSI病毒分离株。与携带SI病毒的个体相比，携带NSI病毒的个体艾滋病患病率较低（39%对19%；P<0.01），CD4+淋巴细胞计数较高（289±188×10⁶/l对153±162×10⁶/l；P=0.001），病毒载量较低（中位数，4.45 log₁₀对4.91 log₁₀拷贝/ml；P<0.01），且Δ32/wt基因型的患病率较低（19%对29%；P=0.067）。当对材料进一步细分时，携带Δ32/wt基因型和SI病毒的受试者艾滋病患病率最高（P<0.001），CD4+淋巴细胞计数最低（P=0.0001），病毒载量最高（P=0.023），而携带Δ32/wt基因型和NSI病毒的受试者情况则相反。携带NSI病毒且CCR-5基因型为Δ32/wt和wt/wt的受试者中，接受重组gp160免疫的比例明显更高。