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在慢性HIV感染期间,淋巴组织中存在的CD8 T淋巴细胞的细胞毒性颗粒内,穿孔素不与颗粒酶A共表达。

Perforin is not co-expressed with granzyme A within cytotoxic granules in CD8 T lymphocytes present in lymphoid tissue during chronic HIV infection.

作者信息

Andersson J, Behbahani H, Lieberman J, Connick E, Landay A, Patterson B, Sönnerborg A, Loré K, Uccini S, Fehniger T E

机构信息

Department of Infectious Diseases, Karolinska Institutet, Huddinge University Hospital, Stockholm, Sweden.

出版信息

AIDS. 1999 Jul 30;13(11):1295-303. doi: 10.1097/00002030-199907300-00005.

Abstract

BACKGROUND

Residual HIV-1-infected cells are poorly eliminated from lymphoid tissue (LT) reservoirs by effector cytotoxic T lymphocytes (eCTL) despite antiretroviral therapy. Perforin and granzyme A (grA) constitute major effector molecules within eCTL granules that induce apoptosis and lysis of virally infected cells.

OBJECTIVE

Expression of perforin and grA was studied at the single cell level in LT and blood from 16 patients infected with HIV-1 (stage A1-C) who were not taking antiretroviral therapy.

METHOD

Immunohistochemical analysis by in situ imaging of cells from blood and LT.

RESULTS

Quantitative in situ imaging showed that perforin-expressing CD8 T cells comprised 0.3-1.5% of total cells within the LT from recent HIV-1 seroconverters, while grA was found in 2.1-7.2% of total cells. However, despite high-level grA upregulation (1.5-4.5% of total cells) compared with that in non-infected individuals (0.4-0.9%), perforin expression remained low (< 0.1% of total cells) (P < 0.02) in LT from patients with chronic HIV-1 infection (stage A2-C). This contrasted with findings in peripheral blood mononuclear cells (PBMC) from the same HIV-1 infected cohort where perforin was detected in 13-31% of all PBMC, which was 10- to 100-fold higher than in lymphoid tissue (P < 0.001); grA was found in 14-32% of total PBMC. Two-colour staining showed that granular expression of perforin and grA was restricted to CD8 T cells in over 90% of total cells in both LT and blood.

CONCLUSIONS

These findings indicate that cytotoxic perforin expression is impaired at local sites of HIV replication within lymphoid tissue. Since perforin is required together with grA for granule-mediated cytolysis, the low perforin expression in the LT may limit the ability of eCTL to eliminate HIV-1 infected cells in lymphoid tissue.

摘要

背景

尽管进行了抗逆转录病毒治疗,但效应性细胞毒性T淋巴细胞(eCTL)仍难以从淋巴组织(LT)储存库中清除残留的HIV-1感染细胞。穿孔素和颗粒酶A(grA)是eCTL颗粒内的主要效应分子,可诱导病毒感染细胞的凋亡和裂解。

目的

研究16例未接受抗逆转录病毒治疗的HIV-1感染患者(A1-C期)的LT和血液中穿孔素和grA在单细胞水平的表达。

方法

通过对血液和LT中的细胞进行原位成像进行免疫组织化学分析。

结果

定量原位成像显示,近期HIV-1血清转化者的LT中,表达穿孔素的CD8 T细胞占总细胞的0.3%-1.5%,而grA存在于2.1%-7.2%的总细胞中。然而,与未感染个体(0.4%-0.9%)相比,尽管慢性HIV-1感染患者(A2-C期)的LT中grA上调水平较高(占总细胞的1.5%-4.5%),但穿孔素表达仍然较低(<总细胞的0.1%)(P<0.02)。这与同一HIV-1感染队列外周血单个核细胞(PBMC)中的发现形成对比,在所有PBMC中,13%-31%检测到穿孔素,比淋巴组织高10至100倍(P<0.001);grA存在于14%-32%的总PBMC中。双色染色显示,在LT和血液中,超过90%的总细胞中穿孔素和grA的颗粒表达仅限于CD8 T细胞。

结论

这些发现表明,在淋巴组织内HIV复制的局部部位,细胞毒性穿孔素的表达受损。由于穿孔素与grA共同作用才能实现颗粒介导的细胞溶解,LT中穿孔素表达较低可能会限制eCTL清除淋巴组织中HIV-1感染细胞的能力。

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