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系统性硬化症患者循环中的α/β和γ/δ T淋巴细胞对细胞凋亡的抵抗作用。

Resistance to apoptosis in circulating alpha/beta and gamma/delta T lymphocytes from patients with systemic sclerosis.

作者信息

Cipriani Paola, Fulminis Antonietta, Pingiotti Elisa, Marrelli Alessandra, Liakouli Vasiliki, Perricone Roberto, Pignone Alberto, Matucci-Cerinic Marco, Giacomelli Roberto

机构信息

Department of Internal Medicine, University of L'Aquila, School of Medicine, Rheumatology Unit, University of Rome Tor Vergata School of Medicine, Rome, Italy.

出版信息

J Rheumatol. 2006 Oct;33(10):2003-14.

Abstract

OBJECTIVE

T cell activation plays a pivotal role in the immunopathogenesis of systemic sclerosis (SSc). Lymphocyte processes are tightly controlled by molecules activating either proliferation or programmed cell death (apoptosis). We investigated whether an imbalance in apoptotic function, increasing the survival rate of autoreactive cells, may lead to persistent autoreactive phenomena.

METHODS

We studied peripheral a/b and g/d T lymphocytes of 22 patients with SSc and 22 healthy controls for their spontaneous and stimulated (phytohemagglutinin, dexamethasone) apoptotic rate and surface phenotype including expression of Fas (CD95) and Bcl-2, determined by flow cytometry. sFas and sFas ligand in sera and supernatants were measured by ELISA. Caspase-3 activation in response to agonistic anti-Fas Mab treatment was assessed.

RESULTS

Lymphocytes of SSc patients showed a significant decrease in the percentage of apoptotic cells over time, in both unstimulated and stimulated cultures, compared to controls. We observed no difference between patients and controls, in stimulated or unstimulated cells, in the phenotypic expression of apoptotic cells, including surface Fas. SSc T cells were less susceptible to undergoing apoptosis after anti-Fas stimulation. We observed a significant decrease of apoptotic cells from stimulated culture of isolated SSc g/d T cells. Serum levels of sFas in SSc patients were significantly higher compared to controls. Similar data were obtained in the supernatants of stimulated and unstimulated cultures. By contrast, sFas ligand was always reduced. Bcl-2 expression in SSc was significantly elevated. A significant decrease in caspase-3 activity was detected in SSc patients after treatment by agonistic anti-Fas antibody.

CONCLUSION

Resistance to apoptosis is present in a/b and g/d T cell lymphocyte subsets of patients with SSc, and several pathways seem to be connected in this setting.

摘要

目的

T细胞活化在系统性硬化症(SSc)的免疫发病机制中起关键作用。淋巴细胞过程受到激活增殖或程序性细胞死亡(凋亡)的分子的严格控制。我们研究了凋亡功能的失衡是否会增加自身反应性细胞的存活率,从而导致持续的自身反应现象。

方法

我们研究了22例SSc患者和22例健康对照者外周血α/β和γ/δ T淋巴细胞的自发凋亡率和刺激(植物血凝素、地塞米松)凋亡率以及表面表型,包括Fas(CD95)和Bcl-2的表达,通过流式细胞术进行测定。通过ELISA检测血清和上清液中的可溶性Fas(sFas)和sFas配体。评估抗Fas单克隆抗体激动剂处理后Caspase-3的激活情况。

结果

与对照组相比,SSc患者的淋巴细胞在未刺激和刺激培养中,随着时间的推移凋亡细胞百分比均显著降低。在刺激或未刺激的细胞中,患者和对照在凋亡细胞的表型表达(包括表面Fas)方面没有差异。SSc T细胞在抗Fas刺激后对凋亡更不敏感。我们观察到分离的SSc γ/δ T细胞刺激培养后凋亡细胞显著减少。SSc患者血清sFas水平显著高于对照组。在刺激和未刺激培养上清液中也获得了类似的数据。相比之下,sFas配体总是降低的。SSc中Bcl-2表达显著升高。抗Fas抗体激动剂处理后,SSc患者Caspase-3活性显著降低。

结论

SSc患者α/β和γ/δ T细胞淋巴细胞亚群存在凋亡抵抗,在这种情况下似乎有几种途径相互关联。

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