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T细胞共刺激抑制剂:阿巴西普。

The inhibitor of costimulation of T cells: abatacept.

作者信息

Iannone Florenzo, Lapadula Giovanni

机构信息

DiMIMP-Rheumatogy Unit, University of Bari, Bari, Italy.

出版信息

J Rheumatol Suppl. 2012 Jul;89:100-2. doi: 10.3899/jrheum.120257.

DOI:10.3899/jrheum.120257
PMID:22751606
Abstract

OBJECTIVE

T cell costimulation is a key point in the regulation of immune tolerance, immune response, and autoimmunity. T cell activation does not take place upon the simple engagement of T cell receptor; a second signal is needed to fully stimulate T cells. There are a variety of molecules that can act as costimulators, and among those CD28/CD80 signaling plays a crucial role in modulating T cell response. Cytotoxic T lymphocyte antigen-4, CD152 (CTLA4) is a physiologic antagonist of CD28, and abatacept, a synthetic analog of CTLA4, has recently been approved to treat rheumatoid arthritis. An abnormal T cell activation is also believed to sustain psoriatic disease both at skin and joint sites. We aimed to evaluate the rationale of blocking CD28/CD80 signaling and the possible use of abatacept for treating psoriatic arthritis (PsA).

METHODS

We reviewed the role of CD28/CD80 signaling in promoting T cell inflammation in psoriasis and the effects of CTLA4 modulation in experimental models of psoriasis and in humans.

RESULTS

CD28/CD80 seems to be crucial in stimulating T cell activation and inflammation in psoriasis, and its inhibition by CTLA4 analogs or by anti-CD28 blocking antibodies is effective against psoriasis. Few data are available on abatacept, which seems to be valuable for the treatment of PsA but less useful in the therapy of skin psoriasis.

CONCLUSION

Although the CD28 molecule is crucial in activating T cells and inflammation in psoriasis, data on the efficacy of abatacept in the treatment of PsA are still not conclusive.

摘要

目的

T细胞共刺激是免疫耐受、免疫反应和自身免疫调节的关键点。T细胞受体简单结合时T细胞不会被激活;需要第二个信号来充分刺激T细胞。有多种分子可作为共刺激分子,其中CD28/CD80信号在调节T细胞反应中起关键作用。细胞毒性T淋巴细胞抗原4,即CD152(CTLA4)是CD28的生理性拮抗剂,阿巴西普作为CTLA4的合成类似物,最近已被批准用于治疗类风湿性关节炎。异常的T细胞激活也被认为在皮肤和关节部位维持银屑病病情。我们旨在评估阻断CD28/CD80信号的理论依据以及阿巴西普治疗银屑病关节炎(PsA)的可能性。

方法

我们回顾了CD28/CD80信号在促进银屑病中T细胞炎症方面的作用以及CTLA4调节在银屑病实验模型和人类中的效果。

结果

CD28/CD80似乎在刺激银屑病中T细胞激活和炎症方面至关重要,CTLA4类似物或抗CD28阻断抗体对其抑制可有效对抗银屑病。关于阿巴西普的数据较少,它似乎对PsA治疗有价值,但对皮肤银屑病治疗作用较小。

结论

尽管CD28分子在激活银屑病中T细胞和炎症方面至关重要,但阿巴西普治疗PsA疗效的数据仍不确凿。

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