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人类趋化因子:最新进展。

Human chemokines: an update.

作者信息

Baggiolini M, Dewald B, Moser B

机构信息

Theodor Kocher Institute, University of Bern, Switzerland.

出版信息

Annu Rev Immunol. 1997;15:675-705. doi: 10.1146/annurev.immunol.15.1.675.

Abstract

Interleukin 8, the first chemokine to be characterized, was discovered nearly ten years ago. Today, more than 30 human chemokines are known. They are often upregulated in inflammation and act mainly on leukocytes inducing migration and release responses. The present review deals largely with the new developments of the last three years. Several structural studies have shown that most chemokines form dimers. The dimers, however, dissociate upon dilution, and the monomers constitute the biologically active form. Chemokine activities are mediated by seven-transmembrane-domain, G protein coupled receptors, five of which were discovered in the past three years. The primary receptor-binding domain of all chemokines is near the NH2 terminus, and antagonists can be obtained by truncation or substitutions in this region. Major progress has been made in the understanding of chemokine actions on T lymphocytes that respond to several CC chemokines but also to IP10 and Mig, two CXC chemokines that selectively attract T cells via a novel receptor. Effects of chemokines on angiogenesis and tumor growth have been reported, but the data are still contradictory and the mechanisms unknown. Of considerable interest is the recent discovery that some chemokines function as HIV-suppressive factors by interacting with chemokine receptors which, together with CD4, were recognized as the binding sites for HIV-1.

摘要

白细胞介素8是最早被鉴定的趋化因子,大约在十年前被发现。如今,已知的人类趋化因子超过30种。它们在炎症中常被上调,主要作用于白细胞,诱导其迁移和释放反应。本综述主要涉及过去三年的新进展。多项结构研究表明,大多数趋化因子形成二聚体。然而,二聚体在稀释时会解离,单体构成生物活性形式。趋化因子的活性由七跨膜结构域G蛋白偶联受体介导,其中五种是在过去三年中发现的。所有趋化因子的主要受体结合域靠近NH2末端,通过在该区域进行截短或替换可获得拮抗剂。在理解趋化因子对T淋巴细胞的作用方面取得了重大进展,T淋巴细胞对几种CC趋化因子有反应,但也对IP10和Mig有反应,这两种CXC趋化因子通过一种新型受体选择性地吸引T细胞。已有报道趋化因子对血管生成和肿瘤生长的影响,但数据仍相互矛盾,机制尚不清楚。最近发现一些趋化因子通过与趋化因子受体相互作用而发挥HIV抑制因子的作用,这一发现引起了人们的极大兴趣,趋化因子受体与CD4一起被认为是HIV-1的结合位点。

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