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一类新的具有CX3C基序的膜结合趋化因子。

A new class of membrane-bound chemokine with a CX3C motif.

作者信息

Bazan J F, Bacon K B, Hardiman G, Wang W, Soo K, Rossi D, Greaves D R, Zlotnik A, Schall T J

机构信息

Department of Molecular Biology, DNAX Research Institute, Palo Alto, California 94304, USA.

出版信息

Nature. 1997 Feb 13;385(6617):640-4. doi: 10.1038/385640a0.

Abstract

Chemokines direct the trafficking of white blood cells in immune surveillance, playing a key role in inflammatory and infectious diseases such as AIDS. All chemokines studied so far are secreted proteins of relative molecular mass approximately 7K-15K and fall into three families that are defined by a cysteine signature motif: CXC, CC and C (refs 3, 6, 7), where C is a cysteine and X any amino-acid residue. We report here the identification and characterization of a fourth human chemokine type, derived from non-haemopoietic cells and bearing a new CX3C fingerprint. Unlike other chemokine types, the polypeptide chain of the human CX3C chemokine is predicted to be part of a 373-amino-acid protein that carries the chemokine domain on top of an extended mucin-like stalk. This molecule can exist in two forms: either membrane-anchored or as a shed 95K glycoprotein. The soluble CX3C chemokine has potent chemoattractant activity for T cells and monocytes, and the cell-surface-bound protein, which is induced on activated primary endothelial cells, promotes strong adhesion of those leukocytes. The structure, biochemical features, tissue distribution and chromosomal localization of CX3C chemokine all indicate that it represents a unique class of chemokine that may constitute part of the molecular control of leukocyte traffic at the endothelium.

摘要

趋化因子在免疫监视中引导白细胞的迁移,在诸如艾滋病等炎症和感染性疾病中发挥关键作用。迄今为止所研究的所有趋化因子都是相对分子质量约为7K - 15K的分泌蛋白,可分为由半胱氨酸特征基序定义的三个家族:CXC、CC和C(参考文献3、6、7),其中C代表半胱氨酸,X代表任何氨基酸残基。我们在此报告了第四种人类趋化因子类型的鉴定和特征,它源自非造血细胞,并带有新的CX3C指纹。与其他趋化因子类型不同,人类CX3C趋化因子的多肽链预计是一个373个氨基酸的蛋白质的一部分,该蛋白质在一个延伸的粘蛋白样茎干顶部带有趋化因子结构域。这种分子可以以两种形式存在:要么是膜锚定形式,要么是脱落的95K糖蛋白形式。可溶性CX3C趋化因子对T细胞和单核细胞具有强大的趋化活性,而在活化的原代内皮细胞上诱导产生的细胞表面结合蛋白可促进这些白细胞的强烈黏附。CX3C趋化因子的结构、生化特性、组织分布和染色体定位均表明它代表了一类独特的趋化因子,可能构成内皮细胞处白细胞迁移分子控制的一部分。

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