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人类中性粒细胞中的CD69分子:其在信号转导机制中的表达及作用

CD69 molecule in human neutrophils: its expression and role in signal-transducing mechanisms.

作者信息

Gavioli R, Risso A, Smilovich D, Baldissarro I, Capra M C, Bargellesi A, Cosulich M E

机构信息

Istituto di Chimica Biologica Università degli Studi di Ferrara, Italy.

出版信息

Cell Immunol. 1992 Jun;142(1):186-96. doi: 10.1016/0008-8749(92)90279-x.

Abstract

The CD69 glycoprotein is an early activation antigen of T and B lymphocytes and it is constitutively expressed on thymocytes and platelets. Here we report its presence on neutrophils and on bone marrow-derived myeloid precursors. Indeed, promyelocytic cells are CD69+ on the cell membrane, while in resting neutrophils this molecule is located inside the cell. However, intracellular CD69 molecules are rapidly mobilized to the cell surface upon activation by PMA or fMLP. This translocation is independent on a new protein synthesis, as it is not inhibited by cycloheximide; furthermore, CD69 molecules are likely stored in a trans-Golgi structure since their expression is not affected by brefeldin A, a drug that blocks molecular trafficking from ER to Golgi vesicles. Immunoprecipitation of CD69 molecules either from activated neutrophils or from bone marrow cells showed that this protein has the same molecular size (28-34 kDa) as observed in platelets, T and B lymphocytes, and thymocytes. This similarity is reflected also in the functional role played by this molecule: in neutrophils as well as in lymphocytes and platelets, CD69 stimulation induced Ca2+ influx through cellular membrane; furthermore, the perturbation of the CD69 antigen on PMA-activated neutrophils enhances the lysozyme release, suggesting a role of this molecule in the regulation of granule exocytosis, probably through a Ca(2+)-dependent mechanism.

摘要

CD69糖蛋白是T和B淋巴细胞的早期激活抗原,在胸腺细胞和血小板上组成性表达。在此我们报道其在中性粒细胞和骨髓来源的髓系前体细胞上的存在。实际上,早幼粒细胞在细胞膜上呈CD69阳性,而在静息中性粒细胞中该分子位于细胞内。然而,经佛波酯(PMA)或N-甲酰甲硫氨酰-亮氨酰-苯丙氨酸(fMLP)激活后,细胞内的CD69分子会迅速转运至细胞表面。这种转运不依赖于新的蛋白质合成,因为它不受放线菌酮的抑制;此外,CD69分子可能储存在反式高尔基体结构中,因为其表达不受布雷菲德菌素A的影响,布雷菲德菌素A是一种阻断从内质网到高尔基体囊泡分子转运的药物。对激活的中性粒细胞或骨髓细胞中的CD69分子进行免疫沉淀显示,该蛋白的分子大小(28 - 34 kDa)与在血小板、T和B淋巴细胞以及胸腺细胞中观察到的相同。这种相似性也反映在该分子所起的功能作用中:在中性粒细胞以及淋巴细胞和血小板中,CD69刺激诱导Ca2+通过细胞膜内流;此外,对PMA激活的中性粒细胞上CD69抗原的干扰会增强溶菌酶的释放,这表明该分子可能通过Ca(2+)依赖性机制在调节颗粒胞吐作用中发挥作用。

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