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大鼠淋巴结中淋巴细胞从高内皮微静脉的迁出。

Lymphocyte emigration from high endothelial venules in rat lymph nodes.

作者信息

Anderson A O, Anderson N D

出版信息

Immunology. 1976 Nov;31(5):731-48.

Abstract

Sequential events during lymphocyte emigration from high endothelial venuses (HEV) were studied by scanning and transmission electron microscopy combined with regional perfusion techniques. The results indicate that blood lymphocytes selectively adhere to HEV surfaces through microvilli which attach to shallow pits on the luminal surfaces of high endothelial cells. These intercellular contact points resist hydrodynamic and osmotic shearing forces, but can be disrupted by treatments which remove endothelial glycocalyx, hydrolyse lymphocyte surface glycoproteins, or chelate divalent cations. After this initial attachment phase, lymphocytes enter apical clefts between endothelial cells where they assume a motile configuration characterized by loss of microvilli and formation of irregular surface folds. Intramural lymphocytes adhere to adjacent endothelial cells through macular and villous contacts. Fibrillar electron-dense material traverses the 15-20 nm gap at these points of adhesion. Microtubules and microfilaments are also seen around areas of cytoplasmic constriction in these motile lymphocytes. The migrating lymphocytes show cytoplasmic polarity which is oriented in the direction of movement as they pass through extracellular spaces in the venular wall and cross successive laminations in the perivascular sheath to enter the node. Since these lymphocytes enter channels between endothelial cells which are stained by intralymphatic injections with horseradish peroxidase, it is suggested that their entry into the node depends upon migration along a chemotactic gradient.

摘要

通过扫描电子显微镜和透射电子显微镜结合局部灌注技术,研究了淋巴细胞从高内皮静脉(HEV)移出过程中的一系列事件。结果表明,血液中的淋巴细胞通过微绒毛选择性地黏附于HEV表面,这些微绒毛附着于高内皮细胞腔面的浅凹处。这些细胞间接触点能够抵抗流体动力和渗透压剪切力,但可被去除内皮糖萼、水解淋巴细胞表面糖蛋白或螯合二价阳离子的处理所破坏。在这个初始黏附阶段之后,淋巴细胞进入内皮细胞之间的顶端裂隙,在那里它们呈现出一种运动形态,其特征是微绒毛消失并形成不规则的表面褶皱。壁内淋巴细胞通过斑状和绒毛状接触黏附于相邻的内皮细胞。在这些黏附点,纤维状电子致密物质穿过15 - 20纳米的间隙。在这些运动的淋巴细胞的细胞质收缩区域周围也可见微管和微丝。迁移的淋巴细胞表现出细胞质极性,当它们穿过小静脉壁的细胞外空间并穿过血管周围鞘中的连续层时,这种极性沿运动方向排列,从而进入淋巴结。由于这些淋巴细胞进入内皮细胞之间的通道,而这些通道可被淋巴管内注射辣根过氧化物酶染色,因此提示它们进入淋巴结取决于沿趋化梯度的迁移。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/540c/1445135/50f2636052b2/immunology00298-0058-a.jpg

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