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白细胞介素-2刺激期间淋巴细胞在细胞外基质中的黏附与运动发育。

Lymphocyte development of adherence and motility in extracellular matrix during IL-2 stimulation.

作者信息

Ratner S, Patrick P, Bora G

机构信息

Department of Immunology, Michigan Cancer Foundation, Detroit 48201.

出版信息

J Immunol. 1992 Jul 15;149(2):681-8.

PMID:1385607
Abstract

To extravasate into normal and neoplastic tissue, lymphocytes must migrate through the subendothelial basement membrane and underlying interstitium, structures rich in extracellular matrix (ECM). We have performed a time-course study of the development of motility in ECM by murine lymphocytes during in vitro exposure to high titers of IL-2 (1000 Cetus units/ml). This protocol generates immunotherapeutic lymphocyte populations expressing lymphokine-activated killer activity. Spontaneous motility was measured in three-dimensional gels of type I (interstitial) collagen or Matrigel, a model basement membrane. A newly developed assay permitted not only the measurement of distance traveled by the leading cell front, but also the separation of lymphocytes on the basis of three types of behavior. The motile fraction consisted of lymphocytes that penetrated beneath the ECM gel surface during an 18-h migration period. There were also two nonmotile fractions: the nonadherent fraction, which failed to bind to the gel surface; and the adherent fraction, which bound but did not penetrate during the assay period. During a 3- to 5-day exposure to high titer IL-2, both adherence and motility increased significantly. In type I collagen, cells of the NK lineage developed greater surface adherence and less motility than cells of the T lineage. The surface-adherent fraction expressed higher lymphokine-activated killer and NK activity than did the nonadherent or motile fractions. Under prolonged IL-2 stimulation (7 to 12 days), there was a decline in the percentage of cells exhibiting motility in both types of ECM, and an increase in the percentage of surface-adherent cells. The findings indicate that the behavior of an IL-2-stimulated lymphocyte population in ECM is profoundly influenced by the duration of IL-2 exposure. Furthermore, lack of lymphocyte motility may reflect two different behaviors, nonadherence and adherence without motility. The nonadherent and surface-adherent populations may differ in phenotypic distribution and function. The motility system described in this report will be useful in separating and studying the mechanisms that produce lymphocyte adherence and motility, and in understanding the in vivo implications of these behaviors.

摘要

淋巴细胞要渗入正常组织和肿瘤组织,就必须穿过富含细胞外基质(ECM)的内皮下基底膜及下方的间质。我们进行了一项时间进程研究,观察小鼠淋巴细胞在体外暴露于高滴度白细胞介素-2(IL-2,1000 赛特斯单位/毫升)期间在细胞外基质中的运动能力发展情况。该方案可产生表达淋巴因子激活的杀伤活性的免疫治疗性淋巴细胞群体。在 I 型(间质)胶原蛋白或基质胶(一种基底膜模型)的三维凝胶中测量自发运动能力。一种新开发的检测方法不仅可以测量领先细胞前沿移动的距离,还能根据三种行为类型分离淋巴细胞。运动部分由在 18 小时迁移期内穿透到细胞外基质凝胶表面下方的淋巴细胞组成。还有两个非运动部分:非黏附部分,即未能与凝胶表面结合的部分;以及黏附部分,即在检测期内结合但未穿透的部分。在暴露于高滴度 IL-2 的 3 至 5 天内,黏附性和运动能力均显著增加。在 I 型胶原蛋白中,自然杀伤(NK)细胞系的细胞比 T 细胞系的细胞表现出更高的表面黏附性和更低的运动能力。表面黏附部分比非黏附或运动部分表达更高的淋巴因子激活的杀伤活性和 NK 活性。在长时间 IL-2 刺激(7 至 12 天)下,两种类型的细胞外基质中表现出运动能力的细胞百分比均下降,表面黏附细胞的百分比增加。这些发现表明,IL-细胞外基质中受 2 刺激的淋巴细胞群体的行为受到 IL-2 暴露持续时间的深刻影响。此外,淋巴细胞运动能力的缺乏可能反映了两种不同的行为,即不黏附和黏附但不运动。非黏附群体和表面黏附群体在表型分布和功能上可能存在差异。本报告中描述的运动系统将有助于分离和研究产生淋巴细胞黏附和运动的机制,以及理解这些行为在体内的意义。

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