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淋巴瘤细胞在培养中与基质细胞结合及在其下迁移时对VLA - 4和VLA - 5整合素的需求。

Requirement for VLA-4 and VLA-5 integrins in lymphoma cells binding to and migration beneath stromal cells in culture.

作者信息

Miyake K, Hasunuma Y, Yagita H, Kimoto M

机构信息

Department of Immunology, Saga Medical School, Japan.

出版信息

J Cell Biol. 1992 Nov;119(3):653-62. doi: 10.1083/jcb.119.3.653.

Abstract

Physical interaction between human lymphomas and murine bone marrow derived stromal cells were studied. Nalm-6 pre-B cells adhered to BMS2 stromal cells and subsequently migrated beneath them, while Ramos Burkitt lymphoma cells, adhered but did not migrate. Four mAbs were established against Nalm-6 cells, which were able to block initial adhesion of Nalm-6 cells. Two of them were directed against the alpha 4 chain of VLA-4, and other two recognized the beta 1 chain of VLA integrins. Therefore, the initial adhesion of Ramos and Nalm-6 cells to BMS2 was largely mediated by the VLA-4 integrin expressed on lymphocytes. The corresponding ligand on stromal cells appears to be VCAM-1, because antibodies against murine VCAM-1 blocked the adhesion. However, antibodies against the alpha chain of VLA-4 were not capable of blocking subsequent migration beneath stromal cells. In contrast, antibodies against the beta chain of VLA integrins blocked the migration beneath stromal cells as well as the initial adhesion. Because a common beta chain can be shared among integrins, the role of other VLA integrins in Nalm-6 cells migration was investigated. VLA-5 and VLA-6 as well as VLA-4 were expressed on Nalm-6 cells, but not on Ramos cells. Additional blocking experiments revealed that VLA-4 and VLA-5 are likely to work in concert to mediate the migration of Nalm-6 cells beneath stromal cells. Thus, particular VLA integrins appear to be responsible not only for lymphocyte adhesion but also for migration with respect to stromal cells. These findings may have implications for cell-cell interactions and directed migration of lymphocytes in bone marrow and other tissues.

摘要

对人类淋巴瘤与小鼠骨髓来源的基质细胞之间的物理相互作用进行了研究。Nalm-6前B细胞黏附于BMS2基质细胞,随后迁移至其下方,而Ramos伯基特淋巴瘤细胞虽能黏附但不迁移。制备了4种针对Nalm-6细胞的单克隆抗体,它们能够阻断Nalm-6细胞的初始黏附。其中两种针对VLA-4的α4链,另外两种识别VLA整合素的β1链。因此,Ramos和Nalm-6细胞对BMS2的初始黏附很大程度上是由淋巴细胞上表达的VLA-4整合素介导的。基质细胞上相应的配体似乎是VCAM-1,因为抗小鼠VCAM-1的抗体可阻断黏附。然而,抗VLA-4α链的抗体不能阻断随后在基质细胞下方的迁移。相反,抗VLA整合素β链的抗体既能阻断在基质细胞下方的迁移,也能阻断初始黏附。由于整合素之间可共享一条共同的β链,因此研究了其他VLA整合素在Nalm-6细胞迁移中的作用。Nalm-6细胞表达VLA-5、VLA-6以及VLA-4,而Ramos细胞不表达。额外的阻断实验表明,VLA-4和VLA-5可能协同作用介导Nalm-6细胞在基质细胞下方的迁移。因此,特定的VLA整合素似乎不仅负责淋巴细胞与基质细胞的黏附,还负责其迁移。这些发现可能对骨髓和其他组织中淋巴细胞的细胞间相互作用和定向迁移具有重要意义。

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