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整合素VLA - 2(α2β1)在人横纹肌肉瘤RD细胞于肝脏中的渗出后运动中的作用。

Integrin VLA-2 (alpha2beta1) function in postextravasation movement of human rhabdomyosarcoma RD cells in the liver.

作者信息

Hangan D, Uniyal S, Morris V L, MacDonald I C, von Ballestrem C, Chau T, Schmidt E E, Chambers A F, Groom A C, Chan B M

机构信息

Department of Microbiology and Immunology, John P. Robarts Research Institute, University of Western Ontario, Lodon, Canada.

出版信息

Cancer Res. 1996 Jul 1;56(13):3142-9.

PMID:8674074
Abstract

It is now known that members of the selectin and integrin families are critical in the initial interaction of cells in circulation with endothelial surfaces. Also, platelet/endothelial cell adhesion molecule-1 has been shown to be involved in transendothelial migration of extravasating cells. Little is known about adhesion molecules involved in subsequent postextravasation events. In this study, the significance of VLA-2 (alpha2beta1) integrin in the movement of human rhabdomyosarcoma RD cells in the liver was characterized by in vivo videomicroscopy. Results show that after extravasation, the mock-transfected RDpF cells were able to migrate to the subcapsular region of the liver. Although the RDX2C2 transfectant expressing VLA-2 integrin extravasated equally well, a majority of RDX2C2 cells remained in close proximity to blood vessels and failed to reach the subcapsular region. The functional involvement of VLA-2 in affecting the ability of RD cells to reach the subcapsular region was verified by the preparation of an RD transfectant [RDX2C2(I-)] expressing a nonfunctional variant of VLA-2 lacking the inserted (I)-domain of alpha2 subunit. In vivo microscopy showed that RDX2C2(I-) cells migrated in a manner similar to control RDpF cells. To demonstrate that RDX2C2 cells that remained in dose proximity to blood vessels were due to VLA-2 function, a blocking monoclonal antibody against VLA-2 (BHA2.1) was prepared. Mice were injected with BHA2.1 or control monoclonal antibody P3 at the time when RDX2C2 cells completed their extravasation. Treatment with BHA2.1 increased the number of RDX2C2 cells that reached the subcapsular region and subsequently formed tumor foci. Therefore, VLA-2 integrin expression has major roles in postextravasation movement and affects tumor foci formation at the liver surface.

摘要

现已明确,选择素家族和整合素家族成员在循环中的细胞与内皮表面的初始相互作用中起关键作用。此外,血小板/内皮细胞黏附分子-1已被证明参与渗出细胞的跨内皮迁移。关于渗出后事件中涉及的黏附分子知之甚少。在本研究中,通过体内视频显微镜观察,对VLA-2(α2β1)整合素在人横纹肌肉瘤RD细胞在肝脏中的运动的意义进行了表征。结果显示,渗出后,mock转染的RDpF细胞能够迁移至肝脏的被膜下区域。尽管表达VLA-2整合素的RDX2C2转染细胞渗出情况同样良好,但大多数RDX2C2细胞仍紧邻血管,未能到达被膜下区域。通过制备表达缺乏α2亚基插入(I)结构域的无功能VLA-2变体的RD转染细胞[RDX2C2(I-)],证实了VLA-2在影响RD细胞到达被膜下区域能力方面的功能参与。体内显微镜观察显示,RDX2C2(I-)细胞的迁移方式与对照RDpF细胞相似。为了证明紧邻血管的RDX2C2细胞是由于VLA-2功能所致,制备了一种针对VLA-2的阻断单克隆抗体(BHA2.1)。在RDX2C2细胞完成渗出时,给小鼠注射BHA2.1或对照单克隆抗体P3。用BHA2.1处理增加了到达被膜下区域并随后形成肿瘤灶的RDX2C2细胞数量。因此,VLA-2整合素表达在渗出后运动中起主要作用,并影响肝脏表面肿瘤灶的形成。

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