缺乏层粘连蛋白-2小鼠胸腺细胞的异常发育。

W J Magner, A C Chang, J Owens, M J Hong, A Brooks, J E Coligan
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引用次数: 39

摘要

在之前的体外研究中,我们提出了细胞外基质成分层粘连蛋白-2及其整合素受体VLA-6在胸腺细胞发育中的作用。两种具有不同层粘连蛋白-2缺陷的营养不良小鼠品系的特征使我们能够在体内检查这一建议。与正常窝鼠相比,缺乏层粘连蛋白-2的小鼠胸腺大小和胸腺细胞数量显著减少。这些小鼠也表现出胸腺结构的明显改变。对1天/ 1天胸腺CD4/CD8群体的检查显示,DN (CD4- CD8-)和SP (CD4+ CD8-, CD4- CD8+)群体相对增加,DP (CD4+ CD8+)群体显著减少。进一步检测DN群体的CD44和CD25表达,发现在更成熟的前t细胞群体中显著降低。原位凋亡分析和流式细胞术显示,胸腺被囊区和被囊下区DN胸腺细胞凋亡显著增加。有趣的是,在表达层粘连蛋白-2 (dy2J)突变形式的营养不良小鼠以及胎儿和新生儿dy/dy小鼠中,胸腺细胞的发育似乎正常进行。我们认为,在年轻成年小鼠的特定发育阶段,层粘胶蛋白-2通过传递细胞存活和分化信号,在胸腺细胞发育中发挥积极作用。
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Aberrant development of thymocytes in mice lacking laminin-2.

In previous in vitro studies, we proposed a role for the extracellular matrix component, laminin-2, and its integrin receptor, VLA-6, in thymocyte development. The characterization of two dystrophic mouse strains with different defects in laminin-2 allowed us to examine this proposal in vivo. Mice deficient in laminin-2, dy/dy, show a significant reduction in thymus size and number of thymocytes compared to normal littermates. These mice also exhibited apparent alterations of thymic architecture. Examination of the CD4/CD8 populations in dy/dy thymi showed large relative increases in the DN (CD4- CD8-) and SP (CD4+ CD8-, CD4- CD8+) populations and a significant decrease in the DP (CD4+ CD8+) population. Further examination of the DN population for CD44 and CD25 expression showed a remarkable decrease in the more mature pre-T cell populations. Analysis of apoptosis in situ, and by flow cytometry, in dy/dy thymi revealed a significant increase in apoptotic DN thymocytes in the capsule and subcapsular regions. Interestingly, thymocyte development appeared to proceed normally in dystrophic mice expressing a mutant form of laminin-2, dy2J, as well as, in fetal and neonatal dy/dy mice. We propose that laminin-2 plays an active role in thymocyte development by delivering cell survival and differentiation signals at specific stages of development in young adult mice.

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