Wilson E, Aydintug M K, Jutila M A
Department of Veterinary Molecular Biology, Montana State University, Bozeman 59717, USA.
J Immunol. 1999 Apr 15;162(8):4914-9.
Tissue-specific localization of TCR-defined subsets of gamma delta T cells has been widely reported; however, the mechanisms responsible for this phenomenon are poorly understood. We describe a bovine gamma delta T cell TCR-associated subset that preferentially localizes in the spleen. This subset was characterized by coexpression of CD8, and was found to lack surface expression of E-selectin ligands, GR Ag ligands, as well as low expression of L-selectin. The CD8-positive gamma delta T cell subset did not accumulate at sites of inflammation as efficiently as CD8-negative gamma delta T cells that, in contrast, express E-selectin and GR ligands and high levels of L-selectin. This is the first demonstration of a gamma delta T cell subset, which exhibits a defined tissue tropism, having a unique adhesion molecule expression profile. These results demonstrate that in some cases tissue-specific accumulation of gamma delta T cell subsets can be predicted by expression, or lack of expression, of defined homing molecules.
TCR 定义的 γδ T 细胞亚群的组织特异性定位已被广泛报道;然而,导致这种现象的机制却知之甚少。我们描述了一个优先定位于脾脏的牛 γδ T 细胞 TCR 相关亚群。该亚群的特征是共表达 CD8,并且发现其缺乏 E-选择素配体、GR Ag 配体的表面表达,以及低水平的 L-选择素表达。与表达 E-选择素和 GR 配体以及高水平 L-选择素的 CD8 阴性 γδ T 细胞相比,CD8 阳性 γδ T 细胞亚群在炎症部位的聚集效率不高。这是首次证明具有特定组织嗜性的 γδ T 细胞亚群具有独特的黏附分子表达谱。这些结果表明,在某些情况下,γδ T 细胞亚群的组织特异性聚集可以通过特定归巢分子的表达或不表达来预测。
