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表皮整联配体蛋白是上皮基底膜的一个组成成分,是α3β1阳性T淋巴细胞的一种黏附配体。

Epiligrin, a component of epithelial basement membranes, is an adhesive ligand for alpha 3 beta 1 positive T lymphocytes.

作者信息

Wayner E A, Gil S G, Murphy G F, Wilke M S, Carter W G

机构信息

Department of Laboratory Medicine and Pathology, University of Minnesota, Minneapolis 55455.

出版信息

J Cell Biol. 1993 Jun;121(5):1141-52. doi: 10.1083/jcb.121.5.1141.

Abstract

The cutaneous T cell lymphomas (CTCL), typified by mycosis fungoides, and several chronic T cell mediated dermatoses are characterized by the migration of T lymphocytes into the epidermis (epidermotropism). Alternatively, other types of cutaneous inflammation (malignant cutaneous B cell lymphoma, CBCL, or lymphocytoma cutis, non-malignant T or B cell type) do not show evidence of epidermotropism. This suggests that certain T lymphocyte subpopulations are able to interact with and penetrate the epidermal basement membrane. We show here that T lymphocytes derived from patients with CTCL (HUT 78 or HUT 102 cells), adhere to the detergent-insoluble extracellular matrix prepared from cultured basal keratinocytes (HFK ECM). HUT cell adhesion to HFK ECM was inhibitable with monoclonal antibodies (mAbs) directed to the alpha 3 (P1B5) or beta 1 (P4C10) integrin receptors, and could be up-regulated by an activating anti-beta 1 mAb (P4G11). An inhibitory mAb, P3H9-2, raised against keratinocytes identified epiligrin as the ligand for alpha 3 beta 1 positive T cells in HFK ECM. Interestingly, two lymphocyte populations could be clearly distinguished relative to expression of alpha 3 beta 1 by flow cytometry analysis. Lymphokine activated killer cells, alloreactive cytotoxic T cells and T cells derived from patients with CTCL expressed high levels of alpha 3 beta 1 (alpha 3 beta 1high). Non-adherent peripheral blood mononuclear cells, acute T or B lymphocytic leukemias, or non-cutaneous T or B lymphocyte cell lines expressed low levels of alpha 3 beta 1 (alpha 3 beta 1low). Resting PBL or alpha 3 beta 1low T or B cell lines did not adhere to HFK ECM or purified epiligrin. However, adhesion to epiligrin could be up-regulated by mAbs which activate the beta 1 subunit indicating that alpha 3 beta 1 activity is a function of expression and affinity. In skin derived from patients with graft-vs.-host (GVH) disease, experimentally induced delayed hypersensitivity reactions, and CTCL, the infiltrating T cells could be stained with mAbs to alpha 3 or beta 1 and were localized in close proximity to the epiligrin-containing basement membrane. Infiltrating lymphocytes in malignant cutaneous B disease (CBCL) did not express alpha 3 beta 1 by immunohistochemical techniques and did not associate with the epidermal basement membrane. The present findings clearly define a function for alpha 3 beta 1 in T cells and strongly suggest that alpha 3 beta 1 interaction with epiligrin may be involved in the pathogenesis of cutaneous inflammation.

摘要

以蕈样肉芽肿为代表的皮肤T细胞淋巴瘤(CTCL)以及几种慢性T细胞介导的皮肤病,其特征在于T淋巴细胞向表皮迁移(亲表皮性)。相比之下,其他类型的皮肤炎症(恶性皮肤B细胞淋巴瘤,CBCL,或皮肤淋巴细胞瘤,非恶性T或B细胞类型)则没有亲表皮性的证据。这表明某些T淋巴细胞亚群能够与表皮基底膜相互作用并穿透它。我们在此表明,源自CTCL患者的T淋巴细胞(HUT 78或HUT 102细胞),能够黏附于由培养的基底角质形成细胞制备的去污剂不溶性细胞外基质(HFK ECM)。HUT细胞与HFK ECM的黏附可被针对α3(P1B5)或β1(P4C10)整合素受体的单克隆抗体(mAb)抑制,并且可被一种激活抗β1 mAb(P4G11)上调。一种针对角质形成细胞产生的抑制性mAb P3H9 - 2,确定表皮整联配体蛋白为HFK ECM中α3β1阳性T细胞的配体。有趣的是,通过流式细胞术分析,相对于α3β1的表达,可以清楚地区分两个淋巴细胞群体。淋巴因子激活的杀伤细胞、同种异体反应性细胞毒性T细胞以及源自CTCL患者的T细胞表达高水平的α3β1(α3β1高)。非黏附性外周血单核细胞、急性T或B淋巴细胞白血病,或非皮肤T或B淋巴细胞系表达低水平的α3β1(α3β1低)。静息的外周血淋巴细胞或α3β1低的T或B细胞系不黏附于HFK ECM或纯化的表皮整联配体蛋白。然而,对表皮整联配体蛋白的黏附可被激活β1亚基的mAb上调,表明α3β1活性是表达和亲和力的函数。在移植物抗宿主(GVH)病、实验性诱导的迟发型超敏反应以及CTCL患者的皮肤中,浸润的T细胞可用针对α3或β1的mAb染色,并定位在靠近含表皮整联配体蛋白的基底膜附近。恶性皮肤B病(CBCL)中的浸润淋巴细胞通过免疫组织化学技术不表达α3β1,并且不与表皮基底膜相关联。目前的研究结果明确了α3β1在T细胞中的功能,并强烈表明α3β1与表皮整联配体蛋白的相互作用可能参与皮肤炎症的发病机制。

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