首页> 外文OA文献 >Accumulation of low-avidity anti-melanocortin receptor 1 (anti-MC1R) CD8+ T cells in the lesional skin of a patient with melanoma-related depigmentation
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Accumulation of low-avidity anti-melanocortin receptor 1 (anti-MC1R) CD8+ T cells in the lesional skin of a patient with melanoma-related depigmentation

机译:黑色素瘤相关色素沉着患者病变皮肤中低强度抗黑皮质素受体1(抗MC1R)CD8 + T细胞的积累

摘要

Spontaneous or therapy-induced depigmentation in patients with melanoma has long been considered a favourable prognostic indicator. In this report, we isolated T cells infiltrating the depigmented skin of an HLA-A2+/DR4+ patient with melanoma, and detected a very high frequency of CD8+ T cells specific for melanocortin receptor 1 (MC1R), a hormone receptor involved in cutaneous pigmentation. In particular, tissue-infiltrating CD8+ T cells dominantly recognized the novel MC1R52-60 peptide epitope in an HLA-A2-restricted manner, and peptide-reactive CD8+ T cells were also detected in freshly isolated peripheral blood from this patient. Although type 1 CD4+ T-cell responses against MC1R were not detected in fresh tissue isolates, short-term in-vitro stimulation of peripheral blood lymphocytes resulted in the rapid expansion of CD4+ T cells reactive against novel HLA-DR4-presented epitopes derived from the MC1R protein (i.e. MC1R82-95, MC1R105-118 and MC1R149-161). MC1R peptide-specific CD8+ T-cell clones isolated from the depigmented skin of this patient were characterized by comparatively low functional avidity for specific major histocompatibility complex-peptide complexes and were poorly lytic; however, these effector cells were capable of secreting both interferon-gamma and granzyme B against relevant target cells in vitro, and may have played an important role in the induction of leucoderma in situ in this patient
机译:长期以来,黑素瘤患者自发性或治疗性脱色素一直被认为是良好的预后指标。在本报告中,我们分离了浸润了黑色素瘤HLA-A2 + / DR4 +患者色素沉着皮肤的T细胞,并检测了特异于黑色素皮质激素受体1(MC1R)(一种参与皮肤色素沉着的激素受体)的CD8 + T细胞的非常高的频率。特别是,组织浸润的CD8 + T细胞以HLA-A2限制性方式主要识别了新型MC1R52-60肽表位,并且还在从该患者新鲜分离的外周血中检测到了肽反应性CD8 + T细胞。尽管在新鲜的组织分离物中未检测到针对MC1R的1型CD4 + T细胞应答,但短期体外刺激外周血淋巴细胞导致CD4 + T细胞迅速扩增,该CD4 + T细胞可与源自HLA-DR4的新抗原表位反应MC1R蛋白(即MC1R82-95,MC1R105-118和MC1R149-161)。从该患者色素沉着的皮肤中分离出的MC1R肽特异性CD8 + T细胞克隆的特点是对特定的主要组织相容性复合物-肽复合物的功能亲和力较低,并且溶解性较差;然而,这些效应细胞能够在体外针对相关靶细胞分泌γ-干扰素和粒酶B,并且可能在该患者原位诱导白带病中发挥了重要作用。

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