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与胰岛素依赖型糖尿病相关的胰岛免疫杀伤机制:人类细胞和抗体介导的胰岛细胞细胞毒性的体外表达

Immune islet killing mechanisms associated with insulin-dependent diabetes: in vitro expression of cellular and antibody-mediated islet cell cytotoxicity in humans.

作者信息

Charles M A, Suzuki M, Waldeck N, Dodson L E, Slater L, Ong K, Kershnar A, Buckingham B, Golden M

出版信息

J Immunol. 1983 Mar;130(3):1189-94.

PMID:6337213
Abstract

Because immune mechanisms are associated with insulin-dependent diabetes, multiple organ specific and xenogeneic cytotoxicity assays were developed. Human cellular and antibody effector systems were incubated with 51Cr-labeled dispersed normal rat islet target cells. In eight of 11 diabetic patients, nonenriched mononuclear cells incubated with islet target cells were more cytotoxic than cells from age- and sex-matched controls (p less than 0.01). When non-T cell-enriched mononuclear cells were used at diabetes onset, seven of 11 patients' cells showed excessive islet cytotoxicity (p less than 0.05). In four patients showing elevated cytotoxicity at diabetes onset, cytotoxicity decreased to control levels during diabetes remission. Islet specificity was suggested in that mononuclear cells derived from diabetic subjects did not mediate cytotoxicity against rat spleen or macrophage target cells. Three cytotoxic antibody mechanisms were also evaluated. C-dependent antibody-mediated cytotoxicity with the use of patient serum-coated islet target cells was elevated above control levels in four of 14 patients. Antibody-dependent cellular cytotoxicity exceeded control values in only two of 16 patients, although four assay systems were evaluated. C-augmented antibody-dependent cellular cytotoxicity was elevated in three of 14 patients. No differences were observed for antibody-mediated mechanisms in four patients evaluated at both diabetes onset and remission. Cytotoxic antibody was present in only about one-half of the patients showing increased cellular cytotoxicity, whereas most patients expressing increased cytotoxic antibody had cellular cytotoxicity. Islet cell cytotoxicity assays with the use of effector systems from patients with recent onset insulin-dependent diabetes suggest that direct cellular cytotoxicity is more active than antibody-mediated cytotoxic mechanisms, and that cellular cytotoxicity can correlate with disease activity.

摘要

由于免疫机制与胰岛素依赖型糖尿病相关,因此开发了多种器官特异性和异种细胞毒性检测方法。将人细胞和抗体效应系统与51Cr标记的分散正常大鼠胰岛靶细胞一起孵育。在11例糖尿病患者中的8例中,与胰岛靶细胞孵育的未富集单核细胞比年龄和性别匹配的对照组细胞具有更高的细胞毒性(p小于0.01)。在糖尿病发病时使用未富集T细胞的单核细胞,11例患者中的7例细胞表现出过度的胰岛细胞毒性(p小于0.05)。在4例糖尿病发病时细胞毒性升高的患者中,糖尿病缓解期间细胞毒性降至对照水平。胰岛特异性表现为糖尿病受试者来源的单核细胞不介导对大鼠脾脏或巨噬细胞靶细胞的细胞毒性。还评估了三种细胞毒性抗体机制。在14例患者中的4例中,使用患者血清包被的胰岛靶细胞的补体依赖性抗体介导的细胞毒性高于对照水平。尽管评估了四种检测系统,但在16例患者中只有2例抗体依赖性细胞毒性超过对照值。在14例患者中的3例中,补体增强的抗体依赖性细胞毒性升高。在糖尿病发病和缓解时评估的4例患者中,抗体介导的机制未观察到差异。在显示细胞毒性增加的患者中,只有约一半存在细胞毒性抗体,而大多数表达增加的细胞毒性抗体的患者具有细胞毒性。使用近期发病的胰岛素依赖型糖尿病患者的效应系统进行胰岛细胞毒性检测表明,直接细胞毒性比抗体介导的细胞毒性机制更活跃,并且细胞毒性与疾病活动相关。

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