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1型糖尿病免疫干预的研究进展

Progress in the immunointervention of type-1 diabetes mellitus.

作者信息

Schernthaner G

机构信息

Department of Medicine I, Rudolfstiftung Hospital Vienna, Vienna, Austria.

出版信息

Horm Metab Res. 1995 Dec;27(12):547-54. doi: 10.1055/s-2007-980023.

Abstract

Immunointervention studies with immunosuppressive drugs (Cyclosporin A, Azathioprine) in type-1 diabetic patients after clinical diagnosis demonstrated that improvement of beta-cell function is not sufficient and longlasting. Since 80 - 90 % of the beta-cell mass are already destroyed at onset of type-1 diabetes, intervention studies with nicotinamide and insulin (parenteral or oral) were undertaken in the early phase of type-1 diabetes. However, immunomodulation is restricted to familial cases of type-1 diabetes (only 10% of all cases), since prediction of the disease is not possible in the general population. It cannot be excluded that the described immunintervention may only postpone but not hinder the manifestation of type-1 diabetes. Interventions with tolerance induction by BCG or GAD are promising, but did not yet result in prevention of type-1 diabetes in humans. Finally, the most effective strategy would be primary prevention by vaccination or exposure prophylaxis. Should type-1 diabetes prove to be a disease that is provoked through molecular mimicry, i.e. an immunization by an environmental antigen, then strategies to avoid contact with the environmental trigger (f.e. cow's milk protein) or to vaccinate against it (f.e. Coxsackie virus protein P2-c) could be adopted. If all these interventions are not effective in the long term run, research should be concentrated on molecular approaches after improvement in gene transfer technology.

摘要

在1型糖尿病患者临床诊断后,使用免疫抑制药物(环孢素A、硫唑嘌呤)进行的免疫干预研究表明,β细胞功能的改善并不充分且持久。由于在1型糖尿病发病时80%-90%的β细胞团已被破坏,因此在1型糖尿病早期进行了烟酰胺和胰岛素(肠外或口服)的干预研究。然而,免疫调节仅限于1型糖尿病的家族性病例(仅占所有病例的10%),因为在普通人群中无法对该病进行预测。不能排除所描述的免疫干预可能只是推迟而不是阻碍1型糖尿病的表现。通过卡介苗或谷氨酸脱羧酶诱导耐受性的干预很有前景,但尚未在人类中预防1型糖尿病。最后,最有效的策略将是通过疫苗接种或暴露预防进行一级预防。如果1型糖尿病被证明是一种通过分子模拟引发的疾病,即由环境抗原进行免疫,那么可以采取避免接触环境触发因素(如牛奶蛋白)或针对其进行疫苗接种(如柯萨奇病毒蛋白P2-c)的策略。如果所有这些干预措施从长远来看都无效,那么在基因转移技术得到改进后,研究应集中在分子方法上。

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