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神经节苷脂与自身免疫性糖尿病

Gangliosides and autoimmune diabetes.

作者信息

Misasi R, Dionisi S, Farilla L, Carabba B, Lenti L, Di Mario U, Dotta F

机构信息

Department of Experimental Medicine, University of Rome, La Sapienza, Italy.

出版信息

Diabetes Metab Rev. 1997 Sep;13(3):163-79. doi: 10.1002/(sici)1099-0895(199709)13:3<163::aid-dmr189>3.0.co;2-z.

DOI:10.1002/(sici)1099-0895(199709)13:3<163::aid-dmr189>3.0.co;2-z
PMID:9307889
Abstract

Gangliosides are sialic acid-containing glycolipids which are formed by a hydrophobic portion, the ceramide, and a hydrophilic part, i.e. the oligosaccharide chain. First described in neural tissue, several studies have shown that gangliosides are almost ubiquitous molecules expressed in all vertebrate tissues. Within cells, gangliosides are usually associated with plasma membranes, where they can act as receptors for a variety of molecules and have been shown to take part in cell-to-cell interaction and in signal transduction. In addition, gangliosides are expressed in cytosol membranes like those of secretory granules of some endocrine cells (adrenal medulla, pancreatic islets). As far as the role of gangliosides in diseases is concerned, there are some cases in which an aberrant ganglioside expression plays a crucial role in the disease pathogenetic process. These diseases include two major forms of ganglioside storage, namely GM2-gangliosidosis (Tay-Sachs and its beta-hexosaminidase deficiency) and GM1-gangliosidosis (beta-galactosidase deficiency), where the most prominent pathological characteristic is the lysosomal ganglioside accumulation in neurons. Other inflammatory or degenerative diseases both within and outside the nervous system have been shown to be associated with an altered pattern of ganglioside expression in the target organ. Since monoclonal antibodies have been discovered and used in immunology, a large variety of ganglioside antigens has been described both as blood group antigens and as tumour-related antigens. Several studies have also indicated that gangliosides can act not only as antigens, but also as autoantigens. As a matter of fact, auto-antibodies to gangliosides, detected by immunostaining methods performed directly on TLC plates or by ELISA, have been described in several autoimmune disorders such as Guillain-Barré syndrome, multiple sclerosis, lupus erythematosus, Hashimoto's thyroiditis and, last but not least, insulin-dependent (type 1) diabetes mellitus. This last disease is caused by the autoimmune destruction of insulin-producing pancreatic islet cells in genetically predisposed individuals. Autoantibodies and T lymphocytes directed towards multiple islet autoantigens have been detected in the circulation, well before the clinical onset of the disease, in a prodromal phase during which pancreatic islet beta-cells are presumably destroyed. Among the target autoantigens, some are of protein nature but others are acidic glycolipids such as sulphatides158 and the gangliosides GT3, GD3 and especially GM2-1. This last component is specifically expressed in pancreatic islets and has been shown to represent a target of IgG autoantibodies highly associated with diabetes development in first-degree relatives of type 1 diabetic individuals. In addition, the GM2-1 ganglioside appears to be one of the antigens recognized by cytoplasmic ICA, a heterogeneous group of antibodies which specifically react with islets on pancreatic frozen sections. In conclusion, studies performed in the last decade have clearly indicated that gangliosides represent a heterogeneous class of molecules that are involved in several cellular processes that are of crucial importance in physiological as well as in pathological conditions. Interestingly, these molecules, despite their small size, have been shown to represent not only important antigens in tumour immunology but are also able to elicit a specific autoimmune response, thus representing important autoantigens in some autoimmune disorders. It is of interest that, in addition to neurological autoimmune disorders where autoimmunity to gangliosides is frequent and usually of considerable magnitude, an autoimmune response to this class of molecules has been observed in autoimmune diabetes. (ABSTRACT TRUNCATED)

摘要

神经节苷脂是含唾液酸的糖脂,由疏水部分神经酰胺和亲水部分即寡糖链组成。神经节苷脂最初在神经组织中被描述,多项研究表明,它们几乎是在所有脊椎动物组织中都有表达的普遍存在的分子。在细胞内,神经节苷脂通常与质膜相关,在质膜上它们可作为多种分子的受体,并已被证明参与细胞间相互作用和信号转导。此外,神经节苷脂也在一些内分泌细胞(肾上腺髓质、胰岛)分泌颗粒等胞内膜中表达。就神经节苷脂在疾病中的作用而言,在某些情况下,异常的神经节苷脂表达在疾病发病过程中起关键作用。这些疾病包括两种主要形式的神经节苷脂贮积症,即GM2神经节苷脂贮积症(泰-萨克斯病及其β-己糖胺酶缺乏症)和GM1神经节苷脂贮积症(β-半乳糖苷酶缺乏症),其最突出的病理特征是神经元中溶酶体神经节苷脂蓄积。神经系统内外的其他炎症性或退行性疾病已被证明与靶器官中神经节苷脂表达模式的改变有关。自从单克隆抗体在免疫学中被发现和应用以来,多种神经节苷脂抗原已被描述为血型抗原和肿瘤相关抗原。多项研究还表明,神经节苷脂不仅可作为抗原,还可作为自身抗原。事实上,通过直接在薄层层析板上进行免疫染色或酶联免疫吸附测定法检测到的针对神经节苷脂的自身抗体,已在多种自身免疫性疾病中被描述,如格林-巴利综合征、多发性硬化症、红斑狼疮、桥本甲状腺炎,以及最后但同样重要的胰岛素依赖型(1型)糖尿病。最后这种疾病是由遗传易感性个体中产生胰岛素的胰岛细胞的自身免疫性破坏引起的。在疾病临床发作之前,即在胰岛β细胞可能被破坏的前驱期,在循环中就已检测到针对多种胰岛自身抗原的自身抗体和T淋巴细胞。在靶自身抗原中,有些是蛋白质性质的,但其他的是酸性糖脂,如硫苷脂158以及神经节苷脂GT3、GD3,尤其是GM2-1。最后这种成分在胰岛中特异性表达,并已被证明是与1型糖尿病患者一级亲属中糖尿病发生高度相关的IgG自身抗体的靶标。此外,GM2-1神经节苷脂似乎是细胞质胰岛细胞自身抗体(ICA)识别的抗原之一,ICA是一组异质性抗体,可与胰腺冰冻切片上的胰岛特异性反应。总之,过去十年进行的研究清楚地表明,神经节苷脂代表一类异质性分子,它们参与了在生理和病理状况下都至关重要的多个细胞过程。有趣的是,这些分子尽管体积小,但已被证明不仅是肿瘤免疫学中的重要抗原,而且还能够引发特异性自身免疫反应,因此在某些自身免疫性疾病中是重要的自身抗原。值得注意的是,除了神经节苷脂自身免疫常见且通常程度相当大的神经自身免疫性疾病外,在自身免疫性糖尿病中也观察到了针对这类分子的自身免疫反应。 (摘要截选)

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Autoimmunity to the GM2-1 islet ganglioside before and at the onset of type I diabetes.在I型糖尿病发病前及发病时对GM2-1胰岛神经节苷脂的自身免疫反应。
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Rat pancreatic ganglioside expression: differences between a model of autoimmune islet B cell destruction and a normal strain.大鼠胰腺神经节苷脂表达:自身免疫性胰岛B细胞破坏模型与正常品系之间的差异。
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