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癌症相关糖鞘脂抗原:其结构、组织及功能

Cancer-associated glycosphingolipid antigens: their structure, organization, and function.

作者信息

Hakomori S

机构信息

Pacific Northwest Research Institute and Department of Pathobiology University of Washington, Seattle, WA 98122, USA.

出版信息

Acta Anat (Basel). 1998;161(1-4):79-90. doi: 10.1159/000046451.

Abstract

Experimental and human cancers are often characterized by the presence of tumor-associated glycosphingolipid (GSL) antigens defined by monoclonal antibodies. Major progress has been made during the past two decades on structural identification of these antigens. None of these structures are truly 'tumor-specific'. However, many of the antibodies show preferential or 'specific' reactivity with tumors, based on organizational differences of membrane GSLs in tumor cells versus normal cells. Clustered GSL antigens organized with transducer molecules in microdomain have been found recently to comprise a structural and functional unit involved in tumor cell adhesion coupled with signal transduction. Some of the GSL antigens have been identified as adhesion molecules recognized by carbohydrate-binding proteins or by complementary carbohydrates on target cells. Such adhesion, coupled with signaling, may initiate the metastatic process. Elucidating the mechanism of this initial adhesion/signaling step may lead to discovery of therapeutic agents that disrupt adhesion ('antiadhesion therapy') or normalize signaling ('ortho-signaling therapy'). Tumor-associated GSL antigens are also a target in immunotherapy of tumors, including development of antitumor vaccines.

摘要

实验性癌症和人类癌症通常具有由单克隆抗体定义的肿瘤相关糖鞘脂(GSL)抗原。在过去二十年中,这些抗原的结构鉴定取得了重大进展。这些结构都不是真正的“肿瘤特异性”。然而,基于肿瘤细胞与正常细胞膜GSL的组织差异,许多抗体对肿瘤表现出优先或“特异性”反应。最近发现,在微结构域中与转导分子一起组织的聚集GSL抗原构成了一个涉及肿瘤细胞粘附并与信号转导相关的结构和功能单元。一些GSL抗原已被鉴定为被碳水化合物结合蛋白或靶细胞上的互补碳水化合物识别的粘附分子。这种粘附与信号传导相结合,可能启动转移过程。阐明这一初始粘附/信号步骤的机制可能会导致发现破坏粘附的治疗剂(“抗粘附疗法”)或使信号正常化的治疗剂(“正信号疗法”)。肿瘤相关GSL抗原也是肿瘤免疫治疗的靶点,包括抗肿瘤疫苗的开发。

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