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鉴定淋巴细胞膜糖蛋白上半乳糖凝集素配体的方法。

Method for Identifying Galectin Ligands on Lymphocyte Membrane Glycoproteins.

机构信息

Joint Program in Transfusion Medicine, Department of Pathology, Brigham and Women's Hospital, Harvard Medical School, Boston, MA, USA.

Harvard Glycomics Center, Harvard Medical School, Boston, MA, USA.

出版信息

Methods Mol Biol. 2022;2442:215-232. doi: 10.1007/978-1-0716-2055-7_13.

Abstract

Glycosylation is one of the most common protein posttranslational modifications. Most human lymphocyte membrane receptors are modified by diverse glycan structures, and functional studies have indicated that a family of glycan-binding proteins, galectins, can significantly modulate lymphocyte development and function by interacting with these glycans. Several galectins have a varying degree of affinity for the N-acetyllactosamine (LacNAc) disaccharide, and some critical lymphocyte receptors can be modified by glycan structures carrying this motif. However, the site-specific glycan composition on primary lymphocyte membrane receptors in healthy individuals is largely limited. The main reason for the limitation is low abundance of available material from a single donor and compositional heterogeneity in glycan structures that can potentially modify a protein. Donor-dependent variability in N-glycan structures on CD16a isolated from primary NK cells of healthy human donors was recently reported. NK cell CD16a is glycosylated at five N-glycosylation sites, and two of the five sites are modified, almost exclusively, by N-glycans with multiple LacNAc repeats which can serve as ligands for endogenous galectins. Thus, the protocol described in this section can be utilized to identify galectin ligands at specific glycosylation sites of endogenous membrane receptor from circulating primary human lymphocytes.

摘要

糖基化是最常见的蛋白质翻译后修饰之一。大多数人类淋巴细胞膜受体都被不同的聚糖结构所修饰,功能研究表明,一类糖结合蛋白(半乳糖凝集素)可以通过与这些聚糖相互作用,显著调节淋巴细胞的发育和功能。一些半乳糖凝集素有不同程度的亲和性与 N-乙酰乳糖胺(LacNAc)二糖结合,一些关键的淋巴细胞受体可以被携带该基序的糖结构修饰。然而,健康个体中初级淋巴细胞膜受体上的特定糖基化组成在很大程度上是有限的。造成这种限制的主要原因是从单个供体获得的可用物质的丰度低,以及可能修饰蛋白质的聚糖结构的组成异质性。最近报道了从健康人类供体的原代自然杀伤 (NK) 细胞中分离的 CD16a 的 N-糖基化结构的供体依赖性变异性。NK 细胞 CD16a 在五个 N-糖基化位点被糖基化,其中两个位点几乎完全被具有多个 LacNAc 重复的 N-糖基化修饰,这些糖基化可以作为内源性半乳糖凝集素的配体。因此,本节中描述的方案可用于鉴定循环原代人淋巴细胞内源性膜受体特定糖基化位点的半乳糖凝集素配体。

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