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非碳水化合物糖类似物和糖蛋白类似物作为 DC-SIGN 的拮抗剂和激动剂。

Noncarbohydrate glycomimetics and glycoprotein surrogates as DC-SIGN antagonists and agonists.

机构信息

Department of Biochemistry, University of Wisconsin-Madison, Madison, WI 53706, USA.

出版信息

ACS Chem Biol. 2012 Sep 21;7(9):1603-8. doi: 10.1021/cb300260p. Epub 2012 Jul 19.

Abstract

An understanding of the biological roles of lectins will be advanced by ligands that can inhibit or even recruit lectin function. To this end, glycomimetics, noncarbohydrate ligands that function analogously to endogenous carbohydrates, are being sought. The advantage of having such ligands is illustrated by the many roles of the protein DC-SIGN. DC-SIGN is a C-type lectin displayed on dendritic cells, where it binds to mannosides and fucosides to mediate interactions with other host cells or bacterial or viral pathogens. DC-SIGN engagement can modulate host immune responses (e.g., suppress autoimmunity) or benefit pathogens (e.g., promote HIV dissemination). DC-SIGN can bind to glycoconjugates, internalize glycosylated cargo for antigen processing, and transduce signals. DC-SIGN ligands can serve as inhibitors as well as probes of the lectin's function, so they are especially valuable for elucidating and controlling DC-SIGN's roles in immunity. We previously reported a small molecule that embodies key features of the carbohydrates that bind DC-SIGN. Here, we demonstrate that this noncarbohydrate ligand acts as a true glycomimetic. Using NMR HSQC experiments, we found that the compound mimics saccharide ligands: It occupies the same carbohydrate-binding site and interacts with the same amino acid residues on DC-SIGN. The glycomimetic also is functional. It had been shown previously to antagonize DC-SIGN function, but here we use it to generate DC-SIGN agonists. Specifically, appending this glycomimetic to a protein scaffold affords a conjugate that elicits key cellular signaling responses. Thus, the glycomimetic can give rise to functional glycoprotein surrogates that elicit lectin-mediated signaling.

摘要

通过能够抑制甚至招募凝集素功能的配体,可以深入了解凝集素的生物学作用。为此,人们正在寻找糖模拟物,即类似内源性碳水化合物发挥作用的非碳水化合物配体。具有此类配体的优势体现在蛋白质 DC-SIGN 的许多作用中。DC-SIGN 是一种在树突状细胞上表达的 C 型凝集素,在那里它与甘露糖和岩藻糖结合,介导与其他宿主细胞或细菌或病毒病原体的相互作用。DC-SIGN 的结合可以调节宿主免疫反应(例如,抑制自身免疫)或有益于病原体(例如,促进 HIV 的传播)。DC-SIGN 可以与糖缀合物结合,内化糖化货物进行抗原加工,并转导信号。DC-SIGN 配体可以作为凝集素功能的抑制剂和探针,因此对于阐明和控制 DC-SIGN 在免疫中的作用特别有价值。我们之前报道了一种小分子,它体现了与 DC-SIGN 结合的碳水化合物的关键特征。在这里,我们证明这种非碳水化合物配体充当真正的糖模拟物。通过 NMR HSQC 实验,我们发现该化合物模拟了糖配体:它占据相同的碳水化合物结合位点,并与 DC-SIGN 上的相同氨基酸残基相互作用。糖模拟物也具有功能。它之前已被证明可拮抗 DC-SIGN 功能,但在这里我们将其用于生成 DC-SIGN 激动剂。具体来说,将这种糖模拟物附加到蛋白质支架上,就会得到一种引发关键细胞信号响应的缀合物。因此,糖模拟物可以产生功能性糖蛋白替代物,引发凝集素介导的信号。

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