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禽类CD1的晶体结构显示,与哺乳动物CD1相比,其抗原结合口袋更小、更原始。

The crystal structure of avian CD1 reveals a smaller, more primordial antigen-binding pocket compared to mammalian CD1.

作者信息

Zajonc Dirk M, Striegl Harald, Dascher Christopher C, Wilson Ian A

机构信息

Division of Cell Biology, La Jolla Institute for Allergy and Immunology, 9420 Athena Circle, La Jolla, CA 92037, USA.

出版信息

Proc Natl Acad Sci U S A. 2008 Nov 18;105(46):17925-30. doi: 10.1073/pnas.0809814105. Epub 2008 Nov 12.

DOI:10.1073/pnas.0809814105
PMID:19004781
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2584731/
Abstract

The molecular details of glycolipid presentation by CD1 antigen-presenting molecules are well studied in mammalian systems. However, little is known about how these non-classical MHC class I (MHCI) molecules diverged from the MHC locus to create a more complex, hydrophobic binding groove that binds lipids rather than peptides. To address this fundamental question, we have determined the crystal structure of an avian CD1 (chCD1-2) that shares common ancestry with mammalian CD1 from approximately 310 million years ago. The chCD1-2 antigen-binding site consists of a compact, narrow, central hydrophobic groove or pore rather than the more open, 2-pocket architecture observed in mammalian CD1s. Potential antigens then would be restricted in size to single-chain lipids or glycolipids. An endogenous ligand, possibly palmitic acid, serves to illuminate the mode and mechanism of ligand interaction with chCD1-2. The palmitate alkyl chain is inserted into the relatively shallow hydrophobic pore; its carboxyl group emerges at the receptor surface and is stabilized by electrostatic and hydrogen bond interactions with an arginine residue that is conserved in all known CD1 proteins. In addition, other novel features, such as an A' loop that interrupts and segments the normally long, continuous alpha1 helix, are unique to chCD1-2 and contribute to the unusually narrow binding groove, thereby limiting its size. Because birds and mammals share a common ancestor, but the rate of evolution is slower in birds than in mammals, the chCD1-2-binding groove probably represents a more primordial CD1-binding groove.

摘要

在哺乳动物系统中,CD1抗原呈递分子呈递糖脂的分子细节已得到充分研究。然而,对于这些非经典的MHC I类(MHCI)分子如何从MHC基因座分化出来,从而形成一个更复杂的、结合脂质而非肽段的疏水结合槽,人们却知之甚少。为了解决这个基本问题,我们确定了一种禽类CD1(chCD1-2)的晶体结构,它与哺乳动物CD1大约在3.1亿年前拥有共同的祖先。chCD1-2抗原结合位点由一个紧凑、狭窄的中央疏水凹槽或孔隙组成,而不是在哺乳动物CD1中观察到的更开放的双口袋结构。那么潜在的抗原在大小上可能会被限制为单链脂质或糖脂。一种内源性配体,可能是棕榈酸,有助于阐明配体与chCD1-2相互作用的方式和机制。棕榈酸的烷基链插入相对较浅的疏水孔隙中;其羧基在受体表面露出,并通过与所有已知CD1蛋白中保守的精氨酸残基的静电和氢键相互作用而稳定。此外,其他一些新特征,比如一个打断并分割通常较长的连续α1螺旋的A'环,是chCD1-2所特有的,并且导致了异常狭窄的结合槽,从而限制了其大小。由于鸟类和哺乳动物有共同的祖先,但鸟类的进化速度比哺乳动物慢,chCD1-2结合槽可能代表了一种更原始的CD1结合槽。

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