Structural and functional conservation of CLEC-2 with the species-specific regulation of transcript expression in evolution

被引:0
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作者
Lan Wang
Shifang Ren
Haiyan Zhu
Dongmei Zhang
Yuqing Hao
Yuanyuan Ruan
Lei Zhou
Chiayu Lee
Lin Qiu
Xiaojing Yun
Jianhui Xie
机构
[1] Shanghai Medical College of Fudan University,Department of Biochemistry and Molecular Biology
[2] Fudan University,Gene research center, Institutes of Biomedical Sciences
[3] Chinese Academy of Sciences,Institute for Nutritional Sciences, Shanghai Institutes for Biological Sciences
来源
Glycoconjugate Journal | 2012年 / 29卷
关键词
CLEC-2; Homology; N-glycosylation; Ligand-binding; Alternative splicing;
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学科分类号
摘要
CLEC-2 was first identified by sequence similarity to C-type lectin-like molecules with immune functions and has been reported as a receptor for the platelet-aggregating snake venom toxin rhodocytin and the endogenous sialoglycoprotein podoplanin. Recent researches indicate that CLEC-2-deficient mice were lethal at the embryonic stage associated with disorganized and blood-filled lymphatic vessels and severe edema. In view of a necessary role of CLEC-2 in the individual development, it is of interest to investigate its phylogenetic homology and highly conserved functional regions. In this work, we reported that CLEC-2 from different species holds with an extraordinary conservation by sequence alignment and phylogenetic tree analysis. The functional structures including N-linked oligosaccharide sites and ligand-binding domain implement a structural and functional conservation in a variety of species. The glycosylation sites (N120 and N134) are necessary for the surface expression CLEC-2. CLEC-2 from different species possesses the binding activity of mouse podoplanin. Nevertheless, the expression of CLEC-2 is regulated with a species-specific manner. The alternative splicing of pre-mRNA, a regulatory mechanism of gene expression, and the binding sites on promoter for several key transcription factors vary between different species. Therefore, CLEC-2 shares high sequence homology and functional identity. However the transcript expression might be tightly regulated by different mechanisms in evolution.
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页码:335 / 345
页数:10
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