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首页> 外文期刊>International journal of immunogenetics >The Pekin duck programmed death-ligand 1: cDNA cloning, genomic structure, molecular characterization and mRNA expression analysis
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The Pekin duck programmed death-ligand 1: cDNA cloning, genomic structure, molecular characterization and mRNA expression analysis

机译:北京鸭编程的死亡配体1:cDNA克隆,基因组结构,分子表征和mRNA表达分析

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Programmed death ligand-1 (PD-L1) plays an important role in the attenuation of adaptive immune responses in higher vertebrates. Here, we describe the identification of the Pekin duck PD-L1 orthologue (duPD-L1) and its gene structure. The duPD-L1 cDNA encodes a 311-amino acid protein that has an amino acid identity of 78% and 42% with chicken and human PD-L1, respectively. Mapping of the duPD-L1 cDNA with duck genomic sequences revealed an exonic structure of its coding sequence similar to those of other vertebrates but lacked a noncoding exon 1. Homology modelling of the duPD-L1 extracellular domain was compatible with the tandem IgV-like and IgC-like IgSF domain structure of human PD-L1 (PDB ID: 3BIS). Residues known to be important for receptor binding of human PD-L1 were mostly conserved in duPD-L1 within the N-terminus and the G sheet, and partially conserved within the F sheet but not within sheets C and C'. DuPD-L1 mRNA was constitutively expressed in all tissues examined with highest expression levels in lung and spleen and very low levels of expression in muscle, kidney and brain. Mitogen stimulation of duck peripheral blood mononuclear cells transiently increased duPD-L1 mRNA expression. Our observations demonstrate evolutionary conservation of the exonic structure of its coding sequence, the extracellular domain structure and residues implicated in receptor binding, but the role of the longer cytoplasmic tail in avian PD-L1 proteins remains to be determined.
机译:程序性死亡配体1(PD-L1)在减轻高等脊椎动物的适应性免疫反应中起重要作用。在这里,我们描述了北京烤鸭PD-L1直系同源物(duPD-L1)的鉴定及其基因结构。 duPD-L1 cDNA编码一个311个氨基酸的蛋白质,与鸡和人PD-L1的氨基酸同一性分别为78%和42%。用鸭基因组序列对duPD-L1 cDNA进行定位,发现其编码序列的外显子结构与其他脊椎动物相似,但缺少非编码外显子1。duPD-L1胞外域的同源性建模与串联IgV样和人类PD-L1的IgC样IgSF域结构(PDB ID:3BIS)。已知对人PD-L1的受体结合很重要的残基在N端和G片中的duPD-L1中大多数保守,在F片中部分保守,但在C和C'片中不保守。 DuPD-L1 mRNA在所有检查的组织中组成性表达,在肺和脾中的表达水平最高,而在肌肉,肾脏和脑中的表达水平非常低。鸭外周血单核细胞的丝裂原刺激短暂增加了duPD-L1 mRNA表达。我们的观察结果表明其编码序列的外显子结构,胞外域结构和与受体结合有关的残基的进化保守性,但禽PD-L1蛋白中较长的细胞质尾巴的作用仍有待确定。

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