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根据 HLA-F 遗传多态性的差异,研究 HLA-F 的转录和蛋白表达情况。

HLA-F transcriptional and protein differential expression according to its genetic polymorphisms.

机构信息

Xegen, Gemenos, France.

GenPhySE, Université de Toulouse, INRAE, INPT, INP-ENVT, Castanet Tolosan, France.

出版信息

HLA. 2023 Nov;102(5):578-589. doi: 10.1111/tan.15087. Epub 2023 May 11.

Abstract

Many specificities single out HLA-F: its structure, expression regulation at cell membrane and function. HLA-F mRNA is detected in the most cell types and the protein is localized in the ER and Golgi apparatus. When expressed at cell surface, HLA-F may be associated to β2-microglobulin and peptide or expressed as an open-conformer molecule. HLA-F reaches the membrane upon activation of different primary cell types and cell-lines. HLA-F has its highest affinity for the KIR3DS1-activating NK receptor, but also binds inhibitory immune receptors. Some studies reported that HLA-F expression is associated with its genotype. Higher HLA-F mRNA expression associated with F*01:01:02, and 3 noncoding SNPs, rs1362126, rs2523405, and rs2523393, located in HLA-F-AS1 or upstream the HLA-F sequence were associated with HLA-F mRNA expression. Given the implication of HLA-F in many clinical setting, and the undisclosed process of its expression regulation, we aim to confirm the effect of the aforementioned SNPs with HLA-F transcriptional and protein expression. We analyzed the distribution, frequency and linkage disequilibrium of these SNPs at worldwide scale in the 1000 Genomes Project samples. Influence on the genotype of each SNP on HLA-F expression was explored using RNAseq data from the 1000 Genomes Project, and using Q-PCR and intracellular cytometry in PBMC from healthy individuals. Our results show that the SNPs under studied displayed remarkably different allelic proportion according to geography and confirm that rs1362126, rs2523405, and rs2523393 displayed the most concordant results, with the highest effect size and a double-dose effect.

摘要

许多特异性使 HLA-F 脱颖而出:其结构、细胞膜表达调控和功能。HLA-F mRNA 可在大多数细胞类型中检测到,其蛋白定位于内质网和高尔基体。当在细胞表面表达时,HLA-F 可能与β2-微球蛋白和肽结合,或表达为开放构象分子。HLA-F 在不同的原代细胞类型和细胞系激活时到达细胞膜。HLA-F 对激活 NK 受体的 KIR3DS1 具有最高亲和力,但也结合抑制性免疫受体。一些研究报道 HLA-F 表达与其基因型相关。较高的 HLA-F mRNA 表达与 F*01:01:02 和 3 个非编码 SNPs(rs1362126、rs2523405 和 rs2523393)相关,这些 SNPs 位于 HLA-F-AS1 或 HLA-F 序列的上游,与 HLA-F mRNA 表达相关。鉴于 HLA-F 在许多临床环境中的重要性,以及其表达调控的未知过程,我们旨在确认上述 SNPs 对 HLA-F 转录和蛋白表达的影响。我们在 1000 基因组项目样本中分析了这些 SNPs 在全球范围内的分布、频率和连锁不平衡。使用 1000 基因组项目的 RNAseq 数据和来自健康个体的 PBMC 的 Q-PCR 和细胞内细胞仪,探索了每个 SNP 的基因型对 HLA-F 表达的影响。我们的结果表明,在所研究的 SNP 中,等位基因比例因地理位置而异,并且证实 rs1362126、rs2523405 和 rs2523393 显示出最一致的结果,具有最大的效应大小和双倍剂量效应。

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