Whole-genome Sequencing Association Analysis of Quantitative Platelet Traits in A Large Cohort of β-thalassemia.

Xingmin Wang, Qianqian Zhang, Xianming Chen, Yushan Huang, Wei Zhang, Liuhua Liao, Xinhua Zhang, Binbin Huang, Yueyan Huang, Yuhua Ye, Mengyang Song, Jinquan Lao, Juanjuan Chen, Xiaoqin Feng, Xingjiang Long, Zhixiang Liu, Weijian Zhu, Lian Yu, Chengwu Fan, Deguo Tang, Tianyu Zhong, Mingyan Fang, Caiyun Li, Chao Niu, Li Huang, Bin Lin, Xiaoyun Hua, Xin Jin, Zilin Li, Xiangmin Xu
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Abstract

Platelet acts as a crucial monitoring indicator for hypercoagulability and thrombosis and a key target for drug regulation. Genotype-phenotype association studies have confirmed that platelet traits are quantitatively regulated by multiple genes. However, there is currently a lack of genetic studies on the heterogeneity of platelet traits in β-thalassemia under hypercoagulable state. Here, we studied the phenotypic heterogeneity of platelet count (PLT) and mean platelet volume (MPV) in 1020 β-thalassemia patients. We further performed a functionally informed whole genome sequencing association analysis of common variants and rare variants (RVs) for PLT and MPV in 916 patients through integrative analysis of whole-genome sequencing data and functional annotation data. Extreme phenotypic heterogeneity of platelet traits was observed in β-thalassemia patients. Additionally, the common variant based gene-level analysis identified the novel gene of RNF144B associated with MPV. The RV analysis identified several novel associations in both coding and noncoding genome, including missense RVs of PPP2R5C associated with PLT and missense RVs of TSSK1B associated with MPV. In conclusion, we performed a comprehensive and systematic whole genome scan of platelet traits in the β-thalassemia cohort, demonstrating the specificity of genetic regulation of platelet traits in the context of β-thalassemia, providing potential targets for intervention.

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大样本β地中海贫血患者血小板定量特征的全基因组测序关联分析
血小板是高凝状态和血栓形成的重要监测指标,也是药物调控的关键靶点。基因型-表型关联研究证实,血小板性状受多个基因的定量调控。然而,目前缺乏对高凝状态下β-地中海贫血患者血小板性状异质性的基因研究。在此,我们对 1020 名β地中海贫血患者的血小板计数(PLT)和平均血小板体积(MPV)的表型异质性进行了研究。通过对全基因组测序数据和功能注释数据的综合分析,我们进一步对 916 名患者的血小板计数和平均血小板体积的常见变异和罕见变异(RVs)进行了功能全基因组测序关联分析。在β地中海贫血患者中观察到血小板性状的极端表型异质性。此外,基于常见变异的基因水平分析发现了与 MPV 相关的新基因 RNF144B。RV分析在编码和非编码基因组中发现了几个新的关联,包括与PLT相关的PPP2R5C的错义RV和与MPV相关的TSSK1B的错义RV。总之,我们对β地中海贫血队列中的血小板性状进行了全面系统的全基因组扫描,证明了β地中海贫血背景下血小板性状遗传调控的特异性,为干预提供了潜在靶点。
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