Novel and recurrent hemizygous variants in BCORL1 cause oligoasthenoteratozoospermia by interfering transcription.

IF 3.2 2区 医学 Q1 ANDROLOGY
Andrology Pub Date : 2024-08-27 DOI:10.1111/andr.13743
Yu Wang, Mingfei Xiang, Yiru Zhou, Na Zheng, Jingjing Zhang, Xiaomin Zha, Zongliu Duan, Fengsong Wang, Ying Zhang, Zhongxin Wang, Yunxia Cao, Fuxi Zhu
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引用次数: 0

Abstract

Background: Oligoasthenoteratozoospermia (OAT) is a common cause of male infertility, of which the causes remain largely unknown. Recently, BCORL1 was identified as a contributor to male infertility from non-obstructive azoospermia (NOA) to OAT.

Objectives: To identify novel and hotspot variants in BCORL1 from infertile men with OAT and reveal their outcomes of assisted reproductive treatments (ARTs).

Materials and methods: Forty-six infertile men characterized by OAT were recruited from 2017 to 2022. Variants in OAT patients were identified by whole-exome sequencing (WES) and verified by Sanger sequencing. Papanicolaou staining was used for sperm morphology analysis. Pathogenicity of BCORL1 variants were analyzed by bioinformatics analysis, and further confirmed in vitro by using recombinant plasmids and cells. Meanwhile, ARTs were performed on these patients to investigate the appropriate clinical treatment strategy.

Results: We identified a novel hemizygous missense variant (NM_021946: c.G4171A; p.G1391R) and a recurrent variant (NM_021946: c.T2615G; p.V872G) in BCORL1 from four OAT patients. Notably, routine semen assessment and Papanicolaou staining revealed a special OAT phenotype of patients with BCORL1 variants, whose rare mature sperm characterized by acephalic and abnormal acrosome. Pathogenicity analysis showed the interaction between BCORL1 with histone deacetylases (HDACs) were disrupted after variance, accompanied with epigenetic alterations and finally the orderly transcriptions of spermatogenetic genes were interfering. Besides, clinical record presented the poor outcomes of ARTs in these patients with BCORL1 variants.

Discussion and conclusions: Our findings further expand the variant spectrum of BCORL1 related to OAT, and provide new evidences that BCORL1 acts as an important transcriptional regulator, participating in epigenetic regulation and directing the expression of key genes throughout spermatogenesis. The outcomes of ARTs will facilitate the genetic counseling and clinical treatment of infertile men with BCORL1 variants in the future.

BCORL1的新型和复发性半杂合子变异通过干扰转录导致少精症。
背景:少精子症(OAT)是男性不育症的常见病因,其病因在很大程度上仍然不明。最近,人们发现 BCORL1 是导致男性不育(从非梗阻性无精子症(NOA)到 OAT)的一个因素:目的:从患有OAT的不育男性中鉴定BCORL1的新变异和热点变异,并揭示其辅助生殖治疗(ART)的结果:从2017年至2022年招募了46名以OAT为特征的不育男性。通过全外显子组测序(WES)确定了OAT患者的变异,并通过桑格测序进行了验证。精子形态分析采用巴氏染色法。通过生物信息学分析对 BCORL1 变体的致病性进行了分析,并使用重组质粒和细胞在体外进行了进一步确认。同时,对这些患者进行了抗逆转录病毒疗法,以研究适当的临床治疗策略:结果:我们从四名OAT患者中发现了BCORL1中的一个新的半杂合错义变体(NM_021946:c.G4171A;p.G1391R)和一个复发性变体(NM_021946:c.T2615G;p.V872G)。值得注意的是,常规精液评估和巴氏染色法显示,BCORL1 变异患者的 OAT 表型特殊,其罕见的成熟精子具有头状和顶体异常的特征。致病性分析表明,变异后,BCORL1 与组蛋白去乙酰化酶(HDACs)之间的相互作用被破坏,并伴有表观遗传学改变,最终干扰了精子发生基因的有序转录。此外,临床记录显示,这些BCORL1变异患者的抗逆转录病毒疗法效果不佳:我们的研究结果进一步扩展了与OAT相关的BCORL1变异谱,并为BCORL1作为一个重要的转录调节因子,参与表观遗传调控并引导整个精子发生过程中关键基因的表达提供了新的证据。抗逆转录病毒疗法的研究成果将有助于今后为患有 BCORL1 变异的不育男性提供遗传咨询和临床治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Andrology
Andrology ANDROLOGY-
CiteScore
9.10
自引率
6.70%
发文量
200
期刊介绍: Andrology is the study of the male reproductive system and other male gender related health issues. Andrology deals with basic and clinical aspects of the male reproductive system (gonads, endocrine and accessory organs) in all species, including the diagnosis and treatment of medical problems associated with sexual development, infertility, sexual dysfunction, sex hormone action and other urological problems. In medicine, Andrology as a specialty is a recent development, as it had previously been considered a subspecialty of urology or endocrinology
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