先天性性腺功能减退症的遗传结构:葡萄牙队列分析的启示。

IF 8.3 Q1 OBSTETRICS & GYNECOLOGY
Human reproduction open Pub Date : 2024-09-11 eCollection Date: 2024-01-01 DOI:10.1093/hropen/hoae053
Josianne Nunes Carriço, Catarina Inês Gonçalves, Asma Al-Naama, Najeeb Syed, José Maria Aragüés, Margarida Bastos, Fernando Fonseca, Teresa Borges, Bernardo Dias Pereira, Duarte Pignatelli, Davide Carvalho, Filipe Cunha, Ana Saavedra, Elisabete Rodrigues, Joana Saraiva, Luisa Ruas, Nuno Vicente, João Martin Martins, Adriana De Sousa Lages, Maria João Oliveira, Cíntia Castro-Correia, Miguel Melo, Raquel Gomes Martins, Joana Couto, Carolina Moreno, Diana Martins, Patrícia Oliveira, Teresa Martins, Sofia Almeida Martins, Olinda Marques, Carla Meireles, António Garrão, Cláudia Nogueira, Carla Baptista, Susana Gama-de-Sousa, Cláudia Amaral, Mariana Martinho, Catarina Limbert, Luisa Barros, Inês Henriques Vieira, Teresa Sabino, Luís R Saraiva, Manuel Carlos Lemos
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引用次数: 0

摘要

研究问题:葡萄牙先天性性腺功能减退症(CHH)患者的遗传缺陷有哪些影响?研究发现,约三分之一的CHH患者有遗传病因,致病基因和可能致病的种系变异分布在10个不同的基因中;寡基因遗传的病例也包括在内:CHH是一种罕见的遗传异质性疾病,其特征是GnRH、LH和FSH的产生、分泌或作用不足,导致青春期延迟或缺失以及不育:对 81 名葡萄牙 CHH 患者(36 名 Kallmann 综合征患者和 45 名正常性腺功能减退症患者)和 263 名未受影响的对照组进行了基因筛查:遗传分析通过全外显子组测序进行,然后对 169 个 CHH 相关基因的虚拟面板进行分析。主要结果指标是非同义罕见序列变异(群体等位基因频率主要结果和偶然性的作用:29.6%的患者确定了遗传原因。致病基因变异和可能致病基因变异分布在 10 个分析基因中。最常涉及的基因是 GNRHR、FGFR1、ANOS1 和 CHD7。在 6.2% 的患者中观察到致病和可能致病变异的寡致病性。在 85.2% 和 54.3% 的患者中分别观察到 VUS 和 VUS 变异的寡源性,但与在对照组中观察到的差异不大:不适用:大量 VUS 的鉴定给解释带来了挑战,随着更多证据的出现,这些 VUS 可能需要重新分类。未对非编码变异和拷贝数变异进行研究。未对变异进行功能研究:这项研究强调了CHH的遗传异质性,并发现了几个新的变异体,扩大了该疾病的变异谱。相当一部分患者仍未得到遗传学诊断,这表明还有其他遗传、表观遗传或环境因素的参与。VUS的高频率强调了谨慎解读变异的重要性。这些发现有助于人们了解CHH的遗传结构,并强调了进一步研究的必要性,以阐明CHH的潜在机制并确定其他病因:本研究由葡萄牙科技基金会(资助编号:PTDC/SAU-GMG/098419/2008、UIDB/00709/2020、CEECINST/00016/2021/CP2828/CT0002 和 2020.04924.BD)和卡塔尔基金会成员 Sidra Medicine(资助编号:SDR400038)资助。作者不声明任何利益冲突。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Genetic architecture of congenital hypogonadotropic hypogonadism: insights from analysis of a Portuguese cohort.

Study question: What is the contribution of genetic defects in Portuguese patients with congenital hypogonadotropic hypogonadism (CHH)?

Summary answer: Approximately one-third of patients with CHH were found to have a genetic cause for their disorder, with causal pathogenic and likely pathogenic germline variants distributed among 10 different genes; cases of oligogenic inheritance were also included.

What is known already: CHH is a rare and genetically heterogeneous disorder characterized by deficient production, secretion, or action of GnRH, LH, and FSH, resulting in delayed or absent puberty, and infertility.

Study design size duration: Genetic screening was performed on a cohort of 81 Portuguese patients with CHH (36 with Kallmann syndrome and 45 with normosmic hypogonadotropic hypogonadism) and 263 unaffected controls.

Participants/materials setting methods: The genetic analysis was performed by whole-exome sequencing followed by the analysis of a virtual panel of 169 CHH-associated genes. The main outcome measures were non-synonymous rare sequence variants (population allele frequency <0.01) classified as pathogenic, likely pathogenic, and variants of uncertain significance (VUS).

Main results and the role of chance: A genetic cause was identified in 29.6% of patients. Causal pathogenic and likely pathogenic variants were distributed among 10 of the analysed genes. The most frequently implicated genes were GNRHR, FGFR1, ANOS1, and CHD7. Oligogenicity for pathogenic and likely pathogenic variants was observed in 6.2% of patients. VUS and oligogenicity for VUS variants were observed in 85.2% and 54.3% of patients, respectively, but were not significantly different from that observed in controls.

Large scale data: N/A.

Limitations reasons for caution: The identification of a large number of VUS presents challenges in interpretation and these may require reclassification as more evidence becomes available. Non-coding and copy number variants were not studied. Functional studies of the variants were not undertaken.

Wider implications of the findings: This study highlights the genetic heterogeneity of CHH and identified several novel variants that expand the mutational spectrum of the disorder. A significant proportion of patients remained without a genetic diagnosis, suggesting the involvement of additional genetic, epigenetic, or environmental factors. The high frequency of VUS underscores the importance of cautious variant interpretation. These findings contribute to the understanding of the genetic architecture of CHH and emphasize the need for further studies to elucidate the underlying mechanisms and identify additional causes of CHH.

Study funding/competing interests: This research was funded by the Portuguese Foundation for Science and Technology (grant numbers PTDC/SAU-GMG/098419/2008, UIDB/00709/2020, CEECINST/00016/2021/CP2828/CT0002, and 2020.04924.BD) and by Sidra Medicine-a member of the Qatar Foundation (grant number SDR400038). The authors declare no competing interests.

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