Cerván-Martín Miriam, Bossini-Castillo Lara, Rivera-Egea Rocío, Garrido Nicolás, Luján Saturnino, Romeu Gema, Santos-Ribeiro Samuel, Castilla José A, Gonzalvo M Carmen, Clavero Ana, Vicente F Javier, Guzmán-Jiménez Andrea, Costa Cláudia, Llinares-Burguet Inés, Khantham Chiranan, Burgos Miguel, Barrionuevo Francisco J, Jiménez Rafael, Sánchez-Curbelo Josvany, López-Rodrigo Olga, Peraza M Fernanda, Pereira-Caetano Iris, Marques Patricia I, Carvalho Filipa, Barros Alberto, Bassas Lluís, Seixas Susana, Gonçalves João, Larriba Sara, Lopes Alexandra M, Palomino-Morales Rogelio J, Carmona F David
Departamento de Genética e Instituto de Biotecnología, Universidad de Granada, 18016 Granada, Spain.
Instituto de Investigación Biosanitaria ibs.GRANADA, 18012 Granada, Spain.
J Pers Med. 2020 Dec 29;11(1):22. doi: 10.3390/jpm11010022.
Infertility is a growing concern in developed societies. Two extreme phenotypes of male infertility are non-obstructive azoospermia (NOA) and severe oligospermia (SO), which are characterized by severe spermatogenic failure (SpF). We designed a genetic association study comprising 725 Iberian infertile men as a consequence of SpF and 1058 unaffected controls to evaluate whether five single-nucleotide polymorphisms (SNPs), previously associated with reduced fertility in Hutterites, are also involved in the genetic susceptibility to idiopathic SpF and specific clinical entities. A significant difference in the allele frequencies of -rs7174015 was observed under the recessive model between the NOA group and both the control group ( = 0.0226, OR = 1.33) and the SO group ( = 0.0048, OR = 1.78). Other genetic associations for -rs12870438 and -rs7867029 with SO and between -rs10966811 and testicular sperm extraction (TESE) success in the context of NOA were observed. In silico analysis of functional annotations demonstrated cis-eQTL effects of such SNPs likely due to the modification of binding motif sites for relevant transcription factors of the spermatogenic process. The findings reported here shed light on the molecular mechanisms leading to severe phenotypes of idiopathic male infertility, and may help to better understand the contribution of the common genetic variation to the development of these conditions.
在发达社会中,不孕问题日益受到关注。男性不育的两种极端表型是非梗阻性无精子症(NOA)和严重少精子症(SO),其特征为严重的生精功能衰竭(SpF)。我们设计了一项基因关联研究,纳入725名因SpF导致不育的伊比利亚男性以及1058名未受影响的对照者,以评估此前在哈特派人群中发现的与生育力降低相关的5个单核苷酸多态性(SNP)是否也与特发性SpF及特定临床实体的遗传易感性有关。在隐性模型下,观察到NOA组与对照组(P = 0.0226,OR = 1.33)以及SO组(P = 0.0048,OR = 1.78)之间,-rs7174015的等位基因频率存在显著差异。还观察到-rs12870438和-rs7867029与SO之间以及-rs10966811与NOA背景下的睾丸精子提取(TESE)成功率之间存在其他基因关联。对功能注释的电子分析表明,这些SNP可能通过改变生精过程相关转录因子的结合基序位点而产生顺式eQTL效应。本文报道的研究结果揭示了导致特发性男性不育严重表型的分子机制,可能有助于更好地理解常见基因变异在这些疾病发生发展中的作用。
