María Cecilia Lardone, Marina Díaz-Fontdevila, Eliana Ortiz, Germán Iñiguez, Pamela Inostroza, Cristóbal Espinoza, Mauricio Ebensperger, Kristian Almstrup, Andrea Castro
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One hundred and eleven oligozoospermic (cases) and 258 men with normal sperm concentration (controls) were genotyped for five LIN28B SNPs (rs7759938, rs395962, rs314268, rs314277 and rs314280). The abundance of the LIN28B transcript, let-7a and let-7c miRNAs were measured by qRT-PCR in RNA isolated from purified sperm. Serum blood samples were analysed for reproductive hormones. Lower abundance of the LIN28B transcript and higher expression of let-7c were observed in cases (P < 0.001). Furthermore, rs395962_T was associated with a reduced abundance of the LIN28B transcript in cases (dominant: P = 0.032). On the other side, we observed a positive association of rs314277_A (Additive: P = 0.024), rs7759938_C (dominant: P = 0.025) and rs314280_A (dominant: P = 0.024) with total testosterone levels in cases. The decreased transcript abundance of LIN28B in sperm of idiopathic oligozoospermic men and its association with SNPs known to affect the onset of puberty and total testosterone levels suggests a role for LIN28B in the primary impairment of spermatogenesis through its expression in early germ cells or regulating the testicular biosynthesis of testosterone at a central level. 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引用次数: 0
摘要
LIN28B是一种rna结合蛋白,通过与let-7 mirna的相互作用,作为参与发育时间和自我更新的基因的转录后调节剂。大规模的基因组研究表明,LIN28B的snp与男性青春期时间有关。此外,青春期延迟的发生与精液质量下降有关。因此,我们旨在研究特发性少精子男性中青春期相关的LIN28B snp与精液参数、生殖激素以及LIN28B/Let-7轴表达的关系。111例少精子症患者和258例精子浓度正常的男性(对照)对5个LIN28B snp (rs7759938、rs395962、rs314268、rs314277和rs314280)进行基因分型。用qRT-PCR方法检测精精子分离RNA中LIN28B转录本、let-7a和let-7c mirna的丰度。血清血液样本进行生殖激素分析。LIN28B转录物丰度较低,let-7c表达较高(p
LIN 28B expression is downregulated in mature spermatozoa of oligozoospermic men and associates with genetic variants previously linked to pubertal onset.
LIN28B is an RNA-binding protein that acts as a post-transcriptional regulator of genes involved in developmental timing and self-renewal through its interaction with let-7 miRNAs. Large-scale genomic studies have strongly implicated SNPs in LIN28B with male puberty timing. In addition, the occurrence of late puberty is linked to diminished semen quality in adult life. Therefore, we aimed to study the association of puberty-linked LIN28B genetic variants with semen parameters, reproductive hormones and the spermatozoa expression of the LIN28B/Let-7 axis in idiopathic oligozoospermic men. One hundred and eleven oligozoospermic (cases) and 258 men with normal sperm concentration (controls) were genotyped for five LIN28B SNPs (rs7759938, rs395962, rs314268, rs314277 and rs314280). The abundance of the LIN28B transcript, let-7a and let-7c miRNAs were measured by qRT-PCR in RNA isolated from purified sperm. Serum blood samples were analysed for reproductive hormones. Lower abundance of the LIN28B transcript and higher expression of let-7c were observed in cases (P < 0.001). Furthermore, rs395962_T was associated with a reduced abundance of the LIN28B transcript in cases (dominant: P = 0.032). On the other side, we observed a positive association of rs314277_A (Additive: P = 0.024), rs7759938_C (dominant: P = 0.025) and rs314280_A (dominant: P = 0.024) with total testosterone levels in cases. The decreased transcript abundance of LIN28B in sperm of idiopathic oligozoospermic men and its association with SNPs known to affect the onset of puberty and total testosterone levels suggests a role for LIN28B in the primary impairment of spermatogenesis through its expression in early germ cells or regulating the testicular biosynthesis of testosterone at a central level. Therefore, our results provide a potential mechanistic link between the regulation of pubertal timing and adult testicular function.
期刊介绍:
Endocrine Connections publishes original quality research and reviews in all areas of endocrinology, including papers that deal with non-classical tissues as source or targets of hormones and endocrine papers that have relevance to endocrine-related and intersecting disciplines and the wider biomedical community.
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