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睾丸活检和精液样本的分子分析作为非梗阻性无精子症睾丸组织病理学分析的补充方法。

Molecular analysis of testis biopsy and semen pellet as complementary methods with histopathological analysis of testis in non-obstructive azoospermia.

作者信息

Eghbali Maryam, Sadeghi Mohammad Reza, Lakpour Niknam, Edalatkhah Hale, Zeraati Hojjat, Soltanghoraee Haleh, Akhondi Mohammad Mehdi, Hashemi S Behnam, Modarressi Mohammad Hossein

机构信息

Department of Medical Genetics, School of Medicine, Tehran University of Medical Sciences, Poursina Ave, 16 Azar St. Keshavarz BLVD, Tehran, Iran, 1417613151.

出版信息

J Assist Reprod Genet. 2014 Jun;31(6):707-15. doi: 10.1007/s10815-014-0220-5. Epub 2014 Apr 12.

Abstract

PURPOSE

Non-obstructive azoospermia (NOA) is one the many causes of male infertility (10 %) resulting from testicular failure. Multiple testicular biopsies fail to find mature sperm in at least 50 % of cases Therefore; hunting for sensitive and specific biomarkers of spermatogenesis that could better determine the fertility status in NOA can lead to improved management of male infertility. Therefore, we evaluated sperm production through analyses of germ cell-specific transcripts (DAZ, TSPY1, SPTRX3 and SPTRX1) in semen and testicular biopsies of men with azoospermia.

METHODS

We collected semen (N=83) and testis biopsies (N=31) from men with non-obstructive azoospermia. We later extracted RNA and synthesized cDNA using washed semen precipitate and testicular tissues. We also performed semi-nested PCR with designed specific primers. Using H&E method, an expert pathologist performed the histopathological evaluation. Having categorized the patients into three groups based on histopathological results, we calculated the agreement between molecular results of semen and tissues with histopathological findings for each patient using Kappa statistical test.

RESULTS

Molecular findings of precipitated semen and testicular tissues were in disagreement with histopathological results in most cases. Molecular analysis of testis biopsies showed significant difference (Kappa coefficient=0.009, P value=0.894) with histopathological results; TSPY1, DAZ, SPTRX3 and SPTRX1 were respectively detected in 94 %, 94 %, 17.6 % and 52.9 % of men diagnosed with germ cell aplasia.

CONCLUSIONS

Molecular analysis of semen does not provide sufficient sensitivity and specificity to be used as a screening test at the present time, but it is a useful adjunct to histopathological methods in men with NOA. Spermatid/sperm specific transcripts indicated the possibility to find mature sperm following repeated multiple testicular sperm extraction (TESE) or microdisection TESE (mTESE).

摘要

目的

非梗阻性无精子症(NOA)是睾丸功能衰竭导致男性不育的众多原因之一(占10%)。在至少50%的病例中,多次睾丸活检未能找到成熟精子。因此,寻找能够更好地确定NOA患者生育状况的敏感且特异的生精生物标志物,有助于改善男性不育的治疗。因此,我们通过分析无精子症男性精液和睾丸活检组织中生殖细胞特异性转录本(DAZ、TSPY1、SPTRX3和SPTRX1)来评估精子生成情况。

方法

我们收集了非梗阻性无精子症男性的精液(n = 83份)和睾丸活检组织(n = 31份)。随后,我们使用洗涤后的精液沉淀和睾丸组织提取RNA并合成cDNA。我们还使用设计好的特异性引物进行半巢式PCR。一位专业病理学家采用苏木精-伊红(H&E)方法进行组织病理学评估。根据组织病理学结果将患者分为三组后,我们使用Kappa统计检验计算每位患者精液和组织的分子结果与组织病理学结果之间的一致性。

结果

在大多数情况下,精液沉淀和睾丸组织的分子结果与组织病理学结果不一致。睾丸活检组织的分子分析显示与组织病理学结果存在显著差异(Kappa系数 = 0.009,P值 = 0.894);在诊断为生殖细胞发育不全的男性中,分别有94%、94%、17.6%和52.9%检测到TSPY1、DAZ、SPTRX3和SPTRX1。

结论

目前,精液的分子分析作为筛查试验的敏感性和特异性不足,但对于NOA男性而言,它是组织病理学方法的有用辅助手段。精子细胞/精子特异性转录本表明,在多次重复睾丸精子提取(TESE)或显微切割TESE(mTESE)后有可能找到成熟精子。

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