High levels of the extracellular matrix proteoglycan decorin are associated with inhibition of testicular function

M. Adam, H. F. Urbanski, V. T. Garyfallou, U. Welsch, F. M. Köhn, J. Ullrich Schwarzer, L. Strauss, M. Poutanen, A. Mayerhofer
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引用次数: 30

Abstract

Decorin (DCN), a component of the extracellular matrix of the peritubular wall and the interstitial areas of the human testis, can interact with growth factor (GF) signalling, thereby blocking downstream actions of GFs. In the present study the expression and regulation of DCN using both human testes and two experimental animal models, namely the rhesus monkey and mouse, were examined. DCN protein was present in peritubular and interstitial areas of adult human and monkey testes, while it was almost undetectable in adult wild type mice. Interestingly, the levels and sites of testicular DCN expression in the monkeys were inversely correlated with testicular maturation markers. A strong DCN expression associated with the abundant connective tissue of the interstitial areas in the postnatal through pre-pubertal phases was observed. In adult and old monkeys the DCN pattern was similar to the one in normal human testes, presenting strong expression at the peritubular region. In the testes of both infertile men and in a mouse model of inflammation associated infertility (aromatase-overexpressing transgenic mice), the fibrotic changes and increased numbers of tumour necrosis factor (TNF)-α-producing immune cells were shown to be associated with increased production of DCN. Furthermore, studies with human testicular peritubular cells isolated from fibrotic testis indicated that TNF-α significantly increased DCN production. The data, thus, show that an increased DCN level is associated with impaired testicular function, supporting our hypothesis that DCN interferes with paracrine signalling of the testis in health and disease.

Abstract Image

高水平的细胞外基质蛋白聚糖decorin与睾丸功能的抑制有关
Decorin (DCN)是人类睾丸小管周围壁和间质区细胞外基质的一种成分,可与生长因子(GF)信号相互作用,从而阻断生长因子的下游作用。本研究用人类睾丸和恒河猴和小鼠两种实验动物模型检测了DCN的表达和调控。DCN蛋白存在于成人和猴子睾丸的小管周围和间质区域,而在成年野生型小鼠中几乎检测不到。有趣的是,猴子睾丸DCN的表达水平和部位与睾丸成熟标志物呈负相关。在出生后至青春期前,观察到与间质区丰富结缔组织相关的强DCN表达。在成年和老年猴子中,DCN模式与正常人类睾丸相似,在小管周围区域表现出强烈的表达。在不育男性和炎症相关不育小鼠模型(芳香化酶过表达转基因小鼠)的睾丸中,纤维化改变和产生肿瘤坏死因子(TNF)-α-的免疫细胞数量增加被证明与DCN的产生增加有关。此外,对从纤维化睾丸中分离的人睾丸小管周围细胞的研究表明,TNF-α显著增加DCN的产生。因此,这些数据表明,DCN水平升高与睾丸功能受损有关,支持了我们的假设,即DCN在健康和疾病中干扰睾丸的旁分泌信号。
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6-12 weeks
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