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Sequential testicular atrophy involves changes in cellular proliferation and apoptosis associated with variations in aromatase P450 expression levels in Irs‐2‐deficient mice
Authors:Leonardo Catalano‐Iniesta,Virginia S  nchez‐Robledo,Maria Carmen Iglesias‐Osma,Maria Jos   Garcí  a‐Barrado,Marta Carretero‐Hern  ndez,Enrique J. Blanco,Teresa Vicente‐Garcí  a,Deborah Jane Burks,Jos   Carretero
Affiliation:Leonardo Catalano‐Iniesta,Virginia Sánchez‐Robledo,Maria Carmen Iglesias‐Osma,Maria José García‐Barrado,Marta Carretero‐Hernández,Enrique J. Blanco,Teresa Vicente‐García,Deborah Jane Burks,José Carretero
Abstract:
Insulin receptor substrate 2 (Irs‐2) is an intracellular protein susceptible to phosphorylation after activation of the insulin receptor. Its suppression affects testis development and its absence induces peripheral resistance to insulin. The aim of this study was to identify changes induced by the deletion of Irs‐2 in the testicular structure and by the altered expression of cytochrome P450 aromatase, a protein necessary for the development and maturation of germ cells. Adult knockout (KO) mice (Irs‐2?/?, 6 and 12 weeks old) and age‐matched wild‐type (WT) mice were used in this study. Immunohistochemistry and Western blot analyses were performed to study proliferation (PCNA), apoptosis (active caspase‐3) and P450 aromatase expression in testicular histological sections. Deletion of Irs‐2 decreased the number of epithelial cells in the seminiferous tubule and rete testis. Aberrant cells were frequently detected in the epithelia of Irs‐2?/? mice, accompanied by variations in spermatogonia, which were shown to exhibit small hyperchromatic nuclei as well as polynuclear and anuclear structures. The amount of cell proliferation was significantly lower in Irs‐2?/? mice than in WT mice, whereas apoptotic processes were more common in Irs‐2?/? mice. Aromatase P450 reactivity was higher in 6‐week‐old KO mice than in WT mice of the same age and was even higher at 12 weeks. Our results suggest that Irs‐2 is a key element in spermatogenesis because silencing Irs‐2 induces the sequential development of testicular atrophy. The effects are observed mainly in germ cells present in the seminiferous tubule, which may be due to changes in cytochrome P450 aromatase expression.
Keywords:apoptosis  aromatase  cellular proliferation  insulin receptor substrate 2  testis
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