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TSPY expression is variably altered in transgenic mice with testicular feminization

  作者 Schubert, S; Kamino, K; Bohm, D; Adham, I; Engel, W; von Wasielewski, R; Moharregh-Khiabani, D; Mauceri, G; Vaske, B; Meinhardt, A; Schoner, A; Gonzalez-Fassrainer, D; Schmidtke, J  
  选自 期刊  Biology of Reproduction;  卷期  2008年79-1;  页码  125-133  
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[摘要]TSPY (testis-specific protein, Y-encoded) genes are expressed in premeiotic germ cells and round spermatids. The topology and timing of TSPY expression, and also its homology to members of the TTSN-family, suggest that TSPY is a proliferation factor for germ cells. There is also evidence for a role of TSPY in the aetiology of testis cancer. TSPY is a candidate for GBY, the elusive gonadoblastoma locus on the human Y chromosome, which is thought to predispose dysgenetic gonads of 46, XY sex-reversed females to develop gonadoblastoma. We have previously generated a TSPY transgenic mouse line (Tg(TSPY)9Jshm) that carries approximately 50 copies of the human TSPY gene on the mouse Y chromosome. in order to elucidate TSPY expression under complete androgen insensitivity and to investigate a possible role of TSPY in gonadal tumorigenesis, we have now generated sex-reversed TSPY transgenic Ar-Tfm mice hemizygous for the X-linked testicular feminization mutation (Ar-Tfm). We can show that the TSPY transcript is aberrantly spliced in the testes of TSPY-Ar-Tfm mice, and that TSPY expression is upregulated by androgen insensitivity in some but not all animals. TSPY transgenic mice showed significantly increased testes weights. In one TSPY transgenic Ar-Tfm animal, spermatogenesis proceeded beyond meiotic prophase. No tumors of germ cell origin were found in the testes of TSPY-Ar-Tfm mice. Five out of 46 TSPY transgenic Ar-Tfm mice, and 3 out of 31 age-related NMRI-Ar-Tfm controls developed Leydig cell tumors, whereas none of the age-matched Ar-Tfm mice (n = 44) on a wild type background were affected by Leydig cell tumorigenesis.

 
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