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小鼠磺基转移酶(Sults)性别特异性调控的机制。

Mechanisms of gender-specific regulation of mouse sulfotransferases (Sults).

作者信息

Alnouti Yazen, Klaassen Curtis D

机构信息

Department of Pharmaceutical Sciences, University of Nebraska Medical Center, Omaha, NE, USA.

出版信息

Xenobiotica. 2011 Mar;41(3):187-97. doi: 10.3109/00498254.2010.535923. Epub 2010 Nov 23.

Abstract
  1. Marked gender differences in the expression of sulfotransferases (Sults) are known to exist in several species including rats, mice and hamsters. However, the mechanism for this gender difference is not known. Therefore, in the present study, it was determined whether sex and/or growth hormone (GH) are responsible for the gender difference in the expression of Sults using gonadectomized (GNX), hypophysectomized (HX) and GH-releasing hormone receptor-deficient little (lit/lit) mouse models. 2. Sult1a1 and Papss2 in liver and kidney, and Sult1d1 in liver are female-predominant in mice because of suppressive effects of both androgens and male-pattern GH secretion. Sult2a1/a2 is the most markedly female-predominant Sult in mouse liver due to suppressive effects of androgens and male-pattern GH secretion, as well as stimulatory effects by estrogens and female-pattern GH secretion. Sult3a1 is female-predominant in mouse liver due to suppressive effects of androgens as well as stimulatory effects of estrogens and female-pattern GH secretion. Sult1c1 expression is male-predominant in mouse liver and kidney because of stimulatory effects of androgens in males. Sult4a1 expression is female-predominant in mouse brain due to stimulatory effects of estrogens. 3. In conclusion, gender-divergent Sults are mostly female-predominant and Sult1c1 is the only male-dominant Sult. The gender differences in expression of various mouse Sults are influenced by various mechanisms involving sex and/or GHs.
摘要
  1. 已知在包括大鼠、小鼠和仓鼠在内的多个物种中,硫酸转移酶(Sults)的表达存在明显的性别差异。然而,这种性别差异的机制尚不清楚。因此,在本研究中,使用去性腺(GNX)、垂体切除(HX)和生长激素释放激素受体缺陷型矮小(lit/lit)小鼠模型,确定性别和/或生长激素(GH)是否是导致Sults表达性别差异的原因。2. 由于雄激素和雄性模式生长激素分泌的抑制作用,小鼠肝脏和肾脏中的Sult1a1和Papss2以及肝脏中的Sult1d1以雌性为主。由于雄激素和雄性模式生长激素分泌的抑制作用以及雌激素和雌性模式生长激素分泌的刺激作用,Sult2a1/a2是小鼠肝脏中最明显以雌性为主的硫酸转移酶。由于雄激素的抑制作用以及雌激素和雌性模式生长激素分泌的刺激作用,Sult3a1在小鼠肝脏中以雌性为主。由于雄性中雄激素的刺激作用,Sult1c1在小鼠肝脏和肾脏中的表达以雄性为主。由于雌激素的刺激作用,Sult4a1在小鼠大脑中的表达以雌性为主。3. 总之,不同性别的硫酸转移酶大多以雌性为主,Sult1c1是唯一以雄性为主的硫酸转移酶。各种小鼠硫酸转移酶表达的性别差异受涉及性别和/或生长激素的多种机制影响。

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