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短期禁食和长期食物限制期间大鼠肝脏中甲状腺激素葡萄糖醛酸化酶的性别特异性变化。

Gender-specific changes in thyroid hormone-glucuronidating enzymes in rat liver during short-term fasting and long-term food restriction.

作者信息

Visser T J, van Haasteren G A, Linkels E, Kaptein E, van Toor H, de Greef W J

机构信息

Department of Internal Medicine III, Erasmus University Medical School, Rotterdam, The Netherlands.

出版信息

Eur J Endocrinol. 1996 Oct;135(4):489-97. doi: 10.1530/eje.0.1350489.

Abstract

Glucuronidation is a major pathway of thyroid hormone metabolism in rats, involving at least three different hepatic UDP-glucuronyltransferases (UGTs): bilirubin UGT, phenol UGT and androsterone UGT. We have studied the effects of short-term (3 days) fasting and long-term (3 weeks) food restriction to one-third of normal intake (FR33) on hepatic UGT activities for thyroxine (T4), triiodothyronine (T3), bilirubin and androsterone in male and female Wistar rats with either a functional (high activity, HA) or a defective (low activity, LA) androsterone UGT gene. Because food deprivation is known to induce centrally mediated hypothyroidism in rats, results were compared with those obtained in methimazole (MMI)-induced hypothyroid rats. Both fasting and FR33 produced largely parallel increases in T4 and bilirubin UGT activities. These effects were greater in males than in females, and were reproduced in MMI-treated rats. In male and female HA rats, fasting induced insignificant increases in T3 UGT activity and had no effect on androsterone UGT activity. In male HA rats, FR33 was associated with an increase in T3 UGT activity, while androsterone UGT activity showed little change. However, in female HA rats both T3 and androsterone UGT activities were markedly decreased by FR33. Triiodothyronine UGT activity in LA rats was strongly decreased compared with HA rats, but was not further decreased by FR33 in female LA rats, supporting the importance of androsterone UGT for T3 glucuronidation. These results demonstrate different sex-dependent effects of food deprivation on hepatic T4 and T3 glucuronidation that are associated with changes in the expression of bilirubin UGT and androsterone UGT, respectively. For the increased T4 and bilirubin UGT activities at least, these effects appear to be mediated by the hypothyroid state of the (semi)starved animals.

摘要

葡糖醛酸化是大鼠甲状腺激素代谢的主要途径,涉及至少三种不同的肝脏尿苷二磷酸葡糖醛酸基转移酶(UGTs):胆红素UGT、苯酚UGT和雄甾酮UGT。我们研究了短期(3天)禁食和长期(3周)食物限制至正常摄入量的三分之一(FR33)对具有功能性(高活性,HA)或缺陷性(低活性,LA)雄甾酮UGT基因的雄性和雌性Wistar大鼠肝脏中甲状腺素(T4)、三碘甲状腺原氨酸(T3)、胆红素和雄甾酮的UGT活性的影响。由于已知食物剥夺会在大鼠中诱发中枢介导的甲状腺功能减退,因此将结果与在甲巯咪唑(MMI)诱导的甲状腺功能减退大鼠中获得的结果进行了比较。禁食和FR33均使T4和胆红素UGT活性在很大程度上平行增加。这些作用在雄性中比在雌性中更大,并且在MMI处理的大鼠中也出现。在雄性和雌性HA大鼠中,禁食使T3 UGT活性增加不显著,并且对雄甾酮UGT活性没有影响。在雄性HA大鼠中,FR33与T3 UGT活性增加有关,而雄甾酮UGT活性变化不大。然而,在雌性HA大鼠中,FR33使T3和雄甾酮UGT活性均显著降低。与HA大鼠相比,LA大鼠中的T3 UGT活性强烈降低,但在雌性LA大鼠中未因FR33而进一步降低,这支持了雄甾酮UGT对T3葡糖醛酸化的重要性。这些结果表明,食物剥夺对肝脏T4和T3葡糖醛酸化具有不同的性别依赖性影响,分别与胆红素UGT和雄甾酮UGT表达的变化有关。至少对于增加的T4和胆红素UGT活性而言,这些影响似乎是由(半)饥饿动物的甲状腺功能减退状态介导的。

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