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促甲状腺激素释放激素(TRH)两种新类似物的体外和体内促甲状腺激素释放活性

In vitro and in vivo TSH releasing activity of two new analogues of TRH.

作者信息

Roussel J P, Tapia-Arancibia L, Astier H, Klingler W

出版信息

Acta Endocrinol (Copenh). 1987 Feb;114(2):314-20. doi: 10.1530/acta.0.1140314.

DOI:10.1530/acta.0.1140314
PMID:3103364
Abstract

The TSH releasing activity of two new analogues of TRH 'Pyr-(N3-Im-methyl)-His-Pro-NH-(n-amyl)' (I) and 'Pyr-His-Pro-(tyramine)' (II) was tested and compared with that of TRH in adult rats to test how structural modifications in the TRH molecule affect its biological activity: 1) in vitro in superfused pituitaries and 2) in vivo after ip injection, with measurement of TSH by RIA before and after addition of each secretagogue. Analogue I was found to be more potent than both TRH itself and Analogue II in stimulating TSH release: at 10 nmol/l in vitro, the ratio of induced to spontaneous release was 4.13 +/- 0.35, 2.98 +/- 0.20, and 1.19 +/- 0.17, respectively for each secretagogue, with a 50% effective dose of 6 X 10(-9) mol/l for Analogue I and 5 X 10(-8) mol/l for TRH. A similar order of potency in increasing plasma TSH (Analogue I greater than TRH greater than Analogue II) was found in vivo, as shown by dose-response curves. After a 4-day pre-treatment with TRH (2 X 100 micrograms/day) a similar TSH response to TRH and Analogue I (500 nmol/kg body weight) was observed. By contrast, the dose of Analogue II needed to obtain the same stimulatory effect on TSH release was twice as high. The biological activity of TRH appears to be more effectively increased by replacing an H atom by an amyl group in the C-terminal amide function of the proline residue of TRH than by a tyramyl group in the same residue.

摘要

测试了促甲状腺激素释放激素(TRH)的两种新类似物“Pyr-(N3-Im-甲基)-His-Pro-NH-(正戊基)”(I)和“Pyr-His-Pro-(酪胺)”(II)的促甲状腺激素释放活性,并与成年大鼠体内的TRH进行比较,以研究TRH分子结构修饰如何影响其生物活性:1)在体外对垂体进行灌流时;2)在腹腔注射后进行体内实验,在添加每种促分泌素前后通过放射免疫分析(RIA)测定促甲状腺激素(TSH)。结果发现类似物I在刺激TSH释放方面比TRH本身和类似物II都更有效:在体外浓度为10 nmol/l时,每种促分泌素诱导释放与自发释放的比率分别为4.13±0.35、2.98±0.20和1.19±0.17,类似物I的半数有效剂量为6×10⁻⁹ mol/l,TRH为5×10⁻⁸ mol/l。如剂量反应曲线所示,在体内也发现了类似的效力顺序(类似物I>TRH>类似物II)来增加血浆TSH。在用TRH(2×100微克/天)进行4天预处理后,观察到对TRH和类似物I(500 nmol/kg体重)的TSH反应相似。相比之下,获得对TSH释放相同刺激作用所需的类似物II剂量则是前者的两倍。将TRH脯氨酸残基C末端酰胺功能中的一个氢原子用戊基取代,似乎比用同一残基中的酪胺基更有效地提高了TRH的生物活性。

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