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实验性糖尿病对去卵巢大鼠子宫自发收缩、前列腺素分泌及标记花生四烯酸代谢的影响。雌二醇的作用。

Effects of experimental diabetes on spontaneous contractions, on the output of prostaglandins and on the metabolism of labelled arachidonic acid, in uteri isolated from ovariectomized rats. Influences of estradiol.

作者信息

Franchi A M, Chaud M, Gonzalez E T, Gimeno M A, Gimeno A L

机构信息

Centro de Estudios Farmacológicos y de Principios Naturales, Universidad de Buenos Aires.

出版信息

Prostaglandins. 1988 Feb;35(2):191-205. doi: 10.1016/0090-6980(88)90087-1.

Abstract

Spontaneous changes in isometric developed tension (IDT) as a function of time after isolation (contractile constancy) in uteri from control-castrated and castrated chronic streptozotocin-diabetic rats, were explored. The effects of injecting 17-beta estradiol (Eo) were also studied. No differences in the minor changes of contractile constancy, between control and diabetic preparations, during a period of 60 min, were detected, whereas uteri from non-diabetic Eo injected animals (0.5 + 1.0 ug, prior to sacrifice), exhibited a profound reduction of IDT, significantly greater than in tissues obtained from Eo injected-diabetic rats. Moreover, basal generation and outputs into the suspending solution of prostaglandins (PGs) E1, E2 and F2 alpha, were explored in the same groups, at 60 min following tissue isolation. The basal outputs of these three PGs were similar in castrated control rats, but preparations from castrated-diabetics released significantly more PGE1. The administration of Eo to castrated-diabetics, failed to alter the releases of the three PGs explored. In addition, the metabolism of labelled arachidonic acid (AA) into different prostanoids (6-keto-PGF1, PGF2, PGE2 and thromboxane B2-TXB2), was also investigated. The non-diabetic spayed rat uterus converted AA into these four prostanoids, the transformation into 6-keto-PGF1 alpha (as an index of PGI2 formation) being the most prominent. In preparations from diabetic rats the formation) being the most prominent. In preparations from diabetic rats the formation of 6-keto-PGF1 alpha, PGF2 alpha and PGE2, was significantly smaller than in controls, whereas a greater % of TXB2 formation (as an index of TXA2), was detected. On the other hand uterine preparations from non-diabetic spayed rats injected with Eo formed less 6-keto-PGF1 alpha and PGE2 and similar amounts of PGF2 alpha or of TXB2 from AA, than Eo injected controls, whereas uteri from castrated diabetic animals injected with Eo, formed a similar % of 6-keto-PGF1 alpha, PGF2 alpha and PGE2 from AA, than tissue preparations from non-estrogenized controls. However, the enhanced transformation of the labelled fatty acid precursor (AA) into TXB2 in the diabetic group, was significantly reduced by the steroid. The role of the augmented generation and release of PGE1 in uteri from diabetic rats is discussed in terms of precedents indicating the relevance of PGs type E supporting rat uterine motility. In addition the influence of Eo is attractive, because its reducing effect on TX production, in diabetes, a disease known to be accompanied by enhanced synthesis of vasoconstrictor and platelet aggregation TXA2, and by frequent obstructive circulat

摘要

研究了来自对照去势和去势慢性链脲佐菌素诱导糖尿病大鼠子宫的等长收缩张力(IDT)在离体后随时间的自发变化(收缩稳定性)。还研究了注射17-β雌二醇(E₂)的影响。在60分钟期间,未检测到对照和糖尿病制剂之间收缩稳定性的微小变化有差异,而在处死前注射非糖尿病E₂的动物(0.5 + 1.0微克)的子宫,IDT显著降低,明显大于注射E₂的糖尿病大鼠组织。此外,在组织离体60分钟后,对同一组动物中前列腺素(PGs)E₁、E₂和F₂α的基础生成及向悬浮液中的释放进行了研究。这三种PGs的基础释放在去势对照大鼠中相似,但去势糖尿病大鼠的制剂释放的PGE₁明显更多。给去势糖尿病大鼠注射E₂未能改变所研究的三种PGs的释放。此外,还研究了标记的花生四烯酸(AA)向不同前列腺素(6-酮-PGF₁α、PGF₂α、PGE₂和血栓素B₂ - TXB₂)的代谢。非糖尿病去卵巢大鼠子宫将AA转化为这四种前列腺素,转化为6-酮-PGF₁α(作为PGI₂形成的指标)最为显著。在糖尿病大鼠的制剂中,6-酮-PGF₁α、PGF₂α和PGE₂的形成明显小于对照组,而检测到更高百分比的TXB₂形成(作为TXA₂的指标)。另一方面,注射E₂的非糖尿病去卵巢大鼠子宫从AA形成的6-酮-PGF₁α和PGE₂较少,PGF₂α或TXB₂的量与注射E₂的对照组相似,而注射E₂的去势糖尿病动物子宫从AA形成的6-酮-PGF₁α、PGF₂α和PGE₂的百分比与未用雌激素处理的对照组组织制剂相似。然而,类固醇显著降低了糖尿病组中标记脂肪酸前体(AA)向TXB₂的增强转化。根据表明E型PG支持大鼠子宫运动相关性的先例,讨论了糖尿病大鼠子宫中PGE₁生成和释放增加的作用。此外,E₂的影响很有吸引力,因为它对TX产生的降低作用,在糖尿病这种已知伴有血管收缩剂和血小板聚集TXA₂合成增强以及频繁阻塞性循环的疾病中。

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