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大鼠发育中的大脑皮层和小脑中三碘甲状腺原氨酸的产生率和周转率。对甲状腺功能减退的反应。

Production rates and turnover of triiodothyronine in rat-developing cerebral cortex and cerebellum. Responses to hypothyroidism.

作者信息

Silva J E, Matthews P S

出版信息

J Clin Invest. 1984 Sep;74(3):1035-49. doi: 10.1172/JCI111471.

Abstract

Local 5'-deiodination of serum thyroxine (T4) is the main source of triiodothyronine (T3) for the brain. Since we noted in previous studies that the cerebral cortex of neonatal rats tolerated marked reductions in serum T4 without biochemical hypothyroidism, we examined the in vivo T4 and T3 metabolism in that tissue and in the cerebellum of euthyroid and hypothyroid 2-wk-old rats. We also assessed the contribution of enhanced tissue T4 to T3 conversion and decreased T3 removal from the tissues to the T3 homeostasis in hypothyroid brain. Congenital and neonatal hypothyroidism was induced by adding methimazole to the drinking water. Serum, cerebral cortex (Cx), cerebellum (Cm), liver (L) and kidney (R) concentrations of 125I-T4, 125I-T3(T4), and 131I-T3 were measured at various times after injecting 125I-T4 and 131I-T3. The rate of T3 removal from the tissues was measured after injecting an excess of anti-T3-antibody to rats previously injected with tracer T3. In euthyroid rats, fractional turnover rates of T3 per hour were: Cx, 0.26 +/- 0.02 (SE); Cm, 0.20 +/- 0.02; L, 0.98 +/- 0.07; R, 0.97 +/- 0.12; and the calculated unidirectional plasma T3 clearance by these tissues were, in milliliters per gram per hour: Cx = 0.38, Cm = 0.32, L = 5.0, and R = 5.6. In hypothyroidism, the fractional removal rates and clearances were reduced in all tissues, in cortex and cerebellum by 70%, and in liver and kidney ranging from 30 to 50%. While greater than 80% of the 125I-T3(T4) in the brain tissues of euthyroid rats was locally produced, in hypothyroid cerebral cortex and cerebellum the integrated concentrations of 125I-T3(T4) were 2.7- and 1.5-fold greater than in euthyroid rats. In the Cx, this response resulted from an approximately sixfold increase in fractional conversion and an approximately fourfold decrease in T3 removal rate hampered by a decreased uptake of T4 from plasma, whereas in Cm the response resulted only from the reduced T3 removal rate. In euthyroid rats, the calculated production rate of T3 in nanograms per gram per hour by the Cx was 0.96 and 0.89 by the Cm, which on a per organ basis equals 15 and 2%, respectively, of the extrathyroidal production rate as assessed in the body pool exchanging with plasma. Several conclusions can be drawn: Production of T3 by developing brain is a very active process in agreement with the need of thyroid hormones during this period. (b) The brain-plasma exchange of T3 is slow compared with that of L or R. (c) This, along with the active local production, explains the predominant role of the latter as a source of T3 for the brain. (d) In hypothyroidism, the Cx is protected by an increase in the efficiency of T4 to T3 conversion and a prolong residence time of T3 in the tissue, whereas the Cm is protected only by the latter. Because of the large fraction of the T3 produced locally and the active turnover rate of T3 in the brain, reductions in T3 removal rate are of utmost importance for T3 homeostasis in these tissues.

摘要

血清甲状腺素(T4)的局部5'-脱碘是大脑中三碘甲状腺原氨酸(T3)的主要来源。由于我们在先前的研究中注意到,新生大鼠的大脑皮质在没有生化性甲状腺功能减退的情况下能够耐受血清T4的显著降低,因此我们研究了甲状腺功能正常和甲状腺功能减退的2周龄大鼠的该组织以及小脑中T4和T3的体内代谢情况。我们还评估了甲状腺功能减退大脑中组织T4向T3转化增强以及T3从组织中清除减少对T3稳态的影响。通过在饮用水中添加甲巯咪唑诱导先天性和新生儿甲状腺功能减退。在注射125I-T4和131I-T3后的不同时间测量血清、大脑皮质(Cx)、小脑(Cm)、肝脏(L)和肾脏(R)中125I-T4、125I-T3(T4)和131I-T3的浓度。在给预先注射示踪剂T3的大鼠注射过量抗T3抗体后,测量T3从组织中的清除率。在甲状腺功能正常的大鼠中,每小时T3的分数周转率为:Cx,0.26±0.02(SE);Cm,0.20±0.02;L,0.98±0.07;R,0.97±0.12;这些组织计算得到的单向血浆T3清除率,以每克每小时毫升数计为:Cx = 0.38,Cm = 0.32,L = 5.0,R = 5.6。在甲状腺功能减退时,所有组织中的分数清除率和清除量均降低,皮质和小脑中降低70%,肝脏和肾脏中降低30%至50%。虽然甲状腺功能正常的大鼠脑组织中超过80%的125I-T3(T4)是局部产生的,但在甲状腺功能减退的大脑皮质和小脑中,125I-T3(T4)的综合浓度比甲状腺功能正常的大鼠高2.7倍和1.5倍。在Cx中,这种反应是由于分数转化率增加约6倍以及T3清除率降低约4倍,这是由于血浆中T4摄取减少所致,而在Cm中,这种反应仅由T3清除率降低引起。在甲状腺功能正常的大鼠中,Cx每克每小时计算得到的T3产生率为0.96,Cm为0.89,以每个器官计算,分别相当于与血浆交换的体内池中评估的甲状腺外产生率的15%和2%。可以得出几个结论:(a)发育中的大脑产生T3是一个非常活跃的过程,这与该时期对甲状腺激素的需求一致。(b)与肝脏或肾脏相比,大脑与血浆之间的T3交换较慢。(c)这一点,连同活跃的局部产生,解释了后者作为大脑T3来源的主要作用。(d)在甲状腺功能减退时,Cx通过T4向T3转化效率的提高和T3在组织中的停留时间延长而得到保护,而Cm仅通过后者得到保护。由于大脑中局部产生的T3占很大比例且T3的周转率活跃,T3清除率的降低对这些组织中的T3稳态至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4bcf/425263/ecc00eebb6ef/jcinvest00135-0378-a.jpg

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