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雌激素对未成熟雏鸡视黄醇结合蛋白的调节作用:与核黄素载体蛋白的比较。

Estrogen modulation of retinol-binding protein in immature chicks: comparison with riboflavin carrier protein.

作者信息

DurgaKumari B, Adiga P R

出版信息

Mol Cell Endocrinol. 1986 Jul;46(2):121-30. doi: 10.1016/0303-7207(86)90090-0.

Abstract

The kinetics of estrogen (E) modulation of retinol-binding protein (RBP) production in the liver of immature chicks were compared with those governing de novo induction of riboflavin carrier protein (RCP) in the same tissue. A single dose of E markedly enhanced the plasma levels of RBP without any detectable lag period to reach peak value by 24 h and this was followed by a decline to attain the baseline by 4 days. There was no amplification of the response during secondary stimulation unlike the case with RCP induction. With multiple E administration, the 4-fold increased plasma RBP concentrations were sustained at a steady state during both primary and secondary stimulations, whereas concomitant RCP concentration progressively increased with each hormone administration and this response was further amplified during secondary stimulation. Unlike RCP induction, enhanced RBP accumulation was not strictly E dose dependent although a minimal threshold level of the steroid was required to elicit measurable response. Progesterone (P) could neither modulate nor substitute for E in enhancing plasma levels of either of the 2 proteins while the anti-estrogens, en- and zuclomifene citrate severely suppressed the production of both the proteins. RCP induction was completely inhibited by both alpha-amanitin and cycloheximide for prolonged periods while E-stimulated RBP production was affected only partially by alpha-amanitin. Likewise, cycloheximide inhibition of RBP accumulation followed a pattern similar to that of hepatic general protein synthesis.

摘要

将未成熟雏鸡肝脏中雌激素(E)对视黄醇结合蛋白(RBP)产生的调节动力学与同一组织中核黄素载体蛋白(RCP)从头诱导的动力学进行了比较。单次给予E可显著提高RBP的血浆水平,在24小时内达到峰值且无任何可检测的延迟期,随后在4天时下降至基线水平。与RCP诱导不同,二次刺激期间反应没有放大。多次给予E时,在初次和二次刺激期间,血浆RBP浓度增加4倍并维持在稳定状态,而伴随每次激素给药,RCP浓度逐渐增加,且该反应在二次刺激期间进一步放大。与RCP诱导不同,尽管需要最低阈值水平的类固醇来引发可测量的反应,但RBP积累的增强并不严格依赖于E剂量。孕酮(P)在提高这两种蛋白质的血浆水平方面既不能调节也不能替代E,而抗雌激素药物,即恩杂鲁胺和枸橼酸氯米芬则严重抑制这两种蛋白质的产生。α-鹅膏蕈碱和环己酰亚胺可长期完全抑制RCP的诱导,而E刺激的RBP产生仅部分受α-鹅膏蕈碱影响。同样,环己酰亚胺对RBP积累的抑制模式与肝脏总蛋白合成相似。

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