首页> 外文期刊>Medical hypotheses >Estrogen agonists/antagonists may down-regulate growth hormone signaling in hepatocytes-An explanation for their impact on IGF-I, IGFBP-1, and lipoprotein(a).
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Estrogen agonists/antagonists may down-regulate growth hormone signaling in hepatocytes-An explanation for their impact on IGF-I, IGFBP-1, and lipoprotein(a).

机译:雌激素激动剂/拮抗剂可能会下调肝细胞中的生长激素信号传导-解释其对IGF-1,IGFBP-1和脂蛋白的影响(a)。

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摘要

Estrogen agonists/antagonists, when administered orally, exert a range of effects on hepatic function, some of which are potentially protective. These effects include reduced synthesis of IGF-I and apolipoprotein(a), and increased synthesis of IGFBP-1-shifts which arguably could decrease risk for vascular disease and certain cancers. These effects are diametrically opposite to those of growth hormone (GH), which boosts hepatic production of IGF-I and apolipoprotein(a), while suppressing that of IGFBP-1. Thus, a parsimonious explanation of these phenomena is that oral estrogen blunts the efficiency of GH signaling in the liver. Oral androgenic progestins may have the reverse effect. It may be of particular value to determine whether certain estrogen agonists/antagonists can exert relatively 'hepatospecific' activity when administered orally-thus enabling down-regulation of systemic IGF-I activity and of lipoprotein(a), without however inducing a significant increase in systemic estrogen activity. Preliminary evidence suggests that flax lignans and perhaps other phytoestrogens may have potential in this regard.
机译:口服雌激素激动剂/拮抗剂对肝功能产生一系列影响,其中一些具有潜在的保护作用。这些作用包括减少IGF-1和载脂蛋白(a)的合成,以及增加IGFBP-1转移的合成,可以减少血管疾病和某些癌症的风险。这些作用与生长激素(GH)截然相反,后者可抑制肝脏IGF-1和载脂蛋白(a)的肝产量。因此,这些现象的简化解释是口服雌激素使肝脏中GH信号传导的效率减弱。口服雄激素孕激素可能有相反的作用。确定某些雌激素激动剂/拮抗剂在口服时是否可以发挥相对的“肝特异性”活性可能具有特殊价值,从而可以下调全身性IGF-I活性和脂蛋白(a),而不会导致其显着增加。全身雌激素活性。初步证据表明,亚麻木脂素和其他植物雌激素可能在这方面具有潜力。

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