首页> 美国卫生研究院文献>PLoS Clinical Trials >Growth Hormone Improves Growth Retardation Induced by Rapamycin without Blocking Its Antiproliferative and Antiangiogenic Effects on Rat Growth Plate
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Growth Hormone Improves Growth Retardation Induced by Rapamycin without Blocking Its Antiproliferative and Antiangiogenic Effects on Rat Growth Plate

机译:生长激素可改善雷帕霉素诱导的生长迟缓,而不会阻止其对大鼠生长板的抗增殖和抗血管生成作用

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摘要

Rapamycin, an immunosuppressant agent used in renal transplantation with antitumoral properties, has been reported to impair longitudinal growth in young individuals. As growth hormone (GH) can be used to treat growth retardation in transplanted children, we aimed this study to find out the effect of GH therapy in a model of young rat with growth retardation induced by rapamycin administration. Three groups of 4-week-old rats treated with vehicle (C), daily injections of rapamycin alone (RAPA) or in combination with GH (RGH) at pharmacological doses for 1 week were compared. GH treatment caused a 20% increase in both growth velocity and body length in RGH animals when compared with RAPA group. GH treatment did not increase circulating levels of insulin-like growth factor I, a systemic mediator of GH actions. Instead, GH promoted the maturation and hypertrophy of growth plate chondrocytes, an effect likely related to AKT and ERK1/2 mediated inactivation of GSK3β, increase of glycogen deposits and stabilization of β-catenin. Interestingly, GH did not interfere with the antiproliferative and antiangiogenic activities of rapamycin in the growth plate and did not cause changes in chondrocyte autophagy markers. In summary, these findings indicate that GH administration improves longitudinal growth in rapamycin-treated rats by specifically acting on the process of growth plate chondrocyte hypertrophy but not by counteracting the effects of rapamycin on proliferation and angiogenesis.
机译:雷帕霉素是一种用于肾脏移植的具有抗肿瘤特性的免疫抑制剂,据报道会损害年轻人的纵向生长。由于生长激素(GH)可用于治疗移植儿童的生长发育迟缓,因此我们的目的是为了研究GH治疗在雷帕霉素诱导的生长发育迟缓的幼鼠模型中的作用。比较了三组用媒介物(C),每天单独注射雷帕霉素(RAPA)或与GH(RGH)联合以药理剂量治疗1周的4周龄大鼠。与RAPA组相比,GH治疗使RGH动物的生长速度和体长都增加了20%。 GH治疗并未增加胰岛素样生长因子I(GH作用的系统性介质)的循环水平。相反,GH促进了生长板软骨细胞的成熟和肥大,这种作用可能与AKT和ERK1 / 2介导的GSK3β失活,糖原沉积增加和β-catenin稳定有关。有趣的是,GH不会干扰雷帕霉素在生长平板中的抗增殖和抗血管生成活性,也不会引起软骨细胞自噬标记的变化。总而言之,这些发现表明,GH的给药通过特异性地作用于生长板软骨细胞肥大的过程而不是通过抵消雷帕霉素对增殖和血管生成的作用来改善雷帕霉素治疗的大鼠的纵向生长。

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