首页> 美国卫生研究院文献>American Journal of Physiology - Endocrinology and Metabolism >17β-Hydroxyestra-4911-trien-3-one (trenbolone) exhibits tissue selective anabolic activity: effects on muscle bone adiposity hemoglobin and prostate
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17β-Hydroxyestra-4911-trien-3-one (trenbolone) exhibits tissue selective anabolic activity: effects on muscle bone adiposity hemoglobin and prostate

机译:17β-羟基雌二醇-4911-trien-3-one(群勃龙)具有组织选择性合成代谢活性:对肌肉骨骼脂肪血红蛋白和前列腺的影响

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摘要

Selective androgen receptor modulators (SARMs) now under development can protect against muscle and bone loss without causing prostate growth or polycythemia. 17β-Hydroxyestra-4,9,11-trien-3-one (trenbolone), a potent testosterone analog, may have SARM-like actions because, unlike testosterone, trenbolone does not undergo tissue-specific 5α-reduction to form more potent androgens. We tested the hypothesis that trenbolone-enanthate (TREN) might prevent orchiectomy-induced losses in muscle and bone and visceral fat accumulation without increasing prostate mass or resulting in adverse hemoglobin elevations. Male F344 rats aged 3 mo underwent orchiectomy or remained intact and were administered graded doses of TREN, supraphysiological testosterone-enanthate, or vehicle for 29 days. In both intact and orchiectomized animals, all TREN doses and supraphysiological testosterone-enanthate augmented androgen-sensitive levator ani/bulbocavernosus muscle mass by 35–40% above shams (P ≤ 0.001) and produced a dose-dependent partial protection against orchiectomy-induced total and trabecular bone mineral density losses (P < 0.05) and visceral fat accumulation (P < 0.05). The lowest doses of TREN successfully maintained prostate mass and hemoglobin concentrations at sham levels in both intact and orchiectomized animals, whereas supraphysiological testosterone-enanthate and high-dose TREN elevated prostate mass by 84 and 68%, respectively (P < 0.01). In summary, low-dose administration of the non-5α-reducible androgen TREN maintains prostate mass and hemoglobin concentrations near the level of shams while producing potent myotrophic actions in skeletal muscle and partial protection against orchiectomy-induced bone loss and visceral fat accumulation. Our findings indicate that TREN has advantages over supraphysiological testosterone and supports the need for future preclinical studies examining the viability of TREN as an option for androgen replacement therapy.
机译:目前正在开发的选择性雄激素受体调节剂(SARM)可以防止肌肉和骨质流失,而不会引起前列腺生长或红细胞增多症。 17β-羟基雌激素-4,9,11-trien-3-one(群勃龙)可能是一种类似雄激素的作用,因为与睾丸酮不同,群勃龙不进行组织特异性5α还原反应而形成更有效的雄激素。我们检验了群勃龙-庚酸酯(TREN)可以预防睾丸切除术诱导的肌肉和骨骼损失以及内脏脂肪积聚的假设,而不会增加前列腺肿块或导致不良的血红蛋白升高。对3个月大的F344雄性大鼠进行睾丸切除术或保持完整无缺,并对其进行29天的分级剂量TREN,超生理性睾丸激素-庚酸酯或赋形剂给药。在完整和经睾丸切除的动物中,所有TREN剂量和睾丸上睾丸激素-庚酸酯对雄激素敏感的提肛ani / bulbocavernosus肌肉的质量均比毛发高出35–40%(P≤0.001),并且对睾丸切除术引起的总剂量产生剂量依赖性的部分保护作用和小梁骨矿物质密度损失(P <0.05)和内脏脂肪堆积(P <0.05)。最低剂量的TREN成功地将完整和经睾丸切除的动物的前列腺质量和血红蛋白浓度维持在假水平,而超生理性睾丸激素-庚酸酯和大剂量TREN分别使前列腺质量增加84%和68%(P <0.01)。总之,低剂量的非5α还原型雄激素TREN可使前列腺肿块和血红蛋白浓度保持在接近毛发水平,同时在骨骼肌中产生强力的肌营养作用,并部分抵抗睾丸切除术引起的骨质流失和内脏脂肪蓄积。我们的研究结果表明,TREN优于睾丸上生理学睾丸激素,并支持未来的临床前研究需要检查TREN作为雄激素替代疗法的可行性。

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