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评估 17α-雌二醇在雄性恒河猴体内的耐受性和生理反应。

Assessing tolerability and physiological responses to 17α-estradiol administration in male rhesus macaques.

机构信息

Aging and Metabolism Research Program, Oklahoma Medical Research Foundation, Oklahoma City, OK, US.

Oklahoma City Veterans Affairs Medical Center, Oklahoma City, OK, US.

出版信息

Geroscience. 2023 Aug;45(4):2337-2349. doi: 10.1007/s11357-023-00767-9. Epub 2023 Mar 10.

DOI:10.1007/s11357-023-00767-9
PMID:36897526
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10651821/
Abstract

17α-estradiol has recently been shown to extend healthspan and lifespan in male mice through multiple mechanisms. These benefits occur in the absence of significant feminization or deleterious effects on reproductive function, which makes 17α-estradiol a candidate for translation into humans. However, human dosing paradigms for the treatment of aging and chronic disease are yet to be established. Therefore, the goals of the current studies were to assess tolerability of 17α-estradiol treatment, in addition to evaluating metabolic and endocrine responses in male rhesus macaque monkeys during a relatively short treatment period. We found that our dosing regimens (0.30 and 0.20 mg/kg/day) were tolerable as evidenced by a lack of GI distress, changes in blood chemistry or complete blood counts, and unaffected vital signs. We also found that the higher dose did elicit mild benefits on metabolic parameters including body mass, adiposity, and glycosylated hemoglobin. However, both of our 17α-estradiol trial doses elicited significant feminization to include testicular atrophy, increased circulating estrogens, and suppressed circulating androgens and gonadotropins. We suspect that the observed level of feminization results from a saturation of the endogenous conjugation enzymes, thereby promoting a greater concentration of unconjugated 17α-estradiol in serum, which has more biological activity. We also surmise that the elevated level of unconjugated 17α-estradiol was subjected to a greater degree of isomerization to 17β-estradiol, which is aligned with the sevenfold increase in serum 17β-estradiol in 17α-estradiol treated animals in our first trial. Future studies in monkeys, and certainly humans, would likely benefit from the development and implementation of 17α-estradiol transdermal patches, which are commonly prescribed in humans and would circumvent potential issues with bolus dosing effects.

摘要

17α-雌二醇最近被证明通过多种机制延长雄性小鼠的健康寿命和寿命。这些益处发生在没有明显女性化或对生殖功能产生有害影响的情况下,这使得 17α-雌二醇成为转化为人类的候选药物。然而,用于治疗衰老和慢性疾病的人体给药方案尚未建立。因此,当前研究的目标是评估 17α-雌二醇治疗的耐受性,此外还评估雄性恒河猴在相对较短的治疗期间的代谢和内分泌反应。我们发现,我们的给药方案(0.30 和 0.20mg/kg/天)是可以耐受的,因为没有胃肠道不适、血液化学或全血细胞计数的变化,以及不受影响的生命体征。我们还发现,较高剂量确实对代谢参数产生了轻微的益处,包括体重、肥胖和糖化血红蛋白。然而,我们的两种 17α-雌二醇试验剂量都引起了明显的女性化,包括睾丸萎缩、循环雌激素增加以及循环雄激素和促性腺激素受抑制。我们怀疑观察到的女性化程度是由于内源性结合酶的饱和,从而促进了更多未结合的 17α-雌二醇在血清中的浓度,这具有更大的生物学活性。我们还推测,未结合的 17α-雌二醇的水平升高会导致更大程度的异构化为 17β-雌二醇,这与我们的第一个试验中 17α-雌二醇处理动物的血清 17β-雌二醇增加七倍相一致。未来在猴子中的研究,当然还有人类中的研究,可能会受益于 17α-雌二醇透皮贴片的开发和实施,这种贴片在人类中常用,并可以避免潜在的剂量冲击效应问题。

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