活化的自体卵巢内富血小板血浆及其衍生物的多通道恢复潜力。

E Scott Sills, Samuel H Wood
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摘要

富血小板血浆(PRP)是一种“整形生物学”,在整形外科、肌肉骨骼疾病、牙科、皮肤病学以及最近的“卵巢年轻化”中发挥着公认的作用。卵巢内PRP涉及血小板激活后释放的复杂分泌组,包括多种细胞因子介质,通过手术输送到较老或无活性的卵巢组织。卵子减数分裂保真度的丧失和伴随高龄产妇的受精受损已经可以通过体外受精来解决,但只能使用年轻捐赠者提供的卵子。然而,如果观察到的纠正胚胎倍性错误的效果可以在病例报告和小系列之外得到证明,激活的PRP(或其凝聚的血浆细胞因子)将带来令人欢迎的治疗中断,这是很难夸大的。由于卵巢功能的缺陷目前主要通过药理学方法解决(即通过重组促性腺激素,GnRH类似物或黄体支持),自体PRP将代表着这些干预措施的不同寻常的偏离。鉴于血小板载货蛋白的多样性,卵巢内PRP的靶反应可能并不局限于卵母细胞或卵泡。例如,PRP操纵信号网络,驱动灌注改善、HOX调节、n -聚糖翻译后修饰、电压门控离子通道调节、端粒稳定、SIRT3优化以及老年卵母细胞的核糖体和线粒体恢复。虽然多通道信号在各种途径上运作并不是生殖生物学所独有的,但在卵巢内PRP中,这一特征几乎没有得到研究,这可能有助于解释为什么其标准化一直很困难。在此背景下,我们的报告考察了被认为最有可能塑造临床实践的研究主题。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Multichannel Recovery Potential with Activated Autologous Intraovarian Platelet-Rich Plasma and Its Derivatives.

Platelet-rich plasma (PRP) is an 'orthobiologic' with recognized roles in plastic surgery, musculoskeletal disorders, dentistry, dermatology, and more recently, 'ovarian rejuvenation'. Intraovarian PRP involves a complex secretome discharged after platelet activation, comprising multiple cytokine mediators delivered surgically to older or inactive ovarian tissue. Loss of oocyte meiotic fidelity and impaired fertilization accompanying advanced maternal age are already managed by IVF, but only with eggs provided by younger donors. However, if the observed effect of rectifying embryo ploidy error can be proven beyond case reports and small series, activated PRP (or its condensed plasma cytokines) would deliver a welcome therapeutic disruption that is difficult to overstate. Because shortcomings in ovarian function are presently addressed mainly by pharmacological approaches (i.e., via recombinant gonadotropins, GnRH analogs, or luteal support), autologous PRP would represent an unusual departure from these interventions. Given the diversity of platelet cargo proteins, the target response of intraovarian PRP is probably not confined to oocytes or follicles. For example, PRP manipulates signal networks driving improved perfusion, HOX regulation, N-glycan post-translational modification, adjustment of voltage-gated ion channels, telomere stabilization, optimization of SIRT3, and ribosome and mitochondria recovery in older oocytes. While multichannel signals operating on various pathways are not unique to reproductive biology, in intraovarian PRP this feature has received little study and may help explain why its standardization has been difficult. Against this background, our report examines the research themes considered most likely to shape clinical practice.

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