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首页> 外文期刊>Endocrinology >Prevention of the onset of Ovarian Hyperstimulation Syndrome (OHSS) in the rat after ovulation induction with a low molecular weight agonist of the LH receptor compared with hCG and rec-LH
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Prevention of the onset of Ovarian Hyperstimulation Syndrome (OHSS) in the rat after ovulation induction with a low molecular weight agonist of the LH receptor compared with hCG and rec-LH

机译:与hCG和rec-LH相比,LH受体低分子量激动剂诱导排卵后预防大鼠卵巢过度刺激综合症(OHSS)的发作

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Ovarian hyperstimulation syndrome (OHSS) incidentally occurs in controlled ovarian stimulation protocols and is associated with human chorionic gonadotropin (hCG) administration. OHSS is caused by increased vascular permeability (VP) and thought to be mediated by hypersecretion of vascular endothelial growth factor (VEGF) by granulosa cells. Low molecular weight (LMW)-LH agonists have a similar mode of action but a shorter half-life compared with hCG, which could potentially lead to a clinical benefit in reducing the risk for OHSS in controlled ovarian stimulation protocols. The objective of this study is to investigate the role of an orally active LMW-LH agonist in OHSS induction compared with recombinant LH (rec-LH) and hCG. Immature rats were hyper-stimulated with pregnant mare serum gonadotropin, and ovulation was induced by hCG, rec-LH or a LMW-LH agonist. The degree of VP was determined by Evans Blue in the abdominal cavity. Ovaries were weighed, and VEGF concentration in the ovary was determined. Pregnant mareserum gonadotropin stimulation followed by single-dose hCG or rec-LH resulted in clear enlargement of the ovaries and increased VP and VEGF levels. However, ovulation induction with a single dose of the LMW-LH agonist did not result in increased VP and VEGF levels, and even multiple dosing to mimic a longer exposure did not induce OHSS symptoms. In conclusion, we demonstrated that the oral LMW-LH agonist did not induce VP in rat, indicative for OHSS, possibly due to reduced VEGF production. If this is translatable to human, this could potentially represent a clinical benefit in reducing the risk for OHSS when using these compounds in controlled ovarian stimulation protocols.
机译:卵巢过度刺激综合症(OHSS)偶然发生在受控的卵巢刺激方案中,并且与人绒毛膜促性腺激素(hCG)给药有关。 OHSS由血管通透性(VP)升高引起,并被认为是由颗粒细胞过度分泌血管内皮生长因子(VEGF)介导的。与hCG相比,低分子量(LMW)-LH激动剂具有相似的作用方式,但半衰期更短,这有可能在降低可控卵巢刺激方案中降低OHSS的风险方面带来临床益处。这项研究的目的是研究与重组LH(rec-LH)和hCG相比,口服活性LMW-LH激动剂在OHSS诱导中的作用。未成熟的大鼠用母马血清促性腺激素过度刺激,并通过hCG,rec-LH或LMW-LH激动剂诱导排卵。 VP的程度由腹腔中的Evans Blue确定。称重卵巢,并测定卵巢中的VEGF浓度。怀孕的Mareserum促性腺激素刺激,然后单剂量hCG或rec-LH导致卵巢明显增大,VP和VEGF水平升高。但是,单剂LMW-LH激动剂诱导排卵并不会导致VP和VEGF水平升高,即使多次给药以模仿更长的暴露时间也不会引起OHSS症状。总之,我们证明了口服LMW-LH激动剂不会在大鼠中诱导VP,这表明OHSS,这可能是由于VEGF产生减少所致。如果这可翻译为人类,则在控制卵巢刺激方案中使用这些化合物时,这可能代表降低OHSS风险的临床益处。

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