控制性卵巢过度刺激
不育
卵巢过度刺激综合征
卵巢储备
辅助生殖技术
排卵
卵胞浆内精子注射
促排卵
无排卵
体外受精
医学
受精
卵巢
人口
妇科
怀孕
男科
生物
内分泌学
激素
精子
糖尿病
多囊卵巢
胰岛素抵抗
环境卫生
遗传学
作者
Olga Goiana Martins Sampaio,Sacha Aubrey Alves Rodrigues Santos,Marina de Barros Mamede Vidal Damasceno,Larissa Brandão Joventino,Augusto Schneider,Michał M. Masternak,Adriana Rolim Campos,Marcelo Borges Cavalcante
标识
DOI:10.1016/j.jri.2024.104277
摘要
One of six couples (17.5% of the adult population) worldwide is affected by infertility during their lifetime. This number represents a substantial increase in the prevalence of this gynecological condition over the last decade. Ovulatory dysfunction and anovulation are the main causes of female infertility. Timed intercourse, intrauterine insemination, and assisted reproductive technology (ART), such as in vitro fertilization (IVF) and intracytoplasmic sperm injection (ICSI), are the most common interventions for infertile couples. Ovulation induction protocols for IVF/ICSI routinely use supraphysiological doses of gonadotropins to stimulate many preovulatory follicles. Animal and human studies suggested that ovarian hyperstimulation, alone or repeatedly, for ART cycles can induce changes in the immune response and increase the oxidative stress (OS) in the ovarian microenvironment. The consequences of repeated ovarian hyperstimulation on the human ovary remain poorly understood, particularly in relation to the effects of ovarian stimulation on the immune system and the potential for ovarian stimulation to cause OS. Animal studies have observed that repeated cycles of ovarian hyperstimulation can accelerate ovarian aging. Changes in ovarian hormone levels, accelerated loss of ovarian reserve, disorders in ovarian ultrastructure, ovarian senescence, and decreased reproductive performance represent possible long-term effects of repeated ovarian hyperstimulation. The short and long-term impact of the combination of antioxidant agents in ovarian hyperstimulation protocols in women undergoing ART must urgently be better understood. The recent increase in the number of ART and fertility preservation cycles may accelerate ovarian aging in these women, promoting consequences beyond the reproductive function and including health deterioration.
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