母亲接受紫杉类药物化疗对女儿卵巢储备和生育能力的影响

Julienne Chaqour B.S. , Meghan C.H. Ozcan M.D. , Payton De La Cruz M.S. , Morgan F. Woodman-Sousa B.S. , Julia N. McAdams B.S. , Kathryn J. Grive Ph.D.
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引用次数: 0

摘要

目的研究子宫内暴露于紫杉类药物对暴露女儿的卵巢储备和生殖潜能的长期影响。设计在胚胎第16.5天对怀孕母鼠进行单次人类相关动物等效剂量的生理盐水、多西他赛或紫杉醇治疗。子宫内暴露的女儿在出生后的多个时间点进行卵巢和内分泌分析,或进行繁殖以评估生育能力。干预措施子宫内暴露于生理盐水、多西他赛或紫杉醇。主要结果测量指标分析所有暴露组的卵泡组成、卵泡闭锁率和多卵泡率。此外,还评估了血清激素水平和卵巢过度刺激后的卵母细胞检索结果。最后,对所有暴露组的动物进行了繁殖,并分析了产仔数、每窝产仔数、活产仔数、产仔间隔时间和最后一窝产仔年龄。此外,存活率染色显示,在子宫内接触过紫杉类药物的女儿的卵巢中,末端脱氧核苷酸转移酶 dUTP 缺口标记阳性卵泡的数量明显增多。激素测定结果还显示,暴露于紫杉类药物的女儿的血清卵泡刺激素浓度发生了显著变化,尤其是在暴露于紫杉醇后,黄体生成素与卵泡刺激素的比率明显升高,这与这些动物无法对卵巢刺激做出适当反应的情况相吻合。为期一年的繁殖研究也表明,这些暴露于紫杉醇的小鼠具有生育能力,但生育期缩短,产仔数明显减少。最后,卵巢效应在接受多西他赛治疗的小鼠的孙女身上也很明显,这表明暴露于紫杉类药物会产生持续的多代效应。 结论:我们的研究表明,在妊娠晚期子宫内暴露于紫杉类药物治疗会对暴露女儿(以及它们的女儿)的长期生殖健康产生重大影响,这将有助于临床医生更好地了解哪种母体恶性肿瘤化疗对发育中的胎儿危害最小。
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Effects of maternal taxane chemotherapy exposure on daughters’ ovarian reserve and fertility potential

Objective

To investigate the long-term effects of in utero taxane exposure on exposed daughters’ ovarian reserve and reproductive potential.

Design

Pregnant dams were treated with a single, human-relevant animal-equivalent dose of saline, docetaxel, or paclitaxel at embryonic day 16.5. In utero-exposed daughters were aged to multiple postnatal time points for ovarian and endocrine analysis or were bred to assess fertility and fecundity. Granddaughters of treated dams were assessed also for ovarian follicle composition and atresia.

Setting

Laboratory study.

Animals

C57BL/6 mice.

Intervention(s)

In utero exposure to saline, docetaxel, or paclitaxel.

Main Outcome Measure(s)

Ovarian follicle composition, rates of follicle atresia, and rates of multioocyte follicles were analyzed in all exposure groups. Serum hormone levels and oocyte retrieval outcomes following ovarian hyperstimulation were also assessed. Finally, animals from all exposure groups were bred with the number of litters, pups per litter, live births, interlitter time interval, and age at the last litter analyzed.

Result(s)

We found that docetaxel and paclitaxel exposure in utero results in ovarian toxicity later in life, significantly affecting folliculogenesis as well as increasing the rate of follicular abnormalities, including follicle atresia and multioocyte follicles. Furthermore, viability staining indicates that the ovaries of daughters exposed to taxanes in utero demonstrate a significantly higher number of terminal deoxynucleotidyl transferase dUTP nick end labeling-positive follicles. Hormone measurements also revealed that serum follicle-stimulating hormone concentration was significantly altered in taxane-exposed daughters, with the ratio of luteinizing hormone to follicle-stimulating hormone significantly elevated, specifically after paclitaxel exposure, coincident with the inability of these animals to properly respond to ovarian stimulation. Breeding studies over the course of a year also suggest that these taxane-exposed mice are fertile, although the duration of their fertility is shortened and they produce significantly fewer litters. Finally, ovarian effects are apparent in granddaughters of mice treated with docetaxel, suggesting persistent and multigenerational effects of taxane exposure.

Conclusion(s)

Our studies demonstrate that in utero exposure to taxane-based therapy during late gestation has a significant effect on the long-term reproductive health of exposed daughters (as well as their daughters) and will be instrumental in helping clinicians better understand which chemotherapies for maternal malignancy are least detrimental to a developing fetus.

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来源期刊
F&S science
F&S science Endocrinology, Diabetes and Metabolism, Obstetrics, Gynecology and Women's Health, Urology
CiteScore
2.00
自引率
0.00%
发文量
0
审稿时长
51 days
期刊最新文献
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