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通过胚胎移植诱导的宫内生长受限的性别二态性小鼠模型。

A sexually dimorphic murine model of IUGR induced by embryo transfer.

作者信息

Kaur Harleen, Care Alison S, Wilson Rebecca L, Piltz Sandra G, Thomas Paul Q, Muhlhausler Beverly S, Roberts Claire T, Gatford Kathryn L

机构信息

Robinson Research Institute, University of Adelaide, Adelaide, Australia.

Adelaide Medical School, University of Adelaide, Adelaide, Australia.

出版信息

Reproduction. 2021 Feb;161(2):135-144. doi: 10.1530/REP-20-0209.

Abstract

Animal models are needed to develop interventions to prevent or treat intrauterine growth restriction (IUGR). Foetal growth rates and effects of in utero exposures differ between sexes, but little is known about sex-specific effects of increasing litter size. We established a murine IUGR model using pregnancies generated by multiple embryo transfers, and evaluated sex-specific responses to increasing litter size. CBAF1 embryos were collected at gestation day 0.5 (GD0.5) and 6, 8, 10 or 12 embryos were transferred into each uterine horn of pseudopregnant female CD1 mice (n = 32). Foetal and placental outcomes were measured at GD18.5. In the main experiment, foetuses were genotyped (Sry) for analysis of sex-specific outcomes. The number of implantation sites (P = 0.033) and litter size (number of foetuses, P = 0.008) correlated positively with the number of embryos transferred, while placental weight correlated negatively with litter size (both P < 0.01). The relationship between viable litter size and foetal weight differed between sexes (interaction P = 0.002), such that foetal weights of males (P = 0.002), but not females (P = 0.233), correlated negatively with litter size. Placental weight decreased with increasing litter size (P < 0.001) and was lower in females than males (P = 0.020). Our results suggest that male foetuses grow as fast as permitted by nutrient supply, whereas the female maintains placental reserve capacity. This strategy reflecting sex-specific gene expression is likely to place the male foetus at greater risk of death in the event of a 'second hit'.

摘要

需要动物模型来开发预防或治疗宫内生长受限(IUGR)的干预措施。胎儿生长速率和子宫内暴露的影响存在性别差异,但关于窝仔数增加的性别特异性影响知之甚少。我们通过多次胚胎移植产生的妊娠建立了一种小鼠IUGR模型,并评估了对窝仔数增加的性别特异性反应。在妊娠第0.5天(GD0.5)收集CBAF1胚胎,并将6、8、10或12个胚胎移植到假孕雌性CD1小鼠的每个子宫角中(n = 32)。在GD18.5测量胎儿和胎盘结局。在主要实验中,对胎儿进行基因分型(Sry)以分析性别特异性结局。着床部位数量(P = 0.033)和窝仔数(胎儿数量,P = 0.008)与移植胚胎数量呈正相关,而胎盘重量与窝仔数呈负相关(均P < 0.01)。存活窝仔数与胎儿体重之间的关系存在性别差异(交互作用P = 0.002),即雄性胎儿体重(P = 0.002)与窝仔数呈负相关,而雌性胎儿体重(P = 0.233)与窝仔数无相关性。胎盘重量随着窝仔数增加而降低(P < 0.001),且雌性低于雄性(P = 0.020)。我们的结果表明,雄性胎儿在营养供应允许的情况下尽可能快速生长,而雌性则维持胎盘储备能力。这种反映性别特异性基因表达的策略可能使雄性胎儿在遭遇“二次打击”时死亡风险更高。

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