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骨石化(op/op)小鼠的妊娠缺陷表明雌性生育能力中对集落刺激因子-1(CSF-1)的需求。

A pregnancy defect in the osteopetrotic (op/op) mouse demonstrates the requirement for CSF-1 in female fertility.

作者信息

Pollard J W, Hunt J S, Wiktor-Jedrzejczak W, Stanley E R

机构信息

Department of Developmental Biology and Cancer, Albert Einstein College of Medicine (AECOM), Bronx, New York 10461.

出版信息

Dev Biol. 1991 Nov;148(1):273-83. doi: 10.1016/0012-1606(91)90336-2.

Abstract

Correlative evidence suggests that maternal production of the mononuclear phagocyte growth factor colony stimulating factor-1 (CSF-1) regulates placental development. In order to study the role of CSF-1 in pregnancy the fertility of CSF-1-less osteopetrotic (op/op) mutant mice was investigated. Homozygous mutant crosses (op/op x op/op) were consistently infertile. As expected, op/op males were almost completely fertile when crossed with heterozygous females. Surprisingly, op/op females when mated to heterozygote males were fertile, although at a rate that was 46% of the rate for +/op females x op/op males. These data suggest that CSF-1 is required for pregnancy. However, a maternal CSF-1 source is not absolutely necessary in that pregnancies involving +/op fathers were partially rescued, suggesting that +/op fetuses and/or +/op seminal fluid provides CSF-1 or CSF-1-induced factors which compensate for the absence of maternally produced CSF-1. Despite the complete absence of CSF-1 in the uterus and placenta of op/op mice placental weights were normal, suggesting that proliferation of decidual cells and trophoblasts, both of which express the CSF-1 receptor, may not be solely regulated by CSF-1. Histochemical staining for F4/80 antigen was used to identify macrophages in the uterus and placenta. Uterine macrophages could not be detected in virgin op/op mice although they were abundant in +/op uteri. Interestingly, macrophages could be detected in op/op uteri as uncharacteristically rounded cells in early gestation, however, they were not maintained and no macrophages were apparent beyond Day 14 of pregnancy in op/op mice. Further studies in the osteopetrotic mouse will be useful in delineating those functions required for pregnancy that are regulated by CSF-1.

摘要

相关证据表明,母体产生的单核吞噬细胞生长因子集落刺激因子-1(CSF-1)调节胎盘发育。为了研究CSF-1在妊娠中的作用,对缺乏CSF-1的骨硬化症(op/op)突变小鼠的生育能力进行了研究。纯合突变体杂交(op/op×op/op)始终不育。正如预期的那样,op/op雄性与杂合雌性杂交时几乎完全可育。令人惊讶的是,op/op雌性与杂合子雄性交配时是可育的,尽管其生育率仅为+/op雌性×op/op雄性生育率的46%。这些数据表明,妊娠需要CSF-1。然而,母体CSF-1来源并非绝对必要,因为涉及+/op父亲的妊娠部分得到挽救,这表明+/op胎儿和/或+/op精液提供了CSF-1或CSF-1诱导因子,可弥补母体产生的CSF-1的缺失。尽管op/op小鼠的子宫和胎盘中完全没有CSF-1,但胎盘重量正常,这表明蜕膜细胞和滋养层细胞(两者均表达CSF-1受体)的增殖可能并非仅受CSF-1调节。用F4/80抗原进行组织化学染色以鉴定子宫和胎盘中的巨噬细胞。在未交配的op/op小鼠子宫中未检测到子宫巨噬细胞,而在+/op子宫中则大量存在。有趣的是,在op/op小鼠子宫中,巨噬细胞在妊娠早期可作为异常圆形细胞被检测到,然而,它们并未持续存在,在妊娠第14天之后,op/op小鼠子宫中就不再有明显的巨噬细胞。对骨硬化症小鼠的进一步研究将有助于阐明妊娠中受CSF-1调节的那些功能。

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