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注射到雌性新生小鼠体内的角质形成细胞生长因子可刺激子宫和阴道上皮生长。

Keratinocyte growth factor injected into female mouse neonates stimulates uterine and vaginal epithelial growth.

作者信息

Hom Y K, Young P, Thomson A A, Cunha G R

机构信息

Department of Anatomy, University of California, San Francisco 94143, USA.

出版信息

Endocrinology. 1998 Sep;139(9):3772-9. doi: 10.1210/endo.139.9.6182.

Abstract

Estradiol (E2) stimulates epithelial growth in the female genital tract via estrogen receptors (ER) in the stroma using paracrine mechanisms. Keratinocyte growth factor (KGF), a member of the fibroblast growth factor family, is produced by mesenchymal cells and is mitogenic for epithelial cells making it a strong candidate as a paracrine mediator. Transcripts for KGF and the KGF receptor were detected in the neonatal mouse uterus and vagina. Treatment of neonatal mice with KGF elicited changes in uterine and vaginal epithelium within five days and induced long term effects in these tissues. Newborn female Balb/c mice were injected daily with 5 microg/g body weight of KGF or saline for five days. KGF-treated mice exhibited a 5- to 6-fold increase in uterine epithelial BrdU-labeling index and a 4- and 5-fold increase in vaginal epithelial BrdU-labeling index vs. respective saline-treated controls. Histological sections of KGF-treated uteri revealed dramatic increases in epithelial surface area due to extensive folding of the luminal epithelium. In some areas, the evaginated luminal epithelium invaded zones normally occupied by myometrium. Vaginal epithelium was thicker than that of saline-treated controls following 5 days of KGF treatment. When KGF-treated newborn mice grew to adulthood and were ovariectomized, vaginal smears exhibited persistent diestrus in all animals. Histologic analysis demonstrated a thick parakeratotic vaginal epithelium (approximately 10 cell layers) 9 days postovariectomy in adult neonatally KGF-treated mice. Our studies indicate that KGF injected into neonates markedly stimulated proliferation of neonatal uterine and vaginal epithelium and elicited long-term, persistent abnormal changes in vaginal epithelium.

摘要

雌二醇(E2)通过基质中的雌激素受体(ER)利用旁分泌机制刺激雌性生殖道上皮生长。角质形成细胞生长因子(KGF)是成纤维细胞生长因子家族的一员,由间充质细胞产生,对上皮细胞有促有丝分裂作用,使其成为旁分泌介质的有力候选者。在新生小鼠子宫和阴道中检测到KGF及其受体的转录本。用KGF处理新生小鼠5天,可引起子宫和阴道上皮的变化,并在这些组织中产生长期影响。新生雌性Balb/c小鼠每天注射5微克/克体重的KGF或生理盐水,持续5天。与相应的生理盐水处理对照组相比,KGF处理的小鼠子宫上皮BrdU标记指数增加了5至6倍,阴道上皮BrdU标记指数增加了4至5倍。KGF处理的子宫组织切片显示,由于管腔上皮的广泛折叠,上皮表面积显著增加。在某些区域,外翻的管腔上皮侵入了通常由子宫肌层占据的区域。KGF处理5天后,阴道上皮比生理盐水处理的对照组更厚。当KGF处理的新生小鼠成年后进行卵巢切除时,所有动物的阴道涂片均显示持续的间情期。组织学分析表明,成年新生期接受KGF处理的小鼠在卵巢切除术后9天,阴道上皮出现厚的不全角化(约10个细胞层)。我们的研究表明,向新生儿注射KGF可显著刺激新生儿子宫和阴道上皮的增殖,并引起阴道上皮长期、持续的异常变化。

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