Cunha Gerald R, Kurita Takeshi, Cao Mei, Shen Joel, Robboy Stanley J, Baskin Laurence
Department of Urology, University of California, 400 Parnassus Avenue, San Francisco, CA 94143, United States.
Department of Cancer Biology and Genetics, College of Medicine, Comprehensive Cancer Center, 812 Biomedical Research Tower, 460 West 12th Avenue, Columbus, OH 43210, United States.
Differentiation. 2017 Nov-Dec;98:35-54. doi: 10.1016/j.diff.2017.10.001. Epub 2017 Oct 4.
Human female fetal reproductive tracts 9.5-22 weeks of gestation were grown for 1 month in ovariectomized athymic adult female mouse hosts that were either untreated or treated continuously with diethylstilbestrol (DES) via subcutaneous pellet. Normal morphogenesis and normal patterns of differentiation marker expression (KRT6, KRT7, KRT8, KRT10, KRT14, KRT19, ESR1, PGR, TP63, RUNX1, ISL1, HOXA11 and α-ACT2) were observed in xenografts grown in untreated hosts and mimicked observations of previously reported (Cunha et al., 2017) non-grafted specimens of comparable age. DES elicited several notable morphological affects: (a) induction of endometrial/cervical glands, (b) increased plication (folding) of tubal epithelium, (c) stratified squamous maturation of vaginal epithelium and (d) vaginal adenosis. DES also induced ESR1 in epithelia of the uterine corpus, cervix and globally induced PGR in most cells of the developing human female reproductive tract. Keratin expression (KRT6, KRT7, KRT8, KRT14 and KRT19) was minimally affected by DES. Simple columnar adenotic epithelium was devoid of TP63 and RUNX1, while DES-induced mature vaginal epithelium was positive for both transcription factors. Another striking effect of DES was observed in grafts of human uterine tube, in which DES perturbed smooth muscle patterning. These results define for the first time IHC protein markers of DES action on the developing human reproductive tract, which provide bio-endpoints of estrogen-induced teratogenesis in the developing human female reproductive tract for future testing of estrogenic endocrine disruptors.
将妊娠9.5 - 22周的人类女性胎儿生殖道在切除卵巢的成年雌性无胸腺小鼠宿主体内培养1个月,这些宿主要么未接受治疗,要么通过皮下植入物持续接受己烯雌酚(DES)治疗。在未接受治疗的宿主体内生长的异种移植物中观察到正常的形态发生和分化标志物表达的正常模式(KRT6、KRT7、KRT8、KRT10、KRT14、KRT19、ESR1、PGR、TP63、RUNX1、ISL1、HOXA11和α - ACT2),并且与先前报道的(Cunha等人,2017年)年龄相当的未移植标本的观察结果相似。DES引发了几种显著的形态学影响:(a)子宫内膜/宫颈腺体的诱导,(b)输卵管上皮褶皱增加,(c)阴道上皮分层鳞状成熟,以及(d)阴道腺病。DES还在子宫体上皮中诱导ESR1表达,并且在发育中的人类女性生殖道的大多数细胞中整体诱导PGR表达。角蛋白表达(KRT6、KRT7、KRT8、KRT14和KRT19)受DES影响最小。简单柱状腺性上皮缺乏TP63和RUNX1,而DES诱导的成熟阴道上皮对这两种转录因子均呈阳性。在人类输卵管移植物中观察到DES的另一个显著作用,其中DES扰乱了平滑肌模式。这些结果首次确定了DES对发育中的人类生殖道作用的免疫组化蛋白质标志物,为未来雌激素内分泌干扰物的测试提供了发育中的人类女性生殖道中雌激素诱导致畸作用的生物终点。