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HOXA10 缺失导致子宫内膜增生进展为子宫内膜癌。

Loss of HOXA10 causes endometrial hyperplasia progressing to endometrial cancer.

机构信息

National Institute for Research in Reproductive and Child Health, ICMR, Parel, Mumbai, India.

National Institute of Immunology, New Delhi, India.

出版信息

J Mol Endocrinol. 2022 Aug 26;69(3):431-444. doi: 10.1530/JME-22-0051. Print 2022 Oct 1.

Abstract

Endometrial cancer is the fourth most common malignancy in women and the precursor lesion is endometrial hyperplasia. HOXA10 is a transcription factor that plays key roles in endometrial functions such as the endowment of receptivity, embryo implantation, and trophoblast invasion. Herein, using testicular transgenesis, we developed transgenic mice that expressed a shRNA against HOXA10 and there was a nearly 70% reduction in the expression of HOXA10 in these animals. We observed that downregulation of HOXA10 led to the development of endometrial hyperplasia in the young animals (3 months), and as they aged (>1 year), most animals developed well-differentiated endometrial adenocarcinoma. In the endometrium of animals with reduced HOXA10, there was increased proliferation and elevated levels of ERα and ERβ. In parallel, there was increased expression of Wnt4 and β-Catenin, SOX9, and YAP1. We propose that chronic reduction in HOXA10 expression disrupts multiple pathways in the uterus that aids in the development of endometrial hyperplasia which progresses to endometrial cancer with age.

摘要

子宫内膜癌是女性第四大常见恶性肿瘤,其前体病变是子宫内膜增生。HOXA10 是一种转录因子,在子宫内膜功能中发挥关键作用,如赋予接受性、胚胎着床和滋养细胞浸润。在此,我们使用睾丸转基因技术,开发了表达 HOXA10 短发夹 RNA 的转基因小鼠,这些动物中 HOXA10 的表达几乎减少了 70%。我们观察到 HOXA10 的下调导致年轻动物(3 个月)子宫内膜增生的发展,随着年龄的增长(>1 年),大多数动物发展为分化良好的子宫内膜腺癌。在 HOXA10 减少的动物的子宫内膜中,增殖增加,并且 ERα 和 ERβ 的水平升高。平行地,Wnt4 和 β-连环蛋白、SOX9 和 YAP1 的表达增加。我们提出,HOXA10 表达的慢性减少破坏了子宫中的多个途径,有助于子宫内膜增生的发展,随着年龄的增长进展为子宫内膜癌。

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