Affiliation:
1. Department of Biological Sciences BITS Pilani KK Birla Goa Campus Goa India
2. Department of Surgery Wanless Mission Hospital Miraj Maharashtra India
3. Mahatma Gandhi Cancer Hospital Miraj Maharashtra India
4. Nanobioscience Group, Agharkar Research Institute Pune India
5. Department of Electrical and Electronics Engineering BITS Pilani KK Birla Goa Campus Goa India
Abstract
ABSTRACTAdipocyte is a predominant component of the omental adipose tissue that influences the tumor microenvironment and increases the risk of endometrial cancer progression (EC), however, little is known about the underlying mechanism. In this study, using a co‐culture model, we found that the adipocyte‐EC cell interaction promoted SIRT1 signaling in vitro and in vivo xenograft mice models. Furthermore, immunostaining of SIRT1 protein showed significantly higher expression of SIRT1 in endometrial cancer patients than in normal endometria. RNA sequencing analysis revealed HMMR (hyaluronan‐mediated motility receptor), an oncogene, as a downstream effector of SIRT1 in adipocyte‐associated EC. Transient knockdown and chromatin immunoprecipitation assays showed that SIRT1 inhibition impedes transcription of the HMMR gene via FOXM1, and reduced expression of HMMR in co‐cultured EC cells blocks AURKA activation via TPX2, leading to cell cycle arrest. This is the first study to report the positive correlation between SIRT1 and HMMR in EC patient tumors and might be used as a potential biomarker in EC. Notably, SIRT1 regulates HMMR expression in a FOXM1‐dependent manner, and interfering with SIRT1 may provide a promising strategy for the management of endometrial cancer.
Funder
Department of Biotechnology, Ministry of Science and Technology, India