Single-cell RNA-sequencing analysis of estrogen- and endocrine-disrupting chemical-induced reorganization of mouse mammary gland.
Noriko KanayaGregory ChangXiwei WuKohei SaekiLauren BernalHyun-Jeong ShimJinhui WangCharles David WardenTakuro YamamotoJay LiJune-Soo ParkTimothy SynoldSteve VonderfechtMichele RakoffSusan L NeuhausenShiuan ChenPublished in: Communications biology (2019)
Menopause is a critical window of susceptibility for its sensitivity to endocrine disrupting chemicals due to the decline of endogenous estrogen. Using a surgical menopausal (ovariectomized) mouse model, we assessed how mammary tissue was affected by both 17β-estradiol (E2) and polybrominated diphenyl ethers (PBDEs). As flame retardants in household products, PBDEs are widely detected in human serum. During physiologically-relevant exposure to E2, PBDEs enhanced E2-mediated regrowth of mammary glands with terminal end bud-like structures. Analysis of mammary gland RNA revealed that PBDEs both augmented E2-facilitated gene expression and modulated immune regulation. Through single-cell RNA sequencing (scRNAseq) analysis, E2 was found to induce Pgr expression in both Esr1 + and Esr1 - luminal epithelial cells and Ccl2 expression in Esr1 + fibroblasts. PBDEs promote the E2-AREG-EGFR-M2 macrophage pathway. Our findings support that E2 + PBDE increases the risk of developing breast cancer through the expansion of estrogen-responsive luminal epithelial cells and immune modulation.
Keyphrases
- single cell
- estrogen receptor
- rna seq
- gene expression
- poor prognosis
- high throughput
- mouse model
- small cell lung cancer
- dna methylation
- high resolution
- binding protein
- epidermal growth factor receptor
- tyrosine kinase
- adipose tissue
- drug delivery
- cancer therapy
- diabetic rats
- drug induced
- oxidative stress
- liver injury
- high glucose
- liver fibrosis
- extracellular matrix
- stress induced
- nucleic acid