Integrated Cancer Genomics Laboratory, Advanced Centre for Treatment, Research, and Education in Cancer (ACTREC), Tata Memorial Centre, Kharghar, Navi Mumbai, Maharashtra, 410210, India.
Homi Bhabha National Institute, Training School Complex, Anushakti Nagar, Mumbai, Maharashtra, 400094, India.
Breast Cancer Res. 2022 Dec 28;24(1):97. doi: 10.1186/s13058-022-01597-x.
A preoperative-progesterone intervention increases disease-free survival in patients with breast cancer, with an unknown underlying mechanism. We elucidated the role of non-coding RNAs in response to progesterone in human breast cancer.
Whole transcriptome sequencing dataset of 30 breast primary tumors (10 tumors exposed to hydroxyprogesterone and 20 tumors as control) were re-analyzed to identify differentially expressed non-coding RNAs followed by real-time PCR analyses to validate the expression of candidates. Functional analyses were performed by genetic knockdown, biochemical, and cell-based assays.
We identified a significant downregulation in the expression of a long non-coding RNA, Down syndrome cell adhesion molecule antisense DSCAM-AS1, in response to progesterone treatment in breast cancer. The progesterone-induced expression of DSCAM-AS1 could be effectively blocked by the knockdown of progesterone receptor (PR) or treatment of cells with mifepristone (PR-antagonist). We further show that knockdown of DSCAM-AS1 mimics the effect of progesterone in impeding cell migration and invasion in PR-positive breast cancer cells, while its overexpression shows an opposite effect. Additionally, DSCAM-AS1 sponges the activity of miR-130a that regulates the expression of ESR1 by binding to its 3'-UTR to mediate the effect of progesterone in breast cancer cells. Consistent with our findings, TCGA analysis suggests that high levels of miR-130a correlate with a tendency toward better overall survival in patients with breast cancer.
This study presents a mechanism involving the DSCAM-AS1/miR-130a/ESR1 genomic axis through which progesterone impedes breast cancer cell invasion and migration. The findings highlight the utility of progesterone treatment in impeding metastasis and improving survival outcomes in patients with breast cancer.
孕激素预处理可提高乳腺癌患者无病生存率,但作用机制尚不清楚。本研究旨在阐明孕激素作用于人类乳腺癌后非编码 RNA 的变化。
重新分析了 30 例原发性乳腺癌患者(10 例接受羟孕酮治疗,20 例作为对照)的全转录组测序数据集,以鉴定差异表达的非编码 RNA,并用实时 PCR 分析验证候选基因的表达。通过基因敲低、生化和细胞实验进行功能分析。
我们发现,孕激素处理后乳腺癌中长链非编码 RNA 唐氏综合征细胞黏附分子反义 RNA(DSCAM-AS1)的表达显著下调。孕激素诱导的 DSCAM-AS1 表达可被孕激素受体(PR)敲低或米非司酮(PR 拮抗剂)处理有效阻断。进一步研究表明,DSCAM-AS1 敲低模拟了孕激素抑制 PR 阳性乳腺癌细胞迁移和侵袭的作用,而过表达则显示出相反的作用。此外,DSCAM-AS1 可作为 miR-130a 的海绵体,通过与 ESR1 的 3'-UTR 结合来调节其表达,从而介导孕激素在乳腺癌细胞中的作用。TCGA 分析表明,高 miR-130a 水平与乳腺癌患者总生存率提高的趋势相关,这与我们的研究结果一致。
本研究揭示了孕激素通过 DSCAM-AS1/miR-130a/ESR1 基因组轴抑制乳腺癌细胞侵袭和迁移的机制。这些发现强调了孕激素治疗在阻止乳腺癌转移和改善患者生存结果方面的应用价值。
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