Development of improved SRC-3 inhibitors as breast cancer therapeutic agents.
Li QinJianwei ChenDong LuPrashi JainYang YuDavid CardenasXiaohui PengXiaobin YuJianming XuJin WangBert W O'MalleyDavid M LonardPublished in: Endocrine-related cancer (2021)
Steroid receptor coactivators (SRCs) possess specific and distinct oncogenic roles in the initiation of cancer and in its progression to a more aggressive disease. These coactivators interact with nuclear receptors and other transcription factors to boost transcription of multiple genes, which potentiate cancer cell proliferation, migration, invasion, tumor angiogenesis and epithelial-mesenchymal transition (EMT). Targeting SRCs using small molecule inhibitors (SMIs) is a promising approach to control cancer progression and metastasis. By high-throughput screening analysis, we recently identified SI-2 as a potent SRC SMI. To develop therapeutic agents, SI-10 and SI-12, the SI-2 analogs are synthesized that incorporate the addition of F atoms to the SI-2 chemical structure. As a result, these analogs exhibit a significantly prolonged plasma half-life, minimal toxicity and improved hERG activity. Biological functional analysis showed that SI-10 and SI-12 treatment (5-50 nM) can significantly inhibit viability, migration and invasion of breast cancer cells in vitro and repress the growth of breast cancer PDX organoids. Treatment of mice with 10 mg/kg/day of either SI-10 or SI-12 was sufficient to repress the growth of xenograft tumors derived from MDA-MB-231 and LM2 cells. Furthermore, in spontaneous and experimental metastasis mouse models developed from MDA-MB-231 and LM2 cells, respectively, SI-10 and SI-12 effectively inhibited the progression of breast cancer lung metastasis. These results demonstrate that SI-10 and SI-12 are promising therapeutic agents and are specifically effective in blocking tumor metastasis, a key point in tumor progression to a more lethal state that results in patient mortality in the majority of cases.
Keyphrases
- room temperature
- epithelial mesenchymal transition
- small molecule
- breast cancer cells
- transcription factor
- cell proliferation
- induced apoptosis
- oxidative stress
- squamous cell carcinoma
- cardiovascular disease
- case report
- cell cycle
- adipose tissue
- molecular docking
- tyrosine kinase
- genome wide
- photodynamic therapy
- ionic liquid
- insulin resistance
- binding protein
- smoking cessation
- poor prognosis
- high fat diet induced