1. Insulin receptor substrate-4 is overexpressed in colorectal cancer and promotes retinoblastoma–cyclin-dependent kinase activation
- Author
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Maria V.T. Lobo, Patricia Sanmartín-Salinas, Miguel Toro Londoño, Fernando Noguerales-Fraguas, Antonio Jiménez-Ruiz, and Luis G. Guijarro
- Subjects
Adenoma ,Male ,0301 basic medicine ,Cytoplasm ,Carcinoma, Hepatocellular ,Cell cycle checkpoint ,Cyclin E ,Colon ,Adenocarcinoma ,Retinoblastoma Protein ,Wortmannin ,03 medical and health sciences ,chemistry.chemical_compound ,0302 clinical medicine ,Cyclin D1 ,Insulin Receptor Substrate 4 ,Cyclin-dependent kinase ,Cell Line, Tumor ,Proliferating Cell Nuclear Antigen ,Humans ,Insulin-Like Growth Factor I ,Aged ,Cell Proliferation ,Neoplasm Staging ,Aged, 80 and over ,Cell Nucleus ,biology ,Chemistry ,Kinase ,Cell Membrane ,Liver Neoplasms ,Rectum ,Gastroenterology ,Middle Aged ,Cell cycle ,Up-Regulation ,Protein Transport ,030104 developmental biology ,030220 oncology & carcinogenesis ,Insulin Receptor Substrate Proteins ,biology.protein ,Cancer research ,Female ,Neoplasm Grading ,Colorectal Neoplasms ,E2F1 Transcription Factor ,Signal Transduction - Abstract
Insulin receptor substrate 4 (IRS-4) is an adaptor protein for which new evidence suggests plays a role in tumour promotion. We described nuclear IRS-4 in RKO colon cancer cell lines in biopsies of patients with colorectal cancer (CRC) (n = 20) and in matched adjacent normal colorectal (MANC) tissue (n = 20). Treatment with physiological doses of IGF-1 promoted nuclear influx of IRS-4 from cellular cytosol in RKO cells. When exogenous IRS-4 was overexpressed in RKO cells, there was an increase in cyclin D1, cyclin E, E2F1, pRB Ser 809/811 and pRB Ser 705 levels compared with the empty vector-transfected cells. Some of these changes returned to control values after wortmannin treatment. Subcellular fractionation showed an overexpression of IRS-4 in the cytoplasm, membrane, and nuclei of tumour samples, whereas the levels of the protein were barely detectable in the three compartments of normal samples. Immunohistochemical studies showed positive nuclear IRS-4 staining in over 74% of the tumour cells. IRS-4 was strongly overexpressed in tumoural tissues from CRC patients compared to MANC tissues. The up-regulation of IRS-4 in CRC samples correlated significantly with the increase of several G1 checkpoint proteins including cyclin D1 (r = 0.6662), Rb (r = 0.7779), pRb Serine 809/811 (r = 0.6864), pRb serine 705 (r = 0.6261) and E2F1 (r = 0.8702). Taken together, our findings suggest that IRS-4 promotes retinoblastoma–cyclin-dependent kinase activation and it may serve as a pharmacological target since its expression is very low in normal tissue, including colonic epithelium.
- Published
- 2018
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