| Literature DB >> 31993221 |
Bruna Alves Fenerich1,2, Jaqueline Cristina Fernandes1,2, Ana Paula Nunes Rodrigues Alves1,2, Juan Luiz Coelho-Silva1,2, Renata Scopim-Ribeiro1,2, Priscila Santos Scheucher1, Christopher A Eide3,4, Cristina E Tognon3,4, Brian J Druker3,4, Eduardo Magalhães Rego1,2,5, João Agostinho Machado-Neto1,6, Fabiola Traina1,2.
Abstract
Recent data indicate that IGF1R/IRS signaling is a potential therapeutic target in BCR-ABL1-negative myeloproliferative neoplasms (MPN); in this pathway, IRS2 is involved in the malignant transformation induced by JAK2V617F, and upregulation of IGF1R signaling induces the MPN phenotype. NT157, a synthetic compound designed as an IGF1R-IRS1/2 inhibitor, has been shown to induce antineoplastic effects in solid tumors. Herein, we aimed to characterize the molecular and cellular effects of NT157 in JAK2V617F-positive MPN cell lines (HEL and SET2) and primary patient hematopoietic cells. In JAK2V617F cell lines, NT157 decreased cell viability, clonogenicity, and cell proliferation, resulting in increases in apoptosis and cell cycle arrest in the G2/M phase (p < 0.05). NT157 treatment inhibited IRS1/2, JAK2/STAT, and NFκB signaling, and it activated the AP-1 complex, downregulated four oncogenes (CCND1, MYB, WT1, and NFKB1), and upregulated three apoptotic-related genes (CDKN1A, FOS, and JUN) (p < 0.05). NT157 induced genotoxic stress in a JAK2/STAT-independent manner. NT157 inhibited erythropoietin-independent colony formation in cells from polycythemia vera patients (p < 0.05). These findings further elucidate the mechanism of NT157 action in a MPN context and suggest that targeting IRS1/2 proteins may represent a promising therapeutic strategy for MPN.Keywords: Haematological cancer; Preclinical research
Year: 2020 PMID: 31993221 PMCID: PMC6978524 DOI: 10.1038/s41392-019-0102-5
Source DB: PubMed Journal: Signal Transduct Target Ther ISSN: 2059-3635