IGF1R/IRS1 Targeting Has Cytotoxic Activity and Inhibits PI3K/AKT/mTOR and MAPK Signaling in Acute Lymphoblastic Leukemia Cells

Overview

Journal Cancer Lett

Specialty Oncology

Date 2019 May 3

PMID 31042587

Citations 19

Authors

Ana Paula Nunes Rodrigues Alves

Jaqueline Cristina Fernandes

Bruna Alves Fenerich

Juan Luiz Coelho-Silva

Priscila Santos Scheucher

Belinda Pinto Simoes

Eduardo Magalhaes Rego

Anne J Ridley

Joao Agostinho Machado-Neto

Fabiola Traina

Affiliations

Soon will be listed here.

Abstract

The IGF1R/IRS1 signaling is activated in acute lymphoblastic leukemia (ALL) and can be targeted by the pharmacological inhibitors NT157 (IGF1R-IRS1/2 inhibitor) and OSI-906 (IGF1R/IR inhibitor). Here we investigate the cellular and molecular effects of NT157 and OSI-906 in ALL cells. NT157 and OSI-906 treatment reduced viability, proliferation and cell cycle progression in ALL cell lines. Similarly, in primary samples of patients with ALL, both OSI-906 and NT157 reduced viability, but only NT157 induced apoptosis. NT157 and OSI-906 did not show cytotoxicity in primary samples from healthy donor. NT157 and OSI-906 significantly decreased Jurkat cell migration, but did not modulate Namalwa migration. Consistent with the more potent effect of NT157 on cells, NT157 significantly modulated expression of 25 genes related to the MAPK signaling pathway in Jurkat cells, including oncogenes and tumor suppressor genes. Both compounds inhibited mTOR and p70S6K activity, but only NT157 inhibited AKT and 4-EBP1 activation. In summary, in ALL cells, NT157 has cytotoxic activity, whereas OSI-906 is cytostatic. NT157 has a stronger effect on ALL cells, and thus the direct inhibition of IRS1 may be a potential therapeutic target in ALL.

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