| Literature DB >> 31142661 |
Suryavathi Viswanadhapalli1, Yiliao Luo1,2, Gangadhara R Sareddy1,3, Bindu Santhamma4, Mei Zhou1,5, Mengxing Li1,6, Shihong Ma7, Rajni Sonavane7, Uday P Pratap1, Kristin A Altwegg1, Xiaonan Li1, Annabel Chang7, Alejandra Chávez-Riveros4, Kalarickal V Dileep8, Kam Y J Zhang8, Xinlei Pan9, Ramachandran Murali9, Marek Bajda10, Ganesh V Raj7, Andrew J Brenner3,11, Vijaya Manthati4, Manjeet K Rao3,12, Rajeshwar R Tekmal1,3, Hareesh B Nair13, Klaus J Nickisch4, Ratna K Vadlamudi14,3.
Abstract
Leukemia inhibitory factor receptor (LIFR) and its ligand LIF play a critical role in cancer progression, metastasis, stem cell maintenance, and therapy resistance. Here, we describe a rationally designed first-in-class inhibitor of LIFR, EC359, which directly interacts with LIFR to effectively block LIF/LIFR interactions. EC359 treatment exhibits antiproliferative effects, reduces invasiveness and stemness, and promotes apoptosis in triple-negative breast cancer (TNBC) cell lines. The activity of EC359 is dependent on LIF and LIFR expression, and treatment with EC359 attenuated the activation of LIF/LIFR-driven pathways, including STAT3, mTOR, and AKT. Concomitantly, EC359 was also effective in blocking signaling by other LIFR ligands (CTF1, CNTF, and OSM) that interact at LIF/LIFR interface. EC359 significantly reduced tumor progression in TNBC xenografts and patient-derived xenografts (PDX), and reduced proliferation in patient-derived primary TNBC explants. EC359 exhibits distinct pharmacologic advantages, including oral bioavailability, and in vivo stability. Collectively, these data support EC359 as a novel targeted therapeutic that inhibits LIFR oncogenic signaling.See related commentary by Shi et al., p. 1337. ©2019 American Association for Cancer Research.Entities:
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Year: 2019 PMID: 31142661 PMCID: PMC6677593 DOI: 10.1158/1535-7163.MCT-18-1258
Source DB: PubMed Journal: Mol Cancer Ther ISSN: 1535-7163 Impact factor: 6.261