Targeting GOF p53 and c-MYC through LZK inhibition or degradation suppresses head and neck tumor growth
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Authors
Funk, A. L.Katerji, M.
Afifi, M.
Nyswaner, K.
Woodroofe, C. C.
Edwards, Zoe C
Lindberg, E.
Bergman, K. L.
Gough, N. R.
Rubin, M. R.
Karpińska, K.
Trotter, Eleanor W
Dash, S.
Ries, A. L.
James, A.
Robinson, C. M.
Difilippantonio, S.
Karim, B. O.
Chang, T. C.
Chen, L.
Xu, X.
Doroshow, J. H.
Ahel, I.
Marusiak, A. A.
Swenson, R. E.
Cappell, S. D.
Brognard, J.
Affiliation
Cell Division Group, Cancer Research UK Manchester Institute, The University of Manchester, Manchester M20 4BX, UK.Issue Date
2024
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The worldwide frequency of head and neck squamous cell carcinoma (HNSCC) is approximately 800,000 new cases, with 430,000 deaths annually. We determined that LZK (encoded by MAP3K13) is a therapeutic target in HNSCC and showed that inhibition with small molecule inhibitors decreases the viability of HNSCC cells with amplified MAP3K13. A drug-resistant mutant of LZK blocks decreases in cell viability due to LZK inhibition, indicating on-target activity by two separate small molecules. Inhibition of LZK catalytic activity suppressed tumor growth in HNSCC PDX models with amplified MAP3K13. We found that the kinase activity of LZK stabilized c-MYC and that LZK stabilized gain-of-function (GOF) p53 through a kinase-independent mechanism. Therefore, we designed proteolysis-targeting chimeras (PROTACs) and demonstrate that our lead PROTAC promotes LZK degradation and suppresses expression of GOF p53 and c-MYC leading to impaired viability of HNSCC cell lines. This research provides a strong basis for development of therapeutics targeting LZK in HNSCCs with amplification of the gene.Citation
Funk AL, Katerji M, Afifi M, Nyswaner K, Woodroofe CC, Edwards ZC, et al. Targeting GOF p53 and c-MYC through LZK Inhibition or Degradation Suppresses Head and Neck Tumor Growth. bioRxiv : the preprint server for biology. 2024 Nov 20. PubMed PMID: 39605563. Pubmed Central PMCID: PMC11601640 Institute (NCI) with inventors John Brognard, Rolf Swenson, Caroyln C. Woodroofe, Amy L. Funk, Meghri Katerji, Knickole Bergman, Steve Cappell, and Katherine Nyswaner for the development of novel inhibitors and PROTACs to target LZK in HNSCC to promote tumor regression and suppress c-MYC expression. There are no other conflicts of interest for any authors. Epub 2024/11/28. eng.Journal
bioRxivDOI
10.1101/2024.11.19.623840PubMed ID
39605563Additional Links
https://dx.doi.org/10.1101/2024.11.19.623840Type
PreprintLanguage
enae974a485f413a2113503eed53cd6c53
10.1101/2024.11.19.623840
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