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NUMB is a tumor suppressor gene that functions by inhibiting the action of the NOTCH proto-oncogene and enhancing the levels and activity of the tumor suppressor protein p53. In breast cancer (BC), NUMB loss of function (LOF), mediated by various molecular mechanisms, is a frequent and causal event. Herein, it is established that loss of NUMB protein, resulting from protein hyper-degradation, is the prevalent mechanism of NUMB LOF in BC. Through an RNAi-based screening, the CRL7FBXW8 complex is identified as the E3 ligase complex responsible for NUMB hyper-degradation in BC. Genetic and pharmacological inhibition of CRL7FBXW8 rescues the transformation-related phenotypes induced by NUMB LOF in BC cell lines and in patient-derived xenografts. These effects are directly dependent on the restoration of NUMB protein levels. Thus, enhanced CRL7FBXW8 activity, through its interference with the tumor suppressor activity of NUMB, is a causal alteration in BC, suggesting it as a potential therapeutic target for precision medicine.

The CRL7FBXW8 Complex Controls the Mammary Stem Cell Compartment through Regulation of NUMB Levels / S. Sabbioni, M.G. Filippone, L. Amadori, S. Confalonieri, R. Bonfanti, S. Capoano, I.N. Colaluca, S. Freddi, G. Bertalot, G. Fagà, E. Zagarrí, M. Varasi, R.H. Gunby, C. Mercurio, S. Pece, P.P. Di Fiore, D. Tosoni. - In: ADVANCED SCIENCE. - ISSN 2198-3844. - 12:25(2025 Jul 03), pp. 2405812.1-2405812.17. [10.1002/advs.202405812]

The CRL7FBXW8 Complex Controls the Mammary Stem Cell Compartment through Regulation of NUMB Levels

S. Sabbioni
Primo
;M.G. Filippone
Secondo
;L. Amadori;R. Bonfanti;S. Capoano;S. Freddi;S. Pece;P.P. Di Fiore
Penultimo
;D. Tosoni
Ultimo
2025

Abstract

NUMB is a tumor suppressor gene that functions by inhibiting the action of the NOTCH proto-oncogene and enhancing the levels and activity of the tumor suppressor protein p53. In breast cancer (BC), NUMB loss of function (LOF), mediated by various molecular mechanisms, is a frequent and causal event. Herein, it is established that loss of NUMB protein, resulting from protein hyper-degradation, is the prevalent mechanism of NUMB LOF in BC. Through an RNAi-based screening, the CRL7FBXW8 complex is identified as the E3 ligase complex responsible for NUMB hyper-degradation in BC. Genetic and pharmacological inhibition of CRL7FBXW8 rescues the transformation-related phenotypes induced by NUMB LOF in BC cell lines and in patient-derived xenografts. These effects are directly dependent on the restoration of NUMB protein levels. Thus, enhanced CRL7FBXW8 activity, through its interference with the tumor suppressor activity of NUMB, is a causal alteration in BC, suggesting it as a potential therapeutic target for precision medicine.
CRL7FBXW8 complex; NUMB; breast cancer; cancer stem cells; proteasomal degradation;
Settore MEDS-02/A - Patologia generale
3-lug-2025
ADVANCED SCIENCE
Article (author)
01 - Articolo su periodico
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/1202225
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