Publication:
LUBAC determines chemotherapy resistance in squamous cell lung cancer.

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Date

2018-12-18

Authors

Ruiz, E Josue
Diefenbacher, Markus E
Nelson, Jessica K
Sancho, Rocio
Pucci, Fabio
Chakraborty, Atanu
Moreno, Paula
Annibaldi, Alessandro
Liccardi, Gianmaria
Encheva, Vesela

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Rockefeller University Press
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Lung squamous cell carcinoma (LSCC) and adenocarcinoma (LADC) are the most common lung cancer subtypes. Molecular targeted treatments have improved LADC patient survival but are largely ineffective in LSCC. The tumor suppressor FBW7 is commonly mutated or down-regulated in human LSCC, and oncogenic KRasG12D activation combined with Fbxw7 inactivation in mice (KF model) caused both LSCC and LADC. Lineage-tracing experiments showed that CC10+, but not basal, cells are the cells of origin of LSCC in KF mice. KF LSCC tumors recapitulated human LSCC resistance to cisplatin-based chemotherapy, and we identified LUBAC-mediated NF-κB signaling as a determinant of chemotherapy resistance in human and mouse. Inhibition of NF-κB activation using TAK1 or LUBAC inhibitors resensitized LSCC tumors to cisplatin, suggesting a future avenue for LSCC patient treatment.

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MeSH Terms

Adenocarcinoma of lung
Animals
Carcinoma, squamous cell
Cisplatin
Drug resistance, neoplasm
Humans
Lung neoplasms
Mice
Multienzyme complexes
Proto-oncogene proteins p21(ras)
Ubiquitination

DeCS Terms

Adenocarcinoma del pulmón
Carcinoma de células escamosas
Cisplatino
Complejos multienzimáticos
Neoplasias pulmonares
Resistencia a antineoplásicos
Ubiquitinación

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Ruiz EJ, Diefenbacher ME, Nelson JK, Sancho R, Pucci F, Chakraborty A, et al. LUBAC determines chemotherapy resistance in squamous cell lung cancer. J Exp Med. 2019 Feb 4;216(2):450-465