In vivo phosphoproteomics reveals kinase activity profiles that predict treatment outcome in triple-negative breast cancer
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2018-08-29
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Abstract
Triple-negative breast cancer (TNBC) lacks prognostic and predictive markers. Here, we use high-throughput phosphoproteomics to build a functional TNBC taxonomy. A cluster of 159 phosphosites is upregulated in relapsed cases of a training set (n = 34 patients), with 11 hyperactive kinases accounting for this phosphoprofile. A mass-spectrometry-to-immunohistochemistry translation step, assessing 2 independent validation sets, reveals 6 kinases with preserved independent prognostic value. The kinases split the validation set into two patterns: one without hyperactive kinases being associated with a >90% relapse-free rate, and the other one showing ≥1 hyperactive kinase and being associated with an up to 9.5-fold higher relapse risk. Each kinase pattern encompasses different mutational patterns, simplifying mutation-based taxonomy. Drug regimens designed based on these 6 kinases show promising antitumour activity in TNBC cell lines and patient-derived xenografts. In summary, the present study elucidates phosphosites and kinases implicated in TNBC and suggests a target-based clinical classification system for TNBC.
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SDG 3 - Good Health and Well-being
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Zagorac, I, Fernandez-Gaitero, S, Penning, R, Post, H, Bueno, M J, Mouron, S, Manso, L, Morente, M M, Alonso, S, Serra, V, Muñoz, J, Gómez-López, G, Lopez-Acosta, J F, Jimenez-Renard, V, Gris-Oliver, A, Al-Shahrour, F, Piñeiro-Yañez, E, Montoya-Suarez, J L, Apala, J V, Moreno-Torres, A, Colomer, R, Dopazo, A, Heck, A J R, Altelaar, M & Quintela-Fandino, M 2018, 'In vivo phosphoproteomics reveals kinase activity profiles that predict treatment outcome in triple-negative breast cancer', Nature Communications, vol. 9, no. 1, 3501. https://doi.org/10.1038/s41467-018-05742-z