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Literature DB >> 28210003

Differential signaling through p190 and p210 BCR-ABL fusion proteins revealed by interactome and phosphoproteome analysis.

J A Cutler^1,2,3, R Tahir^4,5, S K Sreenivasamurthy^4,6, C Mitchell^5,7, S Renuse^4,8, R S Nirujogi^4,6, A H Patil^4,6,9, M Heydarian^2,3, X Wong¹⁰, X Wu^2,4, T-C Huang^1,4,11, M-S Kim^2,4,12, K L Reddy^2,3,13, A Pandey^2,4,8,14.

Abstract

Two major types of leukemogenic BCR-ABL fusion proteins are p190BCR-ABLand p210BCR-ABL. Although the two fusion proteins are closely related, they can lead to different clinical outcomes. A thorough understanding of the signaling programs employed by these two fusion proteins is necessary to explain these clinical differences. We took an integrated approach by coupling protein-protein interaction analysis using biotinylation identification with global phosphorylation analysis to investigate the differences in signaling between these two fusion proteins. Our findings suggest that p190BCR-ABL and p210BCR-ABL differentially activate important signaling pathways, such as JAK-STAT, and engage with molecules that indicate interaction with different subcellular compartments. In the case of p210BCR-ABL, we observed an increased engagement of molecules active proximal to the membrane and in the case of p190BCR-ABL, an engagement of molecules of the cytoskeleton. These differences in signaling could underlie the distinct leukemogenic process induced by these two protein variants.

Entities: Gene

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Year: 2017 PMID： 28210003 DOI： 10.1038/leu.2017.61

Source DB: PubMed Journal: Leukemia ISSN： 0887-6924 Impact factor: 11.528

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