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

J. A. Cutler; R. Tahir; S. K. Sreenivasamurthy; C. Mitchell; S. Renuse; R. S. Nirujogi; A. H. Patil; M. Heydarian; X. Wong; X. Wu; T. C. Huang; M. S. Kim; K. L. Reddy; A. Pandey

doi:10.1038/leu.2017.61

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

J. A. Cutler, R. Tahir, S. K. Sreenivasamurthy, C. Mitchell, S. Renuse, R. S. Nirujogi, A. H. Patil, M. Heydarian, X. Wong, X. Wu, T. C. Huang, M. S. Kim, K. L. Reddy, A. Pandey

Department of New Biology

Research output: Contribution to journal › Article › peer-review

40 Scopus citations

Abstract

Two major types of leukemogenic BCR-ABL fusion proteins are p190^BCR-ABL and p210^BCR-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 p190^BCR-ABL and p210^BCR-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 p210^BCR-ABL, we observed an increased engagement of molecules active proximal to the membrane and in the case of p190^BCR-ABL, an engagement of molecules of the cytoskeleton. These differences in signaling could underlie the distinct leukemogenic process induced by these two protein variants.

Original language	English
Pages (from-to)	1513-1524
Number of pages	12
Journal	Leukemia
Volume	31
Issue number	7
DOIs	https://doi.org/10.1038/leu.2017.61
State	Published - 1 Jul 2017

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© 2017 Macmillan Publishers Limited, part of Springer Nature. All rights reserved.

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Cutler, J. A., Tahir, R., Sreenivasamurthy, S. K., Mitchell, C., Renuse, S., Nirujogi, R. S., Patil, A. H., Heydarian, M., Wong, X., Wu, X., Huang, T. C., Kim, M. S., Reddy, K. L., & Pandey, A. (2017). Differential signaling through p190 and p210 BCR-ABL fusion proteins revealed by interactome and phosphoproteome analysis. Leukemia, 31(7), 1513-1524. https://doi.org/10.1038/leu.2017.61

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title = "Differential signaling through p190 and p210 BCR-ABL fusion proteins revealed by interactome and phosphoproteome analysis",

abstract = "Two major types of leukemogenic BCR-ABL fusion proteins are p190BCR-ABL and 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.",

author = "Cutler, {J. A.} and R. Tahir and Sreenivasamurthy, {S. K.} and C. Mitchell and S. Renuse and Nirujogi, {R. S.} and Patil, {A. H.} and M. Heydarian and X. Wong and X. Wu and Huang, {T. C.} and Kim, {M. S.} and Reddy, {K. L.} and A. Pandey",

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Cutler, JA, Tahir, R, Sreenivasamurthy, SK, Mitchell, C, Renuse, S, Nirujogi, RS, Patil, AH, Heydarian, M, Wong, X, Wu, X, Huang, TC, Kim, MS, Reddy, KL & Pandey, A 2017, 'Differential signaling through p190 and p210 BCR-ABL fusion proteins revealed by interactome and phosphoproteome analysis', Leukemia, vol. 31, no. 7, pp. 1513-1524. https://doi.org/10.1038/leu.2017.61

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AU - Cutler, J. A.

AU - Tahir, R.

AU - Sreenivasamurthy, S. K.

AU - Mitchell, C.

AU - Renuse, S.

AU - Nirujogi, R. S.

AU - Patil, A. H.

AU - Heydarian, M.

AU - Wong, X.

AU - Wu, X.

AU - Huang, T. C.

AU - Kim, M. S.

AU - Reddy, K. L.

AU - Pandey, A.

PY - 2017/7/1

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AB - Two major types of leukemogenic BCR-ABL fusion proteins are p190BCR-ABL and 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.

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

Abstract

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