Functional characterization of NPM1–TYK2 fusion oncogene

Sudhakiranmayi Kuravi; Riley W. Baker; Muhammad Umair Mushtaq; Irfan Saadi; Tara L. Lin; Carolyn J. Vivian; Anusha Valluripalli; Sunil Abhyankar; Siddhartha Ganguly; Wei Cui; Kojo S.J. Elenitoba-Johnson; Danny R. Welch; Roy A. Jensen; Yogen Saunthararajah; Joseph P. McGuirk; Ramesh Balusu

doi:10.1038/s41698-021-00246-4

Functional characterization of NPM1–TYK2 fusion oncogene

Sudhakiranmayi Kuravi, Riley W. Baker, Muhammad Umair Mushtaq, Irfan Saadi, Tara L. Lin, Carolyn J. Vivian, Anusha Valluripalli, Sunil Abhyankar, Siddhartha Ganguly, Wei Cui, Kojo S.J. Elenitoba-Johnson, Danny R. Welch, Roy A. Jensen, Yogen Saunthararajah, Joseph P. McGuirk, Ramesh Balusu

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

3 Scopus citations

Abstract

Gene fusions are known to drive many human cancers. Therefore, the functional characterization of newly discovered fusions is critical to understanding the oncobiology of these tumors and to enable therapeutic development. NPM1–TYK2 is a novel fusion identified in CD30 + lymphoproliferative disorders, and here we present the functional evaluation of this fusion gene as an oncogene. The chimeric protein consists of the amino-terminus of nucleophosmin 1 (NPM1) and the carboxyl-terminus of tyrosine kinase 2 (TYK2), including the kinase domain. Using in vitro lymphoid cell transformation assays and in vivo tumorigenic xenograft models we present direct evidence that the fusion gene is an oncogene. NPM1 fusion partner provides the critical homodimerization needed for the fusion kinase constitutive activation and downstream signaling that are responsible for cell transformation. As a result, our studies identify NPM1–TYK2 as a novel fusion oncogene and suggest that inhibition of fusion homodimerization could be a precision therapeutic approach in cutaneous T-cell lymphoma patients expressing this chimera.

Original language	English (US)
Article number	3
Pages (from-to)	3
Journal	npj Precision Oncology
Volume	6
Issue number	1
DOIs	https://doi.org/10.1038/s41698-021-00246-4
State	Published - Jan 18 2022

ASJC Scopus subject areas

Cancer Research
Oncology

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Kuravi, S., Baker, R. W., Mushtaq, M. U., Saadi, I., Lin, T. L., Vivian, C. J., Valluripalli, A., Abhyankar, S., Ganguly, S., Cui, W., Elenitoba-Johnson, K. S. J., Welch, D. R., Jensen, R. A., Saunthararajah, Y., McGuirk, J. P., & Balusu, R. (2022). Functional characterization of NPM1–TYK2 fusion oncogene. npj Precision Oncology, 6(1), 3. Article 3. https://doi.org/10.1038/s41698-021-00246-4

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title = "Functional characterization of NPM1–TYK2 fusion oncogene",

abstract = "Gene fusions are known to drive many human cancers. Therefore, the functional characterization of newly discovered fusions is critical to understanding the oncobiology of these tumors and to enable therapeutic development. NPM1–TYK2 is a novel fusion identified in CD30 + lymphoproliferative disorders, and here we present the functional evaluation of this fusion gene as an oncogene. The chimeric protein consists of the amino-terminus of nucleophosmin 1 (NPM1) and the carboxyl-terminus of tyrosine kinase 2 (TYK2), including the kinase domain. Using in vitro lymphoid cell transformation assays and in vivo tumorigenic xenograft models we present direct evidence that the fusion gene is an oncogene. NPM1 fusion partner provides the critical homodimerization needed for the fusion kinase constitutive activation and downstream signaling that are responsible for cell transformation. As a result, our studies identify NPM1–TYK2 as a novel fusion oncogene and suggest that inhibition of fusion homodimerization could be a precision therapeutic approach in cutaneous T-cell lymphoma patients expressing this chimera.",

author = "Sudhakiranmayi Kuravi and Baker, {Riley W.} and Mushtaq, {Muhammad Umair} and Irfan Saadi and Lin, {Tara L.} and Vivian, {Carolyn J.} and Anusha Valluripalli and Sunil Abhyankar and Siddhartha Ganguly and Wei Cui and Elenitoba-Johnson, {Kojo S.J.} and Welch, {Danny R.} and Jensen, {Roy A.} and Yogen Saunthararajah and McGuirk, {Joseph P.} and Ramesh Balusu",

note = "Funding Information: R. Balusu acknowledges the Sosland Family Foundation Research Award, Hale Family Foundation, Frontiers Clinical and Translational Pilot Award UL1T, and Lied Preclinical Pilot Award. R. Jensen is a recipient of P30-CA168524 from NCI. Publisher Copyright: {\textcopyright} 2022, The Author(s).",

year = "2022",

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doi = "10.1038/s41698-021-00246-4",

language = "English (US)",

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AU - Kuravi, Sudhakiranmayi

AU - Baker, Riley W.

AU - Mushtaq, Muhammad Umair

AU - Saadi, Irfan

AU - Lin, Tara L.

AU - Vivian, Carolyn J.

AU - Valluripalli, Anusha

AU - Abhyankar, Sunil

AU - Ganguly, Siddhartha

AU - Cui, Wei

AU - Elenitoba-Johnson, Kojo S.J.

AU - Welch, Danny R.

AU - Jensen, Roy A.

AU - Saunthararajah, Yogen

AU - McGuirk, Joseph P.

AU - Balusu, Ramesh

N1 - Funding Information: R. Balusu acknowledges the Sosland Family Foundation Research Award, Hale Family Foundation, Frontiers Clinical and Translational Pilot Award UL1T, and Lied Preclinical Pilot Award. R. Jensen is a recipient of P30-CA168524 from NCI. Publisher Copyright: © 2022, The Author(s).

PY - 2022/1/18

Y1 - 2022/1/18

N2 - Gene fusions are known to drive many human cancers. Therefore, the functional characterization of newly discovered fusions is critical to understanding the oncobiology of these tumors and to enable therapeutic development. NPM1–TYK2 is a novel fusion identified in CD30 + lymphoproliferative disorders, and here we present the functional evaluation of this fusion gene as an oncogene. The chimeric protein consists of the amino-terminus of nucleophosmin 1 (NPM1) and the carboxyl-terminus of tyrosine kinase 2 (TYK2), including the kinase domain. Using in vitro lymphoid cell transformation assays and in vivo tumorigenic xenograft models we present direct evidence that the fusion gene is an oncogene. NPM1 fusion partner provides the critical homodimerization needed for the fusion kinase constitutive activation and downstream signaling that are responsible for cell transformation. As a result, our studies identify NPM1–TYK2 as a novel fusion oncogene and suggest that inhibition of fusion homodimerization could be a precision therapeutic approach in cutaneous T-cell lymphoma patients expressing this chimera.

AB - Gene fusions are known to drive many human cancers. Therefore, the functional characterization of newly discovered fusions is critical to understanding the oncobiology of these tumors and to enable therapeutic development. NPM1–TYK2 is a novel fusion identified in CD30 + lymphoproliferative disorders, and here we present the functional evaluation of this fusion gene as an oncogene. The chimeric protein consists of the amino-terminus of nucleophosmin 1 (NPM1) and the carboxyl-terminus of tyrosine kinase 2 (TYK2), including the kinase domain. Using in vitro lymphoid cell transformation assays and in vivo tumorigenic xenograft models we present direct evidence that the fusion gene is an oncogene. NPM1 fusion partner provides the critical homodimerization needed for the fusion kinase constitutive activation and downstream signaling that are responsible for cell transformation. As a result, our studies identify NPM1–TYK2 as a novel fusion oncogene and suggest that inhibition of fusion homodimerization could be a precision therapeutic approach in cutaneous T-cell lymphoma patients expressing this chimera.

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Functional characterization of NPM1–TYK2 fusion oncogene

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