Loss of prdm1a accelerates melanoma onset and progression

Ritsuko Iwanaga; Brittany T. Truong; Jessica Y. Hsu; Karoline A. Lambert; Rajesh Vyas; David Orlicky; Yiqun G. Shellman; Aik Choon Tan; Craig Ceol; Kristin Bruk Artinger

doi:10.1002/mc.23236

Loss of prdm1a accelerates melanoma onset and progression

Ritsuko Iwanaga, Brittany T. Truong, Jessica Y. Hsu, Karoline A. Lambert, Rajesh Vyas, David Orlicky, Yiqun G. Shellman, Aik Choon Tan, Craig Ceol, Kristin Bruk Artinger

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

8 Scopus citations

Abstract

Melanoma is an aggressive, deadly skin cancer derived from melanocytes, a neural crest cell derivative. Melanoma cells mirror the developmental program of neural crest cells in that they exhibit the same gene expression patterns and utilize similar cellular mechanisms, including increased cell proliferation, epithelial-mesenchymal transition, and migration. Here we studied the role of neural crest regulator PRDM1 in melanoma onset and progression. In development, Prdm1a functions to promote neural crest progenitor fate, and in melanoma, we found that PRDM1 has reduced copy number and is recurrently deleted in both zebrafish and humans. When examining expression of neural crest and melanocyte development genes, we show that sox10 progenitor expression is high in prdm1a^−/− mutants, while more differentiated melanocyte markers are reduced, suggesting that normally Prdm1a is required for differentiation. Data mining of human melanoma datasets indicates that high PRDM1 expression in human melanoma is correlated with better patient survival and decreased PRDM1 expression is common in metastatic tumors. When one copy of prdm1a is lost in the zebrafish melanoma model Tg(mitfa:BRAF^V600E);p53^−/−;prdm1a^+/−, melanoma onset occurs more quickly, and the tumors that form have a larger area with increased expression of sox10. These data demonstrate a novel role for PRDM1 as a tumor suppressor in melanoma.

Original language	English (US)
Pages (from-to)	1052-1063
Number of pages	12
Journal	Molecular Carcinogenesis
Volume	59
Issue number	9
DOIs	https://doi.org/10.1002/mc.23236
State	Published - Sep 1 2020

Bibliographical note

Funding Information:
We thank the Artinger and Shellman labs for experimental feedback; Morgan Singleton and UCD‐AMC CLAC for zebrafish care; Virginia Ware and Aaron Clark for technical help with experiments; and Richard White for sharing microarray data, fish lines, and advice. This work is supported by pilot grants from the Skin Disease Research Center at the University of Colorado Anschutz Medical Campus P30AR057212‐10, The State of Colorado, Tobacco Settlement funds pilot grants, and P30CA046934 to the University of Colorado Cancer Center.

Funding Information:
We thank the Artinger and Shellman labs for experimental feedback; Morgan Singleton and UCD-AMC CLAC for zebrafish care; Virginia Ware and Aaron Clark for technical help with experiments; and Richard White for sharing microarray data, fish lines, and advice. This work is supported by pilot grants from the Skin Disease Research Center at the University of Colorado Anschutz Medical Campus P30AR057212-10, The State of Colorado, Tobacco Settlement funds pilot grants, and P30CA046934 to the University of Colorado Cancer Center.

Publisher Copyright:
© 2020 Wiley Periodicals LLC

Keywords

melanoma
neural crest cells
PRDM1
zebrafish

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This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1002/mc.23236

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title = "Loss of prdm1a accelerates melanoma onset and progression",

abstract = "Melanoma is an aggressive, deadly skin cancer derived from melanocytes, a neural crest cell derivative. Melanoma cells mirror the developmental program of neural crest cells in that they exhibit the same gene expression patterns and utilize similar cellular mechanisms, including increased cell proliferation, epithelial-mesenchymal transition, and migration. Here we studied the role of neural crest regulator PRDM1 in melanoma onset and progression. In development, Prdm1a functions to promote neural crest progenitor fate, and in melanoma, we found that PRDM1 has reduced copy number and is recurrently deleted in both zebrafish and humans. When examining expression of neural crest and melanocyte development genes, we show that sox10 progenitor expression is high in prdm1a−/− mutants, while more differentiated melanocyte markers are reduced, suggesting that normally Prdm1a is required for differentiation. Data mining of human melanoma datasets indicates that high PRDM1 expression in human melanoma is correlated with better patient survival and decreased PRDM1 expression is common in metastatic tumors. When one copy of prdm1a is lost in the zebrafish melanoma model Tg(mitfa:BRAFV600E);p53−/−;prdm1a+/−, melanoma onset occurs more quickly, and the tumors that form have a larger area with increased expression of sox10. These data demonstrate a novel role for PRDM1 as a tumor suppressor in melanoma.",

keywords = "melanoma, neural crest cells, PRDM1, zebrafish",

author = "Ritsuko Iwanaga and Truong, \{Brittany T.\} and Hsu, \{Jessica Y.\} and Lambert, \{Karoline A.\} and Rajesh Vyas and David Orlicky and Shellman, \{Yiqun G.\} and Tan, \{Aik Choon\} and Craig Ceol and Artinger, \{Kristin Bruk\}",

note = "Funding Information: We thank the Artinger and Shellman labs for experimental feedback; Morgan Singleton and UCD‐AMC CLAC for zebrafish care; Virginia Ware and Aaron Clark for technical help with experiments; and Richard White for sharing microarray data, fish lines, and advice. This work is supported by pilot grants from the Skin Disease Research Center at the University of Colorado Anschutz Medical Campus P30AR057212‐10, The State of Colorado, Tobacco Settlement funds pilot grants, and P30CA046934 to the University of Colorado Cancer Center. Funding Information: We thank the Artinger and Shellman labs for experimental feedback; Morgan Singleton and UCD-AMC CLAC for zebrafish care; Virginia Ware and Aaron Clark for technical help with experiments; and Richard White for sharing microarray data, fish lines, and advice. This work is supported by pilot grants from the Skin Disease Research Center at the University of Colorado Anschutz Medical Campus P30AR057212-10, The State of Colorado, Tobacco Settlement funds pilot grants, and P30CA046934 to the University of Colorado Cancer Center. Publisher Copyright: {\textcopyright} 2020 Wiley Periodicals LLC",

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doi = "10.1002/mc.23236",

language = "English (US)",

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AU - Iwanaga, Ritsuko

AU - Truong, Brittany T.

AU - Hsu, Jessica Y.

AU - Lambert, Karoline A.

AU - Vyas, Rajesh

AU - Orlicky, David

AU - Shellman, Yiqun G.

AU - Tan, Aik Choon

AU - Ceol, Craig

AU - Artinger, Kristin Bruk

N1 - Funding Information: We thank the Artinger and Shellman labs for experimental feedback; Morgan Singleton and UCD‐AMC CLAC for zebrafish care; Virginia Ware and Aaron Clark for technical help with experiments; and Richard White for sharing microarray data, fish lines, and advice. This work is supported by pilot grants from the Skin Disease Research Center at the University of Colorado Anschutz Medical Campus P30AR057212‐10, The State of Colorado, Tobacco Settlement funds pilot grants, and P30CA046934 to the University of Colorado Cancer Center. Funding Information: We thank the Artinger and Shellman labs for experimental feedback; Morgan Singleton and UCD-AMC CLAC for zebrafish care; Virginia Ware and Aaron Clark for technical help with experiments; and Richard White for sharing microarray data, fish lines, and advice. This work is supported by pilot grants from the Skin Disease Research Center at the University of Colorado Anschutz Medical Campus P30AR057212-10, The State of Colorado, Tobacco Settlement funds pilot grants, and P30CA046934 to the University of Colorado Cancer Center. Publisher Copyright: © 2020 Wiley Periodicals LLC

PY - 2020/9/1

Y1 - 2020/9/1

N2 - Melanoma is an aggressive, deadly skin cancer derived from melanocytes, a neural crest cell derivative. Melanoma cells mirror the developmental program of neural crest cells in that they exhibit the same gene expression patterns and utilize similar cellular mechanisms, including increased cell proliferation, epithelial-mesenchymal transition, and migration. Here we studied the role of neural crest regulator PRDM1 in melanoma onset and progression. In development, Prdm1a functions to promote neural crest progenitor fate, and in melanoma, we found that PRDM1 has reduced copy number and is recurrently deleted in both zebrafish and humans. When examining expression of neural crest and melanocyte development genes, we show that sox10 progenitor expression is high in prdm1a−/− mutants, while more differentiated melanocyte markers are reduced, suggesting that normally Prdm1a is required for differentiation. Data mining of human melanoma datasets indicates that high PRDM1 expression in human melanoma is correlated with better patient survival and decreased PRDM1 expression is common in metastatic tumors. When one copy of prdm1a is lost in the zebrafish melanoma model Tg(mitfa:BRAFV600E);p53−/−;prdm1a+/−, melanoma onset occurs more quickly, and the tumors that form have a larger area with increased expression of sox10. These data demonstrate a novel role for PRDM1 as a tumor suppressor in melanoma.

AB - Melanoma is an aggressive, deadly skin cancer derived from melanocytes, a neural crest cell derivative. Melanoma cells mirror the developmental program of neural crest cells in that they exhibit the same gene expression patterns and utilize similar cellular mechanisms, including increased cell proliferation, epithelial-mesenchymal transition, and migration. Here we studied the role of neural crest regulator PRDM1 in melanoma onset and progression. In development, Prdm1a functions to promote neural crest progenitor fate, and in melanoma, we found that PRDM1 has reduced copy number and is recurrently deleted in both zebrafish and humans. When examining expression of neural crest and melanocyte development genes, we show that sox10 progenitor expression is high in prdm1a−/− mutants, while more differentiated melanocyte markers are reduced, suggesting that normally Prdm1a is required for differentiation. Data mining of human melanoma datasets indicates that high PRDM1 expression in human melanoma is correlated with better patient survival and decreased PRDM1 expression is common in metastatic tumors. When one copy of prdm1a is lost in the zebrafish melanoma model Tg(mitfa:BRAFV600E);p53−/−;prdm1a+/−, melanoma onset occurs more quickly, and the tumors that form have a larger area with increased expression of sox10. These data demonstrate a novel role for PRDM1 as a tumor suppressor in melanoma.

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ER -

Loss of prdm1a accelerates melanoma onset and progression

Abstract

Bibliographical note

Keywords

UN SDGs

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