Binary pan-cancer classes with distinct vulnerabilities defined by pro- or anti-cancer YAP/TEAD activity

Joel D. Pearson; Katherine Huang; Marek Pacal; Sean R. McCurdy; Suying Lu; Arthur Aubry; Tao Yu; Kristine M. Wadosky; Letian Zhang; Tao Wang; Alex Gregorieff; Mohammad Ahmad; Helen Dimaras; Ellen Langille; Susan P.C. Cole; Philippe P. Monnier; Benjamin H. Lok; Ming Sound Tsao; Nagako Akeno; Daniel Schramek; Kathryn A. Wikenheiser-Brokamp; Erik S. Knudsen; Agnieszka K. Witkiewicz; Jeffrey L. Wrana; David W. Goodrich; Rod Bremner

doi:10.1016/j.ccell.2021.06.016

Binary pan-cancer classes with distinct vulnerabilities defined by pro- or anti-cancer YAP/TEAD activity

Joel D. Pearson, Katherine Huang, Marek Pacal, Sean R. McCurdy, Suying Lu, Arthur Aubry, Tao Yu, Kristine M. Wadosky, Letian Zhang, Tao Wang, Alex Gregorieff, Mohammad Ahmad, Helen Dimaras, Ellen Langille, Susan P.C. Cole, Philippe P. Monnier, Benjamin H. Lok, Ming Sound Tsao, Nagako Akeno, Daniel SchramekKathryn A. Wikenheiser-Brokamp, Erik S. Knudsen, Agnieszka K. Witkiewicz, Jeffrey L. Wrana, David W. Goodrich, Rod Bremner

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

78 Scopus citations

Abstract

Cancer heterogeneity impacts therapeutic response, driving efforts to discover over-arching rules that supersede variability. Here, we define pan-cancer binary classes based on distinct expression of YAP and YAP-responsive adhesion regulators. Combining informatics with in vivo and in vitro gain- and loss-of-function studies across multiple murine and human tumor types, we show that opposite pro- or anti-cancer YAP activity functionally defines binary YAP^on or YAP^off cancer classes that express or silence YAP, respectively. YAP^off solid cancers are neural/neuroendocrine and frequently RB1^−/−, such as retinoblastoma, small cell lung cancer, and neuroendocrine prostate cancer. YAP silencing is intrinsic to the cell of origin, or acquired with lineage switching and drug resistance. The binary cancer groups exhibit distinct YAP-dependent adhesive behavior and pharmaceutical vulnerabilities, underscoring clinical relevance. Mechanistically, distinct YAP/TEAD enhancers in YAP^off or YAP^on cancers deploy anti-cancer integrin or pro-cancer proliferative programs, respectively. YAP is thus pivotal across cancer, but in opposite ways, with therapeutic implications.

Original language	English (US)
Pages (from-to)	1115-1134.e12
Journal	Cancer Cell
Volume	39
Issue number	8
DOIs	https://doi.org/10.1016/j.ccell.2021.06.016
State	Published - Aug 9 2021
Externally published	Yes

Keywords

RB1
TAZ/WWTR1
TEAD
YAP
cancer plasticity
cancer stratification
neuroendocrine cancer
retinoblastoma
retinoma
small cell cancers

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1016/j.ccell.2021.06.016

Cite this

Pearson, J. D., Huang, K., Pacal, M., McCurdy, S. R., Lu, S., Aubry, A., Yu, T., Wadosky, K. M., Zhang, L., Wang, T., Gregorieff, A., Ahmad, M., Dimaras, H., Langille, E., Cole, S. P. C., Monnier, P. P., Lok, B. H., Tsao, M. S., Akeno, N., ... Bremner, R. (2021). Binary pan-cancer classes with distinct vulnerabilities defined by pro- or anti-cancer YAP/TEAD activity. Cancer Cell, 39(8), 1115-1134.e12. https://doi.org/10.1016/j.ccell.2021.06.016

Pearson, JD, Huang, K, Pacal, M, McCurdy, SR, Lu, S, Aubry, A, Yu, T, Wadosky, KM, Zhang, L, Wang, T, Gregorieff, A, Ahmad, M, Dimaras, H, Langille, E, Cole, SPC, Monnier, PP, Lok, BH, Tsao, MS, Akeno, N, Schramek, D, Wikenheiser-Brokamp, KA, Knudsen, ES, Witkiewicz, AK, Wrana, JL, Goodrich, DW & Bremner, R 2021, 'Binary pan-cancer classes with distinct vulnerabilities defined by pro- or anti-cancer YAP/TEAD activity', Cancer Cell, vol. 39, no. 8, pp. 1115-1134.e12. https://doi.org/10.1016/j.ccell.2021.06.016

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title = "Binary pan-cancer classes with distinct vulnerabilities defined by pro- or anti-cancer YAP/TEAD activity",

abstract = "Cancer heterogeneity impacts therapeutic response, driving efforts to discover over-arching rules that supersede variability. Here, we define pan-cancer binary classes based on distinct expression of YAP and YAP-responsive adhesion regulators. Combining informatics with in vivo and in vitro gain- and loss-of-function studies across multiple murine and human tumor types, we show that opposite pro- or anti-cancer YAP activity functionally defines binary YAPon or YAPoff cancer classes that express or silence YAP, respectively. YAPoff solid cancers are neural/neuroendocrine and frequently RB1−/−, such as retinoblastoma, small cell lung cancer, and neuroendocrine prostate cancer. YAP silencing is intrinsic to the cell of origin, or acquired with lineage switching and drug resistance. The binary cancer groups exhibit distinct YAP-dependent adhesive behavior and pharmaceutical vulnerabilities, underscoring clinical relevance. Mechanistically, distinct YAP/TEAD enhancers in YAPoff or YAPon cancers deploy anti-cancer integrin or pro-cancer proliferative programs, respectively. YAP is thus pivotal across cancer, but in opposite ways, with therapeutic implications.",

keywords = "RB1, TAZ/WWTR1, TEAD, YAP, cancer plasticity, cancer stratification, neuroendocrine cancer, retinoblastoma, retinoma, small cell cancers",

author = "Pearson, {Joel D.} and Katherine Huang and Marek Pacal and McCurdy, {Sean R.} and Suying Lu and Arthur Aubry and Tao Yu and Wadosky, {Kristine M.} and Letian Zhang and Tao Wang and Alex Gregorieff and Mohammad Ahmad and Helen Dimaras and Ellen Langille and Cole, {Susan P.C.} and Monnier, {Philippe P.} and Lok, {Benjamin H.} and Tsao, {Ming Sound} and Nagako Akeno and Daniel Schramek and Wikenheiser-Brokamp, {Kathryn A.} and Knudsen, {Erik S.} and Witkiewicz, {Agnieszka K.} and Wrana, {Jeffrey L.} and Goodrich, {David W.} and Rod Bremner",

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doi = "10.1016/j.ccell.2021.06.016",

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AU - Pearson, Joel D.

AU - Huang, Katherine

AU - Pacal, Marek

AU - McCurdy, Sean R.

AU - Lu, Suying

AU - Aubry, Arthur

AU - Yu, Tao

AU - Wadosky, Kristine M.

AU - Zhang, Letian

AU - Wang, Tao

AU - Gregorieff, Alex

AU - Ahmad, Mohammad

AU - Dimaras, Helen

AU - Langille, Ellen

AU - Cole, Susan P.C.

AU - Monnier, Philippe P.

AU - Lok, Benjamin H.

AU - Tsao, Ming Sound

AU - Akeno, Nagako

AU - Schramek, Daniel

AU - Wikenheiser-Brokamp, Kathryn A.

AU - Knudsen, Erik S.

AU - Witkiewicz, Agnieszka K.

AU - Wrana, Jeffrey L.

AU - Goodrich, David W.

AU - Bremner, Rod

PY - 2021/8/9

Y1 - 2021/8/9

N2 - Cancer heterogeneity impacts therapeutic response, driving efforts to discover over-arching rules that supersede variability. Here, we define pan-cancer binary classes based on distinct expression of YAP and YAP-responsive adhesion regulators. Combining informatics with in vivo and in vitro gain- and loss-of-function studies across multiple murine and human tumor types, we show that opposite pro- or anti-cancer YAP activity functionally defines binary YAPon or YAPoff cancer classes that express or silence YAP, respectively. YAPoff solid cancers are neural/neuroendocrine and frequently RB1−/−, such as retinoblastoma, small cell lung cancer, and neuroendocrine prostate cancer. YAP silencing is intrinsic to the cell of origin, or acquired with lineage switching and drug resistance. The binary cancer groups exhibit distinct YAP-dependent adhesive behavior and pharmaceutical vulnerabilities, underscoring clinical relevance. Mechanistically, distinct YAP/TEAD enhancers in YAPoff or YAPon cancers deploy anti-cancer integrin or pro-cancer proliferative programs, respectively. YAP is thus pivotal across cancer, but in opposite ways, with therapeutic implications.

AB - Cancer heterogeneity impacts therapeutic response, driving efforts to discover over-arching rules that supersede variability. Here, we define pan-cancer binary classes based on distinct expression of YAP and YAP-responsive adhesion regulators. Combining informatics with in vivo and in vitro gain- and loss-of-function studies across multiple murine and human tumor types, we show that opposite pro- or anti-cancer YAP activity functionally defines binary YAPon or YAPoff cancer classes that express or silence YAP, respectively. YAPoff solid cancers are neural/neuroendocrine and frequently RB1−/−, such as retinoblastoma, small cell lung cancer, and neuroendocrine prostate cancer. YAP silencing is intrinsic to the cell of origin, or acquired with lineage switching and drug resistance. The binary cancer groups exhibit distinct YAP-dependent adhesive behavior and pharmaceutical vulnerabilities, underscoring clinical relevance. Mechanistically, distinct YAP/TEAD enhancers in YAPoff or YAPon cancers deploy anti-cancer integrin or pro-cancer proliferative programs, respectively. YAP is thus pivotal across cancer, but in opposite ways, with therapeutic implications.

KW - RB1

KW - TAZ/WWTR1

KW - TEAD

KW - YAP

KW - cancer plasticity

KW - cancer stratification

KW - neuroendocrine cancer

KW - retinoblastoma

KW - retinoma

KW - small cell cancers

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M3 - Article

C2 - 34270926

AN - SCOPUS:85111943821

SN - 1535-6108

VL - 39

SP - 1115-1134.e12

JO - Cancer Cell

JF - Cancer Cell

IS - 8

ER -

Binary pan-cancer classes with distinct vulnerabilities defined by pro- or anti-cancer YAP/TEAD activity

Abstract

Keywords

ASJC Scopus subject areas

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