Genetic screens identify a context-specific pi3k/p27kip1 node driving extrahepatic biliary cancer

Chiara Falcomatà; Stefanie Bärthel; Angelika Ulrich; Sandra Diersch; Christian Veltkamp; Lena Rad; Fabio Boniolo; Myriam Solar; Katja Steiger; Barbara Seidler; Magdalena Zukowska; Joanna Madej; Mingsong Wang; Rupert Öllinger; Roman Maresch; Maxim Barenboim; Stefan Eser; Markus Tschurtschenthaler; Arianeb Mehrabi; Stephanie Roessler; Benjamin Goeppert; Alexander Kind; Angelika Schnieke; Maria S. Robles; Allan Bradley; Roland M. Schmid; Marc Schmidt-Supprian; Maximilian Reichert; Wilko Weichert; Owen J. Sansom; Jennifer P. Morton; Roland Rad; Günter Schneider; Dieter Saur

doi:10.1158/2159-8290.CD-21-0209

Genetic screens identify a context-specific pi3k/p27^kip1 node driving extrahepatic biliary cancer

Chiara Falcomatà
, Stefanie Bärthel
, Angelika Ulrich
, Sandra Diersch
, Christian Veltkamp
, Lena Rad
, Fabio Boniolo
, Myriam Solar
, Katja Steiger
, Barbara Seidler
, Magdalena Zukowska
, Joanna Madej
, Mingsong Wang
, Rupert Öllinger
, Roman Maresch
, Maxim Barenboim
, Stefan Eser
, Markus Tschurtschenthaler
, Arianeb Mehrabi
, Stephanie Roessler

Benjamin Goeppert, Alexander Kind, Angelika Schnieke, Maria S. Robles, Allan Bradley, Roland M. Schmid, Marc Schmidt-Supprian, Maximilian Reichert, Wilko Weichert, Owen J. Sansom, Jennifer P. Morton, Roland Rad, Günter Schneider, Dieter Saur

German Cancer Research Center
Technical University of Munich
Department of Pathology
Heidelberg University
University of Munich
Wellcome Sanger Institute
University of Glasgow
University Medical Center

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

19 Scopus citations

Abstract

Biliary tract cancer ranks among the most lethal human malignancies, representing an unmet clinical need. Its abysmal prognosis is tied to an increasing incidence and a fundamental lack of mechanistic knowledge regarding the molecular basis of the disease. Here, we show that the Pdx1-positive extrahepatic biliary epithelium is highly susceptible toward transformation by activated PIK3CA^H1047R but refractory to oncogenic Kras^G12D. Using genome-wide transposon screens and genetic loss-of-function experiments, we discover context-dependent genetic interactions that drive extrahepatic cholangiocarcinoma (ECC) and show that PI3K signaling output strength and repression of the tumor suppressor p27^Kip1 are critical context-specific determinants of tumor formation. This contrasts with the pancreas, where oncogenic Kras in concert with p53 loss is a key cancer driver. Notably, inactivation of p27^Kip1 permits Kras^G12D-driven ECC development. These studies provide a mechanistic link between PI3K signaling, tissue-specific tumor suppressor barriers, and ECC pathogenesis, and present a novel genetic model of autochthonous ECC and genes driving this highly lethal tumor subtype. SIGNIFICANCE: We used the first genetically engineered mouse model for extrahepatic bile duct carcinoma to identify cancer genes by genome-wide transposon-based mutagenesis screening. Thereby, we show that PI3K signaling output strength and p27^Kip1 function are critical determinants for contextspecific ECC formation.

Original language	English
Pages (from-to)	3158-3177
Number of pages	20
Journal	Cancer Discovery
Volume	11
Issue number	12
DOIs	https://doi.org/10.1158/2159-8290.CD-21-0209
State	Published - Dec 2021

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10.1158/2159-8290.CD-21-0209

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Falcomatà, C., Bärthel, S., Ulrich, A., Diersch, S., Veltkamp, C., Rad, L., Boniolo, F., Solar, M., Steiger, K., Seidler, B., Zukowska, M., Madej, J., Wang, M., Öllinger, R., Maresch, R., Barenboim, M., Eser, S., Tschurtschenthaler, M., Mehrabi, A., ... Saur, D. (2021). Genetic screens identify a context-specific pi3k/p27^kip1 node driving extrahepatic biliary cancer. Cancer Discovery, 11(12), 3158-3177. https://doi.org/10.1158/2159-8290.CD-21-0209

@article{7ff6f879c8d24e258e7f6f7d1e3e81ac,

title = "Genetic screens identify a context-specific pi3k/p27kip1 node driving extrahepatic biliary cancer",

abstract = "Biliary tract cancer ranks among the most lethal human malignancies, representing an unmet clinical need. Its abysmal prognosis is tied to an increasing incidence and a fundamental lack of mechanistic knowledge regarding the molecular basis of the disease. Here, we show that the Pdx1-positive extrahepatic biliary epithelium is highly susceptible toward transformation by activated PIK3CAH1047R but refractory to oncogenic KrasG12D. Using genome-wide transposon screens and genetic loss-of-function experiments, we discover context-dependent genetic interactions that drive extrahepatic cholangiocarcinoma (ECC) and show that PI3K signaling output strength and repression of the tumor suppressor p27Kip1 are critical context-specific determinants of tumor formation. This contrasts with the pancreas, where oncogenic Kras in concert with p53 loss is a key cancer driver. Notably, inactivation of p27Kip1 permits KrasG12D-driven ECC development. These studies provide a mechanistic link between PI3K signaling, tissue-specific tumor suppressor barriers, and ECC pathogenesis, and present a novel genetic model of autochthonous ECC and genes driving this highly lethal tumor subtype. SIGNIFICANCE: We used the first genetically engineered mouse model for extrahepatic bile duct carcinoma to identify cancer genes by genome-wide transposon-based mutagenesis screening. Thereby, we show that PI3K signaling output strength and p27Kip1 function are critical determinants for contextspecific ECC formation.",

author = "Chiara Falcomat{\`a} and Stefanie B{\"a}rthel and Angelika Ulrich and Sandra Diersch and Christian Veltkamp and Lena Rad and Fabio Boniolo and Myriam Solar and Katja Steiger and Barbara Seidler and Magdalena Zukowska and Joanna Madej and Mingsong Wang and Rupert {\"O}llinger and Roman Maresch and Maxim Barenboim and Stefan Eser and Markus Tschurtschenthaler and Arianeb Mehrabi and Stephanie Roessler and Benjamin Goeppert and Alexander Kind and Angelika Schnieke and Robles, \{Maria S.\} and Allan Bradley and Schmid, \{Roland M.\} and Marc Schmidt-Supprian and Maximilian Reichert and Wilko Weichert and Sansom, \{Owen J.\} and Morton, \{Jennifer P.\} and Roland Rad and G{\"u}nter Schneider and Dieter Saur",

year = "2021",

month = dec,

doi = "10.1158/2159-8290.CD-21-0209",

language = "English",

volume = "11",

pages = "3158--3177",

journal = "Cancer Discovery",

issn = "2159-8274",

publisher = "American Association for Cancer Research Inc.",

number = "12",

}

Falcomatà, C, Bärthel, S, Ulrich, A, Diersch, S, Veltkamp, C, Rad, L, Boniolo, F, Solar, M, Steiger, K, Seidler, B, Zukowska, M, Madej, J, Wang, M, Öllinger, R, Maresch, R, Barenboim, M, Eser, S, Tschurtschenthaler, M, Mehrabi, A, Roessler, S, Goeppert, B, Kind, A, Schnieke, A, Robles, MS, Bradley, A, Schmid, RM, Schmidt-Supprian, M , Reichert, M , Weichert, W, Sansom, OJ, Morton, JP, Rad, R, Schneider, G & Saur, D 2021, 'Genetic screens identify a context-specific pi3k/p27^kip1 node driving extrahepatic biliary cancer', Cancer Discovery, vol. 11, no. 12, pp. 3158-3177. https://doi.org/10.1158/2159-8290.CD-21-0209

TY - JOUR

T1 - Genetic screens identify a context-specific pi3k/p27kip1 node driving extrahepatic biliary cancer

AU - Falcomatà, Chiara

AU - Bärthel, Stefanie

AU - Ulrich, Angelika

AU - Diersch, Sandra

AU - Veltkamp, Christian

AU - Rad, Lena

AU - Boniolo, Fabio

AU - Solar, Myriam

AU - Steiger, Katja

AU - Seidler, Barbara

AU - Zukowska, Magdalena

AU - Madej, Joanna

AU - Wang, Mingsong

AU - Öllinger, Rupert

AU - Maresch, Roman

AU - Barenboim, Maxim

AU - Eser, Stefan

AU - Tschurtschenthaler, Markus

AU - Mehrabi, Arianeb

AU - Roessler, Stephanie

AU - Goeppert, Benjamin

AU - Kind, Alexander

AU - Schnieke, Angelika

AU - Robles, Maria S.

AU - Bradley, Allan

AU - Schmid, Roland M.

AU - Schmidt-Supprian, Marc

AU - Reichert, Maximilian

AU - Weichert, Wilko

AU - Sansom, Owen J.

AU - Morton, Jennifer P.

AU - Rad, Roland

AU - Schneider, Günter

AU - Saur, Dieter

PY - 2021/12

Y1 - 2021/12

N2 - Biliary tract cancer ranks among the most lethal human malignancies, representing an unmet clinical need. Its abysmal prognosis is tied to an increasing incidence and a fundamental lack of mechanistic knowledge regarding the molecular basis of the disease. Here, we show that the Pdx1-positive extrahepatic biliary epithelium is highly susceptible toward transformation by activated PIK3CAH1047R but refractory to oncogenic KrasG12D. Using genome-wide transposon screens and genetic loss-of-function experiments, we discover context-dependent genetic interactions that drive extrahepatic cholangiocarcinoma (ECC) and show that PI3K signaling output strength and repression of the tumor suppressor p27Kip1 are critical context-specific determinants of tumor formation. This contrasts with the pancreas, where oncogenic Kras in concert with p53 loss is a key cancer driver. Notably, inactivation of p27Kip1 permits KrasG12D-driven ECC development. These studies provide a mechanistic link between PI3K signaling, tissue-specific tumor suppressor barriers, and ECC pathogenesis, and present a novel genetic model of autochthonous ECC and genes driving this highly lethal tumor subtype. SIGNIFICANCE: We used the first genetically engineered mouse model for extrahepatic bile duct carcinoma to identify cancer genes by genome-wide transposon-based mutagenesis screening. Thereby, we show that PI3K signaling output strength and p27Kip1 function are critical determinants for contextspecific ECC formation.

AB - Biliary tract cancer ranks among the most lethal human malignancies, representing an unmet clinical need. Its abysmal prognosis is tied to an increasing incidence and a fundamental lack of mechanistic knowledge regarding the molecular basis of the disease. Here, we show that the Pdx1-positive extrahepatic biliary epithelium is highly susceptible toward transformation by activated PIK3CAH1047R but refractory to oncogenic KrasG12D. Using genome-wide transposon screens and genetic loss-of-function experiments, we discover context-dependent genetic interactions that drive extrahepatic cholangiocarcinoma (ECC) and show that PI3K signaling output strength and repression of the tumor suppressor p27Kip1 are critical context-specific determinants of tumor formation. This contrasts with the pancreas, where oncogenic Kras in concert with p53 loss is a key cancer driver. Notably, inactivation of p27Kip1 permits KrasG12D-driven ECC development. These studies provide a mechanistic link between PI3K signaling, tissue-specific tumor suppressor barriers, and ECC pathogenesis, and present a novel genetic model of autochthonous ECC and genes driving this highly lethal tumor subtype. SIGNIFICANCE: We used the first genetically engineered mouse model for extrahepatic bile duct carcinoma to identify cancer genes by genome-wide transposon-based mutagenesis screening. Thereby, we show that PI3K signaling output strength and p27Kip1 function are critical determinants for contextspecific ECC formation.

UR - https://www.scopus.com/pages/publications/85121982407

U2 - 10.1158/2159-8290.CD-21-0209

DO - 10.1158/2159-8290.CD-21-0209

M3 - Article

C2 - 34282029

AN - SCOPUS:85121982407

SN - 2159-8274

VL - 11

SP - 3158

EP - 3177

JO - Cancer Discovery

JF - Cancer Discovery

IS - 12

ER -

Genetic screens identify a context-specific pi3k/p27^kip1 node driving extrahepatic biliary cancer

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