AP1/Fra1 confers resistance to MAPK cascade inhibition in pancreatic cancer

Christian Schneeweis; Sandra Diersch; Zonera Hassan; Lukas Krauß; Carolin Schneider; Daniele Lucarelli; Chiara Falcomatà; Katja Steiger; Rupert Öllinger; Oliver H. Krämer; Alexander Arlt; Marian Grade; Marc Schmidt-Supprian; Elisabeth Hessmann; Matthias Wirth; Roland Rad; Maximilian Reichert; Dieter Saur; Günter Schneider

doi:10.1007/s00018-022-04638-y

AP1/Fra1 confers resistance to MAPK cascade inhibition in pancreatic cancer

Christian Schneeweis, Sandra Diersch, Zonera Hassan, Lukas Krauß, Carolin Schneider, Daniele Lucarelli, Chiara Falcomatà, Katja Steiger, Rupert Öllinger, Oliver H. Krämer, Alexander Arlt, Marian Grade, Marc Schmidt-Supprian, Elisabeth Hessmann, Matthias Wirth, Roland Rad, Maximilian Reichert, Dieter Saur, Günter Schneider

Publikation: Beitrag in Fachzeitschrift › Artikel › Begutachtung

8 Zitate (Scopus)

Abstract

Targeting KRAS downstream signaling remains an important therapeutic approach in pancreatic cancer. We used primary pancreatic ductal epithelial cells and mouse models allowing the conditional expression of oncogenic Kras^G12D, to investigate KRAS signaling integrators. We observed that the AP1 family member FRA1 is tightly linked to the KRAS signal and expressed in pre-malignant lesions and the basal-like subtype of pancreatic cancer. However, genetic-loss-of-function experiments revealed that FRA1 is dispensable for Kras^G12D-induced pancreatic cancer development in mice. Using FRA1 gain- and loss-of-function models in an unbiased drug screen, we observed that FRA1 is a modulator of the responsiveness of pancreatic cancer to inhibitors of the RAF–MEK–ERK cascade. Mechanistically, context-dependent FRA1-associated adaptive rewiring of oncogenic ERK signaling was observed and correlated with sensitivity to inhibitors of canonical KRAS signaling. Furthermore, pharmacological-induced degradation of FRA1 synergizes with MEK inhibitors. Our studies establish FRA1 as a part of the molecular machinery controlling sensitivity to MAPK cascade inhibition allowing the development of mechanism-based therapies.

Originalsprache	Englisch
Aufsatznummer	12
Fachzeitschrift	Cellular and Molecular Life Sciences
Jahrgang	80
Ausgabenummer	1
DOIs	https://doi.org/10.1007/s00018-022-04638-y
Publikationsstatus	Veröffentlicht - Jan. 2023

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Schneeweis, C., Diersch, S., Hassan, Z., Krauß, L., Schneider, C., Lucarelli, D., Falcomatà, C., Steiger, K., Öllinger, R., Krämer, O. H., Arlt, A., Grade, M., Schmidt-Supprian, M., Hessmann, E., Wirth, M., Rad, R., Reichert, M., Saur, D., & Schneider, G. (2023). AP1/Fra1 confers resistance to MAPK cascade inhibition in pancreatic cancer. Cellular and Molecular Life Sciences, 80(1), Artikel 12. https://doi.org/10.1007/s00018-022-04638-y

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title = "AP1/Fra1 confers resistance to MAPK cascade inhibition in pancreatic cancer",

abstract = "Targeting KRAS downstream signaling remains an important therapeutic approach in pancreatic cancer. We used primary pancreatic ductal epithelial cells and mouse models allowing the conditional expression of oncogenic KrasG12D, to investigate KRAS signaling integrators. We observed that the AP1 family member FRA1 is tightly linked to the KRAS signal and expressed in pre-malignant lesions and the basal-like subtype of pancreatic cancer. However, genetic-loss-of-function experiments revealed that FRA1 is dispensable for KrasG12D-induced pancreatic cancer development in mice. Using FRA1 gain- and loss-of-function models in an unbiased drug screen, we observed that FRA1 is a modulator of the responsiveness of pancreatic cancer to inhibitors of the RAF–MEK–ERK cascade. Mechanistically, context-dependent FRA1-associated adaptive rewiring of oncogenic ERK signaling was observed and correlated with sensitivity to inhibitors of canonical KRAS signaling. Furthermore, pharmacological-induced degradation of FRA1 synergizes with MEK inhibitors. Our studies establish FRA1 as a part of the molecular machinery controlling sensitivity to MAPK cascade inhibition allowing the development of mechanism-based therapies.",

keywords = "AP1, ERK, FRA1, KRAS, MEK, Pancreatic cancer",

author = "Christian Schneeweis and Sandra Diersch and Zonera Hassan and Lukas Krau{\ss} and Carolin Schneider and Daniele Lucarelli and Chiara Falcomat{\`a} and Katja Steiger and Rupert {\"O}llinger and Kr{\"a}mer, {Oliver H.} and Alexander Arlt and Marian Grade and Marc Schmidt-Supprian and Elisabeth Hessmann and Matthias Wirth and Roland Rad and Maximilian Reichert and Dieter Saur and G{\"u}nter Schneider",

note = "Publisher Copyright: {\textcopyright} 2022, The Author(s).",

year = "2023",

month = jan,

doi = "10.1007/s00018-022-04638-y",

language = "English",

volume = "80",

journal = "Cellular and Molecular Life Sciences",

issn = "1420-682X",

publisher = "Springer Science and Business Media Deutschland GmbH",

number = "1",

}

Schneeweis, C, Diersch, S, Hassan, Z, Krauß, L, Schneider, C, Lucarelli, D, Falcomatà, C, Steiger, K, Öllinger, R, Krämer, OH, Arlt, A, Grade, M, Schmidt-Supprian, M, Hessmann, E, Wirth, M, Rad, R , Reichert, M , Saur, D & Schneider, G 2023, 'AP1/Fra1 confers resistance to MAPK cascade inhibition in pancreatic cancer', Cellular and Molecular Life Sciences, Jg. 80, Nr. 1, 12. https://doi.org/10.1007/s00018-022-04638-y

TY - JOUR

T1 - AP1/Fra1 confers resistance to MAPK cascade inhibition in pancreatic cancer

AU - Schneeweis, Christian

AU - Diersch, Sandra

AU - Hassan, Zonera

AU - Krauß, Lukas

AU - Schneider, Carolin

AU - Lucarelli, Daniele

AU - Falcomatà, Chiara

AU - Steiger, Katja

AU - Öllinger, Rupert

AU - Krämer, Oliver H.

AU - Arlt, Alexander

AU - Grade, Marian

AU - Schmidt-Supprian, Marc

AU - Hessmann, Elisabeth

AU - Wirth, Matthias

AU - Rad, Roland

AU - Reichert, Maximilian

AU - Saur, Dieter

AU - Schneider, Günter

PY - 2023/1

Y1 - 2023/1

N2 - Targeting KRAS downstream signaling remains an important therapeutic approach in pancreatic cancer. We used primary pancreatic ductal epithelial cells and mouse models allowing the conditional expression of oncogenic KrasG12D, to investigate KRAS signaling integrators. We observed that the AP1 family member FRA1 is tightly linked to the KRAS signal and expressed in pre-malignant lesions and the basal-like subtype of pancreatic cancer. However, genetic-loss-of-function experiments revealed that FRA1 is dispensable for KrasG12D-induced pancreatic cancer development in mice. Using FRA1 gain- and loss-of-function models in an unbiased drug screen, we observed that FRA1 is a modulator of the responsiveness of pancreatic cancer to inhibitors of the RAF–MEK–ERK cascade. Mechanistically, context-dependent FRA1-associated adaptive rewiring of oncogenic ERK signaling was observed and correlated with sensitivity to inhibitors of canonical KRAS signaling. Furthermore, pharmacological-induced degradation of FRA1 synergizes with MEK inhibitors. Our studies establish FRA1 as a part of the molecular machinery controlling sensitivity to MAPK cascade inhibition allowing the development of mechanism-based therapies.

AB - Targeting KRAS downstream signaling remains an important therapeutic approach in pancreatic cancer. We used primary pancreatic ductal epithelial cells and mouse models allowing the conditional expression of oncogenic KrasG12D, to investigate KRAS signaling integrators. We observed that the AP1 family member FRA1 is tightly linked to the KRAS signal and expressed in pre-malignant lesions and the basal-like subtype of pancreatic cancer. However, genetic-loss-of-function experiments revealed that FRA1 is dispensable for KrasG12D-induced pancreatic cancer development in mice. Using FRA1 gain- and loss-of-function models in an unbiased drug screen, we observed that FRA1 is a modulator of the responsiveness of pancreatic cancer to inhibitors of the RAF–MEK–ERK cascade. Mechanistically, context-dependent FRA1-associated adaptive rewiring of oncogenic ERK signaling was observed and correlated with sensitivity to inhibitors of canonical KRAS signaling. Furthermore, pharmacological-induced degradation of FRA1 synergizes with MEK inhibitors. Our studies establish FRA1 as a part of the molecular machinery controlling sensitivity to MAPK cascade inhibition allowing the development of mechanism-based therapies.

KW - AP1

KW - ERK

KW - FRA1

KW - KRAS

KW - MEK

KW - Pancreatic cancer

UR - http://www.scopus.com/inward/record.url?scp=85144310306&partnerID=8YFLogxK

U2 - 10.1007/s00018-022-04638-y

DO - 10.1007/s00018-022-04638-y

M3 - Article

C2 - 36534167

AN - SCOPUS:85144310306

SN - 1420-682X

VL - 80

JO - Cellular and Molecular Life Sciences

JF - Cellular and Molecular Life Sciences

IS - 1

M1 - 12

ER -

AP1/Fra1 confers resistance to MAPK cascade inhibition in pancreatic cancer

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