Oncogenic KRAS and the EGFR loop in pancreatic carcinogenesis—A connection to licensing nodes

Christian Schneeweis; Matthias Wirth; Dieter Saur; Maximilian Reichert; Günter Schneider

doi:10.1080/21541248.2016.1262935

Oncogenic KRAS and the EGFR loop in pancreatic carcinogenesis—A connection to licensing nodes

Christian Schneeweis
, Matthias Wirth
, Dieter Saur
, Maximilian Reichert
, Günter Schneider

Publikation: Beitrag in Fachzeitschrift › Kommentar/Debatte

14 Zitate (Scopus)

Abstract

EGFR signaling has a critical role in oncogenic KRAS-driven tumorigenesis of the pancreas, whereas it is dispensable in other organs. The complex signaling network engaged by oncogenic KRAS and its modulation by EGFR signaling, remains incompletely understood. In order to study early signaling events activated by oncogenic KRAS in the pancreas, we recently developed a novel model system based on murine primary pancreatic epithelial cells enabling the time-specific expression of mutant Kras^G12D from its endogenous promoter. Here, we discuss our findings of a Kras^G12D-induced autocrine EGFR loop, how this loop is integrated by the MYC oncogene, and point to possible translational implications.

Originalsprache	Englisch
Seiten (von - bis)	457-464
Seitenumfang	8
Fachzeitschrift	Small GTPases
Jahrgang	9
Ausgabenummer	6
DOIs	https://doi.org/10.1080/21541248.2016.1262935
Publikationsstatus	Veröffentlicht - 2 Nov. 2018

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abstract = "EGFR signaling has a critical role in oncogenic KRAS-driven tumorigenesis of the pancreas, whereas it is dispensable in other organs. The complex signaling network engaged by oncogenic KRAS and its modulation by EGFR signaling, remains incompletely understood. In order to study early signaling events activated by oncogenic KRAS in the pancreas, we recently developed a novel model system based on murine primary pancreatic epithelial cells enabling the time-specific expression of mutant KrasG12D from its endogenous promoter. Here, we discuss our findings of a KrasG12D-induced autocrine EGFR loop, how this loop is integrated by the MYC oncogene, and point to possible translational implications.",

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AU - Schneeweis, Christian

AU - Wirth, Matthias

AU - Saur, Dieter

AU - Reichert, Maximilian

AU - Schneider, Günter

PY - 2018/11/2

Y1 - 2018/11/2

N2 - EGFR signaling has a critical role in oncogenic KRAS-driven tumorigenesis of the pancreas, whereas it is dispensable in other organs. The complex signaling network engaged by oncogenic KRAS and its modulation by EGFR signaling, remains incompletely understood. In order to study early signaling events activated by oncogenic KRAS in the pancreas, we recently developed a novel model system based on murine primary pancreatic epithelial cells enabling the time-specific expression of mutant KrasG12D from its endogenous promoter. Here, we discuss our findings of a KrasG12D-induced autocrine EGFR loop, how this loop is integrated by the MYC oncogene, and point to possible translational implications.

AB - EGFR signaling has a critical role in oncogenic KRAS-driven tumorigenesis of the pancreas, whereas it is dispensable in other organs. The complex signaling network engaged by oncogenic KRAS and its modulation by EGFR signaling, remains incompletely understood. In order to study early signaling events activated by oncogenic KRAS in the pancreas, we recently developed a novel model system based on murine primary pancreatic epithelial cells enabling the time-specific expression of mutant KrasG12D from its endogenous promoter. Here, we discuss our findings of a KrasG12D-induced autocrine EGFR loop, how this loop is integrated by the MYC oncogene, and point to possible translational implications.

KW - EGFR

KW - MYC

KW - autocrine signaling

KW - kras

KW - pancreatic cancer

UR - https://www.scopus.com/pages/publications/85009964809

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DO - 10.1080/21541248.2016.1262935

M3 - Comment/debate

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AN - SCOPUS:85009964809

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EP - 464

JO - Small GTPases

JF - Small GTPases

IS - 6

ER -

Oncogenic KRAS and the EGFR loop in pancreatic carcinogenesis—A connection to licensing nodes

Abstract

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