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DOI: 10.1055/s-0033-1360039
Stress und Pankreaskarzinom
β-adrenerge Signaltransduktion und TumorbiologieStress and pancreatic carcinoma – β-adrenergic signaling and tumor biologyPublication History
04 July 2013
02 October 2013
Publication Date:
04 February 2014 (online)
Zusammenfassung
Aus Untersuchungen zu verschiedenen Karzinomen sind Regulationsmöglichkeiten der Tumorbiologie durch die β-adrenerge Signaltransduktion bekannt. Bis vor wenigen Jahren wurde das Pankreaskarzinom hierzu vergleichsweise wenig beforscht. Dabei sind neue Erkenntnisse zu Biologie und Therapieoptionen aufgrund der Inzidenz und ungünstigen Prognose gerade bei dieser Tumorentität von besonderer Bedeutung. Inzwischen beschreiben mehrere Arbeiten zum β-adrenergen System Einflüsse auf das Pankreaskarzinom in vitro und in vivo. Diese beziehen sich sowohl auf das Proliferations-und Apoptoseverhalten der Karzinomzellen als auch auf Wechselwirkungen mit dem Tumor-Microenvironment und Folgen für die Disseminations-und Metastasierungsneigung. Im Gegensatz zu anderen malignen Tumoren ergeben sich beim Pankreaskarzinom sogar Hinweise auf einen Zusammenhang zwischen β-adrenergen Signalwegen und dem Neuauftreten der Erkrankung. In der folgenden Arbeit sollen die wesentlichen Erkenntnisse zusammengefasst und Implikationen für die weitere Forschung beschrieben werden.
Abstract
In several carcinomas, β-adrenergic signaling has been found to regulate relevant processes of cancer biology. Until recently, pancreatic cancer has not been in the focus of respective research. But in view of the incidence and poor prognosis of pancreatic cancer, new insights in biology and therapeutic strategies are of prime importance. Nowadays, several reports describe influences of the catecholaminergic system on pancreatic cancer in vitro and in vivo. Effects were shown on proliferation and apoptosis of carcinoma cells as well as on interactions with tumor-microenvironment and dissemination and metastasis formation. In contrast to other entities, evidence even suggests links between β-adrenergic signaling and initiation of the disease. The following report summarizes the most relevant results demonstrating implications for further research and possible interventions.
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