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Coordinated Transcriptional and Catabolic Programs Support Iron-Dependent Adaptation to RAS-MAPK Pathway Inhibition in Pancreatic Cancer.

Mirunalini RavichandranJingjie HuCharles CaiNathan P WardAnthony VenidaCallum FoakesMiljan KuljaninAnnan YangConnor J HennesseyYang YangBrandon R DesousaGilles RademakerAnnelot A L StaesZeynep CakirIsha H JainAndrew J AguirreJoseph D ManciasYin ShenGina M DeNicolaRushika M Perera
Published in: Cancer discovery (2022)
Reduced c-MYC levels following MAPK pathway suppression facilitate the upregulation of autophagy and lysosome biogenesis. Increased autophagy-lysosome activity is required for increased ferritinophagy-mediated iron supply, which supports mitochondrial respiration under therapy stress. Disruption of ferritinophagy synergizes with KRAS-MAPK inhibition and blocks PDA growth, thus highlighting a key targetable metabolic dependency. See related commentary by Jain and Amaravadi, p. 2023. See related article by Santana-Codina et al., p. 2180. This article is highlighted in the In This Issue feature, p. 2007.
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