PO.MCB09.02 · 分子与细胞生物学

Cytosolic transport of citrate protects nutrient-austere pancreatic cancer from ferroptosis

海报缩略图:Cytosolic transport of citrate protects nutrient-austere pancreatic cancer from ferroptosis
编号 7325 展板 11 时间 4/22 09:00–12:00 区域 Section 23 主讲 Adam Kneebone, BA
分会场 Metabolic Vulnerabilities in Pancreatic, Hepatic, and Renal Cancers
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作者与单位

Adam Kneebone1, Kailey Lindaur1, Ata Abbas2, Joel Cassel3, Sarah Graff4, Caudia Rose Keating1, Gerard Abood1, Xianzhong Ding1, William Small5, Clodia Osipo1, Wei Qiu1, Curtis Tatsuoka6, Simone Sidoli4, Costas Andreas Lyssiotis7, Joseph M. Salvino3, Ali Vaziri-Gohar1

1Loyola University Chicago Stritch School of Medicine, Maywood, IL,2Case Western Reserve University, Cleveland, OH,3The Wistar Institute, Philadelphia, PA,4Albert Einstein College of Medicine, New York, NY,5Professor, Loyola University Medical Center, Maywood, IL,6University of Maryland, Baltimore, MD,7University of Michigan, Ann Arbor, MI

摘要 Abstract

Pancreatic cancer (PDAC) cells experience nutrient starvation in a poorly perfused tumor microenvironment. Metabolic dependencies that protect PDAC cells from detrimental oxidative stress in a nutrient-restricted niche represent as tumor-specific targets. While the role of mitochondria in supporting energy production and biosynthetic requirements of cells has been well investigated, their contribution to maintaining intracellular redox homeostasis when PDAC cells are exposed to nutrient deprivation is unknown. Our results demonstrate that cytosolic transport of citrate via SLC25A1 confers a survival advantage to PDAC cells by protecting them from ferroptosis, a well-established iron-dependent cell death mechanism, under nutrient-limited conditions. Employing selective SLC25A1 inhibitor or targeting mitochondrial OXPHOS dramatically reduced GPX4 expression and PDAC cell viability. Rescuing GPX4 expression with the products of both ACLY and ACO1-dependent pathways uncovered their critical role in conferring survival advantage under metabolic stress. Importantly, exogenous expression of GPX4 reversed redox imbalance and metabolic discordance resulting from the lack of SLC25A1 activity, indicating the requirement of citrate-induced GPX4 expression to support mitochondrial health and function. As observed with cultured cells under nutrient limitation, SLC25A1 function was revealed to be indispensable in pancreatic tumor microenvironment, and the reduced growth, due to the lack of SLC25A1 activity, was rescued with antioxidant NAC in preclinical models of PDAC. Lastly, SLC25A1 suppression was accompanied by elevated glutamine metabolism, and combination therapy with pharmacologic inhibitors of SLC25A1 and glutaminase inhibitor CB-839 dramatically suppressed tumor growth, highlighting this combinatorial approach as a potential therapeutic strategy in PDAC.
利益披露 Disclosure
A. Kneebone, None.. K. Lindaur, None.. A. Abbas, None.. J. Cassel, None.. S. Graff, None.. C. R. Keating, None.. G. Abood, None.. X. Ding, None.. C. Osipo, None.. W. Qiu, None.. C. Tatsuoka, None.. S. Sidoli, None.. A. Vaziri-Gohar, None.

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