Austin J. Corbett scite author profile

Malignant transformation is often accompanied by significant metabolic changes. To identify drivers underlying these changes, we calculated metabolic flux states for the NCI60 cell line collection and correlated the variance between metabolic states of these lines with their other properties. The analysis revealed a remarkably consistent structure underlying high flux metabolism. The three primary uptake pathways, glucose, glutamine and serine, are each characterized by three features: (1) metabolite uptake sufficient for the stoichiometric requirement to sustain observed growth, (2) overflow metabolism, which scales with excess nutrient uptake over the basal growth requirement, and (3) redox production, which also scales with nutrient uptake but greatly exceeds the requirement for growth. We discovered that resistance to chemotherapeutic drugs in these lines broadly correlates with the amount of glucose uptake. These results support an interpretation of the Warburg effect and glutamine addiction as features of a growth state that provides resistance to metabolic stress through excess redox and energy production. Furthermore, overflow metabolism observed may indicate that mitochondrial catabolic capacity is a key constraint setting an upper limit on the rate of cofactor production possible. These results provide a greater context within which the metabolic alterations in cancer can be understood.

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Case report 303

El‐Khoury

Corbett

Summers

1985

Skeletal Radiol

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Tumor of the Carotid Body Associated With Nodular Goiter

Corbett¹,

Mcclintock²

1950

Arch Surg

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Reye Syndrome Associated with Aspirin Therapy for Systemic Lupus Erythematosus

Hansen

McCray

Bale

et al. 1985

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Duodenal diverticula

Glasier¹,

Corbett²

1952

The American Journal of Surgery

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Austin J. Corbett

Systems biology analysis of drivers underlying hallmarks of cancer cell metabolism

Case report 303

Tumor of the Carotid Body Associated With Nodular Goiter

Reye Syndrome Associated with Aspirin Therapy for Systemic Lupus Erythematosus

Duodenal diverticula

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