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Metabolic Cycles in Cancer Cells?

Bioessays 42 (4):2000048 (2020)

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  1. Metabolic Reprogramming is a Hallmark of Metabolism Itself.Miguel Ángel Medina - 2020 - Bioessays 42 (10):2000058.
    The reprogramming of metabolism has been identified as one of the hallmarks of cancer. It is becoming more and more frequent to connect other diseases with metabolic reprogramming. This article aims to argue that metabolic reprogramming is not driven by disease but instead is the main hallmark of metabolism, based on its dynamic behavior that allows it to continuously adapt to changes in the internal and external conditions.
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  • Can natural selection and druggable targets synergize? Of nutrient scarcity, cancer, and the evolution of cooperation.Neil W. Blackstone & Jordan U. Gutterman - 2021 - Bioessays 43 (2):2000160.
    Since the dawn of molecular biology, cancer therapy has focused on druggable targets. Despite some remarkable successes, cell‐level evolution remains a potent antagonist to this approach. We suggest that a deeper understanding of the breakdown of cooperation can synergize the evolutionary and druggable‐targets approaches. Complexity requires cooperation, whether between cells of different species (symbiosis) or between cells of the same organism (multicellularity). Both forms of cooperation may be associated with nutrient scarcity, which in turn may be associated with a chemiosmotic (...)
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  • Why do cancer cells break from host circadian rhythm? Insights from unicellular organisms.Aliaa A. Alamoudi - 2021 - Bioessays 43 (4):2000205.
    It is not clear why cancer cells choose to disrupt their circadian clock rhythms, and whether such disruption governs a selective fitness and a survival advantage. In this review, I focus on understanding the impacts of clock gene disruption on a simpler model, such as the unicellular cyanobacterium, in order to explain how cancer cells may alter the circadian rhythm to reprogram their metabolism based on their needs and status. It appears to be that the activation of the oxidative pentose (...)
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