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Open AccessJournal ArticleDOI

The Contextual Essentiality of Mitochondrial Genes in Cancer.

TLDR
In this article, the authors discuss recent advances in understanding of the contribution of NEMGs to cancer from CRISPR-Cas9 deletion screens, and discuss emerging concepts surrounding the context-dependent nature of mitochondrial gene essentiality.
Abstract
Mitochondria are key organelles in eukaryotic evolution that perform crucial roles as metabolic and cellular signaling hubs. Mitochondrial function and dysfunction are associated with a range of diseases, including cancer. Mitochondria support cancer cell proliferation through biosynthetic reactions and their role in signaling, and can also promote tumorigenesis via processes such as the production of reactive oxygen species (ROS). The advent of (nuclear) genome-wide CRISPR-Cas9 deletion screens has provided gene-level resolution of the requirement of nuclear-encoded mitochondrial genes (NEMGs) for cancer cell viability (essentiality). More recently, it has become apparent that the essentiality of NEMGs is highly dependent on the cancer cell context. In particular, key tumor microenvironmental factors such as hypoxia, and changes in nutrient (e.g., glucose) availability, significantly influence the essentiality of NEMGs. In this mini-review we will discuss recent advances in our understanding of the contribution of NEMGs to cancer from CRISPR-Cas9 deletion screens, and discuss emerging concepts surrounding the context-dependent nature of mitochondrial gene essentiality.

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The role of BMI1 in endometrial cancer and other cancers.

TL;DR: In this article , a review summarizes the structure and upstream regulatory mechanisms of BMI1 and its role in endometrial cancer, focusing on the role of the BMI1 in chemoradiotherapy resistance and summarized the current drugs that target BMI1.
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Degradome-focused RNA interference screens to identify proteases important for breast cancer cell growth

TL;DR: Interestingly, it was discovered that the environmental conditions influence the degree of breast cancer cell dependency on certain proteases, and breast cancer stem cell-like cells were less susceptible to depletion of several mitochondrial proteases in hypoxic conditions.
References
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Journal ArticleDOI

Hallmarks of cancer: the next generation.

TL;DR: Recognition of the widespread applicability of these concepts will increasingly affect the development of new means to treat human cancer.
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Beyond aerobic glycolysis : Transformed cells can engage in glutamine metabolism that exceeds the requirement for protein and nucleotide synthesis

TL;DR: Transformed cells exhibit a high rate of glutamine consumption that cannot be explained by the nitrogen demand imposed by nucleotide synthesis or maintenance of nonessential amino acid pools, and glutamine metabolism provides a carbon source that facilitates the cell's ability to use glucose-derived carbon and TCA cycle intermediates as biosynthetic precursors.
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Mitochondria and cancer

TL;DR: Cancer cells then reprogramme adjacent stromal cells to optimize the cancer cell environment and activate out-of-context programmes that are important in development, stress response, wound healing and nutritional status.
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The genome sequence of Rickettsia prowazekii and the origin of mitochondria

TL;DR: The complete genome sequence of the obligate intracellular parasite Rickettsia prowazekii, the causative agent of epidemic typhus, is described, which contains 834 protein-coding genes and is more closely related to mitochondria than is any other microbe studied so far.
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Mitochondria and Cancer

TL;DR: Evaluating mechanisms of mitochondrial function during tumorigenesis will be critical for the next generation of cancer therapeutics as multiple aspects of mitochondrial biology beyond bioenergetics support transformation.
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