Severe Energy Impairment Consequent to Inactivation of Mitochondrial ATP Synthase as an Early Event in Cell Death: A Mechanism for the Selective Sensitivity to H2O2 of Differentiating Erythroleukemia Cells

FUS (fused in sarcoma) proteinopathy is a group of neurodegenerative diseases characterized by the formation of inclusion bodies containing the FUS protein, including frontotemporal lobar degeneration and amyotrophic lateral sclerosis. Previous studies show that mitochondrial damage is an important aspect of FUS proteinopathy. However, the molecular mechanisms by which FUS induces mitochondrial damage remain to be elucidated. Our biochemical and genetic experiments demonstrate that FUS interacts with the catalytic subunit of mitochondrial ATP synthase (ATP5B), disrupts the formation of ATP synthase complexes, and inhibits mitochondrial ATP synthesis. FUS expression activates the mitochondrial unfolded protein response (UPRmt). Importantly, down-regulating expression of ATP5B or UPRmt genes in FUS transgenic flies ameliorates neurodegenerative phenotypes. Our data show that mitochondrial impairment is a critical early event in FUS proteinopathy, and provide insights into the pathogenic mechanism of FUS-induced neurodegeneration.

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Faculty Opinions recommendation of Arrangement of subunits in intact mammalian mitochondrial ATP synthase determined by cryo-EM.

Faculty Opinions – Post-Publication Peer Review of the Biomedical Literature ◽

10.3410/f.717797900.793153400 ◽

2012 ◽

Author(s):

Thomas Meier

Keyword(s):

Atp Synthase ◽

Mitochondrial Atp Synthase

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Faculty Opinions recommendation of Dimers of mitochondrial ATP synthase form the permeability transition pore.

Faculty Opinions – Post-Publication Peer Review of the Biomedical Literature ◽

10.3410/f.718013284.793478290 ◽

2013 ◽

Author(s):

David Criddle ◽

Muhammad Ahsan Javed

Keyword(s):

Atp Synthase ◽

Permeability Transition Pore ◽

Permeability Transition ◽

Mitochondrial Atp Synthase

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Faculty Opinions recommendation of Structural basis of proton translocation and force generation in mitochondrial ATP synthase.

Faculty Opinions – Post-Publication Peer Review of the Biomedical Literature ◽

10.3410/f.732234357.793540561 ◽

2017 ◽

Author(s):

Alexey Amunts

Keyword(s):

Atp Synthase ◽

Proton Translocation ◽

Force Generation ◽

Structural Basis ◽

Mitochondrial Atp Synthase

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Faculty Opinions recommendation of Rotary substates of mitochondrial ATP synthase reveal the basis of flexible F1 -Fo coupling.

Faculty Opinions – Post-Publication Peer Review of the Biomedical Literature ◽

10.3410/f.735018996.793556523 ◽

2019 ◽

Author(s):

Ken Yokoyama

Keyword(s):

Atp Synthase ◽

Mitochondrial Atp Synthase

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Novel regulatory enhancer in the nuclear gene of the human mitochondrial ATP synthase beta-subunit.

Journal of Biological Chemistry ◽

10.1016/s0021-9258(19)39175-6 ◽

1990 ◽

Vol 265 (12) ◽

pp. 6525-6527

Author(s):

H Tomura ◽

H Endo ◽

Y Kagawa ◽

S Ohta

Keyword(s):

Atp Synthase ◽

Nuclear Gene ◽

Beta Subunit ◽

Mitochondrial Atp Synthase

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The ATP Synthase Deficiency in Human Diseases

Life ◽

10.3390/life11040325 ◽

2021 ◽

Vol 11 (4) ◽

pp. 325

Author(s):

Chiara Galber ◽

Stefania Carissimi ◽

Alessandra Baracca ◽

Valentina Giorgio

Keyword(s):

Oxidative Phosphorylation ◽

Atp Synthase ◽

Mitochondrial Protein ◽

High Energy ◽

Neurocognitive Disorders ◽

Human Diseases ◽

Age Related ◽

Muscle Tissues ◽

Mitochondrial Atp Synthase ◽

Genes Encoding

Human diseases range from gene-associated to gene-non-associated disorders, including age-related diseases, neurodegenerative, neuromuscular, cardiovascular, diabetic diseases, neurocognitive disorders and cancer. Mitochondria participate to the cascades of pathogenic events leading to the onset and progression of these diseases independently of their association to mutations of genes encoding mitochondrial protein. Under physiological conditions, the mitochondrial ATP synthase provides the most energy of the cell via the oxidative phosphorylation. Alterations of oxidative phosphorylation mainly affect the tissues characterized by a high-energy metabolism, such as nervous, cardiac and skeletal muscle tissues. In this review, we focus on human diseases caused by altered expressions of ATP synthase genes of both mitochondrial and nuclear origin. Moreover, we describe the contribution of ATP synthase to the pathophysiological mechanisms of other human diseases such as cardiovascular, neurodegenerative diseases or neurocognitive disorders.

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Lysine methylation of mitochondrial ATP synthase subunit c stored in tissues of dogs with hereditary ceroid lipofuscinosis

Journal of Biological Chemistry ◽

10.1016/s0021-9258(17)36968-5 ◽

1994 ◽

Vol 269 (13) ◽

pp. 9906-9911

Author(s):

M.L. Katz ◽

J.S. Christianson ◽

N.E. Norbury ◽

C.L. Gao ◽

A.N. Siakotos ◽

...

Keyword(s):

Atp Synthase ◽

Lysine Methylation ◽

Subunit C ◽

Ceroid Lipofuscinosis ◽

Mitochondrial Atp Synthase

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Bedaquiline, an FDA-approved drug, inhibits mitochondrial ATP production and metastasis in vivo, by targeting the gamma subunit (ATP5F1C) of the ATP synthase

Cell Death and Differentiation ◽

10.1038/s41418-021-00788-x ◽

2021 ◽

Author(s):

Marco Fiorillo ◽

Cristian Scatena ◽

Antonio Giuseppe Naccarato ◽

Federica Sotgia ◽

Michael P. Lisanti

Keyword(s):

Cell Migration ◽

Treatment Failure ◽

Atp Synthase ◽

Atp Depletion ◽

Multi Drug Resistance ◽

Gamma Subunit ◽

Primary Tumors ◽

Atp Production ◽

Mitochondrial Atp Synthase

AbstractHere, we provide evidence that high ATP production by the mitochondrial ATP-synthase is a new therapeutic target for anticancer therapy, especially for preventing tumor progression. More specifically, we isolated a subpopulation of ATP-high cancer cells which are phenotypically aggressive and demonstrate increases in proliferation, stemness, anchorage-independence, cell migration, invasion and multi-drug resistance, as well as high antioxidant capacity. Clinically, these findings have important implications for understanding treatment failure and cancer cell dormancy. Using bioinformatic analysis of patient samples, we defined a mitochondrial-related gene signature for metastasis, which features the gamma-subunit of the mitochondrial ATP-synthase (ATP5F1C). The relationship between ATP5F1C protein expression and metastasis was indeed confirmed by immunohistochemistry. Next, we used MDA-MB-231 cells as a model system to functionally validate these findings. Importantly, ATP-high MDA-MB-231 cells showed a nearly fivefold increase in metastatic capacity in vivo. Consistent with these observations, ATP-high cells overexpressed (i) components of mitochondrial complexes I–V, including ATP5F1C, and (ii) markers associated with circulating tumor cells (CTCs) and metastasis, such as EpCAM and VCAM1. Knockdown of ATP5F1C expression significantly reduced ATP-production, anchorage-independent growth, and cell migration, as predicted. Similarly, therapeutic administration of the FDA-approved drug, Bedaquiline, downregulated ATP5F1C expression in vitro and prevented spontaneous metastasis in vivo. In contrast, Bedaquiline had no effect on the growth of non-tumorigenic mammary epithelial cells (MCF10A) or primary tumors in vivo. Taken together, our results suggest that mitochondrial ATP depletion is a new therapeutic strategy for metastasis prophylaxis, to avoid treatment failure. In summary, we conclude that mitochondrial ATP5F1C is a promising new biomarker and molecular target for future drug development, for the prevention of metastatic disease progression.

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Biochemical and Genetic Analysis of the Mitochondrial Response of Yeast to BAX and BCL-XL

Molecular and Cellular Biology ◽

10.1128/mcb.20.9.3125-3136.2000 ◽

2000 ◽

Vol 20 (9) ◽

pp. 3125-3136 ◽

Cited By ~ 114

Author(s):

Atan Gross ◽

Kirsten Pilcher ◽

Elizabeth Blachly-Dyson ◽

Emy Basso ◽

Jennifer Jockel ◽

...

Keyword(s):

Cell Death ◽

Mitochondrial Genome ◽

Atp Synthase ◽

Mitochondrial Permeability Transition ◽

Family Members ◽

Growth Arrest ◽

Anion Channel ◽

Cell Killing ◽

Β Subunit ◽

Voltage Dependent Anion Channel

ABSTRACT The BCL-2 family includes both proapoptotic (e.g., BAX and BAK) and antiapoptotic (e.g., BCL-2 and BCL-XL) molecules. The cell death-regulating activity of BCL-2 members appears to depend on their ability to modulate mitochondrial function, which may include regulation of the mitochondrial permeability transition pore (PTP). We examined the function of BAX and BCL-XL using genetic and biochemical approaches in budding yeast because studies with yeast suggest that BCL-2 family members act upon highly conserved mitochondrial components. In this study we found that in wild-type yeast, BAX induced hyperpolarization of mitochondria, production of reactive oxygen species, growth arrest, and cell death; however, cytochrome c was not released detectably despite the induction of mitochondrial dysfunction. Coexpression of BCL-XL prevented all BAX-mediated responses. We also assessed the function of BCL-XL and BAX in the same strain of Saccharomyces cerevisiae with deletions of selected mitochondrial proteins that have been implicated in the function of BCL-2 family members. BAX-induced growth arrest was independent of the tested mitochondrial components, including voltage-dependent anion channel (VDAC), the catalytic β subunit or the δ subunit of the F0F1-ATP synthase, mitochondrial cyclophilin, cytochrome c, and proteins encoded by the mitochondrial genome as revealed by [rho 0] cells. In contrast, actual cell killing was dependent upon select mitochondrial components including the β subunit of ATP synthase and mitochondrial genome-encoded proteins but not VDAC. The BCL-XL protection from either BAX-induced growth arrest or cell killing proved to be independent of mitochondrial components. Thus, BAX induces two cellular processes in yeast which can each be abrogated by BCL-XL: cell arrest, which does not require aspects of mitochondrial biochemistry, and cell killing, which does.

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