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Multiple Molecular Mechanisms Rescue mtDNA Disease in C. elegans

Suraiya Haroon, Annie Li, Jaye L. Weinert, Clark Fritsch, Nolan G. Ericson, Jasmine Alexander-Floyd, Bart P. Braeckman, Cole M. Haynes, Jason H. Bielas, Tali Gidalevitz, Marc Vermulst

Cell Reports · 2018 · ▲ 50 citations

Abstract

Genetic instability of the mitochondrial genome (mtDNA) plays an important role in human aging and disease. Thus far, it has proven difficult to develop successful treatment strategies for diseases that are caused by mtDNA instability. To address this issue, we developed a model of mtDNA disease in the nematode C. elegans, an animal model that can rapidly be screened for genes and biological pathways that reduce mitochondrial pathology. These worms recapitulate all the major hallmarks of mtDNA disease in humans, including increased mtDNA instability, loss of respiration, reduced neuromuscular function, and a shortened lifespan. We found that these phenotypes could be rescued by intervening in numerous biological pathways, including IGF-1/insulin signaling, mitophagy, and the mitochondrial unfolded protein response, suggesting that it may be possible to ameliorate mtDNA disease through multiple molecular mechanisms.

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OpenAlex
DOI
10.1016/j.celrep.2018.02.099
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2026-06-28 MST

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APA
Haroon, S., Li, A., Weinert, J.L., Fritsch, C., Ericson, N.G., Alexander-Floyd, J., Braeckman, B.P., Haynes, C.M., Bielas, J.H., Gidalevitz, T., &amp; Vermulst, M. (2018). Multiple Molecular Mechanisms Rescue mtDNA Disease in C. elegans. <em>Cell Reports</em>. https://doi.org/10.1016/j.celrep.2018.02.099
Vancouver
Haroon S, Li A, Weinert JL, Fritsch C, Ericson NG, Alexander-Floyd J, et al. Multiple Molecular Mechanisms Rescue mtDNA Disease in C. elegans. Cell Reports. 2018. doi:10.1016/j.celrep.2018.02.099.
BibTeX
@article{suraiya2018Multip, title = {Multiple Molecular Mechanisms Rescue mtDNA Disease in C. elegans}, author = {Suraiya Haroon and Annie Li and Jaye L. Weinert and Clark Fritsch and Nolan G. Ericson and Jasmine Alexander-Floyd and Bart P. Braeckman and Cole M. Haynes and Jason H. Bielas and Tali Gidalevitz and Marc Vermulst}, journal = {Cell Reports}, year = {2018}, doi = {10.1016/j.celrep.2018.02.099}, }

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