Abstract

The goal of this administrative supplement request is to provide a state-of-the-art microscope for cell biological studies of mitochondrial fission for R01GM067180. The requested instrument will be equally shared with Drs. Amy Hudson (R01GM120735) and Matt Scaglione (R35GM119544) for their cell biological studies in lysosomal trafficking and proteostasis, respectively. Altered mitochondrial fission has severe consequences even death. Yet the reasons for this are unknown. It is postulated that the mitochondria have their own lifecycle that involves fission of unhealthy mitochondria to remove them. In this model, the proper balance of fission is critical: either excess or impaired fission both result in unhealthy mitochondria. This model is compelling because it explains how alterations in fission can cause or contribute to many fundamentally different diseases including recovery from heart attack and stroke, increased metabolic stress from diabetes, normal aging, and neurodegenerative diseases such as Parkinson's and Alzheimer's disease. The proposed instrument will allow visualization of the multi-protein machinery responsible for mitochondrial fission. To understand the protein- protein interactions that govern this, biochemical and structural studies have identified mutations that will be imaged using the acquired microscope. A better understanding of the protein machinery and how it works will identify key points of regulation that may be targeted with small molecules to inhibit, and activate, fission. The discovery of such molecules may ultimately lead to treatments for diseases in which enhanced, or impaired, fission is central.

Public Health Relevance

Mitochondria are components of cells that perform many functions critical for life and are known for being the 'power plant' of the cells. The mitochondria have their own life cycle with a mechanism to destroy damaged mitochondria that involves a splitting event that separates a healthy daughter mitochondrion from an unhealthy one that is subsequently removed by the cell. This splitting event is called mitochondrial fission and is vital to human health. Mitochondrial fission is accomplished by distinct protein machineries and defects in this machinery cause infant death. Disordered mitochondrial fission is increasingly recognized as a contributor to both rare and common human diseases, including cardiac and neurodegenerative diseases, cancer, diabetes, aging, and neonatal lethality syndrome. The work proposed will illuminate mechanistic details of these processes and represents an important step towards the discovery of new therapeutic strategies for these diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
3R01GM067180-14S1
Application #
9706280
Study Section
Program Officer
Flicker, Paula F
Project Start
2004-01-01
Project End
2019-03-31
Budget Start
2018-04-01
Budget End
2019-03-31
Support Year
14
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Medical College of Wisconsin
Department
Biochemistry
Type
Schools of Medicine
DUNS #
937639060
City
Milwaukee
State
WI
Country
United States
Zip Code
53226

  Publications

Ma, Cui; Beyer, Andreas M; Durand, Matthew et al. (2018) Hyperoxia Causes Mitochondrial Fragmentation in Pulmonary Endothelial Cells by Increasing Expression of Pro-Fission Proteins. Arterioscler Thromb Vasc Biol 38:622-635
Egner, John M; Jensen, Davin R; Olp, Michael D et al. (2018) Development and Validation of 2D Difference Intensity Analysis for Chemical Library Screening by Protein-Detected NMR Spectroscopy. Chembiochem 19:448-458
Santarriaga, Stephanie; Haver, Holly N; Kanack, Adam J et al. (2018) SRCP1 Conveys Resistance to Polyglutamine Aggregation. Mol Cell 71:216-228.e7
Harwig, Megan C; Viana, Matheus P; Egner, John M et al. (2018) Methods for imaging mammalian mitochondrial morphology: A prospective on MitoGraph. Anal Biochem 552:81-99
Widlansky, Michael E; Hill, R Blake (2018) Mitochondrial regulation of diabetic vascular disease: an emerging opportunity. Transl Res 202:83-98
Bordt, Evan A; Clerc, Pascaline; Roelofs, Brian A et al. (2017) The Putative Drp1 Inhibitor mdivi-1 Is a Reversible Mitochondrial Complex I Inhibitor that Modulates Reactive Oxygen Species. Dev Cell 40:583-594.e6
Bakkum, Amber L; Hill, R Blake (2017) Removal of a consensus proline is not sufficient to allow tetratricopeptide repeat oligomerization. Protein Sci 26:1974-1983
Lee, Michelle W; Lee, Ernest Y; Lai, Ghee Hwee et al. (2017) Molecular Motor Dnm1 Synergistically Induces Membrane Curvature To Facilitate Mitochondrial Fission. ACS Cent Sci 3:1156-1167
Koppenol-Raab, Marijke; Harwig, Megan Cleland; Posey, Ammon E et al. (2016) A Targeted Mutation Identified through pKa Measurements Indicates a Postrecruitment Role for Fis1 in Yeast Mitochondrial Fission. J Biol Chem 291:20329-44
Cahill, Thomas J; Leo, Vincenzo; Kelly, Matthew et al. (2016) Resistance of dynamin-related protein 1 oligomers to disassembly impairs mitophagy, resulting in myocardial inflammation and heart failure. J Biol Chem 291:25762

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