The Department of Physiology and Biophysics - School of Medicine

Xin Qi, PhD

Jeanette M. and Joseph S. Silber Professor of Brain Sciences

Co-Director, Center for Mitochondrial Research and Therapeutics

Director, Physiology & Biophysics Graduate Program

PhD, Hokkaido University, Japan

Postdoc training, Stanford University

Mailing Address:
Robbins E516

Phone: +12163684459
ORCiD:0000-0002-9578-3890
xin.qi2@case.edu

Qi Lab

Research Interests

Mitochondrial quality control and neurodegenerative diseases

Our laboratory focuses on understanding the roles of mitochondrial quality control and metabolism in neurodegenerative diseases. We use unbiased proteomics and genomics, cellular and molecular biology, patient iPS cells-derived cell culture and diseased animals to investigate the fundamental mechanisms by which mitochondrial impairment contributes to cellular metabolism disturbance and neurodegeneration. We also utilize rationally designed peptide inhibitors of protein-protein interactions and the high throughput screening approach to developing “mitochondrial medicine” as therapeutic strategies for treating neurodegenerative diseases.

Mitochondria are critical organelles for cellular function by regulating energy metabolism, ATP generation, and calcium handling. Dysfunctional mitochondria elicit ROS production and deficits in metabolic activity, which ultimately affect numerous biological processes, including cellular bioenergetics, immune response, genomic stability, and programmed cell death.

To attenuate negative effects, mitochondria deploy several quality control pathways essential to maintain their pleiotropic functions and reduce mitochondrial stress. Mitochondrial quality control includes mitochondrial dynamics (fusion/fission), mitochondrial unfolded protein response (UPRmt), and mitochondria-related autophagy (mitophagy). These events repair damaged mitochondrial proteins, facilitate mitochondrial adaption to the stress, and remove/degrade the irreversibly damaged mitochondria.

One of our research focuses is to understand the roles of mitochondrial dynamics-related proteins in mitochondrial and cellular functions, especially in the context of neurodegenerative diseases. Using a set of inhibitors targeting aberrant mitochondrial fission, we determine whether manipulation of mitochondrial dynamics could provide a useful strategy for the treatment of neurodegenerative diseases. As another arc of research, we utilize unbiased proteomics to identify factors that participate in UPRmt and mitophagy regulation. We aim to understand how protein homeostasis of mitochondria controls cell life and influences neurodegeneration.

Mitochondrial quality control mechanism

Mitochondrial quality control includes mitochondrial dynamics (fusion/fission), mitochondrial protein homeostasis (UPR^mt), and mitochondria-associated autophagy (mitophagy). These events maintain mitochondrial health and cell survival. Impairment of the mitochondrial quality control system contributes to neurodegeneration.

Featured Publications

Shang Y, Sun X, Chen X, Wang Q, Wang EJ, Miller E, Xu R, Pieper AA and Qi X* A CHCHD6-APP axis connects amyloid and mitochondrial pathology in Alzheimer's disease. Acta Neuropathologica , 2022 Nov;144(5):911-938.
Zhao YY^#, Hu D^#, Wang RH^#, Sun XY, Ropelewski P, Hubler Z, Lundberg K, Wang QQ, Adams D, Xu R and Qi X* ATAD3A oligomerization promotes neuropathology and cognitive deficits in Alzheimer's disease models. Nature Communications, 2022 Mar 2;13(1):1121. (#, co-first author)
Hu D, Sun SY, Magpusao A, Fedorov Y, Thompson M, Wang BL, Lundberg K, Adams D and Qi X*, Small-molecule suppression of calpastatin degradation reduces neuropathology in models of Huntington’s disease. Nature Communications, 2021 Sep 6;12(1):5305.
Zhang X, R Wang, HU D, Sun X, Fujioka K, Lundberg K, Chan ER, Wang Q, Xu R, Flanagan ME, Pieper AA and Qi X*. Oligodendroglial glycolytic stress triggers inflammasome activation and neuropathology in Alzheimer's disease. Science Advances, 2020 Dec 4;6(49):eabb8680.
Zhao Y, Sun X, Hu D, Prosdocimo DA, Hoppel C, Jain MK, Ramachandran R & Qi X*. ATAD3A oligomerization causes neurodegeneration by coupling mitochondrial fragmentation and bioenergetics defects. Nature Communications, 2019 Mar 26;10(1):1371.
Hu D, Sun X, Liao X, Zhang X, Zarabi S, Schimmer A, Hong Y, Ford C, Luo Y and Qi X*. Alpha-synuclein suppresses mitochondrial protease ClpP to trigger mitochondrial oxidative damage and neurotoxicity. Acta Neuropathologica, 2019 Jun;137(6):939-960.

Related Research Areas

Major Research Areas
Cell Death Mechanisms
Mitochondrial biology and pathology
Neurodegenerative diseases
Therapeutics
Cell Death Mechanisms, Mitochondrial biology and pathology, Neurodegenerative diseases, Therapeutics
Disciplines
Drug discovery
Metabolism
Molecular and cellular biology
Neuodegenerative diseases
Neuroscience
Pharmacology and Therapeutics
Signal Transduction
Drug discovery , Metabolism, Molecular and cellular biology, Neuodegenerative diseases , Neuroscience, Pharmacology and Therapeutics, Signal Transduction
Organ Systems
Nervous System
Nervous System
Diseases
Alzheimer's Disease
Huntington's Disease
Metabolic syndrome
Neurodegenerative Diseases
Neurological Disorders
Parkinson's Disease
Alzheimer's Disease, Huntington's Disease, Metabolic syndrome , Neurodegenerative Diseases, Neurological Disorders, Parkinson's Disease
Major Techniques
Cell Culture
Cellular and Molecular Biology
In-vivo Animal Models
Induced Pluripotent Stem Cells (iPSCs) from Patients
Peptide Drug Design
Cell Culture, Cellular and Molecular Biology, In-vivo Animal Models, Induced Pluripotent Stem Cells (iPSCs) from Patients, Peptide Drug Design