Research Interests
Cell Biology, Mitochondrial protein import, Mitochondrial stress, Molecular Biology, Organelle Biology, Protein quality control
Research Focus Teams
Aging, Rare Diseases
Departments
Cellular & Physiological Sciences
Contact
Email: hilla.weidberg@ubc.ca
Office Phone: phone: 604–827–6293
Publications
Lab Website
Postdoctoral fellow in the Amon laboratory at The Massachusetts Institute of Technology
PhD in the Elazar laboratory at The Weizmann Institute of Science, Israel
MSc in the Horowitz laboratory at Tel Aviv University, Israel
The Jane Coffin Childs Memorial Fund for Medical Research Fellowship (2013)
EMBO Long-Term Fellowship (2012)
Israeli National Postdoctoral Award for Advancing Women in Science (2011)
Lady Anne Chain Memorial Prize for PhD students (2011)
Mitochondria are organelles that serve as a hub for cellular signaling and the biogenesis of indispensable metabolites. We aim to understand how mitochondrial homeostasis is maintained under challenging physiological and disease conditions.
Even though mitochondria contain their own genome, 99% of their proteome is encoded by the eukaryotic genome. Therefore, the constant import of proteins into the organelle is essential to eukaryotic cell function. Perturbations in this process cause multiple human disorders and are associated with aging and neurodegenerative diseases.
We discovered a cellular response to protein import defects which we have termed the mitoCPR (mitochondrial compromised protein import response). The mitoCPR maintains mitochondrial functionality during import stress and prevents permanent damage to the mitochondrial DNA.
Our lab employs cell biology, biochemical and genetic approaches to investigate how cells cope with defects in protein import. Using budding yeast and mammalian cells we aim to elucidate the molecular mechanisms that ensure mitochondrial health in the face of import defects.
Mitochondria to nucleus signaling: Communication between mitochondria and the nucleus is crucial for maintaining mitochondrial function and, consequently, for cell viability. We study the signaling route between these organelles during protein import stress. Our goal is to identify the mitochondrial signal that is sensed by cells to activate the mitoCPR.
Mitochondrial protein quality control: During import stress un-imported proteins stall in the mitochondrial import channels. One function of the mitoCPR is to alleviate this stress by extracting stalled proteins from the channels. We aim to elucidate the mechanisms by which proteins are recognized and extracted from the membrane during import stress.For more details visit lab website: https://www.weidberglab.com