CRISPR-Cas9 Mediated TSPO Gene Knockout alters Respiration and Cellular Metabolism in Human Primary Microglia Cells.
Vladimir M MilenkovicDounia SlimStefanie BaderVictoria KochElena-Sofia HeinlDavid Alvarez-CarbonellCaroline NothdurfterRainer RupprechtChristian H WetzelPublished in: International journal of molecular sciences (2019)
The 18 kDa translocator protein (TSPO) is an evolutionary conserved cholesterol binding protein localized in the outer mitochondrial membrane. It has been implicated in the regulation of various cellular processes including oxidative stress, proliferation, apoptosis, and steroid hormone biosynthesis. Since the expression of TSPO in activated microglia is upregulated in various neuroinflammatory and neurodegenerative disorders, we set out to examine the role of TSPO in an immortalized human microglia C20 cell line. To this end, we performed a dual approach and used (i) lentiviral shRNA silencing to reduce TSPO expression, and (ii) the CRISPR/Cas9 technology to generate complete TSPO knockout microglia cell lines. Functional characterization of control and TSPO knockdown as well as knockout cells, revealed only low de novo steroidogenesis in C20 cells, which was not dependent on the level of TSPO expression or influenced by the treatment with TSPO-specific ligands. In contrast to TSPO knockdown C20 cells, which did not show altered mitochondrial function, the TSPO deficient knockout cells displayed a significantly decreased mitochondrial membrane potential and cytosolic Ca2+ levels, as well as reduced respiratory function. Performing the rescue experiment by lentiviral overexpression of TSPO in knockout cells, increased oxygen consumption and restored respiratory function. Our study provides further evidence for a significant role of TSPO in cellular and mitochondrial metabolism and demonstrates that different phenotypes of mitochondrial function are dependent on the level of TSPO expression.
Keyphrases
- induced apoptosis
- pet imaging
- cell cycle arrest
- oxidative stress
- crispr cas
- binding protein
- endoplasmic reticulum stress
- poor prognosis
- cell death
- inflammatory response
- signaling pathway
- endothelial cells
- neuropathic pain
- genome editing
- genome wide
- computed tomography
- spinal cord injury
- cell proliferation
- dna methylation
- long non coding rna
- spinal cord
- small molecule
- copy number
- contrast enhanced
- low density lipoprotein