CaaX-motif adjacent residues control G protein prenylation under suboptimal conditions.
Mithila TennakoonWaruna ThotamuneJohn L PaytonAjith KarunarathnePublished in: bioRxiv : the preprint server for biology (2023)
Prenylation is a universal and irreversible post-translational modification that supports membrane interactions of proteins involved in various cellular processes, including migration, proliferation, and survival. Thus, dysregulation of prenylation contributes to multiple disorders, including cancers, vascular diseases, and neurodegenerative diseases. During prenylation, prenyltransferase enzymes tether metabolically produced isoprenoid lipids to proteins via a thioether linkage. Pharmacological inhibition of the lipid synthesis pathway by statins has long been a therapeutic approach to control hyperlipidemia. Building on our previous finding that statins inhibit membrane association of G protein γ (Gγ) in a subtype-dependent manner, we investigated the molecular reasoning for this differential. We examined the prenylation efficacy of carboxy terminus (Ct) mutated Gγ in cells exposed to Fluvastatin and prenyl transferase inhibitors and monitored the subcellular localization of fluorescently tagged Gγ subunits and their mutants using live-cell confocal imaging. Reversible optogenetic unmasking-masking of Ct residues was used to probe their contribution to the prenylation process and membrane interactions of the prenylated proteins. Our findings suggest that specific Ct residues regulate membrane interactions of the Gγ polypeptide statin sensitivity, and prenylation efficacy. Our results also show that a few hydrophobic and charged residues at the Ct are crucial determinants of a protein's prenylation ability, especially under suboptimal conditions. Given the cell and tissue-specific expression of different Gγ subtypes, our findings explain how and why statins differentially perturb heterotrimeric G protein signaling in specific cells and tissues. Our results may provide molecular reasoning for repurposing statins as Ras oncogene inhibitors and the failure of using prenyltransferase inhibitors in cancer treatment.
Keyphrases
- cardiovascular disease
- image quality
- computed tomography
- dual energy
- contrast enhanced
- induced apoptosis
- poor prognosis
- signaling pathway
- positron emission tomography
- gene expression
- binding protein
- high resolution
- magnetic resonance imaging
- wild type
- coronary artery disease
- skeletal muscle
- dna methylation
- type diabetes
- stem cells
- single cell
- metabolic syndrome
- bone marrow
- cell proliferation
- high fat diet
- mesenchymal stem cells
- photodynamic therapy
- adipose tissue
- genome wide
- men who have sex with men
- hepatitis c virus
- quantum dots
- single molecule
- cell death
- long non coding rna
- hiv testing
- insulin resistance