L18: Protein Breakdown Flashcards
Why degrade proteins?
Regulation of protein levels
Defective proteins (incorrectly inserted AA, misfolded partially or unfolded, incorrectly modified, damaged by oxidation or proteolytic cleavage -> carbonyl group)
Lysosomes
Vesicles 0.2-0.5 um in diameter
Bounded by single membrane
Contain hydrolytic enzyme
Formed from Golgi apparatus
Digest molecules from outside of cell and inside cell
Protein degradation
Proteins- extracellular, membrane and intracellular
Acidic environment: helps unfold protein to make more susceptible proteases
Acidic proteases
Macroautophagy (lysosome autophagy)
Regulated catabolic process
Degrade macromolecular & organelle constituents
Steps in macroautophagy
Phagophore: cup-shaped structure formed in cytoplasm (formed from ATG proteins and associated lipids)
Autophagosome- closure of phagophore around sequestered material. Double membrane
Fusion with lysosome
Microautophagy
Lysosomal membrane undergoes invagination of protrusion to enclose cargo for degradation
Chaperone mediated autophagy
Hsc70-containing chaperone complex recognises protein -> bind to receptor
Delivery to lysosome-associated membrane protein type-2a (LAMP 2A)
Proteasomes
Eukaryotic cells- 20S proteosomes and 26S proteosomes
26S proteosome- 2 x 19S regulators plus 20S proteosome
19S regulators- cap structures & selected ubiquinated proteins for degradation
Eukaryotic proteins are targeted for proteasome destruction by ubiquitination
Ubiquination
Covalent addition of ubiquitin. Ubiquitin highly conserved, 76 residue (8.5kD) protein found widely in eukaryotes
Widely utilised form of posttranslational modification in eukaryotes (but not prokaryotes)
Marks proteins for regulated proteolytic destruction by proteosome
Ub bunds onto lysine residue
Attach ub group through c terminal to AA residues -> repeated -> ub bound to lysine through c terminus. Lysine binds to c terminus of other ub and so on
Ways which proteins can be ubiquinated
Mono-ubiquitylation -> histone regulation, regulate DNA repair and gene expression
Multi-ubiquitylation -> endocytosis
Polyubiquitylation -> proteasomal degradation. Protein degradation
Polyubiquitylation -> DNA repair
Proteins involved in ubiquination process
E1: Ubiquitin-activating enzyme
E2: ubiquitin-carrier protein
E3: ubiquitin-protein ligase. Different ligases with differing substrate specificity
Ubiquination steps
- Terminal carboxyl group of ubiquitin is joined to E1. ATP dependent step
- Ubiquitin transferred to E2
- E3 transfers activated to the epsilon-amino group of Lys residue of target protein
Muscle weakness in ageing
Loss of myofibres -> cell death
Decreased myofibre size
Protein synthesis < protein catabolism
Protein catabolism
Proteins have finite lifespan
Different proteins in same tissue have different half-lives. <1hr to a week for liver enzymes. Stability correlates with sequence at N-terminus
Proteins in different tissues have different half-lives
Cathepsins: example of protein targeting and post-translational modifications
Major lysosomal proteases
Signal peptide: directs insertion of nascent polypeptide chain into ER
ER: signal peptide is cleaved with assistance of proregion. Disulfide bond formation. N-linked glycosylation with high-mannose glycans
Golgi: mannose residues phosphorylated -> mannose 6-phosphate. M6p routes protein into endosomal/lysosomal compartment via m6p receptor. Portion not converted to m6p form and is shunted into exocytosis pathway
Endosome: acidification. Activation: cleavage of proregion and proteolytic processing in lysosome into heavy and light chains
