Regulation Of Protein Activity Flashcards
Long term regulation
change in the rate of protein synthesis
change in the rate of protein degradation
Isoezymes
Different forms of the same enzymes that often have different kinetic properties
Product inhibition
Accumulation of a product inhibits its own production
e.g. Glucose-6-phosphate inhibits hexokinase activity - important in controlling the rate at which different tissues metabolise glucose
Allosteric regulation
Allosteric activators increase the proportion of enzymes in the R state (high affinity)
Allosteric inhibitors increase the proportion of enzymes in the T state (low affinity)
Phosphofructokinase is allosterically regulated and sets the pace for glycolysis (activated by AMP, inhibited by ATP)
Covalent modification - phosphorylation
Protein kinases - transfer of terminal phosphate from ATP to -OH group of Ser, Thr, Tyr (large negative charge)
Protein phosphatase - catalyses the hydrolytic removal of phosphoryl groups from proteins
Enzyme cascade
Enzymes activate enzymes - the number of affected molecules increases geometrically. Amplifies the initial signal by several orders of magnitude within a few milliseconds.
Specific proteolytic cleavage
Cut at specific amino acids
Don’t want active enzymes, that are usually secreted, inside of cells so are made in the inactive form - zymogens - they are then cleaved to an active form when they are needed
Rate of protein synthesis
The body responds to an increase in metabolites by making more enzymes - happens with alcohol - body responds to high alcohol consumption by making more enzyme to break down the alcohol
The blood clotting cascade
allows the formation of a clot form activation of very small amounts of the initial factor
Extrinsic pathway - (simulates the intrinsic pathway) activated by trauma
Factor X activation (common endpoint for both pathways
Leads to thrombin activation (Gla domains)
Which leads to the formation of a fibril clot
+ve Ca2+ pulls the clotting factors out of the blood since they are -ve (localises the clot)
Extrinsic pathway
due to vascular damage
Tissue factor III activates Tissue factor VII which activates Factor X
Thrombin activates the formation of the Fibrin clot
(This then stimulates the intrinsic pathway)
Intrinsic Pathway
Factor XI activates Factor IV which then activates Factor X
Leads to the activation of Thrombin and then the formation of the Fibrin clot
Formation of a Fibrin Clot
Thrombin cleaves fibrinopeptides A and B from the central globular domain of fibrinogen.
Globular domains at the C-terminal ends of the beta and gamma.chains interact with exposed sequences at the N-terminal of the cleaves beta and alpha chains to form a fibrin mesh or clot.
The newly formed clot is stabilised by the formation of a ice bonds.
Haemophilia
Defect in factor VIII
Stopping the clotting process
Dilution of clotting factors by blood flow and by removal by liver
Digestion by proteases
Specific inhibitors - antithrombin III
Fibrinolytic - breaks up of the clot after the tissue has been repaired (can be stimulated by streptokinase)
Short term regulation
substrate and product concentration change in enzyme conformation ~ allosteric regulation ~ covalent modification ~ proteolytic cleavage
