MCBG Session 8 - Protein Function & Regulation Flashcards
Name 4 different protein (such as enzymes) regulation mechanisms.
1) Isoenzymes - different enzymes forms
2) Allosteric regulation - change in enzyme conformation
3) Phosphorylation - reversible covalent modification
4) Proteolytic activation
What are isoenzymes and how do they regulate protein function? - give an example
- Enzymes that catalyse the same reaction but have a different AA sequence - therefore have different activity. Made from different genes or different splicing of same gene.
- Activity can be higher or lower, e.g.: glucokinase is an isoenzyme of hexokinase and increases the rate of reaction.
How does allosteric regulation of enzymes work
- Binding to a site other than the active site to cause a conformational change in the protein.
- Can change the protein into a low affinity state (T-state) which lowers the rate of reaction (done by allosteric activators) or into a high affinity state (R-state) which increases rate of reaction (allosteric inhibitors).
- Does NOT obey Michaelis-Menten kinetics
Give an example of an enzyme that undergoes allosteric regulation
PFK-1 - activators that stabilise enzyme into R-state = AMP, Fructose-2,6-BP. Inhibitors that stabilise into T-state = citrate, AMP and H+
What is phosphorylation? How can it be reversed?
- Phosphorylation is the transfer of terminal phosphate on ATP to the -OH group of Ser, Thr & Tyr via protein kinases.
- Can be reversed by hydrolytic removal of phosphoryl by protein phosphotases.
Why is phosphorylation such an effective regulatory mechanism?
Free energy of PP is large as it adds 2 negative charges and the phosphoryl group can be H-bonds. Also allows for massive amplification effect.
- e.g.: when enzymes activate other enzymes the number of molecules affected increases geometrically in a cascade (can easily get 1,000,000 fold amplification)
What is proteolytic activation - when is it important?
Give an example.
Inactive precursor molecules, e.g.: zymogens or proenzymes having peptide bond cleaved (irreversibly) to make precursor active. Important when processes nee to be tightly controlled, e.g.: blood clotting, digestive enzymes, apoptosis.
- Enteropeptidases breaking down trypsinogen into active trypsin for digestion in GIT.
What are the main differences between Hb and myoglobin?
Hb:
- Carried in blood to transport oxygen all around the body.
- 4 polypeptie chains
- 4 haem groups per molecule
Myoglobin:
- Short term storage of oxygen, supplies it to muscle
- Higher affinity for oxygen
- 1 polypeptide chain + 1 haem group per molecule
The oxygen dissociation curve for Hb is sigmoidal - affinity for oxygen increases with PO2 of oxygen - why?
This is due to the co-operativity effect. Once oxygen binds Hb undergoes a conformational change into the R state (allosteric effect), which favours the further binding of oxygen. Therefore co-operativity enhances oxygen transport by Hb. This allows greater oxygen transport compared to myoglobin, as it is more within the R state.
Explain the allosteric effects of 2,3 - bisphosphoglycerate (2,3-BPG) on Hb.
- 2,3BPG binds to positively charge residues on B-subunit of Hb.
- This holds subunits together stabilising Hb in the low affinity T-state.
- Therefore favours unloading of oxygen and shifts oxygen dissociation curve to the right.
Explain the allosteric effects of H+ and CO2 on Hb. (AKA: the Bohr effect)
- Both H+ and CO2 bind and stabilise Hb in the low-affinity T-state
- This shifts the oxygen dissociation curve to the right
- Allows delivery of oxygen to metabolically active tissues that produce H+ and CO2.
Explain the effects of CO on oxygen binding to Hb.
- CO binds to Hb 250 x more readily than O2
- Blocks further oxygen binding once bound
- Stabilised Hb in R state - prevents dissociation at tissues (shifts curve to the left).
Describe the molecular basis for sickle cell disease.
1) Mutation of glutamate to valine in B-globin.
2) Val lies on surface in T-state (low affinity)
3) Reduces oxygen carrying capability, cells prone to lyse (anaemia) and are more rigid.
4) This blocks microvasculature such as capillaries.
Describe the 2 ways the blood clotting cascade can be activated to form a fibrin clot.
1) Intrinsic (damaged endothelial lining promotes binding of factor Xll) or extrinsic (trauma release tissue factor lll)
2) Both cause factor X activation, leads to thrombin activation
3) Thrombin causes formation of fibrin clot.
Why are only very small amounts of initial signal required to trigger formation of a clot?
As amplification occurs during each step in the cascade reaction - as a lot of these reactions are carried out by enzymes such as proteases.
