Characteristics of the type of Inhibition

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uncompetitive inhibition

no ES complex is formed

substrate mimics

-bind to the active site act as competitive inhibition - does not let the substrate react ex: ibuprofen inhibit prostaglandin synthase acting as an anti-inflammatory drug

Uncompetitive inhibitors

-forms ternary complex -blocks turnover of the substrate to the product -binds to a different site on the enzyme or protein -blocks the proper association of enzyme subunits

mix/noncompetitive inhibition

-it can form a complex with E to form an EI complex or form a complex with ES to form the ESI complex - neither has affinity

Examples if inhibitor design

-mimic the substrate -mimic the inhibitor - irreversibly react with a key enzyme involve in the pathway change the conformation or state of assembly of the enzyme

uncompetitive inhibition

-not possible to overcome the inhibition -vmax cannot be reached by adding more and more substrate - adding more substrate gives inhibitor more ES complex to bind to which gives more opportunity for inhibition

Heaavy metal toxicity

Once heavy metal is bond the sulfhydryl cannot be used for catalysis

combination therapy

combining two inhibitors that target the same pathway

Competitive Inhibitor

compete with substrate for binding to the enzyme

KI

can also be noted as an inhibitory dissociation constant

in competitive inhibition the↑ concentration of substrate

can restore the rate of the rxn

Heavy Metal Toxicity

enzymes with sulfhydryl groups that are needed for catalytic activity form tight bonds with mercury, lead, silver, iron, copper

in competitive inhibition an ↑ concentration

equals ↑ in Km

competetitive inhibitor

forms the EI complex

Irreversible inhibitionn

links covalently and irreversibly with the enzyme ex: aspirin in actylatng a key serine residue in the active site oof cyclooxygenase

nerve agents

react with agents that inhibit acetylcholinesterases used to kill insects parathion, durban

Transition state mimic

resembles the transition state does not complete the reaction appears to be stabilizing

Heavy metal toxicity ex:

syphylis treatment which deactivates the enzyme via treatment with mercury and bismuth

suicide substrate

the enzyme "kills itself" when binding to the inhibitor

Suicide substrate

the enzyme binds to the inhibitor and the inhibitor permanently kills the enzyme

irreversible inhibition

the enzyme is no longer active new enzyme is the only way enzymatic activity can be restored

in competitive inhibition competitive inhibitor

the plot is linear v max doesn't change the slope off the plot ↑ as the inhibitor increases

combination therapy example

trimethylprim and sulfamethoxazole -trimethylprim- targets purine synthesis, pyrimidine synthesis, and synthesis of certain amino acids

uncompetitive inhibition

uncommon inhibitor binds to the ES complex not to the free enzyme forms an ESI complex

Irreversible inhibition

--covalent attachment of the enzyme to the inhibitor - covalent modification to the key residues of the enzyme

Transition state mimic

2' deoxycoformycin ( inhibits adenosine deaminase)

Statins

inhibit HMGCoA reductase lowers cholesterol levels they are reversible

Suicide substrate

inhibitor reactive until the enzyme attempts to use it as an enzyme

Gleevc

inhibits protein kinase production and block proliferation of cancer cells


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