Deck 6: Enzymes: The Catalysts of Life

A)crystallize urease, the first enzyme isolated.
B)originate the term ferments to describe enzymes.
C)isolate the insulin hormone.
D)prove that enzymes were carbohydrates.
E)discover ribozymes.

A)specific to the organs in which they are produced.
B)inactivated by inhibitors in the small intestine.
C)sensitive to changes in pH.
D)inactivated by movement.
E)consumed by the quantities of substrate in the small intestine.

A)[S] >> Km.
B)[S] << Km.
C)[S] = Km.
D)both A and B
E)both B and C

A)can be determined using the Lineweaver- Burk plot.
B)is equal to twice the Vmax.
C)is equal to the substrate concentration at Vmax/2.
D)choices A, B, and C
E)both A and C

A)quantum tunneling
B)altering the temperature within the cell to one appropriate for reactions to proceed
C)inefficient collisions
D)permanently binding substrates
E)decreasing the number of reactive molecules

A)accepting protons from the enzyme.
B)donation of protons to the enzyme.
C)a change in enzyme conformation induced by substrate binding.
D)formation of temporary covalent bonds.
E)all of the above

A)binds at the regulatory site.
B)increases the rate of substrate binding.
C)binds and activates the high- affinity state of the enzymes.
D)is identical to the active site.
E)is converted to an activator by the enzyme.

A)This state is composed of the difference in activation energy of a catalyzed versus an uncatalyzed reaction.
B)This state changes the position of the equilibrium, but not the rate.
C)The metastable state is formed by transient complexes with the substrate.
D)The metastable state is created by the prosthetic group of the enzyme.
E)The metastable state is a state of the substrate in which the reaction can proceed, but usually will not proceed, without a catalyst.

A)has the y intercept as Vmax.
B)has the x axis as substrate concentration.
C)slope can be used to determine Km.
D)has the y axis as v/[S].
E)both C and D

A)a noncompetitive inhibitor.
B)penicillin.
C)isoleucine.
D)a competitive inhibitor.
E)acetylcholinesterase.

A)substrate analogs
B)nitrous oxide
C)noncompetitive inhibitors
D)intercalating agents
E)X- rays

A)Some enzymes accept any of a whole group of substrates.
B)Many enzymes are extremely specific regarding a substrate.
C)Cells are often able to carry out metabolic activity with only a handful of enzymes.
D)Many enzymes cannot recognize a stereoisomer of their substrate.
E)Carboxypeptidase recognizes any of the amino acids from the carboxyl end of a polypeptide.

A)carboxypeptidase A
B)iron
C)histidine
D)ATP
E)N- acetylmuramic acid

A)It is non- linear.
B)It illustrates enzyme specificity.
C)It reveals the presence of prosthetic groups in enzymes.
D)It is a single- reciprocal plot.
E)It makes it easier to determine Vmax.

A)enzymes do not function as well at temperatures other than the optimal temperature.
B)sweating removes prosthetic groups from biological enzymes.
C)the higher temperature increases the activity of lysases.
D)bacteria reproduce more rapidly at higher body temperature.
E)fever blocks synthesis of proteins in the bacterial nucleus.

A)contains amino acids that are contiguous to one another along the primary sequence of the protein.
B)involves only six out of a total of 307 amino acids.
C)uses iron as the prosthetic group.
D)is formed by the interaction of two polypeptide chains.
E)contains a glutamate residue at position 69.

A)produces modifications that can sometimes be reversed.
B)affects the activity of an enzyme by adding or removing a chemical group.
C)can involve the addition of phosphate groups.
D)can activate an enzyme.
E)all of the above

A)the six major classes of enzyme function
B)the size of the enzyme
C)the name of the substrate
D)an indication of the size of the substrate
E)a description of substrate function

A)denaturation of an enzyme.
B)inhibition of enzyme function by blocking the active site.
C)the substrate concentration at which velocity reaches one- half maximum velocity.
D)the inability to increase reaction velocity beyond a finite upper limit.
E)a characteristic of all uncatalyzed reactions.

A)allosteric regulation
B)substrate- level phosphorylation
C)saturation
D)feedback inhibition
E)covalent modification

A)intron removal from pre- rRNA.
B)zymogen.
C)ribonuclease P.
D)autocatalytic RNAs.
E)peptidyl transferase.

A)hydrolase
B)oxidoreductase
C)protease
D)transferase
E)ligase

A)proposes that very strong covalent bonds are formed upon substrate binding.
B)is also called the lock- and- key model.
C)was proposed by Hans Buchner.
D)states that substrate- enzyme interactions are rigid.
E)involves a conformational change in the shape of the enzyme.

A)v
B)kcat
C)[S]
D)Km
E)Vmax

A)a glycine residue
B)a polypeptide chain
C)carboxypeptidase A
D)a zinc ion
E)a nickel catalyst

A)binds at a site other than the active site.
B)does not inhibit enzyme activity, but lowers substrate concentration.
C)irreversibly binds and inactivates the enzyme.
D)binds to and inactivates the substrate.
E)cannot be processed by the enzyme.

A)transferases
B)isomerases
C)oxidoreductases
D)ligases
E)hydrolases

A)The y intercept is equal to 1/Vmax.
B)It is a linear plot.
C)The x intercept is - 1/Km.
D)Its slope is the same as the Eadie- Hofstee plot.
E)It is a double reciprocal plot.

A)activation site.
B)metastable site.
C)active site.
D)catalyst.
E)prosthetic group.

A)hydrolases
B)oxidoreductases
C)ligases
D)isomerases
E)transferases

A)binds substrates in a manner that facilitates the formation of product.
B)does not change the rate at which the equilibrium is achieved.
C)is always a protein.
D)decreases the rate of a reaction.
E)changes the position of the equilibrium of the reaction.