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CHEM 210 BIOCHEMISTRY MODULE 1 TO 8 EXAMS’ & FINAL EXAM (2025 / 2026) PORTAGE LEARNING – QUESTIONS AND CORRECT ANSWERS (VERIFIED ANSWERS) PLUS RATIONALES 2026 Q&A | INSTANT DOWNLOAD PDF.

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CHEM 210 BIOCHEMISTRY MODULE 1 TO 8 EXAMS’ & FINAL EXAM (2025 / 2026) PORTAGE LEARNING – QUESTIONS AND CORRECT ANSWERS (VERIFIED ANSWERS) PLUS RATIONALES 2026 Q&A | INSTANT DOWNLOAD PDF.

Institución
CHEM 210 BIOCHEMISTRY
Grado
CHEM 210 BIOCHEMISTRY

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CHEM 210 BIOCHEMISTRY MODULE 1 TO 8 EXAMS’ & FINAL EXAM () PORTAGE LEARNING – QUESTIONS AND
CORRECT ANSWERS (VERIFIED ANSWERS) PLUS RATIONALES 2026 Q&A | INSTANT DOWNLOAD PDF.
*Core Domains
Water, pH, and Buffers

Amino Acids, Peptides, and Proteins

Enzyme Kinetics and Inhibition

Carbohydrate Structure and Metabolism

Lipid Structure and Membranes

Lipid and Amino Acid Metabolism

Nucleic Acid Structure and Information Flow

Bioenergetics and Oxidative Phosphorylation

Biochemical Ethics and Regulatory Compliance
Introduction
This comprehensive assessment bank serves as a rigorous evaluative tool designed to measure mastery of essential biochemical principles
across foundational and applied contexts. Assessing key competencies in molecular structure, metabolic pathways, and enzymatic
mechanisms, the examination utilizes both standard multiple-choice questions and complex, scenario-based problems. These items
simulate real-world clinical, diagnostic, and research dilemmas, demanding high-level critical thinking and ethical decision-making. By
integrating regulatory compliance and ethical standards with core theoretical science, this test bank ensures candidates demonstrate the
practical problem-solving skills necessary for professional excellence in healthcare, research, and laboratory settings.


Section One: Questions 1–100
Question 1
A 45-year-old male presents to the emergency department with severe chest pain. Lab results indicate elevated serum levels of cardiac
troponin and lactate dehydrogenase (LDH). Biochemically, which structural property of enzymes allows LDH isoenzymes to be utilized as
tissue-specific diagnostic markers?
A. They possess identical primary structures but utilize different cofactors.
B. They consist of different subunit combinations that catalyze the same reaction in specific tissues.
C. They have different tertiary structures that bind completely distinct substrates.
D. They alter the overall equilibrium constant (Keq ) of the reaction depending on tissue requirements.


,🟢 B. They consist of different subunit combinations that catalyze the same reaction in specific tissues.
🔴 RATIONALE: LDH is a tetrameric enzyme composed of combinations of H (heart) and M (muscle) subunits. Different tissues express
distinct combinations of these subunits (isoenzymes), which catalyze the same chemical reaction but possess different kinetic properties
and electrophoretic mobilities, making them excellent tissue-specific biomarkers.
Question 2
A researcher is designing a buffer system at pH 7.4 for an in vitro translation assay. Which of the following weak acids would be the most
effective choice for maintaining this pH?
A. Acetic acid (pKa = 4.76)​




B. MES (pKa = 6.15)





C. HEPES (pKa = 7.55)





D. Boric acid (pKa = 9.24)





🟢 C. HEPES (pKa = 7.55) ​




🔴 RATIONALE: A buffer is most effective at resisting changes in pH within one pH unit of its pKa . Because the desired pH is 7.4, HEPES,





with a pKa of 7.55, is the closest to the target value and will provide maximum buffering capacity.





Question 3
A patient presents with a rare metabolic disorder characterized by an inability to properly methylate biomolecules. A deficiency in the
metabolism of which amino acid is most likely responsible for this condition?
A. Methionine
B. Alanine
C. Leucine
D. Phenylalanine
🟢 A. Methionine
🔴 RATIONALE: Methionine is the precursor to S-adenosylmethionine (SAM), which serves as the primary methyl group donor in numerous
biochemical methylation reactions, including DNA and lipid methylation.
Question 4
During a laboratory quality control audit, a technician discovers a solution of immunoglobulin G (IgG) has denatured after being stored at an
incorrect temperature. Which of the following non-covalent interactions is primarily responsible for stabilizing the tertiary structure of proteins
like IgG?
A. Peptide bonds
B. Hydrophobic interactions
C. Phosphodiester linkages
D. Coordination covalent bonds
🟢 B. Hydrophobic interactions

,🔴 RATIONALE: The tertiary structure of globular proteins is primarily driven and stabilized by the hydrophobic effect, where nonpolar side
chains cluster away from water in the protein's interior. Peptide bonds define the primary structure.
Question 5
An investigator characterising a novel competitive inhibitor of acetylcholinesterase notes its effects on enzyme kinetics. How does a
competitive inhibitor affect the Vmax and apparent Km of an enzymatic reaction?
​ ​




A. Decreases Vmax , decreases apparent Km
​ ​




B. Does not change Vmax , decreases apparent Km
​ ​




C. Decreases Vmax , increases apparent Km
​ ​




D. Does not change Vmax , increases apparent Km
​ ​




🟢 D. Does not change Vmax , increases apparent Km
​ ​




🔴 RATIONALE: Competitive inhibitors bind reversibly to the active site of the free enzyme. High substrate concentrations can overcome
this inhibition to reach the original maximum velocity (Vmax ), but more substrate is required to reach half-Vmax , effectively increasing the
​ ​




apparent Michaelis constant (Km ). ​




Question 6
A pharmaceutical company must pull a new drug candidate from clinical trials because it irreversibly binds to a vital cytochrome P450
enzyme via covalent modification. According to ethical and regulatory safety standards, this molecule would be classified as what type of
inhibitor?
A. Competitive inhibitor
B. Uncompetitive inhibitor
C. Noncompetitive inhibitor
D. Suicide inhibitor
🟢 D. Suicide inhibitor
🔴 RATIONALE: Suicide inhibitors (or mechanism-based inactivators) are structural analogs of the substrate that bind to the enzyme active
site and undergo chemical transformation by the enzyme itself, forming a permanent covalent bond that irreversibly inactivates it.
Question 7
A molecule of D-glucose and a molecule of D-galactose differ structurally only by the spatial configuration of the hydroxyl group around
carbon-4. These two sugars are best described as:
A. Anomers
B. Epimers
C. Enantiomers
D. Diastereomers that are not epimers
🟢 B. Epimers
🔴 RATIONALE: Epimers are a specific type of diastereomer that differ in configuration around only one chiral carbon atom. Since D-
glucose and D-galactose differ exclusively at C-4, they are C-4 epimers.

, Question 8
A patient with severe abdominal pain and hemolytic anemia is suspected of having a glucose-6-phosphate dehydrogenase (G6PD)
deficiency. This enzyme is crucial for generating which biochemical species required to protect erythrocytes from oxidative stress?
A. NADH
B. NADPH
C. FADH2
D. ATP
🟢 B. NADPH
🔴 RATIONALE: Glucose-6-phosphate dehydrogenase is the rate-limiting enzyme of the pentose phosphate pathway. It reduces N AD+ to
N ADP H , which provides the reducing equivalents necessary for glutathione reductase to convert oxidized glutathione back to its reduced
form, protecting cells from reactive oxygen species.
Question 9
Under anaerobic conditions in actively exercising human skeletal muscle, pyruvate is reduced to lactate. What is the primary biological
purpose of this reaction?
A. To generate extra ATP through substrate-level phosphorylation
B. To regenerate N AD + required for glycolysis to continue
C. To produce lactate for structural synthesis within the cell
D. To lower intracellular pH to activate phosphofructokinase-1
🟢 B. To regenerate N AD+ required for glycolysis to continue
🔴 RATIONALE: Glycolysis requires a steady supply of N AD+ at the glyceraldehyde-3-phosphate dehydrogenase step. Under anaerobic
conditions, oxidative phosphorylation cannot regenerate N AD + , so the reduction of pyruvate to lactate by lactate dehydrogenase fulfills this
requirement.
Question 10
A clinical research protocol involves studying the regulation of glycogen synthesis. Which of the following modifications directly activates
glycogen synthase?
A. Phosphorylation by protein kinase A (PKA)
B. Phosphorylation by glycogen synthase kinase-3 (GSK3)
C. Dephosphorylation by protein phosphatase 1 (PP1)
D. Allosteric binding of adenosine triphosphate (ATP)
🟢 C. Dephosphorylation by protein phosphatase 1 (PP1)
🔴 RATIONALE: Glycolysis and glycogen storage enzymes are often regulated reciprocal to breakdown. Glycogen synthase is active in its
dephosphorylated form (glycogen synthase a) and inactive when phosphorylated. Protein phosphatase 1 removes these phosphate groups,
activating the enzyme.
Question 11
A newborn presents with vomiting, lethargy, and hepatomegaly shortly after consuming breast milk. Tests indicate a hereditary deficiency in

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Institución
CHEM 210 BIOCHEMISTRY
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CHEM 210 BIOCHEMISTRY

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Subido en
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Escrito en
2025/2026
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