A 45-year-old woman with type 1 diabetes mellitus is brought to the emergency department by her husband because of polyuria, nausea, vomiting, and altered mental status for 4 hours. On arrival, she is unconscious. Treatment with a drug is begun that increases glucose transport to skeletal muscle and adipose tissue. Which of the following cellular events is most likely to also occur in response to this drug?

Dephosphorylation of fructose-1,6-bisphosphatase

Increased activity of acyl-CoA dehydrogenases

Cleavage of UDP from UDP-glucose

Upregulation of glucose transporter type 3 expression

Phosphorylation of glycogen phosphorylase kinase

You have been asked to deliver a lecture to medical students about the effects of various body hormones and neurotransmitters on the metabolism of glucose. Which of the following statements best describes the effects of sympathetic stimulation on glucose metabolism?

Epinephrine increases liver glycogenolysis.

Norepinephrine causes increased glucose absorption within the intestines.

Without epinephrine, insulin cannot act on the liver.

Peripheral tissues require epinephrine to take up glucose.

Sympathetic stimulation to alpha receptors of the pancreas increases insulin release.

To maintain blood glucose levels even after glycogen stores have been depleted, the body, mainly the liver, is able to synthesize glucose in a process called gluconeogenesis. Which of the following reactions of gluconeogenesis requires an enzyme different from glycolysis?

Fructose 1,6-bisphosphate --> Fructose-6-phosphate

Glyceraldehyde 3-phosphate --> 1,3-bisphosphoglycerate

2-phosphoglycerate --> 3-phosphoglycerate

Dihydroxyacetone phosphate --> Glyceraldehyde 3-phosphate

Phosphoenolpyruvate --> 2-phosphoglycerate

Maturity Onset Diabetes of the Young (MODY) type 2 is a consequence of a defective pancreatic enzyme, which normally acts as a glucose sensor, resulting in a mild hyperglycemia. The hyperglycemia is especially exacerbated during pregnancy. Which of the following pathways is controlled by this enzyme?

Glucose --> glucose-6-phosphate

Fructose-6-phosphate --> fructose-1,6-bisphosphate

Phosphoenolpyruvate --> pyruvate

Glucose-6-phosphate --> fructose-6-phosphate

Glyceraldehyde-3-phosphate --> 1,3-bisphosphoglycerate

A newborn undergoing the standard screening tests is found to have a positive test for reducing sugars. Further testing is performed and reveals that the patient does not have galactosemia, but rather is given a diagnosis of fructosuria. What levels of enzymatic activity are altered in this patient?

Hexokinase unchanged; fructokinase decreased

Hexokinase decreased; fructokinase decreased

Hexokinase unchanged; fructokinase unchanged

Hexokinase increased; fructokinase increased

Hexokinase increased; fructokinase decreased

Rate-limiting enzymes and control points for USMLE Step 2 CK: High-Yield Biochemistry Lessons

The Irreversible Steps - Glycolysis Gatekeepers

Glycolysis pathway with key enzymes and metabolic fates These three irreversible enzymes are the key control points. 📌 Mnemonic: Hungry People Prefer Pie.

Hexokinase / Glucokinase:
- Hexokinase is inhibited by its product, glucose-6-phosphate.
- Glucokinase (liver, pancreas) is induced by insulin.
Phosphofructokinase-1 (PFK-1):
- The main rate-limiting, committed step.
- Activators: ↑ AMP, ↑ fructose-2,6-bisphosphate.
- Inhibitors: ↓ ATP, ↓ citrate.
Pyruvate Kinase:
- Activated by fructose-1,6-bisphosphate (feed-forward).
- Inhibited by ↓ ATP, ↓ alanine.

⭐ Fructose-2,6-bisphosphate is the most potent PFK-1 activator, ensuring glycolysis proceeds in a well-fed state (high insulin).

Step 1 Control - The Glucose Sensors

Hexokinase and Glucokinase Kinetics

Feature	Hexokinase	Glucokinase (Hexokinase IV)
Location	Most tissues	Liver, β-cells of pancreas
$K_m$	Low (↑ affinity)	High (↓ affinity)
$V_{max}$	Low (↓ capacity)	High (↑ capacity)
Regulation	Feedback inhibited by Glucose-6-Phosphate (G6P).	Induced by insulin; inhibited by Fructose-6-Phosphate (F6P).

The Committed Step - PFK-1 Master Switch

Phosphofructokinase-1 (PFK-1) is the major rate-limiting and committed step of glycolysis. It catalyzes the irreversible phosphorylation of Fructose-6-Phosphate to Fructose-1,6-bisphosphate.

Allosteric Regulation: PFK-1 activity is finely tuned by cellular energy levels.

Hormonal Control via PFK-2/FBPase-2: This bifunctional enzyme regulates Fructose-2,6-bisphosphate (F-2,6-BP), the most potent allosteric activator of PFK-1.
- Fed State (↑Insulin/↓Glucagon): ↓cAMP → ↓PKA → Dephosphorylated PFK-2 is active → ↑F-2,6-BP → ↑Glycolysis.
- Fasting State (↓Insulin/↑Glucagon): ↑cAMP → ↑PKA → Phosphorylated FBPase-2 is active → ↓F-2,6-BP → ↓Glycolysis.

⭐ High-Yield: Fructose-2,6-bisphosphate is the most powerful activator of PFK-1, overriding inhibition by ATP.

Regulation of PFK-2/FBPase-2 by phosphorylation

📌 Mnemonic: AMP Activates, ATP Alleviates (Inhibits).

Final Checkpoint - Pyruvate Kinase Rules

Catalyzes the final irreversible step of glycolysis ($PEP \rightarrow Pyruvate$). It's a key control point, especially in the liver.

Feed-forward Activation:
- - Strongly activated by Fructose-1,6-bisphosphate (F-1,6-BP). This links it to the PFK-1 commitment step.
Allosteric Inhibition:
- - ATP (high energy signal).
- - Alanine (alternative pyruvate source).
Hormonal Control (Liver only):
- - Glucagon (fasting state) → Phosphorylation → Inactivation.
- - Insulin (fed state) → Dephosphorylation → Activation.

⭐ A deficiency in pyruvate kinase causes chronic hemolytic anemia. Mature RBCs depend entirely on glycolysis for ATP to maintain their membrane integrity.

Glycolysis and Gluconeogenesis Regulation

Phosphofructokinase-1 (PFK-1) is the major rate-limiting enzyme of glycolysis.

ATP and citrate are key allosteric inhibitors, signaling an energy-rich state.

AMP and fructose-2,6-bisphosphate are the most potent allosteric activators.

Hexokinase is inhibited by its product, glucose-6-phosphate; glucokinase is induced by insulin.

Pyruvate kinase is allosterically activated by fructose-1,6-bisphosphate (feed-forward regulation) and inhibited by ATP and alanine.

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