Which enzyme in the Krebs cycle is indirectly affected by hyperammonemia due to its impact on metabolic pathways?

Alpha-Ketoglutarate dehydrogenase

Protein metabolism after trauma is characterized by the following except:

Inhibition of skeletal muscle breakdown by interleukin 1 and tumour necrosis factor

Increased liver gluconeogenesis

Increased urinary nitrogen loss

Hepatic synthesis of acute phase reactants

Which of the following is NOT required for gluconeogenesis from lactate?

Transamination of pyruvate to alanine

Transport of lactate from muscle to liver

Conversion of lactate to pyruvate

Interorgan Metabolite Exchange for NEET-PG: High-Yield Biochemistry Lessons

Interorgan Metabolite Exchange - Metabolic Symphony

Organs communicate via circulating metabolites to meet energy demands.
- Liver: "Metabolic Maestro". Exports glucose (gluconeogenesis, glycogenolysis), ketone bodies, VLDL. Processes lactate, alanine, glycerol.
- Skeletal Muscle: Uses glucose, fatty acids, ketone bodies. Stores glycogen. Exports lactate (Cori cycle), alanine (glucose-alanine cycle).
- Adipose Tissue: Stores TAGs. Releases fatty acids & glycerol during fasting.
- Brain: Obligate glucose user (normally ~120g/day); adapts to ketone bodies in prolonged starvation.
- Kidney: Gluconeogenesis (e.g., from glutamine) during prolonged fasting/acidosis. Excretes nitrogenous waste.
- Intestine: Uses glutamine as primary fuel. Exports citrulline.

⭐ During prolonged starvation, the kidney can contribute up to 50% of glucose production via gluconeogenesis.

Fed State Exchange - Postprandial Powwow

Hormones: ↑ Insulin, ↓ Glucagon.
Goal: Anabolism (storage of glucose, AAs, fats).
📌 Insulin: "INto cells" for glucose (muscle/adipose).
Gut: Absorbs glucose, AAs (portal vein → Liver); CMs (lymph → blood).
Liver: Central hub.
- Glucose → Glycogen; excess → FAs → VLDL.
- AAs → Protein synthesis; BCAAs → Muscle.
- CM remnants cleared; FAs → VLDL.
Muscle:
- Glucose (GLUT4, insulin) → Glycogen, ATP.
- BCAAs → Protein synthesis.
Adipose:
- Glucose (GLUT4, insulin) → Glycerol-3-P.
- FAs (CMs, VLDL via LPL) + Glycerol-3-P → TAG storage.
Brain/RBCs: Glucose uptake (insulin-independent).

⭐ > Insulin is key: promotes glucose uptake in muscle & adipose tissue by translocating GLUT4 transporters to the cell membrane.

Fasting State Exchange - Famine Fortitude

Glucagon ↑, Insulin ↓. Goal: Maintain blood glucose for brain & RBCs; spare protein.

Initial Phase (Post-absorptive to ~24h)
- Liver: Glycogenolysis (main glucose source, depletes by ~18-24h). Gluconeogenesis (GNG) begins (lactate, alanine, glycerol).
- Adipose: Lipolysis ↑ (Hormone Sensitive Lipase - HSL) → FFAs (energy for muscle/liver) + Glycerol (GNG substrate).
- Muscle: Protein breakdown → Alanine, Glutamine (GNG substrates).
Prolonged Phase (Starvation >24-48h)
- Liver: GNG (primary glucose source). Ketogenesis ↑↑ (from FFAs) → $\beta$-hydroxybutyrate, acetoacetate.
- Adipose: Sustained lipolysis.
- Muscle: ↓ Glucose uptake. Uses FFAs, ketone bodies. Protein catabolism ↓ (sparing).
- Brain: Adapts to use ketone bodies (up to 70% energy).
- Kidney: Significant GNG (up to 50% of total GNG in late starvation).

Interorgan Metabolite Exchange in Fed and Fasting States

⭐ During prolonged starvation, the kidney can contribute up to 50% of total gluconeogenesis, highlighting its crucial role beyond excretion.

Key Metabolic Cycles - Shuttles & Switches

Cori Cycle (Lactic Acid Cycle):
- Muscle (anaerobic): Glucose $\rightarrow$ Lactate $\rightarrow$ Liver.
- Liver: Lactate $\rightarrow$ Glucose (gluconeogenesis) $\rightarrow$ Muscle.
- Function: Sustains muscle glycolysis; prevents acidosis. Net cost: 4 ATP.
Glucose-Alanine Cycle (Cahill Cycle):
- Muscle: Glucose $\rightarrow$ Pyruvate; Pyruvate + NH2 $\rightarrow$ Alanine $\rightarrow$ Liver.
- Liver: Alanine $\rightarrow$ Pyruvate (gluconeogenesis) + NH2 (urea cycle).
- Function: N-transport from muscle; glucose for muscle.
Glycerol-3-Phosphate Shuttle:
- Cytosolic NADH e- $\rightarrow$ Mitochondrial FADH2 (to Complex II).
- Yield: ~1.5 ATP / NADH. Sites: Skeletal muscle, brain.
Malate-Aspartate Shuttle:
- Cytosolic NADH e- $\rightarrow$ Mitochondrial NADH (to Complex I).
- Yield: ~2.5 ATP / NADH. Sites: Liver, heart, kidney.

Glucose-Alanine Cycle: Liver and Muscle Metabolism

⭐ The Cori Cycle recycles lactate from anaerobic muscle glycolysis to glucose in the liver, costing a net 4 ATP, thus shifting metabolic burden.

High‑Yield Points - ⚡ Biggest Takeaways

Liver: Central metabolic hub for gluconeogenesis, urea cycle, ketogenesis.

Muscle: Uses glucose, fatty acids, ketones; releases alanine, lactate.

Brain: Primarily glucose-dependent; adapts to ketone bodies in starvation.

Adipose Tissue: Stores triglycerides; mobilizes fatty acids, glycerol.

Kidney: Contributes to gluconeogenesis (prolonged fast); ammonia excretion.

RBCs: Solely glucose-dependent (anaerobic); produce lactate for Cori cycle.

Glucose-Alanine cycle: Key for nitrogen transport from muscle to liver.

Continue reading on Oncourse

CONTINUE READING — FREE

or get the app

App Store|Google Play