A patient in renal failure exhibits metabolic acidosis. What compensatory mechanism is most likely activated?

Increased renal HCO3- reabsorption

What is the primary mechanism for maintaining acid-base balance during prolonged vomiting?

Increased bicarbonate excretion

Increased chloride reabsorption

A person with type 1 diabetes ran out of her prescription insulin and has not been able to inject insulin for the past 3 days. The patient is hyperventilating to compensate for her metabolic acidosis. Which of the following reactions explains this respiratory compensation for metabolic acidosis?

CO2 + H2O ⇌ H2CO3 ⇌ H+ + HCO3-

CH3CHOHCH2COOH ⇌ CH3CHOHCH2COO- + H+

Assertion: In a patient with chronic kidney disease (CKD) and metabolic acidosis, sodium bicarbonate should be initiated to correct acidosis. Reason: Sodium bicarbonate therapy reduces the progression of kidney disease by decreasing tubular injury and slowing fibrosis.

Both Assertion and Reason are true, but Reason is NOT the correct explanation of Assertion

Assertion is false, but Reason is true

Both Assertion and Reason are true, and Reason is the correct explanation of Assertion

Assertion is true, but Reason is false

What is the primary enzyme responsible for the conversion of carbon dioxide to bicarbonate in erythrocytes?

The action of carbonic anhydrase in erythrocytes

The high solubility of CO2 in water

The role of hemoglobin in CO2 transport

The conversion of carbon dioxide to carbonic acid

Renal Regulation of Acid-Base Balance for INI-CET: High-Yield Physiology Lessons

Renal Regulation: Overview - Kidney's Balancing Act

Kidneys: Primary long-term regulators of systemic acid-base balance.
Crucial for maintaining blood pH within narrow physiological limits.
Key actions:
- Excrete non-volatile acids (H⁺).
- Reabsorb virtually all filtered HCO₃⁻.
- Generate new HCO₃⁻ to replenish buffer stores.
Response: Slower onset (hours to days) vs. lungs, but more potent and definitive for chronic imbalances.

⭐ Kidneys are slower but ultimately more powerful than lungs in correcting chronic acid-base disturbances.

Renal Regulation: HCO3- Handling - Bicarb's Big Rescue

Kidneys reclaim virtually all filtered bicarbonate ($HCO_3^-$) to prevent its loss in urine, crucial for acid-base homeostasis.
Reabsorption sites:
- ~80-90% in Proximal Convoluted Tubule (PCT).
- ~10-15% in Thick Ascending Limb (TAL).
- Remaining in Distal Tubule & Collecting Ducts (CD).
Mechanism: Indirect reabsorption; filtered $HCO_3^-$ isn't directly transported across apical membrane.

Renal bicarbonate reabsorption in proximal tubule

Key Enzymes: Carbonic Anhydrase (CA) - Type IV (luminal brush border) & Type II (cytoplasmic).
Basolateral $HCO_3^-$ exit from cell (PCT):
- Na+-$HCO_3^-$ cotransporter (NBCe1-A): 1 Na+ : 3 $HCO_3^-$.
- Cl-/$HCO_3^-$ exchanger (AE1).
Regulation: ↑ $HCO_3^-$ reabsorption with ↑ PCO2, ↓ ECF volume (Angiotensin II ↑NHE3), ↓ K+ (hypokalemia).

⭐ Carbonic anhydrase inhibitors (e.g., acetazolamide) impair $HCO_3^-$ reabsorption, leading to metabolic acidosis.

Renal Regulation: Acid Excretion - Proton Purge Party

Kidneys excrete fixed acids (~50-100 mEq/day) and regenerate buffered $HCO_3^-$.
Key $H^+$ Excretion & $HCO_3^-$ Regeneration Mechanisms:
- 1. Titratable Acid (TA) Excretion:
  - Secreted $H^+$ combines with filtered buffers (mainly phosphate): $HPO_4^{2-} + H^+ \leftrightarrow H_2PO_4^-$.
  - Occurs in PCT, DCT, and collecting ducts (CD).
  - Each $H^+$ excreted as TA adds one new $HCO_3^-$ to blood.
  - Limited by buffer availability (max ~30-40 mEq/day).
- 2. Ammonium ($NH_4^+$) Excretion:
  - PCT metabolizes glutamine $\rightarrow NH_3$ (diffuses to lumen) + $\alpha$-KG.
  - Lumen: $NH_3$ (from cell) $+ H^+$ (secreted) $\leftrightarrow NH_4^+$ (trapped).
  - Each $NH_4^+$ excreted adds one new $HCO_3^-$ to blood.
  - Crucial adaptive response, especially in chronic acidosis. 📌 "AmmONIA for AcidOSIS"

⭐ In chronic acidosis, $NH_4^+$ excretion can increase more than 10-fold, becoming the dominant mechanism for acid elimination.

Renal Regulation: Control & Chaos - Kidney's Command Center

Key Modulators:
- Arterial $PCO_2$:
  - ↑$PCO_2$: ↑$H^+$ secretion, ↑$HCO_3^-$ reabsorption (resp. acidosis comp.).
  - ↓$PCO_2$: ↓$H^+$ secretion, ↓$HCO_3^-$ reabsorption (resp. alkalosis comp.).
- ECF Volume:
  - Contraction (e.g., diuretics): ↑$Ang II$ → ↑NHE3, ↑$H^+$-ATPase → ↑$HCO_3^-$ reabsorption (Contraction Alkalosis).
  - Expansion: ↓$HCO_3^-$ reabsorption.
- Plasma $[K^+]$:
  - Hypokalemia: ↑$H^+$ secretion, ↑$HCO_3^-$ reabsorption → Metabolic Alkalosis.
  - Hyperkalemia: ↓$H^+$ secretion, ↓$HCO_3^-$ reabsorption → Metabolic Acidosis.
- Aldosterone:
  - Stimulates $H^+$ secretion (α-intercalated cells: $H^+$-ATPase, $H^+$-$K^+$-ATPase).
  - Excess → Metabolic Alkalosis.
- PTH:
  - ↓PCT $HCO_3^-$ reabsorption.
  - ↓PCT $PO_4^{3-}$ reabsorption → ↑Titratable acid.
- Systemic Acid/Alkali Load:
  - Chronic Acidosis: ↑$NH_3$/$NH_4^+$ production & excretion.
  - Chronic Alkalosis: ↓$NH_3$/$NH_4^+$ production & excretion.

⭐ Hypokalemia stimulates H+ secretion and HCO3- reabsorption, contributing to metabolic alkalosis.

High‑Yield Points - ⚡ Biggest Takeaways

Kidneys are crucial for long-term acid-base balance via HCO₃⁻ handling and H⁺ excretion.

PCT reabsorbs ~85% of filtered HCO₃⁻, dependent on carbonic anhydrase.

Net acid excretion (and new HCO₃⁻ gain) occurs via titratable acidity (H₂PO₄⁻) and NH₄⁺ excretion.

NH₄⁺ excretion (from glutamine) is the most important adaptive mechanism for acid load.

Aldosterone stimulates H⁺ secretion in collecting ducts (Type A intercalated cells).

Urine pH varies (4.5-8.0); K⁺ levels significantly impact renal acid handling.

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