In hypoparathyroidism:

Plasma calcium is low and inorganic phosphorous high

Plasma calcium is high and inorganic phosphorous low

Plasma calcium and inorganic phosphorous are low

Plasma calcium and inorganic phosphorous are high

Which of the following is the primary mechanism that drives sodium reabsorption in the proximal tubule?

Active sodium transport via the Na+-K+-ATPase pump at the basolateral membrane.

Sodium reabsorption through cotransport with amino acids at the luminal membrane.

Sodium reabsorption through cotransport with glucose at the luminal membrane.

Sodium reabsorption through countertransport with hydrogen ions at the luminal membrane.

All of the following statements regarding stones in the submandibular gland are true except one:

Majority of submandibular stones are radiolucent

Patient presents with acute pain and swelling in the region of the submandibular gland

80% of stones occur in the submandibular gland

The hypoglossal nerve is at risk during submandibular gland excision

The function of which of the following is increased by an elevated parathyroid hormone concentration:

Phosphate reabsorptive pathways in the renal tubules

Hepatic formation of 25-hydroxycholecalciferol

Calcium and Phosphate Handling for UPSC-CMS: High-Yield Physiology Lessons

Ca & PO4 Basics - The Dynamic Duo

Calcium ($Ca^{2+}$):
- Total plasma: 9-11 mg/dL (2.2-2.7 mmol/L).
- Forms: Ionized (~50%, active), albumin-bound (~40%), complexed (citrate, phosphate, ~10%).
- Key Functions: Bone/teeth mineralization, muscle contraction, nerve impulse, blood coagulation.
- Major Regulators: Parathyroid Hormone (PTH), Vitamin D, Calcitonin.
Phosphate ($PO_4^{3-}$):
- Plasma: 2.5-4.5 mg/dL (0.8-1.45 mmol/L).
- Key Functions: Bone/teeth structure, energy (ATP), DNA/RNA, acid-base buffer.
- Major Regulators: PTH, Vitamin D, Fibroblast Growth Factor 23 (FGF-23).
Key Interplay:
- Often reciprocal: PTH $\uparrow Ca^{2+}$ reabsorption, $\downarrow PO_4^{3-}$ reabsorption in kidney.
- $Ca \times PO_4$ product: If > 55 mg²/dL², risk of ectopic calcification.

⭐ Ionized calcium (~50% of total) is the biologically active form and its levels are meticulously controlled.

Calcium's Kidney Journey - Tight Leash Calcium

Overall: ~99% filtered $Ca^{2+}$ reabsorbed.
Segments & % Reabsorption:
- PCT: 60-70% (mainly paracellular, solvent drag).
- TAL: 20-25% (paracellular via claudins; transcellular).
- DCT: 5-10% (active, transcellular; main regulatory site).
  - Apical: TRPV5 channels.
  - Intracellular: Calbindin-D28K.
  - Basolateral: PMCA ($Ca^{2+}$-ATPase), NCX1 ($Na^{+}/Ca^{2+}$ exchanger).
- CD: <1%.
Key Regulators (DCT/TAL):
- ↑ Reabsorption:
  - PTH (↑ TRPV5, calbindin, PMCA).
  - Vitamin D (Calcitriol) (↑ TRPV5, calbindin).
  - Thiazide diuretics (📌 Thia-HIDE $Ca^{2+}$: ↑ reabsorption).
  - Hypocalcemia, Alkalosis.
- ↓ Reabsorption:
  - Hypercalcemia (via CaSR).
  - Loop diuretics (↓ TAL paracellular transport).
  - Acidosis.
  - Calcitonin (minor effect).

⭐ Thiazide diuretics enhance calcium reabsorption in the DCT, beneficial for preventing recurrent calcium kidney stones.

Phosphate's Path - Phosphorus Freeway

Primary Reabsorption Sites: Proximal Convoluted Tubule (PCT) (~80%), Distal Convoluted Tubule (DCT).
PCT Mechanisms:
- Apical Na⁺-Phosphate cotransporters: NaPi-IIa, NaPi-IIc.
- Secondary active transport, dependent on Na⁺/K⁺-ATPase.
- Process is saturable (Tm-limited).
Key Regulators:
- PTH (Parathyroid Hormone): ↓ Phosphate reabsorption (internalizes NaPi-IIa/c in PCT) → phosphaturia.
- FGF-23 (Fibroblast Growth Factor 23): ↓ Phosphate reabsorption (↓ NaPi-IIa/c expression in PCT) → phosphaturia.
- Vitamin D (Active - Calcitriol): ↑ Phosphate reabsorption (stimulates NaPi-IIa/c expression).
- Dietary Phosphate: ↑ intake → ↓ reabsorption; ↓ intake → ↑ reabsorption.
- Insulin: ↑ reabsorption.
- Acidosis: ↓ reabsorption; Alkalosis: ↑ reabsorption.
Excretion: Primarily renal; matches net intestinal absorption.

Phosphate Handling: Hormonal Regulation

⭐ PTH and FGF-23 are the principal phosphaturic hormones, significantly decreasing renal phosphate reabsorption, primarily in the PCT.

Hormonal Harmony - The Calcium Commandos

Three main hormones precisely control renal Ca²⁺ & PO₄³⁻ levels: PTH, Vitamin D, and Calcitonin. Their interplay is crucial.

Parathyroid Hormone (PTH): Secreted by parathyroid glands.
- Kidney Actions:
  - ↑ Ca²⁺ reabsorption (mainly DCT, TAL).
  - ↓ PO₄³⁻ reabsorption (PCT) → phosphaturia.
  - ↑ $1\alpha$-hydroxylase activity → ↑ active Vitamin D ($1,25(OH)_2D_3$).
Vitamin D (Calcitriol - $1,25(OH)_2D_3$): Steroid hormone, activated in kidney.
- Kidney Actions: ↑ Ca²⁺ reabsorption & ↑ PO₄³⁻ reabsorption (mainly PCT, DCT).
Calcitonin: Secreted by thyroid C-cells (parafollicular cells).
- Kidney Actions: Weakly ↓ Ca²⁺ & ↓ PO₄³⁻ reabsorption.
- 📌 Calcitonin tones down serum Ca²⁺.

Hormonal control of calcium and phosphate

⭐ PTH's major effect on phosphate is to cause phosphaturia by inhibiting Na⁺/PO₄³⁻ cotransporters in the PCT.

High‑Yield Points - ⚡ Biggest Takeaways

PTH ↑ Ca²⁺ reabsorption (DCT, TAL) & ↓ PO₄³⁻ reabsorption (PCT).

Vitamin D (Calcitriol) ↑ Ca²⁺ & PO₄³⁻ reabsorption across PCT & DCT.

FGF-23 ↓ PO₄³⁻ reabsorption (PCT) & ↓ 1α-hydroxylase activity (↓ calcitriol).

PCT reabsorbs the majority: ~65% Ca²⁺ & ~80% PO₄³⁻.

TAL reabsorbs ~25% Ca²⁺ paracellularly, driven by Na⁺-K⁺-2Cl⁻ cotransporter.

DCT fine-tunes Ca²⁺ reabsorption (~8%), regulated by PTH & Vitamin D.

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