Gitelman syndrome: Difference between revisions
Ostermayer (talk | contribs) (Created page with "Gitelman syndrome is an autosomal recessive salt-losing tubulopathy caused by loss-of-function mutations in the '''thiazide-sensitive sodium-chloride cotransporter (NCC)''' in the distal convoluted tubule.<ref name="StatPearls">Gitelman Syndrome. ''StatPearls''. NCBI. 2024.</ref> It is the '''most common inherited renal tubulopathy''' (~1 in 40,000) and presents with '''hypokalemic metabolic alkalosis, hypomagnesemia, and hypocalciuria''' — biochemically identical to '...") |
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==Background== | ==Background== | ||
*Gitelman syndrome is an autosomal recessive salt-losing tubulopathy caused by loss-of-function mutations in the thiazide-sensitive sodium-chloride cotransporter (NCC) in the distal convoluted tubule<ref name="StatPearls">Gitelman Syndrome. ''StatPearls''. NCBI. 2024.</ref> | |||
*It is the most common inherited renal tubulopathy (~1 in 40,000) and presents with hypokalemic metabolic alkalosis, hypomagnesemia, and hypocalciuria — biochemically identical to chronic thiazide diuretic use<ref name="KDIGO">Gitelman syndrome: consensus and guidance from a KDIGO Controversies Conference. ''Kidney Int''. 2017;91(1):24-33.</ref> | |||
*Usually diagnosed in adolescence or adulthood, it is generally benign but can cause life-threatening hypokalemia, cardiac arrhythmias, tetany, paralysis, and rhabdomyolysis | |||
*The EM physician encounters Gitelman syndrome as unexplained refractory hypokalemia in a young normotensive patient, tetany or muscle cramps, or cardiac arrhythmia from combined hypokalemia and hypomagnesemia | |||
*Prevalence ~1 in 40,000 (heterozygote carrier frequency ~1% in Caucasians); higher in Asian populations | *Prevalence ~1 in 40,000 (heterozygote carrier frequency ~1% in Caucasians); higher in Asian populations | ||
*Much more common than [[Bartter syndrome]] (~1 in 1,000,000) | *Much more common than [[Bartter syndrome]] (~1 in 1,000,000) | ||
*Usually presents | *Usually presents after age 6; most diagnosed in adolescence or adulthood — many patients are asymptomatic for years | ||
*Mimics | *Mimics chronic thiazide (HCTZ) use — the NCC cotransporter is the same target as thiazide diuretics | ||
* | *Sudden cardiac death has been reported from severe hypokalemia/hypomagnesemia<ref name="KDIGO"/> | ||
==Clinical Features== | ==Clinical Features== | ||
*Many patients are | *Many patients are asymptomatic — discovered incidentally on routine labs showing hypokalemia | ||
* | *Muscle cramps, weakness, fatigue — the most common complaints | ||
* | *Tetany, carpopedal spasm — from hypomagnesemia; especially during illness or with vomiting/diarrhea | ||
* | *Facial paresthesias — characteristic | ||
* | *Salt craving (sometimes intense; also craving sour foods) | ||
* | *Thirst, nocturia, polyuria (milder than Bartter) | ||
* | *Constipation | ||
* | *Low or normal blood pressure — despite elevated renin/aldosterone | ||
* | *Chondrocalcinosis — calcium pyrophosphate crystal deposition in joints (from chronic hypomagnesemia); may present with acute pseudogout-like joint pain and swelling<ref name="KDIGO"/> | ||
* | *Prolonged QT interval — present in ~50%; risk of ventricular arrhythmias | ||
* | *Severe presentations (uncommon): hypokalemic paralysis (especially in Asian populations), rhabdomyolysis, seizures, ventricular arrhythmia/cardiac arrest | ||
==Differential Diagnosis== | ==Differential Diagnosis== | ||
* | *[[Bartter syndrome]]: the key differential — more severe, earlier onset, '''hypercalciuria''' (vs hypocalciuria in Gitelman), mimics loop diuretic (vs thiazide); see comparison table on [[Bartter syndrome]] page | ||
* | *Surreptitious vomiting / bulimia: urine chloride <25 mEq/L (Gitelman: urine Cl >35 mEq/L) | ||
* | *Thiazide diuretic use/abuse: identical lab picture — screen urine for diuretics | ||
* | *Laxative abuse: low urine potassium (renal potassium wasting distinguishes Gitelman) | ||
* | *Primary hyperaldosteronism: hypertension present (Gitelman is normotensive/hypotensive) | ||
* | *Renal tubular acidosis: metabolic acidosis (not alkalosis) | ||
* | *Hypomagnesemia from other causes: PPI use, alcoholism, aminoglycosides, cisplatin — check medication history | ||
* | *Pseudogout (if presenting with chondrocalcinosis): check electrolytes in any young patient with calcium pyrophosphate arthropathy — may unmask Gitelman | ||
==Evaluation== | ==Evaluation== | ||
===Workup=== | ===Workup=== | ||
* | *BMP: hypokalemia (often 2.5-3.0 mEq/L), hypochloremia, elevated bicarbonate (metabolic alkalosis) | ||
* | *Magnesium: low (<1.6 mg/dL) in most patients — '''always check magnesium when you find hypokalemia''' | ||
* | *Urine electrolytes: | ||
** | **Urine chloride >35 mEq/L — confirms renal salt wasting (excludes vomiting) | ||
**Urine potassium elevated (inappropriate renal K wasting) | **Urine potassium elevated (inappropriate renal K wasting) | ||
** | **Urine calcium:creatinine ratio LOW (hypocalciuria) — the key distinction from Bartter (which has hypercalciuria) | ||
* | *ECG: prolonged QT, flattened T waves, U waves, ST depression; assess for arrhythmia | ||
* | *Urine drug screen for diuretics — must exclude thiazide abuse before diagnosing Gitelman | ||
===Diagnosis=== | ===Diagnosis=== | ||
* | *Hypokalemic hypochloremic metabolic alkalosis + hypomagnesemia + hypocalciuria + normal/low BP + urine Cl >35 = Gitelman pattern | ||
*Exclude vomiting (urine Cl <25), diuretic abuse (urine drug screen), and medications causing hypomagnesemia | *Exclude vomiting (urine Cl <25), diuretic abuse (urine drug screen), and medications causing hypomagnesemia | ||
*Genetic testing (SLC12A3 mutations) is confirmatory but not an ED test | *Genetic testing (SLC12A3 mutations) is confirmatory but not an ED test | ||
* | *Clinical and biochemical diagnosis is sufficient to initiate treatment | ||
==Management== | ==Management== | ||
* | *Correct hypokalemia: | ||
** | **IV KCl for severe hypokalemia (<2.5 mEq/L), ECG changes, or arrhythmias | ||
**Oral KCl for mild-moderate cases | **Oral KCl for mild-moderate cases | ||
**'''Correct hypomagnesemia FIRST''' — magnesium deficiency causes | **'''Correct hypomagnesemia FIRST''' — magnesium deficiency causes refractory hypokalemia that will not correct until magnesium is repleted<ref name="StatPearls"/> | ||
* | *Correct hypomagnesemia: | ||
** | **IV magnesium sulfate (2 g over 15-30 min, then infusion) for severe hypomagnesemia, tetany, or arrhythmias | ||
**Oral magnesium supplementation for chronic management (magnesium oxide, magnesium citrate) | **Oral magnesium supplementation for chronic management (magnesium oxide, magnesium citrate) | ||
**GI side effects (diarrhea) limit oral magnesium dosing — a major compliance issue | **GI side effects (diarrhea) limit oral magnesium dosing — a major compliance issue | ||
* | *Cardiac monitoring: continuous telemetry if K <3.0 mEq/L, prolonged QT, or any arrhythmia | ||
* | *Continue home medications: potassium-sparing diuretics (amiloride, spironolactone), oral potassium and magnesium supplements — '''do NOT discontinue''' | ||
*'''Do NOT use thiazide diuretics''' — this worsens the underlying defect | *'''Do NOT use thiazide diuretics''' — this worsens the underlying defect | ||
* | *NSAIDs (indomethacin): sometimes used chronically as adjunctive therapy (reduces prostaglandin-mediated salt wasting) — continue if prescribed | ||
* | *Treat precipitating illness: any condition causing vomiting, diarrhea, or fever can precipitate electrolyte crisis in Gitelman patients | ||
==Disposition== | ==Disposition== | ||
* | *Admit: | ||
**Severe hypokalemia (<2.5 mEq/L) or symptomatic hypokalemia (arrhythmia, paralysis, rhabdomyolysis) | **Severe hypokalemia (<2.5 mEq/L) or symptomatic hypokalemia (arrhythmia, paralysis, rhabdomyolysis) | ||
**Tetany or seizures | **Tetany or seizures | ||
**QT prolongation with arrhythmia | **QT prolongation with arrhythmia | ||
**Unable to tolerate oral supplements | **Unable to tolerate oral supplements | ||
* | *Discharge with close follow-up: | ||
**Mild-moderate hypokalemia correctable with oral supplements | **Mild-moderate hypokalemia correctable with oral supplements | ||
**No cardiac symptoms or ECG abnormalities | **No cardiac symptoms or ECG abnormalities | ||
**Tolerating PO | **Tolerating PO | ||
**Nephrology follow-up within 1-2 weeks | **Nephrology follow-up within 1-2 weeks | ||
* | *New diagnosis suspected (unexplained hypokalemic alkalosis + hypomagnesemia + hypocalciuria in a normotensive patient): arrange nephrology referral for confirmation and long-term management | ||
* | *Counsel patients: liberal salt intake; high-potassium foods; take magnesium and potassium supplements reliably; seek care promptly during illness (vomiting/diarrhea can precipitate dangerous electrolyte drops); report palpitations, weakness, or muscle spasms immediately | ||
==See Also== | ==See Also== | ||
Revision as of 11:14, 19 March 2026
Background
- Gitelman syndrome is an autosomal recessive salt-losing tubulopathy caused by loss-of-function mutations in the thiazide-sensitive sodium-chloride cotransporter (NCC) in the distal convoluted tubule[1]
- It is the most common inherited renal tubulopathy (~1 in 40,000) and presents with hypokalemic metabolic alkalosis, hypomagnesemia, and hypocalciuria — biochemically identical to chronic thiazide diuretic use[2]
- Usually diagnosed in adolescence or adulthood, it is generally benign but can cause life-threatening hypokalemia, cardiac arrhythmias, tetany, paralysis, and rhabdomyolysis
- The EM physician encounters Gitelman syndrome as unexplained refractory hypokalemia in a young normotensive patient, tetany or muscle cramps, or cardiac arrhythmia from combined hypokalemia and hypomagnesemia
- Prevalence ~1 in 40,000 (heterozygote carrier frequency ~1% in Caucasians); higher in Asian populations
- Much more common than Bartter syndrome (~1 in 1,000,000)
- Usually presents after age 6; most diagnosed in adolescence or adulthood — many patients are asymptomatic for years
- Mimics chronic thiazide (HCTZ) use — the NCC cotransporter is the same target as thiazide diuretics
- Sudden cardiac death has been reported from severe hypokalemia/hypomagnesemia[2]
Clinical Features
- Many patients are asymptomatic — discovered incidentally on routine labs showing hypokalemia
- Muscle cramps, weakness, fatigue — the most common complaints
- Tetany, carpopedal spasm — from hypomagnesemia; especially during illness or with vomiting/diarrhea
- Facial paresthesias — characteristic
- Salt craving (sometimes intense; also craving sour foods)
- Thirst, nocturia, polyuria (milder than Bartter)
- Constipation
- Low or normal blood pressure — despite elevated renin/aldosterone
- Chondrocalcinosis — calcium pyrophosphate crystal deposition in joints (from chronic hypomagnesemia); may present with acute pseudogout-like joint pain and swelling[2]
- Prolonged QT interval — present in ~50%; risk of ventricular arrhythmias
- Severe presentations (uncommon): hypokalemic paralysis (especially in Asian populations), rhabdomyolysis, seizures, ventricular arrhythmia/cardiac arrest
Differential Diagnosis
- Bartter syndrome: the key differential — more severe, earlier onset, hypercalciuria (vs hypocalciuria in Gitelman), mimics loop diuretic (vs thiazide); see comparison table on Bartter syndrome page
- Surreptitious vomiting / bulimia: urine chloride <25 mEq/L (Gitelman: urine Cl >35 mEq/L)
- Thiazide diuretic use/abuse: identical lab picture — screen urine for diuretics
- Laxative abuse: low urine potassium (renal potassium wasting distinguishes Gitelman)
- Primary hyperaldosteronism: hypertension present (Gitelman is normotensive/hypotensive)
- Renal tubular acidosis: metabolic acidosis (not alkalosis)
- Hypomagnesemia from other causes: PPI use, alcoholism, aminoglycosides, cisplatin — check medication history
- Pseudogout (if presenting with chondrocalcinosis): check electrolytes in any young patient with calcium pyrophosphate arthropathy — may unmask Gitelman
Evaluation
Workup
- BMP: hypokalemia (often 2.5-3.0 mEq/L), hypochloremia, elevated bicarbonate (metabolic alkalosis)
- Magnesium: low (<1.6 mg/dL) in most patients — always check magnesium when you find hypokalemia
- Urine electrolytes:
- Urine chloride >35 mEq/L — confirms renal salt wasting (excludes vomiting)
- Urine potassium elevated (inappropriate renal K wasting)
- Urine calcium:creatinine ratio LOW (hypocalciuria) — the key distinction from Bartter (which has hypercalciuria)
- ECG: prolonged QT, flattened T waves, U waves, ST depression; assess for arrhythmia
- Urine drug screen for diuretics — must exclude thiazide abuse before diagnosing Gitelman
Diagnosis
- Hypokalemic hypochloremic metabolic alkalosis + hypomagnesemia + hypocalciuria + normal/low BP + urine Cl >35 = Gitelman pattern
- Exclude vomiting (urine Cl <25), diuretic abuse (urine drug screen), and medications causing hypomagnesemia
- Genetic testing (SLC12A3 mutations) is confirmatory but not an ED test
- Clinical and biochemical diagnosis is sufficient to initiate treatment
Management
- Correct hypokalemia:
- IV KCl for severe hypokalemia (<2.5 mEq/L), ECG changes, or arrhythmias
- Oral KCl for mild-moderate cases
- Correct hypomagnesemia FIRST — magnesium deficiency causes refractory hypokalemia that will not correct until magnesium is repleted[1]
- Correct hypomagnesemia:
- IV magnesium sulfate (2 g over 15-30 min, then infusion) for severe hypomagnesemia, tetany, or arrhythmias
- Oral magnesium supplementation for chronic management (magnesium oxide, magnesium citrate)
- GI side effects (diarrhea) limit oral magnesium dosing — a major compliance issue
- Cardiac monitoring: continuous telemetry if K <3.0 mEq/L, prolonged QT, or any arrhythmia
- Continue home medications: potassium-sparing diuretics (amiloride, spironolactone), oral potassium and magnesium supplements — do NOT discontinue
- Do NOT use thiazide diuretics — this worsens the underlying defect
- NSAIDs (indomethacin): sometimes used chronically as adjunctive therapy (reduces prostaglandin-mediated salt wasting) — continue if prescribed
- Treat precipitating illness: any condition causing vomiting, diarrhea, or fever can precipitate electrolyte crisis in Gitelman patients
Disposition
- Admit:
- Severe hypokalemia (<2.5 mEq/L) or symptomatic hypokalemia (arrhythmia, paralysis, rhabdomyolysis)
- Tetany or seizures
- QT prolongation with arrhythmia
- Unable to tolerate oral supplements
- Discharge with close follow-up:
- Mild-moderate hypokalemia correctable with oral supplements
- No cardiac symptoms or ECG abnormalities
- Tolerating PO
- Nephrology follow-up within 1-2 weeks
- New diagnosis suspected (unexplained hypokalemic alkalosis + hypomagnesemia + hypocalciuria in a normotensive patient): arrange nephrology referral for confirmation and long-term management
- Counsel patients: liberal salt intake; high-potassium foods; take magnesium and potassium supplements reliably; seek care promptly during illness (vomiting/diarrhea can precipitate dangerous electrolyte drops); report palpitations, weakness, or muscle spasms immediately
See Also
External Links
- StatPearls — Gitelman Syndrome
- Kidney Int — KDIGO Controversies Conference: Gitelman syndrome (2017)
- Orphanet J Rare Dis — Gitelman syndrome (2008)