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HYPERKALEMIA DR. K. K. GUPTA MD ASSOCIATE PROF. DEPARTMENT OF MEDICINE, KGMU.

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Presentation on theme: "HYPERKALEMIA DR. K. K. GUPTA MD ASSOCIATE PROF. DEPARTMENT OF MEDICINE, KGMU."— Presentation transcript:

1 HYPERKALEMIA DR. K. K. GUPTA MD ASSOCIATE PROF. DEPARTMENT OF MEDICINE, KGMU

2 HyperkalemiaMCQs 1.Hyperkalemia can occur in all except-- - a) Insulin Deficiency b) Metabolic Acidosis c) Acute Renal Failure d) Cushing’s Syndrome

3 2.True about Hyperkalemia--- a) ECG changes correlates with S.potassium b) ECG is diagnostic c) Stops heart in systole d) Insulin –Glucose is given

4 3.All of following are used for treatment of hyperkalemia except--- a)Calciumgluconate b)Sodium bicarbonate c) Beta blockers d)i.v. infusion of glucose with insulin

5 4.Which secretion contributes to the maximum ammount of K + ---  Gastric  Pancreatic  Salivary  Biliary

6 5. All are TRUE about hyperkalemia except— a) Prolonged PR interval b) Prolonged QRS interval c) Sine wave pattern d) Prolonged QT interval

7 DEFINITION : Hyperkalemiais defined as a plasma potassium level of 5.5 mM. It occurs in up to 10% of hospitalized patients; severe hyperkalemia(>6.0 mM) occurs in approximately 1%, with a significantly increased risk of mortality

8 factitious hyperkalemiaor pseudohyperkalemia: an artifactual increase in serum K+ due to the release of K+ during or after venipuncture. Pseudohyperkalemiacan occur in the setting of excessive muscle activity during venipuncture (fist clenching, etc.),

9 Causes of Hyperkalemia I. “Pseudo” hyperkalemia: A. Cellular efflux: thrombocytosis, erythrocytosis, leukocytosis, in vitro hemolysis B. Hereditary defects in red cell membrane transport

10 II. Intra- to extracellular shift A. Acidosis B. Hyperosmolality; radiocontrast, hypertonic dextrose, mannitol C. β-adrenergic antagonists (noncardioselective agents) D. Digoxin and related glycosides (yellow oleander, foxglove, bufadienolide) E. Hyperkalemic periodic paralysis F. Lysine, arginine, and ε-aminocaproic acid (structurally similar, positively charged) G. Succinylcholine; thermal trauma, neuromuscular injury, disuse atrophy, mucositis, or prolonged immobilization H. Rapid tumor lysis

11 III. Inadequate excretion A. Inhibition of the renin-angiotensin-aldosterone axis; ↑ risk of hyperkalemia when used in combination 1. Angiotensin-converting enzyme (ACE) inhibitors 2. Renin inhibitors: aliskiren [in combination with ACE-inhibitors or angiotensin receptor blockers (ARBs)] 3. ARBs 4. Blockade of the mineralocorticoid receptor: spironolactone, eplerenone, drospirenone 5. Blockade of ENaC: amiloride, triamterene, trimethoprim, pentamidine, nafamostat B. Decreased distal delivery 1. Congestive heart failure 2. Volume depletion

12 C. Hyporeninemichypoaldosteronism 1. Tubulointerstitial diseases: systemic lupus erythematosus (SLE), sickle cell anemia, obstructive uropathy 2. Diabetes, diabetic nephropathy 3. Drugs: nonsteroidal anti-inflammatory drugs, cyclooxygenase 2 (COX-2) inhibitors, beta blockers, cyclosporine, tacrolimus 4. Chronic kidney disease, advanced age 5. Pseudohypoaldosteronism type II: defects in WNK1 or WNK4 kinases D. Renal resistance to mineralocorticoid 1. Tubulointerstitial diseases: SLE, amyloidosis, sickle cell anemia, obstructive uropathy, post-acute tubular necrosis 2. Hereditary: pseudohypoaldosteronism type I: defects in the mineralocorticoid receptor or ENaC

13 E. Advanced renal insufficiency 1. Chronic kidney disease 2. End-stage renal disease 3. Acute oliguric kidney injury F. Primary adrenal insufficiency 1. Autoimmune: Addison’s disease, polyglandularendocrinopathy 2. Infectious: HIV, cytomegalovirus, tuberculosis, disseminated fungal infection 3. Infiltrative: amyloidosis, malignancy, metastatic cancer 4. Drug-associated: heparin, low-molecular-weight heparin 5. Hereditary: adrenal hypoplasiacongenita, congenital lipoid adrenal hyperplasia, aldosteronesynthase deficiency 6. Adrenal hemorrhage or infarction, including in antiphospholipid syndrome

14 Clinical features Cardiac arrhythmias associated with hyperkalemia include sinus bradycardia, sinus arrest, slow idioventricular rhythms, ventricular tachycardia, ventricular fibrillation, and asystole. Other effects of hyperkalemiainclude weakness, neuromuscular paralysis(without central nervous system disturbances) And suppression of renal ammonia genesis, which may result in metabolic acidosis. Mild increases in extracellular K+ resulting in changes in T-wave morpho logy; further increase in plasma K+ concentration depresses intracardiac conduction, with progressive prolongation of the PR and QRS intervals. Severe hyperkalemiaresults in loss of the P wave and a progressive widening of the QRS complex.

15 electrocardiographic manifestations in hyperkalemia

16 DIAGNOSTIC APPROACH

17 Treatment of Hyperkalemia 1. Immediate antagonism of the cardiac effects of hyperkalemia: Use of 10 ml of 10% calcium gluconate(3-4 ml of calcium chloride) infused intravenously over 2 to 3 min. The effect of the infusion starts in 1-3min and lasts 30- 60 minutes.

18 Reduction of plasma K + by redistribution into the cells: 1. The recommended drug is 10 units of IV regular Insulin followed immediately by 50 ml of 50% dextrose. The effect begins in 10-20 minutes, peaks at 30-60 minutes and lasts 4-6 hours. As hypoglycemia is common with insulin and glucose this should be followed by 10% of dextrose at 50-75 ml/hour.

19 2. Beta 2 agonists most commonly albuterol are also effective agents in the treatment of hyperkalemia. However ~20% of patients with end stage renal disease are resistant to the effects of beta 2 agonists. The recommended dose of nebulizedalbuterol is 10-20 mg in 4 ml of normal saline inhaled over 10 minutes.

20 The effect of beta 2 agonists starts at about 30 minutes reaches its peak at about 90 minutes and lasts 2-6 hours. 3. Intravenous bicarbonate has no role in the routine treatment of hyperkalemia. It should be reserved for patients with hyperkalemia and metabolic acidosis. It should be infused in an isotonic or hypotonic fluid.

21 4. Removal of potassium: Accomplished by the use of cation exchange resins, diuretics or dialysis. Sodium polystyrene sulfonate exchanges Na + for K + in the gastrointestinal tract and increases the fecal excretion of K +. The dose of SPS is 15-30 gram. The full effect may take up to 24 hours and usually requires repeated doses every 4-6 years. Intestinal necrosis is the most serious complication of SPS.

22 Loop and Thiazide diuretics can be utilized to reduce plasma K +. Hemodialysis is the most effective and reliable method to reduce K + concentration. Peritoneal dialysis is considerably less effective.

23 THANKING YOU

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