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ELECTROLYTE DISASTERS POTASSIUM JOSE-MARIE EL-AMM NEPHROLOGY DIVISION WSU/DMC/HUH AUGUST, 2006 COMPOSITION OF BODY FLUID COMPARTMENTS COMPOSITION OF ECF AND ICF ECF ICF Na K Cl HCO3 PHOSPHATE 141 4.1 113 26 2.0 10 120-150 3 10 140(ORGANIC) GENERATION OF THE RMP THE RESTING MEMBRANE POTENTIAL VIRTUALLY ALL K EXCRETION OCCURS IN THE CCD MAJOR SITE OF K+ SECRETION 70-80% 600-700 mmol Mid to Late DT and CCD 15-20% 3000 mmol 60-90 mmol Collecting tubules have selective Na channels in luminal surface (favored movement by Na levels low in cells and intracellular negativity). Pumped out of tubular cells by NaK-ATPase. Tubular lumen negatively charged and favors K movement into lumen by K channels. Aldo when combined with its receptor enhances Na reabsorption & K secretion via # Na channels & # NaK-ATPase pumps. Amiloride & Triamterene close Na channels directly Spironolactone competes w/ aldosterone ANP inhibits Na reabsorption by closing Na channels HYPERKALEMIA PSEUDOHYPERKALEMIA SHIFTS IMPAIRED RENAL EXCRETION PSEUDOHYPERKALEMIA MECHANICAL TRAUMA INCREASED WBC INCREASED PLATELETS A 30 YEAR OLD MAN WITH TYPE 1 DIABETES MELLITUS IS COMATOSE. EXAM: BP 110/70 HR 100/MIN LYING 80/50 116 AT 45 ° TEMP 101 ° RR 24 LABS 128 94 6.1 11 34 538 1.9 WHY IS HIS POTASSIUM HIGH? !!!!! INTAKE/SHIFT/OUTPUT !!!!! A 30 YEAR OLD MAN WITH TYPE 1 DIABETES MELLITUS IS COMATOSE. Low serum sodium Corrected Na= 128 + 7 = 135 Low bicarbonate <14 so metabolic acidosis AG= 23 Corrected bicarb 24 Elevated BUN/creatinine ARF vs. CRF vs. Acute on Chronic Hyperkalemia HORMONES THAT SHIFT K INTO CELLS ACTIVATED BY 3 Na+ 2 K+ 2ADRENERGICS ELECTROGENIC ATP ADP Na+ K+ ATP H+ ACTIVATED BY ADP ACTIVATED BY SYNTHESIS OF NEW NaK ATPase G6P2(CREATES ELECTRONEUTRAL NEW ANIONS) INSULIN GLUCOSE INSULIN BUFFERING OF H+ AND THE K+ SHIFT H+ HCl ClH+ H-BUFFER+ BUFFER K+ KIDNEY HYPOXIA, NO INSULIN L-LACTATE -, -HB - L-LACTATE H+ , -HB H-BUFFER+ BUFFER K SHIFTS OUT OF CELL IN ACIDOSIS WITH HCl-NOT ORGANIC ACIDOSIS K EXCRETION ALTERED BY ALDOSTERONE, RENAL STATUS SHIFTS Rhabdomyolysis; tissue breakdown Drugs; Digoxin, succinyl choline DKA, hyperosmolar state 54 YEAR OLD MAN WITH MILD RENAL FAILURE. C/O DIFFICULTY IN GETTING OUT OF CHAIRS. HE RECENTLY WAS STARTED ON A LOW SODIUM DIET BUT NO NEW MEDICATIONS. EXAM: SLIGHTLY DECREASED SKIN TURGOR MARKED PROXIMAL MUSCLE WEAKNESS LABS: ECG HAS PEAKED T WAVES, WIDENED QRS 130 9.8 98 17 “mild hemolysis” pH=7.32 CREATININE 2.7 (WAS 2.1) THE INTERN DRAWS BLOOD TO REPEAT THE LABS (R/O “LAB ERROR”). THE RESIDENT HAS A SEIZURE. WHY? LABORATORY ERROR IS NOT ASSOCIATED WITH SYMPTOMS! THIS MAN HAS BOTH SKELETAL MUSCLE AND CARDIAC MUSCLE SYMPTOMS OF HYPERKALEMIA. WHY DID HE SUDDENLY BECOME HYPERKALEMIC? WHY IS HIS POTASSIUM HIGH? !!!!! INTAKE/SHIFT/OUTPUT !!!!! IS HE TAKING A SALT SUBSTITUTE???? CRF: RENAL DISEASE CONTRIBUTES BUT DIDN’T CAUSE HIS K PROBLEMS. PEOPLE WITH CRF CAN HAVE TROUBLE WITH SODIUM CONSERVATION IF THERE ARE SUDDEN CHANGES IN THEIR INTAKE. DECREASED TOTAL BODY SODIUM LEADS TO DECREASED RENAL BLOOD FLOW, DECREASED Na PAST THE DISTAL TUBULE AND HENCE DECREASED K EXCRETION. !!!!! INTAKE/SHIFT/OUTPUT !!!!! FACTORS THAT DECREASE URINARY POTASSIUM EXCRETION 1. LOW URINE FLOW RATES 2. DECREASED Na DELIVERY TO DISTAL TUBULE (ARF, AGN, ESLD) 3. DECREASED MINERALOCORTICOID ACTIVITY (Renin-Ag system) VIRTUALLY ALL K EXCRETION OCCURS IN THE CCD MAJOR SITE OF K+ SECRETION Na+ Na+ H2O + CO2 H2CO3 K+ H+ K+ ALDO NONALDO HCO3+ + H+ TREATMENT OF HYPERKALEMIA 1.CALCIUM 2.INSULIN 3.ALBUTEROL 4.KAYEXALATE 5.HEMODIALYSIS 10mL OF 10% Ca GLUCONATE OVER 10 MINUTES 10 U IVP (REGULAR) WITH 50mL 50% DEXTROSE 10 mg NEBULIZED 0.5 mg IV 30-60 G PO OR 60 G AS ENEMA TREATMENT OF HYPERKALEMIA 1.CALCIUM 2.INSULIN 3.ALBUTEROL 4.KAYEXALATE 5.HEMODIALYSIS 10mL OF 10% Ca GLUCONATE OVER 10 MINUTES 10 U IVP (REGULAR) WITH 50mL 50% DEXTROSE 10 mg NEBULIZED 0.5 mg IV 30-60 G PO OR 60 G AS ENEMA Emergency Treatment of Hyperkalemia medication Mechanism effect Calcium Gluconate Antagonism of Membrane effect ACTION Onset 1-2 Min Peak 5 Min Insulin and glucose Increased K+ entry Into the cells 5-10 Min 30-60 Min Sodium Bicarbonate Increased K+ entry Into the cells 15-30 Min 30-60 Min Albuterol Increased K+ entry into the cells Kayexalate Removal of excess K+ from the body Hemodialysis Removal of excess K+ from the body 30 Min 30-60 Min 60 Min 2-4 hours Removes 25-30 meq hourly Continous, most Efficient 1st hour A 22 YEAR OLD COMPLAINS OF FATIGABILITY AND WEAKNESS. PHYSICAL EXAM: BP 122/68 HR 72/MIN NO ORTHOSTATIC CHANGES NO EDEMA LABS: WHAT TEST(S) 135 85 2.1 UNa=80 UK=70 45 WILL HELP YOU MAKE THE DIAGNOSIS? WHY IS HIS POTASSIUM LOW? !!!!! INTAKE/SHIFT/OUTPUT !!!!! METABOLIC ALKALOSIS AND HYPOKALEMIA 1. VOMITING 2. DIURETIC USE 3. BARTTER’S/GITELMAN’S THE LACK OF HYPERTENSION RULES OUT MINERALOCORTICOID OR MINERALOCORTICOID-LIKE EXCESS HORMONES LABS: 135 85 2.1 45 UNa=80 UK=70 URINE CHLORIDE = 6 DIAGNOSIS IS VOMITING WITH URINARY K LOSSES FROM THE OSMOTIC DIURESIS AND SECONDARY HYPERALDOSTERONISM URINE CHLORIDE = 60 DIAGNOSIS IS RECENT USE OF DIURETICS OR BARTTER’S SYNDROME (or GITELMAN’S SYNDROME) FACTORS THAT INCREASE URINARY POTASSIUM LOSSES 1. 2. 3. 4. 5. HIGH URINE FLOW RATES INCREASED Na DELIVERY TO DISTAL TUBULE INCREASED MINERALOCORTICOID ACTIVITY ALKALOSIS POORLY REABSORBED LUMINAL ANION VIRTUALLY ALL K EXCRETION OCCURS IN THE CCD MAJOR SITE OF K+ SECRETION 480 mmol 720 mmol 60-90 mmol 3000 mmol 60 mmol HYPOKALEMIA HAS DRAMATIC EFFECTS ON MUSCLE ACTION TREATMENT OF HYPOKALEMIA The safest route of replacement is PO. KCl is the preparation of choice for K w/ ECF volume contraction, diuretic use metabolic alkalosis. Potassium bicarbonate (or citrate) for K w/ RTA diarrhea associated K losses. K phosphate for K w/ anabolism (TPN) phosphate depletion (recovering DKA). TREATMENT OF HYPOKALEMIA The goal of emergency therapy should be to get the patient out of danger rapidly but replacing the entire potassium deficit quickly is not desirable. During chronic hypokalemia, renal mechanisms develop to minimize aldosterone-induced K losses. These may persist for 1 to 2 days after correction. Aggressive, rapid replacement of potassium may lead to hyperkalemia EVER HEAR THE SAYING ABOUT TOO MUCH OF A GOOD THING? TREATMENT OF HYPOKALEMIA Peripheral IV potassium infusions should be less than 60mEq/L to avoid vascular spasm or sclerosis. Rates should be less than 20mEq/hr unless done in a monitored setting. 20mEq of KCl in 1 liter of D5W can lead to a further drop in serum potassium. Concentrated potassium solutions through a central line can lead to dangerous cardiac sequelae. A 54 YEAR OLD MAN WITH NO PRIOR MEDICAL HISTORY COMPLAINS OF CHRONIC FATIGUE. EXAM: BP 100/60 WITHOUT ORTHOSTATIC CHANGE. NO EDEMA LABS: 137 106 6.8 20 28 90 1.0 UNa=50 UK=48 Uosm=450 !!!!! INTAKE/SHIFT/OUTPUT !!!!! TESTS USED TO MONITOR K EXCRETION TEST TTKG STRENGTHS PHYSIOLOGIC BASIS TRANSLATES URINE TO CCD SEPARATES + K FROM URINE FLOW RATE WEAKNESSES EXPECTED EXPECTED VALUE K VALUE K MANY UNVERIFIED ASSUMPTIONS <2 >10 TTKG: TRANSTUBULAR POTASSIUM GRADIENT ASSUME A TTKG OF 3.3 10 mmol/L 3 mmol/L K+ CORTEX CCD 300 mOsm/L 1 LITER LEAVES CCD MEDULLA MCD 1 L=10mmol/L URINE UOSM=300 0L 10 mmol/L OSM=300 OSM 0.75 L 0.25 L=40mmol/L UOSM=1200 TTKG TTKG= [ K+ ]urine /(urine/plasma)osm / [ K+ ]plasma ASSUMPTIONS: 1. OSMOLALITY IS KNOWN IN CCD. TTKG CANNOT BE USED IF UOSM< POSM 2. WATER REABSORPTION IN MCD CAN BE ESTIMATED, BUT IF ANP IS COMPLETELY SHUT OFF THERE IS Na REABSORPTION IN THE MCD AND TTKG IS AN OVERESTIMATE. 3. K+ IS NOT REABSORBED OR SECRETED IN MCD. THIS IS TRUE UNLESS PROFOUND K DEPLETION OR TAKING “INDUSTRIAL” DOSES OF K 4. THE K IN PLASMA REFLECTS THE PERITUBULAR K A 54 YEAR OLD MAN WITH NO PRIOR MEDICAL HISTORY COMPLAINS OF CHRONIC FATIGUE. EXAM: BP 100/60 WITHOUT ORTHOSTATIC CHANGE. NO EDEMA LABS: 137 106 6.8 20 28 90 1.0 UNa=50 UK=48 Uosm=450 137 106 6.8 20 28 90 1.0 UNa=50 UK=48 Uosm=450 TTKG={48 (450 289)} 6.8= 4.5 HYPERKALEMIA STIMULATES ALDOSTERONE RELEASE. IN HYPERKALEMIA THE TTKG SHOULD BE 10 OR ABOVE. THIS FELLOW LACKS SUFFICIENT MINERALOCORTICOID ACTIVITY. ADDISON’S DISEASE A LACK OF ALDOSTERONE LEADS TO: INCREASED URINARY SODIUM LOSSES HYPERKALEMIA METABOLIC ACIDOSIS