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Contents
Practical Therapeutics
Drugs 39 (6): 841-855, 19900012-6667/90/0006-0841/$07.50/0© ADlS Press LimitedAll rights reserved.DRUG03353
Rational Treatment of Acid-Base Disorders
Margaret L. McLaughlin and Jerome P. Kassirer
Nephrology Di vision, Department of Medicine , New England Medical Center,and Department of Med icine, Tufts Un iversity School of Medi cine , Boston ,Massachusetts, USA
Summary , ,.., , ,.., ,.., ,..,.. 842I. Metabolic Acidosis 843
1.1 Clinical Manifestations 8431.2 Causes of Metabolic Acidosis 843
1.3 Treatment of Metabolic Acidosis 8441.3.1 General Remarks 844
1.3.2 Loss of Alkaline Gastrointestinal Fluids 8451.3.3 Carbonic Anhydrase Inhibitors 845
1.3.4 Urinary Diversion , 8451.3.5 Lactic Acidosis 8451.3.6 Diabetic Ketoacidosis 8461.3.7 Alcoholic Ketoacidosis 8461.3.8 Renal Tubul ar Acidosis ll471.3.9 Renal Acidosis (Uraem ic Acidosis) 848
2. Metabolic Alkalosis , 8482.1 Clinical Manifestations 848
2.2 Causes of Metabolic Alkalosis 8482.3 Treatment of Metabolic Alkalosis 849
2.3.1 Milk-Alkali Syndrome 8502.3.2 Combined Therapy with Nonabsorbabl e Alkali and Exchange Resins 8502.3.3 Acute Alkali Loading 8502.3.4 Gastric Fluid Losses 850
2.3.5 Diuretic Therapy , 8512.3.6 Posthypercapnic Alkalosis 8512.3.7 Primary Aldosteron ism 8512.3.8 Bartt er's Syndrom e 85I2.3.9 Cushing's Syndrome 852
3. Respiratory Acidosis 852
3.1 Clinical Manifestations 8523.2 Causes of Respiratory Acidosis , 852
3.3 Treatment of Respiratory Acidosis , 8524. Respiratory Alkalosis 852
842
Summary
Drugs 39 (6) 1990
4.1 Clinical Manifestations 8534.2 Causes of Respiratory Alkalosis 8534.3 Treatment of Respiratory Alkalosis 853
5. Mixed Acid-Base Disturbances 8535.1 Metabolic and Respiratory Acidosis 8535.2 Metabolic and Respiratory Alkalosis 8535.3 Metabolic Acidosis and Respiratory Alkalosis 8545.4 Metabolic Alkalosis and Respiratory Acidosis 854
6. Conclusions 854
Acid-base derangements are encountered frequently in clinical practice and many havelife-threatening implications. Treatment is dependent on correctly identifying the acidbase disorder and , whenever possible, repairing the underlying causal process. Bicarbonate is the agent of choice for the treatment of acute metabolic acidosis. Controversysurrounds the use of alkali therapy in lactic acidosis and diabetic ketoacidosis, but bicarbonate should clearly be administered for severe acidos is. In most patients with mildto moderate chloride-responsive metabolic alkalosis, providing an adequate amount ofa chloride salt will restore acid-base balance to normal over a matter of days. In contrast,therapy of the chloride-resistant metabolic alkaloses is best directed at the underlyingdisease . When alkalaemia is severe , administering hydrochloric acid or a hydrochloricacid precursor may be necessary .
Treatment of respiratory acidosis should be targeted at restoring ventilation ; alkalishould be administered only for superimposed metabolic acidosis . The therapy of respiratory alkalosis is centred on reversal of the root cause ; short of this goal, there is noeffective treatment of primary hypocapnia.
The coexistence of more than one acid-base disorder (i.e. a mixed disorder) is notuncommon. When plasma bicarbonate concentration and arterial carbon dioxide tension(paCOl) are altered in opposite directions, extreme shifts in pH may occur. In such cases,it is imperative that the nature of the disturbance is identified early and therapy directedat both disorders.
Disturbances of acid-base balance are widespread in practice and many pose serious threatsto the well-being of patients. A rational approachto the treatment of acid-base disorders is dependent on an understanding of the basic pathophysiological mechanisms that give rise to them. Correct identification of the underlying disturbancemay suggest new diagnostic avenues, as well asprovide a guide to specific, and often life-saving,therapy.
The carbonic acid-bicarbonate buffer systemplays a central role in acid-base balance because ofits prevalence and its relation to physiological regulatory mechanisms. The hydration of dissolvedC02 forms carbonic acid which then dissociates toyield bicarbonate and hydrogen ions. These chem-
ical reactions rapidly achieve equilibrium conditions, allowing a simple expression of their relationship (Henderson 1908):
(Eq. I)
Thus, hydrogen ion concentration is a functionof the ratio of the arterial carbon dioxide tension(paC02) to the bicarbonate concentration. It follows that changes in hydrogen ion concentrationand, consequently, all acid-base disorders, resultfrom changes in one or other of these 2 variables.
Acid-base disturbances are classified into 4 primary disorders - metabolic acidosis, metabolic alkalosis, respiratory acidosis and respiratory alkalosis - and various combinations of these disorderscategorised as mixed disturbances.
Treatment of Acid-Base Disorders
1. Metabolic Acidosis
Metabolic acidosis is initiated by a reduction inplasma bicarbonate concentration. The most immediate consequence of a fall in bicarbonate concentration is an increase in plasma acidity. Corresponding changes in cerebral hydrogen ionconcentration are sensed by central chemoreceptors, giving rise to reflex hyperventilation, a fall inpaC02, and a consequent attenuation in the degreeof acidification.
1.1 Clinical Manifestations
The clinical manifestations of metabolic acidosis include effects on the cardiovascular and pulmonary systems, the circulation, oxygen transport,and potassium metabolism (Mitchell et al. 1972;Relman 1972). Hyperventilation, or Kussmaul respirations, is one of the most readily apparentmanifestations of severe acidosis. Myocardial dysfunction due to acidosis and a reduced thresholdfor ventricular fibrillation also occur. Acidosis hasseveral effects on vascular tone, producing directarterial vasodilatation, indirect sympathetic-mediated vasoconstriction, and direct venous vasoconstriction. In addition , acute acidaemia shifts thehaemoglobin dissociation curve to the right, butacidosis-induced depletion in cellular 2,3-diphosphoglycerate shifts the curve back in a matter ofhours (Mitchell et al. 1972). Hyperkalaemia is afrequent accompaniment of acute metabolic acidosis and has been attributed to transcellular shiftsofpotassium in response to acidosis. However, certain types of metabolic acidosis due to organic acids(e.g, lactic acid and acetoacetic acid) have little orno direct effect on serum potassium concentration(Fulop 1979). When hyperkalaemia does occur inthese kinds of acidosis, decreased renal function orinsulin deficiency is probably more important inits genesis.
1.2 Causes of Metabolic Acidosis
Three distinct pathological processes work aloneor in concert to produce metabolic acidosis: (a) lossof bicarbonate; (b) addition of acid; and (c) re-
843
duced capacity of the kidneys to excrete acid (seetable I).
Loss of bicarbonate-rich fluid results in depletion of extracellular fluid volume and a reductionin bicarbonate concentration. At the same time,chloride concentration rises as the remainingchloride is confined to a smaller volume of distribution. Such a hyperchloraemic metabolic acidosisresults from diarrhoea (Darrow et al. 1949), pancreatic or biliary drainage, administration of carbonic anhydrase inhibitors, and certain forms ofurinary diversion . Administration of hydrochloricacid and substances which give rise to hydrochloricacid when metabolised (e.g. ammonium chloride,
Table I. Causes of metabolic acidosis (from Kassirer et al. 1989.with permission)
Normal anion gapLoss of bicarbonate
DiarrhoeaSmall bowel lossesCarbonic anhydrase inhibitorsUreterosigmoidostomyIleal loop bladderDilutional acidosis
Addition of hydrochloric acidAmmonium chlorideArginine-HCILysine-HCITotal parenteral nutrition
Disproportionate failure of renal tubular functionRenal tubular acidosisMild renal failureHyporeninaemic hypoaldosteronismAdrenal insufficiency
Increased anion gapOverproduction of organic acids
Lactic acidosisDiabetic ketoacidosisStarvation ketosisAlcoholic ketoacidosisMethyl alcohol ingestionEthylene glycol ingestionParaldehyde ingestionSalicylate intoxicationInfantile organic acidosis
Severe renal failure
AcuteChronic
844
lysine-HC1, and arginine-HCl) also produce hyperchloraemic acidosis. The normal kidney responds to the reduction in plasma bicarbonate byaugmenting net acid excretion, resulting in the conservation of sodium with newly generated bicarbonate and in the excretion of chloride and hydrogen ion.
Overproduction of organic acids results in a fallin plasma bicarbonate concentration and an increase in the plasma concentration of the anion ofthat acid. In contrast to the pattern seen with directloss of bicarbonate or administration of substancesthat yield hydrochloric acid, the acidosis that results from organic acid overproduction is characterised by a normal plasma chloride concentrationand an increase in the concentration of plasma unmeasured anions. The causes of metabolic acidosiswith an increased anion gap include: lactic acidosis; diabetic ketoacidosis; starvation ketosis; alcoholic ketoacidosis ; methyl alcohol, ethylene glycol and paraldehyde intoxication; and salicylateoverdose (Gabow 1985). Some degree of sodiumand potassium depletion often accompanies thistype of metabolic acidosis because these cations areexcreted in the urine with the acid anions .
The third type of metabolic acidosis results froma failure of the kidney to excrete the daily acid load.A hyperchloraemic metabolic acidosis developswith distal renal tubular acidosis and with mildchronic renal insufficiency (Harrington & Cohen1982), but when glomerular function is severelyimpaired, anions (such as phosphate and sulphate)are retained by the kidney and the plasma unmeasured anion concentration increases as well.
1.3 Treatment of Metabolic Acidosis
1.3.1 General RemarksWhenever possible, efforts should be directed at
identifying and treating the underlying processwhich gave rise to the metabolic acidosis. No matter what the cause, it is recommended that alkalibe administered for severe metabolic acidosis (i.e.plasma bicarbonate < 5 mmol/L). Patients withplasma bicarbonate values in this range are at riskof a sudden worsening in acidaemia with only a
Drugs 39 (6) 1990
small additional decrement in bicarbonate concentration or increase in paC02. In normal individuals, administered bicarbonate distributes througha space of approximately 40 to 50%of bodyweight,but the space of distribution may be more thantwice that large when plasma bicarbonate is extremely low (Garella et al. 1973). In addition , thereis often no way to assess the magnitude of organicacid production or on-going alkali loss. Consequently, estimates of bicarbonate space to predicta desired increment in plasma bicarbonate must beconsidered a first approximation only. Given thelarge number of variables, acid-base parametersshould be assessed frequently and appropriate adjustments made in the quantity of alkali administered.
Sodium bicarbonate is the agent of choice forthe treatment of acute metabolic acidosis. Sodiumlactate, citrate and acetate require metabolic conversion to bicarbonate to exert their alkalinisingeffect, and hence their therapeutic effect may bedelayed. For long term use, as in the treatment ofrenal tubular acidosis, chronic diarrhoea , or endstage renal disease, some patients find sodium citrate more palatable than bicarbonate salts.
In the acute setting, sodium bicarbonate shouldbe administered intravenously, either as a bolus oradded to a hyponatric solution and given continuously. An ampoule of sodium bicarbonate contains 50 mEq of sodium and bicarbonate . A readilyaccessible oral form of alkali therapy is sodium bicarbonate tablets; a 650mg tablet contains 8 mEqof bicarbonate . Sodium citrate is available in a liquid form; Iml contains I mEcj of sodium and theequivalent of I mEq of bicarbonate .
Hypernatraemia and volume overload are themajor complications of administering large quantities of sodium bicarbonate. Metabolic alkalosismay result after treatment of organic acidosis (e.g.diabetic ketoacidosis, lactic acidosis) if bicarbonateis generated from the metabolism of retained organic anions, and post-treatment respiratory alkalosis can occur in any form of metabolic acidosisif hyperventilation persists as a consequence oflagging spinal fluid acidification. Transient hypoka-
Treatment of Acid-Base Disorders
laemia, resulting from the shift of potassium intocells, also may develop during the course of therapy.
/.3.2 Loss ofAlkaline Gastrointestinal FluidsMetabolic acidosis caused by loss of gastroin
testinal fluid is often accompanied by large deficitsof sodium, potassium, chloride and water, in addition to bicarbonate. The severity of the acidosiscaused by stool loss varies with the aetiology of thediarrhoea. Stool bicarbonate concentrations in excess of 40 mrnol/L occur in patients with massivewatery diarrhoea (Watten et al. 1959) and villousadenomas of the rectum, and such losses can resultin moderate to severe metabolic acidosis. The bicarbonate concentration in pancreatic and biliarydrainage always exceeds that in plasma, but severemetabolic acidosis rarely results unless drainagevolumes are unusually large.
In severe diarrhoea, volume repletion is an important target of initial therapy . Ideally, replacement therapy is guided by measurements of theelectrolyte composition of the diarrhoeal fluid. Because such measurements are not very practical,however, a 0.45% saline solution containing 50mfiq/L of sodium bicarbonate is a reasonable initial replacement fluid. Potassium losses are typically large and should also be replaced. Acid-baseparameters and serum potassium should be assessed frequently and therapy modified accordingly.
1.3.3 Carbonic Anhydrase InhibitorsCarbonic anhydrase inhibitors such as aceta
zolamide are only moderately potent in producingrenal bicarbonate loss; thus, plasma bicarbonateconcentrations rarely fall below 18 mrnol/L as aresult of their use (Harrington & Cohen 1982).Aside from discontinuing these agents, no othertherapy is usually necessary.
/.3.4 Urinary DiversionHyperchloraemic metabolic acidosis is seen less
frequently today with ureteroileostomies than whenureterosigmoidostomies were the preferred approach to urinary diversion. Chloride-bicarbonateexchange, reabsorption of urinary ammonium, and
845
renal tubular damage due to obstruction and infection are the mechanisms which produce metabolic acidosis. In contrast to ureterosigmoidostomy, an ileal conduit permits continuous urinarydrainage to the outside, obviating prolonged contact with intestinal mucosa and reducing the opportunity for exchange. Hyperchloraemic metabolic acidosis, particularly if new in onset, shoulddirect attention toward the possibility that an ilealloop has become partially obstructed. Few patientswith ileal diversions need daily alkali therapy.
1.3.5 Lactic AcidosisThe therapy of lactic acidosis is controversial,
but all agree that effective treatment centres on theidentification and correction of the underlying process. Prompt treatment of low-cardiac-output states,repletion of volume deficits, correction of shockand administration of antibiotics (in the septicpatient) should be given the highest priority. Theuse of vasoconstrictive substances should be minimised to avoid aggravation of ischaemia of peripheral tissues. Invasive haemodynamic monitoring in an intensive care unit should be employedto guide the use of volume replacement, cardiotrophic agents and pressors (Madias 1986).
Controversy surrounds the use of alkali therapyin the treatment of lactic acidosis. Experimentalstudies in dogs suggest that administering sodiumbicarbonate may augment the accumulation of lactic acid by stimulating its production or interferingwith its metabolism by the liver (Graf et al. 1985).In addition, the evidence in humans of an adverseeffect of alkali therapy in lactic acidosis is not convincing. We recommend that sodium bicarbonatebe administered for severe, life-threatening lacticacidosis, that is, when the pH falls below 7.20(which usually corresponds to a plasma bicarbonate below 10 mrnol/L). Certainly, at a pH belowthis value, the negative inotropic and arrhythmogenic effects of acidaemia are substantial, and alkali therapy gains time to address the principal disorder. No specific guidelines can be given regardingthe amount of alkali to be administered becausethe rate of lactic acid production varies tremendously. As a general rule, however, it is desirable
846
to give sufficient alkali to maintain plasma bicarbonate concentration at 15 to 18 mmol/L, Acid-baseparameters should be assessed frequently andtherapy modified accordingly.
Adjunctive or alternative therapy to sodium bicarbonate in the treatment of lactic acidosis withdichloroacetate also has been proposed. Whiledichloroacetate augments the oxidation of lactateto acetyl-CoA, and evidence from human studiesis promising (Stacpoole et al. 1983), toxicity maybe a major drawback to its use.
1.3.6 Diabet ic KetoacidosisThe mainstay of therapy of diabetic ketoacid
osis is insulin, but repletion of fluid and electrolytedeficits and appropriate use of alkali are of equalimportance (Sanson & Levine 1989). In recentyears, the effectiveness of physiological doses of insulin has been well established. Several insulin dosage schedules have been shown to be effective.Typically, a small loading dose of regular insulin(2 to 12 units) is administered intravenously, or adose of 20 units is given intramuscularly followedby a continuous infusion (2 to 12 units/hour). Theamount of insulin administered hourly is adjustedto achieve a decrement in glucose concentration ofapproximately 100 mg/dl/h (5.6 mrnol/L) [Kassirer et al. 1989]. In the initial stages of treatment,blood glucose levels and electrolytes should bemeasured hourly. Insulin therapy should be continued until hyperglycaemia and ketonaemia haveresolved . To avoid hypoglycaemia, glucose shouldbe added to the replacement fluids when the bloodsugar level falls below 300 mg/dl (16.7 rnrnol/L).Given the short half-life of intravenous insulin, approximately one-half to two-thirds of the usual dailyinsulin dose should be given subcutaneously asintermediate-acting insulin one hour before discontinuing the insulin infusion .
As with lactic acidosis , the use of endogenousalkali in the treatment of diabetic ketoacidosis isthe subject of debate . Post-treatment alkalaemia,worsening hypokalaemia due to an alkali-inducedtranscellular shift of potassium, and persistent hyperventilation because of lagging equilibration ofarterial blood with the spinal fluid, have been cited
Drugs 39 (6) 1990
as the major objections to the use of sodium bicarbonate. One recent randomised, prospectivestudy in patients with severe diabeti c ketoacidosis(arterial pH 6.9 to 7.14) found no significant difference in the rate of decline of plasma glucose orketone levels or in the rate of increase in pH orplasma bicarbonate levels in patients who receivedbicarbonate or in those who did not (Morris et al.1986). It is difficult to draw conclusions from thisstudy because the number of subjects was smalland the patients selected were free of complicatingillnesses. When acidosis is severe (plasma bicarbonate concentration less than 5 mmol/L), a smalladditional loss of bicarbonate, or an increase in endogenous acid production from superimposed sepsis and lactic acidosis , might easily result in lifethreatening acidosis. Likewise, any faltering inventilation because of fatigue, pneumonia or otherdisorders could cause paC02 to rise (or to fail todecrease) and the blood pH could fall below 7.00.Consequently, in patients with plasma bicarbonateconcentration less than 5 mmol/L, and particularlyin those with complicating illnesses, we believe thatthe benefits of administering enough alkali to raiseplasma bicarbonate by 3 to 4 mmol/L outweigh therisks.
1.3.7 Alcoholic KetoacidosisThis disorder is typically diagnosed in chronic
alcoholics following a prolonged drinking bout.Profound acidosis is the rule, with plasma bicarbonate concentrations frequently less than 10 mmol/L (Miller et al. 1978). Accumulation of 3-hydroxybutyric acid is mainly responsible for the acidosis.However, despite the severe acidaemia, alcoholicketoacidosis corrects with relative ease, and alkalitherapy or insulin administration is rarely necessary. Infusion of glucose and saline frequently results in rapid correction of the acidosis in a matterof hours .
IntoxicationsMethyl Alcohol: Ingestion of methyl alcohol may
result in serious consequences even when treatment is promptly initiated (Jacobsen & McMartin1986). The major manifestations are diminution in
Treatment of Acid-Base Disorders
vision accompanied by peripapillary oedema andhyperaemia of the optic discs, severe metabolicacidosis (with an increased anion gap), and abdominal pain probably due to pancreatitis (Bennett etal. 1953). Methyl alcohol is metabolised by the enzyme alcohol dehydrogenase to produce formaldehyde and formic acid, the latter being the primary toxin .
Dialysis is the mainstay of the treatment ofmethyl alcohol intoxication. Haemodialysis effectively removes both the parent compound and itsmetabolites and also rapidly corrects the metabolicacidosis. Peritoneal dialysis is less efficient but canbe used if haemodialysis is not feasible. The affinity of alcohol dehydrogenase for ethyl alcoholgreatly exceeds that for methyl alcohol, and for thisreason administration of ethyl alcohol is commonly employed to interfere with the metabolismof methyl alcohol to its toxic metabolites. Ethyl alcohol can be given either orally or intravenously.Usually a loading dose of 0.6 g/kg followed by aninfusion of 100 mg/kg/h is adequate to achieve thedesired blood ethyl alcohol level of 100 mg/dl (22rnmol/L). During haemodialysis the infusion ratemust be increased or ethyl alcohol added to thedialysate at a concentration of 100 mg/dl (Garella1988). Blood levels of ethyl alcohol must be monitored carefully because its half-life varies considerably from individual to individual. Treatmentshould cont inue until acidosis is corrected andserum methyl alcohol and formate levels are undetectable.
Ethylene Glycol.' Like methyl alcohol, ingestionof ethylene glycol can result in profound metabolicacidosis (Jacobsen & McMartin 1986). Cardiopulmonary failure, coma and acute renal failure mayevolve over a period of hours to days. As withmethyl alcohol, administration of ethyl alcoholblocks the metabolism of the parent compound toits toxic metabolite, glycolic acid, by virtue of itsgreater affinity for alcohol dehydrogenase . Alkalitherapy , haemodialysis and ethyl alcohol administration (see Methyl Alcohol) constitute appropriate therapy. A pharmacological inhibitor of alcoholdehydrogenase, 4-methylpyrazole, may prove to bea safe and easier alternative to ethyl alcohol infu-
847
sion, but clinical experience with this agent is limited (Baud et al. 1988).
Salicylate: Salicylates affect acid-base equilibrium by directly stimulating alveolar ventilationand by increasing both carbon dioxide and endogenous acid production. Consequently, mixed acidbase disturbances frequently result from salicylateoverdose . Metabolic acidosis may be the presenting feature of salicylate intoxication in children, butit is less common in adults . In addition, the presentation will vary depending on whether the ingestion is acute or chronic (Greer et al. 1965).
Because of the likelihood of a mixed acid-basepicture , it is essential that arterial blood gases beused to guide therapy. If metabolic acidosis predominates, sodium bicarbonate should be administered. In addition, treatment with sodium bicarbonate alkalinises the urine and augments therenal excretion of salicylate by inhibiting its reabsorption. Of course, giving alkali in the presenceof respiratory alkalosis may produce marked alkalaemia, but alkali can be administered safely ifacid-base parameters are monitored carefully. Closeattention should be paid to the patient's volumestatus because alkali therapy and its attendant sodium load can aggravate the noncardiogenic pulmonary oedema frequently seen in adults with salicylate intoxication (Tweeddale 1974). Serumpotassium concentration must be carefully followed because alkali therapy can aggravate hypokalaemia.
In an otherwise healthy patient, administrationof intravenous fluids including alkali will enhancerenal excretion of salicylate and reduce blood salicylate to the safe range in a matter of hours. Whenthe intoxication is unusually severe, or when renalfailure or cardiac disease complicate the picture ,dialysis or haemoperfusion may be necessary. Ofthese options, haemodialysis is preferred becauseit promptly corrects the metabolic acidosis as wellas removing salicylate from the blood.
1.3.8 Renal Tubular Acidosis (RTA)Patients with distal RTA (type I, gradient-lim
ited) almost always require long term alkali therapyto prevent severe acidosis, decrease renal potas-
848
sium losses, and prevent bone disease. The maintenance dose of alkali required varies considerably,primarily because the degree of bicarbonate wasting that may accompany the distal defect is alsohighly variable. In the absence of appreciable bicarbonate wasting, approximately I mliq/kg/day ofalkali should suffice. In practice, however, mostadults and older children require 2 to 3 mfiq/kg,'day of supplemental alkali because of some bicarbonate wasting (Kassirer et al. 1989).
Occasionally these patients may present withprofound metabolic acidosis and severe hypokalaemia. The deficits of bicarbonate and potassiummay be several hundred milli-equivalents each.Rapid simultaneous administration of sodium bicarbonate and potassium chloride is required insuch individuals.
In contrast, patients with proximal RTA (typeII, bicarbonate-wasting) rarely develop severe acidosis yet they may need to ingest alkali in the rangeof 5 to 15 mliq/kg/day to achieve normal plasmabicarbonate concentrations because of huge renalbicarbonate losses (Kassirer et al. 1989). While alkali therapy tends to ameliorate the hypokalaemiain distal RTA, the increased delivery of bicarbonate to the distal nephron promotes potassiumsecretion in proximal RTA.
1.3.9 Renal Acidosis (Uraemic Acidosis)Some degree of acidosis is usually present in
patients with chronic renal insufficiency when theglomerular filtration rate is reduced to 25 ml/minor less (Harrington et al. 1982), but the degree ofacidosis is not usually severe enough to warranttreatment. However, when plasma bicarbonate fallsbelow 15 mmol/L, alkali should be provided in adose of I to 2 mliq/kg/day. Patients with severerenal insufficiency should be monitored carefullyfor signs of volume overload because of the accompanying increase in sodium intake .
2. Metabolic Alkalosis
Metabolic alkalosis is initiated by an increase inplasma bicarbonate. This alkalinisation gives riseto a compensatory decrease in alveolar ventilation,
Drugs 39 (6) 1990
and the resulting hypercapnia attenuates the increase in systemic pH.
2.1 Clinical Manifestations
Even in the absence of underlying lung disease,secondary hypoventilation is accompanied by somedegree of hypoxia. With plasma bicarbonate concentrations greater than 60 mrnol/L, values forpa02 as low as 45 to 50mm Hg may occur inpatients even with normal pulmonary function(Tuller & Meddi 1971). In patients with pre-existing pulmonary disease, the hypoxia may be evenmore severe. Two other prominent manifestationsof alkalaemia are hypokalaemia and central nervous system dysfunction. The hypokalaemia that isfrequently associated with metabolic alkalosis ismultifactorial. While substantial potassium lossesoften accompany the processes that generate alkalosis (e.g. diuretic administration, gastric fluidlosses), transcellular shifts of potassium and renalpotassium wasting also play an important part inthe genesis of hypokalaem ia.
The common central nervous system manifestations of alkalaemia include lethargy and confusion. In severe alkalaemia muscle twitching andgeneralised seizures can occur. Whether alkalaemiaper se is responsible for these derangements orwhether they can be ascribed to the hypoxia andvolume depletion that often accompanies themetabolic alkalosis remains speculative.
2.2 Causes of Metabolic Alkalosis
The causes of metabolic alkalosis can be divided into 4 groups (table II). The first group consists of alkaloses secondary to alkali administration. Administration of exogenous alkali at ratesgreater than endogenous acid production will increase plasma bicarbonate concentration, but whenthe alkali is discontinued prompt excretion of analkaline urine restores plasma bicarbonate to normal. Examples of metabolic alkalosis that fall intothis category are the milk-alkali syndrome and acutesodium bicarbonate or sodium acetate loading.
The second group consists of chloride-respon-
Treatment of Acid-Base Disorders
Table II. Causes of metabolic alkalosis (from Kassirer et al. 1989,with permission)
Alkalosis secondary to alkali administrationContinuous alkali administration
Milk-alkali syndromeIngestion of large quantities of sodium bicarbonateIngestion of soybean formula dietCombined therapy with nonabsorbable alkali and exchangeresinsRecovery from organic acidosis
Acute alkali loadingChloride-responsive alkalosisGastric fluid lossesDiuretic therapyPosthypercapnic stateStool losses
Congenital chloridorrhoeaVillous adenoma
Chloride-resistant alkalosisPrimary aldosteronismBartter's syndromeCushing's syndromeDisorders that simulate adrenocortical excessIdiopathicMiscellaneousSecondary aldosteronism
Malignant hypertensionRenovascular hypertensionRenin-secreting tumours
Mineralocorticoid excess (other than aldosterone)Penicillin therapyParathyroid disease and hypercalcaemiaRefeeding fof/owing fasting
sive alkaloses. In this variety , alkalosis is perpetuated by sodium avidity and disproportionatechloride depletion. Common examples are the alkalosis due to diuretic therapy and gastric fluidlosses. Typically, little or no sodium chloride is excreted in the urine because losses of sodium chloride and water during the development of the alkalosis have induced mild to moderate volumedepletion. This type of metabolic alkalosis is corrected promptly by either sodium or potassiumchloride administration.
In contrast, in the third group, chloride-resistant alkaloses, alkalosis is maintained in the absence of volume contraction and in the face ofabundant dietary (and urinary) chloride . The alkalosis accompanying Bartter's syndrome, Cush-
849
ing's syndrome, and primary aldosteronism fall intothis category. Urinary chloride excretion is oftenhigh and the alkalosis persists despite chlorideadministration.
The disorders that fall into the last category(idiopathic alkalosis) are not well defined, althoughat least some have been attributed to extreme potassium depletion.
2.3 Treatment of Metabolic Alkalosis
The treatment of metabolic alkalosis also centreson the prompt identification and removal of theunderlying process that caused the alkalosis. If thecause is not obvious or if surreptitious vomiting orself-administration of diuretics are being entertained as aetiologies, measurement of urinarychloride and pH may be useful. A low urine chloride (less than 10 to 20 mmol/L) points toward achloride-responsive alkalosis, whereas a highervalue suggests the recent administration of a diuretic, or less commonly, a chloride-resistant formof metabolic alkalosis. The presence of a persistently alkaline urine should raise the possibility ofexcessive alkali intake, as in the milk-alkali syndrome.
In most cases of mild to moderate chloride-responsive metabolic alkalosis, when adequate chloride is provided the kidney excretes the surplus alkali and restores acid-base balance to normal overa matter of days. The alkalosis associated with thechloride-resistant disorders is not generally severeand therapy should be directed at the primary defect. When severe alkalaemia is present (plasma bicarbonate greater than 40 mmol/L), the administration of hydrochloric acid or a hydrochloric acidprecursor may be required . In the same fashion asestimating the quantity of alkali to administer toseverely acidotic patients, the quantity of acid required in mEq can be calculated by assuming thatthe volume of distribution of bicarbonate is roughlyequivalent to 50% of bodyweight and by multiplying this figure by the desired decrement in bicarbonate concentration.
Hydrochloric acid, ammonium chloride and arginine monohydrochloride infusions are useful for
850
the treatment of severe metabolic alkalosis. Hydrochloric acid solutions must be administeredthrough a central line to avoid severe corrosive reactions. One litre of 0.1N HC! contains 100 mEqof hydrogen ions; the rate of administration of thissolut ion should not exceed 300 to 500 ml/h (Kassirer et al. 1989). Alternatively, a 2.14% solutionof ammonium chloride containing approximately400 mEq of hydrogen ion/L can be made from a26.75% stock solution. Ammonium chloride shouldnot be administered at rates greater than 300 to400 ml/h, Hepatic conversion of ammoniumchloride yields urea and hydrochloric acid. Themajor contraindication to administering a solutioncontaining ammonia is liver disease. The third option for acidification is the use of arginine monohydrochloride. 300ml of a 10% solution containsapproximately 150 mEq of hydrogen ions; thisamount can be given over I hour, if necessary(Kassirer et al. 1989). Dangerous hyperkalaemia canoccur during the course ofarginine administration,presumably from displacement of intracellular potassium by the arginine cation (Bushinsky & Gennari 1978). This effect seems to be more commonin patients with abnormal renal function . Serumpotassium should always be monitored carefullyduring and after an arginine monochloride infusion.
2.3.1 Milk-Alkali SyndromeIn its classic form, the milk-alkali syndrome de
velops in patients who ingest large quantities ofmilk and absorbable alkali, but it occurs in patientswho have ingested only calcium carbonate. Thesyndrome is characterised by the triad of metabolicalkalosis, hypercalcaemia and renal insufficiency.In most cases, therapy consists of eliminating thealkali load. When the milk-alkali syndrome occursin the setting of vomiting or gastric suction, adequate chloride must also be provided.
2.3.2 Combined Therapy with NonabsorbableAlkali and Exchange ResinsWhen nonabsorbable alkali (e.g. magnesium hy
droxide, aluminium hydroxide) and cation-exchange resins are administered simultaneously to
Drugs 39 (6) 1990
patients with severe renal insufficiency, metabolicalkalosis may result (Schroeder 1969). As the resinabsorbs the ingested cation, intestinal bicarbonateis made available for absorption. Discontinuingeither one or both of these agents results in dissipation of the alkalosis, but because of the underlying renal impairment it may take several days forplasma bicarbonate concentration to return to control levels.
2.3.3 Acute Alkali LoadingRapid administration of sodium bicarbonate or
sodium acetate results in metabolic alkalosis whenthe rate of infusion exceeds the capacity of the kidney to excrete the excess alkali. In addition to animmediate increase in plasma bicarbonate concentration, plasma carbon dioxide tension will increase acutely because carbonic acid is generatedfrom the titration of nonbicarbonate buffers. Thiseffect is only relevant clinically when ventilationis controlled by artificial means. In such patientsarterial blood gases should be monitored during alkali infusion.
2.3.4 Gastric Fluid LossesThe primary therapy of metabol ic alkalosis in
duced by vomiting or nasogastric suctioning is toprovide an adequate supply of chloride salt andthus to curtail renal bicarbonate generation. In thisregard, urinary chloride excretion is a valuable index of whether chloride intake is sufficient. Valuesof at least 50 mliq/day generally signify adequatereplacement. When large amounts of gastric fluidare being lost, it may be useful to measure the electrolyte composition of the fluid, and estimate thehydrogen ion concentration (as the difference between the sum of the sodium and potassium concentrations and the chloride concentration). Replacement of hydrogen ion losses with hydrochloricacid or a hydrochloric acid precursor will preventmetabolic alkalosis from developing, but this approach is generally not needed unless gastric lossesare unusually large. Alternatively, histamine H2receptor antagonists, by inhibiting gastric acid secretion, may be effective in preventing the generation of metabolic alkalosis. These agents are not
Treatment of Acid-Base Disorders
effective, of course, in the correction of establishedalkalosis.
2.3.5 Diuretic TherapyDiuretic-induced metabolic alkalosis falls into
the chloride-responsive category. The agents typically responsible include furosemide (frusemide),ethacrynic acid, bumetanide and metolazone. Diuretics cause metabolic alkalosis by 3 mechanisms:(a) an increase in renal acid excretion; (b) a disproportionate loss of chloride-rich fluid; and (c) atranscellular shift of hydrogen ions. As with gastricalkalosis, administering sufficient chloride salt willprevent metabolic alkalosis from developing during diuretic therapy . In the majority of patients ,potassium chloride is the appropriate therapy, butin the presence of volume depletion sodium chloride should be provided as well. By inhibiting sodium reabsorption and hydrogen secretion, distalblocking agents (e.g. spironolactone, triamterene,amiloride), are effective in preventing diuretic-induced alkalosis. Caution should be exercised whenthese agents are administered to patients with renalinsufficiency because of the danger of severe hyperkalaemia. Acetazolamide, a carbonic anhydrase inhibitor, is effective in the treatment of metabolicalkalosis particularly when used on alternate days.Severe hypokalaemia may occur, however, if careis not taken to replete potassium stores duringadministration of the drug.
2.3.6 Posthypercapnic AlkalosisPosthypercapnic metabolic alkalosis occurs when
hypercapnia is corrected acutely with mechanicalventilation and the plasma bicarbonate concentration remains inappropriately high. Care should betaken to lower the paCOz gradually in the presenceof chronic hypercapnia, and adequate chlorideshould be provided to permit bicarbonate excretion. If severe alkalosis develops acutely, the respirator should be adjusted to allow the paCOz torise. Persistent metabolic alkalosis can reduce theventilatory drive and impede weaning. Acetazolamide may be of value in augmenting bicarbonaturia, but it should be used as an adjuvant to administering chloride salts, not as a substitute. At
851
times it may be necessary to lower plasma bicarbonate concentration with hydrochloric acid or ahydrochloric acid precursor. Reducing the plasmabicarbonate concentration to a value unsuitably lowfor the prevailing paCOz in patients with chroniclung disease may result in acidaemia, however,when the patient is removed from the ventilator.
2.3.7 Primary AldosteronismHypersecretion of aldosterone by the adrenal
cortex induces sodium retention, hypertension, andmetabolic alkalosis of the chloride-resistant type.Administration of sodium chloride to patients withthe syndrome of primary aldosteronism does notcorrect the alkalosis and aggravates hypokalaemiaby increasing urinary potassium losses. In contrast,spironolactone, an aldosterone antagonist, promptlycorrects the hypertension and hypokalaemia, andrestores acid-base balance to normal. Amiloride, anonspecific distal blocking agent with propertiessimilar to spironolactone, is also effective.
2.3.8 Bartter's SyndromeBartter's syndrome is a rare disorder character
ised by hypokalaemia, metabolic alkalosis and normal blood pressure. Histologically the juxtaglomerular apparatus of the kidney is hyperplastic andhyperreninaemic hyperaldosteronism is a characteristic finding. The exaggerated synthesis and excretion of renal prostaglandins that accompany thehyperreninaemic state are probably a secondary effect (Halushka et al. 1977).
Hypokalaemia and alkalosis in these patients canbe difficult to treat. Prostaglandin inhibitors aredramatically effective in some patients, but inothers the defects are only partially responsive andthe beneficial effect is short-lived (Verberckmoeset al. 1976). Indomethacin, at a dose of 150 to 200mg/day, is an appropriate starting regimen. Additional potassium chloride may be needed. Shouldthe response to indomethacin not be sustained, another prostaglandin inhibitor may be successful. Inpatients in whom prostaglandin inhibitors areotherwise contraindicated, potassium sparing agentsin combination with potassium chloride may improve the alkalosis and hypokalaemia. Clearly, the
852
combination of a potassium sparing diuretic and apotassium salt is potentially dangerous and shouldonly be used with careful monitoring of plasma potassium concentration.
2.3.9 Cushing 's SyndromeThe metabolic alkalosis that accompanies Cush
ing's syndrome is typically mild and occurs in onlyone-third of patients. In contrast, severe alkalosisand hypokalaemia are more common in patientswith carcinoma of the adrenal cortex and in thosewith adrenal hyperplasia associated with corticotrophin (ACTH)-producing tumours (particularlylung cancer). Administration of potassium chlorideis appropriate, but therapy is best directed at theunderlying process.
3. Respiratory Acidosis
Respiratory acidosis is initiated by an increasein carbon dioxide tension. The immediate consequence of an increase in arterial carbon dioxidetension (paC02) is an increase in plasma acidity.Acutely, titration of nonbicarbonate buffers resultsin a small increase in plasma bicarbonate concentration, but when hypercapnia is sustained, enhanced renal reabsorption of bicarbonate furtherincreases plasma bicarbonate concentration.
3.1 Clinical Manifestations
Central nervous system manifestations are themost important clinical consequences of hypercapnia. The factors correlated with cerebral dysfunction are the magnitude of the hypercapnia, the rapidity with which it develops, the severity of theacidaemia and the degree of attendant hypoxia .Acute hypercapnia induces peripheral vasodilatation, stimulates the sympathetic nervous systemand increases cardiac output. Arrhythmias frequently occur during acute and chronic hypercapnia. Whether the absolute level of hypercapnia isarrhythmogenic or whether rapid change in paC02,hypoxia or acidaemia is the culprit remains to bedetermined.
Drugs 39 (6) 1990
3.2 Causes of Respiratory Acidosis
Airway obstruction or dysfunction of the regulatory system controlling ventilation can result inalveolar hypoventilation and hypercapnia. Causesof respiratory acidosis include obstruction of largeor small airways , respiratory centre depression, circulatory catastrophes, or neuromuscular and restrictive defects.
3.3 Treatment of Respiratory Acidosis
The treatment of respiratory acidosis should bedirected at prompt correction of the underlyingcausal process. The major insult of acute respiratory acidosis is hypoxaernia, and oxygen must beadministered at the onset. If ventilatory support isnecessary in acute hypercapnia, the paC02 can berapidly dropped to normal without adverse consequences. Alkali administration should be givenonly for superimposed metabolic acidosis .
In chronic respiratory acidosis efforts to correctthe cause are often less fruitful because of the irreversible nature of the underlying disease process.Careful attention to volume status, nutrition, chestphysiotherapy and the administration of bronchodilators and antibiotics are often effective in improving ventilation. In view of the chronic natureof the hypercapnia, it is prudent to decrease paC02toward normal over a period of hours to days andsimultaneously to provide sufficient chloride to allow the kidneys to excrete previously retained bicarbonate. As described above, more rapid repairmay result in posthypercapnic alkalosis. Likewise,any coexisting metabolic alkalosis should bepromptly treated because alkalosis may blunt ventilation and induce hypoxia.
4. Respiratory Alkalosis
Respiratory alkalosis is initiated by a reductionin arterial carbon dioxide tension, which alkalinises the body fluids. Titration of nonbicarbonatebuffers results in a small decrement in plasma bicarbonate concentration. Over time, changes in the
Treatm ent of Acid-Base Disorders
renal absorption of bicarbonate serve to attenuatethe degree of alkalinisation.
4.1 Clinical Manifestations
As with respiratory acidosis, central nervoussystem dysfunction is the most prominent clinicalfeature of respiratory alkalosis. Acute hypocapniainduces lightheadedness, confusion and, on occasion, seizures. These manifestations are mediatedthrough a decrease in cerebral blood flow: for example , a 40% reduction in flow is observed at apaC02 of 20mm Hg. In fact, this effect on bloodflow provides the rationale for inducing acute hypocapnia in selected settings to reduce cerebraloedema. Chronic respiratory alkalosis appears tobe better tolerated in terms of cerebral dysfunction.
4.2 Causes of Respiratory Alkalosis
Respiratory alkalosis is associated with manyserious illnesses. In an intensive care unit , respiratory alkalosis appears to be the most commonacid-base derangement. In such patients, a paC02of 15mm Hg or less has been associated with amortality rate of almost 90% (Mazzara et al. 1974).The causes of hypocapnia are many , including hypoxia, pulmonary disease and various central nervous system disorders.
4.3 Treatment of Respiratory Alkalosis
As in treating all acid-base disorders, the therapyof respiratory alkalosis is centred on reversal of theroot cause. Short of this goal, there is no effectivetreatment of primary hypocapnia. Hypoxia itself isa frequent cause of hypocapnia, and administration of oxygen alone often suffices to correct thealkalosis. If the cause is not immediately apparent,consideration should be given to salicylate intoxication , early Gram-negative sepsis and meningitis ,because early intervention may be life-saving.
5. Mixed Acid-Base Disturbances
The coexistence of more than one acid-base disorder is a frequent occurrence and is termed amixed disturbance. Virtually any combination of
853
simple disorders can arise. When plasma bicarbonate concentration and paC02 are altered in opposite directions extreme shifts in hydrogen ionconcentration may ensue, whereas changes in thesame direction tend to ameliorate the change inpH. Some common mixed disorders are discussed.
5.1 Metabolic and Respiratory Acidosis
A mixed metabolic and respiratory acidosis isreadily apparent whenever the plasma bicarbonateis low and the paC02 is high. A more subtle version of this mixed disorder is present in patientswith respiratory acidosis and a normal rather thanelevated plasma bicarbonate concentration. Similarly, when metabolic acidosis is not accompaniedby an appropriate decrease in paC02, a mixed disorder exists. Common examples of mixed metabolic and respiratory acidosis are untreated cardiopulmonary arrest , chronic obstructive lung diseasecomplicated by septic shock, and poisoning withvarious drugs and toxins. Because an extreme degree of acidosis can occur with mixed metabolicand respiratory acidosis, it is imperative that themixed nature of the disturbance is identified earlyand therapy is directed at both disorders.
5.2 Metabolic and Respiratory Alkalosis
Similarly, a mixed metabolic and respiratory alkalosis can be diagnosed whenever the plasma bicarbonate is high and the paC02 is low. Here, too,the extreme shift in hydrogen ion concentration thatoccurs makes recognition of vital importance.Mixed metabolic and respiratory alkalosis can occur when patients with respiratory alkalosis (e.g.from congestive heart failure) are treated with potent diuretics . Another setting where this disturbance may occur is when patients with primary hypocapnia associated with liver disease are treatedwith diuretics or gastric drainage. Clearly, therapyshould be directed at removing the underlyingcause, if possible. In view of the difficulty in treating primary hypocapnia , efforts to reduce the elevated plasma bicarbonate concentration are morefruitful.
854
5.3 Metabolic Acidosis and RespiratoryAlkalosis
The mixed disturbance comprised of metabolicacidosis and respiratory alkalosis can be diagnosedwhen plasma bicarbonate concentration and paC02are both low and the pH is normal or near normal.This disturbance can occur when severe metabolicacidosis is rapidly corrected, when lactic acidosiscomplicates septic shock, in salicylate intoxication,and in the hepatorenal syndrome. Treatment mustbe directed at the specific acid-base disorders andthe underlying process.
5.4 Metabolic Alkalosis and RespiratoryAcidosis
A diagnosis of mixed metabolic alkalosis andrespiratory acidosis can be made when plasma bicarbonate concentration and paC02 are both elevated and the pH is normal or near normal. Thisdisturbance is commonly seen in patients withchronic lung disease who are treated with diuretics.Gastric drainage, vomiting or various other causesof metabolic alkalosis will produce a similar picture when superimposed on respiratory failure. Efforts should be directed at improving ventilationand specifically treating the metabolic alkalosis.Even a small component of coexisting metabolicalkalosis will decrease ventilation and interfere withweaning efforts. As noted previously, administration of carbonic anhydrase inhibitors (e.g. acetazolamide) may be useful in this setting. When severe alkalaemia is present, hydrochloric acid or ahydrochloric acid precursor should be administered.
6. Conclusions
Prompt and appropriate therapy reduces oreliminates many morbid effects of acid-base disturbances.
In many forms of metabolic acidosis, administration of sodium bicarbonate increases plasmabicarbonate concentration predictably. In disorders characterised by rapid alkali loss or rapid acid
Drugs 39 (6) 1990
accumulation, the amount of alkali needed will beincreased, and the quantity to be administered canbe determined only by repeated monitoring of apatient's acid-base status. Excessiveadministrationof alkali has its own dangers.
Therapy in metabolic alkalosis also depends onthe nature of the underlying cause. Those disorderscharacterised by depletion of body chloride storeswill respond well to treatment with sodium or potassium chloride; those unassociated with chloridedeficiency (principally hyperadrenal states) requireelimination of the root cause. In both forms,administration of hydrochloric acid or a hydrochloric acid precursor may be needed when alkalaemia is particularly severe.
In acute respiratory acidosis and acute respiratory alkalosis, prompt restoration of carbon dioxide tension to normal immediately restores normalacid-base equilibrium and avoids the complications of hypercapnia or hypocapnia.
The therapy of chronic respiratory acidosis musttake into account the increase in plasma bicarbonate concentration that occurs during adaptationto chronic hypercapnia . When carbon dioxide tension in such patients is reduced abruptly, plasmabicarbonate concentration must be reduced simultaneously, so as to avoid posthypercapnic metabolic alkalosis. Administration of the sodium orpotassium salts of chloride is usually sufficient toavoid this complication .
Elimination of the cause of the sustained hypocapnia is the only approach to the treatment ofchronic respiratory alkalosis. Attempts to treat theacid-base disorder per se are usually futile.
In all acid-base disturbances, therapy is an iterative process. No therapeutic algorithm existswhich offers a prospective, preset therapeutic package. Repeated, and sometimes continuous observation of the patient and repeated measurements ofthe patient's acid-base parameters are required foroptimal therapy.
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