Use of plasma levels in evaluation of procainamide dosage.

Shaw, T. R. D.; Kumana, CR; Royds, R B; Padgham, C.; Hamer, Janice

doi:10.1136/hrt.36.3.265

Cited by 12 publications

(6 citation statements)

References 6 publications

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“…There was a wide variation in individual peak values despite the relatively minor dose differences. This was previously reported by Koch-Weser &Klein (1971) andShaw et al (1974) using the conventional tablet and more recently by Cunningham, Sloman & Nyberg (1977) with Durules. Ihlen & Ditlefsen (1975) in a clinical trial comparing Durules and Retard reported a consistent difference in levels achieved 8 h after commencement of treatment, with Durules reaching higher levels than Retard.…”

Section: Discussionsupporting

confidence: 52%

“…Its use as a prophylactic agent has been severely restricted by the short half-life of 3.5 h (Koch-Weser & Klein, 1971) of the conventional oral preparation (Pronestyl, procainamide hydrochloride, Squibb). This has meant that 3 hourly administration of the drug has been necessary to maintain therapeutic plasma levels (Koch-Weser et al, 1969;Shaw, Kumana, Royds, Padgham & Hamer, 1974).…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

A pharmacokinetic comparison of two sustained‐release oral procainamide preparations.

Hore¹,

Bones²,

Rollinson³

et al. 1979

Brit J Clinical Pharma

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1 The pharmacokinetics of two different sustained‐release oral procainamide preparations were studied in ten hospital patients with normal blood ureas and no clinical evidence of heart failure. Each patient received either one or other preparation at 12 hourly intervals for four doses. Frequent blood sampling enabled close monitoring of blood levels. 2 Results showed that both preparations were essentially similar in their pharmacokinetics. Both effectively double the half‐ life of conventional oral procainamide to 6.5 h and are suitable as prophylactic preparations. One patient developed toxic levels, thought to be related to her metabolic status of being a very slow acetylator. To avoid toxicity pre‐therapy assessment of a patient's cardiac and renal function and acetylator status is advised.

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Section: Discussionsupporting

confidence: 52%

Section: Introductionmentioning

confidence: 99%

A pharmacokinetic comparison of two sustained‐release oral procainamide preparations.

Hore¹,

Bones²,

Rollinson³

et al. 1979

Brit J Clinical Pharma

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“…1972;Karlsson et al, 1974;Graffner, 1975). Furthermore, it is often 'abnormal' precisely in those clinical situations for which the drug is commonly used (Koch-Weser, 1971;Shaw et al. 1974).…”

Section: Unpredictable Dose-concentration Relationshipmentioning

confidence: 94%

“…1952;Enselberg and Lipkin, 1952;Bigger and Heissenbuttel, 1969;Gey et al. 1974;Shaw et al, 1974;Karlsson and Sonnhag, 1976;Karlsson et al, 1977).…”

Section: Establishment Of the Therapeutic Rangementioning

confidence: 98%

Serum Procainamide Levels As Therapeutic Guides

Koch‐Weser

1977

Clinical Pharmacokinetics

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Dosage schedules o( procaillamide should be individualised. because the amount of the drug required to colllrol velllricular tachyarrhythmias varies widely among patiellls. Individual differences in procainamide pharmacokinetics are responsible for most of this variation and are reflected by the serum COllcelllratioll (!f the drug. Proc(1inamide concelllratiolls ill serum and in myocardial interstitial fluid must equilibrate rapidly and be similar at equilibrium. The effects lif the drug Oil the myocardial cell membrane are proportional to the concentration at that site. develop quickly alld are readily reversible. Accordingly. there is a useful relation between the serulII concentration and the illtensity (I{ cardiac action lif procainamide.Procainamide serum levels are most helpful fiJI' adjusting dosage schedules in patiellls whose response to the drug is difficult to el'aluate or appears to be abnormal. Serum concentrations of 4 to 10mg/ litre correct alld prevel1l over 90 % ofvelllricular tachyarrhythmias responsive to procainamide without causing important adverse effects. Lower concelllrations are partially effective in some patiellts. A dditional therapeutic benefit is rarely obtained by raising the serul11 level above IOmg/ litre. alld serious toxicity becomes illcreasingly common above 12mg/ litre. Sen/m concentration i/!formation must always be illlerpreted in the light lif all other clinical il!formatirJlJ. since the type o( arrhythmia and many other factors influence the response (!f the heart to procainamide. N-Acetylprocainamide. a metabolite (!f procainamide. possess antiarrhythmic activity and is not measured by the usual methods for determining serum procainamide. The concentration ratio I!f drug and metabolite in serum varies greatly among patiellls. and their potency ratio against Farious ventricular dysrhythmias in man remains in question. By measuring Nacetylprocainamide as well as procainamide. it may ultimately be possible to de.fine a therapeutic rallge (Jf the sum (!f the appropriately weighted concentrations lif the 2 compounds.For the present. tile therapist must rely primarily on·the serum concelllration (!f procainamide for supplementillg his c1illicaljudgmelll.

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“…The frequency of adverse effects was higher in patients with both acute myocardial infarction and congestive failure than in those with either condition singly or with neither, although the results did not attain conventional levels of statistical significance. This is presumably due to the severity of the underlying cardiac disease, although it has also been reported that absorption of this drug is reduced and metabolism and excretion impaired in patients with cardiac failure (Shaw, Kumana, Royds, Padgham & Hamer, 1974;Biggar, 1975), and in the early phases after myocardial infarction (Koch-Weser, Klein, Foo-Canto, Kastor & de Sanctis, 1969). 45 Procainamide is excreted partly by the kidney and partly by hepatic transformation to N-acetylprocainamide.…”

Section: Methodsmentioning

confidence: 99%

Adverse reactions to procainamide.

Lawson¹,

Jick²

1977

Brit J Clinical Pharma

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1 Data from a comprehensive drug surveillance programme are analysed to provide details of procainamide use and toxicity in medical wards of teaching hospitals in five countries. 2 Out of a total of 488 recipients 9.2% had one or more adverse effect attributed to the drug; common effects being arrhythmias, gastro‐intestinal upsets and drug fever. Although occasionally of major severity, no patient died as a consequence of procainamide toxicity. 3 Toxicity was directly related to total daily dose and duration of hospitalization but was not related to age, weight of the patient or presenting urea or albumin concentrations.

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Use of plasma levels in evaluation of procainamide dosage.

Cited by 12 publications

References 6 publications

A pharmacokinetic comparison of two sustained‐release oral procainamide preparations.

A pharmacokinetic comparison of two sustained‐release oral procainamide preparations.

Serum Procainamide Levels As Therapeutic Guides

Adverse reactions to procainamide.

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