Should we routinely add CRP to clozapine titrations? - Learning from three cases

Should we routinely add CRP to clozapine titrations? - Learning from three cases

Objectives: An international guideline recently provided certain personalized schedules for titrating clozapine in adult inpatients by considering: 1) DNA ancestry group, 2) sexsmoking subgroup, and 3) presence/absence of clozapine poor metabolizer (PM) status. Measuring CRP levels at baseline and d...

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Bibliographic Details
Published in:Neuropsychopharmacologia Hungarica : a Magyar Pszichofarmakológiai Egyesület lapja Vol. 24; no. 4; p. 153
Main Authors: Shelton, Charles, Ruan, Can-Jun, Ertuğrul, Aygün, Cotes, Robert O, De Leon, Jose
Format: Journal Article
Language:English
Published: Hungary 01-12-2022
Subjects:
Adult
Antipsychotic Agents - adverse effects
C-Reactive Protein
Clozapine - adverse effects
Female
Humans
Inflammation - chemically induced
Male
Myocarditis - chemically induced
Myocarditis - diagnosis
Prospective Studies
clozapine/metabolism
inflammation
CYP1A2
clozapine/blood
myocarditis/chemically induced
clozapine/adverse effects
myocarditis/etiology
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Summary:Objectives: An international guideline recently provided certain personalized schedules for titrating clozapine in adult inpatients by considering: 1) DNA ancestry group, 2) sexsmoking subgroup, and 3) presence/absence of clozapine poor metabolizer (PM) status. Measuring CRP levels at baseline and during the first 4 weeks is recommended. Titrations too fast for the metabolism of specific patients can lead to clozapine-induced inflammations and CRP elevations. Methods: Three published cases are reinterpreted. Better outcomes might have been obtained by using the guideline. Results: Case 1 was a Chinese male non-smoker, a clozapine PM due to an underlying inflammation. Case 2 was a Turkish female non-smoker who developed clozapine-induced myocarditis in the context of 4 risk factors (undiagnosed infl ammation, obesity, valproate and olanzapine co-prescription). Case 3 was a United States patient of European ancestry with no known risk factors who developed myocarditis after a routine titration and had an unsuccessful rechallenge with 12.5 mg/day. Application of the international clozapine titration guideline may have prevented: 1) Case 1 by recommending against clozapine titration for a patient with an abnormal CRP level, 2) Case 2 by considering 4 risk factors and using a slow titration for clozapine PMs, and 3) Case 3 by using CRP elevations for early identification of a possible genetic PM. Conclusions: When baseline or prior CRPs are normal and then become abnormal during a clozapine titration, this indicates: 1) clozapine-induced inflammation associated with too-rapid titration for that specific patient, and/or 2) co-occurrence of an infection. Prospective studies need to verify this hypothesis.
ISSN:1419-8711