Abstract

Dear editor I read with admiration an article published in your prestigious journal on the rare adverse effects of clozapine (CLZ).1 I write to address a specific issue in this article. In the second paragraph of the section “Dermatological adverse effects”, it was stated that a 54-year-old patient with schizophrenia treated for 28 days with CLZ developed a generalized rash compatible with pityriasis rosea (skin rash that usually begins as one large circular or oval spot on your chest, abdomen, or back). I wish to point out certain problems for coining pityriasis rosea (PR) as the diagnostic label in the patient concerned. First, PR is a paraviral exanthem that might be associated with primary infections or endogenous reactivations of human herpesvirus-7, -6,2,3 or other viruses.4,5 The underlying immunopathogenesis of PR is likely to be entirely different from that in PR-like drug eruptions.6 Second, rashes with morphological and distributional resemblances to PR that may be caused by drugs are currently considered as a separate condition distinct from PR in ICD-10.7 Thus, we recommend a revision to “pityriasis rosea-like drug eruption” as the diagnostic label in the article.1 Third, quoting the diagnostic label as “PR-like drug eruption” is compatible with the current diagnostic criteria8,9 and the modern classification10 of PR. Fourth, it was stated that PR is “…skin rash that usually begins as one large circular or oval spot on your chest, abdomen, or back, …”1 This statement refers to PR in general and is incorrect as only about 30%–40% of patients with PR have identifiable herald patches.6 Moreover, it gives us no information on the morphology, distribution, and time sequence of rash for the 54-year-old patient with schizophrenia. The characteristics of PR-like drug eruptions are 1) absence of the herald patch, 2) bright violet-red color of the rash with marked inflammation, 3) being more pruritic, 4) dominance of eosinophils in the skin infiltrate, and 5) eosinophilia in the peripheral blood.11 From reading the article by De Fazio et al1 the readers could get a false impression that PR-like drug eruptions usually begin as one larger circular or oval spot. The reverse is true – there is usually no herald patch for PR-like drug eruptions. It is thus not an issue of nomenclature per se – it might lead to confusions to readers and other investigators as to the clinical manifestations of PR-like drug eruptions. Fifth, most recent articles coin the term “PR-like drug eruptions” rather than “PR” for drug-induced PR-like rashes.12–15 I advocate that this convention should be followed. Finally, some patients with PR-like drug eruptions could have been recruited into clinical studies and trials (Villarama and Lansang, unpublished data, 2003).16,17 I recommend that such practices be discontinued. Therefore, I hope that through this item of correspondence, the status of PR-like drug eruption can be rectified. Otherwise, I am extremely impressed by the high quality of the article by De Fazio et al1 and reading the article has been of immense educational value for me.

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