Publication details

Léčba anakinrou u Schnitzler-syndromu - výsledky první retrospektivní multicentrické studie šesti pacientů z České republiky

Title in English Anakinra Treatment in Schnitzler Syndrome - Results of the First Retrospective Multi-center Study in Six Patients from the Czech Republic
Authors

SZTURZ Petr ŠEDIVÁ Anna ŽUREK M. ADAM Zdeněk ŠTORK J. ČERMÁKOVÁ Zdeňka STEYEROVÁ P. VOKÁČOVÁ A. HRBEK J. SÝKORA M. ŠPIČKA I. MECHL Zdeněk MAYER Jiří

Year of publication 2014
Type Article in Periodical
Magazine / Source Klinická onkologie
MU Faculty or unit

Faculty of Medicine

Citation
Field Oncology and hematology
Keywords Schnitzler syndrome – monoclonal gammopathy; interleukins; anakinra; acute; phase proteins; osteogenesis
Description Background: Schnitzler syndrome is a very rare, acquired, autoinflammatory disease of mostly adult onset with characteristic combination of chronic recurrent urticaria and monoclonal immunoglobulin M or G gammopathy predisposing the patients to malignant lymphoproliferation. In this work, we analyzed the results of biological therapy with anakinra on a national level aiming to supply data for effective pharmacoeconomic estimates, lay the grounds of nationwide patient registry, raise awareness among professional public and optimize provided health care. Patients and Methods: The retrospective study (10/2006-9/2013) included six males with definite Schnitzler syndrome verified by the new Strasbourg criteria. All patients were pretreated with antihistamines, nonsteroidal anti-inflammatory drugs and glucocorticoids. Four patients underwent two or more treatment lines including intravenous bisphosphonates, 2- chlorodeoxyadenosine (cladribine), interferon-alpha, PUVA photochemotherapy, cyclosporine A, thalidomide, bortezomib, chlorambucil, cyclophosphamide, colchicine and methotrexate. Anakinra monotherapy was initiated in standard dosing (100 mg subcutaneously daily). Results: Complete and partial remissions were achieved in five (83%) and one patients (17%), respectively. Complete remission was characterized by urticaria and pain regression (within hours), normalization of inflammatory markers(within days) and bone metabolism improvement assessed by the markers of osteoblastic osteoformation and osteoclastic osteoresorption in one case (within weeks). With normalized inflammatory markers (including interleukin-6 and interleukin-18), arthralgia and sporadic exacerbations of urticaria and fevers persist in the patient in partial remission with proven Q703K polymorphism in NLRP3 gene. The median treatment follow-up was 30.5 months (37.2 +/- 31.2 (n=6)). The dosing interval was prolonged in one case of complete remission to 48 hours. No serious adverse reactions occurred during anakinra application. Conclusion: In Schnitzler syndrome, anakinra represents an effective, verified and safe medication with potentionally long-term administration not compromising its original efficacy and subjective tolerance. Anakinra, blocking autonomous inflammatory reaction of the organism via interleukin-1 pathway, is a generally accepted first line treatment that should be made available in standard dosing for all Schnitzler patients.
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