The study objective was to report treatment with an interleukin (IL)-1 receptor antagonist, anakinra, in patients with multiorgan Behcet's disease (BD). Comparison of clinical manifestations, previous treatments, markers of inflammation, concomitant medications, treatment regimen modifications, relapses, and adverse events before and during anakinra administration among patients with BD were evaluated. Nine BD patients (mean age 34.55 ± 16.30 years) refractory to tumor necrosis factor blockers and standardized therapies are reported in our survey. Their mean age at disease onset was 25 ± 13.88 years and their overall disease duration was 9.55 ± 5.33 years. All patients were positive for the HLA-B51 allele. Within 1 or 2 weeks following the initiation of anakinra, eight out of nine patients promptly responded, and most of them were maintained on 100 mg of daily anakinra with low doses of prednisone. However, most patients experienced a relapse in one or more clinical manifestations over time (mean time to relapse 29 ± 21.65 weeks), and only one patient remained completely under control on anakinra monotherapy. Despite a relapse in one or more disease manifestations, treatment was continued in most patients for a mean period of 13.75 ± 6.49 months. No serious adverse events occurred. Eight out of nine refractory BD patients showed a prompt improvement after starting anakinra, supporting the concept that IL-1 plays a pathological role in this disease. Nevertheless, after several months, most patients experienced a relapse. It remains unclear whether increasing the dose of anakinra would have prevented the reoccurrence of disease activity.

Cantarini, L., Vitale, A., Scalini, P., Dinarello, C. A., Rigante, D., Franceschini, R., Simonini, G., Borsari, G., Caso, F., Lucherini, O. M., Frediani, B., Bertoldi, I., Punzi, L., Galeazzi, M., Cimaz, R., Anakinra treatment in patients with gout and type 2 diabetes, <<CLINICAL RHEUMATOLOGY>>, 2015; 34 (7): 1293-1301. [doi:10.1007/s10067-013-2443-8] [http://hdl.handle.net/10807/87535]

Anakinra treatment in patients with gout and type 2 diabetes

Rigante, Donato;
2015

Abstract

The study objective was to report treatment with an interleukin (IL)-1 receptor antagonist, anakinra, in patients with multiorgan Behcet's disease (BD). Comparison of clinical manifestations, previous treatments, markers of inflammation, concomitant medications, treatment regimen modifications, relapses, and adverse events before and during anakinra administration among patients with BD were evaluated. Nine BD patients (mean age 34.55 ± 16.30 years) refractory to tumor necrosis factor blockers and standardized therapies are reported in our survey. Their mean age at disease onset was 25 ± 13.88 years and their overall disease duration was 9.55 ± 5.33 years. All patients were positive for the HLA-B51 allele. Within 1 or 2 weeks following the initiation of anakinra, eight out of nine patients promptly responded, and most of them were maintained on 100 mg of daily anakinra with low doses of prednisone. However, most patients experienced a relapse in one or more clinical manifestations over time (mean time to relapse 29 ± 21.65 weeks), and only one patient remained completely under control on anakinra monotherapy. Despite a relapse in one or more disease manifestations, treatment was continued in most patients for a mean period of 13.75 ± 6.49 months. No serious adverse events occurred. Eight out of nine refractory BD patients showed a prompt improvement after starting anakinra, supporting the concept that IL-1 plays a pathological role in this disease. Nevertheless, after several months, most patients experienced a relapse. It remains unclear whether increasing the dose of anakinra would have prevented the reoccurrence of disease activity.
2015
Inglese
Cantarini, L., Vitale, A., Scalini, P., Dinarello, C. A., Rigante, D., Franceschini, R., Simonini, G., Borsari, G., Caso, F., Lucherini, O. M., Frediani, B., Bertoldi, I., Punzi, L., Galeazzi, M., Cimaz, R., Anakinra treatment in patients with gout and type 2 diabetes, <<CLINICAL RHEUMATOLOGY>>, 2015; 34 (7): 1293-1301. [doi:10.1007/s10067-013-2443-8] [http://hdl.handle.net/10807/87535]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/10807/87535
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