Humanized anti–interleukin-6 receptor antibody treatment of multicentric Castleman disease

Norihiro Nishimoto(Osaka University Hospital), Yuzuru Kanakura(Osaka University Hospital), Katsuyuki Aozasa(Osaka University Hospital), Takeshi Johkoh(Osaka University Hospital), Minoru Nakamura(Osaka University Hospital), Shuji Nakano(Osaka University Hospital), Nobuaki Nakano(Osaka University Hospital), Yasuo Ikeda(Osaka University Hospital), Takeshi Sasaki(Osaka University Hospital), Kiyoshi Nishioka(Osaka University Hospital), Masamichi Hara(Osaka University Hospital), Hirokuni Taguchi(Osaka University Hospital), Yukihiko Kimura(Osaka University Hospital), Yoshiro Kato(Osaka University Hospital), Hideki Asaoku(Osaka University Hospital), Shunichi Kumagai(Osaka University Hospital), Fumio Kodama(Osaka University Hospital), Hideko Nakahara(Osaka University Hospital), Keisuke Hagihara(Osaka University Hospital), Kazuyuki Yoshizaki(Osaka University Hospital), Tadamitsu Kishimoto(Osaka University Hospital)
Blood
July 6, 2005
10.1182/blood-2004-12-4602
Cited by 749Open Access
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Abstract

Multicentric Castleman disease (MCD) is an atypical lymphoproliferative disorder characterized by systemic lymphadenopathy and constitutional inflammatory symptoms. Dysregulated overproduction of interleukin-6 is responsible for the clinical abnormalities. This multicenter prospective study was undertaken to evaluate the safety and efficacy of a humanized anti-human interleukin-6 (IL-6) receptor monoclonal antibody (MRA) in patients with MCD. We report here results of the first 60 weeks of the study enrolling 28 patients. The initial dosing period consisted of 8 infusions of 8 mg/kg MRA administered biweekly. Adjustments in the dose and treatment interval were allowed for each patient in an extension phase after 16 weeks. Within 16 weeks, treatment with MRA consistently alleviated lymphadenopathy and all the inflammatory parameters. Hemoglobin, albumin, and total cholesterol levels, high-density lipoprotein cholesterol values, and body mass index all increased significantly. In addition, fatigue diminished. Chronic inflammatory symptoms were successfully managed over 60 weeks. In 8 (28.6%) patients, the MRA dose was decreased or the treatment interval was extended without exacerbation. Eleven (73.3%) of 15 patients who had received oral corticosteroids before study entry were able to do well on a reduced corticosteroid dose. Most adverse events were mild to moderate in severity. MRA was tolerated well and significantly alleviated chronic inflammatory symptoms and wasting in patients with MCD.

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