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Immunosuppressive treatment in severe connective tissue diseases: effects of low dose intravenous cyclophosphamide

机译:严重结缔组织疾病的免疫抑制治疗:低剂量静脉内环磷酰胺的作用

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摘要

OBJECTIVE—To review our experience with low dose intravenous pulse cyclophosphamide in the treatment of patients with severe connective tissue diseases.
PATIENTS—Ninety patients (68F:22M) with severe connective tissue diseases received a total of 883 cyclophosphamide pulses with 78 of 90 patients initially having weekly 500 mg pulses for a median of three (2-10) weeks. Diagnoses included: systemic lupus erythematosus (SLE) (n=43); systemic vasculitides (n=42); idiopathic inflammatory myopathies (n=4); mixed essential cryoglobulinaemic vasculitis (n=1). The median age was 48 (range 22-76) years with a median disease duration of 94 (18-250) months.
RESULTS—Complete or partial remission was noted in 68 of 90 patients (75.5%) after a median follow up of 56 (5-213) months. At follow up significant median changes were noted in SLE patients: erythrocyte sedimentation rate (ESR) from 44 to 22 mm 1st hour; anti-dsDNA antibody concentrations from 81 to 48 IU/ml; proteinuria from 2.5 to 1.5 g/day; serum albumin from 36 to 40 g/l; complement C3 from 0.88 to 0.90 g/l, and C4 from 0.18 to 0.22 g/l. In the vasculitis patients significant median changes were seen in: ESR from 44 to 15 mm 1st hour; C reactive protein (CRP) from 16 to 5 g/dl; neutrophils from 8.55 to 4.3 × 109/l; platelets from 340 to 261 × 103/l, and haemoglobin from 12.6 to 13.2 g/dl. Patients with Churg-Strauss syndrome, Wegener's granulomatosis, and neuropsychiatric lupus showed the best initial response but 58% of Wegener's patients relapsed. Median corticosteroid doses were significantly reduced from 15 (5-60) mg to 10 (3-35) mg daily. Adverse events: infections (7 patients), neutropenia (5), lymphopenia (18), and haemorrhagic cystitis (1 intravenous and 2 oral cyclophosphamide), allergies to mesna (2). None of the women at risk had prolonged amenorrhoea. Five patients doubled their serum creatinine and five died from sepsis (2) or severe disease (3).
CONCLUSION—Treatment of severe connective tissue diseases with `low dose' intravenous cyclophosphamide pulses compares in efficacy with the higher monthly doses previously advocated. Treatment was well tolerated with fewer adverse effects and most significantly, there were no cases of premature ovarian failure.

机译:目的—回顾我们在低剂量静脉脉冲环磷酰胺治疗严重结缔组织疾病患者中的经验。
患者— 90名严重结缔组织疾病的患者(68F:22M)总共接受了883次环磷酰胺脉冲治疗,其中78例最初接受每周500 mg脉搏治疗的90名患者,平均三(2-10)周。诊断包括:系统性红斑狼疮(SLE)(n = 43);全身性血管炎(n = 42);特发性炎症性肌病(n = 4);混合性原发性冷球蛋白性血管炎(n = 1)。中位年龄为48岁(范围22-76)岁,中位疾病持续时间为94(18-250)个月。
结果-在中位随访56(5-213)个月后,有90例患者中有68例(75.5%)完全或部分缓解。在随访中,SLE患者的中位数有显着变化:第一小时从44毫米到22毫米的红细胞沉降率(ESR);抗dsDNA抗体浓度从81到48 IU / ml;蛋白尿从2.5至1.5克/天;血清白蛋白从36至40 g / l;补体C3从0.88至0.90 g / l,C4从0.18至0.22 g / l。在血管炎患者中,在第1小时的ESR从44到15毫米出现了明显的中值变化; C反应蛋白(CRP)从16到5 g / dl;中性粒细胞从8.55到4.3×10 9 / l;血小板从340至261×10 3 / l,血红蛋白从12.6至13.2 g / dl。 Churg-Strauss综合征,Wegener肉芽肿病和神经精神性狼疮患者表现出最佳的初始反应,但58%的Wegener患者复发。皮质类固醇的中位剂量从每天15(5-60)mg显着减少到10(3-35)mg。不良事件:感染(7例患者),中性粒细胞减少症(5),淋巴细胞减少(18),和出血性膀胱炎(1静脉和2口服环磷酰胺),对中膜过敏(2)。没有危险的妇女没有长时间的闭经。五名患者的血清肌酐增加了一倍,五名死于败血症(2)或严重疾病(3)。
结论—使用“低剂量”静脉内环磷酰胺脉冲治疗严重结缔组织疾病的疗效与以前较高的每月剂量相比提倡。治疗耐受性好,不良反应少,最显着的是,没有卵巢早衰的病例。

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