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首页> 外文期刊>JAMA dermatology >Safety of Systemic Agents for the Treatment of Pediatric Psoriasis
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Safety of Systemic Agents for the Treatment of Pediatric Psoriasis

机译:用于治疗儿科牛皮癣的全身性药剂的安全性

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IMPORTANCE Use of systemic therapies for moderate to severe psoriasis in children is increasing, but comparative data on their use and toxicities are limited.& para;& para;OBJECTIVE To assess patterns of use and relative risks of systemic agents for moderate to severe psoriasis in children.& para;& para;DESIGN, SETTING, AND PARTICIPANTS A retrospective review was conducted at 20 centers in North America and Europe, and included all consecutive children with moderate to severe psoriasis who used systemic medications or phototherapy for at least 3 months from December 1,1990, to September 16,2014.& para;& para;MAIN OUTCOMES AND MEASURES The minimal core data set included age, sex, severity of psoriasis, systemic interventions, monitoring, adverse events (AEs), and reason for discontinuation.& para;& para;RESULTS For 390 children (203 girls and 187 boys; mean [SD] age at diagnosis, 8.4 [3.7] years) with psoriasis who used 1 or more systemic medications, the mean interval between diagnosis and starting systemic therapy was 3.0 years. Methotrexate was used by 270 patients (69.2 % ), biologic agents (primarily etanercept) by 106 (27.2%), acitretin by 57 (14,6%), cyclosporine by 30 (7.7%), fumaric acid esters by 19 (4.9 % ), and more than 1 medication was used by 73 (18.7%). Of 270 children taking methotrexate, 130 (48.1%) reported 1 or more AEs associated with methotrexate, primarily gastrointestinal (67 [24 ,8%]). Folic acid 6 days per week (odds ratio, 0.16; 9 5 % Cl, 0,06-0.41; P < .001) or 7 days per week (OR, 0.21; 9 5 % Cl, 0.08-0,58; P = .003) protected against gastrointestinal AEs more than once-weekly folic acid, regardless of the total weekly dosage. Methotrexate-associated hepatic transaminase elevations were associated with obesity (35 of 270 patients [13.0%]), but a folic acid regimen was not. Injection site reactions occurred in 20 of 106 patients (18.9%) treated with tumor necrosis factor inhibitors, but did not lead to discontinuation of treatment. Having 1 or more AEs related to medication, gastrointestinal AE, laboratory abnormality, or AE leading to discontinuation of the drug was more likely with methotrexate than tumor necrosis factor inhibitors, but having 1 or more infections related to medication (predominantly upper airway) was less likely. Six patients developed a serious treatment-related AE (methotrexate, 3; fumaric acid esters, 2; and adalimumab, 1), but methotrexate and biologic agents w ere taken for a mean duration that was 2-fold greater than the mean duration for cyclosporine or fumaric acid esters. No patient developed tuberculosis or a malignant neoplasm.& para;& para;CONCLUSIONS AND RELEVANCE Medication-related AEs occur less often with tum or necrosis factor inhibitors than with methotrexate. Folic acid administration 6 or 7 times per week protected more against methotrexate-induced gastrointestinal AEs than did weekly administration. A prospective registry is needed to track the long-term risks of systemic agents for pediatric psoriasis.
机译:在儿童中,中度至严重牛皮癣的系统性疗法的重要性正在增加,但对其使用和毒性的比较数据是有限的。&段;&段;目的评估适度至严重牛皮癣的全身性药物的使用模式和相对风险儿童。&段;&段;设计,设置和与会者回顾性审查是在北美和欧洲的20个中心进行的,并包括所有连续的儿童,中度至严重牛皮癣,他们使用了至少3个月的系统性药物或光疗法12月1,190年12月1日,到2014年9月16,2014。&Para;&Para;主要结果和测量最小的核心数据集包括年龄,性别,牛皮癣的严重程度,系统性干预,监测,不良事件(AES),以及停止原因。&para;&para;结果390名儿童(203名女孩和187名男孩;意思是诊断时的年龄,8.4 [3.7]年龄)与使用1或以上的系统性药物,诊断之间的平均间隔的牛皮癣。并开始全身疗法3.0年。甲氨蝶呤由270名患者(69.2%),生物剂(主要依托西普)用106(27.2%),丙酸汀(14.6%),环孢菌素(7.7%),富马酸酯,富马酸酯(4.9%) ),73(18.7%)使用超过1种药物。 270例服用甲氨蝶呤的儿童,130名(48.1%)报告了与甲氨蝶呤相关的1或更多AE,主要是胃肠道(67 [24,8%])。叶酸每周6天(差距,0.16; 9 5%Cl,0.06-0.41; p <.001)或每周7天(或0.21; 9 5%Cl,0.08-0,58; p = .003)免受胃肠道的影响,不止一周叶酸,无论总每周剂量如何。甲氨蝶呤相关的肝脏转氨酶升高与肥胖有关(35名患者的35名患者[13.0%]),但叶酸方案不是。用肿瘤坏死因子抑制剂治疗的106名患者(18.9%)发生注射部位反应,但没有导致停止治疗。具有与药物的1种或更多的AES,胃肠AE,实验室异常或导致药物中断的AE比肿瘤坏死因子抑制剂更可能与甲氨蝶呤更可能,但具有1或更多与药物(主要上呼吸道)的感染较少可能。六名患者开发了一个严重的治疗相关的AE(甲氨蝶呤,3;富马酸酯,2;和Adalimumab,1),但甲氨蝶呤和生物学剂WERE的平均持续时间比环孢菌素的平均持续时间大2倍或富马酸酯。没有患者开发结核病或恶性肿瘤。&para;&para;结论和相关的药物相关的AES与肿瘤或坏死因子抑制剂的较少发生而不是甲氨蝶呤。叶酸给药每周6或7次,对甲氨蝶呤诱导的胃肠道相比,比每周给药更多。需要一个预期的注册处,以跟踪儿科牛皮癣的全身性药物的长期风险。

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