Lee W I, Yang M H, Lee K F, Chen L C, Lin S J, Yeh K W, Huang J L
Department of Pediatrics, Chang-Gung Children's Hospital and Chang Gung University, Taoyuan, Taiwan.
Clin Rheumatol. 1999;18(3):207-13. doi: 10.1007/s100670050086.
This paper aims to remind paediatric clinicians to suspect and confirm 'PFAPA' syndrome (Periodic Fever, Aphthous stomatitis, Pharyngitis and cervical Adenitis syndrome). We report two cases of PFAPA syndrome: a 3-year-old healthy boy with atopic rhinitis and a boy aged 8 years 5 months who simultaneously had lymphocytic vasculitis syndrome treated with immunosuppressive drugs. Both met Marshall's criteria. The literature regarding PFAPA syndrome was complied using a Medline search for articles published between 1963 and 1998 and we then reviewed the reference lists of the articles. The Medline search revealed 28 cases with available clinical manifestations, management and prognosis. Our study describes two additional cases. We divided the cases into typical (28 cases) and atypical (two cases) PFAPA syndrome. In typical PFAPA, the age of onset was less than 5 years in most cases and the patients presented 4.9 +/- 1.4 days of fever (100%), pharyngitis (89.3%), cervical adenitis (72.1%), stomatitis (71.4%), malaise (64.3%), headache (60.7%), abdominal pain (53.6%) and nausea/vomiting (17.9%). Afebrile intervals were 3.2 +/- 2.4 months and increased with age. The time from initial onset to final episode was 3 years 7 months +/- 3 years 6 months. The total number of episodes was 8.3 +/- 2.5 (range 6-14). Effective treatment included steroids, tonsillectomy/adenoidectomy and cimetidine. The general outcome was good. In atypical PFAPF, the clinical manifestations were similar to those of typical PFAPA except that the age of onset was more than 5 years, and life-threatening intestinal perforation happened once in a patient with underlying Fanconi's anaemia. It was concluded that typical PFAPA syndrome is benign and can be diagnosed by detailed history-taking and from physical findings during repeated febrile episodes with tests to rule out other periodic fever syndromes. A review of the literatures since the first report in 1987 has shown that typical PFAPA syndrome is not associated with significant long-term sequelae and has a good response to steroids. One patient with atypical PFAPA, who received low-dose steroids for over 1 year, developed intestinal perforation after an increment of the 7-day steroid dose. If an underlying problem requires long-term immunosuppressive medication, it is wiser to choose cimetidine rather than increasing the steroid dosage to resolve atypical PFAPA.
本文旨在提醒儿科临床医生怀疑并确诊“PFAPA”综合征(周期性发热、阿弗他口炎、咽炎和颈淋巴结炎综合征)。我们报告了两例PFAPA综合征病例:一例是患有特应性鼻炎的3岁健康男孩,另一例是8岁5个月大的男孩,该男孩同时患有淋巴细胞性血管炎综合征,正在接受免疫抑制药物治疗。两例均符合马歇尔标准。我们使用Medline搜索1963年至1998年发表的文章来整理关于PFAPA综合征的文献,然后查阅了这些文章的参考文献列表。Medline搜索显示有28例具备可用的临床表现、治疗和预后信息。我们的研究又描述了另外两例。我们将这些病例分为典型(28例)和非典型(2例)PFAPA综合征。在典型PFAPA中,大多数病例发病年龄小于5岁,患者出现发热(100%)4.9±1.4天、咽炎(89.3%)、颈淋巴结炎(72.1%)、口炎(71.4%)、不适(64.3%)、头痛(60.7%)、腹痛(53.6%)以及恶心/呕吐(17.9%)。无热间期为3.2±2.4个月,且随年龄增长而增加。从首次发病到最后一次发作的时间为3年7个月±3年6个月。发作总数为8.3±2.5次(范围6 - 14次)。有效治疗方法包括使用类固醇、扁桃体切除术/腺样体切除术以及西咪替丁。总体预后良好。在非典型PFAPF中,临床表现与典型PFAPA相似,只是发病年龄超过5岁,并且在一名患有范可尼贫血的患者中曾发生过一次危及生命的肠穿孔。结论是典型PFAPA综合征是良性的,可通过详细询问病史以及在反复发热发作期间进行体格检查并通过检查排除其他周期性发热综合征来诊断。自1987年首次报告以来的文献综述表明,典型PFAPA综合征与严重的长期后遗症无关,并且对类固醇治疗反应良好。一名患有非典型PFAPA的患者接受低剂量类固醇治疗超过1年,在类固醇剂量增加7天后发生了肠穿孔。如果潜在问题需要长期免疫抑制药物治疗,选择西咪替丁而非增加类固醇剂量来解决非典型PFAPA更为明智。
