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遗传性周期性发热和周期性发热、口疮、咽炎、腺炎均无:三级儿科中心的未分化周期性发热

Neither hereditary periodic fever nor periodic fever, aphthae, pharingitis, adenitis: Undifferentiated periodic fever in a tertiary pediatric center.

作者信息

De Pauli Silvia, Lega Sara, Pastore Serena, Grasso Domenico Leonardo, Bianco Anna Monica Rosaria, Severini Giovanni Maria, Tommasini Alberto, Taddio Andrea

机构信息

Department of Medicine, Surgery and Health, University of Trieste, Trieste 34142, Italy.

Institute for Maternal and Child Health, IRCCS Burlo Garofolo, Trieste 34137, Italy.

出版信息

World J Clin Pediatr. 2018 Feb 8;7(1):49-55. doi: 10.5409/wjcp.v7.i1.49.

Abstract

AIM

To describe the frequency and clinical characteristics of patients with undifferentiated periodic fever (UPF) and to investigate whether a clinical classification of UPF based on the PRINTO-Eurofever score can help predicting the response to treatment and the outcome at follow-up.

METHODS

Clinical and therapeutic information of patients with recurrent fever who presented at a single pediatric rheumatology center from January 2006 through April 2016 were retrospectively collected. Patients with a clinical suspicion of hereditary periodic fever (HPF) syndrome and patients with clinical picture of periodic fever, aphthae, pharingitis, adenitis (PFAPA) who were refractory to tonsillectomy underwent molecular analysis of five HPF-related genes: (NM_000243.2), (NM_000431.3), (NM_001065.3), (NM_001079821.2), (NM_001277126.1). All patients who had a negative genetic result were defined as UPF and further investigated. PRINTO-Eurofever score for clinical diagnosis of HPF was calculated in all cases.

RESULTS

Of the 221 patients evaluated for periodic fever, twelve subjects with a clinical picture of PFAPA who were refractory to tonsillectomy and 22 subjects with a clinical suspicion of HPF underwent genetic analysis. Twenty-three patients (10.4%) resulted negative and were classified as UPF. The median age at presentation of patients with UPF was 9.5 mo (IQR 4-24). Patients with UPF had a higher frequency of aphthae (52.2% 0%, = 0.0026) and musculoskeletal pain (65.2% 18.2%, = 0.0255) than patients with genetic confirmed HPF. Also, patients with UPF had a higher frequency of aphthous stomatitis (52.2% 10.7%, < 0.0001), musculoskeletal pain (65.2% 8,0%, < 0.0001), and abdominal pain (52.2% 4.8%, < 0.0001) and a lower frequency of pharyngitis (56.6% 81.3%, = 0.0127) compared with typical PFAPA in the same cohort. Twenty-one of 23 patients with UPF (91.3%) received steroids, being effective in 16; 13 (56.2%) were given colchicine, which was effective in 6. Symptoms resolution occurred in 2 patients with UPF at last follow-up. Classification according to the PRINTO-Eurofever score did not correlate with treatment response and prognosis.

CONCLUSION

UPF is not a rare diagnosis among patients with periodic fever. Clinical presentation place UPF half way on a clinical spectrum between PFAPA and HPF. The PRINTO-Eurofever score is not useful to predict clinical outcome and treatment response in these patients.

摘要

目的

描述未分化周期性发热(UPF)患者的发病频率及临床特征,并研究基于PRINTO - Eurofever评分的UPF临床分类是否有助于预测治疗反应及随访结果。

方法

回顾性收集2006年1月至2016年4月在单一儿童风湿病中心就诊的反复发热患者的临床和治疗信息。对临床怀疑遗传性周期性发热(HPF)综合征的患者以及扁桃体切除无效的周期性发热、口腔溃疡、咽炎、腺炎(PFAPA)临床表现患者,进行5个HPF相关基因( (NM_000243.2)、 (NM_000431.3)、 (NM_001065.3)、 (NM_001079821.2)、 (NM_001277126.1))的分子分析。所有基因检测结果为阴性的患者定义为UPF并进一步研究。计算所有病例用于HPF临床诊断的PRINTO - Eurofever评分。

结果

在评估的221例周期性发热患者中,12例扁桃体切除无效的PFAPA临床表现患者和22例临床怀疑HPF的患者接受了基因分析。23例患者(10.4%)检测结果为阴性,被分类为UPF。UPF患者发病时的中位年龄为9.5个月(四分位间距4 - 24)。与基因确诊的HPF患者相比,UPF患者口腔溃疡(52.2%对0%,P = 0.0026)和肌肉骨骼疼痛(65.2%对18.2%,P = 0.0255)的发生率更高。此外,与同一队列中的典型PFAPA相比,UPF患者复发性口疮性口炎(52.2%对10.7%,P < 0.0001)、肌肉骨骼疼痛(65.2%对8.0%,P < 0.0001)和腹痛(52.2%对4.8%,P < 0.0001)的发生率更高,咽炎发生率更低(56.6%对81.3%,P = 0.0127)。23例UPF患者中有21例(91.3%)接受了类固醇治疗,其中16例有效;13例(56.2%)接受了秋水仙碱治疗,其中6例有效。最后随访时2例UPF患者症状缓解。根据PRINTO - Eurofever评分进行的分类与治疗反应和预后无关。

结论

UPF在周期性发热患者中并非罕见诊断。临床表现显示UPF在临床谱上介于PFAPA和HPF之间。PRINTO - Eurofever评分对预测这些患者的临床结局和治疗反应无用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b3d6/5803565/f0bb5370d5ff/WJCP-7-49-g001.jpg

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