Risk factors for intussusception in children with Henoch-Schönlein purpura:A case-control study

BACKGROUND The etiology of Henoch-Schönlein purpura(HSP)with intussusception remains undefined.AIM To investigate the risk factors for intussusception in children with HSP and gastrointestinal(GI)involvement.METHODS Sixty children with HSP and concomitant intussusception admitted to the Beijing Children’s Hospital of Capital Medical University between January 2006 and December 2018 were enrolled in this study.One hundred pediatric patients with HSP and GI involvement but without intussusception,admitted to the same hospital during the same period,were randomly selected as a control group.The baseline clinical characteristics of all patients,including sex,age of onset,duration of disease,clinical manifestations,laboratory test results,and treatments provided,were assessed.Univariate and multiple logistic regression analyses were performed to identify possible risk factors.RESULTS The 60 children in the intussusception group comprised 27 girls(45%)and 33 boys(55%)and the 100 children in the non-intussusception group comprised 62 girls(62%)and 38 boys(38%).The median age of all patients were 6 years and 5 mo.Univariate and multiple regression analyses revealed age at onset,not receiving glucocorticoid therapy within 72 h of emergence of GI symptoms,hematochezia,and D-dimer levels as independent risk factors for intussusception in children with HSP(P<0.05).CONCLUSION The four independent risk factors for intussusception in pediatric HSP with GI involvement would be a reference for early prevention and treatment of this potentially fatal disease.

Severe Henoch-Schonlein purpura with infliximab forulcerative colitis

Infliximab （IFX） is an anti-tumor necrosis factorchimeric antibody that is effective for treatment ofautoimmune disorders such as Crohn＇s disease andulcerative colitis （UC）. IFX is well tolerated with alow incidence of adverse effects such as infections,skin reactions, autoimmunity, and malignancy.Dermatological manifestations can appear as infusionreaction, vasculitis, cutaneous infections, psoriasis,eczema, and skin cancer. Here, we present anunusual case of extensive and sporadic subcutaneousecchymosis in a 69-year-old woman with severe UC,partial colectomy and cecostomy, following her initialdose of IFX. The reaction occurred during infliximabinfusion, and withdrawal of IFX led to gradual alleviationof her symptoms. We concluded that Henoch-Sch？nleinpurpura, a kind of leukocytoclastic vasculitis, mighthave contributed to the development of the bruising.Although the precise mechanisms of the vasculitis arestill controversial, such a case highlights the importanceof subcutaneous adverse effects in the management ofUC with IFX.

Henoch-Schnlein purpura complicating adalimumab therapy for Crohn's disease

Anti-tumour necrosis factor-α(TNF) therapy has revolutionised the management of chronic inflammatory conditions.With ever increasing numbers of patients being treated with these agents,uncommon adverse reactions will inevitably occur more frequently.Cutaneous manifestations are associated with many of these chronic conditions and can complicate anti-TNF therapy in about 20% of cases.Vasculitic complications are rarely associated with anti-TNF therapy.Henoch-Schnlein purpura(HSP),a small vessel vasculitis,has been described following infliximab and etanercept therapy but never with adalimumab,a fully humanized TNF antibody.The risk of such immune-mediated reactions is theoretically less with adalimumab compared to infliximab but can still occur.Here we report the f irst case in the literature of HSP that can be attributed to the use of adalimumab in a 19-year-old male with recalcitrant Crohn's disease.

Effect of intestinal flora from children with Henoch-Sch?nlein purpura on visceral sensitivity, gastrointestinal hormones and cytokines secretion in pseudo-sterile rats

Objective:To investigate the effect of intestinal flora from Henoch-Schönlein purpura(HSP)on visceral sensitivity,gastrointestinal hormones and cytokines in pseudo-sterile rats.Methods:The pseudo-sterile rat model was established.The rats were was given fecal microbiota solutions of children with abdominal HSP and healthy children,respectively.The visceral sensitivity was determined by abdominal withdrawal reflex(AWR)which was induced by rectal balloon distention in all the rats.And serum gastrin(Gas),motilin(MTL),cholecystokinin(CCK),substance P(SP),tumor necrosis factor(TNF)-αand interleukin(IL)-6 levels in rats were measured with ELISA method.Results:The volume of rectum water injection under the score 3 of AWR in the rats administrated with fecal microbiota solution from HSP children(HSP group)was significantly decreased compared with that in the rats administrated with fecal microbiota solution from healthy children(HC group),and there was significant difference between these two groups(P<0.05).The serum Gas,MTL,CCK and SP levels were higher in HSP group than those in HC group.And serum MTL,CCK and SP levels in HSP group were significantly different from those in the HC group.The serum TNF-αandIL-6 levels were higher in HSP group than those in HC group,there was significant difference between these two groups(P<0.05).Conclusion:Intestinal flora from HSP can induce the production of visceral sensitivity,inhibit gastrointestinal hormone secretion and prompt cytokine production.

Effect of Activation of the Ca2+-Permeable Acid-Sensing Ion Channel 1a on Acid-Induced Vascular Endothelial Cell Injury of Henoch-Schönlein Purpura Children

Acidosis in local environment plays a critical role in cell injury. One key mediator of acidosis-induced cell injury is the acid-sensing ion channels (ASICs), particularly ASIC1a. Herein, we investigated the role of ASIC1a in acid-induced vascular endothelial cell injury of Henoch-Schonlein purpura (HSP) children. Acid-induced ASIC1a, Calpain and Calcineurin expression in vascular endothelial cells pretreated with IgA1 isolated from HSP were detected by real time quantitative polymerase chain reaction and western blot methods, respectively. Cell cytotoxicity was measured by interleukin-8 and nitric oxide production with ELISA. The results showed acid-induced ASIC1a, Calpain and Calcineurin expression in cells increased, especially at PH6.5. The cytotoxicity of vascular endothelial cells was increased by extracellular acidosis. Moreover non-specific or specific blockers of ASIC1a, Amiloride and PcTX-1 could remarkably decrease these parameters. These findings show that increased [Ca2+]i, mediated via ASIC1a, might contribute to acid-induced vascular endothelial cell injury of HSP.

过敏性紫癜合并免疫学异常的临床特点及预后

目的 探讨过敏性紫癜(Henoch-Sch?nlein purpura,HSP)合并抗链球菌溶血素O(antistreptolysin O,ASO)升高伴补体下降患者的临床特点及预后。方法 收集2009年1月至2015年6月在温州医科大学附属第二医院住院的HSP患者,根据有无免疫学异常分为四组:观察组(ASO升高合并补体下降)32例,随机选取高ASO组31例,低补体组32例,对照组(无上述免疫学异常)30例。比较四组患者的临床特点及预后。结果 观察组ASO水平高于高ASO组、补体4(complement4,C4)水平低于低补体组,差异有统计学意义(P<0.01)。观察组、高ASO组发病3个月内肾脏累及率高于对照组(P<0.05),低补体组与对照组比较,差异无统计学意义(P>0.05)。3个月内胃肠道及关节累及率和1年肾脏累及率在四组间无统计学差异。观察组中水肿2例,高血压3例,肾功能损害3例,均在2周内恢复正常;肉眼血尿3例,均在40d内消退;镜下血尿及蛋白尿持续中位时间10(4,510)d、10(4,78)d;ASO、补体3(complement3,C3)、C4水平恢复正常中位时间95(60,133)d、14(8,28)d、21(14,39)d;观察组血清白蛋白水平低于其余三组,血清球蛋白、免疫球蛋白(immunoglobulin,Ig)G、IgA水平均高于其余三组(P<0.05)。125例HSP患者中规律随访49例,平均随访时间(108.41±24.58)个月,最长随访155个月,随访期内均未出现慢性肾功能不全。结论 HSP合并ASO升高伴补体下降患者易早期出现肾脏累及,更易出现IgA、IgG升高及低白蛋白血症,补体均在100d内恢复正常,长期随访无一例出现慢性肾功能不全。

高原地区不同类型过敏性紫癜藏族患者发病的相关危险因素

目的:分析高原地区不同类型过敏性紫癜(Henoch-Schonlein purpura,HSP)藏族患者发病的相关危险因素,为高原地区正确识别过敏性紫癜高危患者提供参考。方法:选择2014年4月至2022年3月西藏自治区人民医院风湿免疫血液内科收治的304例藏族HSP患者的病例资料进行回顾性分析,收集患者性别、年龄、过敏史、家族史、实验室指标[血红蛋白、血小板计数、嗜酸性粒细胞、C反应蛋白(C-reactive protein,CRP)、白蛋白、免疫球蛋白G、免疫球蛋白A、补体C3、补体C4和红细胞沉降率(erythrocyte sedimentation rate,ESR)]等数据,采用单因素和多因素Logistic回归分析不同类型过敏性紫癜藏族患者发病的危险因素。结果:肾型HSP患者表现出较高的IgA[(9.2±1.7)g/L vs.(6.4±2.4)g/L,P=0.015]、较低的补体C3[(203.3±21.6)mg/dL vs.(301.1±19.5)mg/dL,P=0.043]和补体C4[(33.5±2.3)mg/dL vs.(53.0±7.2)mg/dL,P=0.032],腹型HSP患者表现出较低的血红蛋白[(119.6±19.6)g/L vs.(146.6±47.3)g/L,P=0.038]和血浆白蛋白[24.8(22.1,33.9)g/L vs.32.6(24.6,35.1)g/L,P=0.045],关节型HSP患者表现出更高的CRP[13.5(0.2,20.6)g/L vs.7.5(0.1,15.2)g/L,P=0.036]和ESR[24(5,40)mm/h vs.15(4,30)mm/h,P=0.049]。IgA升高、补体C4减低是肾型HSP的危险因素,贫血、血浆白蛋白降低是腹型HSP的危险因素,CRP升高是关节型HSP的危险因素。结论:高原地区不同类型的HSP临床特点存在差异,对于高IgA血症、低补体C4、贫血、低白蛋白血症、CRP明显升高的患者应高度警惕,给予早期有效干预可以提高临床疗效,避免病情向重症发展,改善预后。

Henoch-Schönlein purpura nephritis in children:incidence,pathogenesis and management

Background:Henoch-Schönlein purpura(HSP)is one of the most common vasculitides in children.It is manifested by skin purpura,arthritis,abdominal pain,renal involvement,etc.Typically,HSP is considered to be self-limiting,although renal involvement(HSP purpura nephritis,HSPN)is the principal cause of morbidity from this disease.For this reason,it is important to clarify the mechanism of onset and clinical manifestations of HSPN and to ascertain the most appropriate treatment for HSPN.In this article,we review the updated pathophysiology and treatment strategies for HSPN.Data sources:We searched databases including PubMed,Elsevier and Wanfang for the folowing key words:Henoch-Schönlein purpura,nephritis,mechanism and treatment,and we selected those publications written in English that we judged to be relevant to the topic of this review.Results:Based on the data present in the literature,we reviewed the following topics:1)the possible pathogenesis of HSPN:several studies suggest that immunoglobulin A immune complexes deposit in the mesangium and induce renal injury;2)multiple-drug treatment for HSPN:although there have been few evidence-based treatment strategies for HSPN,several studies have suggested that immunosuppressive drugs and multiple drug combination therapy were effective in ameliorating proteinuria and histological severity.Conclusions:HSPN is a severe disease of childhood.To better understand this disease,detailed investigations into the pathogenesis of HSPN and prospective randomized controlled treatment studies on children with severe HSPN are needed.

Clinicopathological features and prognosis of membranoproliferative-like Henoch-Schönlein purpura nephritis in children

Background: The aim of this retrospective study was to defi ne the clinical manifestations, pathological features and prognosis of children with membranoproliferative-like Henoch-Schönlein purpura nephritis (HSPN), representing International Study of Kidney Disease in Children (ISKDC) grade VI. Methods: Among 245 patients with HSPN treated in our hospital between 2008 and 2010, nine patients (3.7%) were diagnosed with HSPN of ISKDC grade VI (males=5, females=4, age: 9.5±2.03 years, mean±SD). The clinical features, laboratory and pathologicalfi ndings, treatment and outcome of the 9 patients were retrospectively analyzed. Results: Of the 9 patients, 7 (78%) presented with hematuria and nephrotic syndrome, and were treated with steroids (oral prednisone or intravenous methylprednisolone pulse therapy) and immunosuppressants (oral tripterygium glycosides or intravenous cyclophosphamide pulse therapy). One (11%) patient had hematuria and nephrotic range proteinuria (>50 mg/kg per 24 hours) and was treated with oral prednisone and tripterygium glycosides. Another (11%) patient presented with hematuria and moderate proteinuria (25-50 mg/kg per 24 hours) and was treated with oral tripterygium glycoside only. Histopathological examination showed diffuse glomerular mesangial and endocapillary proliferation, mesangial interposition, double-contour formation, podocyte hypertrophy, shedding, and cytoplasmic absorption droplets. The percentages of glomeruli with small cellular crescents varied from 4%-25% in 6 of 9 patients. Follow-up for 2 to 4 years showed excellent recovery in all patients. Conclusions: The main clinical feature of ISKDC grade VI HSPN in children is a nephrotic syndrome with hematuria. The excellent prognosis of the disease was probably related to early diagnosis and treatment with steroids and/or immunosuppressants, and mild degree of glomerulosclerosis and tubulointerstitial damage.

过敏性紫癜患儿肠道菌群结构及多样性研究

目的探讨过敏性紫癜(HSP)患儿的肠道菌群结构及多样性变化和粪便菌群与黏膜菌群结构及多样性的差异。方法收集47例过敏性紫癜患儿粪便样本和其中7例腹型患儿的结肠黏膜样本,以11例健康儿童粪便样本为对照,采用试剂盒提取法提取样本DNA并进行高通量测序,对测序结果进行生物学信息分析。结果 HSP患儿与健康儿童粪便菌群存在结构差异,在门水平两组均以厚壁菌门(47.10%、57.75%),变形菌门(23.04%、10.13%),拟杆菌门(22.81%、21.74%)为主要优势菌群,在科水平,均以肠杆菌科(17.60%、8.72%)、拟杆菌科(18.90%、21.65%)、瘤胃菌科(16.44%、28.93%)、毛螺菌科(11.55%、10.74%)有较高的丰度。HSP患儿粪便菌群中变形菌门、欧文氏菌属(从目到属)、拟杆菌属-uniformis种、巨单胞菌属、肠球菌属(从科到属)丰度高于对照组健康儿童,而双歧杆菌属(从目到属)、链球菌属(从目到属)、普拉梭菌种(从科到种)丰度低于对照组健康儿童。腹型患儿粪便菌群多样性高于黏膜菌群;在门水平,粪便菌群以厚壁菌门(53.64%)、变形菌门(33.65%)、拟杆菌门(9.24%)丰度较高,黏膜菌群以变形菌门(88.13%)丰度最高,在科水平,粪便菌群以肠杆菌科(27.18%)、瘤胃菌科(15.58%)、毛螺菌科(12.31%)为优势菌科,黏膜菌群以肠杆菌科(87.19%)为优势菌科;粪便菌群以双歧杆菌属(从门到属)、链球菌属(从门到属)、动性球菌科(从门到科)、丹毒丝菌科(从门到科)、梭菌科(从门到科)、瘤胃菌科(从门到科)、毛螺菌科(从门到科)为主要特征差异细菌种类,结肠黏膜菌群以欧文氏菌属(从门到属)为主要特征差异细菌种类。结论 HSP患儿粪便菌群病原菌或机会致病菌增多而有益菌减少,腹型HSP患儿黏膜菌群与粪便菌群存在结构和多样性差异。

过敏性紫癜肾炎患儿血清IL-16、IL-18、IGF-1及IGFBP-3水平变化及临床意义

目的探究过敏性紫癜肾炎患儿血清白细胞介素-16(IL-16)、白细胞介素-18(IL-18)、胰岛素一号增长因子(IGF-1)及胰岛素样生长因子结合蛋白-3(IGFBP-3)水平变化及临床意义。方法选取2016年1月至2019年1月西安市中心医院儿科收治的过敏性紫癜患儿(HSP组)38例及过敏性紫癜性肾炎患儿(HSPN组)46例作为研究对象,以同期在我院体检的40例健康儿童作为对照组。其中HSPN组患儿按照国际儿童肾病学会病理分级标准分为Ⅰ级、Ⅱ级、Ⅲ级、Ⅳ级4个亚组。比较各大组受检者的血清IL-16、IL-18、IGF-1及IGFBP-3水平,并分析肾炎患儿IL-16、IL-18、IGF-1、IGFBP-3水平与病理分级的相关性。结果HSPN组患儿的血清IL-16、IL-18、IGF-1、IGFBP-3水平分别为(134.22±26.82)ng/L、(263.5±36.15)ng/L、(0.95±0.51)ng/L、(0.86±0.50)ng/L,明显高于HSP组的(106.63±18.19)ng/L、(190.4±32.92)ng/L、(0.64±0.49)ng/L、(0.62±0.38)ng/L,而HSP组患儿的血清IL-16、IL-18、IGF-1、IGFBP-3水平明显高于对照组的(64.85±13.38)ng/L、(102.3±25.34)ng/L、(0.31±0.19)ng/L、(0.43±0.23)ng/L,差异均有统计学意义(P<0.05);肾炎Ⅳ级、Ⅲ级、Ⅱ级、Ⅰ级患儿血清IL-16、IL-18、IGF-1、IGFBP-3水平分别为(154.22±26.82)ng/L、(279.5±10.28)ng/L、(1.31±0.26)ng/L、(1.47±0.36)ng/L;(117.27±8.20)ng/L、(210.45±10.92)ng/L、(0.98±0.12)ng/L、(0.87±0.24)ng/L;(92.14±6.54)ng/L、(160.46±8.49)ng/L、(0.84±0.17)ng/L、(0.69±0.23)ng/L;(67.36±4.38)ng/L、(105.34±6.33)ng/L、(0.39±0.02)ng/L、(0.48±0.05)ng/L,且肾炎Ⅳ级患者IL-16、IL-18、IGF-1、IGFBP-3水平明显高于肾炎Ⅲ级,肾炎Ⅲ级明显高于肾炎Ⅱ级,肾炎Ⅱ级明显高于肾炎Ⅰ级,差异均有统计学意义(P<0.05);相关性分析结果显示,肾炎患儿血清IL-16、IL-18、IGF-1、IGFBP-3水平与病理分级呈正相关(r=0.946,、0.949、0.833、0.804,P<0.05)。结论HSPN患儿血清IL-16、IL-18、IGF-1及IGFBP-3水平均上升,并随着肾脏损伤程度的加重呈上升趋势,可作为预测早期HSPN的参考指标。

过敏性紫癜患儿肠道菌群对伪无菌大鼠内脏敏感性、胃肠激素和细胞因子水平的影响

目的:探讨过敏性紫癜(henoch-Sch nlein purpura,HSP)患儿肠道菌群对伪无菌大鼠内脏敏感性,胃肠激素和细胞因子分泌的影响。方法:建立伪无菌大鼠模型,收集HSP患儿及健康儿童粪便制备粪菌液,分别灌胃大鼠,结肠扩张实验测定大鼠AWR评分,ELISA法测定大鼠血清中胃泌素(Gas)、胃动素(MTL)、胆囊收缩素(CCK)、P物质(SP)及肿瘤坏死因子(TNF)-α、白介素(IL)-6水平。结果:HSP患儿粪菌植入的大鼠(HSP组)其腹部退缩反射(AWR)评分3分时直肠注水量较健康儿童粪菌植入大鼠(health control,HC组)明显降低,差异具有统计学意义(P<0.05);HSP组大鼠血清中MTL、CCK、SPS水平较HC组明显降低,TNF-α,IL-6水平较HC组明显升高,差异具有统计学意义(P<0.05)。结论:HSP患儿肠道菌群可以促进肠道敏感性产生,抑制胃肠激素的分泌,促进细胞因子的产生。

MEFV基因突变与儿童过敏性紫癜遗传易感性的Meta分析

目的探讨MEFV基因突变与过敏性紫癜(HSP)的相关性。方法计算机检索Pub Med、Web of Science、Medline、Cochrane Library、中国期刊全文数据库(CNKI)、万方数据库,检索从建库至2015年12月31日公开发表的关于M EFV基因突变与HSP相关性的文献,使用Rev Man 5.0软件进行Meta分析。结果最终纳入6篇英文文献,累计总病例数433例,其中MEFV基因突变136例,Meta分析结果显示合并的MEFV基因突变率为0.3(95%CI:0.23,0.37);3个亚组(关节炎组、消化道症状组、肾脏损害组)每组中MEFV基因突变与非突变比较均P>0.05,提示MEFV基因突变与临床症状无显著性差异。结论 MEFV基因突变可能是儿童HSP遗传易感因素,但在临床表现方面MEFV基因突变与非突变无明显的区别。

儿童紫癜性肾炎的危险因素研究

目的探讨儿童紫癜性肾炎(HSPN)的危险因素。方法收集2013-01-01~2017-12-31该院住院的过敏性紫癜(HSP)106例患儿的临床资料和相关实验室检查结果。将这些患儿分为HSPN组和非紫癜性肾炎(HSPWN)组,采用病例对照研究设计方案比较两组患儿的HSPN相关暴露因素。结果106例患儿中男66例,女40例,中位年龄7岁。根据2009年中华医学会儿科学会肾脏病学组制定并发布的《紫癜性肾炎的诊治循证指南(试行)》中的HSPN诊断标准分为HSPN组39例和HSPWN组67例。HSPN发生率为36.79%,其中男24例,女15例;中位年龄9.50岁。HSPN组总胆固醇、肌酐、尿酸、胱抑素C水平显著高于HSPWN组(P<0.05),而内生肌酐清除率(Ccr)显著低于HSPWN组(P<0.05)。多因素Logistic回归分析发现总胆固醇是HSPN的危险因素(OR=1.558,P=0.014)。结论总胆固醇水平升高是儿童HSPN的危险因素。

Heat shock protein 70-2 and tumor necrosis factor-α gene polymorphisms in Chinese children with Henoch- Schönlein purpura

Background:Henoch-Schönlein purpura(HSP)or IgAassociated vasculitis is related to immune disturbances.Polymorphisms of the heat shock protein 70-2 gene(HSP70-2)and the tumor necrosis factor-αgene(TNF-α)are known to be associated with immune diseases.The purpose of this study was to investigate the likely association of HSP70-2(+1267A/G)and TNF-α(+308A/G)gene polymorphisms with HSP in children.Methods:The polymerase chain reaction restriction fragment length polymorphism method was used to detect the HSP70-2 and TNF-αpolymorphisms in 205 cases of children with HSP and 53 controls;and the association of these polymorphisms with HSP and HSP nephritis(HSPN)was analyzed.Results:The G/G genotypic frequencies at the+1267A/G position of HSP70-2 in the HSP group(22.9%)were signifi cantly higher than those in the healthy control group(9.4%)(χ^(2)=4.764,P<0.05).The frequencies of the A/A,A/G and G/G genotypes of HSP70-2 in patients in the nephritis-free group and the HSPN group showed no statistically significant difference.The A/A genotype frequency at the+308G/A position of TNF-αin the HSP group was 8.3%,which was higher than that in the control group(χ^(2)=6.447,P<0.05).The A allele frequency of TNF-αin the HSP group was higher than that in the control group,with a statistically significant difference(χ^(2)=7.241,P<0.05).Conclusions:The HSP70-2(+1267A/G)and TNF-α(+308G/A)gene polymorphisms were associated with HSP in children.The G/G homozygosity of HSP70-2 and the A/A homozygosity of TNF-αmay be genetic predisposing factors for HSP.

兒童過敏性紫癜50例臨床分析

目的瞭解本地區兒童過敏性紫癜的臨床特徵。方法對50例過敏性紫癜住院患兒臨床資料、隨訪情況進行回顧性分析。結果1.平均發病年齡(6.0±2.7)歲,80%患兒於秋冬季節發病,44%患兒有明確誘因,以上呼吸道感染為主。2.所有患兒均有典型皮膚紫癜,分佈於下肢、臀部,94%患兒以皮膚紫癜首發,少數以關節及胃腸道為首發症狀後出疹。關節及胃腸道症狀發生率分別為38%和32%。紫癜性腎炎發生率為8%,臨床上主要表現為鏡下血尿和微量白蛋白尿。3.伴有腹痛或關節痛的患兒早期激素使用率為88%,未發現腸套疊、腸梗阻及腸穿孔等嚴重胃腸道併發症。結論過敏性紫癜為兒童常見血管炎,有其本身臨床特徵及發病規律。

Three-Month-Induction Therapy with Prednisone and Mycophenolate Followed by Maintenance Therapy with Mycophenolate Alone for 2 Years: An Effective and Safe Autoimmune Treatment for Triggering Factors Adults with Acute Non-Crescentic Nephritis Associated with Henoch-Schönlein Purpura

Background: Henoch-Schönlein purpura (HSP) is an acute systemic disorder characterized by IgA associated vasculitis. The available data indicate an inherited predisposition to disease with triggering autoimmune phenomena. Hence, we evaluated prospectively the role of a new autoimmune regimen in treatment of its severe nephrotic/nephritic flares associated with non-crescentic nephritis in adult patients. Patients and methods: The regimen consisted of an initial induction phase of 3-month Prednisone and Mycophenolate followed by a maintenance phase of Mycophenolate alone for 2 years. Results: They were satisfactory with complete remission in 5 of 7 patients and partial in 2. Creatinine clearance was normalized in patients with complete remission and remained stable in the partially-responsive ones. Conclusion: Our study has shown the short- and long-term safety and efficacy of such autoimmune regimen directed towards the autoimmune triggering factors in severe forms of non-crescentic HSP.

基于“伏邪学说”探析国医大师王琦“脱敏消癜汤”的组方规律

过敏性紫癜(HSP)是一种病程长易反复发作、迁延难愈的血管变态反应性疾病,属于中医“肌衄”“斑毒”“葡萄疫”范畴。该病的发病特点与中医“伏邪致病”病机基本一致,中国工程院院士、国医大师王琦教授“辨西医之名,融中医之论”,认为过敏体质是HSP发生背景和土壤,临床上采用“辨体-辨病-辨证”的诊疗模式和“主病主方”的思路自拟“脱敏消癜汤”,临床卓有成效。故文章从伏邪学说角度探析“脱敏消癜汤”的组方规律,为临床防治HSP提供参考。

血液净化与丙种球蛋白治疗儿童重症过敏性紫癜的研究进展

过敏性紫癜(Henoch-Schönlein purpura,HSP)是儿童时期常见的小血管炎症,绝大多数预后良好。对于重症HSP,由于患儿体内存在过多的炎症因子,机体损伤持续存在,激素治疗很难在短期内改善症状。近年研究发现丙种球蛋白或血液净化联合激素治疗能更加快速地缓解临床症状,常用的血液净化模式为血浆置换及血液灌流。该文旨在阐述丙种球蛋白及血液净化治疗重症HSP的现状。

Acute hemorrhagic edema of infancy: the experience of a large tertiary pediatric center in Israel

Background:Acute hemorrhagic edema of infancy (AHEI) is a rare leukocytoclastic vasculitis of the small vessels occurring at a young age and considered as a benign self-limited disease.Due to its low prevalence,there are limited data on the presentation and complications of this disease.Methods:All computerized files of children who were hospitalized at a tertiary pediatric center due to AHEI over a 10 year period were reviewed.Clinical,laboratory and histopathological data were collected.Results:Twenty-six patients were included in our study,accounting for 0.7 cases per 1000 admissions of children aged 2 years or less.Mean age was 12.9 months.More than two thirds of the children had preceding symptoms compatible with a viral infection.Upon admission,all patients presented with typical findings of a rash and edema.Edema was most profound over the lower extremities (73%).Concomitant viral or bacterial infections were found in six children.Skin biopsy was performed in six patients revealing leukocytoclastic vasculitis.Thirteen children (50%) had systemic involvement including joint involvement (n=9),gastrointestinal hemorrhage (n=4),microscopic hematuria (n=1) and compartment syndrome of the limb (n=1).The latter was diagnosed in a patient with familial Mediterranean fever.Conclusions:Our largest data series highlighted what is known regarding clinical and histological findings in children with AHEI.However,contrary to what was previously reported,we found a higher rate of systemic involvement.Although AHEI is a rare entity,pediatricians should be familiar with its presentation,management and our reported complications.