Anti-glomerular basement membrane disease with IgA nephropathy: A case report

BACKGROUND Anti-glomerular basement membrane(GBM)disease is a rare autoimmune disease manifesting as acute progressive nephritis syndrome with or without varying degrees of pulmonary hemorrhage.Anti-GBM disease coexisting with Immunoglobulin A(IgA)nephropathy is rarer and has different clinical manifestations and prognoses than simple anti-GBM disease.We describe a case of coexistence of these two diseases.CASE SUMMARY A 49-year-old man with hematuria and proteinuria accompanied by a slight elevation of serum creatinine was admitted to our hospital.The pathological results of renal biopsy and the elevated serum anti-GBM antibody titer supported a diagnosis of anti-GBM disease combined with IgA nephropathy.After treatment with corticosteroids and cyclophosphamide,the patient's serum creatinine was relatively stable,and the hematuria and proteinuria moderately improved in the subsequent six months.CONCLUSION Anti-GBM disease coexisting with IgA nephropathy is rare.The clinical manifestations and prognosis are better than those of simple anti-GBM disease.In this case,the patient's condition was improved and his renal function remained relatively stable with corticosteroid and cyclophosphamide treatment.New detection methods to identify whether the crescents in this case were derived from anti-GBM disease or IgA nephropathy are worthy of further exploration.

Management of an Adult with Goodpasture’s Syndrome Following Brain Trauma with Extracorporeal Membrane Oxygenation: A Case Report

A 22-year-old man suffered from acute pulmonary hemorrhage and deteriorated renal function occurred within 3 days after traumatic brain injury.Mechanical ventilation cannot correct his severe hypoxemia,therefore,venoarterial extracorporeal membrane oxygenation(VA-ECMO)support was initiated and finally resolved his hypoxemia.Concomitantly,continuous renal replacement therapy was performed to improve his kidney function.Although no anti-glomerular basement membrane(anti-GBM)antibody was detected in serum,Goodpasture’s syndrome was considered.After treated with methylprednisolone pulse therapy and plasmapheresis,his renal function was significantly improved.ECMO was eventually discontinued after 60 hours of treatment and extubated on day 10.He was discharged home with normal pulmonary and renal functions.

"Triple-positive" renal limited vasculitis presenting with rapidly progressive glomerulonephritis: A case report

Rationale:Coexistence of anti-glomerular basement membrane(anti-GBM)disease with anti-neutrophil cytoplasmic antibody(ANCA)in a case of glomerulonephritis is often identified as a"double-positive"disease.Interestingly,the majority of"double positive"ANCA is myeloperoxidase(MPO)-ANCA and some of the MPO-ANCA positive cases showed intrarenal arteritis,suggesting an ANCA-associated kidney lesion.Proteinase 3-ANCA positive diseases are also rarely reported.Patients positive for all three antibodies,i.e.,triple-positive patients,are extremely rare.Patient's Concern:A 53 year-old female presented with anasarca and oliguria of 2 months'duration.Diagnosis:Pauci-immune type renal limited crescentic glomerulonephritis positive for MPO-ANCA,proteinase 3-ANCA,and anti-GBM antibody(triple-positive).Interventions:Intravenous high dose cyclophosphamide,oral azathioprine,intravenous methylprednisolone,and plasma exchange as per British Health Professionals in Rheumatology Guidelines.Outcomes:After one-month follow-up,anasarca and proteinuria were lessened,serum creatinine was normalized,titers of MPO-ANCA levels were decreased,and anti-GBM antibody levels were normalized.Lessons:Triple-positive renal limited vasculitis is rare and response to combined immunosuppressive therapy and plasma exchange can contribute to successful remission.

Triple hit to the kidney-dual pathological crescentic glomerulonephritis and diffuse proliferative immune complexmediated glomerulonephritis: A case report

BACKGROUND Anti-glomerular basement membrane(GBM)disease is a rare rapidly progressive glomerulonephritis,frequently associated with alveolar hemorrhage in the lungs and involving the kidney by crescentic glomerulonephritis.It has been described in association with other glomerulonephritides[such as anti-neutrophilic antibody(ANCA)-glomerulonephritis,membranous nephropathy,and immunoglobulin(Ig)A nephropathy].CASE SUMMARY Herein we present an unusual case of concurrent anti-GBM disease,ANCAassociated crescentic glomerulonephritis and diffuse proliferative immune complex mediated glomerulonephritis with predominant staining for IgA and C3 by immunofluorescence.The patient is a 46-year-old Caucasian male who presented to the emergency department with acute onset of flank pain and was found to have high serum creatinine levels of 15 mg/dL,proteinuria,and hematuria.He rapidly deteriorated and became anuric.He was found to have high anti-GBM antibodies titers(151 units)and high anti-neutrophil cytoplasmic-ANCA.Despite prompt and early treatment,the patient’s condition worsened,and he succumbed to his illness.CONCLUSION Our case emphasizes the importance of a renal biopsy in anti-GBM disease,even in the presence of positive serum anti-GBM antibodies,to identify other potential causes of rapidly progressive glomerulonephritis.The challenge in treating such cases lies in the different therapy modalities.

Analysis of clinical features and prognosis of anti-glomerular basement membrane antibody positive patients with anti-neutrophil cytoplasmic antibodies

Objective To investigate the characteristics and outcome of glomerulonephritis in patients with both antineutrophil cytoplasmic antibody and anti-glomerular basement membrane antibody.Methods The sera of 23 antiGBM glomerulonephritis patients were collected and were tested for ANCA respectively.Characteristics and outcome of patients with coexisting anti-GBM antibody

双硫仑作用机制及其在治疗抗肾小球基底膜型肾小球肾炎中的研究进展

双硫仑作为一种治疗慢性酒精中毒的药物在临床中广泛使用。近年来,研究者提出了双硫仑治疗癌症的具体机制,如抑制乙醛脱氢酶(acetaldehyde dehydrogenase,ALDH)的活性、提高细胞内活性氧(reactive oxygen species,ROS)的浓度、抑制核因子kappa-B(nuclear factor kappa-B,NF-κB)的活性,促进与核蛋白定位蛋白4(nuclear protein localization protein 4,NPL4)的结合、抑制FROUNT蛋白等,并在多种癌症模型中证明了双硫仑的抗癌活性。抗肾小球基底膜型肾小球肾炎是急进性肾小球肾炎中的一种类型,该病一旦被确诊,就需要第一时间给予治疗,尽量帮助患者缓解症状、改善预后。研究表明,双硫仑可通过抑制C-C趋化因子受体2型/C-C趋化因子受体5型(C-C chemokine receptor type 2/C-C chemokine receptor type 5,CCR-2/CCR-5)和FROUNT蛋白之间的相互作用来抑制巨噬细胞的迁移、聚集、活化来缓解抗肾小球基底膜型肾小球肾炎,这表明双硫仑对该类患者具有潜在的治疗价值。本文简要回顾了双硫仑最新研究中阐明的相关作用分子机制,展望了未来双硫仑作为新的药物治疗抗肾小球基底膜型肾小球肾炎的前景。

2例抗肾小球基底膜病患者的护理

目的总结2例抗肾小球基底膜病患者治疗的护理要点。方法密切观察患者病情,做好用药护理、双膜血浆置换治疗的护理,同时做好患者及家属的心理护理。结果 2例患者经治疗外周血中抗肾小球基底膜抗体明显下降,血肌酐下降,肾脏功能明显改善。结论严密观察肾脏和肺的病变,及时准确地遵医嘱用药,并做好药物疗效和不良反应的观察,积极预防双膜血浆置换治疗的并发症,是抗肾小球基底膜病患者康复的关键。

急进性肾小球肾炎动物模型研究进展

急进性肾小球肾炎根据免疫病理特征分为Ⅰ型抗GBM抗体型、Ⅱ型免疫复合物型和Ⅲ型微量免疫复合物型,代表性的动物模型分别是实验性自体免疫肾小球肾炎、肾毒血清肾炎和实验性自体免疫脉管炎。本文就这些模型的造模方法、免疫机制和应用范围进行综述,以供读者参考。

实验性抗基底膜肾小球肾炎——免疫荧光、光镜和电镜研究

采用自制兔抗大鼠肾免疫血清,制造大鼠抗基底膜肾小球肾炎模型,并进行了重复试验。用免疫荧光技术、光镜和电镜进行观察,前后两批实验结果相同,提示在肾小球基底膜上显示出典型的光滑线型荧光图象,在电镜下肾小球毛细血管丛基底膜呈现局灶性电子透明区而疏松增厚,光镜下主要表现为增生性肾小球肾炎变化,未见新月体形成。实验结果可与人类某些肾炎相比较,对了解人类某些类型肾炎的病因、发病机理、病理变化、临床表现及其防治有一定意义。

抗肾小球基膜肾炎合并糖尿病肾病

中年男性,以持续肉眼血尿伴大量蛋白尿、肾功能减退、血抗肾小球基膜(GBM)抗体阳性起病;肾活检组织学符合新月体肾炎,免疫荧光见IgG沿肾小球毛细血管袢线性沉积,符合抗GBM肾炎,同时亦见肾小球呈结节样改变、肾小管基膜(TBM)增厚、动脉透明变性等,超微结构观察GBM呈均匀一致性增厚,经糖耐量检查确诊糖尿病。该患者最终诊断为抗GBM肾炎合并糖尿病肾病(DN)。

血清抗中性粒细胞胞浆抗体阳性的抗肾小球基膜肾炎的临床与病理特征

目的 :回顾性分析血清抗中性粒细胞胞浆抗体 (ANCA)阳性抗肾小球基膜 (GBM)肾炎的临床和病理特征。 方法 :对解放军肾脏病研究所 1 994年至 2 0 0 2年住院确诊抗GBM肾炎的 2 3例患者进行血清ANCA检测 ,对其中 1 1例ANCA阳性患者在流行病学、临床及病理等方面进行分析 ,并与血清ANCA阴性抗GBM肾炎及ANCA相关性寡免疫复合物型新月体肾炎患者进行比较。 结果 :2 3例抗GBM肾炎患者有 1 1例 (47 8% )同时存在血清ANCA阳性。其中髓过氧化物酶 ANCA(MPO ANCA)阳性者 4例 (36 4% ) ,蛋白酶 3 ANCA(PR3 ANCA)阳性者 1例[9 0 9% ,该例同时合并MPO ANCA及胞浆型ANCA(C ANCA阳性 ) ] ,核周型 (P ANCA)阳性者 3例 (2 7 3 % ) ,C ANCA阳性者 5例 (45 5 % )。血清ANCA阳性和阴性抗GBM肾炎患者在流行病学、临床表现、病理改变及预后等方面无差异 ,二者与ANCA相关性寡免疫复合物型新月体肾炎患者相比 ,在发病年龄、性别比例、少尿 (无尿 )及就诊时终末期肾衰发生率、新月体性质、肾小球硬化、肾间质小血管病变及预后等方面差异显著。血清ANCA阳性和阴性抗GBM肾炎患者对治疗的反应和预后均很差 ,ANCA相关性寡免疫复合物型新月体肾炎患者预后相对较好。 结论 :血清ANCA阳性和阴性的抗GBM新月体肾炎可能为同源性疾病 ,

桃红四物汤对实验性肾炎肾内血小板活化因子、血栓素B_2的影响

实验大鼠均制成大加速型抗肾小球基底膜(GBM)肾炎模型,分为两组:模型组、桃红四物汤组(治疗组)。结果治疗组各期尿蛋白量较模型组减少(P<0.05,P<0.01),第21天时血清肌酐含量较模型组降低(P<0.05),光镜和电镜下肾脏病理改变较模型组为轻,同时,肾皮质内血小板活化因子(PAF)、血栓素 B_2(TXB_2)含量显著较模型组减少(P<0.01)。本实验表明:桃红四物汤治疗该大鼠肾炎有效,其机理是通过减少肾内 PAF、 TXB_2等多条途径。

抗肾小球基膜病合并IgA肾病或膜性肾病的临床病理特征分析

目的:探讨抗肾小球基膜(GBM)病合并IgA肾病(IgAN)或膜性肾病(MN)患者的的临床病理特征及预后特点。方法:选取2004年1月~2015年12月于南京总医院国家肾脏疾病临床医学研究中心经肾活检确定为抗GBM病合并IgAN患者(合并IgAN组)10例,抗GBM病合并MN患者(合并MN组)5例,与60例单纯抗GBM病患者(单纯抗GBM病组)比较,分析三组患者在临床表现、肾活检病理特征及预后的差异。结果:与单纯抗GBM病组相比,合并IgAN组、合并MN组患者出现无尿者较少,蛋白尿和镜下血尿较多,抗GBM抗体滴度较低,但均无统计学差异。单纯抗GBM病组患者肾损伤程度较重,临床表现为急进性肾炎综合征(RPGN)的比例明显增高(P=0.004),高血压比例高(P=0.002),血肌酐峰值最高(P<0.001),且贫血程度重(P<0.001)。单纯抗GBM病组患者总新月体比例高(P=0.008)且包囊壁断裂比例亦高(P=0.005)。单纯抗GBM组患者需连续肾脏替代治疗比例最高(P=0.008)。单纯抗GBM病组患者1年内进展至终末期肾病比例最高(P<0.001)。结论:合并Ig AN或MN的抗GBM病在临床表现、实验室检查、病理指标及预后均不同于单纯抗GBM病。

Goodpasture syndrome and hemorrhage after renal biopsy: A case report

BACKGROUND Goodpasture syndrome(GS) is a rare disease, the morbidity of which is estimated to be 0.5-0.8 per million per year. Hemorrhage is the most serious complication in renal biopsy. Despite the fact that both GS and hemorrhage after renal biopsy are rare, it has not been reported that they are likely to occur in the same patient.CASE SUMMARY A 30-year-old man with diffuse pulmonary hemorrhage and rapid progressive renal function caused by anti-glomerular basement membrane disease presented atypical symptoms without hemoptysis, accompanied by life-threatening hypoxemia. Plasmapheresis was performed, and glucocorticoids and cyclophosphamide were administered. The patient started to show signs of improvement. Percutaneous renal biopsy is an appropriate diagnostic measure that is commonly safe, but this patient experienced hemorrhage after operation,thus necessitating embolization of the renal artery to stop the bleeding. The patient’s condition was improved, and the serum anti-glomerular basement membrane antibody level was 106 AU/m L(normal range: < 24 AU/m L) and slowly decreased. His discharge medications were oral daily prednisone(30 mg)and continued maintenance hemodialysis.CONCLUSION GS is a rare organ-specific autoimmune disease that is invariably ubiquitous in the lung and kidney areas. Renal biopsy is the appropriate procedure for the treatment of GS disease, although it is an invasive measure.

肺出血肾炎综合征4例报告

本文报道经皮肾活检病理证实的４例肺出血肾炎综合征（Ｇｏｏｄｐａｓｔｕｒｅ，ＧＰＳ）患者，并结合文献，就病因、发病机理、病理变化、临床特点、诊断及鉴别诊断等方面进行讨论。提出对拟诊为本病的患者，经纤维友气管镜肺活检和经皮肾活检是确诊本病的重要方法。

HMGB1、TLR4、STAT3在抗肾小球基底膜型肾小球肾炎小鼠模型中的表达及意义

目的探讨高迁移率族蛋白1(HMGB1)、Toll样受体-4(TLR4)、信号转导和转录激活因子3(STAT3)在抗肾小球基底膜型肾小球肾炎小鼠模型中的表达及意义。方法收集30只小鼠,随机分为正常小鼠组(对照组)、抗肾小球基底膜型肾小球肾炎建模组(试验组),每组15只。采用对氨基水杨酸(PAS)染色观察肾小球基底膜变化,实时荧光定量聚合酶链反应(RTPCR)法检测肾组织中的HMGB1、p-STAT3mRNA,采用Western blot法检测肾组织中的HMGB1、TLR4、STAT3、p-STAT3。结果与对照组比较,试验组小鼠肾小球基底膜明显增厚,小鼠肾组织中HMGB1、TLR4、STAT3、p-STAT3及HMGB1mRNA、p-STAT3mRNA的相对表达量均明显高于对照组,差异有统计学意义(P<0.05)。试验组小鼠肾组织中HMGB1与TLR4,TLR4与p-STAT3,HMGB1与p-STAT3,HMGB1mRNA与p-STAT3mRNA的表达水平之间呈正相关(r=0.401,P=0.005;r=0.399,P=0.005;r=0.412,P=0.004;r=0.398,P=0.005)。结论 HMGB1在抗肾小球基底膜型肾小球肾炎小鼠中的致炎作用,可以通过结合其受体TLR4而激活STAT3,从而实现抗肾小球基底膜型肾小球肾炎发生。

苦豆子调节JNK信号通路对抗GBM肾炎大鼠的作用研究

目的:研究苦豆子对抗肾小球基底膜(glomerular basement membrane,GBM)肾炎大鼠的作用及机制研究。方法:30只健康雄性大鼠,随机分为5组,每组6只,分别为对照组、模型组、苦豆子低、中、高剂量组,除对照组外,其余各组采用尾静脉注射给予大鼠兔抗大鼠GBM血清的方法建立大鼠抗GBM肾炎模型,然后根据大鼠体重按照1 g/kg、2 g/kg、4 g/kg灌胃给予大鼠苦豆子提取物,对照组及模型组灌胃给予等量生理盐水,1次/d,连续给药21 d,并于给药第14天和21天测定各组大鼠24 h尿量及尿蛋白量,给药结束后,测定大鼠血浆TNF-α、IL-6及IL-1β水平,血清尿素氮及血肌酐水平,苏木精-伊红染色法对大鼠肾脏进行组织病理学观察,western blot检测大鼠肾脏组织JNK、p-JNK水平,实时定量PCR检测各组大鼠肾脏组织中c-Jun及AP-1 mRNA水平。结果:与模型组比较,苦豆子各剂量组大鼠24 h尿量显著增加(P<0.05),24 h尿蛋白量、血清尿素氮、血肌酐水平、血清尿素氮水平、血肌酐水平及其血浆TNF-α、IL-6及IL-1β水平、肾组织JNK及p-JNK水平、c-Jun及AP-1 mRNA水平均显著降低(P<0.05),大鼠肾组织病理学明显改善。结论:苦豆子能够改善抗GBM肾炎大鼠的疾病状态,其作用机制可能与调节抗GBM肾炎大鼠体内JNK信号通路有关。

感染性心内膜炎后急进性肾炎一例报道并文献复习

目的:探讨感染性心内膜炎后急进性肾炎的临床特点及预后。方法:报道1例感染性心内膜炎后I型急进性肾炎的患者,以'感染性'和'心内膜炎'以及'急进性肾炎'或'新月体肾炎'或'急性肾损害'为检索词在中外文主要数据库检索,筛选出感染性心内膜炎后急进性肾炎(肾脏病理确诊)患者的临床资料进行总结。结果:青年女性患者,RPGN出现在感染性心内膜炎、心脏术后半年,以进行性肾功能减退、抗GBM抗体阳性为特征,病理示新月体肾炎,予激素、免疫抑制剂等治疗,仍需肾脏替代治疗。检索文献,复习12例感染性心内膜炎后急进性肾炎病例,结果显示以中老年多见,肾脏病理示新月体肾炎,积极抗感染、激素等治疗,大多患者可恢复正常肾功能,部分患者仍需肾脏替代治疗甚至死亡。结论:感染性心内膜炎后I型急进性肾炎罕见,但若患者合并肾小球病变,建议肾活检以明确,早期干预、治疗,有利于改善预后。

pCol(24-38)诱导抗肾小球基底膜肾病大鼠模型的建立

目的以含大鼠Ⅳ型胶原α3链的非胶原区[α3(Ⅳ)NC1]的多肽pCol(24-38)作为抗原建立抗肾小球基底膜(GBM)病大鼠模型,研究抗GBM病的发病机制。方法选择雄性WKY大鼠20只(8～10周龄),体重120～150g,随机分为对照组和抗GBM病模型组,每组10只。抗GBM病模型组使用多肽pCol(24-38)作为抗原,对照组使用多肽pCol(38-52)作为抗原,两组均用完全弗氏佐剂乳化后,于大鼠背部皮下三点注射免疫。免疫后每周定时收集24h尿,测尿蛋白含量,所有动物在免疫后49d处死,取血清,采用肌氨酸氧化酶法检测血清肌酐,脲酶法检测尿素氮浓度,并用间接ELISA法检测血清抗pCol(24-38)抗体相对滴度。取肾脏组织,一部分石蜡切片后行PAS染色及免疫组化染色,另一部分经OCT包埋冷冻切片后用直接免疫荧光法检测IgG在肾小球的沉积情况。结果与对照组比较,抗GBM病模型组的24h尿蛋白含量自第4周开始明显升高[(52.27±10.50)mg/24h vs.(4.87±0.64)mg/24h,P<0.001],之后逐渐上升,至第7周,抗GBM病模型组的24h尿蛋白含量仍明显高于对照组[(255.80±9.79)mg/24h vs.(5.78±0.39)mg/24h,P<0.001];抗GBM病模型组血清肌酐水平[(145.3±22.60)μmol/L vs.(36.81±2.21)μmol/L,P<0.001]、尿素氮水平[(26.59±5.01)mmol/L vs.(6.92±0.27)mmol/L,P<0.001]均明显升高;抗GBM病模型组的循环抗pCol(24-38)IgG抗体水平明显高于对照组[(1.59±0.18) vs.(0.09±0.01),P<0.05]。抗GBM病模型组PAS染色可见肾小球硬化,弥漫性新月体形成,免疫组化染色可见肾小球有明显的巨噬细胞浸润,荧光染色可见IgG在GBM呈明显线性沉积;而对照组PAS染色未见异常肾小球,免疫组化染色未见巨噬细胞浸润,荧光染色在GBM上未发现IgG沉积。结论使用多肽pCol(24-38)作为抗原免疫WKY大鼠能成功构建抗GBM病动物模型。该抗原制备方法简单,对于设计新的抗GBM病的治疗策略有重要价值。

Production and Characterization of Recombinant Rat Non-Collagen Domain of α3 Chain of Type IV Collagen α3 (IV) NC1 Antigen

The glomerulonephritis disease is characterized by inflammation of glomeruli or small blood vessels in the kidney that causes kidney diseases. The reason of glomerulonephritis disease is to deposit the anti-GBM auto antibody in the glomerular basement membrane. The type IV collagen is the main component of glomerular basement membrane that has α3 chain of type (IV) collagen of non-collagenous domain which contains N-terminal 7S domain, a triple helical collagenous domain and C-terminal non-collagenous glomerular domain (NC1). The amino terminal of α3 (IV) NC1 that induces the Experimental Autoimmuno Glomerulonephritis (EAG) in rat model has been identified. The recombinant rat α3 (IV) NC1 antigen has nine amino acid spans that are consistent with antibody or T cell epitope that induces in EAG. The research is carried out on the recombinant rat α3 (IV) NC1 production, purification, quantification, and characterization. The circulation of anti-GBM antibody in glomerular basement membrane can be measured by the ELISA assay. In addition, the recombinant rat antigen is secreted in HEK293 cell supernatant that is purified by Anti-FLAG M2 monoclonal IgG antibody affinity column and characterized and quantified by SDS-PAGE gel electrophoresis and Western blotting techniques.