Dynamic gut microbiome-metabolome in cationic bovine serum albumin induced experimental immune-complex glomerulonephritis and effect of losartan and mycophenolate mofetil on microbiota modulation

Dynamic changes in gut dysbiosis and metabolomic dysregulation are associated with immune-complex glomerulonephritis(ICGN).However,an in-depth study on this topic is currently lacking.Herein,we report an ICGN model to address this gap.ICGN was induced via the intravenous injection of cationized bovine serum albumin(c-BSA)into Sprague-Dawley(SD)rats for two weeks,after which mycophenolate mofetil(MMF)and losartan were administered orally.Two and six weeks after ICGN establishment,fecal samples were collected and 16S ribosomal DNA(rDNA)sequencing and untargeted metabolomic were conducted.Fecal microbiota transplantation(FMT)was conducted to determine whether gut normali-zation caused by MMF and losartan contributed to their renal protective effects.A gradual decline in microbial diversity and richness was accompanied by a loss of renal function.Approximately 18 genera were found to have significantly different relative abundances between the early and later stages,and Marvinbryantia and Allobaculum were markedly upregulated in both stages.Untargeted metabolomics indicated that the tryptophan metabolism was enhanced in ICGN,characterized by the overproduction of indole and kynurenic acid,while the serotonin pathway was reduced.Administration of losartan and MMF ameliorated microbial dysbiosis and reduced the accumulation of indoxyl conjugates in feces.FMT using feces from animals administered MMF and losartan improved gut dysbiosis by decreasing the Firmicutes/Bacteroidetes(F/B)ratio but did not improve renal function.These findings indicate that ICGN induces serous gut dysbiosis,wherein an altered tryptophan metabolism may contribute to its pro-gression.MMF and losartan significantly reversed the gut microbial and metabolomic dysbiosis,which partially contributed to their renoprotective effects.

Infection related membranoproliferative glomerulonephritis secondary to anaplasmosis:A case

BACKGROUND Anaplasmosis is a tick-borne disease with a range of clinical manifestations,from a flu-like illness with fever and myalgias to a severe systemic disease with multisystem organ failure.Although renal involvement is not a common presentation,there have been few cases reporting acute kidney injury from Anaplasmosis.CASE SUMMARY We present a 55-year-old female with anaplasmosis who developed acute kidney injury due to membranoproliferative glomerulonephritis(MPGN).The patient originally presented with cough and shortness of breath.She was admitted to the hospital with a diagnosis of community acquired pneumonia and received antibiotics.During the hospital course she developed severe acute renal failure.Initial serological work up didn’t provide any conclusive diagnosis.Hence,she underwent kidney biopsy which showed MPGN pattern suggesting autoimmune,multiple myeloma or infectious etiology.Extensive work up was undertaken which was negative for autoimmune diseases,vasculitis panel,paraproteinemias but tested positive for IgG anaplasma with high titers indicating Anaplasmosis.CONCLUSION Our case shows a unique presentation of severe acute renal failure from MPGN from tick borne illness.MPGN is usually seen with autoimmune diseases,hepatitis C virus infections,paraproteinemias.Hence,we suggest that tick borne illness should also be considered when evaluating acute renal failure cases in tick borne prevalent regions.

Reclassification of membranoproliferative glomerulonephritis:Identification of a new GN:C3GN

This review revises the reclassification of the mem-branoproliferative glomerulonephritis （MPGN） after the consensus conference that by 2015 reclassified all the glomerulonephritis basing on etiology and patho-genesis, instead of the histomorphological aspects. After reclassification, two types of MPGN are to date recognized： The immunocomplexes mediated MPGN and the complement mediated MPGN. The latter type is more extensively described in the review either because several of these entities are completely new or because the improved knowledge of the complement cascade allowed for new diagnostic and therapeutic approaches. Overall the complement mediated MPGN are related to acquired or genetic cause. The presence of circulating auto antibodies is the principal acquired cause. Genetic wide association studies and family studies allowed to recognize genetic mutations of different types as causes of the complement dysregulation. The complement cascade is a complex phenomenon and activating factors and regulating factors should be distinguished. Genetic mutations causing abnormalities either in activating or in regulating factors have been described. The diagnosis of the complement mediated MPGN requires a complete study of all these different complement factors. As a consequence, new therapeutic approaches are becoming available. Indeed, in addition to a nonspecifc treatment and to the immunosuppression that has the aim to block the auto antibodies production, the specific inhibition of complement activation is relatively new and may act either blocking the C5 convertase or the C3 convertase. The drugs acting on C3 convertase are still in different phases of clinical development and might represent drugs for the future. Overall the authors consider that one of the principal problems in fnding new types of drugs are both the rarity of the disease and the consequent poor interest in the marketing and the lack of large international cooperative studies.

Differential Treatment for Membranoproliferative Glomerulonephritis with TCM Prescriptions Plus Triptoryph Tablets A Report of 30 Cases

Membranoproliferative glomerulonephritis is aglomerulopathy,which accounts for about 30% of thechronic glomerulonephritis in adults.TCMmedication with addition of triptoryph tablets(Tripterygium Wilfordii polyglycosidium) on thebasis of syndrome differentiation had yieldedsatisfactory results in 30 cases of this disease treatedfrom Jan 1998 to Aug 2002.A report follows.

Rituximab therapy for primary glomerulonephritis: Report on two cases

The evidence in the medical literature on the efficacy and safety of rituximab therapy for primary glomerulonephritis is limited and controversial. We describe two male Caucasian patients with rapidly progressive kidney failure due to primary proliferative glomerulonephritis. Both of them received high-dose intravenous corticosteroids and oral cyclophosphamide with limited benefit. The first patient(hepatitis C virus-negative mixed cryoglobulinemia) underwent plasma-exchange with intravenous immunoglobulins; he showed significant benefit on kidney function(he became dialysis independent with serum creatinine going back to 1.6 mg/d L) after one rituximab pulse even if urinary abnormalities were still present. No improvement in renal function or urinary changes occurred in the second patient. Both these individuals developed sepsis over the follow-up, the first patient died two months after rituximab therapy. This report is in keeping with the occurrence of severe infections after rituximab therapy in patients with renal impairment at baseline and concomitant high-dose steroids.

强的松联合环磷酰胺治疗单克隆IgG3κ沉积的增生性肾小球肾炎1例

目的研究单克隆免疫球蛋白G沉积的增生性肾小球肾炎(PGNMID)的早期诊断及治疗。方法分析复旦大学附属中山医院青浦分院1例66岁单克隆免疫球蛋白G3κ沉积的增生性肾小球肾炎女性从2021年8月至2022年10月的临床资料,病人4年前因尿中泡沫增多就诊行肾活检提示膜增生性肾小球肾炎。既往长期口服黄芪颗粒及血管紧张素受体拮抗剂(ARBs)保守治疗,随访肾功能缓慢进展。2021年8月病人因大量蛋白尿及水肿就诊于复旦大学附属中山医院青浦分院,重复肾穿刺,肾脏病理检查提示膜增生性肾小球肾炎,结合免疫荧光及免疫组化结果,考虑单克隆免疫球蛋白G3κ(IgG3κ)沉积的增生性肾小球肾炎,免疫固定电泳及血清蛋白电泳阴性,故诊断为PGNMID-IgG3κ型。治疗方案选择强的松联合环磷酰胺(CTX),治疗5个月。结果病人疾病完全缓解,随访14个月疾病无复发。血白蛋白从治疗前的21 g/L升高至41 g/L,血肌酐从100μmol/L下降至71μmol/L,24小时蛋白尿从6645 mg/24 h下降至100 mg/24 h,尿白蛋白肌酐比从4882.3 mg/g下降至130.5 mg/g,尿蛋白肌酐比从6604.8 mg/gcr至242.6 mg/gcr。结论PGNMID发病机制目前仍未完全了解。当怀疑该病时,即使免疫固定电泳等阴性,也需行IgG亚型及轻链染色检查。早期诊断及治疗对疾病的预后极为重要;强的松联合CTX治疗可能是PGNMID-IgG3κ病人一种较好的治疗方案,能够改善病人预后,延长其生存期。

C3肾小球病和膜增生性肾小球肾炎

C3肾小球病(C3 glomerulopathy,C3G)是一个基于临床、病理和病因的诊断术语,指一类主要继发于血浆补体替代途径和肾小球微环境失调引起的疾病谱。膜增生性肾小球肾炎(membranoproliferative glomerulonephritis,MPGN)是肾活检光镜下病理改变之一而非某一特种疾病或诊断术语。C3G的光镜病理类型主要为MPGN,是MPGN的主要原发病因之一。本文就C3G和MPGN的病因、临床表现、病理特征等进行综述,特别强调的是C3G可以作为临床第一诊断或主要诊断,而MPGN仅仅是一种光镜病理表现而非某种特定疾病,不建议作为临床第一诊断或主要诊断,在肾活检提示为MPGN病变时,应积极寻求其原发病因以明确诊断。

基于尿液代谢组学和生物网络分析整合策略研究益肾固络合剂治疗慢性肾小球肾炎作用机制

目的:基于尿液代谢组学和生物网络分析整合策略研究益肾固络合剂治疗慢性肾小球肾炎(CGN)的关键代谢途径和潜在靶点。方法:建立阳离子化牛血清白蛋白(C-BSA)诱导的CGN大鼠模型,采用超高效液相色谱-质谱联用(UPLC-MS)代谢组学筛选益肾固络合剂治疗CGN的尿液内源性代谢标志物和代谢途径。整合生物网络分析工具对益肾固络合剂调节的生物标志物进行网络分析,挖掘益肾固络合剂治疗CGN的生物功能和潜在靶点。结果:基于尿液代谢组学技术筛选出花生四烯酸等20个益肾固络合剂治疗CGN的内源性代谢标志物。对益肾固络合剂调控的关键内源性代谢物生物网络分析结果表明,花生四烯酸代谢是益肾固络合剂发挥治疗CGN作用的潜在关键通路,其代谢途径上的细胞色素P4504A11(CYP4A11)等10个靶点为益肾固络合剂治疗CGN的潜在靶点。结论:本研究初步揭示了益肾固络合剂治疗CGN的作用机制,为益肾固络合剂临床推广应用提供科学理论依据。

免疫性全血细胞减少症合并膜增生性肾小球肾炎

11岁男性患儿,既往有免疫性全血细胞减少症、继发性血友病、脑梗死病史。肾脏损害表现为大量蛋白尿伴少量镜下血尿,肾活检病理提示肾小球膜增生性病变,偶见血栓性微血管病(TMA)样病变,电镜下系膜区和内皮下大量微管状超微结构,直径8~12 nm,最终诊断为肾小球膜增生性病变(考虑与免疫复合物及TMA病变相关)。

原发性慢性肾脏病患者脂质代谢及凝血功能变化及临床意义

目的:研究原发性慢性肾脏病(CKD)患者脂质代谢及凝血功能变化及临床意义。方法:选取2020年1月至2022年4月我院接收的CKD患者120例为样本进行横断面研究,入院后测量尿素氮(blood urea nitrogen,BUN)、血肌酐(serum creatinine,Scr)、总胆固醇(total cholesterol,TC)、三酰甘油(triglycerides,TG)、高密度脂蛋白(high-density lipoprotein cholesterol,HDL-C),低密度脂蛋白(low-density lipoprotein cholesterol,LDL-C)、载脂蛋白A1(apolipoprotein A1,apoA1)及apoB等血脂代谢指标;纤维蛋白原(fibrinogen,FIB)、D二聚体(D-dimer,D-D)、活化部分凝血酶原时间(activited partial thomboplastin time,APTT)、纤维蛋白原降解产物(fibrinogen degradation products,FDP)、凝血酶凝结时间(thrombin time,TT)、凝血酶原时间(prothombin time,PT)以及国际化标准比值(international normalized ratio,INR)等凝血功能指标。按照是否合并心血管疾病(cardiovascular disease,CVD)将患者分为CVD组和对照组,比较两组各项指标并建立Logistic回归模型,然后进行校准并分析该模型对CVD患病风险的预测价值。结果:120例CKD患者中合并CVD者34例(28.33%),CVD组CKD分期5期患者占比、BUN、Scr、TC、LDL-C以及FIB均高于对照组,HDL-C低于对照组,差异有统计学意义(P<0.05);CKD分期与脂质代谢指标HDL-C、apoA1和apoB均呈负相关性(P<0.05),与凝血功能指标PT、FIB、D-D和INR均呈正相关性(P<0.05);二元Logistic回归分析显示TC、HDL-C和FIB与CKD患者并发CVD存在密切联系(P<0.05),CKD患者并发CVD风险的预测模型为logit(P)=-2.864+0.571×(TC)-2.748×(HDL-C)+0.620×(FIB),用于预测CKD患者并发CVD的AUC为0.807(95%CI:0.725~0.873),敏感度和特异度分别为82.35%和69.77%。结论:原发性CKD患者脂质代谢和凝血功能存在明显异常,且与CKD分期存在明显相关性,采用TC、HDL-C和FIB等指标建立Logistic回归模型预测CKD患者CVD并发风险具有良好参考价值。

Hepatitis C virus associated glomerulopathies

Hepatitis C virus (HCV) infection is a systemic disorder which is often associated with a number of extrahepatic manifestations including glomerulopathies. Patients with HCV infection were found to have a higher risk of end-stage renal disease. HCV positivity has also been linked to lower graft and patient survivals after kidney transplantation. Various histological types of renal diseases are reported in association with HCV infection including membranoproliferative glomerulonephritis (MPGN), membranous nephropathy, focal segmental glomerulosclerosis, fibrillary glomerulonephritis, immunotactoid glomerulopathy, IgA nephropathy, renal thrombotic microangiopathy, vasculitic renal involvement and interstitial nephritis. The most common type of HCV associated glomerulopathy is type&#x02005;I&#x02005;MPGN associated with type II mixed cryoglobulinemia. Clinically, typical renal manifestations in HCV-infected patients include proteinuria, microscopic hematuria, hypertension, acute nephritis and nephrotic syndrome. Three approaches may be suggested for the treatment of HCV-associated glomerulopathies and cryoglobulinemic renal disease: (1) antiviral therapy to prevent the further direct damage of HCV on kidneys and synthesis of immune-complexes; (2) B-cell depletion therapy to prevent formation of immune-complexes and cryoglobulins; and (3) nonspecific immunosuppressive therapy targeting inflammatory cells to prevent the synthesis of immune-complexes and to treat cryoglobulin associated vasculitis. In patients with moderate proteinuria and stable renal functions, anti-HCV therapy is advised to be started as pegylated interferon-&#x003b1; plus ribavirin. However in patients with nephrotic-range proteinuria and/or progressive kidney injury and other serious extra-renal manifestations, immunosuppressive therapy with cyclophosphamide, rituximab, steroid pulses and plasmapheresis should be administrated.

肿瘤坏死因子在人膜增生性肾小球肾炎中的表达

目的 :探讨肿瘤坏死因子 (TNF -α)在人膜增生性肾小球肾炎发病中的作用。方法 :采用病理组织学及免疫组织化学SABC法对 2 0例人膜增生性肾小球肾炎进行染色观察。结果 :TNF -α蛋白在肾组织内表达增加 ,阳性反应见于肾小管上皮细胞和肾小球内 ,以肾近曲小管上皮细胞阳性最明显 ,与正常组相比有显著性差异 (P <0 .0 1) ,肾小球内呈程度不等的弱阳性 ,但与正常组相比无显著性差异 (P >0 .0 5 ) ,远曲小管阳性反应不明显。结论 :TNF

单克隆免疫球蛋白病相关C3肾炎的临床病理分析

目的：了解单克隆免疫球蛋白病相关的C3肾炎的临床病理特征。方法：回顾性分析2004年3月至2015年5月南京军区南京总医院肾脏科经肾活检病理诊断为C3肾炎的患者,筛选出血清免疫固定电泳见单克隆条带者,统计其临床及病理资料。结果：（1）一般资料：C3肾炎患者共有38例,其中行血清免疫固定电泳检查者16例。血清单克隆免疫球蛋白阳性者7例,男性5例、女性2例,肾活检时年龄44～65岁,病程3～67月。肾脏损害临床表现为肾病综合征4例,多形型血尿者6例,血清肌酐升高3例,贫血4例。（2）补体及补体相关检查：C3下降4例,C4、血清H因子均正常,C3肾炎因子及抗H因子抗体均阴性（6/6）。（3）血液学检查：单克隆免疫球蛋白种类λ型IgG 3例,κ型IgG 2例,λ型IgA 1例,κ轻链1例。血游离轻链比值异常2例。浆细胞升高2例（2/6）。（4）肾脏病理：7例免疫荧光均以C3沉积于肾小球毛细血管袢及系膜区,轻链染色阴性,光镜均呈膜增生样病变,2例伴新月体,肾小管间质病变较轻;电镜下电子致密物无特殊结构,主要沉积于内皮下及系膜区,2例内皮细胞病变明显。（5）治疗及随访：2例浆细胞异常的患者接受沙利度胺联合地塞米松治疗,其中1例肾脏病长期缓解,1例快速进展至终末期肾病;余5例患者接受雷公藤多苷和（或）糖皮质激素治疗,1例失随访,3例尿检改善,4例肾功能稳定。结论：单克隆免疫球蛋白相关的C3肾炎好发于中老年患者,组织学以肾小球膜增生样病变为主,免疫抑制治疗有一定的疗效,但治疗的关键应针对单克隆免疫球蛋白病。

特发性膜性肾病与膜增生性肾炎的比较

目的对比分析特发性膜性肾病(IMN)与原发性膜增生性肾炎(PMPGS)的临床与病理资料,了解其特点及两者的区别。方法对比分析我院近20年来IMN(551例)与PMPGS(105例)的临床病理资料。结果①IMN和PMPGS均为男性多于女性,两组男女比例比较差异无统计学意义(P>0.05);②IMN及PMPGS的平均年龄分别为(47.22±16.32)岁、(39.10±15.47)岁,差异有统计学意义(P<0.01);③IMN的病程中位数为4月,其中50%的病例在(1～11)月,PMPGS病程中位数为6月,其中50%的病例在(3～24)月,两组差异有统计学意义(P<0.01);④IMN及PMPGS均以肾病综合征为主,两组差异无统计学意义;⑤IMN及PMPGS有血尿者分别占33.76%(186/551)及56.19%(59/105),差异有统计学意义(P<0.01);⑥两组血压、尿蛋白定量、血白蛋白浓度、血IgG、IgA浓度比较差异无统计学意义(P>0.05),但血中IgM、C3、C4的浓度及补体(C3)降低的比例比较,差异有统计学意义(P<0.01);⑦两组合并肾功能不全以及血中尿素氮、肌酐的浓度比较,差异有统计学意义(P<0.01);⑧总体疾病危险度比较,两组差异有统计学意义(P<0.01);⑨两组在肾脏免疫病理表现方面,均有较强的免疫球蛋白沉积,但IMN较PMPGN免疫荧光沉积强,两组比较差异有统计学意义(P<0.01)。结论①两种疾病均为男性多于女性;②临床主要表现为肾病综合征;③PMPGS较IMN血尿常见,补体(C3)降低的比例高;④IMN在肾功能损害合并肾功能不全及疾病危险度的评价较PMPGS轻。

电子致密物沉积病的超微结构观察

电子致密物沉积病 (densedepositdisease ,DDD)是一种罕见的肾小球慢性疾病。本文对 5例DDD的超微结构进行观察 ,并结合临床及HE、特殊染色 (PAS、PASM Masson)、免疫组化 (IgG、IgM、IgA、C3、C1q、HBsAg、HBcAg)结果进行分析。结果显示 :DDD的临床表现及组织形态学均具有多样性。 5例中临床表现 2例为肾病综合症 ,2例为慢性肾炎综合征 ,1例为急性肾功不全。形态学改变 3例为膜增殖性肾小球肾炎 (MPGN) ,1例系膜增生伴局灶节段膜增殖 (MePGN伴sMPGN) ,1例弥漫系膜增生性肾小球肾炎 (MePGN)。电镜下肾小球基底膜弥漫性增厚 ,致密层内见条带状高电子致密物沉积 ,其中 1例伴有内皮下和上皮下沉积物 ,4例系膜区块状沉积物。免疫组化提示毛细血管袢以C3、IgM沉积为主 ,系膜区C3沉积 ,1例乙型肝炎标志物阳性。DDD的发生可能与补体C3的激活并沉积及免疫复合物机制有关 。

脂多糖诱导大鼠肾小球系膜细胞增殖和分泌细胞外基质的研究

目的观察脂多糖(LPS)对大鼠肾小球系膜细胞(GMC)增殖及分泌细胞外基质(ECM)的作用。方法建立体外培养的大鼠GMC,鉴定后用于实验。实验分为两组:对照组和LPS诱导组。甲基噻唑基四唑(MTT)比色法测定24h和48h两个时点两组系膜细胞的增殖情况;ELISA法测定6h、12h和24h系膜细胞培养上清液中ECM蛋白含量;荧光半定量反转录PCR(RT-PCR)法检测ECM中层黏连蛋白(LN)β2 mRNA表达的变化。结果(1)LPS组和对照组GMC增殖情况间差别有显著性意义(P<0.05);(2)正常培养的大鼠GMC可分泌一定量的ECM,LPS组在各时点分泌ECM量与对照组间差别有显著性意义(P<0.01);(3)正常培养的大鼠GMC有微量LNβ2 mRNA表达,LPS组在各时点LNβ2 mRNA表达量与对照组间差别均有显著性意义(P<0.01)。结论从蛋白和 mRNA两个水平同时观察到ECM成分(如FN、LN和ColⅣ)的增加,说明在系膜增殖性肾炎中ECM明显增加并起主要作用。

不同年龄原发性膜增殖性肾小球肾炎患者的临床特征研究

目的探讨不同年龄原发性膜增殖性肾小球肾炎(MPGN)患者的临床特征。方法回顾性分析105例于1990年6月—2010年6月在我院住院的原发性MPGN患者的临床资料,将患者按年龄分为4组:1组11例,年龄<20岁;2组44例,年龄20～39岁;3组36例,年龄40～59岁;4组14例,年龄≥60岁。结果 (1)105例患者中男75例(63.7%),女30例(占36.3%);发病年龄为14～69岁,平均(39.2±15.5)岁,其中20～59岁者占76.2%(80/105)。(2)各组病程、水肿发生率、镜下血尿发生率比较,差异均无统计学意义(P>0.05);收缩压升高发生率及平均收缩压比较,差异均有统计学意义(P<0.05),且4组收缩压升高发生率和平均收缩压与其他3组比较,差异亦均有统计学意义(P<0.05)。(3)各组合并肾功能不全发生率比较,差异有统计学意义(P<0.05),且4组与2组间差异有统计学意义(P=0.019)。(4)各组尿蛋白定量、血清蛋白水平、总胆固醇水平比较,差异均有统计学意义(P<0.05),且1组尿蛋白定量和血清蛋白水平与2组、3组比较,3组和4组总胆固醇水平与1组、2组比较,差异均有统计学意义(P<0.05)。(5)各组免疫学指标平均水平及肾组织免疫荧光学表现比较,差异均无统计学意义(P>0.05)。(6)各组疾病危险度比较,差异有统计学意义(P=0.034),且1组与3、4组比较,2组与4组比较,差异均有统计学意义(P<0.05)。结论原发性MPGN好发于中年男性,临床主要表现为肾病综合征,以<20岁及≥60岁的患者较为明显,且老年患者(≥60岁)高血压发病率及疾病危险度较高,病情较重。

泼尼松与吗替麦考酚酯治疗系膜增生性IgA肾小球肾炎患者的综合干预护理分析

目的研究泼尼松与吗替麦考酚酯(Mycophenolate Mofetil,MMF)治疗系膜增生性Ig A肾小球肾炎患者的护理干预价值。方法从2014年11月至2016年11月,接受治疗的86例被确诊患有系膜增生性Ig A肾小球肾炎的患者作为研究对象。采用随机数字表法分成观察组(43例)和对照组(43例)。对照组采用泼尼松与吗替麦考酚酯治疗并加以常规护理;观察组在对照组的基础上增加综合干预护理,治疗12个月后,观察并比较两组护理干预的疗效、生理指标、血管内皮生长因子(VEGF)、基质金属蛋白酶-9(MMP-9)、耐药性、不良反应、复发率及视觉模拟评分(visual analogue scale,VAS)。结果治疗后观察组完全缓解占比37.21%(16例/43例)、总有效率97.67%(42例/43例),显著高于对照组16.28%(7例/43例)、86.05%(37例/43例),差异有统计学意义(χ2=4.807,3.888;P<0.05);治疗前各项生理指标比较差异无统计学意义,治疗后各项生理指标均有显著改善,且观察组改善幅度较对照组差异有统计学意义(t=6.417,7.227,9.760,5.595,12.125,6.399,2.907;均P<0.05);治疗前两组差异无统计学意义,治疗后血清VEGF和MMP-9水平均显著下降,且观察组较对照组下降更明显,差异有统计学意义(t=7.954,8.004;均P<0.001);两组患者在在护理前SAS评分比较差异无统计学意义,护理后观察组SAS评分显著低于对照组,差异有统计学意义(t=14.102,P<0.001);两组患者在治疗期间均有不良反应产生,总不良反应发生率两组差异无统计学意义(χ2=0.551,P>0.05)。结论泼尼松与MMF对系膜增生性Ig A肾小球肾炎患者治疗同时并加以综合性的护理措施,不仅有效提高了治疗效率、改善了患者各项生理指标,降低了血清VEGF和MMP-9水平,同时还有效减轻了患者的焦虑心理,且安全可靠,值得临床借鉴。

补体C5b-9抗血清对抗胸腺细胞血清性肾炎大鼠肾组织一氧化氮合成及其病变的影响

目的 :探讨抗鼠补体C5b - 9复合物抗血清对系膜增生性肾炎大鼠肾组织合成一氧化氮 (NO)及其病变的作用。方法 :复制大鼠系膜增生性肾小球肾炎即抗胸腺细胞血清性肾炎 (ATSN)模型 ,用抗大鼠C5b - 9复合物抗血清处理 ,观察其对ATSN大鼠NO相关指标及其病变的影响。结果 :抗鼠C5b - 9复合物抗血清既能减少ATSN大鼠肾组织诱生性NO合酶 (iNOS)mRNA的表达和大鼠尿液中硝酸盐 /亚硝酸盐 (NO-3 /NO-2 )排泄量 ,还能减低大鼠肾组织病变的程度。NOS抑制剂L -NAME也可降低尿NO-3 /NO-3 排泄量 ,同时减轻肾组织病变程度。结论 :抗鼠C5b -

加味猪苓汤治疗原发性系膜增殖性肾炎的实验研究

【目的】探讨猪苓汤治疗原发性系膜增殖性肾炎的作用机制。【方法】采用兔抗鼠胸腺细胞抗体(Thy-1)大鼠肾炎模型,检测各组大鼠血液生化指标和细胞因子白细胞介素1β(IL-1β)、肿瘤坏死因子α(TNF-α)、白细胞介素6(IL-6)的活性以及白细胞介素6信使核糖核酸(IL-6 mRNA)的表达波。【结果】模型组的IL-1β、TNF-α和IL-6水平均升高,IL-6 mRNA表达增强,与正常对照组比较有显著性差异(P<0.01);猪苓汤组能降低IL-1β、TNF-α和IL-6的水平及减弱IL-6mRNA的表达,与模型组比较均有显著性差异(P<0.05或P<0.01)。【结论】加味猪苓汤可能是通过抑制细胞因子的基因表达、降低细胞因子的活性对原发性系膜增殖性肾炎产生治疗作用。