Clinicopathological features and medium-term outcomes of histologic variants of primary focal segmental glomerulosclerosis in adults:A retrospective study

BACKGROUND The Columbia classification identified five histological variants of focal segmental glomerulosclerosis(FSGS).The prognostic significance of these variants remains controversial.AIM To evaluate the relative frequency,clinicopathologic characteristics,and medium-term outcomes of FSGS variants at a single center in Pakistan.METHODS This retrospective study was conducted at the Department of Nephrology,Sindh Institute of Urology and Transplantation,Karachi,Pakistan on all consecutive adults(≥16 years)with biopsy-proven primary FSGS from January 1995 to December 2017.Studied subjects were treated with steroids as a first-line therapy.The response rates,doubling of serum creatinine,and kidney failure(KF)with replacement therapy were compared between histological variants using ANOVA or Kruskal Wallis,and Chi-square tests as appropriate.Data were analyzed by SPSS version 22.0.P-value≤0.05 was considered significant.RESULTS A total of 401 patients were diagnosed with primary FSGS during the study period.Among these,352(87.7%)had a designated histological variant.The not otherwise specified(NOS)variant was the commonest,being found in 185(53.9%)patients,followed by the tip variant in 100(29.1%)patients.Collapsing(COL),cellular(CEL),and perihilar(PHI)variants were seen in 58(16.9%),6(1.5%),and 3(0.7%)patients,respectively.CEL and PHI variants were excluded from further analysis due to small patient numbers.The mean follow-up period was 36.5±29.2 months.Regarding response rates of variants,patients with TIP lesions achieved remission more frequently(59.5%)than patients with NOS(41.8%)and COL(24.52%)variants(P<0.001).The hazard ratio of complete response among patients with the COL variant was 0.163[95%confidence interval(CI):0.039-0.67]as compared to patients with NOS.The TIP variant showed a hazard ratio of 2.5(95%CI:1.61-3.89)for complete remission compared to the NOS variant.Overall,progressive KF was observed more frequently in patients with the COL variant,43.4%(P<0.001).Among these,24.53%of patients required kidney replacement therapy(P<0.001).The hazard ratio of doubling of serum creatinine among patients with the COL variant was 14.57(95%CI:1.87-113.49)as compared to patients with the TIP variant.CONCLUSION In conclusion,histological variants of FSGS are predictive of response to treatment with immunosuppressants and progressive KF in adults in our setup.

Synergism of calycosin and bone marrow-derived mesenchymal stem cells to combat podocyte apoptosis to alleviate adriamycininduced focal segmental glomerulosclerosis

BACKGROUND Bone marrow-derived mesenchymal stem cells(MSCs)show podocyte-protective effects in chronic kidney disease.Calycosin(CA),a phytoestrogen,is isolated from Astragalus membranaceus with a kidney-tonifying effect.CA preconditioning enhances the protective effect of MSCs against renal fibrosis in mice with unilateral ureteral occlusion.However,the protective effect and underlying mechanism of CA-pretreated MSCs(MSCsCA)on podocytes in adriamycin(ADR)-induced focal segmental glomerulosclerosis(FSGS)mice remain unclear.AIM To investigate whether CA enhances the role of MSCs in protecting against podocyte injury induced by ADR and the possible mechanism involved.METHODS ADR was used to induce FSGS in mice,and MSCs,CA,or MSCsCA were administered to mice.Their protective effect and possible mechanism of action on podocytes were observed by Western blot,immunohistochemistry,immunofluorescence,and real-time polymerase chain reaction.In vitro,ADR was used to stimulate mouse podocytes(MPC5)to induce injury,and the supernatants from MSC-,CA-,or MSCsCA-treated cells were collected to observe their protective effects on podocytes.Subsequently,the apoptosis of podocytes was detected in vivo and in vitro by Western blot,TUNEL assay,and immunofluorescence.Overexpression of Smad3,which is involved in apoptosis,was then induced to evaluate whether the MSCsCA-mediated podocyte protective effect is associated with Smad3 inhibition in MPC5 cells.RESULTS CA-pretreated MSCs enhanced the protective effect of MSCs against podocyte injury and the ability to inhibit podocyte apoptosis in ADR-induced FSGS mice and MPC5 cells.Expression of p-Smad3 was upregulated in mice with ADR-induced FSGS and MPC5 cells,which was reversed by MSCCA treatment more significantly than by MSCs or CA alone.When Smad3 was overexpressed in MPC5 cells,MSCsCA could not fulfill their potential to inhibit podocyte apoptosis.CONCLUSION MSCsCA enhance the protection of MSCs against ADR-induced podocyte apoptosis.The underlying mechanism may be related to MSCsCA-targeted inhibition of p-Smad3 in podocytes.

Update on the treatment of focal segmental glomerulosclerosis in renal transplantation

Focal segmental glomerulosclerosis(FSGS) represents one of the most severe glomerular diseases, with frequent progression to end-stage renal disease and a high rate of recurrence in renal allografts(30%-50%). Recurrent FSGS portends a negative outcome, with the hazard ratio of graft failure being two-fold higher then that of other glomerulonephritis. Two patterns of clinical presentations are observed: Early recurrence, which is characterized by massive proteinuria within hours to days after implantation of the renal graft, and late recurrence, which occurs several months or years after the transplantation. Many clinical conditions have been recognized as risk factors for recurrence, including younger age, rapid progression of the disease to end-stage renal disease on native kidneys, and loss of previous renal allografts due to recurrence. However, much less is known about the incidence and risk factors of the so-called "de novo " type of FSGS, for which sufferers are transplanted patients without disease on native kidneys; but, rapid development of allograft failure is frequently observed. Management of both forms is challenging, and none of the approaches proposed to date have been demonstrated as consistently beneficial or effective. In the present review we report an update on the available therapeutic strategies for FSGS in renal transplantation within the context of a critical overview of the current literature.

Rituximab or plasmapheresis for prevention of recurrent focal segmental glomerulosclerosis after kidney transplantation:A systematic review and meta-analysis

BACKGROUND Focal segmental glomerulosclerosis(FSGS)is one of the most common glomerular diseases leading to renal failure.FSGS has a high risk of recurrence after kidney transplantation.Prevention of recurrent FSGS using rituximab and/or plasmapheresis has been evaluated in multiple small studies with conflicting results.AIM To assess the risk of recurrence of FSGS after transplantation using prophylactic rituximab with or without plasmapheresis,and plasmapheresis alone compared to the standard treatment group without preventive therapy.METHODS This meta-analysis and systematic review were performed by first conducting a literature search of the MEDLINE,EMBASE,and Cochrane databases,from inception through March 2021;search terms included‘FSGS,’’steroid-resistant nephrotic syndrome’,‘rituximab,’and‘plasmapheresis,’.We identified studies that assessed the risk of post-transplant FSGS after use of rituximab with or without plasmapheresis,or plasmapheresis alone.Inclusion criteria were:Original,published,randomized controlled trials or cohort studies(either prospective or retrospective),case-control,or cross-sectional studies;inclusion of odds ratio,relative risk,and standardized incidence ratio with 95%confidence intervals(CI),or sufficient raw data to calculate these ratios;and subjects without interventions(controls)being used as comparators in cohort and cross-sectional studies.Effect estimates from individual studies were extracted and combined using a random effects model.RESULTS Eleven studies,with a total of 399 kidney transplant recipients with FSGS,evaluated the use of rituximab with or without plasmapheresis;thirteen studies,with a total of 571 kidney transplant recipients with FSGS,evaluated plasmapheresis alone.Post-transplant FSGS recurred relatively early.There was no significant difference in recurrence between the group that received rituximab(with or without plasmapheresis)and the standard treatment group,with a pooled risk ratio of 0.82(95%CI:0.47-1.45,I2=65%).Similarly,plasmapheresis alone was not associated with any significant difference in FSGS recurrence when compared with no plasmapheresis;the pooled risk ratio was 0.85(95%CI:0.60-1.21,I2=23%).Subgroup analyses in the pediatric and adult groups did not yield a significant difference in recurrence risk.We also reviewed and analyzed posttransplant outcomes including timing of recurrence and graft survival.CONCLUSION Overall,the use of rituximab with or without plasmapheresis,or plasmapheresis alone,is not associated with a lower risk of FSGS recurrence after kidney transplantation.Future studies are required to assess the effectiveness of rituximab with or without plasmapheresis among specific patient subgroups with high-risk for FSGS recurrence.

Collapsing focal segmental glomerulosclerosis: Current concepts

Collapsing focal segmental glomerulosclerosis(cF SGS), also known as collapsing glomerulopathy is currently classified under the rubric of FSGS. However, its defining morphological features are in stark contrast to those observed in most other variants of FSGS. During the early stage of the disease, the lesion is characterized pathologically by an implosive segmental and/or global collapse of the glomerular capillary tufts, marked hypertrophy and hyperplasia of podocytes, and severe tubulointerstitial disease. With advancement of the disease, segmental and/or global glomerulosclerosis is also observed in association with the collapsing lesions. The etiology of this enigmatic disorder is still elusive, but a growing list of diseases/conditions is being reported in association with this morphological pattern of renal parenchymal injury. The pathogenesis of cF SGS involves discreet epithelial cell injury leading to cell cycle dysregulation and a proliferative cellular phenotype. From the clinical perspective, cF SGS is notorious for its propensity to affect black people, a high incidence and severity of nephrotic syndrome, marked resistance to empirical therapy, and rapid progression to end-stage renal disease. The lesion has also been reported in transplanted kidneys either as recurrent or de novo disease, frequently leading to graft loss. Mostcases have been reported in western countries, but the lesion is also being increasingly recognized in the tropical regions. The recent increase in reporting of cF SGS partly reflects a true increase in the incidence and partly a detection bias. There is no specific treatment for the disorder at present. Newer insights into the pathogenesis may lead to the development of targeted and specific therapy in near future. There is an urgent need to increase awareness of the lesion among pathologists and nephrologists, especially those from developing countries, to ensure accurate diagnosis and appropriate managment. With the accumulation of more and more data, it is hoped that the prevailing confusion about the nosological identity of the lesion will also be resolved in a more logical way.

Primary focal and segmental glomerulosclerosis and soluble factor urokinase-type plasminogen activator receptor

Primary focal and segmental glomerulosclerosis(FSGS) may be due to genetic or acquired etiologies and is a common cause of nephrotic syndrome with high morbidity that often leads to end-stage renal failure. The different available therapeutic approaches are unsuccessful, in part due to partially deciphered heterogeneous and complex pathophysiological mechanisms. Moreover, the term FSGS, even in its primary form, comprises a histological description shared by a number of different causes with completely different molecular pathways of disease. This review focuses on the latest developments regarding the pathophysiology of primary acquired FSGS caused by soluble factor urokinase type plasminogen activator receptor, a circulating permeability factor involved in proteinuria and edema formation, and describes recent advances with potential success in therapy.

Transition from minimal change disease to focal segmental glomerulosclerosis related to occupational exposure:A case report

BACKGROUND Although minimal change disease(MCD)and focal segmental glomerulosclerosis(FSGS)have been described as two separate forms of nephrotic syndrome(NS),they are not completely independent.We report a case of a patient transitioning from MCD to FSGS,review the literature,and explore the relationship between the two diseases.CASE SUMMARY A 42-year-old male welder,presenting with lower extremity edema and elevated serum creatinine,was diagnosed with NS and end-stage kidney disease(ESKD)based on laboratory test results.The patient had undergone a kidney biopsy for NS 20 years previously,which indicated MCD,and a second recent kidney biopsy suggested FSGS.The patient was an electric welder with excessive levels of cadmium and lead in his blood.Consequently,we suspect that his aggravated pathology and occurrence of ESKD were related to metal nephrotoxicity.The patient eventually received kidney replacement therapy and quit his job which involved long-term exposure to metals.During the 1-year follow-up period,the patient was negative for metal elements in the blood and urine and recovered partial kidney function.CONCLUSION MCD and FSGS may be different stages of the same disease.The transition from MCD to FSGS in this case indicates disease progression,which may be related to excessive metal contaminants caused by the patient’s occupation.

Case of human immunodeficiency virus infection presenting as a tip variant of focal segmental glomerulosclerosis: A case report and review of the literature

The incidence of the collapsing variant of focal segmental glomerulosclerosis(FSGS) as a human immunodeficiency virus(HIV)-associated nephropathy has reduced since the introduction of antiretroviral therapy(ART). However, the incidence of other variants of FSGS, except for the collapsing variant, is increasing, and its therapeutic strategies remain uncertain. A 60-year-old HIV infected man in remission with ART was admitted for progressive renal insufficiency and nephrotic-ranged proteinuria. Renal biopsy revealed a tip variant of FSGS and his clinical manifestations resolved with corticosteroid therapy. HIV infected patients might develop non-collapsing FSGS, including tip variant of FSGS and corticosteroid therapy might be effective for them. A renal biopsy might be essential to determine the renal histology and to decide on corticosteroid therapy.

Non-glomerular Tip Lesion Focal Segmental Glomerulosclerosis as a Negative Predictor in Idiopathic Membranous Nephropathy

Objective To assess the significance of focal segmental glomerulosclerosis(FSGS)variants on clinicopathological characteristics and short-term outcomes in idiopathic membranous nephropathy(IMN)patients.Methods The clinicopathological data of 146 IMN patients diagnosed between December 2016 and March 2019 in our center were collected and analyzed.These patients were divided into the pure IMN group,IMN with glomerular tip lesion(GTL)group,and IMN with non-GTL FSGS group.Results The IMN with non-GTL FSGS and IMN with GTL groups both had higher proportions of patients with hypertension,lower serum albumin,and severe proteinuria,while the IMN with non-GTL FSGS group additionally showed higher blood pressure and serum cholesterol,and lower serum IgG than the IMN group(all P<0.05).As for pathology,the IMN with non-GTL FSGS group had higher proportions of patients with acute tubular injury and moderate to severe chronic injuries than the IMN group(all P<0.05).In the IMN,IMN with GTL,and IMN with non-GTL FSGS groups,the overall one-year remission rates were 81.6%,76%,and 58.8%,respectively.Furthermore,the IMN with non-GTL FSGS group showed the lowest cumulative incidence to reach remission within one year.Multivariate Cox logistic analysis demonstrated that higher level of serum anti-M-type phospholipase A2 receptor antibody and the existence of non-GTL FSGS lesion were independent predictors for no remission in IMN patients.Conclusion The non-GTL FSGS lesion was a novel negative predictor in IMN and should be taken into account in the management of IMN.

FSGS小鼠模型中YAP与足细胞凋亡的相关性及其激动剂的保护作用

目的探究YAP与局灶节段性肾小球硬化症(focal segmental glomerulosclerosis,FSGS)中足细胞凋亡的相关性及其激动剂的作用。方法收取复旦大学基础医学院病理学系肾病研究组人FSGS肾穿标本,使用阿霉素刺激构建FSGS小鼠模型和体外足细胞损伤模型,并联合YAP激动剂1-油酰基溶血磷脂酸(1-Oleoyl lysophosphatidic acid,LPA)处理上述体内外模型,使用免疫组化、免疫荧光双染、Western blot及Hoechst 33258染色检测足细胞凋亡和足细胞中YAP表达的相关性;使用LPA处理转染YAP siRNA的足细胞系后,检测足细胞中YAP表达和凋亡的变化。结果在人FSGS、FSGS小鼠模型和体外阿霉素诱导足细胞损伤模型中足细胞凋亡越多,YAP出核越多;LPA处理可以改善FSGS小鼠模型的肾脏形态(t=17.68,P<0.0001)和肾功能(血尿素氮:t=4.576,P=0.0102;尿白蛋白/肌酐:t=2.51,P=0.0456),减少足细胞中p-YAP(S127)的表达,促进YAP入核,减少阿霉素诱导的足细胞凋亡(Cleaved Caspase-3的表达及Hoechst 33258染色结果均为P<0.001);敲减足细胞中YAP后,YAP的总蛋白和磷酸化水平均降低,足细胞凋亡增加,LPA处理减少了p-YAP(S127)的表达,促进YAP入核,减少YAP敲减所致的足细胞凋亡(Cleaved Caspase-3的表达及Hoechst 33258染色结果均为P<0.0001)。结论FSGS模型中活化YAP减少及YAP出核,足细胞凋亡增多;LPA能够通过抑制YAP在Ser127位点的磷酸化,促进足细胞中YAP的入核,减少细胞凋亡,延缓FSGS的疾病进程。

霉酚酸酯对局灶节段性肾小球硬化(FSGS)治疗作用的研究

目的:用霉酚酸酯(MMF)对以阿霉素肾病大鼠建立的局灶节段性肾小球硬化(FSGS)模型,进行干预,检测结缔组织生长因子(CTGF)的表达,研究霉酚酸酯对FSGS的治疗作用,并探讨作用机理。方法:SD大鼠18只,分为对照组、阿霉素肾病组、MMF治疗组(每组大鼠6只)。肾病组、治疗组大鼠尾静脉一次性注入阿霉素7.5mg/kg,对照组大鼠尾静脉注入等量生理盐水。治疗组于第6周起MMF 20mg.kg-1.d-1混悬于1mL蒸馏水灌胃,其他组等量蒸馏水灌胃。第10周处死所有大鼠,观察肾组织病理变化,并以免疫组织化学、Western blot方法检测肾组织CTGF蛋白水平。结果:阿霉素肾病组大鼠较对照组大鼠肾小球系膜及基质明显增生,免疫组织化学染色及western blot显示肾小球和肾小管区CTGF蛋白表达明显上升(P<0.05),霉酚酸酯治疗组肾小球系膜和基质增生较肾病组明显减轻,肾小球和肾小管区CTGF蛋白表达明显低于肾病组(P<0.05)。结论:霉酚酸酯可以减轻肾脏间质纤维化病变,机理与抑制CTGF的表达有关。

MsPGN与FSGS患者血清Angptl 4、suPAR改变及其临床意义

目的观察系膜增生性肾小球肾炎(Ms PGN)与局灶节段性肾小球硬化(FSGS)患者血管生成素样蛋白-4(Angptl-4)及可溶性尿激酶型纤溶酶原激活物受体(su PAR)血清水平改变,并探讨其临床意义。方法选取2015年3月~2016年10月经皮肾穿刺活检患者120例(观察组),其中Ms PGN 66例,FSGS 54例;另取同期健康体检者120例(对照组)。分别比较观察组水肿与蛋白尿的严重程度、血清白蛋白水平与相应的血清Angptl-4、su PAR水平、FSGS行肾移植后复发者与未复发者血清suPAR水平。结果观察组血清Angptl-4、su PAR水平显著高于对照组,Angptl-4、su PAR水平随尿蛋白增加升高,与血清白蛋白呈负相关,Ms PGN患者血清Angptl-4水平显著高于FSGS患者,而FSGS患者血清su PAR水平显著高于Ms PGN患者,且FSGS肾移植后复发患者血清su PAR水平显著高于未复发者,上述差异均有统计学意义(P均<0.05)。结论 Angptl-4、su PAR水平在Ms PGN与FSGS的发生和发展中具有不同病理作用,血清su PAR水平可能作为预测FSGS患者肾移植后复发风险的生物学标志物。

Long-term prognosis of focal segmental glomerulosclerosis treated with therapeutic low-density lipoprotein-apheresis in patients with severe kidney dysfunction and proteinuria

Background:The prognosis of focal segmental glomerulosclerosis patients with nephrotic syndrome is estimated to be 10%-20%in 5 years and 30%-50%in 10 years,leading to end-stage kidney disease.The response rate with steroid therapy is 40%-60%.Therapeutic low-density lipoprotein-apheresis(LDL-A)may be effective in patients with steroid resistance.Information regarding the long-term prognosis of patients with focal segmental glomerulosclerosis receiving this therapy is scarce.Methods:We investigated the effectiveness of treatment in 50 patients with primary focal segmental glomerulosclerosis diagnosed between 1961 and 2017 at Kanazawa University Hospital and related facilities.The patients were observed at least 12 months after biopsy or until end-stage kidney disease occurrence or death.Results:LDL-A was performed in four patients who presented with steroidresistant nephrotic syndrome(two patients had concurrent acute renal failure for which hemodialysis was performed).In comparison with 17 patients who did not receive LDL-A after 1989,the LDL-A group had higher urinary protein excretion(13.7 vs.5.2 g/day,P=0.053)and serum creatinine(4.11 vs.1.65 mg/dL)levels at onset,and a numerically higher remission rate(75.0%vs.58.7%)compared with the nonlipoprotein-apheresis group.Conclusion:Therapeutic LDL-A can be performed for critical cases and may improve the remission rate.

辅肌动蛋白4基因184T>A突变与原发性FSGS的关联研究

目的研究辅肌动蛋白4(ACTN4)基因杂合突变184T>A与原发性局灶节段性肾小球硬化(FSGS)的关系及其发生率。方法收集2012年1月—2016年6月于黑龙江省医院肾内科和哈尔滨医科大学附属第一医院肾内二科经肾穿刺活检确诊为原发性FSGS患者78例,同时期在两所医院体检中心选取健康人68例作为对照组,蛋白酶-盐析法提取外周血白细胞基因组DNA,设计ACTN4基因第2外显子区引物,聚合酶链式反应(PCR)扩增后进行测序发现突变,氯酚法提取父母头发DNA检测ACTN4基因。结果 78例原发性FSGS患者中检测到1例患者存在ACTN4基因第2外显子区杂合突变184T>A,导致编码蛋白质ACTN4的第62位氨基酸由丝氨酸突变为苏氨酸。患者父母,健康对照组均未检测到相同突变,其余FSGS患者未检测到新的致病突变。此外,共发现4个单核苷酸多态:rs2112649、rs761625093、rs146499679和rs781451819,其中rs146499679导致编码氨基酸改变。结论 ACTN4基因第2外显子区184T>A(Ser62Thr)突变在原发性FSGS患者中的发生率较低,因此不是引起本次研究原发性FSGS的突变的主要原因。

miR-124在FSGS小鼠中异常表达的研究

目的探究miR-124在阿霉素(Adriamycin,ADR)诱导的局灶节段性肾小球硬化(focal seg-mental glomerulosclerosis,FSGS)小鼠模型中的表达,为阐明miR-124异常表达导致FSGS的发病机制奠定基础.方法将BALB/c小鼠随机分为对照组和实验组,一次性尾静脉注射ADR 10.5 mg/kg,28 d后取血尿及肾组织,利用ELISA法检测尿蛋白,血清肌酐;通过苏木精-伊红染色法(HE)和Masson三色染色观察肾组织形态变化;RT-PCR检测miR-124的表达水平;Western印迹检测synaptopodin蛋白的表达水平.结果实验组尿蛋白和血肌酐/体重比值水平升高(P<0.05);HE和Masson染色显示肾组织出现FSGS病理变化;miR-124表达明显上调(P<0.05)且synaptopodin蛋白表达降低(P<0.05).结论在FSGS小鼠模型中,miR-124异常高表达,synaptopodin蛋白表达下调,提示miR-124可能参与FSGS疾病中足细胞损伤的发病过程.

栽培桑黄对FSGS肾病大鼠肾功能及肾纤维化机制研究

目的:研究栽培桑黄对局灶节段肾小球硬化(focal stage glomerulosclerosis, FSGS)肾病大鼠早期肾损伤的干预作用及其机制。方法:采用单侧肾切除合并尾静脉注射阿霉素构建FSGS大鼠模型,分别用人工桑黄水煎剂及水提物进行干预治疗。生化检测尿蛋白、血肌酐、尿素氮、血脂及其他指标,Masson染色观察肾组织病理损伤情况,RT-PCR检测肾皮质Col-Ⅳ、FN、MMP9、TIMP-1基因表达水平。结果:和模型组比较,桑黄水煎剂低剂量组可显著降低24 h尿蛋白、血肌酐、尿素氮、三酰甘油、胆固醇的水平(P<0.05)。桑黄水煎剂、水提物均可降低心肌酶或谷丙转氨酶水平,其中水煎剂低剂量组心肌酶显著低于模型组(P<0.05),水提物高剂量组显著降低心肌酶和谷丙转氨酶水平(P<0.05)。桑黄水煎剂低剂量可显著下调Col-Ⅳ、FN的mRNA水平(P<0.05),上调MMP9/TIMP-1水平(P<0.05)。结论:桑黄可显著降低尿蛋白,改善肾功能和肾组织病理损伤,降低细胞外基质沉积,且相同生药剂量的桑黄传统水煎剂好于水提物疗效,其机制可能与其调节金属蛋白酶及其抑制剂表达有关。

CLEC14A在阿霉素诱导FSGS小鼠模型中对足细胞损伤的保护机制

目的:探究CLEC14A在阿霉素诱导局灶节段性肾小球硬化(FSGS)小鼠模型中对足细胞损伤的保护作用,并通过半胱氨酸蛋白酶-3(Caspase-3)、B淋巴细胞癌-2相关蛋白(Bax)和B淋巴细胞瘤-2(Bcl-2)信号通路探讨其机制。方法:将30只C57BL/6小鼠随机分成Sham组(n=10)、Model组(n=10)和CLEC14A siRNA组(siRNA组,n=10)。将小鼠足细胞MPC5分为对照组、FSGS组、FSGS-siCLEC14A组。采用定量聚合酶链反应(qPCR)检测小鼠肾脏中CLEC14A mRNA及血管内皮生长因子(VEGF)mRNA的水平。采用酶联免疫吸附试验(ELISA)检测小鼠肾脏组织中Caspase-3、Bax和Bcl-1水平。结果:FSGS组及FSGS-siCLEC14A组各时间点的细胞增殖能力低于对照组,差异均有统计学意义(均P<0.05)。FSGS-siCLEC14A组的48 h及72 h细胞增殖能力均低于FSGS组,差异均有统计学意义(均P<0.05)。与对照组比较,FSGS组和FSGS-siCLEC14A组的细胞凋亡率、Caspase-3、Bax水平上升,而Bcl-2水平下降,差异均有统计学意义(均P<0.05);与FSGS组比较,FSGS-siCLEC14A组的Caspase-3、Bax水平增加,而Bcl-2水平下降,差异均有统计学意义(均P<0.05)。与对照组比较,FSGS组和FSGS-siCLEC14A组的24 h尿蛋白定量(24 h UTP)、血肌酐(Scr)及血尿素氮(BUN)水平增加,差异均有统计学意义(均P<0.05);与FSGS组比较,FSGS-siCLEC14A组的24 h UTP、Scr及BUN水平增加,差异均有统计学意义(均P<0.05)。与Sham组比较,Model组和siRNA组小鼠的CLEC14A mRNA水平下降,VEGF mRNA上升,差异均有统计学意义(均P<0.05);与Model组比较,siRNA组小鼠的CLEC14A mRNA水平下降,VEGF mRNA上升,差异均有统计学意义(均P<0.05)。与Sham组比较,Model组和siRNA组小鼠肾脏中的Caspase-3、Bax水平上升,而Bcl-2水平下降,差异均有统计学意义(均P<0.05);与Model组比较,siRNA组小鼠肾脏中的Caspase-3、Bax水平升高,而Bcl-2水平下降,差异均有统计学意义(均P<0.05)。结论:CLEC14A可通过抑制Caspase-3、Bax、Bcl-2信号通路起到保护FSGS小鼠足细胞的作用。

Genetic basis of adult-onset nephrotic syndrome and focal segmental glomerulosclerosis

Nephrotic syndrome （NS） is one of the most common glomerular diseases with signs of nephrosis, heavy proteinuria, hypoalbuminemia, and edema. Dysfunction of glomerular filtration barrier causes protein loss through the kidneys. Focal segmental glomerulosclerosis （FSGS） accounts for nearly 20% of NS among children and adults. Adult-onset FSGS/NS is often associated with low response to steroid treatment and immunosup- pressive medication and poor renal survival. Several genes involved in NS and FSGS have been identified by linkage analysis and next-generation sequencing. Most of these genes encode proteins and are highly expressed in glomerular podocytes, which play crucial roles in slit-diaphragm signaling, regulation of actin cytoskeleton dynamics and maintenance of podocyte integrity, and cell-matrix interactions. In this review, we focus on the recently identified genes in the adult-onset NS and FSGS and discuss clinical significance of screening of these genes.

New Mutation of Coenzyme Q10 Monooxygenase 6 Causing Podocyte Injury in a Focal Segmental Glomerulosclerosis Patient

Background:Focal segmental glomerulosclerosis (FSGS)is a kidney disease that is commonly associated with proteinuria and the progressive loss of renal function,which is characterized by podocyte injury and the depletion and collapse of glomerular capillary segments.The pathogenesis of FSGS has not been completely elucidated;however,recent advances in molecular genetics have provided increasing evidence that podocyte structural and functional disruption is central to FSGS pathogenesis.Here,we identified a patient with FSGS and aimed to characterize the pathogenic gene and verify its mechanism. Methods:Using next-generation sequencing and Sanger sequencing,we screened the causative gene that was linked to FSGS in this study.The patient's total blood RNA was extracted to validate the messenger RNA (mRNA)expression of coenzyme Q10 monooxygenase 6(COQ6)and validated it by immunohistochemistry.COQ6 knockdown in podocytes was performed in vitro with small interfering RNA, and then,F-actin was determined using immunofluorescence staining.Cell apoptosis was evaluated by flow cytometry,the expression of active caspase-3was determined by Western blot,and mitochondrial function was detected by MitoSOX. Results:Using whole-exome sequencing and Sanger sequencing,we screened a new causative gene,COQ6,NM_182480:exonl:c.G41A: p.W14X.The mRNA expression of COQ6 in the proband showed decreased.Moreover,the expression of COQ6,which was validated by immunohistochemistry,also had the same change in the proband.Finally,we focused on the COQ6 gene to clarify the mechanism of podocyte injury.Flow cytometry showed significantly increased in apoptotic podocytes,and Western blotting showed increases in active caspase-3in si-COQ6 podocytes.Meanwhile,reactive oxygen species (ROS)levels were increased and F-actin immunofluorescence was irregularly distributed in the si-COQ6 group. Conclusions:This study reported a possible mechanism for FSGS and suggested that a new mutation in COQ6,which could cause respiratory chain defect,increase the generation of ROS,destroy the podocyte cytoskeleton,and induce apoptosis.It provides basic theoretical basis for the screening of FSGS in the future.

Efficacy of tacrolimus in the treatment of children with focal segmental glomerulosclerosis

Background:Focal segmental glomerulosclerosis(FSGS)is the most common glomerular condition leading to end-stage renal disease(ESRD)and the third most common cause of ESRD in pediatric patients.Methods:This is a retrospective study consisting of 22 pediatric patients with FSGS and heavy proteinuria.After demonstrating steroids resistance,the patients were treated with tacrolimus,targeting a trough level 5-8 ng/mL.The primary outcome is the induction of remission with tacrolimus.Results:Thirteen patients(59%)achieved remission(complete in 31.8%and partial in 27.2%)and 12 patients showed stable or improved renal function over an average follow-up of 2.9 years(range:0.5-7 years).There was no significant difference in response rate between African American and Caucasian patients.None of the patients had significant side-effect to tacrolimus and none of the repeat biopsies showed an increase in interstitial fibrosis compared to baseline.The best renal outcome was for patients who achieved complete remission.Partially responsive patients had improved renal function compared with resistant patients.Conclusion:Tacrolimus is a viable option in the treatment of children with idiopathic steroid resistant FSGS.