Loss of decay-accelerating factor triggers podocyte injury and glomerulosclerosis

Angeletti, Andrea; Cantarelli, Chiara; Petrosyan, Astgik; Andrighetto, Sofia; Budge, Kelly L.; D’Agati, Vivette D.; Hartzell, Susan; Malvi, Deborah; Donadei, Chiara; Thurman, Joshua M.; Galešić-Ljubanović, Danica; He, John Cijiang; Xiao, Wu; Campbell, Kirk N.; Wong, Jenny; Fischman, Clara; Manrique, Joaquín; Zaza, Gianluigi; Fiaccadori, Enrico; Manna, Gaetano La; Fribourg, Miguel; Leventhal, Jeremy S.; Sacco, Stefano Da; Perin, Laura; Heeger, Peter S.; Cravedi, Paolo

doi:10.1084/jem.20191699

Cited by 43 publications

(58 citation statements)

References 76 publications

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“…This is the results of increased DAF cleavage by phospholipase, despite increased DAF mRNA levels. Importantly, we also found an association between urinary C3a with the progression of proteinuria ( 25 ). Our data not only established the link between immune dysregulation with FSGS but more importantly, future therapeutic approaches and available drug targets.…”

Section: The Complement Systemsupporting

confidence: 51%

“…Therefore, both C5aR and C3aR propose an attractive target for renoprotection in diabetes. We hypothesized that DKD is associated with glomerular cleavage of the DAF, a key inhibitor of C3 convertase ( 25 ). After diabetes induction by streptozotocin, DAF deficient mice have augmented C3b glomerular deposition and manifested a more severe disease phenotype and aggravated histological lesions when compared to control diabetic wild-type mice ( Figure 1 ).…”

Section: The Complement System In Diabetic Kidney Diseasementioning

confidence: 99%

“…While the upregulation of complement regulatory transcripts may seem to contradict a previously noted downregulation of this protein in non-diabetic glomerular disease leading to uninhibited complement activation, we similarly saw an increase in CD55 mRNA in FSGS patients but a decrease in transmembrane CD55 staining in FSGS biopsies. This decrease in protein is likely due to cleavage of CD55 that can be found in the urine of Adriamycin treated mice and FSGS patients ( 25 ). A similar mechanism could be occurring in DKD.…”

Section: The Complement System In Diabetic Kidney Diseasementioning

confidence: 99%

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Complement, a Therapeutic Target in Diabetic Kidney Disease

Budge

Dellepiane

et al. 2021

Front. Med.

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Currently available treatments of diabetic kidney disease (DKD) remain limited despite improved understanding of DKD pathophysiology. The complement system is a central part of innate immunity, but its dysregulated activation is detrimental and results in systemic diseases with overt inflammation. Growing evidence suggests complement activation in DKD. With existent drugs and clinical success of treating other kidney diseases, complement inhibition has emerged as a potential novel therapy to halt the progression of DKD. This article will review DKD, the complement system's role in diabetic and non-diabetic disease, and the potential benefits of complement targeting therapies especially for DKD patients.

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Section: The Complement Systemsupporting

confidence: 51%

Section: The Complement System In Diabetic Kidney Diseasementioning

confidence: 99%

Section: The Complement System In Diabetic Kidney Diseasementioning

confidence: 99%

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Complement, a Therapeutic Target in Diabetic Kidney Disease

Budge

Dellepiane

et al. 2021

Front. Med.

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“…DAF is a glycophosphatidylinositol-anchored protein expressed both on podocytes and epithelial tubular cells [39] that regulates the C3 and C5 convertases of the classical and alternative pathways [40]. DAF accelerates decay and inhibits the reformation of surface-bound C3 convertases, together with retraining amplification of the cascade [39]. In streptozotocin-induced diabetic glomerulosclerosis, podocyte-specific deficiency of DAF activated C3a/C3aR signaling, causing actin cytoskeleton rearrangement and podocyte injury [39].…”

Section: Discussionmentioning

confidence: 99%

Urinary complement proteins and risk of end-stage renal disease: quantitative urinary proteomics in patients with type 2 diabetes and biopsy-proven diabetic nephropathy

Zhao

Zhang

Liu

et al. 2021

J Endocrinol Invest

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Purpose To investigate the association between urinary complement proteins and renal outcome in biopsy-proven diabetic nephropathy (DN). Methods Untargeted proteomic and Kyoto Encyclopedia of Genes and Genomes (KEGG) functional analyses and targeted proteomic analysis using parallel reaction-monitoring (PRM)-mass spectrometry was performed to determine the abundance of urinary complement proteins in healthy controls, type 2 diabetes mellitus (T2DM) patients, and patients with T2DM and biopsy-proven DN. The abundance of each urinary complement protein was individually included in Cox proportional hazards models for predicting progression to end-stage renal disease (ESRD). Results Untargeted proteomic and functional analysis using the KEGG showed that differentially expressed urinary proteins were primarily associated with the complement and coagulation cascades. Subsequent urinary complement proteins quantification using PRM showed that urinary abundances of C3, C9, and complement factor H (CFAH) correlated negatively with annual estimated glomerular filtration rate (eGFR) decline, while urinary abundances of C5, decay-accelerating factor (DAF), and CD59 correlated positively with annual rate of eGFR decline. Furthermore, higher urinary abundance of CFAH and lower urinary abundance of DAF were independently associated with greater risk of progression to ESRD. Urinary abundance of CFAH and DAF had a larger area under the curve (AUC) than that of eGFR, proteinuria, or any pathological parameter. Moreover, the model that included CFAH or DAF had a larger AUC than that with only clinical or pathological parameters. Conclusion Urinary abundance of complement proteins was significantly associated with ESRD in patients with T2DM and biopsy-proven DN, indicating that therapeutically targeting the complement pathway may alleviate progression of DN.

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“…The reasons for addressing the role of HO-1 in regulating DAF expression include: (a) the demonstration that HO-1 enhances vascular endothelial resistance to complement-mediated injury induced in vitro through the induction of DAF [ 62 ], (b) the demonstration that DAF confers protection against complement-mediated podocyte injury following the administration of anti-GBM antibody-mediated nephritis in mice (71), (c) the observation that in kidney biopsies from patients with focal segmental glomerulosclerosis (FSGS), complement (C3d) deposition in the glomeruli is paralleled by a reduction in DAF expression [ 104 ], and (d) the demonstration that the distribution of DAF in the rat kidney is restricted to the apical surface of glomerular podocytes [ 72 ] where the loss of DAF promotes complement (C3b) deposition and the development of podocytopathy resembling human FSGS [ 73 , 74 ].…”

Section: Complement and Kidney Diseasementioning

confidence: 99%

Regulation of Complement Activation by Heme Oxygenase-1 (HO-1) in Kidney Injury

Detsika

Lianos

2021

Antioxidants

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Heme oxygenase is a cytoprotective enzyme with strong antioxidant and anti-apoptotic properties. Its cytoprotective role is mainly attributed to its enzymatic activity, which involves the degradation of heme to biliverdin with simultaneous release of carbon monoxide (CO). Recent studies uncovered a new cytoprotective role for heme oxygenase-1 (HO-1) by identifying a regulatory role on the complement control protein decay-accelerating factor. This is a key complement regulatory protein preventing dysregulation or overactivation of complement cascades that can cause kidney injury. Cell-specific targeting of HO-1 induction may, therefore, be a novel approach to attenuate complement-dependent forms of kidney disease.

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Loss of decay-accelerating factor triggers podocyte injury and glomerulosclerosis

Cited by 43 publications

References 76 publications

Complement, a Therapeutic Target in Diabetic Kidney Disease

Complement, a Therapeutic Target in Diabetic Kidney Disease

Urinary complement proteins and risk of end-stage renal disease: quantitative urinary proteomics in patients with type 2 diabetes and biopsy-proven diabetic nephropathy

Regulation of Complement Activation by Heme Oxygenase-1 (HO-1) in Kidney Injury

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