Martin Flamant scite author profile

Rapidly progressive glomerulonephritis (RPGN) is a clinical a morphological expression of severe glomerular injury. Glomerular injury manifests as a proliferative histological pattern (“crescents”) with accumulation of T cells and macrophages, and proliferation of intrinsic glomerular cells. We show de novo induction of heparin-binding epidermal growth factor-like growth factor (HB-EGF) in intrinsic glomerular epithelial cells (podocytes) from both mice and humans with RPGN. HB-EGF induction increases phosphorylation of the EGFR/ErbB1 receptor in mice with RPGN. In HB-EGF-deficient mice, EGFR activation in glomeruli is absent and the course of RPGN is improved. Autocrine HB-EGF induces a phenotypic switch in podocytes in vitro. Conditional deletion of the Egfr gene from podocytes of mice alleviates the severity of RPGN. Pharmacological blockade of EGFR also improves the course of RPGN, even when started 4 days after the induction of experimental RPGN. This suggests that targeting the HB-EGF/EGFR pathway could also be beneficial for treatment of human RPGN.

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Estimating glomerular filtration rate for the full age spectrum from serum creatinine and cystatin C

Pottel

Delanaye

Schaeffner

et al. 2017

Nephrol. Dial. Transplant.

142

158

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Phenotype and Outcome in Hereditary Tubulointerstitial Nephritis Secondary to UMOD Mutations

Bollée¹,

Dahan²,

Flamant³

et al. 2011

112

134

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SummaryBackground UMOD mutations cause familial juvenile hyperuricemic nephropathy (FJHN) and medullary cystic kidney disease (MCKD), although these phenotypes are nonspecific.Design, setting, participants, & measurements We reviewed cases of UMOD mutations diagnosed in the genetic laboratories of Necker Hospital (Paris, France) and of Université Catholique de Louvain (Brussels, Belgium). We also analyzed patients with MCKD/FJHN but no UMOD mutation. To determine thresholds for hyperuricemia and uric-acid excretion fraction (UAEF) according to GFR, these parameters were analyzed in 1097 patients with various renal diseases and renal function levels.Results Thirty-seven distinct UMOD mutations were found in 109 patients from 45 families, all in exon 4 or 5 except for three novel mutations in exon 8. Median renal survival was 54 years. The type of mutation had a modest effect on renal survival, and intrafamilial variability was high. Detailed data available in 70 patients showed renal cysts in 24 (34.3%) of nonspecific localization in most patients. Uricemia was Ͼ75th percentile in 31 (71.4%) of 42 patients not under dialysis or allopurinol therapy. UAEF (n ϭ 27) was Ͻ75th percentile in 70.4%. Among 136 probands with MCKD/FJHN phenotype, UMOD mutation was found in 24 (17.8%). Phenotype was not accurately predictive of UMOD mutation. Six probands had HNF1B mutations.Conclusions Hyperuricemia disproportionate to renal function represents the hallmark of renal disease caused by UMOD mutation. Renal survival is highly variable in patients with UMOD mutation. Our data also add novel insights into the interpretation of uricemia and UAEF in patients with chronic kidney diseases.

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Transglutaminase is essential for IgA nephropathy development acting through IgA receptors

et al. 2012

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Change in albuminuria and subsequent risk of end-stage kidney disease: an individual participant-level consortium meta-analysis of observational studies

Coresh¹,

Heerspink²,

Sang³

et al. 2019

The Lancet Diabetes & Endocrinology

213

135

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Background: There is strong biologic plausibility to support change in albuminuria as a surrogate endpoint for progression of chronic kidney disease (CKD), but empirical evidence to supports its validity in epidemiologic studies is lacking. Methods: We analyzed 28 cohorts including 693,816 individuals (80% with diabetes) and 7,461 end-stage kidney disease (ESKD) events, defined as initiation of kidney replacement therapy. Percent change in albuminuria was quantified during a baseline period of 1, 2 and 3 years using linear regression. Associations with subsequent ESKD were quantified using Cox regression in Coresh et al.

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Urinary ammonia and long-term outcomes in chronic kidney disease

Vallet

Metzger

Haymann

et al. 2015

Kidney International

124

119

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Discoidin Domain Receptor 1 Null Mice Are Protected against Hypertension-Induced Renal Disease

et al. 2006

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A frequent complication of hypertension is the development of chronic renal failure. This pathology usually is initiated by inflammatory events and is characterized by the abnormal accumulation of collagens within the renal tissue. The purpose of this study was to investigate the role of discoidin domain receptor 1 (DDR1), a nonintegrin collagen receptor that displays tyrosine-kinase activity, in the development of renal fibrosis. To this end, hypertension was induced with angiotensin in mice that were genetically deficient of DDR1 and in wild-type controls. After 4 or 6 wk of angiotensin II administration, wild-type mice developed hypertension that was associated with perivascular inflammation, glomerular sclerosis, and proteinuria. Systolic pressure increase was similar in the DDR1-deficient mice, but the histologic lesions of glomerular fibrosis and inflammation were significantly blunted and proteinuria was markedly prevented. Immunostaining for lymphocytes, macrophages, and collagens I and IV was prominent in the renal cortex of wild-type mice but substantially reduced in DDR1 null mice. In separate experiments, renal cortical slices of DDR1 null mice showed a blunted response of chemokines to LPS that was accompanied by a considerable protection against the LPS-induced mortality. These results indicate the importance of DDR1 in mediating inflammation and fibrosis. Use of DDR1 inhibitors could provide a completely novel therapeutic approach against diseases that have these combined pathologies. H ypertension frequently is complicated by the development of chronic renal failure, a complex pathology that is initiated by inflammatory events that evolve to increased synthesis and accumulation of extracellular matrix (ECM; mainly collagens) within the renal tissue and lead over time to loss of function and ESRD. To date, no efficient treatment that can stop or, even more desirable, reverse the decline of renal function exists. Therefore, the understanding of the systems and/or mechanisms that are involved in the development of renal vascular inflammation and fibrosis will provide valuable information to design specific pharmacologic targets to treat this incurable disease.Important advancements have been made regarding the mechanisms that are involved in the development of chronic renal failure. These studies focused mainly in the systems or agents that promote ECM synthesis and progression of renal disease. We and other investigators, for instance, clearly identified and characterized the signaling pathways that vasoconstrictor peptides are using to activate collagen synthesis (1-4). Less is known about the mechanisms regarding the postsynthesis regulation of ECM, such as matrix anchoring and interactions with the cell membrane.Among the systems that interact with the ECM are the discoidin domain receptors (DDR). They are the first identified receptor tyrosine kinases that bind directly to the ECM (5). DDR1 binds all types of collagens and is widely expressed in a variety of tissues, including vascular smooth m...

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Martin Flamant

Maintenance of Remission Among Patients With Crohn's Disease on Antimetabolite Therapy After Infliximab Therapy Is Stopped

Epidermal growth factor receptor promotes glomerular injury and renal failure in rapidly progressive crescentic glomerulonephritis

Estimating glomerular filtration rate for the full age spectrum from serum creatinine and cystatin C

Phenotype and Outcome in Hereditary Tubulointerstitial Nephritis Secondary to UMOD Mutations

Transglutaminase is essential for IgA nephropathy development acting through IgA receptors

Change in albuminuria and subsequent risk of end-stage kidney disease: an individual participant-level consortium meta-analysis of observational studies

Urinary ammonia and long-term outcomes in chronic kidney disease

Discoidin Domain Receptor 1 Null Mice Are Protected against Hypertension-Induced Renal Disease

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