Your search keyword '"Vermorel, Agathe"' showing total 14 results

1. WARS1, TYMP and GBP1 display a distinctive microcirculation pattern by immunohistochemistry during antibody-mediated rejection in kidney transplantation

Author

Chauveau, Bertrand, Garric, Antoine, Di Tommaso, Sylvaine, Raymond, Anne-Aurélie, Visentin, Jonathan, Vermorel, Agathe, Dugot-Senant, Nathalie, Déchanet-Merville, Julie, Duong Van Huyen, Jean-Paul, Rabant, Marion, Couzi, Lionel, Saltel, Frédéric, and Merville, Pierre

Published

2022

2. Development and validation of an optimized integrative model using urinary chemokines for noninvasive diagnosis of acute allograft rejection

Author

Tinel, Claire, Devresse, Arnaud, Vermorel, Agathe, Sauvaget, Virginia, Marx, David, Avettand-Fenoel, Véronique, Amrouche, Lucile, Timsit, Marc-Olivier, Snanoudj, Renaud, Caillard, Sophie, Moulin, Bruno, Olagne, Jérome, Essig, Marie, Gwinner, Wilfried, Naesens, Maarten, Marquet, Pierre, Legendre, Christophe, Terzi, Fabiola, Rabant, Marion, and Anglicheau, Dany

Published

2020

3. In situ multiplex immunofluorescence analysis of the inflammatory burden in kidney allograft rejection: A new tool to characterize the alloimmune response

Author

Calvani, Julien, Terada, Megumi, Lesaffre, Corinne, Eloudzeri, Maëva, Lamarthée, Baptiste, Burger, Carole, Tinel, Claire, Anglicheau, Dany, Vermorel, Agathe, Couzi, Lionel, Loupy, Alexandre, Duong Van Huyen, Jean-Paul, Bruneval, Patrick, and Rabant, Marion

Published

2020

4. COVID-19 morbidity decreases with tixagevimab–cilgavimab preexposure prophylaxis in kidney transplant recipient nonresponders or low-vaccine responders

Author

Kaminski, Hannah, Gigan, Mickael, Vermorel, Agathe, Charrier, Manon, Guirle, Laura, Jambon, Frederic, Lacapère, Arthur, Ménard, Coline, Moreau, Karine, Neau-Cransac, Martine, Novion, Marine, Pribat, Frederique, Taton, Benjamin, Borde, Sébastien, Burguet, Laure, Martinez, Charlie, Jasiek, Magali, D’Halluin, Pauline, Lafon, Marie-Edith, Merville, Pierre, and Couzi, Lionel

Published

2022

5. Renal involvement is frequent in adults with primary mitochondrial disorders: an observational study.

Author

Bakis, Hugo, Trimouille, Aurélien, Vermorel, Agathe, Goizet, Cyril, Belaroussi, Yaniss, Schutz, Sacha, Solé, Guilhem, Combe, Christian, Martin-Negrier, Marie-Laure, and Rigothier, Claire

Subjects

MITOCHONDRIAL pathology, KIDNEY glomerulus diseases, NUCLEAR DNA, MITOCHONDRIAL DNA, ADULTS

Abstract

Background Mitochondrial functions are controlled by genes of both mitochondrial and nuclear DNA. Pathogenic variants affecting any of these are responsible for primary mitochondrial disorders (MIDs), which can be diagnosed during adulthood. Kidney functions are highly dependent on mitochondrial respiration. However, the prevalence of MID-associated nephropathies (MIDANs) is unknown in the adult population. We aimed to address this point and to provide a full characterization of MIDANs in this population. Methods We retrospectively included for observational study adults (≥16 years of age) with genetically diagnosed MID between 2000 and 2020 in our tertiary care academic centre when they had a chronic kidney disease (CKD) evaluation. MIDANs were ascertained by CKD occurring in MIDs. The phenotypic, biological, histopathological and genotypic characteristics were recorded from the medical charts. Results We included 80 MID-affected adults and ascertained MIDANs in 28/80 (35%). Kidney diseases under the care of a nephrologist occurred in only 14/28 (50%) of the adults with MIDAN. MIDANs were tubulointerstitial nephropathy in 14/28 patients (50%) and glomerular diseases in 9/28 (32.1%). In adults with MID, MIDAN was negatively associated with higher albumin levels {odds ratio [OR] 0.79 [95% confidence interval (CI) 0.67–0.95]} and vision abnormalities [OR 0.17 (95% CI 0.03–0.94)] and positively associated with hypertension [OR 4.23 (95% CI 1.04–17.17)]. Conclusion MIDANs are frequent among adult MIDs. They are mostly represented by tubulointerstitial nephropathy or glomerular disease. Vision abnormalities, hypertension and albumin levels were independently associated with MIDANs. Our results pave the way for prospective studies investigating the prevalence of MIDANs among undetermined kidney disease populations. [ABSTRACT FROM AUTHOR]

Published

2023

6. The Proteome of Antibody-Mediated Rejection: From Glomerulitis to Transplant Glomerulopathy.

Author

Chauveau, Bertrand, Raymond, Anne-Aurélie, Di Tommaso, Sylvaine, Visentin, Jonathan, Vermorel, Agathe, Dugot-Senant, Nathalie, Dourthe, Cyril, Dupuy, Jean-William, Déchanet-Merville, Julie, Duong Van Huyen, Jean-Paul, Rabant, Marion, Couzi, Lionel, Saltel, Frédéric, and Merville, Pierre

Subjects

GRAFT rejection, KIDNEY failure, INTERFERON gamma, TYPE I interferons, TRANSPLANTATION of organs, tissues, etc., KIDNEY transplantation

Abstract

Antibody-mediated rejection (ABMR) is the leading cause of allograft failure in kidney transplantation. Its histological hallmark is represented by lesions of glomerulitis i.e., inflammatory cells within glomeruli. Current therapies for ABMR fail to prevent chronic allograft damage i.e., transplant glomerulopathy, leading to allograft loss. We used laser microdissection of glomeruli from formalin-fixed allograft biopsies combined with mass spectrometry-based proteomics to describe the proteome modification of 11 active and 10 chronic active ABMR cases compared to 8 stable graft controls. Of 1335 detected proteins, 77 were deregulated in glomerulitis compared to stable grafts, particularly involved in cellular stress mediated by interferons type I and II, leukocyte activation and microcirculation remodeling. Three proteins extracted from this protein profile, TYMP, WARS1 and GBP1, showed a consistent overexpression by immunohistochemistry in glomerular endothelial cells that may represent relevant markers of endothelial stress during active ABMR. In transplant glomerulopathy, 137 proteins were deregulated, which favor a complement-mediated mechanism, wound healing processes through coagulation activation and ultimately a remodeling of the glomerular extracellular matrix, as observed by light microscopy. This study brings novel information on glomerular proteomics of ABMR in kidney transplantation, and highlights potential targets of diagnostic and therapeutic interest. [ABSTRACT FROM AUTHOR]

Published

2022

7. Multisystem T-cell Chronic Active Epstein-Barr Virus Infection: From the Eye to the Kidney.

Author

Vial, Guillaume, Barthod, Laure, Schneider, Sophie, Mercié, Patrick, Duffau, Pierre, Vermorel, Agathe, and Ribeiro, Emmanuel

Subjects

EPSTEIN-Barr virus diseases, EYE infections, T cells, LYMPHOPROLIFERATIVE disorders, EPSTEIN-Barr virus

Abstract

Chronic active Epstein-Barr virus (CAEBV) infection is usually a fatal disease associated with clonal proliferation of EBV-infected T or NK cells. We present the case of a 33-year-old Peruvian patient who developed a multisystem CAEBV, notably responsible for exceptional ophthalmological and renal damage. We describe the clinicopathological features of EBV-induced lymphoproliferative disorder. [ABSTRACT FROM AUTHOR]

Published

2022

8. Selectins impair regulatory T cell function and contribute to systemic lupus erythematosus pathogenesis.

Author

Scherlinger, Marc, Guillotin, Vivien, Douchet, Isabelle, Vacher, Pierre, Boizard-Moracchini, Andréa, Guegan, Jean-Philippe, Garreau, Anne, Merillon, Nathalie, Vermorel, Agathe, Ribeiro, Emmanuel, Machelart, Irène, Lazaro, Estibaliz, Couzi, Lionel, Duffau, Pierre, Barnetche, Thomas, Pellegrin, Jean-Luc, Viallard, Jean-François, Saleh, Maya, Schaeverbeke, Thierry, and Legembre, Patrick

Subjects

REGULATORY T cells, SYSTEMIC lupus erythematosus, CELL physiology, P-selectin glycoprotein ligand-1, SELECTINS, CELL aggregation, T helper cells

Abstract

P-selectin as a treatment for lupus: Dysfunctional regulatory T (Treg) cells are known to be involved in the pathogenesis of systemic lupus erythematosus (SLE), but the mechanisms mediating Treg cell dysfunction are not clear. Here, Scherlinger et al. demonstrated that platelets can impair Treg cell function after forming aggregates mediated by platelet (P)–selectin expression on platelets and P-selectin glycoprotein ligand-1 (PSGL-1) expression on Treg cells. Treg cells aggregated more frequently with platelets from individuals with active SLE as compared to healthy donors. In addition, blocking the interaction between P-selectin and PSGL-1 reduced disease severity in a mouse model of SLE. Thus, the P-selectin/PSGL-1 axis may represent a therapeutic target for SLE. Systemic lupus erythematosus (SLE) is a systemic autoimmune disease characterized by a loss of tolerance toward self-nucleic acids, autoantibody production, interferon expression and signaling, and a defect in the regulatory T (Treg) cell compartment. In this work, we identified that platelets from patients with active SLE preferentially interacted with Treg cells via the P-selectin/P-selectin glycoprotein ligand-1 (PSGL-1) axis. Selectin interaction with PSGL-1 blocked the regulatory and suppressive properties of Treg cells and particularly follicular Treg cells by triggering Syk phosphorylation and an increase in intracytosolic calcium. Mechanistically, P-selectin engagement on Treg cells induced a down-regulation of the transforming growth factor–β axis, altering the phenotype of Treg cells and limiting their immunosuppressive responses. In patients with SLE, we found an up-regulation of P- and E-selectin both on microparticles and in their soluble forms that correlated with disease activity. Last, blocking P-selectin in a mouse model of SLE improved cardinal features of the disease, such as anti-dsDNA antibody concentrations and kidney pathology. Overall, our results identify a P-selectin–dependent pathway that is active in patients with SLE and validate it as a potential therapeutic avenue. [ABSTRACT FROM AUTHOR]

Published

2021

9. Deciphering the Prognostic and Predictive Value of Urinary CXCL10 in Kidney Recipients With BK Virus Reactivation.

Author

Tinel, Claire, Vermorel, Agathe, Picciotto, Daniela, Morin, Lise, Devresse, Arnaud, Sauvaget, Virginia, Lebreton, Xavier, Aouni, Laïla, Prié, Dominique, Brabant, Séverine, Avettand-Fenoel, Véronique, Scemla, Anne, Timsit, Marc Olivier, Snanoudj, Renaud, Legendre, Christophe, Terzi, Fabiola, Rabant, Marion, and Anglicheau, Dany

Subjects

PROGNOSIS, VIRUS reactivation, INFLAMMATION, VIRAL load, KIDNEY transplantation, BK virus

Abstract

BK virus (BKV) replication increases urinary chemokine C-X-C motif ligand 10 (uCXCL10) levels in kidney transplant recipients (KTRs). Here, we investigated uCXCL10 levels across different stages of BKV replication as a prognostic and predictive marker for functional decline in KTRs after BKV-DNAemia. uCXCL10 was assessed in a cross-sectional study (474 paired urine/blood/biopsy samples and a longitudinal study (1,184 samples from 60 KTRs with BKV-DNAemia). uCXCL10 levels gradually increased with urine (P-value < 0.0001) and blood BKV viral load (P < 0.05) but were similar in the viruria and no BKV groups (P > 0.99). In viremic patients, uCXCL10 at biopsy was associated with graft functional decline [HR = 1.65, 95% CI (1.08–2.51), P = 0.02], irrespective of baseline eGFR, blood viral load, or BKVN diagnosis. uCXL10/cr (threshold: 12.86 ng/mmol) discriminated patients with a low risk of graft function decline from high-risk patients (P = 0.01). In the longitudinal study, the uCXCL10 and BKV-DNAemia trajectories were superimposable. Stratification using the same uCXCL10/cr threshold at first viremia predicted the subsequent inflammatory response, assessed by time-adjusted uCXCL10/cr AUC (P < 0.001), and graft functional decline (P = 0.03). In KTRs, uCXCL10 increases in BKV-DNAemia but not in isolated viruria. uCXCL10/cr is a prognostic biomarker of eGFR decrease, and a 12.86 ng/ml threshold predicts higher inflammatory burdens and poor renal outcomes. [ABSTRACT FROM AUTHOR]

Published

2020

10. Adult onset tubulo‐interstitial nephropathy in MT‐ND5‐related phenotypes.

Author

Bakis, Hugo, Trimouille, Aurélien, Vermorel, Agathe, Redonnet, Isabelle, Goizet, Cyril, Boulestreau, Romain, Lacombe, Didier, Combe, Christian, Martin‐Négrier, Marie‐Laure, and Rigothier, Claire

Subjects

KIDNEY diseases, LEFT ventricular hypertrophy, MITOCHONDRIAL pathology, CHRONIC kidney failure, MATHEMATICAL complexes, EXTRACELLULAR fluid

Abstract

Kidney is a highly adenosine triphosphate dependent organ in human body. Healthy and functional mitochondria are essential for normal kidney function. Clinical and genetic variability are the hallmarks of mitochondrial disorders. We report here the involvement of two MT‐ND5 pathogenic variants encoding for ND5 subunit of respiratory chain complex I, the m.13513G>A and the m.13514A>G, in adult‐onset kidney disease in three unrelated patients. The first patient had myopathy encephalopathy lactic acidosis and stroke syndrome, left ventricular hypertrophy with Wolff‐Parkinson‐White syndrome and tubulo‐interstitial kidney disease. The second presented Leber hereditary optic neuropathy associated with tubulo‐interstitial kidney disease. The third presented with an isolated chronic tubulo‐interstitial kidney disease. These mutations have never been associated with adulthood mitochondrial nephropathy. These case reports highlight the importance to consider mitochondrial dysfunction in tubulo‐interstitial kidney disease. [ABSTRACT FROM AUTHOR]

Published

2020

11. No clinical benefit of rapid versus gradual tapering of immunosuppression to treat sustained BK virus viremia after kidney transplantation: a single‐center experience.

Author

Devresse, Arnaud, Tinel, Claire, Vermorel, Agathe, Snanoudj, Renaud, Morin, Lise, Avettand‐Fenoel, Véronique, Amrouche, Lucile, Scemla, Anne, Zuber, Julien, Legendre, Christophe, Rabant, Marion, and Anglicheau, Dany

Subjects

BK virus, KIDNEY transplantation, KIDNEY diseases, VIREMIA, IMMUNOSUPPRESSION, MYCOPHENOLIC acid

Abstract

Summary: Immunosuppressive drug tapering is currently the recommended treatment of BK virus (BKV) viremia after kidney transplantation; however, its exact modalities remain unclear. We retrospectively compared two consecutive strategies in 111 patients with sustained viremia: a gradual monitoring/tapering group (GT, n = 57) before 2012 and a rapid monitoring/tapering group (RT, n = 54) after 2012. At viremia diagnosis, the dose of mycophenolic acid (MPA) and tacrolimus levels (T0) were similar among patient groups. However, following onset, the dose of MPA at 1 month (P = 0.002) and 3 months (P = 0.005) and Tac T0 at 1 month (P = 0.030) and 3 months (P = 0.006) were lower in the RT group. This rapid minimization shortened BKV viremia (P < 0.001) and resulted in a better protection of graft function in patients with confirmed BKV‐associated nephropathy (P = 0.033) without impacting 5‐year graft survival. Survival without rejection was similar (P = 0.571), but the RT group had increased the development of de novo donor‐specific antibodies (dnDSAs; P < 0.001). Multivariate Cox analysis identified basiliximab versus Thymoglobulin® induction [hazard ratio (HR), 3.090; P = 0.001] and the RT strategy (HR, 6.021; P = 0.002) as independently associated with dnDSAs. Compared to a gradual tapering, rapid immunosuppression tapering to treat sustained BKV viremia does not improve medium‐term clinical outcome but increases the risk of developing dnDSAs. [ABSTRACT FROM AUTHOR]

Published

2019

12. Idiopathic Nephrotic Syndrome: Characteristics and Identification of Prognostic Factors.

Author

Dumas De La Roque, Charlotte, Prezelin-Reydit, Mathilde, Vermorel, Agathe, Lepreux, Sébastien, Deminière, Colette, Combe, Christian, and Rigothier, Claire

Subjects

NEPHROTIC syndrome, FOCAL segmental glomerulosclerosis, DISEASE relapse, KIDNEY transplantation, ADRENOCORTICAL hormones, RENAL biopsy, PATIENTS, PROGNOSIS, DISEASE risk factors, THERAPEUTICS

Abstract

There are various histopathological forms of idiopathic nephrotic syndrome, including minimal change disease (MCD) and focal segmental glomerulosclerosis (FSGS). Whereas some relapse predictor factors have been identified in renal transplantation, the clinical future of idiopathic nephrotic syndrome in the native kidney remains uncertain. We designed a multicentric retrospective descriptive cohort study including all patients aged 15 years and over whose renal biopsy confirmed MCD or FSGS between January 2007 and December 2014. We studied 165 patients with idiopathic nephrotic syndrome; 97 with MCD and 68 with FSGS. In the MCD cohort, 91.7% of patients were treated with corticosteroids for a median total duration of 13 months. During 45 months of follow-up, 92.8% of patients achieved remission and 45.5% experienced relapse. In this cohort, 5% of patients experienced terminal kidney disease. With respect to FSGS patients, 51.5% were treated with corticosteroids for a median total duration of 15 months. During 66 months of follow-up, 73.5% of patients achieved remission and 20% experienced relapse. In this cohort, 26.5% of patients experienced terminal kidney disease. No statistical association was observed between clinical and biological initial presentation and relapse occurrence. This study describes the characteristics of a cohort of patients with the nephrotic idiopathic syndromes of MCD and FSGS from the time of renal biopsy and throughout follow-up. [ABSTRACT FROM AUTHOR]

Published

2018

13. Renal involvement is frequent in adults with primary mitochondrial disorders: an observational study.

Author

Bakis H, Trimouille A, Vermorel A, Goizet C, Belaroussi Y, Schutz S, Solé G, Combe C, Martin-Negrier ML, and Rigothier C

Abstract

Background: Mitochondrial functions are controlled by genes of both mitochondrial and nuclear DNA. Pathogenic variants affecting any of these are responsible for primary mitochondrial disorders (MIDs), which can be diagnosed during adulthood. Kidney functions are highly dependent on mitochondrial respiration. However, the prevalence of MID-associated nephropathies (MIDANs) is unknown in the adult population. We aimed to address this point and to provide a full characterization of MIDANs in this population., Methods: We retrospectively included for observational study adults (≥16 years of age) with genetically diagnosed MID between 2000 and 2020 in our tertiary care academic centre when they had a chronic kidney disease (CKD) evaluation. MIDANs were ascertained by CKD occurring in MIDs. The phenotypic, biological, histopathological and genotypic characteristics were recorded from the medical charts., Results: We included 80 MID-affected adults and ascertained MIDANs in 28/80 (35%). Kidney diseases under the care of a nephrologist occurred in only 14/28 (50%) of the adults with MIDAN. MIDANs were tubulointerstitial nephropathy in 14/28 patients (50%) and glomerular diseases in 9/28 (32.1%). In adults with MID, MIDAN was negatively associated with higher albumin levels {odds ratio [OR] 0.79 [95% confidence interval (CI) 0.67-0.95]} and vision abnormalities [OR 0.17 (95% CI 0.03-0.94)] and positively associated with hypertension [OR 4.23 (95% CI 1.04-17.17)]., Conclusion: MIDANs are frequent among adult MIDs. They are mostly represented by tubulointerstitial nephropathy or glomerular disease. Vision abnormalities, hypertension and albumin levels were independently associated with MIDANs. Our results pave the way for prospective studies investigating the prevalence of MIDANs among undetermined kidney disease populations., (© The Author(s) 2022. Published by Oxford University Press on behalf of the ERA.)

Published

2022

14. Magnetic Resonance Elastography as Surrogate Marker of Interstitial Fibrosis in Kidney Transplantation: A Prospective Study.

Author

Chauveau B, Merville P, Soulabaille B, Taton B, Kaminski H, Visentin J, Vermorel A, Bouzgarrou M, Couzi L, and Grenier N

Subjects

Humans, Prospective Studies, Fibrosis, Biomarkers, Elasticity Imaging Techniques methods, Kidney Transplantation adverse effects

Abstract

Background: Fibrosis progression is a major prognosis factor in kidney transplantation. Its assessment requires an allograft biopsy, which remains an invasive procedure at risk of complications., Methods: We assessed renal stiffness by magnetic resonance elastography (MRE) as a surrogate marker of fibrosis in a prospective cohort of kidney transplant recipients compared with the histologic gold standard. Interstitial fibrosis was evaluated by three methods: the semi-quantitative Banff ci score, a visual quantitative evaluation by a pathologist, and a computer-assisted quantitative evaluation. MRE-derived stiffness was assessed at the superior, median, and inferior poles of the allograft., Results: We initially enrolled 73 patients, but only 55 had measurements of their allograft stiffness by MRE before an allograft biopsy. There was no significant correlation between MRE-derived stiffness at the biopsy site and the ci score ( ρ =-0.25, P =0.06) or with the two quantitative assessments (pathologist: ρ =-0.25, P =0.07; computer assisted: ρ =-0.21, P =0.12). We observed negative correlations between the stiffness of both the biopsy site and the whole allograft, with either the glomerulosclerosis percentage ( ρ =-0.32, P =0.02 and ρ =-0.31, P =0.02, respectively) and the overall nephron fibrosis percentage, defined as the mean of the percentages of glomerulosclerosis and interstitial fibrosis ( ρ =-0.30, P =0.02 and ρ =-0.28, P =0.04, respectively). At patient level, mean MRE-derived stiffness was similar across the three poles of the allograft (±0.25 kPa). However, a high variability of mean stiffness was found between patients, suggesting a strong influence of confounding factors. Finally, no significant correlation was found between mean MRE-derived stiffness and the slope of eGFR ( P =0.08)., Conclusions: MRE-derived stiffness does not directly reflect the extent of fibrosis in kidney transplantation., Competing Interests: L. Couzi reports consultancy for Astellas, Biotest, Hansa, Novartis, and Otsuka; and honoraria from Astellas, Biotest; Hansa, and Otsuka. P. Merville reports consultancy for Astellas and BMS; research funding from Astellas; honoraria from CSL Behring and Sanofi; and an advisory or leadership role for BMS and Novartis. J. Visentin reports being the inventor on a patent concerning a method to quantify anti-HLA antibodies in patient samples using surface plasmon resonance (WO 2017/168083). All remaining authors have nothing to disclose., (Copyright © 2022 by the American Society of Nephrology.)

Published

2022