Your search keyword '"Ezzedine, Khaled"' showing total 13 results

1. Type-1 cytokines regulate MMP-9 production and E-cadherin disruption to promote melanocyte loss in vitiligo.

Author

Boukhedouni N, Martins C, Darrigade AS, Drullion C, Rambert J, Barrault C, Garnier J, Jacquemin C, Thiolat D, Lucchese F, Morel F, Ezzedine K, Taieb A, Bernard FX, Seneschal J, and Boniface K

Subjects

Animals, Humans, Keratinocytes metabolism, Keratinocytes pathology, Melanocytes pathology, Mice, Cadherins metabolism, Interferon-gamma metabolism, MAP Kinase Signaling System, Matrix Metalloproteinase 9 biosynthesis, Melanocytes metabolism, Tumor Necrosis Factor-alpha metabolism, Vitiligo metabolism

Abstract

Loss of melanocytes is the pathological hallmark of vitiligo, a chronic inflammatory skin depigmenting disorder induced by exaggerated immune response, including autoreactive CD8 T cells producing high levels of type 1 cytokines. However, the interplay between this inflammatory response and melanocyte disappearance remains to be fully characterized. Here, we demonstrate that vitiligo skin contains a significant proportion of suprabasal melanocytes, associated with disruption of E-cadherin expression, a major protein involved in melanocyte adhesion. This phenomenon is also observed in lesional psoriatic skin. Importantly, apoptotic melanocytes were mainly observed once cells were detached from the basal layer of the epidermis, suggesting that additional mechanism(s) could be involved in melanocyte loss. The type 1 cytokines IFN-γ and TNF-α induce melanocyte detachment through E-cadherin disruption and the release of its soluble form, partly due to MMP-9. The levels of MMP-9 are increased in the skin and sera of patients with vitiligo, and MMP-9 is produced by keratinocytes in response to IFN-γ and TNF-α. Inhibition of MMP-9 or the JAK/STAT signaling pathway prevents melanocyte detachment in vitro and in vivo. Therefore, stabilization of melanocytes in the basal layer of the epidermis by preventing E-cadherin disruption appears promising for the prevention of depigmentation occurring in vitiligo and during chronic skin inflammation.

Published

2020

2. Altered E-Cadherin Levels and Distribution in Melanocytes Precede Clinical Manifestations of Vitiligo.

Author

Wagner RY, Luciani F, Cario-André M, Rubod A, Petit V, Benzekri L, Ezzedine K, Lepreux S, Steingrimsson E, Taieb A, Gauthier Y, Larue L, and Delmas V

Subjects

Adult, Aged, Analysis of Variance, Animals, Biopsy, Needle, Case-Control Studies, Cells, Cultured, Disease Models, Animal, Epidermis pathology, Humans, Immunohistochemistry, Melanocytes pathology, Mice, Mice, Inbred C57BL, Mice, Transgenic, Middle Aged, Oxidative Stress physiology, Reference Values, Risk Factors, Sensitivity and Specificity, Severity of Illness Index, Vitiligo pathology, Young Adult, Cadherins metabolism, Epidermis metabolism, Melanocytes metabolism, Vitiligo metabolism

Abstract

Vitiligo is the most common depigmenting disorder resulting from the loss of melanocytes from the basal epidermal layer. The pathogenesis of the disease is likely multifactorial and involves autoimmune causes, as well as oxidative and mechanical stress. It is important to identify early events in vitiligo to clarify pathogenesis, improve diagnosis, and inform therapy. Here, we show that E-cadherin (Ecad), which mediates the adhesion between melanocytes and keratinocytes in the epidermis, is absent from or discontinuously distributed across melanocyte membranes of vitiligo patients long before clinical lesions appear. This abnormality is associated with the detachment of the melanocytes from the basal to the suprabasal layers in the epidermis. Using human epidermal reconstructed skin and mouse models with normal or defective Ecad expression in melanocytes, we demonstrated that Ecad is required for melanocyte adhesiveness to the basal layer under oxidative and mechanical stress, establishing a link between silent/preclinical, cell-autonomous defects in vitiligo melanocytes and known environmental stressors accelerating disease expression. Our results implicate a primary predisposing skin defect affecting melanocyte adhesiveness that, under stress conditions, leads to disappearance of melanocytes and clinical vitiligo. Melanocyte adhesiveness is thus a potential target for therapy aiming at disease stabilization.

Published

2015

3. Study of CCN3 (NOV) and DDR1 in normal melanocytes and vitiligo skin.

Author

Ricard AS, Pain C, Daubos A, Ezzedine K, Lamrissi-Garcia I, Bibeyran A, Guyonnet-Dupérat V, Taieb A, and Cario-André M

Subjects

Adult, Cell Adhesion, Collagen Type IV metabolism, Discoidin Domain Receptor 1, Female, Gene Silencing, Humans, Male, Middle Aged, Melanocytes metabolism, Nephroblastoma Overexpressed Protein metabolism, Receptor Protein-Tyrosine Kinases metabolism, Vitiligo metabolism

Abstract

We have hypothesised that melanocytes disappear in vitiligo because they are weakly attached to the epidermal basal membrane (melanocytorrhagy). In the epidermis, attachment of melanocytes to collagen IV is mediated through DDR1, which is under the control of CCN3. DDR1 genetic variants have been associated with vitiligo in patients of different ethnic origin. In vitro studies have shown that inhibition of CCN3 induces the detachment of melanocytes. We have studied in parallel the expression of CCN3 and DDR1 in lesional and perilesional skin of patients with vitiligo and the impact of the silencing of CCN3 and DDR1 in normal human melanocytes on their behaviour in epidermal reconstructs. Our in vivo study provides evidence of a dysregulation of the DDR1-CCN3 interaction in vitiligo skin as melanocytes remaining in perilesional skin did not express CCN3. Expression of DDR1 was decreased in lesional versus perilesional vitiligo skin in the majority of patients, and the expression of collagen IV was found decreased in all patients. Silencing of CCN3 in melanocytes induced a significant inhibition of cell adhesion to collagen IV whereas melanocytes transduced with shDDR1 still adhered well on collagen IV and did not increase melanocyte loss in epidermal reconstructs as compared with normal melanocytes. Melanocyte detachment was observed but not in all reconstructs using CCN3 silenced melanocytes. Overall, our study confirms that a downregulation of CCN3 is implicated in melanocyte adhesion in part through DDR1. In vitiligo skin, the interaction of CCN3 with other molecules, such as TGFβ and CCN2, needs to be addressed., (© 2012 John Wiley & Sons A/S.)

Published

2012

4. Ritlecitinib, a JAK3/TEC family kinase inhibitor, stabilizes active lesions and repigments stable lesions in vitiligo.

Author

Yamaguchi, Yuji, Peeva, Elena, Duca, Ester, Facheris, Paola, Bar, Jonathan, Shore, Ronald, Cox, Lori, Sloan, Abigail, Thaçi, Diamant, Ganesan, Anand, Han, George, Ezzedine, Khaled, Ye, Zhan, and Guttman-Yassky, Emma

Subjects

Biomarkers, JAK inhibitor, Non-segmental vitiligo, Ritlecitinib, Vitiligo, Humans, Vitiligo, Male, Female, Adult, Janus Kinase 3, Middle Aged, Protein Kinase Inhibitors, Treatment Outcome, Chemokine CXCL9, Chemokine CCL5, Young Adult, B7-H1 Antigen, Melanocytes, Double-Blind Method, Skin Pigmentation, Administration, Oral, Interferon-gamma

Abstract

The efficacy of ritlecitinib, an oral JAK3/TEC family kinase inhibitor, on active and stable lesions was evaluated in patients with active non-segmental vitiligo in a phase 2b trial (NCT03715829). Patients were randomized to placebo or daily ritlecitinib 50 mg (with or without 4-week 100-mg or 200-mg loading dose), 30 mg, or 10 mg for 24 weeks. Active lesions showed greater baseline expression of inflammatory/immune markers IFNG and CCL5, levels of CD103, and T-cell infiltrates than stable lesions. Patients with more active than stable vitiligo lesions showed higher baseline serum levels of CXCL9 and PD-L1, while patients with more stable than active lesions showed higher baseline serum levels of HO-1. At Week 24, ritlecitinib 50 mg significantly stabilized mean percent change from baseline in depigmentation extent in both active lesions and stable lesions vs. placebo-response, with stable lesions showing greater repigmentation. After 24 weeks of treatment, ritlecitinib 50 mg increased expression of melanocyte markers in stable lesions, while Th1/Th2-related and co-stimulatory molecules decreased significantly in both stable and active lesions. Serum from patients with more active than stable lesions showed decreased levels of ICOS and NK cell activation markers. These data, confirmed at transcription/protein levels, indicate that stable lesion repigmentation occurs early with ritlecitinib, while active lesions require stabilization of inflammation first. ClinicalTrials.gov: NCT03715829.

Published

2024

5. Type-1 cytokines regulate MMP-9 production and E-cadherin disruption to promote melanocyte loss in vitiligo

Author

BOUKHEDOUNI, Nesrine, Martins, Christina, Darrigade, Anne-Sophie, Drullion, Claire, RAMBERT, Jérôme, Barrault, Christine, Garnier, Julien, JACQUEMIN, Clement, THIOLAT, Denis, LUCCHESE, Fabienne, MOREL, Franck, Ezzedine, Khaled, Taieb, Alain, Bernard, François-Xavier, Seneschal, Julien, boniface, katia, Boniface1, Katia, Biothérapies des maladies génétiques et cancers, Université Bordeaux Segalen - Bordeaux 2-Institut National de la Santé et de la Recherche Médicale (INSERM), Service de dermatologie Hôpital Saint-André Bordeaux, CHU Bordeaux [Bordeaux], and Université de Bordeaux (UB)

Subjects

Keratinocytes, integumentary system, Tumor Necrosis Factor-alpha, MAP Kinase Signaling System, Vitiligo, [SDV.BC]Life Sciences [q-bio]/Cellular Biology, Cadherins, Mice, Interferon-gamma, Matrix Metalloproteinase 9, Melanocytes, Humans, Animals, Research Article

Abstract

International audience; Loss of melanocytes is the pathological hallmark of vitiligo, a chronic inflammatory skin depigmenting disorder induced by exaggerated immune response, including autoreactive CD8 T cells producing high levels of type 1 cytokines. However, the interplay between this inflammatory response and melanocyte disappearance remains to be fully characterized. Here, we demonstrate that vitiligo skin contains a significant proportion of suprabasal melanocytes, associated with disruption of E-cadherin expression, a major protein involved in melanocyte adhesion. This phenomenon is also observed in lesional psoriatic skin. Importantly, apoptotic melanocytes were mainly observed once cells were detached from the basal layer of the epidermis, suggesting that additional mechanism(s) could be involved in melanocyte loss. The type 1 cytokines IFN-γ and TNF-α induce melanocyte detachment through E-cadherin disruption and the release of its soluble form, partly due to MMP-9. The levels of MMP-9 are increased in the skin and sera of patients with vitiligo, and MMP-9 is produced by keratinocytes in response to IFN-γ and TNF-α. Inhibition of MMP-9 or the JAK/STAT signaling pathway prevents melanocyte detachment in vitro and in vivo. Therefore, stabilization of melanocytes in the basal layer of the epidermis by preventing E-cadherin disruption appears promising for the prevention of depigmentation occurring in vitiligo and during chronic skin inflammation.

Published

2020

6. Vitiligo: A Review.

Author

Bergqvist, Christina and Ezzedine, Khaled

Subjects

VITILIGO, AUTOIMMUNE diseases, MACULES, MELANOCYTES

Abstract

Vitiligo, a common depigmenting skin disorder, has an estimated prevalence of 0.5–2% of the population worldwide. The disease is characterized by the selective loss of melanocytes which results in typical nonscaly, chalky-white macules. In recent years, considerable progress has been made in our understanding of the pathogenesis of vitiligo which is now clearly classified as an autoimmune disease. Vitiligo is often dismissed as a cosmetic problem, although its effects can be psychologically devastating, often with a considerable burden on daily life. In 2011, an international consensus classified segmental vitiligo separately from all other forms of vitiligo, and the term vitiligo was defined to designate all forms of nonsegmental vitiligo. This review summarizes the current knowledge on vitiligo and attempts to give an overview of the future in vitiligo treatment. [ABSTRACT FROM AUTHOR]

Published

2020

7. Epidermal keratin 5 expression and distribution is under dermal influence.

Author

Cario, Muriel, Pain, Catherine, Kaulanjan‐Checkmodine, Priscilla, Masia, Daniela, Delia, Gabriele, Casoli, Vincent, Costet, Pierre, Goussot, Jean‐François, Guyonnet‐Duperat, Véronique, Bibeyran, Alice, Ezzedine, Khaled, Reymermier, Corinne, Andre‐Frei, Valérie, and Taieb, Alain

Subjects

KERATIN, MELANINS, HUMAN skin color, LENTIGO, SKIN grafting

Abstract

Human skin melanin pigmentation is regulated by systemic and local factors. According to the type of melanin produced by melanocytes, the transfer and degradation of melanosomes differ, thus accounting for most variations between ethnicities. We made the surprising observation that in a drastically changed environment, white and black phenotypes are reversible since Caucasian skin grafted onto nude mice can become black with all black phenotypic characteristics. Black xenografts differed essentially from other grafts by the levels of epidermal FGF‐2 and keratin 5. In vitro analysis confirmed that FGF‐2 directly regulates keratin 5. Interestingly, this phenomenon may be involved in human pathology. Keratin 5 mutations in Dowling–Degos Disease (DDD) have already been associated with the pheomelanosome–eumelanosome transition. In a DDD patient, keratin 5 was expressed in the basal and spinous layers, as observed in black xenografts. Furthermore, in a common age‐related hyperpigmentation disorder like senile lentigo (SL), keratin 5 distribution is also altered. In conclusion, modulation of keratin 5 expression and distribution either due to mutations or factors may account for the development of pigmentary disorders. [ABSTRACT FROM AUTHOR]

Published

2020

8. Improvements in immune/melanocyte biomarkers with JAK3/TEC family kinase inhibitor ritlecitinib in vitiligo.

Author

Guttman-Yassky, Emma, Del Duca, Ester, Da Rosa, Joel Correa, Bar, Jonathan, Ezzedine, Khaled, Ye, Zhan, He, Wen, Hyde, Craig, Hassan-Zahraee, Mina, Yamaguchi, Yuji, and Peeva, Elena

Abstract

Vitiligo is an autoimmune depigmenting disorder with no effective and safe treatments. Its pathogenesis is not fully elucidated. This substudy of a randomized, double-blind, placebo-controlled phase 2b trial (NCT03715829) evaluated effects of ritlecitinib, an oral JAK3/TEC family kinase inhibitor, on skin and blood biomarkers in participants with nonsegmental vitiligo (NSV). Sixty-five adults with NSV participated in the substudy and received daily treatment for 24 weeks with placebo (n = 14) or ritlecitinib with or without a 4-week loading dose: 200 (loading dose)/50 mg (n = 13), 100/50 mg (n = 12), 50 mg (n = 11), 30 mg (n = 8), or 10 mg (n = 6). Skin (lesional and nonlesional) biopsy samples were obtained at baseline and at 4 and 24 weeks. Changes from baseline to weeks 4 and 24 in skin and blood molecular and cellular biomarkers were evaluated by RNA sequencing, quantitative real-time PCR, proteomic analysis, and flow cytometry. Ritlecitinib-treated groups showed downregulation of immune biomarkers and upregulation of melanocyte-related markers at weeks 4 and 24 compared to baseline and/or placebo. Significant reductions were seen in CD3+/CD8+ T-cell infiltrates, with significant increases in melanocyte markers (tyrosinase; Melan-A) in NSV lesions in the 50 mg ritlecitinib groups (both P <.05). There was significant, dose-dependent downregulation in T-cell activation, NK, cytotoxic, and regulatory markers in lesional skin (IL-2, IL2-RA, IL-15, CCR7, CD5, CRTAM, NCR1, XCL1, KIR3DL1, FASLG, KLRD; P <.05). T H 1 and T H 2 markers were also downregulated in lesional skin and blood in a dose-dependent manner (P <.05). Changes in immune biomarkers correlated with clinical response. Ritlecitinib significantly downregulated proinflammatory biomarkers and increased melanocyte products in skin and blood of participants with NSV, suggesting its potential in treatment. Ritlecitinib-mediated changes positively correlated with clinical response. [ABSTRACT FROM AUTHOR]

Published

2024

9. Vitiligo.

Author

Ezzedine, Khaled, Eleftheriadou, Viktoria, Whitton, Maxine, and van Geel, Nanja

Subjects

*VITILIGO, *PIGMENTATION disorders, *MELANOCYTES, *HYPOPIGMENTATION, *PROGNOSIS

Abstract

Vitiligo, an acquired pigmentary disorder of unknown origin, is the most frequent cause of depigmentation worldwide, with an estimated prevalence of 1%. The disorder can be psychologically devastating and stigmatising, especially in dark skinned individuals. Vitiligo is clinically characterised by the development of white macules due to the loss of functioning melanocytes in the skin or hair, or both. Two forms of the disease are well recognised: segmental and non-segmental vitiligo (the commonest form). To distinguish between these two forms is of prime importance because therapeutic options and prognosis are quite different. The importance of early treatment and understanding of the profound psychosocial effect of vitiligo will be emphasised throughout this Seminar. [ABSTRACT FROM AUTHOR]

Published

2015

10. Segmental vitiligo as the possible expression of cutaneous somatic mosaicism: implications for common non-segmental vitiligo.

Author

Taïeb, Alain, Morice-Picard, Fanny, Jouary, Thomas, Ezzedine, Khaled, Cario-André, Muriel, and Gauthier, Yvon

Subjects

VITILIGO, PIGMENTATION disorders, AUTOIMMUNE diseases, HYPOTHESIS, MOSAICISM

Abstract

Clinical findings in vitiligo challenge the widely accepted organ specific autoimmune pathomechanisms. We draw the attention to the fact that the distribution of segmental vitiligo (SV) fits in at least a subset of patients a pattern usually associated with cutaneous mosaicism. The association of SV to non-segmental vitiligo (NSV) now confirmed by several observations indicates a continuum between the two subsets with shared predisposing genetic factors, including genes operating specifically in the skin. Some pedigrees associating SV and NSV further suggest a mechanism of loss of heterozygosity for a dominant gene controlling part of the cutaneous phenotype. The mosaic hypothesis applies only to SV and to the rare SV-NSV association, but suggests that predisposing genetic factors in common NSV should also be searched directly in the skin. SV would be a good candidate disease to explore as a proof of principle of a new gene discovery strategy useful for multigenic disorders with organ specificity, applicable in priority to chronic inflammatory skin disorders. [ABSTRACT FROM AUTHOR]

Published

2008

11. Common variants in FOXP1 are associated with generalized vitiligo.

Author

Ying Jin, Birlea, Stanca A, Fain, Pamela R, Mailloux, Christina M, Riccardi, Sheri L, Gowan, Katherine, Holland, Paulene J, Bennett, Dorothy C, Wallace, Margaret R, McCormack, Wayne T, Kemp, E Helen, Gawkrodger, David J, Weetman, Anthony P, Picardo, Mauro, Leone, Giovanni, Taïeb, Alain, Jouary, Thomas, Ezzedine, Khaled, van Geel, Nanny, and Lambert, Jo

Subjects

VITILIGO, GENOMES, AUTOIMMUNE diseases, MELANOCYTES, LINKAGE (Genetics), LINKAGE disequilibrium, GENETICS

Abstract

In a recent genome-wide association study of generalized vitiligo, we identified ten confirmed susceptibility loci. By testing additional loci that showed suggestive association in the genome-wide study, using two replication cohorts of European descent, we observed replicated association of generalized vitiligo with variants at 3p13 encompassing FOXP1 (rs17008723, combined P = 1.04 × 10−8) and with variants at 6q27 encompassing CCR6 (rs6902119, combined P = 3.94 × 10−7). [ABSTRACT FROM AUTHOR]

Published

2010

12. Accelerating bleaching in vitiligo: balancing benefits versus risks.

Author

Seneschal, Julien, Boniface, Katia, Ezzedine, Khaled, and Taieb, Alain

Subjects

VITILIGO, PIGMENTATION disorders, BLEACHING of skin, IMMUNOLOGICAL adjuvants, MELANOCYTES, IMMUNOLOGY of inflammation, AUTOIMMUNITY, THERAPEUTICS

Abstract

While the goal of available treatment in vitiligo is to regain pigmentation, some patients affected by extensive and treatment-resistant vitiligo, with a major social and emotional impact, may benefit from depigmentation therapy. However, results from such therapy may not always be satisfactory. So to achieve better, faster and complete bleaching, Webb et al. propose a synergistic approach that combines topical application of bleaching phenols which targets melanocytes and initiate local inflammation with immune adjuvants so as to obtain an enhanced immune response against remaining melanocytes. This strategy could be reliable, but should be evaluated cautiously in future studies, in terms of potential side effects and induction of undesired autoimmunity. [ABSTRACT FROM AUTHOR]

Published

2014

13. Genome-Wide Analysis Identifies a Quantitative Trait Locus in the MHC Class II Region Associated with Generalized Vitiligo Age of Onset.

Author

Ying Jin, Birlea, Stanca A., Fain, Pamela R., Gowan, Katherine, Riccardi, Sheri L., Holland, Paulene J., Bennett, Dorothy C., Herbstman, Deborah M., Wallace, Margaret R., McCormack, Wayne T., Kemp, E Helen, Gawkrodger, David J., Weetman, Anthony P., Picardo, Mauro, Leone, Giovanni, Taïeb, Alain, Jouary, Thomas, Ezzedine, Khaled, van Geel, Nanny, and Lambert, Jo

Subjects

*VITILIGO, *GENOMES, *MELANOCYTES, *MAJOR histocompatibility complex, *LOCUS (Genetics), *MUCOUS membranes, *DISEASE susceptibility

Abstract

Generalized vitiligo is a common autoimmune disease in which acquired patchy depigmentation of skin, hair, and mucous membranes results from loss of melanocytes from involved areas. Previous genetic analyses have focused on vitiligo susceptibility, and have identified a number of genes involved in disease risk. Age of onset of generalized vitiligo also involves a substantial genetic component, but has not previously been studied systematically. In this study, we report a genome-wide association study of vitiligo age of onset in 1,339 generalized vitiligo patients, with replication in an independent cohort of 677 cases. We identified a quantitative trait locus for vitiligo age of onset in the major histocompatibility complex (MHC) class II region, located near c6orf10-BTNL2 (rs7758128; P=8.14 × 10−11), a region that is also associated with generalized vitiligo susceptibility. In contrast, there was no association of vitiligo age of onset with any other MHC or non-MHC loci that are associated with vitiligo susceptibility. These findings highlight the differing roles played by genes involved in vitiligo susceptibility versus vitiligo age of onset, and illustrate that genome-wide analyses can be used to identify genes involved in quantitative aspects of disease natural history, as well as disease susceptibility per se. [ABSTRACT FROM AUTHOR]

Published

2011