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Dive into the research topics where Fabienne Jaunin is active.

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Featured researches published by Fabienne Jaunin.


Journal of Cell Science | 2006

New insights into the molecular basis of desmoplakin- and desmin-related cardiomyopathies

Karine Lapouge; Lionel Fontao; Marie-France Champliaud; Fabienne Jaunin; Miguel Frias; Bertrand Favre; Denise Paulin; Kathleen J. Green; Luca Borradori

Desmosomes are intercellular adhesive complexes that anchor the intermediate filament cytoskeleton to the cell membrane in epithelia and cardiac muscle cells. The desmosomal component desmoplakin plays a key role in tethering various intermediate filament networks through its C-terminal plakin repeat domain. To gain better insight into the cytoskeletal organization of cardiomyocytes, we investigated the association of desmoplakin with desmin by cell transfection, yeast two-hybrid, and/or in vitro binding assays. The results indicate that the association of desmoplakin with desmin depends on sequences within the linker region and C-terminal extremity of desmoplakin, where the B and C subdomains contribute to efficient binding; a potentially phosphorylatable serine residue in the C-terminal extremity of desmoplakin affects its association with desmin; the interaction of desmoplakin with non-filamentous desmin requires sequences contained within the desmin C-terminal rod portion and tail domain in yeast, whereas in in vitro binding studies the desmin tail is dispensable for association; and mutations in either the C-terminus of desmoplakin or the desmin tail linked to inherited cardiomyopathy seem to impair desmoplakindesmin interaction. These studies increase our understanding of desmoplakin-intermediate filament interactions, which are important for maintenance of cytoarchitecture in cardiomyocytes, and give new insights into the molecular basis of desmoplakin- and desmin-related human diseases.


British Journal of Dermatology | 2005

Bullous pemphigoid antigen 1 isoforms: potential new target autoantigens in multiple sclerosis?

Emmanuel Laffitte; Pierre Burkhard; Lionel Fontao; Fabienne Jaunin; Jean-Hilaire Saurat; Michel Chofflon; Luca Borradori

Background  The simultaneous occurrence of bullous pemphigoid (BP) and multiple sclerosis (MS), two autoimmune diseases involving the skin and the central nervous system (CNS), respectively, has been described.


British Journal of Dermatology | 2001

Autoantibodies to the extracellular and intracellular domain of bullous pemphigoid 180, the putative key autoantigen in bullous pemphigoid, belong predominantly to the IgG1 and IgG4 subclasses

Emmanuel Laffitte; Skaria M; Fabienne Jaunin; Tamm K; Jean-Hilaire Saurat; Bertrand Favre; Luca Borradori

Background Autoantibodies to the extracellular domain (ECD) of bullous pemphigoid (BP) antigen 180 (BP180) are thought to play a crucial part in the pathophysiology of BP.


British Journal of Dermatology | 2001

Plectin, an unusual target antigen in bullous pemphigoid

Emmanuel Laffitte; Bertrand Favre; Lionel Fontao; Riou S; Fabienne Jaunin; Tamm K; Jean-Hilaire Saurat; Luca Borradori

Background  Bullous pemphigoid (BP) is a blistering disease associated with autoantibodies directed against two components of hemidesmosomes, BP180 and BP230.


Cellular Immunology | 1986

Intracellular epidermal interleukin 1-like factors in the human epidermoid carcinoma cell line A431

Conrad Hauser; Jean-Michel Dayer; Fabienne Jaunin; Béatrice de Rochemonteix; Jean-Hilaire Saurat

Normal human epidermal cells produce, in primary culture, activities which stimulate the release of PGE2 and collagenase by dermal fibroblasts; this factor(s) might play an important role in epidermal-dermal interactions. Since these activities were mainly found in the cell lysates with only little being detected in the conditioned media, we investigated further the problem of cell-associated versus released activity in the model of the human epidermoid carcinoma cell line A431. The activities were consistently found in the cell lysate and in the conditioned media only when the cells were leaky. No membrane-associated activities were identified. Purification of the cytosolic activities were identified. Purification of the cytosolic activities yielded two differently charged species both with a MW of approximately 17K. The copurification of PGE2- and collagenase-stimulating activities with thymocyte comitogenic activity suggests a close physiochemical relation to IL-1. The activities described here might therefore correspond to the intracellular counterpart of epidermal IL-1 formerly described as epidermal cell-derived thymocyte activating factor (ETAF) and identified in the conditioned medium of cultured epidermal cells. These observations are of importance when studying the modulation of these activities.


Journal of Investigative Dermatology | 2013

Inhibition of Putative Hyalurosome Platform in Keratinocytes as a Mechanism for Corticosteroid-Induced Epidermal Atrophy

Laurent Barnes; Frédérique Ino; Fabienne Jaunin; Jean-Hilaire Saurat; Gürkan Kaya

The main limitation of using topical corticosteroids in dermatology is their atrophic effects on the skin. We have previously proposed a molecular platform composed of CD44, EGFR, and hyaluronate synthase (HAS) that is functionally defective in dermatoporosis, a chronic cutaneous insufficiency/fragility syndrome. In this study, we explored the molecular mechanisms of the skin atrophy induced by corticosteroids. We observed an important skin atrophy and a significant decrease of hyaluronic acid (HA), its main cell surface receptor CD44, and F-actin in mouse skin treated with topical clobetasol propionate (CP). Human keratinocytes exposed to CP showed an impaired HA secretion and diminished expression of CD44 and HAS3. CP also abolished filopodia of keratinocytes exposed to CP together with a redistribution of CD44 and F-actin depolymerization. We also show that HA fragments of intermediary size (HAFi) induced keratinocyte filopodia and protected them against CP. Topical HAFi induced hyperplasia in mouse epidermis and prevented CP-induced atrophy. Our results suggest that a CD44/EGFR/HAS platform associated with F-actin and filopodia of keratinocytes is the target of corticosteroids for their atrophogenic effects. These observations may lead to the development of new treatment and prevention strategies for corticosteroid-induced skin atrophy.


Journal of Investigative Dermatology | 1999

IgG Autoantibodies from Bullous Pemphigoid (BP) Patients Bind Antigenic Sites on Both the Extracellular and the Intracellular Domains of the BP Antigen 180

Jacqueline Perriard; Fabienne Jaunin; Bertrand Favre; Jean-Hilaire Saurat; Luca Borradori; Lioba Büdinger; M. Hertl


Journal of Investigative Dermatology | 2000

IgG Autoantibodies from Bullous Pemphigoid Patients Recognize Multiple Antigenic Reactive Sites Located Predominantly Within the B and C Subdomains of the COOH-Terminus of BP230

Mouna Skaria; Fabienne Jaunin; Sara Riou; Jean-Hilaire Saurat; Bertrand Favre; Luca Borradori; Thomas Hunziker; Hauke Schumann; Leena Bruckner-Tuderman; Michael Hertl; Philippe Bernard


Journal of Investigative Dermatology | 1998

Autoantibodies from a Patient with Paraneoplastic Pemphigus Bind Periplakin, a Novel Member of the Plakin Family

Luca Borradori; Ralph M. Trüeb; Fabienne Jaunin; Alain Limat; Bertrand Favre; Jean-Hilaire Saurat


Journal of Investigative Dermatology | 1995

Involvement of Granulocytes and the Adhesion Receptors Intercellular Adhesion Molecule-1 and Lymphocyte Function-Associated Antigen-1 in Tissue Inflammation Induced by Th2-Type Helper Cells

Kai M. Müller; Fabienne Jaunin; Isabelle Masouyé; Pierre-François Piguet; Jean-Hilaire Saurat; Conrad Hauser

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Alain Limat

University of Lausanne

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