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Dive into the research topics where Joke Serneels is active.

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Featured researches published by Joke Serneels.


Current Drug Targets | 2005

Fungal Pathogens Research: Novel and Improved Molecular Approaches for the Discovery of Antifungal Drug Targets

Hélène Tournu; Joke Serneels; Patrick Van Dijck

With the rise of fungal infection incidence amongst the patient population, the importance of developing new antifungal drug targets is higher than ever. This review mainly focuses on the three most prevalent fungal pathogens, Candida, Aspergillus and Cryptococcus, and on the most recent progresses in molecular research that contribute to a better understanding of the pathogen itself, but also its host and the interaction with its host. We consider the progress made in comparative genomics following the huge effort of fungal genome sequence projects undertaken in the last few years. We focus not only on currently used mammalian animal models such as mice, but also on novel non-mammalian models, such as the nematode worm Caenorhabditis elegans and the fruit fly Drosophila melanogaster, which offer useful tools in the area of the innate immune response to fungal infections. In addition we relate to the recent genomic and proteomic studies and focus on the use of these approaches in in vivo experiments in the pathogen itself as well as in the host. Finally, we describe the latest targeted mutagenesis strategy available in C. albicans and the use of RNA interference in both Cryptococcus neoformans and A. fumigatus. Our aim is not to give an exhaustive list of all new strategies but rather to give an overview of what will contribute most to the identification of new antifungal drug targets and the establishment of novel antifungal strategies.


Journal of Biological Chemistry | 2012

Tight Control of Trehalose Content Is Required for Efficient Heat-induced Cell Elongation in Candida albicans

Joke Serneels; Hélène Tournu; Patrick Van Dijck

Background: Heat-induced morphogenetic switch is Hsp90- and PKA-dependent. Results: The G protein-coupled receptor Gpr1, upstream of PKA, regulates trehalose levels in glucose-grown cells. Conclusion: The link between the PKA pathway and Hsp90-mediated regulation of heat-induced morphogenesis is trehalose. Significance: Tight control of trehalose levels is required for morphogenesis in Candida albicans. The ability to form hyphae in the human pathogenic fungus Candida albicans is a prerequisite for virulence. It contributes to tissue infection, biofilm formation, as well as escape from phagocytes. Cell elongation triggered by human body temperature involves the essential heat shock protein Hsp90, which negatively governs a filamentation program dependent upon the Ras-protein kinase A (PKA) pathway. Tight regulation of Hsp90 function is required to ensure fast appropriate response and maintenance of a wide range of regulatory and signaling proteins. Client protein activation by Hsp90 relies on a conformational change of the chaperone, whose ATPase activity is competitively inhibited by geldanamycin. We demonstrate a novel regulatory mechanism of heat- and Hsp90-dependent induced morphogenesis, whereby the nonreducing disaccharide trehalose acts as a negative regulator of Hsp90 release. By means of a mutant strain deleted for Gpr1, the G protein-coupled receptor upstream of PKA, we demonstrate that elevated trehalose content in that strain, resulting from misregulation of enzymatic activities involved in trehalose metabolism, disrupts the filamentation program in response to heat. Addition of geldanamycin does not result in hyphal extensions at 30 °C in the gpr1Δ/gpr1Δ mutant as it does in wild type cells. In addition, validamycin, a specific inhibitor of trehalase, the trehalose-degrading enzyme, inhibits cell elongation in response to heat and geldanamycin. These results place Gpr1 as a regulator of trehalose metabolism in C. albicans and illustrate that trehalose modulates Hsp90-dependent activation of client proteins and signaling pathways leading to filamentation in the human fungal pathogen.


Molecular Biology of the Cell | 2005

The G Protein-coupled Receptor Gpr1 and the Gα Protein Gpa2 Act through the cAMP-Protein Kinase A Pathway to Induce Morphogenesis in Candida albicans

Mykola M. Maidan; Larissa De Rop; Joke Serneels; Simone Exler; Steffen Rupp; Hélène Tournu; Johan M. Thevelein; Patrick Van Dijck


Archive | 2005

Methionine-induced morphogenesis in Candida albicans is dependent on the methionine permease Mup1 and the G protein-coupled receptor Gpr1

Mykola Maydan; Mona Eskandarian; Joke Serneels; Hélène Tournu; Patrick Van Dijck


Archive | 2013

cAMP-PKA pathway to induce morphogenesis in Candida albicans

Mykola M. Maidan; Larissa De Rop; Joke Serneels; Simone Exler; Hélène Tournu; Johan M. Thevelein; Patrick Van Dijck


Archive | 2007

The GPCR system Gpr1-Gpa2 in C. albicans, using S. cerevisiae as a model organism

Joke Serneels; Hélène Tournu; Johan M. Thevelein; Patrick Van Dijck


Archive | 2006

Investigation into the function of Gpr1 receptor in Candida albicans

Hélène Tournu; Joke Serneels; Mykola Maydan; Patrick Van Dijck


Archive | 2006

Analyse de complémentation du complexe formé par Gpr1 et Gpa2 de Candida albicans chez la levure

Joke Serneels; Hélène Tournu; Patrick Van Dijck; Johan M. Thevelein; Mykola M. Maidan


Archive | 2005

CaGpr1-CaGpa2 as a potential GPCR nutrient sensing system in Candida albicans

Joke Serneels; Mykola Maydan; Larissa De Rop; Patrick Van Dijck


Archive | 2004

A homologue of G-protein coupled receptor regulates yeast-hypha transition in Candida albicans

Mykola Maydan; Larissa De Rop; Joke Serneels; Johan M. Thevelein; Patrick Van Dijck

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Patrick Van Dijck

Katholieke Universiteit Leuven

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Johan M. Thevelein

Katholieke Universiteit Leuven

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Larissa De Rop

Katholieke Universiteit Leuven

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Mykola M. Maidan

Katholieke Universiteit Leuven

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Steffen Rupp

University of Stuttgart

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