Your search keyword '"Vanhoenacker, Peter"' showing total 3 results

1. Biochemical and pharmacological study of N-linked glycosylation of the human serotonin 5-HT7(a) receptor.

Author

Gellynck, Evelien, Andressen, Kjetil W., Lintermans, Béatrice, Haegeman, Guy, Levy, Finn O., Vanhoenacker, Peter, and Van Craenenbroeck, Kathleen

Subjects

GLYCOSYLATION, SEROTONIN receptors, G protein coupled receptors, GENE expression, MOLECULAR biology, IMMUNOCYTOCHEMISTRY, LIGAND binding (Biochemistry)

Abstract

The 5-hydroxytryptamine (5-HT)7(a) receptor is a G-protein-coupled receptor critically involved in human psychiatric and neurological disorders. In the present study, we evaluate the presence and the functional role of N-glycosylation of the human 5-HT7 receptor. Western blot analysis of HEK293T cells transiently expressing the 5-HT7(a) receptor in the presence of tunicamycin gave rise to a band shift, indicating the existence of an N-glycosylated form of the 5-HT7(a) receptor. To further investigate this, we mutated the two predicted N-glycosylation sites (N5Q and N66Q) and compared the molecular mass of the immunoreactive bands with those of the wild-type receptor, indicating that both asparagines were N-glycosylated. The mutant receptors had the same binding affinity for [3H]5-CT and the same potency and efficacy with regard to 5-HT-induced activation of adenylyl cyclase. However, there was a reduction in maximal ligand binding for the single and double mutants compared to the wild-type receptor. Next, membrane labelling and immunocytochemical studies demonstrated that the N-glycosylation mutants were expressed at the cell surface. We conclude that N-glycosylation is not important for cell surface expression of the 5-HT7 receptor. [ABSTRACT FROM AUTHOR]

Published

2012

2. Episomal vectors for gene expression in mammalian cells.

Author

Van Craenenbroeck, Kathleen, Vanhoenacker, Peter, and Haegeman, Guy

Subjects

*EPISOMES, *GENETIC vectors, *GENE expression, *VIRUSES

Abstract

Highlights episomal expression vectors for gene expression in mammalian cells. Advantages of using episomal vectors; Potential of episomal vectors for use in gene therapy; BK virus sequences in gene expression vectors; Bovine papilloma virus 1-derived vectors for heterologous gene expression; Epstein-Barr virus as gene expression system.

Published

2000

3. AG013, a mouth rinse formulation of Lactococcus lactis secreting human Trefoil Factor 1, provides a safe and efficacious therapeutic tool for treating oral mucositis

Author

Caluwaerts, Silvia, Vandenbroucke, Klaas, Steidler, Lothar, Neirynck, Sabine, Vanhoenacker, Peter, Corveleyn, Sam, Watkins, Brynmor, Sonis, Stephen, Coulie, Bernard, and Rottiers, Pieter

Subjects

*LACTOCOCCUS lactis, *PHARMACODYNAMICS, *PHARMACOKINETICS, *BACTERIAL genomes, *GENE expression, *RADIOTHERAPY, *INFLAMMATION, *ERYTHROMYCIN, *ORAL diseases, *THERAPEUTICS

Abstract

Summary: Non-clinical studies, focusing on the pharmacodynamics (PD), pharmacokinetics (PK) and safety pharmacology of genetically modified Lactococcus lactis (L. lactis) bacteria, engineered to secrete human Trefoil Factor 1 (hTFF1), were performed to provide proof-of-concept for the treatment of oral mucositis (OM) patients. L. lactis strain sAGX0085 was constructed by stably inserting an htff1 expression cassette into the bacterial genome, and clinically formulated as a mouth rinse (coded AG013). PD studies, using different oral dosing regimens, were performed in a clinically relevant hamster model for radiation-induced OM. The PK profile was assessed in healthy hamsters and in hamsters with radiation-induced OM. In addition, in vitro and in vivo safety pharmacology studies were conducted, in pooled, complement-preserved human serum, and in neutropenic hamsters and rats respectively. Topical administration of L. lactis sAGX0085/AG013 to the oral mucosa significantly reduced the severity and course of radiation-induced OM. PK studies demonstrated that both living L. lactis bacteria, as well as the hTFF1 secreted, could be recovered from the administration site for maximum 24h post-dosing, without systemic exposure. The in vitro and in vivo safety pharmacology studies confirmed that L. lactis sAGX0085 could not survive in systemic circulation, not even under neutropenic conditions. The results from the PD, PK and safety pharmacology studies reported here indicate that in situ secretion of hTFF1 by topically administered L. lactis bacteria provides a safe and efficacious therapeutic tool for the prevention and treatment of OM. [Copyright &y& Elsevier]

Published

2010