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Dive into the research topics where Anna Mitselos is active.

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Featured researches published by Anna Mitselos.


Peptides | 2008

Desensitization and internalization of the human motilin receptor is independent of the C-terminal tail.

Anna Mitselos; Theo L. Peeters; Inge Depoortere

The motilin receptor (MTLR) is an important therapeutic target for the treatment of hypomotility disorders but desensitization may limit its clinical utility. The aim of this study was to investigate the role of the C-terminal tail of the MTLR in the desensitization, phosphorylation and internalization process. Three MTLR mutants, C-terminally truncated from amino acid 412 till 384 (MTLRDelta385), 374 (MTLRDelta375) or 368 (MTLRDelta369), were constructed and C-terminally tagged with an EGFP and stably expressed in CHO cells co-expressing the Ca(2+) indicator apoaequorin. Activity and desensitization were studied by measuring changes in motilin-induced luminescent Ca(2+) rises. Receptor phosphorylation was investigated by immunoprecipitation and MTLR-EGFP internalization was visualized by fluorescence microscopy. Truncation only reduced MTLR affinity and the efficacy to induce Ca(2+) luminescent responses of the MTLRDelta375-EGFP mutant. Furthermore, the region between amino acid 375 and 368 seems to be important for proper cell surface expression of the MTLR since receptors of the MTLRDelta369-EGFP mutant but not of the other mutants were found intracellularly in vesicles. Truncation of the receptor till amino acid 384 or 374 did neither affect desensitization nor internalization. In contrast phosphorylation of the MTLRDelta385-EGFP mutant was reduced by 80% but was not affected in the MTLRDelta375-EGFP mutant. In conclusion, MTLR desensitization and internalization is not dependent on the presence of the C-terminal tail. Truncation favors internalization via either phosphorylation-independent pathways or via phosphorylation of alternative sites in the receptor.


Neurogastroenterology and Motility | 2004

The rat lacks functional genes for motilin and the motilin receptor

J Aerssens; Inge Depoortere; Leen Thielemans; Anna Mitselos; B Coulie; T Peeters


Biochemical Pharmacology | 2008

Differences in motilin receptor desensitization after stimulation with motilin or motilides are due to alternative receptor trafficking

Anna Mitselos; Pieter Vanden Berghe; Theo L. Peeters; Inge Depoortere


Biochemical Pharmacology | 2007

Delineation of the motilin domain involved in desensitization and internalization of the motilin receptor by using full and partial antagonists.

Anna Mitselos; Inge Depoortere; Theo L. Peeters


Regulatory Peptides | 2006

Desensitizing potency of the motilide mitemcinal (GM-611) in CHO-cells expressing the motilin receptor (MTLR)

Leen Thielemans; Anna Mitselos; Inge Depoortere; T Peeters


Regulatory Peptides | 2006

Desensitization and trafficking of the motilin receptor

Anna Mitselos; Inge Depoortere; T Peeters


Acta Gastro-Enterologica Belgica | 2006

Agonist induced trafficking of the motilin receptor

Anna Mitselos; Inge Depoortere; Pieter Vanden Berghe; Theo L. Peeters


Acta Gastro-Enterologica Belgica | 2005

More potent desensitization and slower resensitization of the motilin receptor following stimulation with the motilide ABT-229 than with motilin

Anna Mitselos; Inge Depoortere; T Peeters


Regulatory Peptides | 2004

Desensitization and resensitization of the motilin receptor induced by motilin and the motilide ABT-229

Anna Mitselos; Inge Depoortere; T Peeters


Regulatory Peptides | 2004

The mouse is a natural motilin knockout and ghrelin replaces motilin functionally

T Peeters; J Aerssens; Betty De Smet; Leen Thielemans; Anna Mitselos; B Coulie; Inge Depoortere

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Inge Depoortere

Katholieke Universiteit Leuven

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T Peeters

Katholieke Universiteit Leuven

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Leen Thielemans

Katholieke Universiteit Leuven

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Theo L. Peeters

Catholic University of Leuven

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Pieter Vanden Berghe

Katholieke Universiteit Leuven

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Betty De Smet

Catholic University of Leuven

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