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Featured researches published by F.A.A. van Acker.


Xenobiotica | 1997

Extension of a predictive substrate model for human cytochrome P4502D6

M.J. de Groot; G.J. Bijloo; F.A.A. van Acker; C. Fonseca Guerra; J.G. Snijders; Nico P. E. Vermeulen

1. Metoprolol, indoramine, codeine, tamoxifen and prodipine, compounds which are clinically used, and MDMA (ecstasy) were fitted in a small molecule model for substrates of human cytochrome P4502D6. 2. For both the R- and S-enantiomer of metoprolol, the R- and S-enantiomer of MDMA, and for indoramine and codeine (all proven substrates of cytochrome P4502D6) an acceptable fit in the substrate model was obtained. 3. For tamoxifen, for which the involvement of cytochrome P4502D6 in the 4-hydroxylation is uncertain, no acceptable fit could be obtained in the substrate model. 4. For prodipine, a competitive inhibitor of P4502D6, for which the involvement of P4502D6 in the metabolism is uncertain, no acceptable fit in the substrate model could be obtained. 5. The substrate model was extended in a direction in which two large known substrates extend from the original substrate model. This extension did not change the flat hydrophobic region of the original substrate model.


Toxicology Letters | 1997

Acute exposure to ozone does not influence neuroreceptor density and sensitivity in guinea pig lung

H.J.M. van Hoof; F.A.A. van Acker; Hans-Peter Voss; L. van Bree; A. Bast

The effects of acute exposure of guinea pigs to 3 ppm of ozone for 2 h on the receptor density and sensitivity of the muscarinergic-, the histaminergic- and the beta-adrenergic receptor systems were studied, in order to provide more insight in the complex mechanisms underlying the well known ozone-induced changes in receptor functionality. The exposure to ozone did not change either the total amount of receptors present in lung tissue, nor the receptor sensitivity of the systems studied. Although no effects were observed, this does not yet fully exclude the receptor system for being a target of ozone exposure. The receptor function can be changed after exposure to ozone, e.g., the coupling with the G-protein can be influenced. Furthermore, the G-protein itself may have been altered or changes can occur at lower levels in the receptor signal transmission route leading to functional changes after stimulation of the receptor with an agonist.


Toxicology in Vitro | 2001

Flavonoids as peroxynitrite scavengers: the role of the hydroxyl groups

C.G.M Heijnen; Guido R.M.M. Haenen; F.A.A. van Acker; W.J.F. van der Vijgh; Aalt Bast


Chemical Research in Toxicology | 1996

A three-dimensional protein model for human cytochrome P450 2D6 based on the crystal structures of P450 101, P450 102, and P450 108.

M.J. de Groot; Nico P. E. Vermeulen; J.D. Kramers; F.A.A. van Acker; G.M. Donné-Op den Kelder


Chemical Research in Toxicology | 1997

A refined substrate model for human cytochrome P450 2D6.

M.J. de Groot; G.J. Bijlo; B.J. Martens; F.A.A. van Acker; Nico P. E. Vermeulen


Clinical Cancer Research | 2000

7-Monohydroxyethylrutoside Protects against Chronic Doxorubicin-induced Cardiotoxicity When Administered Only Once Per Week

F.A.A. van Acker; S.A.B.E. van Acker; K. Kramer; G.R.M.M. Haenen; A. Bast; W.J.F. van der Vijgh


Free Radical Biology and Medicine | 2001

NEW SYNTHETIC FLAVONOIDS AS POTENT PROTECTORS AGAINST DOXORUBICIN-INDUCED CARDIOTOXICITY

F.A.A. van Acker; J. Hulshof; Guido R.M.M. Haenen; Wiro M. P. B. Menge; W.J.F. van der Vijgh; Aalt Bast


Anticancer Research | 2000

In vitro screening of antitumour agents for cardiotoxicity by means of isolated mouse left atria

F.A.A. van Acker; S.A.B.E. van Acker; Guido R.M.M. Haenen; Aalt Bast; W.J.F. van der Vijgh


Humane Endpoints in Animal Experiments for Biomedical Research | 1999

Using telemetry to study the effect of protectors on doxorubicin-induced cardiotoxicity in freely moving mice.

K. Kramer; F.A.A. van Acker; S.A.B.E. van Acker; J.A. Grimbergen; W. J. F. van der Vijgh; A. Bast; C.F.M. Hendriksen; D.B. Morton


Toxicology Letters | 2018

Safety assessment of biotechnologically produced 2’-Fucosyllactose, a novel food additive

J. Salverda; D. van Berlo; A. Wallinga; F.A.A. van Acker; D. Delsing

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A. Bast

VU University Amsterdam

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Aalt Bast

Maastricht University

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K. Kramer

VU University Amsterdam

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G.R.M.M. Haenen

Maastricht University Medical Centre

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