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Dive into the research topics where J. Vandenberghe is active.

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Featured researches published by J. Vandenberghe.


Mycoses | 1989

Toxicological Profile and Safety Evaluation of Antifungal Azole Derivatives

H. Van Cauteren; Ann Lampo; J. Vandenberghe; Ph. Vanparys; W. Coussement; R. De Coster; R. Marsboom

Summary: For the development of new sys‐temically acting, oral antifungal azoles, it is of key importance to compare them with ketoconazole, the first available drug in this therapeutic class.


Toxicologic Pathology | 2011

Gavage-Related Reflux in Rats Identification, Pathogenesis, and Toxicological Implications (Review)

Siegrid Damsch; Gary Eichenbaum; Alfred Tonelli; Kathleen Van den Bulck; Bianca Feyen; J. Vandenberghe; Anton Megens; Elaine Knight; Michael F. Kelley

After oral gavage dosing of rats, reflux may occur, resulting in serious respiratory effects and mortality. Published information on gavage-related reflux is limited, as it has not yet been a focus of research. Nevertheless, it represents a recurrent challenge in daily toxicology practice of oral gavage dosing. The absence of clear guidance and criteria for the identification and management of reflux-induced effects can limit the ability to properly interpret toxicity study results. The review presented herein includes an overview of experimental data from gavage studies in rats, in which reflux was observed, and provides a comprehensive analysis of the literature on reflux in general and the different potential pathways contributing to gavage-related reflux in rats. The article aims to increase the awareness and understanding of the pathogenesis of gavage-related reflux and provides guidance on identification of potential risk factors, as well as interpretation of histological changes and their toxicological relevance. Furthermore, differentiation of reflux-induced effects from direct compound-related toxicity and from gavage errors is addressed in particular, and the importance of nasal histology is discussed.


Drug and Chemical Toxicology | 1985

TOXICOLOGICAL PROPERTIES OF CLOSANTEL

H. Van Cauteren; J. Vandenberghe; V. Hérin; Ph. Vanparys; R. Marsboora

The acute, subacute and chronic toxicity studies in laboratory animals showed that closantel is a well tolerated substance. At multiples of the clinical dose, overdosing might result in central nervous system effects and death. Repeated oral dosing was without effects up to 40 mg/kg in rats and dogs except for focal swelling of the epididymis in male rats at 40 mg/kg due to formation of spermatic granulomas. In sheep repeated dosing at 10 and 40 mg/kg orally and at 5 and 20 mg/kg intramuscularly every four weeks during 40 weeks demonstrated an acceptable safety margin in this target species. Reproduction studies including a three-generation study in rats showed that fertility was not affected except slightly in male rats at 40 mg/kg whereas an embryotoxic or teratogenic potential in rats and rabbits was absent. Peri- and postnatal parameters in rats were not affected. In target animals, reproduction was extensively studied in bulls, rams and ewes showing no risk of closantel for reproduction parameters. A mutagenic potential was found to be absent in a Salmonella Ames test, a sex-linked recessive lethal test in Drosophila melanogaster and a dominant lethal test in male and female mice. In 400 mice and 400 rats closantel was shown not to be carcinogenic. Tolerance studies in sheep and cattle demonstrated that oral and parenteral clinical doses were very well tolerated and devoid of serious side-effects.


Drug and Chemical Toxicology | 1987

Mutagenic and Leukemogenic Activity of Haloperidol: A Negative Study

H. Vancauteren; Ph. Vanparys; Conrad De Meester; M. Lambottevandepaer; J. Vandenberghe; R. Marsboom

The mutagenic and leukemogenic potential of haloperidol, a neuroleptic of the butyrophenone class, has been studied in an in vitro Ames Salmonella/microsome test and in an 18-month carcinogenicity study in mice. Three variants of the Salmonella mutation assay were included: the spot test, the standard plate incorporation test and the preincubation test. There was no evidence that haloperidol had any mutagenic activity in any of the Salmonella mutation tests with any of the Salmonella typhimurium tester strains in the presence or absence of Aroclor 1254-induced rat- or mouse-liver S9-mix. In the 18-month study, haloperidol was injected intraperitoneally as a solution (HaldolR) at a dosage of 5 mg/kg daily for 5, 10 and 20 consecutive days in 5-week-old mice. Leucocyte counts at several time points and histopathological tumor evaluation 18 months later did not reveal any leukemogenic or other carcinogenic effect. On the basis of these data, it may be concluded that haloperidol is not mutagenic in Salmonella nor leukemogenic in mice.


The British journal of clinical practice | 1990

Safety aspects of oral antifungal agents.

H. Van Cauteren; Ann Lampo; J. Vandenberghe; Ph. Vanparys; W. Coussement; R. De Coster; R. Marsboom


Drug Development Research | 1986

Protective activity of ketanserin against serotonin-induced embryotoxicity and teratogenicity in rats

Herman Van Cauteren; J. Vandenberghe; R. Marsboom


Cancer Research | 1995

Carcinogenicity Studies of Astemizole in Mice and Rats

Johanna Benze; Ludo Gypen; J. Vandenberghe; Ann Lampo; Roland De Coster; Charles Bowden; Herman Van Cauteren


Toxicology | 2012

Mechanistic investigations on the etiology of Risperdal(®) Consta(®)-induced bone changes in female Wistar Hannover rats.

Eric J. de Waal; Wendy Roosen; Petra Vinken; J. Vandenberghe; Patrick Sterkens


Archive | 2011

emptying: potential role of vagal inhibition Pramlintide, an amylin analog, selectively delays gastric

Lawrence A. Szarka; Adrian Vella; R Alan; Bianca Feyen; J. Vandenberghe; Anton Megens; Elaine Knight; Michael F. Kelley; Siegrid Damsch; Gary Eichenbaum; Alfred Tonelli; Kathleen Van den Bulck


The Journal of Allergy and Clinical Immunology | 1996

641 Astemizole is not carcinogenic in mice and rats

J. Benze; L. Gypen; Ann Lampo; J. Vandenberghe; R. De Coster; Charlie Bowden; H. Van Cauteren

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Ann Lampo

Janssen Pharmaceutica

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