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Featured researches published by Koenraad Jozef Lodewijk Marcel Andries.


Antimicrobial Agents and Chemotherapy | 2010

Rates and Mechanisms of Resistance Development in Mycobacterium tuberculosis to a Novel Diarylquinoline ATP Synthase Inhibitor

E Huitric; P Verhasselt; Anil Koul; Koenraad Jozef Lodewijk Marcel Andries; Sven Hoffner; Dan I. Andersson

ABSTRACT R207910 (also known as TMC207) is an investigational drug currently in clinical studies for the treatment of multidrug-resistant (MDR) tuberculosis. It has a high degree of antimycobacterial activity and is equally effective against drug-susceptible and MDR Mycobacterium tuberculosis isolates. In the present study, we characterized the development of resistance to R207910 in vitro. Ninety-seven independent R207910-resistant mutants were selected from seven different clinical isolates of M. tuberculosis (three drug-susceptible and four MDR isolates) at 10×, 30×, and 100× the MIC. At a concentration of 0.3 mg/liter (10× the MIC), the mutation rates ranged from 4.7 × 10−7 to 8.9 × 10−9 mutations per cell per division, and at 1.0 mg/liter (30× the MIC) the mutation rate ranged from 3.9 × 10−8 to 2.4 × 10−9. No resistant mutants were obtained at 3 mg/liter (100× the MIC). The level of resistance ranged from 0.12 to 3.84 mg/liter for the mutants identified; these concentrations represent 4- to 128-fold increases in the MICs. For 53 of the resistant mutants, the atpE gene, which encodes a transmembrane and oligomeric C subunit of the ATP synthase and which was previously shown to be involved in resistance, was sequenced. For 15/53 mutants, five different point mutations resulting in five different amino acid substitutions were identified in the atpE gene. For 38/53 mutants, no atpE mutations were found and sequencing of the complete F0 ATP synthase operon (atpB, atpE, and atpF genes) and the F1 ATP synthase operon (atpH, atpA, atpG, atpD, and atpC genes) from three mutants revealed no mutations, indicating other, alternative resistance mechanisms. Competition assays showed no measurable reduction in the fitness of the mutants compared to that of the isogenic wild types.


Archive | 1999

HIV inhibiting pyrimidine derivatives

Koenraad Jozef Lodewijk Marcel Andries; Corte Bart De; Jonge Marc Rene De; Jan Heeres; Chih Yung Ho; Marcel Janssen; Paul A. J. Janssen; Lucien Maria Henricus Koymans; Michael Joseph Kukla; Donald William Ludovici; Aken Koen Jeanne Alfons Van


Archive | 2000

Respiratory syncytial virus replication inhibitors

Frans Eduard Janssens; Kathleen Petrus Marie-José Meersman; Francois Maria Sommen; Jérôme Emile Georges Guillemont; Jean Fernand Armand Lacrampe; Koenraad Jozef Lodewijk Marcel Andries


Archive | 1999

HIV inhibiting pyrimidine derivative

Koenraad Jozef Lodewijk Marcel Andries; Bart De Corte; Marc René De Jonge; Jan Heeres; Chih Yung Ho; Marcel Janssen; Paul A. J. Janssen; Lucien Maria Henricus Koymans; Michael Joseph Kukla; Donald William Ludovici; Koen Jeanne Alfons Van Aken


Archive | 1988

Antiviral pharmaceutical compositions containing cyclodextrins

Jean Louis Mesens; Koenraad Jozef Lodewijk Marcel Andries


Archive | 2006

Quinoline derivatives as antibacterial agents

Koenraad Jozef Lodewijk Marcel Andries; Anil Koul; Jérôme Emile Georges Guillemont; Elisabeth Thérèse Jeanne Pasquier


Archive | 2007

ANTIBACTERIAL QUINOLINE DERIVATIVES

Jérôme Emile Georges Guillemont; Ismet Dorange; Magali Madeleine Simone Motte; Koenraad Jozef Lodewijk Marcel Andries; Anil Koul


Archive | 2005

Use of Substituted Quinoline Derivatives for the Treatment of Drug Resistant Mycobacterial Diseases

Koenraad Jozef Lodewijk Marcel Andries; Gestel Jozef Frans Elisabetha Van


Archive | 2006

Quinoline derivatives as antibacterical agents

Koenraad Jozef Lodewijk Marcel Andries; Anil Koul; Jérôme Emile Georges Guillemont; Elisabeth Thérèse Jeanne Pasquier; David Francis Alain Lançois


Archive | 1995

Anti-hiv triple combination

Paulus Aloysius Maria Stoffels; Koenraad Jozef Lodewijk Marcel Andries

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Anil Koul

Janssen Pharmaceutica

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