Béchetoille A
University of Angers
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Featured researches published by Béchetoille A.
Ophthalmology | 1999
Christophe Baudouin; Pierre-Jean Pisella; Kathleen Fillacier; Marie Goldschild; F. Becquet; Magda De Saint Jean; Béchetoille A
OBJECTIVES To investigate conjunctival and trabecular specimens from patients with glaucoma according to the duration and number of drugs received before filtration surgery, and to confirm, in a complementary experimental model, the role of preservative by comparing the effects of preserved and nonpreserved timolol. STUDY DESIGN Experimental animal and human tissue study. PARTICIPANTS Paired specimens of conjunctiva and trabeculum were taken from 61 patients undergoing trabeculectomy. Twenty-six patients were treated with 2 or more drugs for at least 1 year; 30 had received a beta-blocker for more than 1 year and 5 underwent primary surgery. A second study was performed in 25 rats receiving topical solutions in both eyes for 1 month. INTERVENTION Immunohistochemistry was performed in all biopsy specimens using 12 different monoclonal antibodies. Ocular structures from rats treated for 1 month with preserved 0.5% timolol, nonpreserved 0.5% timolol, or 0.01% benzalkonium chloride were similarly investigated in an experimental study. MAIN OUTCOME MEASURES Inflammatory cell infiltrates and fibroblasts were evaluated in biopsies, as well as in animal specimens, together with histologic changes induced by the drugs applied. RESULTS Twenty-four of 26 conjunctivae and 21 of 24 trabecular pieces from multitreated patients were found to be abnormally infiltrated by cells expressing inflammatory or fibroblastic markers or both. Nineteen of 30 conjunctivae and 9 of 22 trabeculums in the monotherapy group and only 1 of 5 specimens from the primary surgery group were abnormal. In rats, preserved timolol and benzalkonium similarly showed infiltrates together with toxic histopathologic changes as compared to the nonpreserved timolol and control groups. CONCLUSIONS These two combined studies confirmed histopathologic effects of antiglaucomatous drugs on the conjunctiva and showed similar effects in the trabecular meshwork. The experimental study showed that benzalkonium chloride is at least, to a large part, responsible for these toxic or immunoinflammatory effects or both on the ocular structures.
Acta Ophthalmologica | 2008
Béchetoille A; B Arnould; Alain M. Bron; Christophe Baudouin; Jean-Paul Renard; Eric Sellem; Yves Brouquet; Philippe Denis; Jean-Philippe Nordmann; Marie-Claude Rigeade; Ana Bassols; Khadra Benmedjahed; Isabelle Guillemin; Jean-François Rouland
Purpose: To validate a glaucoma‐specific health‐related quality of life (HRQoL) questionnaire: the Glau‐QoL©.
Eye | 1992
Frans P. Gunning; Béchetoille A; Erik A. Lippa; Norbert Pfeiffer; Jürgen Gerling; Daniel J. Holder; Coleen M. Clineschmidt; Agnes Buntinx; Françoise. Brunner-Ferber; Franz Grehn; Erik L. Greve
Sezolamide, a potent topical carbonic anhydrase inhibitor previously known as MK-417, was studied to determine its ocular hypotensive activity in patients with elevated intraocular pressure while on continuing therapy with topical timolol. This was a three-centre, double-masked, randomised, placebo-controlled, parallel study in 36 patients with bilateral primary open angle glaucoma or ocular hypertension on therapy receiving 0.5% timolol twice daily, with a morning intraocular pressure greater than or equal to 22 mmHg in both eyes 2–4 hours following an 8 a.m. dose of timolol. Sezolamide 1.8% or placebo twice daily was added to treatment with timolol on the evening of day 1 and continued for 2 weeks. Twelve-hour diurnal curves were performed before the study on day 1 (timolol alone) and on day 15. Intraocular pressure measurements were also taken on days 2 and 8 at 8 a.m. and 9 a.m. Patients who received timolol and sezolamide showed additional intraocular pressure reductions from day 1 (timolol alone) of 8.0 to 15.5%, which were significant at all times. At hours 1, 2, 4 and 8 the reductions in intraocular pressure observed in the group receiving sezolamide and timolol were significantly greater than those in the group receiving timolol and placebo.
Journal Francais D Ophtalmologie | 2000
Christophe Baudouin; Béchetoille A; Alain M. Bron; Philippe Denis; J.-P. Nordmann; J.P. Renard; J.-F. Rouland; Eric Sellem; Rigeade Mc; B Arnould
Journal Francais D Ophtalmologie | 2003
Zanlonghi X; B Arnould; Béchetoille A; Christophe Baudouin; Alain M. Bron; Philippe Denis; J.-P. Nordmann; J.P. Renard; Rigeade Mc; J.-F. Rouland; Eric Sellem
Journal Francais D Ophtalmologie | 2002
J.-F. Rouland; Philippe Denis; Béchetoille A; Rigeade Mc; Y. Brouquet; B Arnould; Christophe Baudouin; J.P. Renard; Alain M. Bron; J.-P. Nordmann; Eric Sellem; Du Groupe D'étude Glaucome Et Qualité De Vie
Journal Francais D Ophtalmologie | 2003
Zanlonghi X; B Arnould; Béchetoille A; Christophe Baudouin; Alain M. Bron; Philippe Denis; J.-P. Nordmann; J.P. Renard; Rigeade Mc; J.-F. Rouland; Eric Sellem
Journal Francais D Ophtalmologie | 2005
Eric Sellem; Christophe Baudouin; J.-P. Nordmann; Alain M. Bron; Yves Lachkar; J.B. Rottier; J.P. Renard; Béchetoille A; Philippe Denis; D. Ameloot
Journal Francais D Ophtalmologie | 1998
Béchetoille A; Alain M. Bron; P Demailly; J.-P. Nordmann
Journal Francais D Ophtalmologie | 1997
Béchetoille A; Philippe Denis; J.-P. Nordmann; Eric Sellem; Valtot F