Search

Your search keyword '"Boxho G"' showing total 8 results
Start Over Author "Boxho G"
8 results on '"Boxho G"'

3. Effect of metoprolol CR XL in chronic heart failure: Metoprolol CR XL Randomised Intervention Trial in Congestive Heart Failure (MERIT-HF)

Author

Hjalmarson, A., Goldstein, S., Fagerberg, B., Wedel, H., Waagstein, F., Kjekshus, J., Wikstrand, J., Westergren, G., Hassle, A., Thimell, M., El Allaf, D., Vitovec, J., Aldershvile, J., Halinen, M., Dietz, R., Neuhaus, Kl, Janosi, A., Thorgeirsson, G., Dunselman, P., Gullestad, L., Kuch, J., Herlitz, J., Rickenbacher, P., Ball, S., Gottlieb, S., Deedwania, P., Vandenhoven, G., Novakova, I., Danker, S., Lundstrom, M., Meyer-Sabellek, W., Balla, I., Sveinsdottir, M., Dorhout, B., Hildebrandt, A., Szczurko, I., Larsson, C., Bucher, E., Scott, E., Dwyer, D., Julian, Dg, Demets, Dl, Chatterjee, K., Feyzi, J., Lehto, S., Karpati, P., Motz, W., Samuelsson, O., Viersma, Jw, Andersson, B., Berthe, C., Boutefeu, Jm, Boxho, G., Decroly, P., Derbaudrenghien, Jp, Pirlet, J., Henry, P., Heyndrickx, G., Missault, L., Nannan, M., Timmermans, P., Vachiery, Jl, Mieghem, W., Vandenbossche, Jl, Dvorak, K., Herold, M., Hradec, J., Kana, A., Petr, P., Rybka, J., Smid, J., Svitil, P., Toman, J., Agner, E., Amtorp, O., Egstrup, K., Eliasen, P., Gotzsche, Co, Hildebrandt, P., Johannesen, A., Kaiser-Nielsen, P., Nielsen, H., Nielsen, Pe, Pedersen, F., Nielsen, Jr, Skagen, K., Honkanen, T., Hussi, E., Juvonen, J., Jaaskelainen, H., Rinne, J., Salonen, T., Andresen, D., Berwing, H., Forster, A., Hauf, Gf, Krosse, B., Luderitz, B., Olshausen, Ke, Schmailzl, Kjg, Schwimmbeck, Pl, Sigmund, M., Voller, H., Czuriga, I., Hetey, M., Katona, A., Lengyel, M., Nyaradi, A., Rednik, A., Sandori, K., Szabo, P., Tarjan, J., Tenczer, J., Timar, S., Valyi, P., Veress, G., Zamolyi, K., Oze, B., Bernink, Pjlm, Bredero, Ac, Breedveld, Rw, Breuls, Pnwm, Bucx, Jjj, jan cornel, Milliano, Par, Dunselman, Phjm, Hamer, Bjb, Holwerda, Nl, Hoogsteen, J., Hoorntje, Jca, Kragten, Ja, Liem, Ah, Linssen, Gcm, Michels, Hr, Misier, Arr, Schaafsma, Hj, Sijbring, P., Taverne, Rjt, Kempen, Lhj, Stralen, R., Veldhuisen, Dj, Veerhoek, Mj, Werter, Cjpj, Wesdorp, Jcl, Willems, Ar, Withagen, Ajam, Zwart, Pag, Bjornerheim, R., Dahle, M., Dickstein, K., Froland, Gs, Gundersen, T., Hofsoy, K., Hole, Tl, Johansen, T., Mannsverk, J., Nesje, P., Omland, Tm, Sjodin, C., Smith, P., Tjonndal, Ha, Vikesdal, O., Waage, K., Jaworska, K., Kolodziej, P., Kornacewicz-Jach, Z., Krzeminska-Pakula, M., Piotrowski, Jw, Piwowarska, W., Stogowski, A., Wodniecki, J., Wrabec, K., Ahlstrom, P., Ekdahl, S., Hemmingson, Lo, Holmberg, L., Lernfelt, B., Nilsson, H., Widgren, B., Angman, K., Erne, P., Mohacsi, P., Polikar, R., Schlapfer, H., Batin, P., Berkin, Ke, Callaghan, Ts, Forfar, J., Frenneaux, M., Greenbaum, Ra, Maltz, M., Murdoch, D., Reynolds, G., Stephens, J., Struthers, A., Swan, J., Tildesley, G., Abbasi, A., Alagona, P., Alderman, J., Alipour, M., Anderson, Jl, Ansari, Z., Ashraf, M., Beanblossom, Bt, Bennett, S., Benvenuti, D., Berk, MR, Bhalla, R., Bilazarian, Sd, Browne, Kf, Buchter, Cm, Carlson, R., Carlson, Cj, Danisa, K., Dauber, I., Dewood, Ma, Dennish, G., Denny, Dm, Dibianco, R., Diller, Pm, Dunlap, M., Dowd, K., Edmiston, A., El Shahawy, M., Elkayam, U., Farnham, J., Fenster, P., Friedman, S., Heywood, T., Galichia, Jp, Geller, M., Ghali, Jk, Gheorghiade, M., Giles, T., Gillespe, R., Goldberg, G., Goldberg, Mc, Goldscher, Da, Gooden, Gp, Goodman, M., Goodman, L., Gorwit, J., Gottlieb, Ss, Gradman, A., Grech, D., Hack, T., Hall, Jh, Hattenhauer, Mt, Higginbotham, Mb, Hutchins, S., Imburgia, M., Iteld, Bj, Jackson, B., Jafri, S., Jauch, W., Jennison, S., Kahn, Bh, Kao, W., Kaplan, K., Karlsberg, R., Kennedy, Hl, Kennedy, Jj, Kirkegaard, L., Kraus, Dh, Labresh, K., Lalonde, L., Lesser, Mf, Levites, R., Levy, M., Lewis, Rk, Loh, Ik, Madyoon, H., Maislos, F., Mann, D., Maurice, Gl, Nisar, A., Old, W., Pappas, Jd, Phadke, K., Promisloff, S., Rashkow, Am, Reeves, B., Rosen, Jh, Rotman, M., Saleem, T., Savran, Sv, Shah, R., Shalev, Y., Shanes, Jg, O Shaughnessy, M., Silverman, B., Steingart, Rm, Swenson, L., Syed, K., Thadani, U., Thorsen, Rd, Tonkon, Mj, Touchon, R., Uhl, G., Vaska, Kj, Wagner, Sg, Weaver, Cj, Weiss, Rj, Wickemeyer, Wj, Willens, Hj, Wilson, Jr, Wright, R., and Yellen, L.

4. [Leiomyosarcoma of the inferior vena cava].

Author

Golinval O, Magnée M, and Boxho G

Subjects
CA-125 Antigen metabolism, CA-19-9 Antigen metabolism, Fatal Outcome, Female, Humans, Leiomyosarcoma metabolism, Middle Aged, Mucin-1 metabolism, Vascular Neoplasms metabolism, Biomarkers, Tumor metabolism, Leiomyosarcoma diagnosis, Vascular Neoplasms diagnosis, Vena Cava, Inferior pathology
Abstract

Leiomyosarcoma of vena cava are rare tumors. They occur preferentially in the inferior vena cava. They affect preferentially women and the median age of incidence is on fifth decade. Their prognosis depends on the severity of venal occlusion, local invasion and presence of metastases. We report the case of a woman who died from occlusion of the inferior vena cava. We review the literature.

Published
2010

5. [Advances concerning aliskiren, direct renin inhibitor and aliskiren-hydrochlorothiazide].

Author

Boxho G, Krzesinski JM, and Scheen AJ

Subjects
Cardiovascular Diseases drug therapy, Clinical Trials as Topic, Diabetic Nephropathies drug therapy, Humans, Renin antagonists & inhibitors, Amides pharmacology, Antihypertensive Agents pharmacology, Fumarates pharmacology
Abstract

Aliskiren (Rasilez), a direct renin inhibitor, is currently indicated for the treatment of essential hypertension, as monotherapy or in combination, especially with hydrochlorothiazide (Rasilez HCT). It may also be use to obtain a more complete blockade of the renin-angiotensin-aldosterone system (RAAS) when it is associated with an angiotensin converting enzyme inhibitor (ACEI) (or an AT1 angiotensin receptor antagonist) (ARA). There is some room for agents that may be more efficacious in reducing the progression of diabetic nephropathy than ACEI or ARA. In this context, the dual blockade of RAAS most probably offers a better efficacy than the simple blockade, but also exposes to a higher risk. Should ongoing trials confirm the preliminary favourable results, aliskiren might reach a forefront position among the armamentarium now available to optimize the RAAS blockade. The present article will summarize advances concerning the biochemical effects of the specific mode of action of aliskiren, especially the potential interferences related to increased renin/pro-renin levels, as well as results of recent clinical trials, not only in hypertension, but also in the fields of diabetes, renal insufficiency and cardiology. The objectives and design of the landmark study ALTITUDE will also be briefly presented.

Published
2009

6. Acute and chronic effect of molsidomine extended release on exercise capacity in patients with stable angina, a double-blind cross-over clinical trial versus placebo.

Author

Messin R, Boxho G, De Smedt J, and Buntinx IM

Subjects
Acute Disease, Adult, Aged, Angina Pectoris physiopathology, Blood Pressure drug effects, Chronic Disease, Cross-Over Studies, Delayed-Action Preparations, Double-Blind Method, Exercise Test, Female, Heart Rate drug effects, Humans, Male, Middle Aged, Molsidomine administration & dosage, Molsidomine adverse effects, Angina Pectoris drug therapy, Exercise physiology, Molsidomine therapeutic use
Abstract

A double-blind, placebo-controlled, cross-over study was performed in 50 patients with ischemic heart disease and stable angina to determine the duration of efficacy of 8 mg molsidomine in extended-release form. Exercise testing was performed at baseline and 2, 4, 6, 8, and 10 h after intake of either the medication or the placebo. Total duration of exercise (in minutes) and total work performance (workload x min) was significantly improved in the molsidomine retard group, not only compared with baseline but also with placebo for all time-points. ST segment depression at 60 W and at maximal exercise improved similarly until 10 h after molsidomine retard treatment. The rate-pressure product (heart rate x systolic blood pressure) showed significant improvement only at 60 W. No attenuation of the obtained effects was observed after 14 days of treatment. The number of anginal attacks and the consumption of sublingual nitroderivates were significantly reduced with molsidomine retard 8 mg as compared with placebo. Molsidomine retard 8 mg is effective until at least 10 h after oral (p.o.) intake. A dose schedule of molsidomine retard 8 mg twice daily definitely reduces anginal symptoms.

Published
1995
Full Text
View/download PDF

7. Placebo-controlled comparison of spirapril at 6, 12 and 24 mg/day in mild to severe essential hypertension.

Author

Guitard C, Alvisi V, Maibach E, Franck J, Cocco G, Boxho G, Mellein B, and Waite R

Subjects
Aged, Analysis of Variance, Angiotensin-Converting Enzyme Inhibitors adverse effects, Blood Pressure drug effects, Blood Pressure physiology, Double-Blind Method, Enalapril administration & dosage, Enalapril adverse effects, Female, Humans, Hypertension physiopathology, Male, Middle Aged, Time Factors, Angiotensin-Converting Enzyme Inhibitors administration & dosage, Enalapril analogs & derivatives, Hypertension drug therapy
Abstract

In a double-blind, parallel-group study, 260 patients with mild to severe essential hypertension were randomized to treatment with placebo or spirapril at 6, 12 or 24 mg once daily for 6 weeks. When blood pressures were measured at the end of the dosing interval (trough), all spirapril regimens had produced similar reductions in sitting systolic and diastolic blood pressures (siSBP/siDBP) which were significantly greater than those observed in placebo-treated patients. There were no relevant changes in resting heart rate in any of the study groups. At the study endpoint, the mean reductions in siSBP/siDBP were 14.9/11.5 mmHg with spirapril at 6 mg, 15.4/12.0 mmHg with spirapril at 12 mg and 17.8/12.4 mmHg with spirapril at 24 mg/day vs. 3.1/3.6 mmHg with placebo. In a subgroup of 122 patients, blood pressure was recorded at the end of the dosing interval and during the 8 hours immediately postdose to monitor the peak effects on blood pressure. All spirapril dosages produced similar reductions at peak with a mean decrease of siDBP of approximately 20 mmHg in comparison to baseline values vs 6-7 mmHg with placebo. The trough:peak ratios for 6, 12 and 24 mg all lay between 60% and 90% for siSBP and siDBP, indicating that most of the peak effect was maintained at trough. Spirapril was well tolerated; the adverse event profile was not different from that with placebo, and no dose-related adverse events were observed.(ABSTRACT TRUNCATED AT 250 WORDS)

Published
1994

8. [3 years of existence of a coronary care unit].

Author

Lisin N, Andriange M, Calay G, Gach J, Hiernaux M, Mbuyamba P, Vandenbosch R, Boxho G, Claessens JJ, Zicot M, van Herck A, and Carlier J

Subjects
Adult, Aged, Arrhythmias, Cardiac therapy, Belgium, Coronary Disease therapy, Evaluation Studies as Topic, Female, Humans, Male, Middle Aged, Coronary Care Units
Published
1973

Catalog

Books, media, physical & digital resources
See catalog results