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42 research outputs found

Cycles oestriens et cycles menstruels

Author: Driancourt Marc Antoine
Hedon B.
Levasseur M.C.
Royère Dominique
Publication venue: INRA Ellipses
Publication date: 01/01/1991
Field of study

chap. 29National audienc

Hal-Diderot

Oestrous and menstrual cycles

Author: Driancourt Marc Antoine
Hedon B.
Levasseur M.C.
Royère Dominique
Publication venue: Ellipses
Publication date: 01/01/1993
Field of study

chap. 29International audienc

Hal-Diderot

The cell cycle control protein cdc25C is present and phosphorylated on serine 214 in the transition from germinal vesicle to metaphase II in human oocyte meiosis

Author: Anahory Ts
Berthenet C.
Cunat S.
Fernandez Arnaud
Hamamah S.
Hedon B.
Lamb Nj
Publication venue: 'Wiley'
Publication date: 01/01/2008
Field of study

International audienc

HAL Descartes

Integrated summary of Ortho Evra (TM)/Evra (TM) contraceptive patch adhesion in varied climates and conditions

Author: Creasy GW
Fisher AC
Hedon B
Mansour D
Shangold GA
Zacur HA
Publication venue: Elsevier Inc.
Publication date: 07/02/2002
Field of study

Newcastle University E-Prints

452 Prostanoids a the peritoneal fluid of infertile women

Author: A.Crastes de Paulet
B. Hedon
H. Thaler
L. Merklein
M. Dämon
R. Denjean
Publication venue: 'Elsevier BV'
Publication date
Field of study

Crossref

Luteal support after in-vitro fertilization: Crinone 8%, a sustained release vaginal progesterone gel, versus Utrogestan, an oral micronized progesterone.

Author: Antoine J.-P.
Bassil S.
Donnez Jacques
Frydman R
Hedon B
Nicollet B
Pouly J L
Prada Y
Zambrano R
Publication venue: 'Oxford University Press (OUP)'
Publication date: 01/01/1996
Field of study

Two progesterone presentations, a vaginal application of 90 mg progesterone per day (Crinone) or 300 mg progesterone administered orally (Utrogestan), were compared for luteal phase support of patients undergoing an in-vitro fertilization (IVF) procedure. A total of 283 patients were randomly allocated to either treatment. The treatment started within 24 h after the embryo transfer procedure and continued until day 30 in cases of implantation. Efficacy was assessed using the pregnancy and delivery rates. Safety was assessed through specific symptoms and usual safety monitoring. The pregnancy rates per transfer were not significantly different in the Crinone and Utrogestan groups at days 12 (Crinone 35.3%, Utrogestan 29.9%, P = 0.55), 30 (Crinone 28.5%, Utrogestan 25.0%, P = 0.61) and 90 (Crinone 25.9%, Utrogestan 22.9%, P = 0.69). No differences in the spontaneous abortion rates were seen thereafter. The delivery rates (number of deliveries per patient; Crinone 23.0%, Utrogestan 22.2%, P = 1.00), as well as the ratio of newborn babies per embryo transferred (Crinone 11.7%, Utrogestan 11.1%, P = 0.91), were not significantly different. Safety parameters were similar in both groups, except for drowsiness, which was more significantly frequent in the oral progesterone group than in the Crinone group at all time points. No serious adverse events were recorded in this study. The fact that Crinone matches the efficacy of the larger doses of progesterone used orally reflects an advantage of the transvaginal route of administration which avoids the metabolic inactivation of progesterone during its first liver pass

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