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21 results on '"Uterine bleeding -- Drug therapy"'

1. Misoprostol to prevent and treat postpartum haemorrhage: a systematic review and meta-analysis of maternal deaths and dose-related effects/Administration de misoprostol pour prevenir et traiter les hemorragies postpartum, revue systematique et meta-analyse de la mortalite maternelle et des effets dose-dependants/Prevencion y tratamiento de la hemorragia posparto con misoprostol: revision sistematica y metanalisis ..

Author

Hofmeyr, G. Justus, Gulmezoglu, A. Metin, Novikova, Natalia, Linder, Verena, Ferreira, Sandra, and Piaggio, Gilda

Subjects
Misoprostol -- Dosage and administration, Misoprostol -- Complications and side effects, Uterine bleeding -- Prevention, Uterine bleeding -- Drug therapy, Mothers -- Patient outcomes, Mothers -- Prevention
Abstract

Objective To review maternal deaths and the dose-related effects of misoprostol on blood loss and pyrexia in randomized trials of misoprostol use for the prevention or treatment of postpartum haemorrhage. Methods We searched the Cochrane Controlled Trials Register and Pubmed, without language restrictions, for "(misoprostol AND postpartum) OR (misoprostol AND haemorrhage) OR (misoprostol AND hemorrhage)", and we evaluated reports identified through the Cochrane Pregnancy and Childbirth Group search strategy. Randomized trials comparing misoprostol with either placebo or another uterotonic to prevent or treat postpartum haemorrhage were checked for eligibility. Data were extracted, tabulated and analysed with Reviewer Manager (RevMan) 4.3 software. Findings We included 46 trials with more than 40 000 participants in the final analysis. Of 11 deaths reported in 5 trials, 8 occurred in women receiving [greater than or equal to] 600 [micro]g of misoprostol (Peto odds ratio, OR: 2.49; 95% confidence interval, CI: 0.76-8.13). Severe morbidity, defined as the need for major surgery, admission to intensive care, organ failure or body temperature [greater than or equal to] 40 [degrees]C, was relatively infrequent. In prevention trials, severe morbidity was experienced by 16 of 10 281 women on misoprostol and by 16 of 10 292 women on conventional uterotonics; in treatment trials, it was experienced by 1 of 32 women on misoprostol and by 1 of 32 women on conventional uterotonics. Misoprostol recipients experienced more adverse events than placebo recipients: 8 of 2070 versus 5 of 2032, respectively, in prevention trials, and 5 of 196 versus 2 of 202, respectively, in treatment trials. Meta-analysis of direct and adjusted indirect comparisons of the results of randomized trials showed no evidence that 600 [micro]g are more effective than 400 [micro]g for preventing blood loss [greater than or equal to] 1000 ml (relative risk, RR: 1.02; 95% CI: 0.71-1.48). Pyrexia was more than twice as common among women who received [greater than or equal to] 600 [micro]g rather than 400 [micro]g of misoprostol (RR: 2.53; 95% CI: 1.78-3.60). Conclusion Further research is needed to more accurately assess the potential beneficial and harmful effects of misoprostol and to determine the smallest dose that is effective and safe. In this review, 400 [micro]g of misoprostol were found to be safer than [greater than or equal to] 600 [micro]pg and just as effective. Objectif Etudier la mortalite maternelle et les effets dose-dependants du misoprostol sur la perte de sang et la pyrexie dans le cadre d&apos;essais randomises portant sur l&apos;utilisation de ce medicament pour prevenir et traiter les hemorragies postpartum. Methodes Nous avons fait des recherches dans le registre Cochrane des essais controles et dans Pubmed sans emettre de restriction concernant la langue et en utilisant l&apos;expression <> OR (misoprostol AND haemorrhage) OR (misoprostol AND hemorrhage), puis nous avons evalue les rapports identifies avec la strategie de recherche du Groupe Cochrane Pregnancy and Childbirth. Nous avons verifie la conformite avec les criteres d&apos;admissibilite dans l&apos;etude des essais randomises comparant le misoprostol a un placebo ou a un autre uterotonique dans la prevention ou le traitement des hemorragies postpartum. Nous avons extrait et tabule des donnees, puis nous les avons analysees avec le Iogiciel Reviewer Manager (RevMan) 4.3. Resultats Dans l&apos;analyse finale, nous avons pris en compre 46 essais portant sur plus de 40 000 participantes. Sur 11 deces rapportes dans 5 essais, 8 sont survenus chez des femmes ayant recu [greater than or equal to] 600 [micro]g de misoprostol (Odds ratio de Peto, OR : 2,49; intervalle de confiance a 95%, IC: 0,76-8,13). La morbidite grave, definie comme la necessite d&apos;une intervention chirurgicale importante, l&apos;admission en soins intensifs, la defaillance d&apos;un organe ou une temperature corporelle [greater than or equal to] 40 [degrees]C, etait relativement rare. Dans les essais de prevention, nous avons releve une morbidite grave chez 16 des 10281 femmes sous misoprostol et chez 16 des 10292 parturientes recevant un uterotonique classique et, dans les essais therapeutiques, chez une des 32 femmes sous misoprostol et chez une des 32 femmes sous uterotonique classique. Les retomes recevant du misoprostol ont manifeste plus d&apos;effets indesirables que celles recevant un placebo : 8 sur 2070 contre 5 sur 2032 respectivement dans les essais de prevention et 5 sur 196 contre 2 sur 202 dans les essais therapeutiques. La meta-analyse des comparaisons directes et indirectes ajustees des resultats d&apos;essais randomises n&apos;a fait apparaitre aucune preuve d&apos;une efficacite superieure de la dose de 600 [micro]g de misoprostol par rapport a la dose de 400 [micro]g, dans la prevention d&apos;une perte de sang [greater than or equal to]1000 mi (risque relatif, RR : 1,02; IC a 95% : 0,71-1,48). La pyrexie etait plus de deux fois plus frequente chez les femmes ayant recu [greater than or equal to] 600 [micro]g de misoprostol que chez celles ayant recu une dose de 400 pg (RR : 2,53; IC a 95% : 1,78-3,60). Conclusion Des recherches supplementaires sont necessaires pour evaluer plus precisement les effets benefiques et nocifs potentiels du misoprostol et pour identifier la plus faible dose de ce medicament a la fois efficace et sans risque. La presente etude a trouve qu&apos;une dose de 400 [micro]g de misoprostol etait plus sure qu&apos;une dose [greater than or equal to] 600 [micro]g et tout aussi efficace. Objetivo Analizar la mortalidad materna y los efectos dosisdependientes del misoprostol sobre la perdida de sangre y en forma de fiebre en los ensayos aleatorizados realizados sobre su uso con tines de prevencion o tratamiento de la hemorragia posparto. Metodos Utilizamos el Registro de Ensayos Controlados de Cochrane y Pubmed para realizar una busqueda en todos los idiomas planteada en los siguientes terminos: << (misoprostol AND postpartum) OR (misoprostol AND haemorrhage) OR (misoprostol AND hemorrhage) >>. Se procedio a evaluar los trabajos identificados mediante la estrategia de busqueda del Grupo Cochrane de Embarazo y Parto, y se determino la elegibilidad de los ensayos aleatorizados en que se comparo el misoprostol ya fuera con un placebo o con otro uterotonico como forma de prevencion o tratamiento de la hemorragia posparto. Los datos extraidos fueron tabulados y analizados con el software Reviewer Manager (RevMan) 4.3. Resultados Incluimos en el analisis final 46 ensayos que abarcaron a mas de 40 000 participantes. De las 11 defunciones notificadas en 5 ensayos, 8 correspondian a mujeres que habian recibido [greater than or equal to] 600 [micro]g de misoprostol (oportunidad relativa [OR] de Peto: 2,49; intervalo de confianza [IC] del 95%: 0,76-8,13). La morbilidad grave, definida como la necesidad de cirugia mayor, el ingreso en cuidados intensivos, la aparicion de insuficiencia organica o una temperatura corporal [greater than or equal to]40 [degrees]C, fue relativamente poco frecuente. En los ensayos de prevencion, sufrieron morbilidad grave 16 de las 10 281 mujeres a las que se administro misoprostol, y 16 de las 10 292 mujeres sometidas a uterotonicos convencionales; en los ensayos de tratamiento, sufrieron cuadros graves 1 de 32 mujeres sometidas a misoprostol y 1 de 32 mujeres tratadas con uterotonicos convencionales. Quienes recibieron misoprostol sufrieron mas eventos adversos que quienes recibieron placebo: 8 de 2070 frente a 5 de 2032, respectivamente, en los ensayos de prevencion, y 5 de 196 frente a 2 de 202, respectivamente, en los ensayos de tratamiento. El metanalisis de las comparaciones directas e indirectas ajustadas de los resultados de los ensayos aleatorizados no aporto ningun indicio de que la dosis de 600 pg sea mas eficaz que la de 400 [micro]g para prevenir las hemorragias [greater than or equal to]1000 ml (riesgo relativo, RR: 1,02; IC95%: 0,71-1,48). La frecuencia de fiebre entre las mujeres que recibieron [greater than or equal to]600 [micro]g de misoprostol fue mas del doble que en las tratadas con 400 [micro]g (RR: 2,53; IC95%: 1,78-3,60). Conclusion Es necesario realizar nuevas investigaciones para evaluar con mas precision los posibles erectos beneficiosos y nocivos del misoprostol y para determinar la dosis mas baja eficaz y segura. Segun los resultados de este analisis, las dosis de 400 [micro]g de misoprostol son mas seguras que las dosis [greater than or equal to]600 [micro]g y tienen la misma eficacia., Introduction In low-income countries, postpartum haemorrhage is a major cause of maternal death (1) and arguably the most preventable. Attempts to reduce deaths from postpartum haemorrhage have been complicated by [...]

Published
2009

2. Oral misoprostol in preventing postpartum haemorrhage in resource-poor communities: a randomised controlled trial

Author

Derman, Richard J., Kodkany, Bhalchandra S., Goudar, Shivaprasad S., Geller, Stacie E., Naik, Vijaya A., Bellad, M.B., Patted, Shobhana S., Patel, Ashlesha, Edlavitch, Stanley A., Hartwell, Tyler, Chakraborty, Hrishikesh, and Moss, Nancy

Subjects
Uterine bleeding -- Drug therapy, Misoprostol -- Dosage and administration, Childbirth -- Complications and side effects, Mothers -- Patient outcomes, Mothers -- Prevention
Published
2006

3. Randomised controlled trial of oxytocin alone versus oxytocin and ergometrine in active management of third stage of labour

Author

McDonald, Susan J., Prendiville, Walter J., and Blair, Eve

Subjects
Oxytocin -- Evaluation, Ergonovine -- Evaluation, Labor (Obstetrics) -- Drug therapy, Puerperal disorders -- Drug therapy, Uterine bleeding -- Drug therapy
Abstract

Abstract Objective--To compare intramuscular oxytocin alone and intramuscular oxytocin with ergometrine (Syntometrine) for their effect in reducing the risk of postpartum haemorrhage when both are used as part of the […]

Published
1993

4. Continuous combined conjugated equine estrogen-progestogen therapy: effects of medroxyprogesterone acetate and norethindrone acetate on bleeding patterns and endometrial histologic diagnosis

Author

Hillard, T.C., Siddle, N.C., Whitehead, M.I., Fraser, D.I., and Pryse-Davies, J.

Subjects
Uterine diseases -- Drug therapy, Amenorrhea -- Care and treatment, Hormone therapy -- Evaluation, Estrogen -- Health aspects, Progestational hormones -- Health aspects, Uterine bleeding -- Drug therapy, Health
Published
1992

5. The combination of a depot gonadotrophin releasing hormone agonist and cyclical hormone replacement therapy for dysfunctional uterine bleeding

Author

Thomas, E.J., Okuda, K.J., and Thomas, N.M.

Subjects
Uterine bleeding -- Drug therapy, Hormone therapy -- Evaluation, Health
Abstract

The effectiveness was investigated of the use of combination of hormones for treating dysfunctional uterine bleeding (DUB), a common problem. The hormones used were goserelin (Zoladex), an agonist of gonadotrophin releasing hormone (GnRH), the hormone that stimulates the pituitary to release gonadotrophins, which then stimulate the ovaries: and hormone replacement therapy (HRT; estradiol and norgestrol) of the type commonly prescribed for postmenopausal women. Twenty women with regular, heavy menstrual bleeding underwent treatment with goserelin and HRT during three cycles. Menstrual blood loss was measured before the study began, during each cycle, and 12 weeks after the last goserelin injection. Results showed reduced menstrual loss for 19 women in the first treatment cycle; for all women in the second cycle; and for 19 in the last cycle. Menstrual loss increased in one woman during treatment. The median length of menstruation decreased significantly during treatment, and fewer women experienced pain, premenstrual symptoms, flooding, and clot passage. Hot flushes occurred in 17 cases, and in two patients they were considered severe. Overall, satisfaction was reported by 18 patients. Although this combination of GnRH agonist and HRT was effective in treating DUB, its high cost suggests that it be recommended only to women with demonstrably heavy menstrual loss. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1991

6. A comparative study of ethamsylate and mefenamic acid in dysfunctional uterine bleeding

Author

Chamberlain, G., Freeman, R., Price, F., Kennedy, A., Casewit, Curtis W., and Eve, L.

Subjects
Mefenamic acid -- Evaluation, Menorrhagia -- Drug therapy, Uterine bleeding -- Drug therapy, Health
Abstract

A comparison was carried out of the effects of two non-hormonal agents, ethamsylate and mefenamic acid, used to treat menorrhagia, excessive blood loss during menstruation (more than 80 milliliters). Thirty-four women with menorrhagia and regular menstrual cycles were assigned to receive either ethamsylate or mefenamic acid, which they took from the first day of bleeding until the bleeding stopped. Sanitary napkins and tampons were collected from the subjects to determine the blood loss during three consecutive cycles. Drug side effects were also noted. Results showed that both drugs caused a statistically significant reduction in monthly blood loss. Although no differences were noted between the effects of the drugs during any given month, more women taking ethamsylate than mefenamic acid had reductions in blood loss equal to or greater than 40 percent during the third month of treatment. Mefenamic acid led to reduced blood loss in each of the three months, while ethamsylate led to reduced blood loss in months two and three only. A similar proportion of women in the two groups showed side effects (56 percent in the mefenamic acid group and 31 percent in the ethamsylate group); these were usually nausea, backache, and bloating, but did not cause any woman to discontinue treatment. The results indicate that both agents are effective in limiting the amount of blood lost in menorrhagic women. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1991

7. Research from Postgraduate Institute of Medical Education & Research Yields New Findings on Women's Health

Subjects
Women -- Health aspects, Uterine bleeding -- Drug therapy, Menopause -- Health aspects, Progesterone -- Dosage and administration, Endometrium -- Medical examination -- Health aspects, Health, Women's issues/gender studies
Abstract

In this recent article published in the Journal of Obstetrics and Gynaecology Research, scientists in Calcutta, India conducted a study 'To investigate the effect of oral progesterone on the accuracy [...]

Published
2012

8. Ob/Gyn

Subjects
Uterine bleeding -- Drug therapy, Ulipristal acetate -- Testing, Sexual disorders -- Drug therapy, Pharmaceutical industry -- Product development, Health
Abstract

Bremelanotide (Rekynda; AMAG/Palatin) a melanocortin-4 receptor agonist delivered subcutaneously via auto-injector pen under development for the treatment of women with hypoactive sexual desire disorder (HSDD)--Phase 3 Ulipristal acetate (Allergan/Gedeon Richter) [...]

Published
2017

9. Management of severe postpartum hemorrhage by intrauterine irrigation with prostaglandin E2

Author

Peyser, M. Reuben and Kupferminc, Michael J.

Subjects
Prostaglandins -- Dosage and administration, Puerperal disorders -- Care and treatment, Prostaglandins -- Health aspects, Uterine bleeding -- Drug therapy, Health
Abstract

Life-threatening uterine hemorrhage is responsible for 25 percent of all maternal deaths after the delivery of a pregnancy. It is caused primarily by the failure of the uterus to contract after delivery. Blood loss from such a hemorrhage can be over a liter, causing a dangerous drop in blood pressure. Prompt treatment includes the administration of drugs that promote uterine contraction (oxytocin and ergot therapy), pressure applied directly to the uterus, uterine massage and replacement of lost blood. In cases where these measures are ineffective, removal of the uterus may be necessary. Prostaglandins are hormone-like substances produced by the body naturally, which exert their effect on smooth muscle by stimulating uterine contractions. Injection of prostaglandins into the uterus results in uterine contractions. However, to achieve direct access to the uterus, injections must be given through the abdomen or vagina. To see if bathing the uterine cavity directly with fluid containing prostaglandin E2 is an effective treatment, 22 patients with postpartum hemorrhages not responding to conventional therapy were studied. Patients were given continuous prostaglandin infusions using a small tube inserted into the uterus. In all 22 cases, uterine contractions were achieved and bleeding was stopped within minutes of prostaglandin infusion. None of the patients experienced any side effects. Infusing the uterine cavity with prostaglandin E2 produced dramatic response in women with postpartum hemorrhage. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1990

10. Acute Uterine Bleeding Treatment with Medroxyprogesterone Acetate or Birth Control Pills

Author

Ling, Frank W.

Subjects
Oral contraceptives -- Dosage and administration, Oral contraceptives -- Evaluation, Medroxyprogesterone -- Dosage and administration, Medroxyprogesterone -- Evaluation, Uterine bleeding -- Drug therapy, Health
Abstract

Acute Uterine Bleeding Treatment with Medroxyprogesterone Acetate or Birth Control Pills Abstract & Commentary By Frank W. Ling, MD, Clinical Professor, Dept. of Obstetrics and Gynecology, Vanderbilt University School of [...]

Published
2006

11. Current Perspectives on OC Formulations

Subjects
Acne, Oral contraceptives -- Health aspects, Uterine bleeding -- Drug therapy
Abstract

When the topic of unintended pregnancy is raised, women in their teen years usually are the first to come to mind. However, statistics on unintended pregnancy show that effective contraception [...]

Published
2001

12. WHO position on misoprostol for post-partum haemorrhage prevention and treatment

Subjects
Misoprostol -- Health aspects, Misoprostol -- Research, Uterine bleeding -- Prevention, Uterine bleeding -- Drug therapy, Uterine bleeding -- Care and treatment, Mothers -- Patient outcomes, Mothers -- Prevention, Family and marriage, Health, Women's issues/gender studies, World Health Organization -- Powers and duties
Abstract

WHO has clarified its position on misoprostol use in the community for post-partum haemorrhage (PPH) prevention and management, to reduce maternal death, following a request in July 2009 from Member [...]

Published
2010

14. Mirena

Subjects
Bayer HealthCare AG -- Product development, Mirena (Contraceptive) -- Licensing, certification and accreditation, Uterine bleeding -- Drug therapy, Levonorgestrel -- Licensing, certification and accreditation, Pharmaceutical industry -- Product development, Pharmaceuticals and cosmetics industries, Drug therapy, Licensing, certification and accreditation, Product development
Abstract

Levonorgestrel-releasing intrauterine system (Mirena, Bayer HealthCare Pharmaceuticals) was approved for additional use to treat heavy menstrual bleeding in women who use intrauterine contraception as their method of pregnancy [...]

Published
2009

15. Acute myocardial infarction after ergonovine administration for uterine bleeding

Author

Liao, James K., Cockrill, Barbara A., and Yurchak, Peter M.

Subjects
Miscarriage -- Complications, Pregnancy, Complications of -- Case studies, Ergonovine -- Adverse and side effects, Heart attack -- Causes of, Uterine bleeding -- Drug therapy, Health
Abstract

Acute myocardial infarction (AMI; heart attack) during pregnancy and after delivery is a rare phenomenon, the cause of which remains unknown. It has been reported to occur in women suffering from diabetes mellitus, coronary artery disease, and high blood pressure; in some cases there appears to be no particular precipitating factor. A case is reported of a physically active, 34-year-old white woman who was hospitalized following a spontaneous abortion (miscarriage) during the course of her third pregnancy. (Her previous pregnancies were uncomplicated.) She had a history of cigarette smoking and migraine headaches, but denied any drug abuse. Because of persistent uterine bleeding, ergonovine (a drug that stimulates uterine contractions) was administered by intramuscular injection. Within 30 minutes of ergonovine injection, the patient developed crushing chest pain, and her blood pressure dropped to dangerously low levels. Electrocardiographic diagnosis indicated that a heart attack was occurring; treatment took the form of fluid, norepinephrine and nitroglycerine administration. Thrombolytic (clot-dissolving) drugs were not administered because of a recent surgical procedure. Follow-up evaluation indicated minimal (but detectable) damage to the heart muscle. The patient was put on a regimen of diltiazem (a calcium channel-blocking drug), and has returned to her previous level of activity with no apparent adverse effects. Physicians administering ergonovine to obstetrical patients should be aware of the possibility of this rare but life-threatening side effect of this drug. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1991

16. Oral medications stop acute nongestational uterine bleeding

Author

Lowry, Fran

Subjects
Medroxyprogesterone -- Usage, Oral contraceptives -- Usage, Uterine bleeding -- Drug therapy, Uterine bleeding -- Case studies, Uterine bleeding -- Statistics
Abstract

Washington -- Oral medroxyprogesterone acetate and oral contraceptives are equally effective in stopping nongestational acute uterine bleeding, according to a small randomized controlled trial presented at the annual meeting of [...]

Published
2006

17. Investigational drug effective in treating fibroid-related bleeding

Author

Bates, Betsy

Subjects
Uterine bleeding -- Drug therapy
Abstract

HOUSTON -- Asoprisnil, an investigational selective progesterone receptor modulator, induced amenorrhea or normal menstrual periods in a clear majority of women with myoma-associated menorrhagia in a multicenter phase II study. [...]

Published
2004

18. Oxytocin vs. misoprostol for postpartum hemorrhage. (Clinical Insights)

Subjects
Oxytocin -- Evaluation, Misoprostol -- Evaluation, Uterine bleeding -- Drug therapy, Vagina -- Hemorrhage, Health
Abstract

Is tried and true oxytocin preferable to misoprostol for the prevention of postpartum hemorrhage? The answer may depend on the setting in which the drugs are used. Because misoprostol, a [...]

Published
2002

19. Provera

Subjects
Provera (Medication) -- Dosage and administration, Provera (Medication) -- Complications and side effects, Medroxyprogesterone -- Dosage and administration, Medroxyprogesterone -- Complications and side effects, Uterine bleeding -- Drug therapy
Published
2008

20. Prometrium

Subjects
Prometrium (Medication) -- Dosage and administration, Prometrium (Medication) -- Complications and side effects, Progesterone -- Dosage and administration, Progesterone -- Complications and side effects, Uterine bleeding -- Drug therapy
Published
2008

21. Deprenyl/Queen's research agreement

Subjects
Deprenyl USA Inc. -- Contracts, Pharmaceutical industry -- Contracts, Uterine bleeding -- Drug therapy, Business, Pharmaceuticals and cosmetics industries, Queen's University -- Contracts
Published
1992

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