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Flowchart: Prostaglandin E2 (Dinoprostone) for Induction of Labour

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Flowchart: Prostaglandin E2 (Dinoprostone) for Induction of Labour Queensland Health Prostaglandin E2 (dinoprostone) for induction of labour Induction of labour Prostaglandin E2 (dinoprostone) See flowchart: Method of induction Indications Pre dinoprostone insertion · Unfavourable cervix (MBS ≤ 6) · Complete pre IOL assessment · Following balloon catheter if no/ · Encourage to empty bladder minimal effect on cervical ripening and ARM not technically possible Contraindications · Known hypersensitivity · Ruptured membranes · Multiparity ≥ 5 Dinoprostone GEL Dinoprostone PESSARY · Previous CS or uterine surgery · Nulliparous: 2 mg PV · 10 mg PV · Malpresentation/high presenting · Multiparous: 1 mg PV · Position transversely in part · Insert high into posterior posterior fornix · Undiagnosed PV bleeding fornix · Wait at least 12 hours after · Abnormal CTG/fetal compromise · Wait at least 6 hours after insertion then reassess insertion then reassess Cautions MBS MBS · Multiple pregnancy · Asthma, chronic obstructive pulmonary disease: may cause bronchospasm [email protected] · Epilepsy · Cardiovascular disease Recommend ARM · Raised intraocular pressure, irrespective of MBS glaucoma · Avoid concurrent oxytocin use Post dose care Queensland Clinical Guidelines, Guidelines, Clinical Queensland ARM Yes · TPR, BP, FHR, uterine activity, successful? PV loss hourly for 4 hours or SROM? · CTG for minimum of 30 minutes · If observations normal, no No 8 contractions and not otherwise nd/3.0/au/deed.en - nc indicated, ongoing care as for - latent first stage of labour · Continuous CTG when in active If GEL used: labour or when contractions are · May repeat to maximum of 3 If PESSARY used: ≥ 3 in 10 minutes doses at least 6 hours apart · Give one dose of · After insertion advise woman to: o Nulliparous 2 mg dinoprostone GEL Remain recumbent for 30 o o Multiparous 1–2 mg · Wait at least 6 hours then minutes · Wait at least 6 hours then reassess MBS o Inform staff as soon as reassess MBS contractions commence State of Queensland (Queensland Health) 201 Health) (Queensland Queensland of State http://creativecommons.org/licenses/by PESSARY removal indications · Onset of regular, painful uterine contractions, occurring every 3 minutes regardless of cervical change No ARM Yes · Ruptured membranes successful? or SROM? · Fetal distress · Uterine hyperstimulation or hypertonic uterine contractions · Maternal systemic adverse effects (e.g. nausea, vomiting, Recommend oxytocin hypotension, tachycardia) Consider balloon · 6 hours after GEL · Insufficient cervical ripening after catheter · 30 minutes after removal 24 hours of PESSARY (minimum) ARM: Artificial rupture of membranes; BP: Blood pressure; CS: Caesarean section; CTG: Cardiotocography; FHR: Fetal heart rate; IOL: Induction of labour; MBS: Modified Bishop Score; PV: Per vaginam; SROM: spontaneous rupture of membranes; TPR: Temperature, pulse and respirations; ≥: greater than or equal to; ≤: less than or equal to Queensland Clinical Guideline: Induction of labour. Flowchart: F17.22-3-V6-R22 Queensland Clinical Guidelines www.health.qld.gov.au/qcg .
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  • E001466.Full.Pdf
    Editorial BMJ Glob Health: first published as 10.1136/bmjgh-2019-001466 on 11 April 2019. Downloaded from WHO recommendations on uterotonics for postpartum haemorrhage prevention: what works, and which one? Joshua P Vogel, 1,2 Myfanwy Williams,3 Ioannis Gallos,4 Fernando Althabe,1 Olufemi T Oladapo1 To cite: Vogel JP, THE GLOBAL BURDEN OF POSTPARTUM trials of tranexamic acid for PPH treatment Williams M, Gallos I, et al. HAEMORRHAGE and a heat-stable formulation of carbetocin WHO recommendations on 6–12 uterotonics for postpartum Obstetric haemorrhage, especially post- for PPH prevention. The increasing haemorrhage prevention: partum haemorrhage (PPH), was responsible number of PPH prevention and management what works, and which for more than a quarter of the estimated 303 options makes it challenging for providers one?BMJ Glob Health 000 maternal deaths that occurred globally in and health system stakeholders to choose 2019;4:e001466. doi:10.1136/ 2015.1 PPH—commonly defined as a blood where and how to invest limited resources in bmjgh-2019-001466 loss of 500 mL or more within 24 hours after order to optimise health outcomes. birth—affects about 6% of all women giving Multiple uterotonics have been eval- Handling editor Seye Abimbola birth.1 Uterine atony is the most common uated for PPH prevention over the past Received 4 February 2019 cause of PPH, but it can also be caused by four decades, including oxytocin receptor Revised 10 March 2019 genital tract trauma, retained placental tissue agonists (oxytocin and carbetocin), prosta- Accepted 16 March 2019 or maternal bleeding disorders. The majority glandin analogues (misoprostol, sulprostone, of women who experience PPH have no iden- carboprost), ergot alkaloids (such as ergo- tifiable risk factor, meaning that PPH preven- metrine/methylergometrine) and combina- tion programmes rely on universal use of PPH tions of these (oxytocin plus ergometrine, © Author(s) (or their prophylaxis for all women in the immediate or oxytocin plus misoprostol).
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