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Preterm labour
- 1. Preterm Labour Dr Fatima Patel
- 2. Summary • Introduction • Definition of preterm labour • Risk factors for preterm birth • Pathophysiology • Prevention • Complications • Management • Followup
- 3. Introduction • Certain dates vital either LMP, early USS • More than 50% of patients with possible threatened preterm labour deliver after 37 weeks • Some medications e.g. tocolytics can be harmful to mother • Identification of risk factors and prevention is the aim
- 4. Definition and diagnosis • The diagnosis of PTL is generally based upon clinical criteria of regular, painful uterine contractions accompanied by cervical dilation and/or effacement between 20 and 36 weeks and 6 days • ‘Preterm’ means we know her gestational age accurately
- 5. Gestational age estimation • LMP based on sure dates (menstrual calender), regular cycle, not on contraception within last 3 months; Naegle’s rule based on 28 day cycle: adjust if more or less than. • May have to change if first trimester scan is >5days different (CRL) or less than 20 weeks scan >7 days different (HC) • Once determined not for change as later scans reflect size of baby
- 6. Special Investigations • Fetal Fibronectin (FFN): swab taken from the post vaginal fornix at speculum examination and tested for FFN. Highish false positive. Value lies in a negative test • Transvaginal ultrasound for cervical length(TV CL) measurement: if TVCL is >2cm then the chances of delivery less than 35 weeks are small.
- 7. Risk Factors for PTL Non-modifiable risk factors • Prior preterm birth • African-American race • Age <18 or >40 years • Poor nutrition/low prepregnancy weight • Low socioeconomic status • Cervical injury or anomaly • Uterine anomaly or fibroid • Premature cervical dilatation (>2 cm) or effacement (>80 percent) • Over distended uterus (multiple pregnancy, polyhydramnios) • Periodontal disease? Vaginal bleeding? Excessive uterine activity
- 8. Risk Factors contd Modifiable risk factors • Cigarette smoking • Substance abuse • Absent prenatal care • Short interpregnancy intervals • Anemia • Bacteriuria/urinary tract infection • Genital infection • ? Strenuous work? High personal stress
- 9. Pathophysiology of PTL • Premature activation of the maternal or fetal hypothalamic-pituitary-adrenal axis • Exaggerated inflammatory response/ infection • Decidual hemorrhage • Pathological uterine distention These processes may be initiated long before PTL or PPROM are diagnosed clinically.
- 10. Prevention – potentially effective • Cessation of smoking, avoid cocaine use • Decrease the rate of multiple gestation from ART • Diagnose and treat asymptomatic bacteriuria • Decrease occupational fatigue • Nutritional intervention • Avoid short interpregnancy interval ‘ideal’ > than 12 months but not >48 months • Progesterone • Inhibition of acute preterm labour • Cervical cerclage
- 11. Unproven • Diagnosis and treatment of genital tract infection • Treatment of periodontal disease • Bed rest and hospitalisation • Abstinence • Prophylactic tocolytics • Antibiotics • Thyroid hormone, social support
- 12. Management • treat only the women with true preterm labour and a real risk of preterm birth by knowledge of TVU CL and FFN • If CL is <20mm then admit, steroids, tocolysis • If CL is 20-29mm and FFN positive then above management, if FFN negative then discharge; if contractions continue consider prolonged observation and ? repeat TVCL • If CL >30mm then discharge
- 13. Optimisation of foetal status • Transfer: to appropriate level hospital usually with level 3 NICU • Corticosteroids for foetal maturity between 24 and 34 weeks gestation. Single course of betamethazone (pending ASTEROID trial results) 11.4mg twice IMI 24 hours apart. A single rescue dose can be given if first course given before 28 weeks gestation and more than 14 days later with appropriate counselling 13
- 14. Tocolysis • The goal is to prevent imminent preterm birth in order to have sufficient time to administer steroids and to have sufficient time if appropriate to allow for in utero transfer to hospital with NICU • Usually nifedipine is first line • Magnesium sulphate has been shown to significantly decrease cerebral palsy in 5 trials 14
- 15. Complications • cerebral palsy • cognitive defects (e.g. low IQ) • school difficulties • behavioural problems • diminished long term survival and reproduction 15
- 16. Follow-up • Post partum counselling on preventive strategies are important after one episode of preterm labour and birth. 16
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