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Premature Rupture of Membranes
Objectives: Describe the theories of pathogenesis of endometriosis List the most common sites of endometriosis Describe the symptoms and physical exam findings in a patient with endometriosis Describe the diagnosis and management of endometriosis
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DEFINITION Premature rupture of membranes (PROM)
Spontaneous rupture of membranes anytime beyond 28wks of pregnancy but before the onset of labour. Preterm premature rupture of membranes (PPROM) rupture of fetal membranes prior to labor in pregnancies btw weeks.
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When rupture of membranes occurs beyond 37 wks
When rupture of membranes occurs beyond 37 wks. but before the onset of labour it is called term PROM. Rupture of membranes for more than 24hrs before delivery is called prolonged rupture of membranes.
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Latency Period: time interval between ROM and onset of labor
Expectant management: management of patients with the goal of prolonging gestation (“watchful waiting” until delivery indication arises)
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RISK FACTORS Chorioamnionitis Vaginal infections
Cervical abnormalities Vascular pathology (incl. abruptio) Smoking 1st, 2nd, 3rd, or multiple trimester bleeding Previous preterm delivery (PPROM) AA ethnicity Acquired or congenital connective tissue disorder Nutritional deficiencies (Vit. C, copper, zinc)
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What causes premature rupture of membranes?
Rupture of the membranes near the end of pregnancy (term) may be caused by a natural weakening of the membranes or from the force of contractions. Before term, PPROM is often due to an infection in the uterus. Other factors that may be linked to PROM include the following: Low socioeconomic conditions (as women in lower socioeconomic conditions are less likely to receive proper prenatal care) Sexually transmitted infections such as chlamydia and gonorrhea Previous preterm birth Vaginal bleeding Cigarette smoking during pregnancy Unknown causes
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SYMPTOMS AND SIGNS Gush of fluid Leaking of fluid Cramping
Vaginal discharge Gush of fluid Leaking of fluid Oligo/ Anhydramnios Cramping Contractions Back pain
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History & Physical Exam
“Gush” of fluid Steady leakage of small amounts of fluid
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Physical examination Sterile vaginal speculum exam
Minimize digital examination of cervix, regardless of gestational age, to avoid risk of ascending infection/ amnionitis Assess cervical dilation and length Obtain cervical cultures (Gonorrhea, Chlamydia) Obtain amniotic fluid samples
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Findings Pooling of amniotic fluid in posterior vaginal fornix
Fluid per cervical os
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DIAGNOSIS Valsava maneuver Sterile Speculum exam (Pooling)
Nitrazine testing Fetal Fibronectin Ultrasonography SSE-Free flow of fluid from cervical os Microscopic Fern testing AmniSure Transabdominal Indigo dye injection
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Nitrazine paper testing
Vaginal pH ( ) Turns blue in presence of alkaline Amniotic fluid 93.3% sensitivity False positive (1-17%) for urine, blood, semen, BV, Trichomoniasis Vaginal pH acidic. Amniotic fluid pH alkaline at
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Fern test Fern test refers to visualization of a characteristic 'fern-like' pattern on a slide (pre- cleaned, saline free slides are required), viewed under low power on a microscope Procedure: When the slide has completely air dried (at least 5 to 7 minutes), place it on the stage of the light microscope provided for the procedure. Examine the slide under low power (10X). Look for fern-like crystals. If positive for amniotic fluid, this crystal formation will be present in most microscopic fields. A small amount of cervical mucus is allowed to air- dry on a clean, saline-free glass slide
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Fetal Fibronectin fFN present in cervical secretions <22 wks, >34 wks Used for assessment of potential PTB Positive result (>50 ng/dl) may be indicative of PROM and represents disruption of decidua- chorionic interface In PPROM, Sensitivity-98.2%, Specificity-26.8%.
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Ultrasonography 50-70% of women with PPROM have low AFV on US
Mild reduction requires further investigation Rule out other causes (Renal agenesis, utero- placental insufficiency, obstructive uropathy) Measure for pockets of fluid and quantitate AFV into AFI Ultrasound showing 7 cm pocket of fluid
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Transabdominal Injection of Dye (Amniocentesis)
Under ultrasound guidance a high- gauge long needle is inserted through the abdomen and membranes into the uterine cavity and amniotic fluid can be collected for testing of chorioamnionitis, in addition to fetal lung maturation studies. After fluid sample collection, 10 cc of mixed Indigo Carmine dye is then injected into the amniotic fluid. The dye is bright blue and if blue is noted on the tampon after mins, the diagnosis of ruptured membranes is made.
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PPROM Sudden gush of clear vaginal fluid with oligohydramnios
SPECULUM EXAM Pooling, Nitrazine, ferning
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Diagnosis of PROM Pooling + Nitrazine + Ferning +
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MANAGEMENT DEPENDS ON THE FOLLOWING FACTORS
Gestational age Availability of NICU Fetal presentation FHR pattern Active distress (maternal/fetal) Is she in labor? Cervical assessment
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Initial Assessment Assess for Maternal-Fetal distress
Assess for Proper dating/GA Assess for infection Exclude occult cord prolapse
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Maternal-Fetal Distress evaluated by Maternal VS, labs, general condition, Fetal distress assessed by FHR pattern, US, Biophysical profile (US examining fetal tone, FBM, AFI, GBM for a score of 2 each if criteria met for a total of 8/8) First priority is to rule out maternal-fetal distress and imminent delivery. Ensure through prenatal records that early US correlate with LMP or EDC is most accurate. Rule out infection through absence of clinical signs and symptoms of chorion in addition to assessment of lab values and amniotic fluid samples obtained through Amniocentesis. Evaluate maternal serum lab values for leukocytosis, left shift, and elevated C-Reactive Protein. Evaluate Amniotic fluid samples for gram stain, leukocyte esterase, glucose, and WBC count.
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Exclude occult cord prolapse through assessment of fetal distress.
Variable FHR decelerations can be seen in the FHR pattern in patients with low or no amniotic fluid. In addition, late decelerations may be seen also in patients with co-existing abruption. Assess for signs and symptoms of chorioamnionitis, abruption, labor, fetal distress. Assess maternal VS for tachycardia and fever.
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Assessing for signs and symptoms of chorioamnionitis
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Secondary Assessment Fetal position Cervical assessment
Determine lung maturity, if indicated Quantify AFV*
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Determine fetal position per Leopold’s and confirm with US for all patients, especially since likelihood of breech presentations is higher at earlier gestations remote from term. Assess for labor by visual examination of the cervix with SSE unless the patient is presenting with regular, painful contractions and appears to be in active labor. Time contractions, assess for pelvic pressure, PALPATE for contractions and strength. Ask mom for length of last labor, if applicable. If patient is in active labor and delivery is inevitable, consider discontinuation of all tocolytics. Again, ONLY do digital cervical exams on patients who are in active labor or patients who need to be delivered for clinical reasons and consistency of cervix needs to be assessed.
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Fetal lung maturity generally assessed at 32 weeks and beyond if necessary. Fetal lungs likely to be immature at gestations less than 32 weeks. Evaluation of FLM should only be evaluated in the absence of absolute delivery indications. Consider risk-benefit ratio of neonatal mortality and morbidity when deciding to induce labor or perform Cesarean section. Quantification of Amniotic fluid volume has increasingly been used to evaluate risk. Patients with vertical pockets of fluid <2 cm have a shorter latency period, and a higher incidence of chorioamnionitis, neonatal sepsis, and endometritis whereas similar patients with a vertical pocket of >2cm have a lesser incidence of these.
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Delivery Indication Maternal-Fetal Distress Infection Abruption
Cord Prolapse
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Expectant Management Typical for GA 32 weeks or less Bed rest
Steroids for lung maturity Tocolytic if indicated for lung maturity Antibiotics Fetal Surveillance Majority Inpatient Observation Assess for Chorioamnionitis Tocolytics – Mgso4, nifedipimine
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Some expectantly manage patients until 34 weeks gestation in the absence of delivery indication.
Betamethasone-may be given 12 mg IM q 12 or 24 hours x 2 total doses. Need at least 48 hours to initiate benefit. May also use Dexamethasone. Steriods may increase WBC’s and therefore baseline CRP should be obtained and consistently monitored. In the absence of delivery indication, may consider tocolysis x 48 hours to assist with benefit of sterods. Tocolysis can be achieved with magnesium sulfate, terbutaline, and nifedipine.
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Prophylactic antibiotics should be obtained after collection of cultures. These cultures may include Group B Strep culture, GC, Chlamydia, Amniotic fluid sample. Broad antimicrobial coverage is recommended. Antibiotic administration reduced the incidence of chorioamnionitis, neonatal infection, and the use of neonatal surfactant. Antibiotic administration for most centers include Ampicillin IV (if no allergy) for 48 hours then a switch to oral amoxillin for an additional five days. Additional of a macrolide considered necessary for broad coverage. Commonly used is a single dose of 1 gram of Azithromycin, or Erythromycin IV with a switch to oral EES after 48 hours for an additional 5 days.
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Infection can be both a cause and a consequence of Preterm Rupture of Membranes.
Most patients require close inpatient observation. Those who might qualify for outpatient management include the extreme previable gestation patients and those who have appeared to have resealed (which is approximately about 5% of PROM patients). Assessment for chorioamnionitis includes amniocentesis (diagnostic), in addition to clinical signs and symptoms and CRP, WBC counts, and other maternal serum infection indices.
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Management: PPROM (24 – 31 wk. gestation)
Expectant management Deliver at 34 wks Unless documented fetal lung maturity GBS prophylaxis Antibiotics Single course corticosteroids Tocolytics No consensus
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Management: PPROM (32 – 33 wk. gestation)
Expectant management Deliver at 34 wks Unless documented fetal lung maturity GBS prophylaxis Antibiotics Corticosteroids No consensus, some experts recommend
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Management: PROM (> 34 wk. gestation)
Proceed to delivery Induction of labor GBS prophylaxis
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Management: Rationale
Antibiotics Prolong latency period Prophylaxis of GBS in neonate Prevention of maternal chorioamnionitis and neonatal sepsis Corticosteroids Enhance fetal lung maturity Decrease risk of RDS, IVH, and necrotizing enterocolitis Tocolytics Delay delivery to allow administration of corticosteroids Controversial, randomized trials have shown no pregnancy prolongation
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Management: Drug Regimen
Antibiotics Ampicillin 2 g IV 6 hrly for 2 days Amoxicillin 500 mg po TDS x 5 days Azithromycin 1 g po x 1 Erythromycin 250mg TDS for 5 days Corticosteroids Betamethasone 12 mg IM OD for 2 days Dexamethasone 6 mg IM BD for 2 days Tocolytics Nifedipine 10 mg po after every 20min 3 times, then 6 hrly for 2 days
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Management: Amniocentesis
Typically performed after 32 wks Tests for fetal lung maturity (FLM) Lecethin/Sphingomyelin ratio (not commonly used, more for historic interest) L/S ratio > 2 indicates pulmonary maturity Phosphatidylglycerol > 0.5 associated with minimal respiratory distress Flouresecence polarization (FLM-TDx II) > 55 mg/g of albumin Lamellar body count 30,000-40,000 If negative, proceed with expectant management until 34 wks
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Risk-Benefit Expectant Management
Benefits Risks Abruption Chorioamnionitis Cord Prolapse Pulmonary Hypoplasia (<19 weeks PPROM Skeletal Deformities Endometritis (1/3) Mature lung profile Advancing GA (reducing risks associated with PTB)
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Maternal complications of prolonged PPROM
Fetal complications of prolonged PPROM Pulmonary hypoplasia Skeletal malformations IUGR IUFD Maternal complications of prolonged PPROM Chorioamnionitis Dry labour Cord prolapse if malpresentation present.
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