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Fetal Fibronectin Testing for Suspected Preterm Labour An emerging standard of care (Note: Please feel free to use your own background design) Fetal Fibronectin Testing for Suspected Preterm Labour Objectives Discuss incidence of preterm labour provincially and nationally Describe the benefits of fetal fibronectin testing Outline insert province approach to this emerging standard of care Provide detailed clinical decision making and procedures for fFN testing Preterm Labour (< 37 weeks) 1 in 5 pregnant women exhibit signs and symptoms of preterm labour. 3-4 % of births occur before 34 weeks Up to 70% of women identified as “highrisk” deliver at term. Maximum clinical judgment sensitivity for del <1week from admission was <50% with minimal cervical dilatation (< 3 cm.). Preterm Birth Preterm birth rate is defined as the number of live births with a gestational age less than 37 weeks completed weeks gestation >7.6% (all Provinces) of all pregnancies result in preterm birth Sources: ACOG Technical Bulletin,1995, No. 206; National Vital Statistics Report 2000;48(3). St John EB et al. Am J Obstet Gynecol. 2000;182:170-175. Macones, Am J ObGyn, Vol 181, 12/99 Rate of Preterm Delivery by Province/Territory (excluding Ontario) 2000 Add own provincial data The Challenge… The preterm birth rate has not decreased in the last thirty years!!! Rate of preterm birth Canada (excluding Ontario), 1991-2000 Preterm Births per 100 live births 8 7 6.6 6.7 6.6 6.8 7.0 7.1 7.1 7.2 7.4 7.6 6 20 percent increase 5 1991 1992 1993 1994 1995 1996 1997 1998 1999 2000 Source: CPSS Report 2003 p. 74 Calendar year Preterm Birth How do we identify who is at Risk? Risk Factors Fetal Fibronectin Cervical Length Symptoms of PTL Prevention/Intervention Strategies Hydration Tocolytics Bedrest Education Home Frequent Targeting Uterine Digital High Risk Monitoring Exam Women Population Based strategies Risk Assessment Markers Biophysical markers Measurement of cervical length Biochemical markers Fetal fibronectin (fFN) Salivary estriol (E3) Corticotropin-releasing hormone (CRH) Interleukin-6 (IL-6) Potential Benefits of An EvidenceBased, Risk Assessment Marker Identify women who are truly at risk. Identify and reassure women who are not at risk. Avoid separation of mother from her family. Avoid unnecessary expense of extended assessment time, admission time, transport to a tertiary centre. Avoid unnecessary tocolytic and steriod use. Improved resource utilization. Potential research benefits e.g. focus tocolytic trials on women who will potentially benefit. Fetal Fibronectin (ƒFN) Fetal Fibronectin (fFN) is not new in obstetrics practice 1st literature appeared in 1985; as an oncogene marker. 1st OB-specific literature appeared in 1991 in New England J. of Medicine by Lockwood, et al. >200 peer reviewed OB articles now published, 3 meta analyses, 9 Canada-specific abstracts presented at SOGC. Canada specific data documents reduced medication use, reduced hospital day stays, reduced transports Canadian data is from level III hospitals, rural and remote hospitals. What is Fetal Fibronectin (ƒFN) Glycoprotein found in extracellular matrix of amniotic membranes. Binds chorion to decidua. Normally found in cervico-vaginal secretions until 22 weeks gestation and again near the time of labour. Released into cervical/vaginal fluid in response to inflammation or separation of amniotic membranes from decidua. • Presence after 24 weeks is indicative of imminent labour Fetal Fibronectin (ƒFN) Normal ƒFN Expression by Gestational Age Key Terminology for Evaluating PTD Diagnostics Negative Predictive Value (NPV): Answers the question, “If a woman has a negative test, how likely is she NOT to deliver prematurely?” Positive Predictive Value (PPV): Answers the question, “If a woman has a positive test, how likely is she to deliver prematurely?” Sensitivity: Percent of women who have preterm delivery whom the test correctly identifies Specificity: Percent of women who do NOT have preterm delivery whom the test correctly identifies Utility of ƒFN for Predicting PTB in Symptomatic Women PPV(%) NPV(%) Cx Dilatation(cm) Lockwood, 1991 (n=117) Morrison, 1993 (n=28) Iams, 1995 (n=192) Burrus, 1995 (n=37) Bartnicki, 1996 (n=112) Peaceman, 1997 (n=725) 83 64 60 79 79 43 81 93 76 63 83 87 None 1 3 3 2 3 Women with Threatened Preterm Labour (1/25 deliver <14 days) ƒFN (80%) ƒFN + (20%) 1/125 Deliver <14 days 1/6 Deliver <14 days Peaceman, AJOG 1997; 177:13-8 Nova Scotia Pilot Study April 2002-March 2004 (Armson & Scott et. al.) Prospective cohort study Objectives To determine if introduction of rapid ƒFN testing for suspected PTL will: 1. Reliably predict preterm birth 2. Result in a reduction of: - PTL admissions/maternal transfer rates - length of stay, tocolytic/corticosteroid use - reproductive health care costs without compromising neonatal outcomes Conclusions from Nova Scotia Study A negative ƒFN test for suspected PTL accurately identifies women not likely to deliver within 14 days (98% -99% accurate) A positive ƒFN test identifies women at high risk for preterm birth - 24% 7 days - 28% 14 days - 31% 34 weeks - 48% 37 weeks Diagnostic accuracy of ƒFN superior to clinical criteria for women with suspected preterm labour Conclusions from Nova Scotia Study Criteria for clinical use of ƒFN appear to be broad and inconsistent Clinicians/patients somewhat reluctant to adhere to guidelines of non-intervention for negative ƒFN results, particularly in regional centres. Potential for reduction in maternal transfers, hospital admissions and associated health care costs Results from the Nova Scotia Study Implementation of province-wide Fetal Fibronectin testing currently ongoing Seed funding provided by NS Department of Health Goals To reduce unnecessary maternal transfers and admissions for suspected preterm labour To reduce psychosocial and financial burdens for families BC Study Fetal Fibronectin collected by speculum exam from admitted patients with symptomatic preterm labour Assays were performed in our laboratory. The results were revealed to the clinician within 1 – 8 hours A retrospective chart review was undertaken to assess pregnancy outcome An estimate of the total hospital days saved was developed using the ALOS for patients admitted with a diagnosis of PTL prior to the utilization of the Fetal Fibronectin Assay Results Of 62 patients tested, outcomes were known for 47 patients. Delivered < 14 days Delivered > 14 days FFN +ve 1 7 FFN –ve 1 38 Sensitivity = 50% PPV = 12.5% Specificity = 84% NPV = 97% Farquharson, D., Lee, L.,Garg, A. Clinical utilization and cost saving analysis of fetal fibronectin assay in a tertiary care institution. Abstracted presented at 2003 SOGC meeting, Charlottetown. BC Study Results A total of 62 assays were conducted between May 2002 and March 2003 Ages 18 – 39, mean 30 GA on admission: 20 – 33 weeks Length of stay ranged 1 – 44 days, mean 4.7 days Nulliparas: 55 % Multiparas: 45 % BC Study Conclusion Our experience in which Fetal Fibronectin Assay (Adeza TLI) was used as an adjunct to diagnosis and management of preterm labour suggest reduced hospital utilization, and earlier reverse transfer of these patients to their referring institutions without adverse sequelae. Cost Savings (literature) Reduction in PTL admissions $486,000 saved (Joffe et al, AJOG 1999) Reduction in maternal transfers $30,297 saved (Giles et al, AJOG 2000) Resource Utilization - Canada Royal Victoria Hospital Observational cohort design 20 week periods before and after ƒFN Singletons, 24-34 weeks, suspected PTL Abenhaim JOGC 2005; 27:689-94 Effect of ƒFN on Resource Utilization _________________________________________________________ Baseline Period Study Period p value _________________________________________________________ Patients 116 116 Preterm Births 9 (7.8%) 10 (8.6%) NS PTL Admissions 28 (24.1%) 14 (12.1%) 0.02 Days Hospitalized 145 28 Mean LOS 5.2 0.6 0.01 Admission Costs $102,660 $26,169 Mean Cost $3,666 $581 0.01 Abenhaim, JOGC 2005; 27:689-94 Considerations Cost: Approximately $100+ per test Patient demand – not experienced by other centres Physician overuse Estimate 20 -25 per years based on 2500 births/yr Close adherence to guideline Savings Cost of admission Cost of transfer Optimal use of tertiary beds Maternal/family reassurance/satisfaction Fetal Fibronectin Decision-Making Algorithm Patient <34 wks Gestation with Symptoms of Preterm Labour • • Evidence of Ruptured Membranes • • Speculum exam before VE fFN swab from posterior fornix (see Appendix A) Cultures • Management of PROM Discard fFN swab Intact Membranes Vaginal Examination Cx ≥ 3 cm Dilation Cx < 3 cm Dilated Cx Long + Closed • Regular uterine activity • Diagnosis preterm labour • • • • Contractions subsided No clinical evidence of preterm labour • • Reassure mother Discard fFN swab • • Ongoing uterine activity Clinical suspicion of preterm labour Treat for preterm labour Discard fFN swab Send fFN swab Positive • • Treat for preterm labour - Tocolytics - Corticosteroids - Antibiotics Consider transfer to appropriate level of care BCRCP (2005) Obstetric Guideline 2A – Preterm Labour, p. 11 Negative • • • • Reassure mother F/U endovaginal ultrasound of the cervix (if available) Treatment of BV Consider repeat test in 7-14 days, if symptomatic Guidelines for Use of fFN test Obtain specimen prior to procedures that may disrupt cervix: Digital examination Vaginal ultrasound Microbiologic culture Pap smear Source: Honest et.al. BMJ, Aug 2002 Specimen should not be obtained in presence of: Cervical dilatation >3 cm PROM Soaps, gels, lubricants, or disinfectants Cervical cerclage Moderate or gross vaginal bleeding Sexual intercourse within 24 hours Specimen Collection for ƒFN Testing Lightly rotate swab across either the posterior fornix of the vagina or the ectocervical region of the external cerical os for 10 seconds. Specimen Collection for ƒFN Testing Remove swab and immerse Dacron® tip in buffer Break the shaft even with the top of the tube (at the score) Specimen Collection for ƒFN Testing Align the shaft with the hole inside the tube cap and push down tightly over the shaft to seal the tube. Fetal Fibronectin (ƒFN) Test Results Rapid fFN for the TLi™ System Analyzer produces results in 23 minutes Around-the-clock availability Rapid fFN is run like a pregnancy test Several sites in Canada run the assay in L&D Implementation of fFN in insert province/territory or region Conclusion Fetal Fibronectin is a useful adjunct to diagnosis and manage preterm labour Reduced hospital admission and transfers of women with symptoms of preterm labour. Decreased costs associated with hospital admissions, transfers Improved identification of women who need corticosteroid and tocolytic therapy Provide reassurance to women and families Thank you!