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Genetic Testing in Pregnancy

Genetic Testing in Pregnancy . Johanna Warren, MD OAFP Women’s Health Winter Conference January 19, 2014. What genetic screening test do you routinely offer your patients? . Quad/ Penta screen Integrated Screening Nuchal Translucency (NT) only Stepwise Sequential Screen NIPT ( cffDNA )

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Genetic Testing in Pregnancy

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  1. Genetic Testing in Pregnancy Johanna Warren, MD OAFP Women’s Health Winter Conference January 19, 2014

  2. What genetic screening test do you routinely offer your patients? • Quad/Penta screen • Integrated Screening • Nuchal Translucency (NT) only • Stepwise Sequential Screen • NIPT (cffDNA) • none

  3. Learning Objectives • Use the concepts of pre-test probability, positive and negative predictive values as they apply to testing for fetal aneuploidy. • Outline advantages and disadvantages of various approaches to first-trimester and second-trimester screening as well as invasive diagnostic testing for Down syndrome. • Discuss emerging cell-free fetal DNA (cffDNA) technology and review indications for use in screening. • Summarize the current recommendations for cystic fibrosis screening.

  4. Statistics • Pre-test probability • Prevalence of the disease • Post-test probability after one or more preceding tests • Rough clinical estimation • Positive predictive value (PPV) • the likelihood that an individual with a positive test result truly is affected/has the genetic condition • inherently dependent upon the prevalence • Negative predictive value (NPV) • the likelihood that an individual with a negative test result is truly unaffected/does NOT have the genetic condition • measure of test accuracy

  5. What Makes a Good Screening Test? • The condition should be an important health problem. • There should be an acceptable test for the condition. • High sensitivity to detect not yet clinically detectable condition • High specificity to minimize false positives • The test should be available to the population. • The test should be affordable. • There should be acceptable treatment for the condition. • There should be a “latent stage” of the disease, allowing for detection/testing before a critical point, during which treatment would be optimal.

  6. What is the purpose of antenatal genetic testing? • Assess risk for chromosome abnormalities • particularly Down syndrome & Trisomy 18 • Determine which pregnancies should be offered invasive prenatal diagnosis

  7. Who Should Be Screened? • ACOG Practice Bulletin (2007) • All pregnant women, regardless of their age, should be offered screening and diagnostic testing for aneuploidy. • Women should be counseled regarding the differences between screening and invasive diagnostic testing. • Ideally, patients seen early in pregnancy should be offered screening that combines 1st and 2nd trimester testing • Screening test chosen will depend on availability of NT US as well as CVS

  8. Testing for Fetal Aneuploidy – Focus on Down Syndrome (trisomy 21) • Explosion of available screening tests • Detection of Down Syndrome 90+% with non-invasive screening tests • Confirmation diagnosis still requires invasive testing • Amniocentesis • Chorionic villus sampling

  9. Quick Review • Several methods for combining first- and second-trimester screening reach higher detection rates for Trisomy 21 than either first- or second-trimester screening alone. • Common options: • Ultrasound: Nuchal Translucency • Integrated Screenings • Quadruple/Penta Marker Screenings • Stepwise Sequential Screening

  10. First Trimester - Ultrasound • Nuchal Translucency (NT) • Normal: 1-3mm • Increased NT is an indication of a chromosomal abnormality, single gene defect, or birth defects (commonly cardiac defects) • Nasal Bone • Absent/hypoplastic in 70% T21 • DuctusVenosus – reversed a-wave flow • Detection rate 75%, FPR 5% • Tricuspid Regurgitation • Detection rate 67.3% in T21, FPR 5.2%

  11. Integrated Screenings • Integrated Screening • Ultrasound for Nuchal Translucency (NT) + serum PAPP-A/hCG analysis between 10-13.6wks GA; results of these tests are HELD • Serum quad screen test between 15 -19 wks GA • At that time, the results of all the studies, combined with risk assessment due to the patient's age, are used to present a single-risk figure • Serum Integrated Screening • first-trimester serum PAPP-A/hCG test result is combined with a second-trimester quad screen test to provide a single-risk figure (no NT US)

  12. Quadruple Marker Screening • Measure raw values of: • AFP (alpha fetoprotein) • ue3 (unconjugatedestriol) • hCG (human chorionic gonadotropin) • DIA (dimericinhibin A) • Compare to median value for the appropriate gestational age (MoM) • Valid between 14-22.9 weeks GA (optimal 16-18wks); risk of NTD not provided for samples collected prior to 15 weeks.

  13. Stepwise Sequential Screening • First Trimester • NT US + serum PAPP-A analysis between 10-13.6wks GA • Results combined with the patient's age-associated risk, • Patient is given a risk assessment for aneuploidy • may choose at this time to undergo invasive testing (e.g., amnio or CVS), or add quad screen test at 15-19 wks GA • Second Trimester • Quad screen test at 15-19 wks GA • a new risk is assessed based on the results of patient’s age and both the first- and second-trimester screening test results

  14. Sequential Screening • How do you decide when to proceed with invasive testing? • Risk of miscarriage (approximate; operator-specific) • chorionic villus sampling (CVS) ~ 0.5-1/100 • amniocentesis ~1/1000 • After 1st trimester results return: • If risk is greater than ~1 in 50, offer CVS • If risk is less than ~1 in 1,000, advise no further testing is necessary. • If risk is between these two (arbitrary) cutoffs, offer quad screen test after 15 wks GA, and determine a new risk assessment

  15. FASTER Trial Data

  16. What do you do with… • Normal Ultrasounds • Other Abnormal Serum Studies

  17. Normal Ultrasounds • Normal ultrasound: 50-60% decrease in risk for chromosome abnormalities • Remember that at least 30% of fetuses with Down syndrome have NO abnormal ultrasound findings!

  18. Low 1st Trimester PAPP-A • Pregnancies with PAPP-A of ≤ 5%tile (0.4MoM) are at increased risk for: • Spontaneous fetal loss < 24 wks GA • Low birth weight • Preeclampsia • Gestational HTN • Preterm birth and stillbirth • Preterm premature rupture of membranes • Placental abruption

  19. Abnormal 2nd Trimester Serum Values

  20. What’s next?

  21. Cell-free Fetal DNA (cffDNA) • Screening or Diagnosis? • Known as “Noninvasive Prenatal Testing” or “NIPT” • Technology uses circulating cell free fetal DNA found in the maternal plasma • Thought to be derived primarily from placenta • New recognition of limitations of screening with pregnancies with placental mosacisms • Unclear data for egg donor pregnancies • Available as early as 10th week of pregnancy • Cleared from maternal blood almost immediately after childbirth

  22. Cell-free Fetal DNA (cffDNA) • 2012 publications (Sparks et al., Ashoor et al., Bianchi et al.) • targeted (chromosome-selective) sequencing of chromosomes 18 and 21 • highly accurate • potentially more cost-effective • Technology can be expected to identify 98% of cases of T21 with a false-positive rate of < 0.5%. • Multiple different labs • MaterniT21plus by Sequenom • Verifiby Verinata • Harmony by Ariosa

  23. Cell-free Fetal DNA (cffDNA) Labs • MaterniT21plus by Sequenom • >99% detection for T21, T18 • ~90% detection for T13 • <1% false positive rate • Cost: $235-2700 • Verifi by Verinata • >99% detection for T21, T18 • ~80% detection for T13 • >90% detection for 45,X • <1% false positive rate • Cost: $200-1200 • Harmony by Ariosa • >99% detection for T21, T18 • ~80% detection for T13 • <1% false positive rate • Cost: up to $795

  24. Cell-free Fetal DNA (cffDNA) • ACOG Committee Opinion, Dec. 2012 – “Noninvasive Prenatal Testing for Fetal Aneuploidy” • cffDNA testing should be an informed patient choice after counseling and should not be part of routine prenatal laboratory assessment. • cffDNA testing should not be offered to low-risk women or women with multiple gestations (has not been studied). • A negative cffDNA test result does not ensure an unaffected pregnancy. • A patient with a positive test result should be referred for genetic counseling and should be offered invasive prenatal diagnosis for confirmation of test results.

  25. Indications for Considering Use of cffDNA for Screening • Maternal Age ≥ 35 years at delivery • Fetal ultrasound findings indicating increased risk of aneuploidy • CPCs? • IEF? • Clinodactyly? • Absent/hypoplastic nasal bone? • History of a prior pregnancy with a trisomy • Positive test result for aneuploidy (any serum test) • Parental balanced translocation with increased risk of fetal trisomy 13 or 21.

  26. Considerations • Primary insurers are generally reimbursing for first-trimester screenings, including NT ultrasounds as well as NIPT. • Are there referral sites available to your patients for appropriate genetic counseling and NT US measurements? What about for CVS and/or amniocentesis? • What testing strategy makes the most sense for your patients? • How do you see it evolving in the next 1-2 years?

  27. Testing for Cystic Fibrosis (CF) • Site of genetic defect = CF Transmembrane Regulator (CFTR) gene, a chloride channel protein • ~ 1700 mutations of CFTR gene have been described • Disease incidence: 1 in 2500 in the non-Hispanic white population • Carrier frequencies: • 1/24-25 Caucasians of European descent or Ashkenazi Jews • 1/58 Hispanic American • 1/61 African American • 1/94 Asian American

  28. CF Genetic Testing • Difficult to assign a single ethnicity to individuals • ACOG 2011 Recommendation – offer CF carrier screening to all women of reproductive age • Need to be screened only once

  29. CF Parental Genetic Testing • Sequential testing • Test mother for carrier state • If positive, test father • Concurrent testing • Test mother and father simultaneously • Advantage: can be done prior to conception • Limitation: depends on accurate ID of father • If both parents are unaffected but family hx of CF exists: • Genetic counseling • Identify if CFTR mutation analysis in affected family member is available

  30. Positive CF Testing • If both parents are carriers… • and prior to conception • offer ART options for diagnosis of embryo • and currently pregnant • offer CVS or amnio to confirm status of fetus • No in-utero treatments exist • Variable clinical scenarios, with median survival for patients 37yrs

  31. “Residual Risk” • Potential risk of having an affected child with CF after testing is completed and is negative • Varies by race and current testing panel for gene abnormalities • Will vary over time and by laboratory • Newborn screening panels that include CF screening do not replace maternal carrier testing

  32. Summary Recommendations • Genetic screening in pregnancy (and pre-conception!) is rapidly getting more complex. • OHSU Online Course (FREE!) • 0.5 CME credits available • www.ohsu.edu/prenatal-screening • Understand your patient population and your local capabilities, specifically as they relate to genetic counseling, ultrasound expertise, and diagnostic testing. • Develop practice workflows that allow women to access early genetic screening should they desire.

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