1. Repeated measurement of pregnancy-associated plasma protein-A (PAPP-A) in Down syndrome screening: A validation study
- Author
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Christian Meier, Louis M. Neveux, Anne Summers, Glenn E. Palomaki, James E. Haddow, Tianhua Huang, Andrea O'Donnell, George J. Knight, and David Wright
- Subjects
Adult ,Canada ,medicine.medical_specialty ,Down syndrome ,Pregnancy-associated plasma protein A ,Aneuploidy ,Prenatal diagnosis ,Cohort Studies ,Pregnancy ,Prenatal Diagnosis ,medicine ,Humans ,Pregnancy-Associated Plasma Protein-A ,Genetic Testing ,Genetics (clinical) ,Gynecology ,business.industry ,Obstetrics ,Ultrasound ,Reproducibility of Results ,Obstetrics and Gynecology ,Repeated measures design ,medicine.disease ,Pregnancy Trimester, First ,Pregnancy Trimester, Second ,Female ,Down Syndrome ,business ,Trisomy - Abstract
Objectives To confirm that measuring pregnancy-associated plasma protein-A (PAPP-A) in both first- and second-trimester serum samples improves Down syndrome screening. Methods We selected paired first- and second-trimester stored serum samples from 34 Down syndrome pregnancies (cases) and 514 unaffected pregnancies (controls) and tested the second-trimester samples for PAPP-A and dimeric inhibin-A (DIA). First-trimester PAPP-A measurements were already available, as were second-trimester measurements of alpha-fetoprotein, unconjugated estriol (uE3), and human chorionic gonadotrophin (hCG). Results PAPP-A was lower among cases than controls (0.47 MoM) in the first trimester (at an average of 12.5 weeks); in the second trimester, it was not different (0.91 MoM). Using repeated measures of PAPP-A alone, 21 of 34 cases were detected (62%, 95%CI 44% to 78%) with 5% false positives. At an observed 2% false-positive rate, the detection rates (DR) for the quadruple (69%) and serum integrated (69%) tests were lower than for the repeated measures test (75%). Modelled performance at 12 weeks was similar to these observed findings (70, 75, and 82%, respectively). If the first-trimester samples were collected at 10 weeks, however, DR would be higher (70, 81, and 91%, respectively). Conclusions Adding a repeated measure of PAPP-A to existing serum markers improves Down syndrome screening to levels that are currently obtainable only by including ultrasound measurement of nuchal translucency (NT). Serum-based screening has the advantages of higher availability and reliability at a lower cost, resulting in a more effective screening strategy. A serum-based repeated measures test has a place in routine Down syndrome screening. Copyright © 2006 John Wiley & Sons, Ltd.
- Published
- 2006
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