- 作者:J. Lawrence Merritt IIa ; lawrence.merritt@seattlechildrens.org" class="auth_mail ; Sverre Vedalb ; Jose E. Abdenurc ; Sylvia M. Aud ; Bruce A. Barshope ; Lisa Feuchtbaumf ; Cary O. Hardingg ; Cheryl Hermerathh ; Fred Loreyf ; David E. Sesserh ; John D. Thompsoni ; Arthur Yud
- 关键词:Newborn screening ; Very-long chain acyl-CoA dehydrogenase deficiency ; False positive ; Clinical outcome research ; VLCADD
- 刊名:Molecular Genetics and Metabolism
- 出版年:April, 2014
- 年:2014
- 卷:111
- 期:4
- 页码:484-492
- 全文大小:741 K
Overall, from 2,802,504 children screened, there were 242 cases screen-positive for VLCADD. There were 34 symptomatic true positive cases, 18 asymptomatic true positives, 112 false positives, 55 heterozygotes, 11 lost to follow-up, and 12 other disorders. One in 11,581 newborns had an abnormal NBS for suspected VLCADD. Comparison of analytes and analyte ratios from the NBS demonstrated statistically significant differences between true positive and false positive groups for C14:1, C14, C14:1/C2, and C14:1/C16. The positive predictive value for all true positive cases was 94%, 54%, and 23% when C14:1 was 鈮?#xA0;2.0 渭M, 鈮?#xA0;1.0 渭M, and 鈮?#xA0;0.7 渭M, respectively. Sequential post-analytical analysis could reduce the referral rate in 25.8% of cases.
This study is the largest reported follow-up of infants with NBS screen-positive results for suspected VLCADD and demonstrates the necessity of developing comprehensive and consistent long-term follow-up NBS systems. Application of clinical information revealed differences between symptomatic and asymptomatic children with VLCADD. Comparison of NBS analytes and analyte ratios may be valuable in developing more effective diagnostic algorithms.