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本文引用的文献

1
Targeted capture enrichment assay for non-invasive prenatal testing of large and small size sub-chromosomal deletions and duplications.用于大小染色体亚端粒缺失和重复的无创产前检测的靶向捕获富集分析
PLoS One. 2017 Feb 3;12(2):e0171319. doi: 10.1371/journal.pone.0171319. eCollection 2017.
2
Noninvasive prenatal screening for fetal aneuploidy, 2016 update: a position statement of the American College of Medical Genetics and Genomics.胎儿非整倍体无创产前筛查,2016年更新:美国医学遗传学与基因组学学会立场声明
Genet Med. 2016 Oct;18(10):1056-65. doi: 10.1038/gim.2016.97. Epub 2016 Jul 28.
3
Limited Clinical Utility of Non-invasive Prenatal Testing for Subchromosomal Abnormalities.亚染色体异常无创产前检测的临床应用有限
Am J Hum Genet. 2016 Jan 7;98(1):34-44. doi: 10.1016/j.ajhg.2015.11.016. Epub 2015 Dec 17.
4
Current Status of Testing for Microdeletion Syndromes and Rare Autosomal Trisomies Using Cell-Free DNA Technology.使用游离DNA技术检测微缺失综合征和罕见常染色体三体的现状
Obstet Gynecol. 2015 Nov;126(5):1095-1099. doi: 10.1097/AOG.0000000000001091.
5
Clinical experience with single-nucleotide polymorphism-based non-invasive prenatal screening for 22q11.2 deletion syndrome.基于单核苷酸多态性的22q11.2缺失综合征无创产前筛查的临床经验。
Ultrasound Obstet Gynecol. 2016 Feb;47(2):177-83. doi: 10.1002/uog.15754. Epub 2016 Jan 5.
6
Clinical performance of non-invasive prenatal testing (NIPT) using targeted cell-free DNA analysis in maternal plasma with microarrays or next generation sequencing (NGS) is consistent across multiple controlled clinical studies.在多项对照临床研究中,使用微阵列或新一代测序(NGS)对母血中游离DNA进行靶向分析的无创产前检测(NIPT)的临床性能是一致的。
Prenat Diagn. 2015 Dec;35(12):1243-6. doi: 10.1002/pd.4686. Epub 2015 Oct 25.
7
Committee Opinion No. 640: Cell-Free DNA Screening For Fetal Aneuploidy.第640号委员会意见:游离DNA筛查胎儿非整倍体。
Obstet Gynecol. 2015 Sep;126(3):e31-e37. doi: 10.1097/AOG.0000000000001051.
8
Clinical outcome of subchromosomal events detected by whole-genome noninvasive prenatal testing.通过全基因组无创产前检测检测到的亚染色体事件的临床结局。
Prenat Diagn. 2015 Oct;35(10):999-1004. doi: 10.1002/pd.4640. Epub 2015 Jul 27.
9
Noninvasive prenatal testing for 22q11.2 deletion syndrome: deeper sequencing increases the positive predictive value.22q11.2缺失综合征的无创产前检测:深度测序可提高阳性预测值。
Am J Obstet Gynecol. 2015 Aug;213(2):254-5. doi: 10.1016/j.ajog.2015.05.028. Epub 2015 May 15.
10
Prevalence of recurrent pathogenic microdeletions and microduplications in over 9500 pregnancies.9500 多例妊娠中复发性致病性微缺失和微重复的患病率
Prenat Diagn. 2015 Aug;35(8):801-9. doi: 10.1002/pd.4613. Epub 2015 Jun 24.

使用基于靶向微阵列的游离DNA检测进行22q11.2缺失的产前筛查。

Prenatal Screening for 22q11.2 Deletion Using a Targeted Microarray-Based Cell-Free DNA Test.

作者信息

Schmid Maximilian, Wang Eric, Bogard Patrick E, Bevilacqua Elisa, Hacker Coleen, Wang Susie, Doshi Jigna, White Karen, Kaplan Jennifer, Sparks Andrew, Jani Jacques C, Stokowski Renee

机构信息

Ariosa Diagnostics Inc., Roche Sequencing Solutions, Inc., San Jose, California,

Ariosa Diagnostics Inc., Roche Sequencing Solutions, Inc., San Jose, California, USA.

出版信息

Fetal Diagn Ther. 2018;44(4):299-304. doi: 10.1159/000484317. Epub 2017 Nov 8.

DOI:10.1159/000484317
PMID:29131052
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6390460/
Abstract

OBJECTIVE

To determine the performance of a targeted microarray-based cell-free DNA (cfDNA) test (Harmony Prenatal Test®) for the identification of pregnancies at increased risk for 22q11.2 deletion.

METHODS

Test performance was determined in 2 steps including a total of 1,953 plasma samples. Analytical validation was performed in 1,736 plasma samples. Clinical verification of performance was performed in an additional 217 prospectively ascertained samples from pregnancies with fetal deletion status determined by diagnostic testing.

RESULTS

Analytical sensitivity was 75.4% (95% CI: 67.1-82.2%) based on 122 samples with deletions ranging from 1.96 to 3.25 Mb. In 1,614 presumed unaffected samples, specificity was determined to be at least 99.5% (95% CI: 99.0-99.7%). In the clinical cohort, 5 of 7 samples from pregnancies affected with 22q11.2 deletion were determined to have a high probability of deletion. There were no false positive results in the 210 unaffected samples in this cohort. These clinical data are consistent with the performance demonstrated in the analytical validation.

CONCLUSIONS

cfDNA testing using a targeted microarray-based technology is able to identify pregnancies at increased risk for 22q11.2 deletions of 3.0 Mb and smaller while maintaining a low false positive rate.

摘要

目的

确定基于靶向微阵列的游离DNA(cfDNA)检测(Harmony产前检测®)在识别22q11.2缺失风险增加的妊娠中的性能。

方法

检测性能分两步确定,共纳入1953份血浆样本。在1736份血浆样本中进行分析验证。在另外217份通过诊断检测确定胎儿缺失状态的前瞻性确定样本中进行性能的临床验证。

结果

基于122份缺失范围为1.96至3.25 Mb的样本,分析灵敏度为75.4%(95%置信区间:67.1 - 82.2%)。在1614份假定未受影响的样本中,特异性确定为至少99.5%(95%置信区间:99.0 - 99.7%)。在临床队列中,7份22q11.2缺失妊娠样本中有5份被确定有高概率的缺失。该队列中210份未受影响的样本没有假阳性结果。这些临床数据与分析验证中显示的性能一致。

结论

使用基于靶向微阵列的技术进行cfDNA检测能够识别3.0 Mb及更小的22q11.2缺失风险增加的妊娠,同时保持低假阳性率。