Your search keyword '"Cram, David S."' showing total 24 results

1. Cell-free DNA test for pathogenic copy number variations: A retrospective study.

Author

Duan HL, Li J, Wang WJ, Cram DS, Liu W, Cao PX, Zhu XY, and Hu YL

Subjects

Adult, Cell-Free Nucleic Acids genetics, Chromosome Aberrations, Chromosome Disorders genetics, Female, Humans, Pregnancy, Retrospective Studies, Sequence Analysis, DNA, Chromosome Disorders diagnosis, DNA blood, DNA Copy Number Variations genetics, Genetic Testing methods, Microarray Analysis methods, Prenatal Diagnosis methods

Abstract

Objective: To evaluate the detection rate (DR) by prenatal cell-free DNA test for pathogenic copy number variations (CNVs)＞2 Mb among pregnancies with fetal ultrasound abnormalities., Materials and Methods: This was a retrospective study on 29 pregnant women with fetuses diagnosed as microdeletion/microduplication syndromes by prenatal chromosome microarray analysis (CMA). Cell-free DNA from the maternal plasma was sequenced on the NextSeq CN500 sequencer. The quality standard of unique map reads in a single sample was greater than 10 M and only gains and losses of more than 2 Mb were reported., Results: A total of 24 CNVs were identified by cell-free DNA test among the 21 fetuses with pathogenic CNVs identified by prenatal CMA, including 20 consistent CNVs and 4 inconsistent CNVs. Overall, the DR of cell-free DNA test for pathogenic CNVs ＞2 Mb was 69%. Microdeletions or microduplications at 22q11.2 were the most common CNVs, with a DR of 4/5 (80%) and 3/4 (75%) respectively., Conclusion: Cell-free DNA test exhibited a moderate DR for pathogenic CNVs ＞2 Mb among fetuses with ultrasound abnormalities. Cell-free DNA test could provide an opportunity for early screening before the appearance of abnormalities on fetal ultrasound, while further clinical data and cost-effectiveness assessment are needed., Competing Interests: Declaration of competing interest There is no conflict of interest in this study., (Copyright © 2021. Published by Elsevier B.V.)

Published

2021

2. REDBot: Natural language process methods for clinical copy number variation reporting in prenatal and products of conception diagnosis.

Author

Liu M, Zhong Y, Liu H, Liang D, Liu E, Zhang Y, Tian F, Liang Q, Cram DS, Wang H, Wu L, and Yu F

Subjects

Humans, DNA Copy Number Variations, Electronic Health Records, Genetic Testing methods, Natural Language Processing, Prenatal Diagnosis methods, Software

Abstract

Background: Current copy number variation (CNV) identification methods have rapidly become mature. However, the postdetection processes such as variant interpretation or reporting are inefficient. To overcome this situation, we developed REDBot as an automated software package for accurate and direct generation of clinical diagnostic reports for prenatal and products of conception (POC) samples., Methods: We applied natural language process (NLP) methods for analyzing 30,235 in-house historical clinical reports through active learning, and then, developed clinical knowledge bases, evidence-based interpretation methods and reporting criteria to support the whole postdetection pipeline., Results: Of the 30,235 reports, we obtained 37,175 CNV-paragraph pairs. For these pairs, the active learning approaches achieved a 0.9466 average F1-score in sentence classification. The overall accuracy for variant classification was 95.7%, 95.2%, and 100.0% in retrospective, prospective, and clinical utility experiments, respectively., Conclusion: By integrating NLP methods in CNVs postdetection pipeline, REDBot is a robust and rapid tool with clinical utility for prenatal and POC diagnosis., (© 2020 The Authors. Molecular Genetics & Genomic Medicine published by Wiley Periodicals LLC.)

Published

2020

3. Non-invasive prenatal testing of pregnancies at risk for phenylketonuria.

Author

Duan H, Liu N, Zhao Z, Liu Y, Wang Y, Li Z, Xu M, Cram DS, and Kong X

Subjects

Hematologic Tests methods, Humans, Phenylketonurias genetics, Retrospective Studies, Phenylalanine Hydroxylase genetics, Phenylketonurias diagnosis, Prenatal Diagnosis methods

Abstract

Background: Phenylketonuria (PKU) is a common metabolic disorder caused predominately by mutations in the phenylalanine hydroxylase ( PAH ) gene. The aim of the study was to design and validate the performance of a non-invasive prenatal test (NIPT) for PKU using circulating single molecule amplification and resequencing technology (cSMART)., Methods: A total of 18 couples at genetic risk for having a child with PKU were recruited to the study. Gold standard invasive prenatal diagnosis (IPD) was performed on amniocyte or villus cell DNA by Sanger sequencing, targeting the known parental PAH mutations. Retrospectively, NIPT was also performed on stored maternal plasma samples from the 18 pregnancies by a multiplex cSMART assay designed to target all known DNA variants in the PAH gene., Results: Benchmarking against IPD results, NIPT correctly genotyped all fetuses, including six compound heterozygotes with PKU, four normal non-carriers of PKU and eight heterozygote carriers of PKU comprising five cases of a maternally inherited mutation and three cases of a paternally inherited mutation., Conclusions: The NIPT cSMART PKU assay was highly sensitive and specific for mutation detection and correct assignment of fetal genotypes. Based on comprehensive mutation coverage across the PAH gene, the assay may initially have clinical utility as a pregnancy screening test for high-risk carrier couples., Competing Interests: Competing interests: YL, YW, ZL, MX and DSC are employees of Berry Genomics Corporation. No one holds any stocks or bonds., (© Article author(s) (or their employer(s) unless otherwise stated in the text of the article) 2019. All rights reserved. No commercial use is permitted unless otherwise expressly granted.)

Published

2019

4. A quantitative cSMART assay for noninvasive prenatal screening of autosomal recessive nonsyndromic hearing loss caused by GJB2 and SLC26A4 mutations.

Author

Han M, Li Z, Wang W, Huang S, Lu Y, Gao Z, Wang L, Kang D, Li L, Liu Y, Xu M, Cram DS, and Dai P

Subjects

Connexin 26, Genotype, Humans, Reproducibility of Results, Sensitivity and Specificity, Sulfate Transporters, Connexins genetics, Deafness diagnosis, Deafness genetics, Genes, Recessive, Genetic Testing methods, Membrane Transport Proteins genetics, Mutation, Prenatal Diagnosis methods

Abstract

PurposeThe aim of this study was to assess the performance of a noninvasive prenatal screening (NIPS) assay for accurate fetal genotyping of pregnancies at genetic risk for autosomal recessive nonsyndromic hearing loss (ARNSHL).MethodsA total of 80 pregnant couples carrying known mutations in either the GJB2 or SLC26A4 genes associated with a risk for ARNSHL were recruited to the study. Fetal amniocyte samples were genotyped by invasive prenatal screening (IPS), whereas the cell-free fetal DNA present in maternal plasma samples was genotyped using a novel NIPS method based on circulating single-molecule amplification and resequencing technology (cSMART).ResultsIPS of the 80 at-risk pregnancies identified 20 normal homozygote, 42 heterozygote, 5 affected homozygote, and 13 affected compound heterozygote fetuses. Benchmarking against IPS, 73 of 80 fetuses (91.3%) were correctly genotyped by the cSMART NIPS assay. A low fetal DNA fraction (<6%) was identified as the main contributing factor in five of seven discordant NIPS results. At fetal DNA fractions >6%, the sensitivity and specificity of the cSMART assay for correctly diagnosing ARNSHL were 100 and 96.5%, respectively.ConclusionBased on key performance indicators, the cSMART NIPS assay has clinical potential as an alternative to traditional IPS of ARNSHL.

Published

2017

5. Contribution of maternal copy number variations to false-positive fetal trisomies detected by noninvasive prenatal testing.

Author

Zhou X, Sui L, Xu Y, Song Y, Qi Q, Zhang J, Zhu H, Sun H, Tian F, Xu M, Cram DS, and Liu J

Subjects

Adult, Diagnostic Errors, False Positive Reactions, Female, Fetal Diseases genetics, High-Throughput Nucleotide Sequencing, Humans, Karyotyping methods, Mothers, Pregnancy, Sequence Analysis, DNA methods, Trisomy genetics, DNA Copy Number Variations genetics, Fetal Diseases diagnosis, Prenatal Diagnosis methods, Trisomy diagnosis

Abstract

Objective: The aim of the study was to determine the contribution and significance of maternal copy number variations (CNVs) to false-positive noninvasive prenatal testing (NIPT) trisomy results., Methods: A total of 112 021 patients were referred for NIPT. Fetal aneuploidy testing was performed using low coverage massively parallel sequencing, and results reported as chromosome Z-scores. Copy number variation sequencing (CNV-Seq) was used to detect maternal DNA CNVs., Results: Confirmatory amniocentesis and karyotyping of 563 of 781 patients (72%) receiving a positive trisomy result revealed 489 true and 74 false positives. In 6 of these 74 patients (8.1%), CNV-Seq revealed non-pathogenic maternal duplications (1.76-10.90 megabases) on the chromosome associated with the fetal trisomy. There was a strong correlation of higher Z-scores with increasing size of the maternal CNVs (R 2  = 0.94). When the contribution of the maternal CNV-Seq reads to chromosome Z-scores were removed, all original Z-scores shifted to the normal range., Conclusions: Maternal CNVs can potentially contribute to a small but significant number of false-positive fetal trisomies detected by NIPT. To avoid unnecessary invasive procedures and better manage patients, we recommend that confirmatory maternal DNA sequencing is performed when the NIPT methodology used indicates a high risk of a maternal CNV. © 2017 John Wiley & Sons, Ltd., (© 2017 John Wiley & Sons, Ltd.)

Published

2017

6. Development and validation of a fetal genotyping assay with potential for noninvasive prenatal diagnosis of hereditary hearing loss.

Author

Chen Y, Liu Y, Wang B, Mao J, Wang T, Ye K, Ye Y, Cram DS, and Li H

Subjects

Connexin 26 genetics, Connexins genetics, DNA blood, Female, Genetic Testing methods, Heterozygote, Homozygote, Humans, Infant, Newborn, Membrane Transport Proteins genetics, Mutation, Phenotype, Pregnancy, Sulfate Transporters, Genotype, Genotyping Techniques methods, Hearing Loss congenital, Hearing Loss genetics, Prenatal Diagnosis methods

Abstract

Objective: Inherited non-syndromic hearing loss (NSHL) is a common sensory disorder that afflicts otherwise healthy individuals. The aim of the study was to evaluate the performance of circulating single molecule amplification and re-sequencing technology (cSMART) for non-invasive prenatal testing (NIPT) of NSHL., Method: Neonatal inheritance of NSHL mutations was determined from bloodspots using SNaPshot genotyping. NIPT of cell-free DNA for fetal NSHL mutations in the GJB2, GJB3 and SLC26A4 genes was performed by a multiplex cSMART assay. The percentage of mutant alleles was used to deduce fetal DNA fractions and assign fetal genotypes., Results: A total of 25 plasma samples selected with different fetal NSHL genotypes were coded and retrospectively analyzed by NIPT. Three normal fetuses, 18 carrier fetuses comprising seven GJB2 109G>A, four GBJ2 235delC, three GJB2 299-300delAT and four SLC26A4 IVS7-2A>G heterozygotes and four affected fetuses comprising two GJB2 109G>A homozygotes, one GBJ2 235delC homozygote and one compound GJB2 235delC/299-300delAT heterozygote were identified. All 25 fetal genotypes determined by the cSMART assay were concordant with neonatal genotypes., Conclusion: The cSMART assay applied to cell-free DNA isolated from maternal plasma of pregnant women is highly accurate for calling correct fetal NSHL genotypes. © 2016 John Wiley & Sons, Ltd., (© 2016 John Wiley & Sons, Ltd.)

Published

2016

7. Identification of copy number variations associated with congenital heart disease by chromosomal microarray analysis and next-generation sequencing.

Author

Zhu X, Li J, Ru T, Wang Y, Xu Y, Yang Y, Wu X, Cram DS, and Hu Y

Subjects

Chromosome Aberrations, Female, Humans, Pregnancy, Prospective Studies, Chromosome Disorders diagnosis, DNA Copy Number Variations, Genetic Testing methods, Heart Defects, Congenital genetics, High-Throughput Nucleotide Sequencing, Microarray Analysis methods, Prenatal Diagnosis methods

Abstract

Objective: To determine the type and frequency of pathogenic chromosomal abnormalities in fetuses diagnosed with congenital heart disease (CHD) using chromosomal microarray analysis (CMA) and validate next-generation sequencing as an alternative diagnostic method., Method: Chromosomal aneuploidies and submicroscopic copy number variations (CNVs) were identified in amniocytes DNA samples from CHD fetuses using high-resolution CMA and copy number variation sequencing (CNV-Seq)., Result: Overall, 21 of 115 CHD fetuses (18.3%) referred for CMA had a pathogenic chromosomal anomaly. In six of 73 fetuses (8.2%) with an isolated CHD, CMA identified two cases of DiGeorge syndrome, and one case each of 1q21.1 microdeletion, 16p11.2 microdeletion and Angelman/Prader Willi syndromes, and 22q11.21 microduplication syndrome. In 12 of 42 fetuses (28.6%) with CHD and additional structural abnormalities, CMA identified eight whole or partial trisomies (19.0%), five CNVs (11.9%) associated with DiGeorge, Wolf-Hirschhorn, Miller-Dieker, Cri du Chat and Blepharophimosis, Ptosis, and Epicanthus Inversus syndromes and four other rare pathogenic CNVs (9.5%). Overall, there was a 100% diagnostic concordance between CMA and CNV-Seq for detecting all 21 pathogenic chromosomal abnormalities associated with CHD., Conclusion: CMA and CNV-Seq are reliable and accurate prenatal techniques for identifying pathogenic fetal chromosomal abnormalities associated with cardiac defects. © 2016 John Wiley & Sons, Ltd., (© 2016 John Wiley & Sons, Ltd.)

Published

2016

8. Maternal X chromosome copy number variations are associated with discordant fetal sex chromosome aneuploidies detected by noninvasive prenatal testing.

Author

Wang S, Huang S, Ma L, Liang L, Zhang J, Zhang J, and Cram DS

Subjects

Female, Humans, Male, Pregnancy, Aneuploidy, Chromosomes, Human, X genetics, DNA Copy Number Variations genetics, Prenatal Diagnosis, Sex Chromosome Disorders genetics

Abstract

Background: The sensitivity and specificity of noninvasive prenatal testing (NIPT) for detection of sex chromosome aneuploidies (SCAs) compared to common autosomal trisomies are significantly lower. We speculated that in addition to altered maternal X chromosome karyotype, maternal X chromosome copy number variations (CNVs) may also contribute to discordant NIPT SCA results., Methods: Clinical NIPT was performed for pregnant women at a single hospital. Copy number variation sequencing (CNV-Seq) was used to identify and quantitate the copy number of maternal X chromosome CNVs for each positive SCA pregnancy., Results: Two out of 25 SCA positive NIPT samples had slightly abnormal ChrX/ChrY z-scores and were referred for invasive test confirmation. However, fetal karyotypes were found to be normal. CNV-Seq analysis of the maternal white blood cell DNA archived from the original two NIPT blood samples identified small CNVs spanning the STS gene, which is associated with X-linked ichthyosis. Correcting for the altered plasma levels of X chromosome DNA caused by the two CNVs and, taking into consideration the phenotypic consequences for X-linked disease, both fetuses were diagnosed as normal., Conclusions: Maternal DNA sequencing is recommended for all positive NIPT SCA results to avoid unnecessary referral for invasive testing and also to evaluate the risk to the fetus of X-linked disease., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2015

9. Feasibility of noninvasive prenatal testing for common fetal aneuploidies in an early gestational window.

Author

Shi X, Zhang Z, Cram DS, and Liu C

Subjects

DNA blood, Feasibility Studies, Female, Fetus embryology, Humans, Pregnancy, Aneuploidy, Fetus metabolism, Pregnancy Trimester, First blood, Pregnancy Trimester, Second blood, Prenatal Diagnosis methods

Abstract

Background: Noninvasive prenatal testing (NIPT) by massively parallel sequencing (MPS) of the circulating cell free fetal (cff) DNA during the second trimester of pregnancy is now a frontline test for detecting common fetal chromosomal abnormalities. However, the availability of an earlier test result in the first trimester would enable better clinical management of high-risk pregnancies. The aim of the study was to determine the feasibility of early gestational NIPT., Methods: Plasma DNA libraries were subjected to MPS and chromosomal read counts normalized to reference. Chromosomal aneuploidy was determined by z-scores (-3

Published

2015

10. Noninvasive prenatal testing for Wilson disease by use of circulating single-molecule amplification and resequencing technology (cSMART).

Author

Lv W, Wei X, Guo R, Liu Q, Zheng Y, Chang J, Bai T, Li H, Zhang J, Song Z, Cram DS, Liang D, and Wu L

Subjects

Adenosine Triphosphatases genetics, Alleles, Cation Transport Proteins genetics, Copper-Transporting ATPases, DNA Probes, Female, Gestational Age, Hepatolenticular Degeneration embryology, Heterozygote, Homozygote, Humans, Male, Molecular Diagnostic Techniques instrumentation, Pregnancy, Prenatal Diagnosis instrumentation, DNA blood, DNA genetics, DNA Mutational Analysis methods, Hepatolenticular Degeneration blood, Hepatolenticular Degeneration genetics, Molecular Diagnostic Techniques methods, Prenatal Diagnosis methods

Abstract

Background: Noninvasive prenatal testing (NIPT) for monogenic diseases by use of PCR-based strategies requires precise quantification of mutant fetal alleles circulating in the maternal plasma. The study describes the development and validation of a novel assay termed circulating single-molecule amplification and resequencing technology (cSMART) for counting single allelic molecules in plasma. Here we demonstrate the suitability of cSMART for NIPT, with Wilson Disease (WD) as proof of concept., Methods: We used Sanger and whole-exome sequencing to identify familial ATP7B (ATPase, Cu(++) transporting, β polypeptide) gene mutations. For cSMART, single molecules were tagged with unique barcodes and circularized, and alleles were targeted and replicated by inverse PCR. The unique single allelic molecules were identified by sequencing and counted, and the percentage of mutant alleles in the original maternal plasma sample was used to determine fetal genotypes., Results: Four families with WD pedigrees consented to the study. Using Sanger and whole-exome sequencing, we mapped the pathogenic ATP7B mutations in each pedigree and confirmed the proband's original diagnosis of WD. After validation of cSMART with defined plasma models mimicking fetal inheritance of paternal, maternal, or both parental mutant alleles, we retrospectively showed in second pregnancies that the fetal genotypes assigned by invasive testing and NIPT were concordant., Conclusions: We developed a reliable and accurate NIPT assay that correctly diagnosed the fetal genotypes in 4 pregnancies at risk for WD. This novel technology has potential as a universal strategy for NIPT of other monogenic disorders, since it requires only knowledge of the parental pathogenic mutations., (© 2014 American Association for Clinical Chemistry.)

Published

2015

11. Potential of syncytiotrophoblasts isolated from the cervical mucus for early non-invasive prenatal diagnosis: evidence of a vanishing twin.

Author

Mantzaris D and Cram DS

Subjects

Adult, Female, Fetus pathology, Gestational Age, Humans, Male, Pregnancy, Pregnancy Trimester, First, Trophoblasts pathology, Twins, Dizygotic, Aborted Fetus, Cervix Mucus cytology, Fetus chemistry, Prenatal Diagnosis methods, Sex Determination Analysis methods, Trophoblasts metabolism

Abstract

Background: Non-invasive methods to assess the foetal genome during pregnancy will provide new opportunities to offer pregnant women a more comprehensive genetic diagnosis of their established foetus. The aim of this study was to determine the presence and frequency of foetal cells in transcervical cell (TCC) mucus samples from pregnant women and determine their suitability for early prenatal diagnosis., Methods: Syncytiotrophoblasts in aspirated TCC mucus samples were identified by immunostaining with the foetal-specific antibody NDOG1. Genetic analysis of foetal cells was performed by laser capture microdissection and quantitative fluorescent PCR (QF-PCR)., Results: In 116 of 207 (56%) TCC samples, abundant syncytiotrophoblasts were retrieved. However, when TCC samples were stratified for the presence of chorionic villous fragments, syncytiotrophoblasts were identified in 85 of 109 (78%) samples. Significant numbers of syncytiotrophoblasts were found in TCC samples collected between 6 and 9weeks of gestation (mean 741, range 25-2884). QF-PCR analysis of NDOG1 positive syncytiotrophoblasts and matching maternal DNA confirmed their foetal origin and correct foetal cell sexing was achieved in 97% of TCC samples. The one discordant sex diagnosis was associated with a dizygotic dichorionic twin pregnancy resulting from the implantation of a female T21 embryo and a normal male embryo, where the female T21 foetus had succumbed at 6weeks of gestation and was vanishing., Conclusions: Syncytiotrophoblasts can be successfully isolated from TCC samples and represent a suitable source of cells for genetic analysis of the established foetus in early pregnancy. The study highlights a vanishing twin as a potential cause for discordant non-invasive prenatal test results., (Copyright © 2014 Elsevier B.V. All rights reserved.)

Published

2015

12. A PGD pregnancy achieved by embryo copy number variation sequencing with confirmation by non-invasive prenatal diagnosis.

Author

Wang H, Wang L, Ma M, Song Z, Zhang J, Xu G, Fan J, Li N, Cram DS, and Yao Y

Subjects

Adult, Female, Humans, Male, Pregnancy, DNA Copy Number Variations genetics, Embryo, Mammalian, Molecular Diagnostic Techniques methods, Prenatal Diagnosis methods, Sequence Analysis, DNA

Published

2014

13. DNA identification of fetal cells isolated from cervical mucus: potential for early non-invasive prenatal diagnosis.

Author

Katz-Jaffe MG, Mantzaris D, and Cram DS

Subjects

Chromosome Disorders diagnosis, Cytogenetic Analysis methods, DNA analysis, DNA Fingerprinting methods, Female, Fluorescent Antibody Technique, Genetic Testing methods, Humans, Pregnancy, Pregnancy Trimester, First, Cervix Mucus cytology, Fetus cytology, Prenatal Diagnosis methods, Trophoblasts cytology

Abstract

Objectives: To develop a reliable method to isolate fetal cells for genetic diagnosis., Design: Aspiration of cervical mucus from pregnant women in the first trimester., Setting: Pregnant women were recruited before an elective termination of pregnancy., Population: Sixty pregnant women (7-10 weeks of gestation)., Methods: Fetal cells were isolated from aspirated cervical mucus of pregnant women using a combination of enzymatic digestion, fluorescent immunohistochemistry, micromanipulation and single-cell DNA allelic profiling., Main Outcome Measures: The isolation and identification of fetal cells., Results: The transformation of the tenacious cervical mucus into a single-cell suspension enabled the isolation and identification of fetal cells by fluorescent immunohistochemistry. Confirmation of fetal origin was accomplished by single-cell DNA allelic profiling alongside known maternal cells., Conclusions: This novel non-invasive method is rapid and efficient with results attainable within 24 hours as early as seven weeks of gestation. The technique would offer earlier reassurance and the option of first trimester therapeutic abortions to both high and low risk pregnant women.

Published

2005

14. Non-invasive prenatal testing of pregnancies at risk for phenylketonuria.

Author

Huikun Duan, Ning Liu, Zhenhua Zhao, Yiqian Liu, Yin Wang, Zhifeng Li, Mengnan Xu, Cram, David S., and Xiangdong Kong

Subjects

PRENATAL diagnosis, PREGNANCY tests, CHORIONIC villus sampling, INVASIVE diagnosis

Published

2019

15. The uncertainty of copy number variants: pregnancy decisions and clinical follow-up.

Author

Shi, Panlai, Liang, Hongbin, Hou, Yaqin, Chen, Duo, Ren, Huanan, Wang, Conghui, Xia, Yanjie, Zhang, Da, Leigh, Don, Cram, David S., and Kong, Xiangdong

Subjects

DNA copy number variations, MEDICAL genomics, MEDICAL genetics, FETAL ultrasonic imaging, PREGNANCY

Abstract

Next-generation sequencing for copy number variants is often used as a follow-up investigation of unusual fetal ultrasound results and is capable of detecting copy number variations with a resolution of ∼0.1 Mb. In a prenatal setting, observation and subsequent management of pregnancies with a fetal variant of uncertain significance remains problematic for counseling. This study aimed to follow the decision-making processes in pregnancies with a fetal variant of uncertain significance and prospectively assess copy number variation interpretations and implications under the newer 2020 American College of Medical Genetics and Genomics guidelines. In a single prenatal unit, prospective chromosome testing using copy number variation sequencing for 8030 fetuses with unexpected noninvasive findings identified 139 pregnancies with a copy number variation classified as a variant of uncertain significance according to the 2015 American College of Medical Genetics and Genomics guidelines current at the time. Parent-of-origin testing was subsequently performed to determine if the copy number variation was inherited or de novo. All couples were offered specialized genetic counseling to assist in pregnancy management decisions. For the continued pregnancies that reached term, newborns were clinically assessed for evidence of any disease at 0 to 10 months and/or at 2 to 4 years of age. Of the 139 variants of uncertain significance found, most (78%) were inherited with no evidence of disease in the carrier parent. On the basis of primary ultrasound findings combined with results from noninvasive prenatal screening tests, most inherited variant of uncertain significance pregnancies were continued, whereas most pregnancies involving de novo variants of uncertain significance were terminated. From clinical follow-up of the 113 live births, only 5 showed any evidence of a phenotype that was not apparently related to the original variant of uncertain significance. Prospective reanalysis of the 139 variants of uncertain significance using recent 2020 American College of Medical Genetics and Genomics guidelines changed the status of 24 variants of uncertain significance, with 15 reclassified as benign and 9 as pathogenic. However, the 5 children born with an inherited variant of uncertain significance reclassified as pathogenic showed no evidence of a disease phenotype on clinical follow-up. The severity of fetal ultrasound findings combined with results from parent-of-origin testing were the key drivers in pregnancy management decisions for patients. According to birth outcomes from continued pregnancies, most variants of uncertain significance proved to be apparently benign in nature and potentially of low risk of adverse disease outcome. There was a discordance rate of 17% for variant of uncertain significance scoring between the 2015 and 2020 American College of Medical Genetics and Genomics guidelines for defining a variant of uncertain significance, suggesting that difficulties remain for predicting true pathogenicity. Nonetheless, with increasing knowledge of population copy number variation polymorphisms, and a more complete assessment for alternative genetic causes, patients having prenatal assessments should feel less anxious when a fetal variant of uncertain significance is identified. [ABSTRACT FROM AUTHOR]

Published

2023

16. Copy number variation sequencing-based prenatal diagnosis using cell-free fetal DNA in amniotic fluid.

Author

Qi, Qingwei, Lu, Sijia, Zhou, Xiya, Yao, Fengxia, Hao, Na, Yin, Guangjun, Li, Wenhui, Bai, Junjie, Li, Ning, and Cram, David S.

Subjects

DIAGNOSIS of Down syndrome, TURNER'S syndrome, AMNIOCENTESIS, AMNION, AMNIOTIC liquid, ANEUPLOIDY, CHROMOSOME abnormalities, DNA, GENETIC polymorphisms, GENETICS, HIGH-risk pregnancy, KARYOTYPES, PRENATAL diagnosis, SEQUENCE analysis, DIAGNOSIS

Abstract

Objective: The study aimed to determine whether cell-free fetal DNA (cffDNA) present in amniotic fluid supernatant can be used as a surrogate for amniocyte-based diagnosis of fetal chromosomal abnormalities.Method: Amniocentesis was performed on 28 high-risk pregnancies. Amniocytes and the cffDNA fraction were prepared from the amniotic fluid samples. Chromosomal analysis of amniocytes was performed by either karyotyping or single nucleotide polymorphism (SNP) arrays. The corresponding cffDNA samples were blindly analyzed by copy number variation (CNV) sequencing in an independent laboratory.Results: In the 28 matching amniocyte and cffDNA samples, there was a high diagnostic concordance for detection of euploidy, aneuploidy and CNVs. From ten samples referred for karyotyping, two aneuploidies (20%) were identified. From 18 samples referred for SNP array analysis, three pathogenic CNVs (16.7%) were identified. CNV sequencing of the 28 cffDNA samples also detected the two aneuploidies and the three pathogenic CNVs, giving an overall concordance rate of 100% for detection of pathogenic chromosome abnormalities. Compared with SNP array analysis, CNV sequencing returned a higher yield of benign or variants of unknown significance.Conclusion: Copy number variation sequencing of cffDNA represents an alternative approach to conventional prenatal diagnostic methods for reliable and accurate detection of clinically significant chromosomal abnormalities. © 2016 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2016

17. Birth of a child with trisomy 9 mosaicism syndrome associated with paternal isodisomy 9: case of a positive noninvasive prenatal test result unconfirmed by invasive prenatal diagnosis.

Author

Jingmei Ma, Cram, David S., Jianguang Zhang, Ling Shang, Huixia Yang, and Hong Pan

Subjects

*CHILDBIRTH, *TRISOMY, *PRENATAL diagnosis, *MEDICAL screening, *ANEUPLOIDY, *DIAGNOSIS

Abstract

Background: Non-invasive prenatal testing (NIPT) is currently used as a frontline screening test to identify fetuses with common aneuploidies. Occasionally, incidental NIPT results are conveyed to the clinician suggestive of fetuses with rare chromosome disease syndromes. We describe a child with trisomy 9 (T9) mosaicism where the prenatal history reported a positive NIPT result for T9 that was unconfirmed by conventional prenatal diagnosis. Methods: NIPT was performed by low coverage whole genome plasma DNA sequencing. Karyotyping and fluorescent in situ hybridization (FISH) analysis with chromosome 9p-ter and 9q-ter probes was used to determine the somatic cell level of T9 mosaicism in the fetus and child. Quantitative fluorescent PCR (Q-PCR) of highly polymorphic short tandem repeat (STR) chromosome 9 markers was also performed to investigate the nature of the T9 mosaicism and the parental origin. Results: A 22 month old girl presented with severe developmental delay, congenital cerebral dysplasia and congenital heart disease consistent with phenotypes associated with T9 mosaicism syndrome. Review of the prenatal testing history revealed a positive NIPT result for chromosome T9. However, follow up confirmatory karyotyping and FISH analysis of fetal cells returned a normal karyotype. Post-natal studies of somatic cell T9 mosaicism by FISH detected levels of approximately 20 % in blood and buccal cells. Q-PCR STR analysis of family DNA samples suggested that the T9 mosaicism originated by post-zygotic trisomic rescue of a paternal meiotic II chromosome 9 non-disjunction error resulting in the formation of two distinct somatic cell lines in the proband, one with paternal isodisomy 9 and one with T9. Conclusion: This study shows that NIPT may also be a useful screening technology to increase prenatal detection rates of rare fetal chromosome disease syndromes. [ABSTRACT FROM AUTHOR]

Published

2015

18. A pregnancy with discordant fetal and placental chromosome 18 aneuploidies revealed by invasive and noninvasive prenatal diagnosis.

Author

Chong Chen, Cram, David S., Fanni Xie, Ping Wang, Xueqin Xu, Huanzheng Li, Zhuo Song, Di Chen, Jianguang Zhang, and Shaohua Tang

Subjects

*HUMAN chromosome abnormality diagnosis, *GENETIC disorder diagnosis, *NONINVASIVE diagnostic tests, *PRENATAL diagnosis, *PREIMPLANTATION genetic diagnosis

Abstract

This study investigated a pregnancy where the fetus was diagnosed with monosomy 18p by invasive amniocentesis and karyotyping. Additional noninvasive prenatal diagnosis, which detects fetal chromosome abnormalities in the circulating cell-free plasma DNA originating from the placenta revealed a related 18p monosomy/18q trisomy, suggesting confined placental mosaicism. Based on recent observations of chromosomal instability in the early preimplantation embryo, this study speculates on the possible embryonic origin(s) of these related but discordant chromosome 18 aneuploidies in the placental and fetal tissues. The findings highlight the potential fo r both false-positive and -negative noninvasive prenatal diagnosis results in pregnancies where there is either confined placental mosaicism or placental mosaicism. [ABSTRACT FROM AUTHOR]

Published

2014

19. Non-invasive prenatal testing of pregnancies at risk for phenylketonuria.

Author

Horton, Rachel Helen, Wellesley, Diana Gay, Duan, Huikun, Liu, Ning, Zhao, Zhenhua, Liu, Yiqian, Wang, Yin, Li, Zhifeng, Xu, Mengnan, Cram, David S, and Kong, Xiangdong

Subjects

PRENATAL diagnosis, PRENATAL genetic testing, CHORIONIC villus sampling, SPINAL muscular atrophy, PHENYLKETONURIA diagnosis, BLOOD testing, OXIDOREDUCTASES, PHENYLKETONURIA

Abstract

Background: Phenylketonuria (PKU) is a common metabolic disorder caused predominately by mutations in the phenylalanine hydroxylase (PAH) gene. The aim of the study was to design and validate the performance of a non-invasive prenatal test (NIPT) for PKU using circulating single molecule amplification and resequencing technology (cSMART).Methods: A total of 18 couples at genetic risk for having a child with PKU were recruited to the study. Gold standard invasive prenatal diagnosis (IPD) was performed on amniocyte or villus cell DNA by Sanger sequencing, targeting the known parental PAH mutations. Retrospectively, NIPT was also performed on stored maternal plasma samples from the 18 pregnancies by a multiplex cSMART assay designed to target all known DNA variants in the PAH gene.Results: Benchmarking against IPD results, NIPT correctly genotyped all fetuses, including six compound heterozygotes with PKU, four normal non-carriers of PKU and eight heterozygote carriers of PKU comprising five cases of a maternally inherited mutation and three cases of a paternally inherited mutation.Conclusions: The NIPT cSMART PKU assay was highly sensitive and specific for mutation detection and correct assignment of fetal genotypes. Based on comprehensive mutation coverage across the PAH gene, the assay may initially have clinical utility as a pregnancy screening test for high-risk carrier couples. [ABSTRACT FROM AUTHOR]

Published

2019

20. Prospective chromosome analysis of 3429 amniocentesis samples in China using copy number variation sequencing.

Author

Wang, Jing, Chen, Lin, Zhou, Cong, Wang, Li, Xie, Hanbing, Xiao, Yuanyuan, Zhu, Hongmei, Hu, Ting, Zhang, Zhu, Zhu, Qian, Liu, Zhiying, Liu, Shanlin, Wang, He, Xu, Mengnan, Ren, Zhilin, Yu, Fuli, Cram, David S., Liu, Hongqian, and Xie, Hanbin

Subjects

DIAGNOSIS of fetal diseases, AMNIOCENTESIS, DNA copy number variations, PREGNANCY complications, MATERNAL health, DIAGNOSIS of Down syndrome, RESEARCH, GENETICS, ANEUPLOIDY, SEQUENCE analysis, PRENATAL diagnosis, RESEARCH methodology, KARYOTYPES, MICROARRAY technology, EVALUATION research, MEDICAL cooperation, SEX chromosome abnormalities, COMPARATIVE studies, CHROMOSOME abnormalities, FLUORESCENCE in situ hybridization, LONGITUDINAL method

Abstract

Background: Next-generation sequencing is emerging as a viable alternative to chromosome microarray analysis for the diagnosis of chromosome disease syndromes. One next-generation sequencing methodology, copy number variation sequencing, has been shown to deliver high reliability, accuracy, and reproducibility for detection of fetal copy number variations in prenatal samples. However, its clinical utility as a first-tier diagnostic method has yet to be demonstrated in a large cohort of pregnant women referred for fetal chromosome testing.Objective: We sought to evaluate copy number variation sequencing as a first-tier diagnostic method for detection of fetal chromosome anomalies in a general population of pregnant women with high-risk prenatal indications.Study Design: This was a prospective analysis of 3429 pregnant women referred for amniocentesis and fetal chromosome testing for different risk indications, including advanced maternal age, high-risk maternal serum screening, and positivity for an ultrasound soft marker. Amniocentesis was performed by standard procedures. Amniocyte DNA was analyzed by copy number variation sequencing with a chromosome resolution of 0.1 Mb. Fetal chromosome anomalies including whole chromosome aneuploidy and segmental imbalances were independently confirmed by gold standard cytogenetic and molecular methods and their pathogenicity determined following guidelines of the American College of Medical Genetics for sequence variants.Results: Clear interpretable copy number variation sequencing results were obtained for all 3429 amniocentesis samples. Copy number variation sequencing identified 3293 samples (96%) with a normal molecular karyotype and 136 samples (4%) with an altered molecular karyotype. A total of 146 fetal chromosome anomalies were detected, comprising 46 whole chromosome aneuploidies (pathogenic), 29 submicroscopic microdeletions/microduplications with known or suspected associations with chromosome disease syndromes (pathogenic), 22 other microdeletions/microduplications (likely pathogenic), and 49 variants of uncertain significance. Overall, the cumulative frequency of pathogenic/likely pathogenic and variants of uncertain significance chromosome anomalies in the patient cohort was 2.83% and 1.43%, respectively. In the 3 high-risk advanced maternal age, high-risk maternal serum screening, and ultrasound soft marker groups, the most common whole chromosome aneuploidy detected was trisomy 21, followed by sex chromosome aneuploidies, trisomy 18, and trisomy 13. Across all clinical indications, there was a similar incidence of submicroscopic copy number variations, with approximately equal proportions of pathogenic/likely pathogenic and variants of uncertain significance copy number variations. If karyotyping had been used as an alternate cytogenetics detection method, copy number variation sequencing would have returned a 1% higher yield of pathogenic or likely pathogenic copy number variations.Conclusion: In a large prospective clinical study, copy number variation sequencing delivered high reliability and accuracy for identifying clinically significant fetal anomalies in prenatal samples. Based on key performance criteria, copy number variation sequencing appears to be a well-suited methodology for first-tier diagnosis of pregnant women in the general population at risk of having a suspected fetal chromosome abnormality. [ABSTRACT FROM AUTHOR]

Published

2018

21. Transcervical cell sampling: a need for clear terminology.

Author

Katz-Jaffe, Mandy G., Mantzaris, Debbie, and Cram, David S.

Subjects

LETTERS to the editor, PRENATAL diagnosis

Abstract

Presents a response by Mandy G. Katz-Jaffe, Debbie Mantzaris and David S. Cram to a letter to the editor about their article "DNA Identification of Fetal Cells Isolated From Cervical Mucus: Potential for Early Non-Invasive Prenatal Diagnosis," published in a 2005 issue.

Published

2005

22. Chromosome 21 mosaic human preimplantation embryos predominantly arise from diploid conceptions

Author

Katz-Jaffe, Mandy G., Trounson, Alan O., and Cram, David S.

Subjects

*CHROMOSOME abnormalities, *CELL proliferation, *MOSAICISM, *PRENATAL diagnosis

Abstract

Objective: High rates of chromosomal mosaicism in human IVF embryos question the accuracy of preimplantation genetic diagnosis, and, with the majority of embryo transfers still resulting in no pregnancy, chromosomal mosaicism is likely to be a contributing factor to human IVF failure. The aim of this study was to investigate the origin and nature of chromosome 21 (Ch21) cell division errors in human IVF embryos. Design: Perform single cell Ch21 allelic profiling on human IVF embryos. Setting: Academic research environment. Patient(s): Women of advanced maternal age (>35 yrs) (n = 65) undergoing infertility treatment; and amniocytes/chorionic cells from trisomy 21 pregnancies (n = 28). Intervention(s): Cells were analyzed by single cell allelic profiling, Main Outcome Measure(s): The origin and nature of cell division errors. Result(s): The vast majority of Ch21 mosaic embryos (∼80%) originated from diploid conceptions. In contrast, all fetal trisomy 21 originated from aneuploid conceptions. Increasing maternal age was significantly associated with aneuploid conceptions, meiotic cell division error, and adverse pregnancy outcome (P&#60;.05). The mean daily FSH dose that produced embryos with normal Ch21 cell division was significantly lower than the mean daily FSH dose that produced embryos with mitotic Ch21 cell division errors (P&#60;.01) and embryos with meiotic cell division errors (P&#60;.05). Conclusion(s): Chromosomal mosaicism of Ch21 in human IVF embryos predominantly originate from diploid conceptions. Further understanding of chromosomal mosaicism with respect to IVF parameters, such as daily FSH dose, may eventually lead to improvements in IVF outcomes. [Copyright &y& Elsevier]

Published

2005

23. Preferential selection and transfer of euploid noncarrier embryos in preimplantation genetic diagnosis cycles for reciprocal translocations.

Author

Wang, Li, Shen, Jiandong, Cram, David S., Ma, Minyue, Wang, Hui, Zhang, Wenke, Fan, Junmei, Gao, Zhiying, Zhang, Liwen, Li, Zhifeng, Xu, Mengnan, Leigh, Don A., Trounson, Alan O., Liu, Jiayin, and Yao, Yuanqing

Subjects

*PREIMPLANTATION genetic diagnosis, *EMBRYO transfer, *FERTILIZATION in vitro, *CLINICAL trials, *POLYMERASE chain reaction, *CHROMOSOME abnormalities, *COMPARATIVE studies, *GENES, *GENETIC techniques, *KARYOTYPES, *RESEARCH methodology, *MEDICAL cooperation, *PRENATAL diagnosis, *RESEARCH, *EVALUATION research, *RETROSPECTIVE studies

Abstract

Objective: To develop and validate a new strategy to distinguish between balanced/euploid carrier and noncarrier embryos in preimplantation genetic diagnosis (PGD) cycles for reciprocal translocations and to successfully achieve a live birth after selective transfer of a noncarrier embryo.Design: Retrospective and prospective study.Setting: In vitro fertilization (IVF) units.Patient(s): Eleven patients undergoing mate pair sequencing for identification of translocation breakpoints, followed by clinical PGD cycles.Intervention(s): Embryo biopsy with 24-chromosome testing to determine carrier status of balanced/euploid embryos.Main Outcome Measure(s): Definition of translocation breakpoints and polymerase chain reaction (PCR) diagnostic primers, correct diagnosis of euploid embryos for carrier status, and a live birth with a normal karyotype after transfer of a noncarrier embryo.Result(s): In 9 of 11 patients (82%), translocation breakpoints were successfully identified. In four patients with a term PGD pregnancy established with a balanced/euploid embryo of unknown carrier status, the correct carrier status was retrospectively determined, matching with the cytogenetic karyotype of the resulting newborns. In a prospective PGD cycle undertaken by a patient with a 46,XY,t(7;14)(q22;q24.3) translocation, the four balanced/euploid embryos identified comprised three carriers and one noncarrier. Transfer of the noncarrier embryo resulted in birth of a healthy girl who was subsequently confirmed with a normal 46,XX karyotype.Conclusion(s): The combination of mate pair sequencing and PCR breakpoint analysis of balanced reciprocal translocation derivatives is a novel, reliable, and accurate strategy for distinguishing between carrier and noncarrier balanced/euploid embryos. The method has potential application in clinical PGD cycles for patients with reciprocal translocations or other structural rearrangements. [ABSTRACT FROM AUTHOR]

Published

2017

24. Quantitation of fetal DNA fraction in maternal plasma using circulating single molecule amplification and re-sequencing technology (cSMART).

Author

Song, Yijun, Zhou, Xiya, Huang, Saiqiong, Li, Xiaohong, Qi, Qingwei, Jiang, Yulin, Liu, Yiqian, Ma, Chengcheng, Li, Zhifeng, Xu, Mengnan, Cram, David S, and Liu, Juntao

Subjects

*BLOOD circulation, *GENE amplification, *DNA damage, *PRENATAL diagnosis, *GENETIC disorders, *NONINVASIVE diagnostic tests, *SINGLE nucleotide polymorphisms

Abstract

Background Calculation of the fetal DNA fraction (FF) is important for reliable and accurate noninvasive prenatal testing (NIPT) for fetal genetic abnormalities. The aim of the study was to develop and validate a novel method for FF determination. Methods FF was calculated using the chromosome Y (ChrY) sequence read assay and by circulating single molecule amplification and re-sequencing technology of 76 autosomal SNPs. Results By Pearson correlation for FF (4.73–22.11%) in 33 male pregnancy samples, the R 2 co-efficient for the 76-SNP versus the ChrY assay was 0.9572 (p < 0.001). In addition, the co-efficient of variation (CV) of FF measurement by the 76-SNP assay was low (0.15–0.35). As a control, the FF measurement for four non-pregnant plasma samples was virtually zero. In prospective longitudinal studies of 14 women with normal pregnancies, FF generally increased with gestational age. However, in eight women (71%) there was a significant decrease in FF between the first trimester (11–13 weeks) and the second trimester (15–19 weeks), and this was attributable to significant maternal weight gain. Conclusions The novel 76-SNP cSMART assay has the precision to accurately measure FF in all pregnancies at a detection threshold of 5%. Based on FF trends in individual pregnancies, our results suggest that the end of the first trimester may be a more optimal window for performing NIPT. [ABSTRACT FROM AUTHOR]

Published

2016