Your search keyword '"Kwong Wai, Choy"' showing total 297 results

1. A Genome-Wide Association Study of Chinese and English Language Phenotypes in Hong Kong Chinese Children

Author

Yu-Ping Lin, Yujia Shi, Ruoyu Zhang, Xiao Xue, Shitao Rao, Liangying Yin, Kelvin Fai Hong Lui, Dora Jue Pan, Urs Maurer, Kwong-Wai Choy, Silvia Paracchini, Catherine McBride, and Hon-Cheong So

Abstract

Dyslexia and developmental language disorders are important learning difficulties. However, their genetic basis remains poorly understood, and most genetic studies were performed on Europeans. There is a lack of genome-wide association studies (GWAS) on literacy phenotypes of Chinese as a native language and English as a second language (ESL) in a Chinese population. In this study, we conducted GWAS on 34 reading/language-related phenotypes in Hong Kong Chinese bilingual children (including both twins and singletons; total N = 1046). We performed association tests at the single-variant, gene, and pathway levels. In addition, we tested genetic overlap of these phenotypes with other neuropsychiatric disorders, as well as cognitive performance (CP) and educational attainment (EA) using polygenic risk score (PRS) analysis. Totally 5 independent loci (LD-clumped at r[superscript 2] = 0.01; MAF > 0.05) reached genome-wide significance (p < 5e-08; filtered by imputation quality metric Rsq>0.3 and having at least 2 correlated SNPs (r[superscript 2] > 0.5) with p < 1e-3). The loci were associated with a range of language/literacy traits such as Chinese vocabulary, character and word reading, and rapid digit naming, as well as English lexical decision. Several SNPs from these loci mapped to genes that were reported to be associated with EA and other neuropsychiatric phenotypes, such as "MANEA" and "PLXNC1." In PRS analysis, EA and CP showed the most consistent and significant polygenic overlap with a variety of language traits, especially English literacy skills. To summarize, this study revealed the genetic basis of Chinese and English abilities in a group of Chinese bilingual children. Further studies are warranted to replicate the findings.

Published

2024

2. Detection of genomic variants by genome sequencing in foetuses with central nervous system abnormalities

Author

Yanfei Wang, Meimei Liu, Zhi Gao, Chunxiao Hua, Jinna Jiang, Yuting Zheng, Zirui Dong, Ye Cao, Kwong Wai Choy, Xiaofan Zhu, and Xiangdong Kong

Subjects

Prenatal diagnosis, genome sequencing, central nervous system, genomic variant, Medicine

Abstract

Objective Clinical validity of genome sequencing (GS) (>30×) has been preliminarily verified in the post-natal setting. This study is to investigate the potential utility of trio-GS as a prenatal test for diagnosis of central nervous system (CNS) anomalies.Methods We performed trio-based GS on a prospective cohort of 17 foetuses with CNS abnormalities. Single nucleotide variation (SNV), small insertion and deletion (Indel), copy number variation (CNV), structural variant (SV), and regions with absence of heterozygosity (AOH) were analyzed and classified according to ACMG guidelines.Results Trio-GS identified diagnostic findings in 29.4% (5/17) of foetuses, with pathogenic variants found in SON, L1CAM, KMT2D, and ASPM. Corpus callosum (CC) and cavum septum pellucidum (CSP) abnormalities were the most frequent CNS abnormalities (47.1%, 8/17) with a diagnostic yield of 50%. A total of 29.4% (5/17) foetuses had variants of uncertain significance (VUS). Particularly, maternal uniparental disomy 16 and a de novo mosaic 4p12p11 duplication were simultaneously detected in one foetus with abnormal sulcus development. In addition, parentally inherited chromosomal inversions were identified in two foetuses.Conclusion GS demonstrates its feasibility in providing genetic diagnosis for foetal CNS abnormalities and shows the potential to expand the application to foetuses with other ultrasound anomalies in prenatal diagnosis.

Published

2024

3. Neuropathological signatures revealed by transcriptomic and proteomic analysis in Pten-deficient mouse models

Author

Stanley K. K. Cheung, Jacinda Kwok, Penelope M. Y. Or, Chi Wai Wong, Bo Feng, Kwong Wai Choy, Raymond C. C. Chang, J. Peter H. Burbach, Alfred S. L. Cheng, and Andrew M. Chan

Subjects

Medicine, Science

Abstract

Abstract PTEN hamartoma tumour syndrome is characterised by mutations in the human PTEN gene. We performed transcriptomic and proteomic analyses of neural tissues and primary cultures from heterozygous and homozygous Pten-knockout mice. The somatosensory cortex of heterozygous Pten-knockout mice was enriched in immune response and oligodendrocyte development Gene Ontology (GO) terms. Parallel proteomic analysis revealed differentially expressed proteins (DEPs) related to dendritic spine development, keratinisation and hamartoma signatures. However, primary astrocytes (ASTs) from heterozygous Pten-knockout mice were enriched in the extracellular matrix GO term, while primary cortical neurons (PCNs) were enriched in immediate-early genes. In ASTs from homozygous Pten-knockout mice, cilium-related activity was enriched, while PCNs exhibited downregulation of forebrain neuron generation and differentiation, implying an altered excitatory/inhibitory balance. By integrating DEPs with pre-filtered differentially expressed genes, we identified the enrichment of traits of intelligence, cognitive function and schizophrenia, while DEPs in ASTs were significantly associated with intelligence and depression.

Published

2023

4. Investigation of the genetic etiology in male infertility with apparently balanced chromosomal structural rearrangements by genome sequencing

Author

Matthew Hoi Kin Chau, Ying Li, Peng Dai, Mengmeng Shi, Xiaofan Zhu, Jacqueline Pui Wah Chung, Yvonne K Kwok, Kwong Wai Choy, Xiangdong Kong, and Zirui Dong

Subjects

azoospermia, balanced structural rearrangements, genome sequencing, male infertility, severe oligospermia, Diseases of the genitourinary system. Urology, RC870-923

Abstract

Apparently balanced chromosomal structural rearrangements are known to cause male infertility and account for approximately 1% of azoospermia or severe oligospermia. However, the underlying mechanisms of pathogenesis and etiologies are still largely unknown. Herein, we investigated apparently balanced interchromosomal structural rearrangements in six cases with azoospermia/severe oligospermia to comprehensively identify and delineate cryptic structural rearrangements and the related copy number variants. In addition, high read-depth genome sequencing (GS) (30-fold) was performed to investigate point mutations causative of male infertility. Mate-pair GS (4-fold) revealed additional structural rearrangements and/or copy number changes in 5 of 6 cases and detected a total of 48 rearrangements. Overall, the breakpoints caused truncations of 30 RefSeq genes, five of which were associated with spermatogenesis. Furthermore, the breakpoints disrupted 43 topological-associated domains. Direct disruptions or potential dysregulations of genes, which play potential roles in male germ cell development, apoptosis, and spermatogenesis, were found in all cases (n = 6). In addition, high read-depth GS detected dual molecular findings in case MI6, involving a complex rearrangement and two point mutations in the gene DNAH1. Overall, our study provided the molecular characteristics of apparently balanced interchromosomal structural rearrangements in patients with male infertility. We demonstrated the complexity of chromosomal structural rearrangements, potential gene disruptions/dysregulation and single-gene mutations could be the contributing mechanisms underlie male infertility.

Published

2022

5. Contributions of common genetic variants to specific languages and to when a language is learned

Author

Patrick C. M. Wong, Xin Kang, Hon-Cheong So, and Kwong Wai Choy

Subjects

Medicine, Science

Abstract

Abstract Research over the past two decades has identified a group of common genetic variants explaining a portion of variance in native language ability. The present study investigates whether the same group of genetic variants are associated with different languages and languages learned at different times in life. We recruited 940 young adults who spoke from childhood Chinese and English as their first (native) (L1) and second (L2) language, respectively, who were learners of a new, third (L3) language. For the variants examined, we found a general decrease of contribution of genes to language functions from native to foreign (L2 and L3) languages, with variance in foreign languages explained largely by non-genetic factors such as musical training and motivation. Furthermore, genetic variants that were found to contribute to traits specific to Chinese and English respectively exerted the strongest effects on L1 and L2. These results seem to speak against the hypothesis of a language- and time-universal genetic core of linguistic functions. Instead, they provide preliminary evidence that genetic contribution to language may depend at least partly on the intricate language-specific features. Future research including a larger sample size, more languages and more genetic variants is required to further explore these hypotheses.

Published

2022

6. Genome sequencing reveals the role of rare genomic variants in Chinese patients with symptomatic intracranial atherosclerotic disease

Author

Xinyi Leng, Sze Ho Ma, Karen Ma, Thomas W Leung, Howan Leung, Ying Li, Yannie OY Soo, Vincent CT Mok, Kwong Wai Choy, Anne Y Y Chan, Alexander Y Lau, Ye Cao, Mengmeng Shi, Zihan Chen, Tiffany Chung, Bonaventure YM Ip, Vincent HL Ip, Florence SY Fan, Lisa WC Au, and Zirui Dong

Subjects

Neurology. Diseases of the nervous system, RC346-429

Published

2022

7. Investigation of Chromosomal Structural Abnormalities in Patients With Undiagnosed Neurodevelopmental Disorders

Author

Ye Cao, Ho Ming Luk, Yanyan Zhang, Matthew Hoi Kin Chau, Shuwen Xue, Shirley S. W. Cheng, Albert Martin Li, Josephine S. C. Chong, Tak Yeung Leung, Zirui Dong, Kwong Wai Choy, and Ivan Fai Man Lo

Subjects

structural variations, mate-pair genome sequencing, neurodevelopmental disorders, Absence of heterozygosity (AOH), CNV (copy number variant), insertion, Genetics, QH426-470

Abstract

Background: Structural variations (SVs) are various types of the genomic rearrangements encompassing at least 50 nucleotides. These include unbalanced gains or losses of DNA segments (copy number changes, CNVs), balanced rearrangements (such as inversion or translocations), and complex combinations of several distinct rearrangements. SVs are known to play a significant role in contributing to human genomic disorders by disrupting the protein-coding genes or the interaction(s) with cis-regulatory elements. Recently, different types of genome sequencing-based tests have been introduced in detecting various types of SVs other than CNVs and regions with absence of heterozygosity (AOH) with clinical significance.Method: In this study, we applied the mate-pair low pass (∼4X) genome sequencing with large DNA-insert (∼5 kb) in a cohort of 100 patients with neurodevelopmental disorders who did not receive informative results from a routine CNV investigation. Read-depth-based CNV analysis and chimeric-read-pairs analysis were used for CNV and SV analyses. The region of AOH was indicated by a simultaneous decrease in the rate of heterozygous SNVs and increase in the rate of homozygous SNVs.Results: First, we reexamined the 25 previously reported CNVs among 24 cases in this cohort. The boundaries of these twenty-five CNVs including 15 duplications and 10 deletions detected were consistent with the ones indicated by the chimeric-read-pairs analysis, while the location and orientation were determined in 80% of duplications (12/15). Particularly, one duplication was involved in complex rearrangements. In addition, among all the 100 cases, 10% of them were detected with rare or complex SVs (>10 Kb), and 3% were with multiple AOH (≥5 Mb) locating in imprinting chromosomes identified. In particular, one patient with an overall value of 214.5 Mb of AOH identified on 13 autosomal chromosomes suspected parental consanguinity.Conclusion: In this study, mate-pair low-pass GS resolved a significant proportion of CNVs with inconclusive significance, and detected additional SVs and regions of AOH in patients with undiagnostic neurodevelopmental disorders. This approach complements the first-tier CNV analysis for NDDs, not only by increasing the resolution of CNV detection but also by enhancing the characterization of SVs and the discovery of potential causative regions (or genes) contributory to could be complex in composition NDDs.

Published

2022

8. MicroRNA-19a-PTEN Axis Is Involved in the Developmental Decline of Axon Regenerative Capacity in Retinal Ganglion Cells

Author

Heather K. Mak, Jasmine S.Y. Yung, Robert N. Weinreb, Shuk Han Ng, Xu Cao, Tracy Y.C. Ho, Tsz Kin Ng, Wai Kit Chu, Wing Ho Yung, Kwong Wai Choy, Chi Chiu Wang, Tin Lap Lee, and Christopher Kai-shun Leung

Subjects

retinal ganglion cells, microRNA-19, phosphatase and tensin homolog, PTEN, axon regenerative capacity, axon regeneration, Therapeutics. Pharmacology, RM1-950

Abstract

Irreversible blindness from glaucoma and optic neuropathies is attributed to retinal ganglion cells (RGCs) losing the ability to regenerate axons. While several transcription factors and proteins have demonstrated enhancement of axon regeneration after optic nerve injury, mechanisms contributing to the age-related decline in axon regenerative capacity remain elusive. In this study, we show that microRNAs are differentially expressed during RGC development and identify microRNA-19a (miR-19a) as a heterochronic marker; developmental decline of miR-19a relieves suppression of phosphatase and tensin homolog (PTEN), a key regulator of axon regeneration, and serves as a temporal indicator of decreasing axon regenerative capacity. Intravitreal injection of miR-19a promotes axon regeneration after optic nerve crush in adult mice, and it increases axon extension in RGCs isolated from aged human donors. This study uncovers a previously unrecognized involvement of the miR-19a-PTEN axis in RGC axon regeneration, and it demonstrates therapeutic potential of microRNA-mediated restoration of axon regenerative capacity in optic neuropathies.

Published

2020

9. Prevalence and heritability of handedness in a Hong Kong Chinese twin and singleton sample

Author

Mo Zheng, Catherine McBride, Connie Suk-Han Ho, Jonathan Ka-Chun Chan, Kwong Wai Choy, and Silvia Paracchini

Subjects

Handedness, Edinburgh handedness inventory, Pegboard, Chinese children, Twins, Psychology, BF1-990

Abstract

Abstract Background Left-handedness prevalence has been consistently reported at around 10% with heritability estimates at around 25%. Higher left-handedness prevalence has been reported in males and in twins. Lower prevalence has been reported in Asia, but it remains unclear whether this is due to biological or cultural factors. Most studies are based on samples with European ethnicities and using the preferred hand for writing as key assessment. Here, we investigated handedness in a sample of Chinese school children in Hong Kong, including 426 singletons and 205 pairs of twins, using both the Edinburgh Handedness Inventory and Pegboard Task. Results Based on a binary definition of writing hand, we found a higher prevalence of left-handedness (8%) than what was previously reported in Asian datasets. We found no evidence of increased left-handedness in twins, but our results were in line with previous findings showing that males have a higher tendency to be left-handed than females. Heritability was similar for both hand preference (21%) and laterality indexes (22%). However, these two handedness measures present only a moderate correlation (.42) and appear to be underpinned by different genetic factors. Conclusion In summary, we report new reference data for an ethnic group usually underrepresented in the literature. Our heritability analysis supports the idea that different measures will capture different components of handedness and, as a consequence, datasets assessed with heterogeneous criteria are not easily combined or compared.

Published

2020

10. Trio-Based Low-Pass Genome Sequencing Reveals Characteristics and Significance of Rare Copy Number Variants in Prenatal Diagnosis

Author

Matthew Hoi Kin Chau, Jicheng Qian, Zihan Chen, Ying Li, Yu Zheng, Wing Ting Tse, Yvonne K. Kwok, Tak Yeung Leung, Zirui Dong, and Kwong Wai Choy

Subjects

low-pass genome sequencing, de novo, inherited, copy number variants, prenatal diagnosis, Genetics, QH426-470

Abstract

Background: Low-pass genome sequencing (GS) detects clinically significant copy number variants (CNVs) in prenatal diagnosis. However, detection at improved resolutions leads to an increase in the number of CNVs identified, increasing the difficulty of clinical interpretation and management.Methods: Trio-based low-pass GS was performed in 315 pregnancies undergoing invasive testing. Rare CNVs detected in the fetuses were investigated. The characteristics of rare CNVs were described and compared to curated CNVs in other studies.Results: A total of 603 rare CNVs, namely, 597 constitutional and 6 mosaic CNVs, were detected in 272 fetuses (272/315, 86.3%), providing 1.9 rare CNVs per fetus (603/315). Most CNVs were smaller than 1 Mb (562/603, 93.2%), while 1% (6/603) were mosaic. Forty-six de novo (7.6%, 46/603) CNVs were detected in 11.4% (36/315) of the cases. Eighty-four CNVs (74 fetuses, 23.5%) involved disease-causing genes of which the mode of inheritance was crucial for interpretation and assessment of recurrence risk. Overall, 31 pathogenic/likely pathogenic CNVs were detected, among which 25.8% (8/31) were small (

Published

2021

11. Genome-Wide Cell-Free DNA Test for Fetal Chromosomal Abnormalities and Variants: Unrestricted Versus Restricted Reporting

Author

Angel H. W. Kwan, Xiaofan Zhu, Maria Mar Gil, Yvonne K. Y. Kwok, Isabella Y. M. Wah, Annie S. Y. Hui, Yuen-Ha Ting, Kwok-Ming Law, Doris Lau, Shuwen Xue, Kwong-Wai Choy, Daljit Sahota, Tak-Yeung Leung, and Liona C. Poon

Subjects

genome-wide, cell-free DNA, screening for trisomies, down syndrome, additional findings, screening performance, Medicine (General), R5-920

Abstract

This study aimed to compare the screening performance of genome-wide cfDNA testing for chromosomal abnormalities between two periods where additional findings were reported and not reported. Data were obtained from consecutive pregnant women with a singleton pregnancy at ≥10 weeks who requested cfDNA testing during 2015–2019. The performance of screening of the cfDNA test was determined by calculating the concordance rate, detection rate, and false-positive rate. Data from 3981 women were included. The no-result rates were similar between the two reporting periods (2.04% vs. 2.08%). Concordance rates for trisomy 21 and 18 were 100% and 100%, respectively. There were two cases tested high risk for trisomy 13, with a concordance rate of 0%. In total, 12 cases were high risk for any sex chromosome aneuploidy with an overall concordance of 75%, and 15 cases tested high risk for any rare autosomal trisomy, with a 13.3% concordance rate. The detection rates for trisomy 21 and 18 were 100% and 100%, respectively. For any SCA, the detection rate was 90%. For the two reporting periods, the combined false-positive rates were 0.93% and 0.17%, which were significantly different (p = 0.002). Restricting the reporting of additional findings from genome-wide cfDNA analysis has reduced the false-positive rate but without a reduction in the no-result rate.

Published

2022

12. Practical Considerations in Providing Preimplantation Genetic Testing for Aneuploidies (PGT-A)

Author

Queenie S.Y. Yeung, Ying Xin Zhang, Jacqueline P.W. Chung, Yvonne K.Y. Kwok, Baoheng Gui, Kwong Wai Choy, and Tin Chiu Li

Subjects

preimplantation genetic testing, pgd/pgs, ivf guidelines, good practice, laboratory, Reproduction, QH471-489

Abstract

Preimplantation genetic testing for aneuploidies (PGT-A) has been controversial in its application to improve reproductive success, reduce time-to-pregnancy, and serve the intention-to-treat. Nevertheless, many in vitro fertilization (IVF) units have already introduced the service for one reason or another. Given PGT-A is not a stand-alone technique but a clinical service involving several disciplines, this mini review discussed the factors that can influence success rates when PGT-A is applied and highlighted practical issues encountered by clinicians, embryology, and genetics laboratories involved in the provision of PGT-A service.

Published

2019

13. The Burden and Benefits of Knowledge: Ethical Considerations Surrounding Population-Based Newborn Genome Screening for Hearing

Author

Calli O. Mitchell, Greysha Rivera-Cruz, Matthew Hoi Kin Chau, Zirui Dong, Kwong Wai Choy, Jun Shen, Sami Amr, Anne B. S. Giersch, and Cynthia C. Morton

Subjects

genome sequencing, newborn hearing screening, newborn screening, newborn genome sequencing, incidental findings, secondary findings, Pediatrics, RJ1-570

Abstract

Recent advances in genomic sequencing technologies have expanded practitioners’ utilization of genetic information in a timely and efficient manner for an accurate diagnosis. With an ever-increasing resource of genomic data from progress in the interpretation of genome sequences, clinicians face decisions about how and when genomic information should be presented to families, and at what potential expense. Presently, there is limited knowledge or experience in establishing the value of implementing genome sequencing into newborn screening. Herein we provide insight into the complexities and the burden and benefits of knowledge resulting from genome sequencing of newborns.

Published

2022

14. Sequencing data of cell-free DNA fragments in living-related liver transplantation for inborn errors of metabolism

Author

Xiaofan Zhu, Hoi Ioi Ng, Liming Xuan, Yan Long, Yan Mao, Yu Shi, Liying Sun, Bo Liang, Fernando Scaglia, Zhijun Zhu, and Kwong Wai Choy

Subjects

Computer applications to medicine. Medical informatics, R858-859.7, Science (General), Q1-390

Abstract

Graft derived cell-free DNA was recently reported as a non-invasive biomarker to detect graft damage or rejection after liver transplantation. There are a number of methods for quantification of Gcf-DNA,3 including quantitative-PCR, digital droplet PCR and massively parallel sequencing (next generation sequencing). Here we present the NGS4 data and fragment size distribution of cell-free DNA in the plasma of patients with inborn errors of metabolism who underwent living-related liver transplantation. For more insights please see Analysis of fragment size distribution of cell-free DNA: a potential noninvasive marker to monitor graft damage in living-related liver transplantation for inborn errors of metabolism. [1]. Keywords: Graft derived cell-free DNA, Fragment size, Living-related liver transplantation, Inborn errors of metabolism

Published

2020

15. Genetic screening in patients with ovarian dysfunction

Author

Yang Zeng, Lin Li, Qingchun Li, Jijun Hu, Nana Zhang, Ling Wu, Zheng Yan, Ronggui Qu, Jie Dong, Ruyi Liu, Kwong Wai Choy, Lei Wang, Qing Sang, Yichun Guan, and Biaobang Chen

Subjects

Genetics, Genetics (clinical)

Abstract

Ovarian dysfunction, including premature ovarian insufficiency and decreased ovarian reserve, affects the ovarian reserve and is one of the leading causes of female infertility. More and more cases of ovarian dysfunction are associated with genetic factors. Here, we identified eight potential variants in five genes (MSH4, HFM1, SYCE1, FSHR, and C14orf39) from six independent families by exome sequencing. The splice-site variants in SYCE1 and MSH4 affected canonical splicing isoforms, leading to missing protein domains or premature termination. Our findings expand the mutational spectrum of ovarian dysfunction and provide potential biomarkers for future genetic counseling and for more personalized treatments. Exome sequencing was shown to be a useful tool to better dissect the genetic basis for ovarian dysfunction and yielded a genetic diagnosis in about 5.0% (6/124) of cases in a cohort of 124 patients with ovarian dysfunction.

Published

2022

16. TEDD: a database of temporal gene expression patterns during multiple developmental periods in human and model organisms

Author

Ziheng Zhou, Cong Tan, Matthew Hoi Kin Chau, Xiaosen Jiang, Ziyuan Ke, Xiaoyan Chen, Ye Cao, Yvonne K Kwok, Matthew Bellgard, Tak Yeung Leung, Kwong Wai Choy, and Zirui Dong

Subjects

Genetics

Abstract

Characterization of the specific expression and chromatin profiles of genes enables understanding how they contribute to tissue/organ development and the mechanisms leading to diseases. Whilst the number of single-cell sequencing studies is increasing dramatically; however, data mining and reanalysis remains challenging. Herein, we systematically curated the up-to-date and most comprehensive datasets of sequencing data originating from 2760 bulk samples and over 5.1 million single-cells from multiple developmental periods from humans and multiple model organisms. With unified and systematic analysis, we profiled the gene expression and chromatin accessibility among 481 cell-types, 79 tissue-types and 92 timepoints, and pinpointed cells with the co-expression of target genes. We also enabled the detection of gene(s) with a temporal and cell-type specific expression profile that is similar to or distinct from that of a target gene. Additionally, we illustrated the potential upstream and downstream gene−gene regulation interactions, particularly under the same biological process(es) or KEGG pathway(s). Thus, TEDD (Temporal Expression during Development Database), a value-added database with a user-friendly interface, not only enables researchers to identify cell-type/tissue-type specific and temporal gene expression and chromatin profiles but also facilitates the association of genes with undefined biological functions in development and diseases. The database URL is https://TEDD.obg.cuhk.edu.hk/.

Published

2022

17. Low-Pass Genome Sequencing-Based Detection of Paternity: Validation in Clinical Cytogenetics

Author

Dong, Keying Li, Yilin Zhao, Matthew Hoi Kin Chau, Ye Cao, Tak Yeung Leung, Yvonne K. Kwok, Kwong Wai Choy, and Zirui

Subjects

paternity test, genome sequencing, prenatal testing, low-pass genome sequencing, single-nucleotide variants

Abstract

Submission of a non-biological parent together with a proband for genetic diagnosis would cause a misattributed parentage (MP), possibly leading to misinterpretation of the pathogenicity of genomic variants. Therefore, a rapid and cost-effective paternity/maternity test is warranted before genetic testing. Although low-pass genome sequencing (GS) has been widely used for the clinical diagnosis of germline structural variants, it is limited in paternity/maternity tests due to the inadequate read coverage for genotyping. Herein, we developed rapid paternity/maternity testing based on low-pass GS with trio-based and duo-based analytical modes provided. The optimal read-depth was determined as 1-fold per case regardless of sequencing read lengths, modes, and library construction methods by using 10 trios with confirmed genetic relationships. In addition, low-pass GS with different library construction methods and 1-fold read-depths were performed for 120 prenatal trios prospectively collected, and 1 trio was identified as non-maternity, providing a rate of MP of 0.83% (1/120). All results were further confirmed via quantitative florescent PCR. Overall, we developed a rapid, cost-effective, and sequencing platform-neutral paternity/maternity test based on low-pass GS and demonstrated the feasibility of its clinical use in confirming the parentage for genetic diagnosis.

Published

2023

18. A Fetus with Congenital Microcephaly, Microphthalmia and Cataract Was Detected with Biallelic Variants in the OCLN Gene: A Case Report

Author

Vivian Kwun Sin Ng, Tze Kin Lau, Anita Sik Yau Kan, Brian Hon Yin Chung, Ho Ming Luk, Wai Fu Ng, Mengmeng Shi, Kwong Wai Choy, Ye Cao, and Wing Cheong Leung

Subjects

OCLN gene, whole genome sequencing, microphthalmia, microcephaly, cataract, prenatal diagnosis, Medicine (General), R5-920

Abstract

Microcephaly and microphthalmia are both rare congenital abnormalities, while concurrently, these two are even rarer. The underlying etiology would be complex interplaying between heterogeneous genetic background and the environmental pathogens, particularly during critical periods of early tissue development. Here, we reported a prenatal case with microcephaly, microphthalmia, and bilateral cataracts detected by ultrasonography and confirmed by autopsy. Various routine infection-related tests and invasive genetic testing were negative. Whole genome sequencing of fetus and parents revealed OCLN gene defects may be associated with these multiple congenital abnormalities.

Published

2021

19. Validation of a high-throughput and robust technique: BACs-on-beads assay (KaryoLite BoBs) for pre-implantation aneuploidy screening

Author

Grace Wing Shan Kong, Yanlin Ma, Jian Ou, Yvonne Ka Yin Kwok, Wei Wang, Queenie Sum Yee Yeung, Cherry Kit Man Wong, Qi Li, Wen Xu, Weiying Lu, Hong Li, Tin Chiu Li, and Kwong Wai Choy

Subjects

BoB, Karyolite, aCGH, PGS, Aneuploidy, Gynecology and obstetrics, RG1-991

Abstract

Objective: This study aims to validate the BACs-on-Beads (BoB) technology as a robust and high throughput method for pre-implantation genetic screening (PGS) for aneuploidy. Material and methods: The performances with respect to the sensitivity, specificity, success rate and detection rate of this technique from new BoBs technology and traditional array chromosomal genomic hybridization (aCGH) were compared. And the use of BoBs as a screening tool for euploid embryos in PGS was evaluated. Result: In the first part of validation study, there were total 75 embryos completed PGS by both BoBs and aCGH. The success rate of PGS was 97.4%, and the results showed 100% concordance between BoBs and aCGH for aneuploidy. In the second part, a total 219 embryos were involved. The success rate of PGS by BoBs was 100%. BoBs identified 28% (62/219) euploidy which were further confirmed to be euploidy by aCGH. Conclusion: This new strategic approach using BoBs as a first tier PGS screening tool and aCGH as a confirmatory tool can increase the throughput of PGS with a reduced cost and time to meet the demand in high volume units.

Published

2017

20. Prenatal Diagnosis of Fetuses With Increased Nuchal Translucency by Genome Sequencing Analysis

Author

Kwong Wai Choy, Huilin Wang, Mengmeng Shi, Jingsi Chen, Zhenjun Yang, Rui Zhang, Huanchen Yan, Yanfang Wang, Shaoyun Chen, Matthew Hoi Kin Chau, Ye Cao, Olivia Y.M. Chan, Yvonne K. Kwok, Yuanfang Zhu, Min Chen, Tak Yeung Leung, and Zirui Dong

Subjects

increased nuchal translucency, genome sequencing, prenatal diagnosis, genomic variants, structural rearrangement, Genetics, QH426-470

Abstract

Background: Increased nuchal translucency (NT) is an important biomarker associated with increased risk of fetal structural anomalies. It is known to be contributed by a wide range of genetic etiologies from single-nucleotide variants to those affecting millions of base pairs. Currently, prenatal diagnosis is routinely performed by karyotyping and chromosomal microarray analysis (CMA); however, both of them have limited resolution. The diversity of the genetic etiologies warrants an integrated assay such as genome sequencing (GS) for comprehensive detection of genomic variants. Herein, we aim to evaluate the feasibility of applying GS in prenatal diagnosis for the fetuses with increased NT.Methods: We retrospectively applied GS (> 30-fold) for fetuses with increased NT (≥3.5 mm) who underwent routine prenatal diagnosis. Detection of single-nucleotide variants, copy number variants, and structural rearrangements was performed simultaneously, and the results were integrated for interpretation in accordance with the guidelines of the American College of Medical Genetics and Genomics. Pathogenic or likely pathogenic (P/LP) variants were selected for validation and parental confirmation, when available.Results: Overall, 50 fetuses were enrolled, including 34 cases with isolated increased NT and 16 cases with other fetal structural malformations. Routine CMA and karyotyping reported eight P/LP CNVs, yielding a diagnostic rate of 16.0% (8/50). In comparison, GS provided a twofold increase in diagnostic yield (32.0%, 16/50), including one mosaic turner syndrome, eight cases with microdeletions/microduplications, and seven cases with P/LP point mutations. Moreover, GS identified two cryptic insertions and two inversions. Follow-up study further demonstrated the potential pathogenicity of an apparently balanced insertion that disrupted an OMIM autosomal dominant disease-causing gene at the insertion site.Conclusions: Our study demonstrates that applying GS in fetuses with increased NT can comprehensively detect and delineate the various genomic variants that are causative to the diseases. Importantly, prenatal diagnosis by GS doubled the diagnostic yield compared with routine protocols. Given a comparable turnaround time and less DNA required, our study provides strong evidence to facilitate GS in prenatal diagnosis, particularly in fetuses with increased NT.

Published

2019

21. A pilot investigation of low-pass genome sequencing identifying site-specific variation in chromosomal mosaicisms by a multiple site sampling approach in first-trimester miscarriages

Author

Ying Li, Matthew Hoi Kin Chau, Ying Xin Zhang, Yilin Zhao, Shuwen Xue, Tin Chiu Li, Ye Cao, Zirui Dong, Kwong Wai Choy, and Jacqueline Pui Wah Chung

Subjects

Reproductive Medicine, Rehabilitation, Obstetrics and Gynecology

Abstract

STUDY QUESTION Can multiple-site low-pass genome sequencing (GS) of products of conception (POCs) improve the detection of genetic abnormalities, especially heterogeneously distributed mosaicism and homogeneously distributed mosaicism in first-trimester miscarriage? SUMMARY ANSWER Multiple-site sampling combined with low-pass GS significantly increased genetic diagnostic yield (77.0%, 127/165) of first-trimester miscarriages, with mosaicisms accounting for 17.0% (28/165), especially heterogeneously distributed mosaicisms (75%, 21/28) that are currently underappreciated. WHAT IS KNOWN ALREADY Aneuploidies are well known to cause first-trimester miscarriage, which are detectable by conventional karyotyping and next-generation sequencing (NGS) on a single-site sampling basis. However, there are limited studies demonstrating the implications of mosaic genetic abnormalities in first-trimester miscarriages, especially when genetic heterogeneity is present in POCs. STUDY DESIGN, SIZE, DURATION This is a cross-sectional cohort study carried out at a university-affiliated public hospital. One hundred seventy-four patients diagnosed with first-trimester miscarriage from December 2018 to November 2021 were offered ultrasound-guided manual vacuum aspiration (USG-MVA) treatment. Products of conception were subjected to multiple-site low-pass GS for the detection of chromosomal imbalances. PARTICIPANTS/MATERIALS, SETTING, METHODS For each POC, multiple sites of villi (three sites on average) were biopsied for low-pass GS. Samples with maternal cell contamination (MCC) and polyploidy were excluded based on the quantitative fluorescence polymerase chain reaction (QF-PCR) results. The spectrum of chromosomal abnormalities, including mosaicism (heterogeneously distributed and homogeneously distributed) and constitutional abnormalities was investigated. Chromosomal microarray analysis and additional DNA fingerprinting were used for validation and MCC exclusion. A cross-platform comparison between conventional karyotyping and our multiple-site approach was also performed. MAIN RESULTS AND THE ROLE OF CHANCE One hundred sixty-five POCs (corresponding to 490 DNA samples) were subjected to low-pass GS. Genetic abnormalities were detected in 77.0% (127/165) of POCs by our novel approach. Specifically, 17.0% (28/165) of cases had either heterogeneously distributed mosaicism (12.7%, 21/165) or homogeneously distributed mosaicism (6.1%, 10/165) (three cases had both types of mosaicism). The remaining 60.0% (99/165) of cases had constitutional abnormalities. In addition, in the 71 cases with karyotyping performed in parallel, 26.8% (19/71) of the results could be revised by our approach. LIMITATIONS, REASONS FOR CAUTION Lack of a normal gestational week-matched cohort might hinder the establishment of a causative link between mosaicisms and first-trimester miscarriage. WIDER IMPLICATIONS OF THE FINDINGS Low-pass GS with multiple-site sampling increased the detection of chromosomal mosaicisms in first-trimester miscarriage POCs. This innovative multiple-site low-pass GS approach enabled the novel discovery of heterogeneously distributed mosaicism, which was prevalent in first-trimester miscarriage POCs and frequently observed in preimplantation embryos, but is currently unappreciated by conventional single-site cytogenetic investigations. STUDY FUNDING/COMPETING INTEREST(S) This work was supported partly by Research Grant Council Collaborative Research Fund (C4062-21GF to K.W.C), Science and Technology Projects in Guangzhou (202102010005 to K.W.C), Guangdong-Hong Kong Technology Cooperation Funding Scheme (TCFS), Innovation and Technology Fund (GHP/117/19GD to K.W.C), HKOG Direct Grant (2019.050 to J.P.W.C), and Hong Kong Health and Medical Research Fund (05160406 to J.P.W.C). The authors have no competing interests to declare. TRIAL REGISTRATION NUMBER N/A.

Published

2023

22. Supplementary Table S2 from MiR-222 Overexpression Confers Cell Migratory Advantages in Hepatocellular Carcinoma through Enhancing AKT Signaling

Author

Nathalie Wong, Paul B-S. Lai, Ka-Fai To, Kwong-Wai Choy, Anthony W-H. Chan, Arthur K-K. Ching, and Queenie W-L. Wong

Abstract

Supplementary Table S2 from MiR-222 Overexpression Confers Cell Migratory Advantages in Hepatocellular Carcinoma through Enhancing AKT Signaling

Published

2023

23. Data from MiR-222 Overexpression Confers Cell Migratory Advantages in Hepatocellular Carcinoma through Enhancing AKT Signaling

Author

Nathalie Wong, Paul B-S. Lai, Ka-Fai To, Kwong-Wai Choy, Anthony W-H. Chan, Arthur K-K. Ching, and Queenie W-L. Wong

Abstract

Purpose: This study aims to profile the expressions of 156 microRNAs (miRNA) in hepatocellular carcinoma (HCC) and to characterize the functions of miR-222, the most significantly upregulated candidate identified.Experimental Design: miRNA expression profile in HCC tumors, matching adjacent cirrhotic livers, and cell lines was conducted using quantitative PCR. Common miR-222 upregulations were further validated in a larger cohort of tumors. The functional effects of miR-222 inhibition on HCC cell lines were examined. The downstream modulated pathways and target of miR-222 were investigated by coupling gene expression profiling and pathway analysis, and by in silico prediction, respectively. Luciferase reporter assay was done to confirm target interaction.Results: We identified a 40-miRNA signature that could discriminate tumors from adjacent cirrhotic liver tissue, and further corroborated common miR-222 overexpression in tumors relative to its premalignant counterpart (55.3%; P < 0.0001). Increased miR-222 expression correlated significantly with advanced stage HCC and with the shorter disease-free survival of patients (P ≤ 0.01). Inhibition of miR-222 in Hep3B and HKCI-9 significantly retarded cell motility (P < 0.05). Further investigations suggested that AKT signaling was the major pathway influenced by miR-222. A consistent reduction of AKT phosphorylation in Hep3B and HKCI-9 was shown following miR-222 suppression. The protein phosphatase 2A subunit B (PPP2R2A) was predicted as a putative miR-222 target in silico. We found that miR-222 inhibition could augment the tumor protein level and restore luciferase activity in reporter construct containing the PPP2R2A 3′ untranslated region (P = 0.0066).Conclusions: Our study showed that miR-222 overexpression is common in HCC and could confer metastatic potentials in HCC cells, possibly through activating AKT signaling. Clin Cancer Res; 16(3); 867–75

Published

2023

24. Supplementary Data from MiR-222 Overexpression Confers Cell Migratory Advantages in Hepatocellular Carcinoma through Enhancing AKT Signaling

Author

Nathalie Wong, Paul B-S. Lai, Ka-Fai To, Kwong-Wai Choy, Anthony W-H. Chan, Arthur K-K. Ching, and Queenie W-L. Wong

Abstract

Supplementary Data from MiR-222 Overexpression Confers Cell Migratory Advantages in Hepatocellular Carcinoma through Enhancing AKT Signaling

Published

2023

25. Supplementary Figure S1 from MiR-222 Overexpression Confers Cell Migratory Advantages in Hepatocellular Carcinoma through Enhancing AKT Signaling

Author

Nathalie Wong, Paul B-S. Lai, Ka-Fai To, Kwong-Wai Choy, Anthony W-H. Chan, Arthur K-K. Ching, and Queenie W-L. Wong

Abstract

Supplementary Figure S1 from MiR-222 Overexpression Confers Cell Migratory Advantages in Hepatocellular Carcinoma through Enhancing AKT Signaling

Published

2023

26. Case report: prenatal recurrent microcephaly and corpus callosum abnormalities in a Chinese family with novel biallelic SASS6 mutations

Author

Yi Man Isabella Wah, Ye Cao, Chun Yiu Law, Kwong Wai CHOY, Tak Yeung Leung, Angel H. W. Kwan, and Liona C.Poon Poon

Subjects

Embryology, Pediatrics, Perinatology and Child Health, Obstetrics and Gynecology, Radiology, Nuclear Medicine and imaging, General Medicine

Abstract

Introduction: Primary microcephaly (MCPH) is not an uncommon disorder with multiple etiologies. There is a growing number of MCPH-related genes discovered due to the extensive application of whole-exome sequencing (WES) in clinical and research settings. Biallelic mutations in the SASS6 gene cause an extremely rare MCPH, type 14. To date, only two families with SASS6 gene-related microcephaly have been reported. Case description: We report a case of recurrent congenital microcephaly in a Chinese family. The two affected fetuses presented with microcephaly early in the second trimester with agenesis of the corpus callosum. In the first affected fetus, trio WES detected two compound heterozygous candidate variants c.1139T>C(p.L380P) and c.1223C>G (p.T408S) in the SASS6 gene. Another affected fetus also inherited both variants, while the normal child carried neither variant through Sanger sequencing analysis. Both variants were classified as a variant of uncertain significance according to the current American College of Medical Genetics and Genomics guidelines. Conclusion: We reported novel biallelic variants in the SASS6 gene, encoding the SAS6 centriolar assembly protein, associated with prenatal onset of autosomal recessive microcephaly. We postulate that the pathomechanism of the compound heterozygous variants in close proximity could potentiate the overall coiled instability leading to the phenotypic features of our case.

Published

2023

27. Contributors

Author

Vimla Aggarwal, T.M. Barber, Christian M. Becker, Karanveer Bhangu, Mats Brännström, Carolyn J. Brown, Richard O. Burney, Antonio Capalbo, Wai-Yee Chan, Andy Chun Hang Chen, Chien-Wen Chen, Ming-Jer Chen, Zi-Jiang Chen, Ya-Ching Chou, Kwong Wai Choy, Hugh J. Clarke, Marcos Cordoba, Pernilla Dahm-Kähler, Mo-Yu Dai, Jessica Garcia de Paredes, Guo-Lian Ding, Zirui Dong, Jin Du, C. Eguizabal, Heather E. Fice, S. Franks, Qing-Qin Gao, Jessica Giordano, Linda C. Giudice, Jordan Gosnell, Ting Guo, Meade Haller, Tristan Hardy, Qilong He, L. Herrera, Ali Honaramooz, Cheng Huang, He-Feng Huang, Ghada Hussein, Sylvie Jaillard, Hai-Ping Jiang, Zi-Ru Jiang, Laura Kasak, Kazuhiro Kawamura, Ali Khatibi, Chaini Konwar, Maris Laan, Guan-Lin Lai, Jonathan LaMarre, Dolores J. Lamb, Yin Lau Lee, Yi-Xuan Lee, Brynn Levy, Xin-Yuan Li, Yao Li, Yu-Fei Li, Jinyue Liao, Ming Liu, Xiaodong Liu, Xin-Mei Liu, Y.M. Dennis Lo, Xinyi Ma, Yun-Yi Ma, M. Martin-Inaraja, Stacey A. Missmer, Kai Kei Miu, Grant Montgomery, N. Montserrat, Cynthia C. Morton, Maria Jose Navarro-Cobos, Robert J. Norman, Marisol O’Neill, Fanghong Ou, Yanli Pang, Maria S. Peñaherrera, Maurizio Poli, Jose M. Polo, Jie Qiao, Yingying Qin, Endah Rahmawati, Nilufer Rahmioglu, Bernard Robaire, Wendy P. Robinson, Alice P. Rogers, Peter A.W. Rogers, I. Romayor, Kristiina Rull, Victor A. Ruthig, Matthew A. Shanahan, Xuan Shao, Andrew H. Sinclair, Leanne Stalker, Kate Stanley, Melissa Stosic, Michael Strug, Hoi-Ching Suen, Jia Ping Tan, Jose M. Teixeira, Nannan Thirumavalavan, Jason C.H. Tsang, Allison Tscherner, Elena J. Tucker, Chii-Ruey Tzeng, Ignatia B. Van den Veyver, Margot van Riel, Joris R. Vermeesch, Liesbeth Vossaert, Wei Wang, Yan-Ling Wang, Zhangting Wang, Ronald Wapner, Nicholas Werry, Jeffrey T. White, Samantha L. Wilson, Jun Wu, Peng Xu, Liying Yan, Zhiqiang Yan, William Shu Biu Yeung, Stephanie C.Y. Yu, Peng Yuan, Victor Yuan, Fan Zhai, Shidou Zhao, Yue Zhao, Boryana Zhelyazkova, Qi Zhou, and Krina Zondervan

Published

2023

28. Molecular cytogenomics of human genetic disorders

Author

Zirui Dong, Kwong Wai Choy, and Cynthia C. Morton

Published

2023

29. Mate-pair genome sequencing reveals structural variants for idiopathic male infertility

Author

Zirui Dong, Jicheng Qian, Tracy Sze Man Law, Matthew Hoi Kin Chau, Ye Cao, Shuwen Xue, Steve Tong, Yilin Zhao, Yvonne K. Kwok, Karen Ng, David Yiu Leung Chan, Peter K-F Chiu, Chi-Fai Ng, Cathy Hoi Sze Chung, Jennifer Sze Man Mak, Tak Yeung Leung, Jacqueline Pui Wah Chung, Cynthia C. Morton, and Kwong Wai Choy

Subjects

Genetics, Genetics (clinical)

Abstract

Currently, routine genetic investigation for males with infertility includes karyotyping analysis and PCR for Y chromosomal microdeletions to provide prognostic information such as sperm retrieval success rate. However, over 85% of the cases remain idiopathic. We assessed 101 males with primary infertility in a retrospective cohort analysis who have previously received negative results from standard-of-care tests. Mate-pair genome sequencing (with ~ 5kb DNA fragment-size), an alternative long-DNA sequencing method was performed to detect clinically significant structural variants (SVs) and copy-number neutral absence of heterozygosity (AOH). Candidate SVs were filtered against our in-house cohort of 1,077 fertile men, and potentially clinically significant variants were correlated with gene expression profiles from single-cell RNA-seq datasets that curated human fetal and postnatal testicular development and adult germ cells. Follow-up studies were conducted for each patient with clinically relevant finding(s). Molecular diagnoses were made for 15.9% (10/63) of patients with non-obstructive azoospermia and 21.1% (8/38) of patients with severe oligozoospermia, respectively. Among them, 17 clinically significant SVs were identified in 16 cases, including five well-known syndromes, two inversions, and 10 SVs with direct disruption of genes by intragenic rearrangements or complex insertions. Importantly, a genetic defect related to Intracytoplasmic Sperm Injection (ICSI) failure was identified in a non-obstructive azoospermia patient illustrating the additional value of an etiologic diagnosis in addition to determining sperm retrieval rate. Our study reveals a landscape of various genomic variants in 101 males with idiopathic infertility, not only advancing understanding of the underlying mechanisms of male infertility, but also impacting clinical management.

Published

2022

30. Implementation of Public Funded Genome Sequencing in Evaluation of Fetal Structural Anomalies

Author

Po Lam So, Annie Shuk Yi Hui, Teresa Wei Ling Ma, Wendy Shu, Amelia Pui Wah Hui, Choi Wah Kong, Tsz Kin Lo, Amanda Nim Chi Kan, Elaine Yee Ling Kan, Shuk Ching Chong, Brian Hon Yin Chung, Ho Ming Luk, Kwong Wai Choy, Anita Sik Yau Kan, and Wing Cheong Leung

Subjects

Fetus, Pregnancy, Prenatal Diagnosis, Exome Sequencing, Genetics, Humans, Female, fetal structural anomalies, genome sequencing, diagnostic yield, clinical impact, Genetics (clinical), Ultrasonography, Prenatal, Retrospective Studies

Abstract

With the advancements in prenatal diagnostics, genome sequencing is now incorporated into clinical use to maximize the diagnostic yield following uninformative conventional tests (karyotype and chromosomal microarray analysis). Hong Kong started publicly funded prenatal genomic sequencing as a sequential test in the investigation of fetal structural anomalies in April 2021. The objective of the study was to evaluate the clinical performance and usefulness of this new service over one year. We established a web-based multidisciplinary team to facilitate case selection among the expert members. We retrospectively analyzed the fetal phenotypes, test results, turnaround time and clinical impact in the first 15 whole exome sequencing and 14 whole genome sequencing. Overall, the molecular diagnostic rate was 37.9% (11/29). De novo autosomal dominant disorders accounted for 72.7% (8/11), inherited autosomal recessive disorders for 18.2% (2/11), and inherited X-linked disorders for 9.1% (1/11). The median turnaround time for ongoing pregnancy was 19.5 days (range, 13–31 days). Our study showed an overall clinical impact of 55.2% (16/29), which influenced reproductive decision-making in four cases, guided perinatal management in two cases and helped future family planning in ten cases. In conclusion, our findings support the important role of genome sequencing services in the prenatal diagnosis of fetal structural anomalies in a population setting. It is important to adopt a multidisciplinary team approach to support the comprehensive genetic service.

Published

2022

31. A genome-wide association study of Chinese and English language abilities in Hong Kong Chinese children

Author

Yu-Ping Lin, Yujia Shi, Ruoyu Zhang, Xiao Xue, Shitao Rao, Kevin Fai-Hong Lui, Dora Jue Pan, Urs Maurer, Richard Kwong-Wai Choy, Silvia Paracchini, Catherine McBride, and Hon-Cheong So

Abstract

BackgroundReading and language skills are important and known to be heritable, and dyslexia and developmental language disorder are commonly recognized learning difficulties worldwide. However, the genetic basis underlying these skills remains poorly understood. In particular, most previous genetic studies were performed on Westerners. To our knowledge, few or no previous genome-wide association studies (GWAS) have been conducted on literacy skills in Chinese as a native language or English as a second language (ESL) in a Chinese population.MethodsWe conducted GWAS and related bioinformatics analyses on 34 reading/language-related phenotypes in Hong Kong Chinese bilingual children (including both twins and singletons; N=1046). We performed association tests at the single-variant, gene, pathway levels, and transcriptome-wide association studies (TWAS) to explore how imputed expression changes might affect the phenotypes. In addition, we tested genetic overlap of these cognitive traits with other neuropsychiatric disorders, as well as cognitive performance (CP) and educational attainment (EA) using polygenic risk score (PRS) analysis.ResultsTotally 9 independent loci (LD-clumped at r2=0.01) reached genome-wide significance (p0.3 and having at least 2 correlated SNPs(r2>0.5) with pMANEA, TNR, PLXNC1 and SHTN1. We also revealed significantly enriched genes and pathways based on SNP-based analysis. In PRS analysis, EA and CP showed significant polygenic overlap with a variety of language traits, especially English literacy skills. ADHD PRS showed a significant association with English vocabulary score.ConclusionsThis study revealed numerous genetic loci that may be associated with Chinese and English abilities in a group of Chinese bilingual children. Further studies are warranted to replicate the findings and elucidate the mechanisms involved.

Published

2022

32. Low-pass genome sequencing-based detection of absence of heterozygosity: validation in clinical cytogenetics

Author

Zirui Dong, Yanyan Zhang, Zhenjun Yang, Matthew Hoi Kin Chau, Cynthia C. Morton, Kwong Wai Choy, Yi Man Wah, Mengmeng Shi, Yvonne K. Kwok, and Tak Yeung Leung

Subjects

0301 basic medicine, medicine.medical_specialty, Genomics, 030105 genetics & heredity, Biology, Polymorphism, Single Nucleotide, DNA sequencing, Article, Loss of heterozygosity, 03 medical and health sciences, Polymorphism (computer science), medicine, Humans, 1000 Genomes Project, Genetics (clinical), Genetics, Base Sequence, Cytogenetics, Chromosome Mapping, Uniparental Disomy, medicine.disease, Microarray Analysis, Uniparental disomy, 030104 developmental biology, Cytogenetic Analysis, Medical genetics

Abstract

Purpose: Absence of heterozygosity (AOH) is a genetic characteristic known to cause human genetic disorders through autosomal recessive or imprinting mechanisms. However, the analysis of AOH via low-pass genome sequencing (GS) is yet to be clinically available. Methods: Low-pass GS (4-fold) with different types of libraries was performed on 17 clinical samples with previously ascertained AOH by chromosomal microarray analysis (CMA). In addition, AOH detection was performed with low-pass GS data in 1,639 cases that had both GS and high-probe-density CMA data available from the 1000 Genomes Project. Cases with multiple AOHs (coefficient of inbreeding F ≥1/32) or terminal AOHs ≥5-Mb (suspected uniparental disomy) were reported based on guidelines of the American College of Medical Genetics and Genomics. Results: Low-pass GS revealed suspected segmental UPD and multiple AOHs (F≥1/32) in nine and eight clinical cases, respectively, consistent with CMA. Among the 1,639 samples, low-pass GS not only consistently detected multiple AOHs (F≥1/32) in 18 cases, but also reported 60 terminal AOHs in 44 cases including four mosaic AOHs at a level ranging from 50% to 75%. Conclusion: Overall, our study demonstrates the feasibility of AOH analysis (≥5-Mb) with low-pass GS data and shows high concordance compared with CMA.

Published

2021

33. Diagnostic Yield of Exome Sequencing in Fetuses with Sonographic Features of Skeletal Dysplasias but Normal Karyotype or Chromosomal Microarray Analysis: A Systematic Review

Author

Kai Yeung Tse, Ilham Utama Surya, Rima Irwinda, Kwok Yin Leung, Yuen Ha Ting, Ye Cao, and Kwong Wai Choy

Subjects

Genetics, Genetics (clinical)

Abstract

Skeletal dysplasias are a group of diseases characterized by bone and joint abnormalities, which can be detected during prenatal ultrasound. Next-generation sequencing has rapidly revolutionized molecular diagnostic approaches in fetuses with structural anomalies. This review studies the additional diagnostic yield of prenatal exome sequencing in fetuses with prenatal sonographic features of skeletal dysplasias. This was a systematic review by searching PubMed for studies published between 2013 and July 2022 that identified the diagnostic yield of exome sequencing after normal karyotype or chromosomal microarray analysis (CMA) for cases with suspected fetal skeletal dysplasias based on prenatal ultrasound. We identified 10 out of 85 studies representing 226 fetuses. The pooled additional diagnostic yield was 69.0%. The majority of the molecular diagnoses involved de novo variants (72%), while 8.7% of cases were due to inherited variants. The incremental diagnostic yield of exome sequencing over CMA was 67.4% for isolated short long bones and 77.2% for non-isolated cases. Among phenotypic subgroup analyses, features with the highest additional diagnostic yield were an abnormal skull (83.3%) and a small chest (82.5%). Prenatal exome sequencing should be considered for cases with suspected fetal skeletal dysplasias with or without a negative karyotype or CMA results. Certain sonographic features, including an abnormal skull and small chest, may indicate a potentially higher diagnostic yield.

Published

2023

34. Neuropathological signatures revealed by transcriptomic and proteomic analysis in Pten-deficient mouse models of autism spectrum disorders

Author

Andrew Man-Lok Chan, Stanley Kwok-Kuen Cheung, Jacinda Kwok, Penelope Mei-Yu Or, Chi Wai Wong, Bo Feng, Kwong Wai Choy, Raymond C.C. Chang, J. Peter H. Burbach, and Alfred Sze-Lok Cheng

Abstract

Background: PTEN Hamartoma Tumor Syndrome (PHTS) is characterized by frequent mutation in PTEN gene. PHTS patients have numerous neurological defects including macrocephaly and autism spectrum disorder. While clinical features of PHTS are likely the result of PTEN haploinsufficiency, the role of PTEN gene dosage in driving transcriptomic changes in specific neural cell types is not known. Methods: We performed transcriptomic and proteomic analysis on neural tissues and primary cultures from Pten heterozygous and homozygous knockout mice. Results: We found that somatosensory cortex (SSC) of Pten heterozygous mice are enriched with immune response and oligodendrocyte development Gene Ontology (GO) terms. Parallel proteomic analysis reveals differentially expressed proteins (DEPs) related to dendritic spine development, keratinization and hamartoma signatures. The lack of concordance between transcriptomic and proteomic data prompted us to profile the transcriptomes of specific neural cell types. Overall, Pten homozygous knockout cells have much greater differential expressed genes (DEGs) than Pten heterozygous knockout cells. Pten heterozygous knockout primary astrocytes (AST) are enriched in Extracellular Matrix GO terms while primary cortical neurons (PCN) are enriched with immediate-early genes. In Pten homozygous knockout AST, cilium-related activity is enriched while PCN exhibited downregulation of forebrain neuron generation and differentiation which may lead to disruption of excitatory/inhibitory balance in brain. By integrating DEPs with a pre-filtered DEGs, we identified traits of intelligence and cognitive function, and schizophrenia being enriched, and DEP from AST is significantly associated with intelligence and depression.Limitations: First, bulk tissues were used for transcriptomic and proteomics analysis. Cell type specific expression changes may not be revealed. Second, primary neural cell cultures were used for transcriptomic analysis, which may not reflect the normal physiological conditions.Conclusions: We have uncovered transcriptomic alterations and molecular pathways that may explain neurological disorders associated with PHTS.

Published

2022

35. A γA-Crystallin Mouse Mutant Secc with Small Eye, Cataract and Closed Eyelid.

Author

Man Hei Cheng, Chung Nga Tam, Kwong Wai Choy, Wai Hung Tsang, Sze Lan Tsang, Chi Pui Pang, You Qiang Song, and Mai Har Sham

Subjects

Medicine, Science

Abstract

Cataract is the most common cause of visual loss in humans. A spontaneously occurred, autosomal dominant mouse mutant Secc, which displayed combined features of small eye, cataract and closed eyelid was discovered in our laboratory. In this study, we identified the mutation and characterized the cataract phenotype of this novel Secc mutant. The Secc mutant mice have eyelids that remain half-closed throughout their life. The mutant lens has a significant reduction in size and with opaque spots clustered in the centre. Histological analysis showed that in the core region of the mutant lens, the fiber cells were disorganized and clefts and vacuoles were observed. The cataract phenotype was evident from new born stage. We identified the Secc mutation by linkage analysis using whole genome microsatellite markers and SNP markers. The Secc locus was mapped at chromosome 1 flanked by SNPs rs3158129 and rs13475900. Based on the chromosomal position, the candidate cataract locus γ-crystallin gene cluster (Cryg) was investigated by sequencing. A single base deletion (299delG) in exon 3 of Cryga which led to a frame-shift of amino acid sequence from position 91 was identified. As a result of this mutation, the sequences of the 3rd and 4th Greek-key motifs of the γA-crystallin are replaced with an unrelated C-terminal peptide of 75 residues long. Coincidentally, the point mutation generated a HindIII restriction site, allowing the identification of the CrygaSecc mutant allele by RFLP. Western blot analysis of 3-week old lenses showed that the expression of γ-crystallins was reduced in the CrygaSecc mutant. Furthermore, in cell transfection assays using CrygaSecc mutant cDNA expression constructs in 293T, COS-7 and human lens epithelial B3 cell lines, the mutant γA-crystallins were enriched in the insoluble fractions and appeared as insoluble aggregates in the transfected cells. In conclusion, we have demonstrated that the Secc mutation leads to the generation of CrygaSecc proteins with reduced solubility and prone to form aggregates within lens cells. Accumulation of mutant proteins in the lens fibers would lead to cataract formation in the Secc mutant.

Published

2016

36. The role of chromosomal microarray analysis among fetuses with normal karyotype and single system anomaly or nonspecific sonographic findings

Author

Yvonne K. Kwok, Matthew Hoi Kin Chau, Xiaofan Zhu, Kwong Wai Choy, Yiu Man Chan, Terence T. Lao, Zihan Chen, Tak Yeung Leung, Ye Cao, Annie Sy Hui, and Angel Hw Kwan

Subjects

Pathology, medicine.medical_specialty, DNA Copy Number Variations, Karyotype, Intrauterine growth restriction, Chromosome Disorders, Prenatal diagnosis, Ultrasonography, Prenatal, Congenital Abnormalities, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, Prenatal Diagnosis, Hydrops fetalis, medicine, Humans, 030212 general & internal medicine, Increased nuchal translucency, Retrospective Studies, Fetal Growth Retardation, 030219 obstetrics & reproductive medicine, Genitourinary system, business.industry, Ultrasound, Obstetrics and Gynecology, Cystic hygroma, General Medicine, Microarray Analysis, medicine.disease, Female, Abnormality, business

Abstract

Introduction Chromosomal microarray analysis is recommended as the first-tier test for the evaluation of fetuses with structural anomalies. This study aims to investigate the incremental diagnostic yield of chromosomal microarray over conventional karyotyping analysis in fetuses with anomalies restricted to one anatomic system and those with nonspecific anomalies detected by sonography. Material and methods This is a retrospective cohort analysis of 749 fetuses undergoing prenatal diagnosis for abnormal ultrasound findings isolated to one anatomic system and normal karyotype, utilizing chromosomal microarray. Overall, 495 (66%) fetuses had anomalies confined to one anatomic system and 254 (34%) had other nonspecific anomalies including increased nuchal translucency (≥3.5 mm), cystic hygroma, intrauterine growth restriction and hydrops fetalis. Results Fetuses with ultrasound anomalies restricted to one anatomic system had a 3.0% risk of carrying a pathogenic copy number variant; the risk varied dependent on the anatomic system affected. Fetuses with confined anomalies of the cardiac system had the highest diagnostic yield at 4.6%, but there were none in the urogenital system. Fetuses with nonspecific ultrasound anomalies had the highest diagnostic yield in fetuses with an intrauterine growth restriction at 5.9%. Overall, fetuses with a nonspecific ultrasound anomaly were affected with pathogenic copy number variants in 1.6% in the cases. Conclusions The diagnostic yield of chromosomal microarray in fetuses with normal karyotype and ultrasound abnormality confined to a single anatomic system was highest if it involved cardiac defects or intrauterine growth restriction. This diagnostic yield ranges from 0% to 4.6% depending on the anatomic system involved. Chromosomal microarray has considerable diagnostic value in these pregnancies.

Published

2020

37. Long-Molecule Sequencing

Author

Hui Liu, Qian Yu, Hailong Huang, Lingji Chen, Yan Wang, Deqin He, David S. Cram, Aiping Mao, Zhang Xiaojie, Xiaoyu Li, Hua Cao, Min Zhang, Jianguang Zhang, Yuan Lin, Han Jin, Baoheng Gui, Meihuan Chen, Na Lin, Liangpu Xu, and Kwong Wai Choy

Subjects

0301 basic medicine, Thalassemia, Single-nucleotide polymorphism, Computational biology, Amplicon, Biology, Compound heterozygosity, medicine.disease, Pathology and Forensic Medicine, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, medicine, Molecular Medicine, Multiplex, Copy-number variation, Genotyping, Reference genome

Abstract

Multiple molecular tests are currently needed for accurate carrier testing for thalassemia. Therefore, long-molecule sequencing (LMS) was evaluated as an alternate on the PacBio Sequel platform for genotyping carriers of α-thalassemia or β-thalassemia. Multiplex long PCR was used to generate representative amplicons for the α (HBA1/2) and β (HBB) gene loci. Following LMS, circular consensus sequencing reads were aligned to the hg19 reference genome and variants called using FreeBayes software version 1.2.0. In a blinded study of 64 known carrier samples, all HBA1/2 and HBB variants detected by LMS were concordant with those independently assigned by targeted PCR assays. For HBA1/2 carrier samples, LMS accurately detected the common South East Asian, -α3.7, and -α4.2 deletions and four different rare single-nucleotide variants (SNVs). For HBB carrier samples, LMS accurately detected the most common Chinese insertion and deletion variant c.126_129delCTTT and 14 different SNVs/insertions and deletions and could discriminate compound heterozygous SNVs (trans configuration) and identify variants linked to benign SNPs (cis configuration). Overall, LMS displayed the hallmarks of a scalable, accurate, and cost-effective genotyping method. With further test coverage to additionally include detection of other clinically significant HBA1/2 copy number variations, such as the Thai, Mediterranean, and Filipino deletions, LMS may eventually serve as a comprehensive method for large-scale thalassemia carrier screening.

Published

2020

38. Deciphering the complexity of simple chromosomal insertions by genome sequencing

Author

Pawel Stankiewicz, Peng Dai, Tak Yeung Leung, Sau Wai Cheung, Xiangdong Kong, Zirui Dong, Yvonne K. Kwok, Xiaofan Zhu, Yanyan Zhang, Matthew Hoi Kin Chau, and Kwong Wai Choy

Subjects

Genetics, 0303 health sciences, Chromothripsis, Sequence analysis, 030305 genetics & heredity, Breakpoint, Chromosome, Karyotype, Chromosomal translocation, Biology, DNA sequencing, Non-homologous end joining, 03 medical and health sciences, Genetics (clinical), 030304 developmental biology

Abstract

Chromosomal insertions are thought to be rare structural rearrangements. The current understanding of the underlying mechanisms of their origin is still limited. In this study, we sequenced 16 cases with apparent simple insertions previously identified by karyotyping and/or chromosomal microarray analysis. Using mate-pair genome sequencing (GS), we identified all 16 insertions and revised previously designated karyotypes in 75.0% (12/16) of the cases. Additional cryptic rearrangements were identified in 68.8% of the cases (11/16). The incidence of additional cryptic rearrangements in chromosomal insertions was significantly higher compared to balanced translocations and inversions reported in other studies by GS. We characterized and classified the cryptic insertion rearrangements into four groups, which were not mutually exclusive: (1) insertion segments were fragmented and their subsegments rearranged and clustered at the insertion site (10/16, 62.5%); (2) one or more cryptic subsegments were not inserted into the insertion site (5/16, 31.3%); (3) segments of the acceptor chromosome were scattered and rejoined with the insertion segments (2/16, 12.5%); and (4) copy number gains were identified in the flanking regions of the insertion site (2/16, 12.5%). In addition to the observation of these chromothripsis- or chromoanasynthesis-like events, breakpoint sequence analysis revealed microhomology to be the predominant feature. However, no significant correlation was found between the number of cryptic rearrangements and the size of the insertion. Overall, our study provide molecular characterization of karyotypically apparent simple insertions, demonstrate previously underappreciated complexities, and evidence that chromosomal insertions are likely formed by nonhomologous end joining and/or microhomology-mediated replication-based DNA repair.

Published

2020

39. The utility of genome‐wide cell‐free <scp>DNA</scp> screening in the prenatal diagnosis of <scp>Pallister‐Killian</scp> syndrome

Author

Tze Kin Lau, Tak Yeung Leung, Sunny Wai Hung Cheung, Matthew Hoi Kin Chau, Kwong Wai Choy, Yuen Ha Ting, Yvonne K. Kwok, Doris Yuk Man Lam, Wan Pang Chan, Mengmeng Shi, Xiaofan Zhu, and Yves Ville

Subjects

Adult, Male, 0301 basic medicine, Oncology, China, medicine.medical_specialty, Microarray, Chromosome Disorders, Prenatal diagnosis, 030105 genetics & heredity, Cohort Studies, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Pallister–Killian syndrome, Predictive Value of Tests, Pregnancy, Prenatal Diagnosis, Internal medicine, Humans, Medicine, Genetic Testing, Genetics (clinical), Chromosome 12, Retrospective Studies, Comparative Genomic Hybridization, Chromosomes, Human, Pair 12, 030219 obstetrics & reproductive medicine, business.industry, Infant, Newborn, Obstetrics and Gynecology, Chromosome, Retrospective cohort study, Karyotype, Microarray Analysis, medicine.disease, Cell-free fetal DNA, Female, business, Cell-Free Nucleic Acids

Abstract

OBJECTIVE To report genome-wide cell-free DNA (cfDNA) screening facilitating the diagnosis of Pallister-Killian syndrome (PKS). METHODS This is a retrospective cohort analysis of positive genome-wide cfDNA screening results showing increased signal from chromosome 12 and the detection of PKS. The genome-wide cfDNA screening results and the subsequent investigations were reviewed. RESULTS Three singleton pregnancies (3/29007) from 2016 to 2017 yielded positive results indicating large gains on the entire p-arm of chromosome 12. In two cases, multiple structural abnormalities were detected by prenatal ultrasound and the couples opted for termination of pregnancy. Chromosomal microarray performed on fetal skin tissues of the two abortuses detected mosaic tetrasomy 12p, consistent with PKS. In the third case, karyotype and chromosomal microarray performed on an amniotic fluid sample also showed mosaic tetrasomy 12p. In each of the three cases, genome-wide cfDNA screening revealed a large gain on chromosome 12p; subsequent prenatal or postnatal diagnostic testing confirmed the diagnosis of PKS. CONCLUSION We report the ability of genome-wide cfDNA screening to provide early suspicion and facilitate the subsequent genetic diagnosis of PKS. As genome-wide cfDNA screening becomes increasingly available, incidental diagnosis of partial aneuploidies is expected to increase.

Published

2020

40. Autism‐associated PTEN missense mutation leads to enhanced nuclear localization and neurite outgrowth in an induced pluripotent stem cell line

Author

Alfred S. L. Cheng, Lisha Li, Tian Liu, Stanley K.K. Cheung, Bo Feng, J. P. H. Burbach, Yubing Wang, Andrew K Chan, Raymond Chuen-Chung Chang, Chi Wai Wong, Kwong Wai Choy, and Penelope M.Y. Or

Subjects

0301 basic medicine, PTEN, Autism Spectrum Disorder, autism spectrum disorders, Blotting, Western, Induced Pluripotent Stem Cells, Neuronal Outgrowth, Mutant, Mutation, Missense, Phosphatidate Phosphatase, macrocephaly, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Cell Line, Tumor, Humans, Missense mutation, Phosphorylation, Progenitor cell, Induced pluripotent stem cell, Molecular Biology, C2 domain, Cell Nucleus, biology, Protein Stability, Chemistry, neurodevelopmental disorders, PTEN Phosphohydrolase, Cell Biology, Cell biology, Editor's Choice, HEK293 Cells, 030104 developmental biology, 030220 oncology & carcinogenesis, PC-3 Cells, biology.protein, PTEN hamartoma tumor syndrome, Nuclear localization sequence

Abstract

Germline mutation in the PTEN gene is the genetic basis of PTEN hamartoma tumor syndrome with the affected individuals harboring features of autism spectrum disorders. Characterizing a panel of 14 autism‐associated PTEN missense mutations revealed reduced protein stability, catalytic activity, and subcellular distribution. Nine out of 14 (64%) PTEN missense mutants had reduced protein expression with most mutations confined to the C2 domain. Selected mutants displayed enhanced polyubiquitination and shortened protein half‐life, but that did not appear to involve the polyubiquitination sites at lysine residues at codon 13 or 289. Analyzing their intrinsic lipid phosphatase activities revealed that 78% (11 out of 14) of these mutants had twofold to 10‐fold reduction in catalytic activity toward phosphatidylinositol phosphate substrates. Analyzing the subcellular localization of the PTEN missense mutants showed that 64% (nine out of 14) had altered nuclear‐to‐cytosol ratios with four mutants (G44D, H123Q, E157G, and D326N) showing greater nuclear localization. The E157G mutant was knocked‐in to an induced pluripotent stem cell line and recapitulated a similar nuclear targeting preference. Furthermore, iPSCs expressing the E157G mutant were more proliferative at the neural progenitor cell stage but exhibited more extensive dendritic outgrowth. In summary, the combination of biological changes in PTEN is expected to contribute to the behavioral and cellular features of this neurodevelopmental disorder., Mutation of the PTEN gene has been linked to autism spectrum disorders (ASDs) and other disorders with autism‐like features. Here, Andrew Chen and co‐authors characterized a panel of PTEN autism‐associated mutants, unearthing a E157G PTEN mutant that displays preferential localization to the cell nucleus. The E157G mutant was knocked‐in to an iPSC line that recapitulated a similar nuclear‐targeting preference. In addition, iPSCs expressing the E157G mutant were more proliferative at the neural progenitor cell stage and exhibited more extensive dendritic outgrowth when induced to undergo neuronal differentiation, hinting at the contribution of PTEN to the cellular features of ASDs.

Published

2020

41. Recent Advances in the Noninvasive Prenatal Testing for Chromosomal Abnormalities Using Maternal Plasma DNA

Author

Tak Yeung Leung, Xiaofan Zhu, Tze Kin Lau, Yvonne K. Kwok, and Kwong Wai Choy

Subjects

0301 basic medicine, medicine.medical_specialty, 030219 obstetrics & reproductive medicine, Screening test, business.industry, Obstetrics, Plasma dna, Reproductive medicine, Diagnostic test, 030105 genetics & heredity, Predictive value, 03 medical and health sciences, 0302 clinical medicine, Prenatal screening, Chromosomal structural abnormalities, Modeling and Simulation, Medicine, Detection rate, business

Abstract

Abstract No single invention in the past has created such a rapid and massive impact on clinical obstetric practice as the introduction of noninvasive prenatal screening (NIPS) for chromosomal abnormalities using cell-free DNA in maternal plasma. However, the technology of NIPS which has also been called noninvasive prenatal testing (NIPT) is rapidly evolving. Most clinicians may not be able to fully understand this new technology to enable good clinical practice. This review will be focused on issues that have important clinical implications. NIPT/S is only a screening test and all positive cases must be confirmed by invasive diagnostic techniques. Although NIPT/S is being expanded rapidly to cover other chromosomes and large chromosomal structural abnormalities, the detection rate is still uncertain, and the positive predictive value is expected to be lower. Pregnant women who are at risk of chromosomal abnormalities other than common trisomies should be offered a diagnostic test instead of NIPT/S. The use of NIPT/S as a primary Down syndrome screening test should not replace the 11–13 weeks scan.

Published

2020

42. Low-pass genome sequencing versus chromosomal microarray analysis: implementation in prenatal diagnosis

Author

Shaoyun Chen, Zhenjun Yang, Hoi Kin Wong, Kwong Wai Choy, Matthew Hoi Kin Chau, Zirui Dong, Yvonne K. Kwok, Kelin Xiao, Tak Yeung Leung, Cynthia C. Morton, Xiaofan Zhu, Rui Zhang, Zhuo Meng, Baoheng Gui, Kathy Yin Ching Tsang, Yanfang Wang, Sau Wai Cheung, Yuanfang Zhu, and Huilin Wang

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, DNA Copy Number Variations, Context (language use), Prenatal diagnosis, Genomics, molecular karyotyping, 030105 genetics & heredity, Article, Chromosomes, DNA sequencing, 03 medical and health sciences, Pregnancy, Prenatal Diagnosis, Internal medicine, Humans, Medicine, Copy-number variation, low-pass genome sequencing, health care economics and organizations, Genetics (clinical), Likely pathogenic, Chromosome Aberrations, Genome, Human, business.industry, Microarray analysis techniques, Microarray Analysis, copy-number variants, mosaicism, 030104 developmental biology, Karyotyping, Medical genetics, Female, business

Abstract

PurposeEmerging studies suggest that low-pass genome sequencing (GS) provides additional diagnostic yield of clinically significant copy-number variants (CNVs) compared with chromosomal microarray analysis (CMA). However, a prospective back-to-back comparison evaluating accuracy, efficacy, and incremental yield of low-pass GS compared with CMA is warranted.MethodsA total of 1023 women undergoing prenatal diagnosis were enrolled. Each sample was subjected to low-pass GS and CMA for CNV analysis in parallel. CNVs were classified according to guidelines of the American College of Medical Genetics and Genomics.ResultsLow-pass GS not only identified all 124 numerical disorders or pathogenic or likely pathogenic (P/LP) CNVs detected by CMA in 121 cases (11.8%, 121/1023), but also defined 17 additional and clinically relevant P/LP CNVs in 17 cases (1.7%, 17/1023). In addition, low-pass GS significantly reduced the technical repeat rate from 4.6% (47/1023) for CMA to 0.5% (5/1023) and required less DNA (50 ng) as input.ConclusionIn the context of prenatal diagnosis, low-pass GS identified additional and clinically significant information with enhanced resolution and increased sensitivity of detecting mosaicism as compared with the CMA platform used. This study provides strong evidence for applying low-pass GS as an alternative prenatal diagnostic test.

Published

2020

43. Genome Sequencing Explores Complexity of Chromosomal Abnormalities in Recurrent Miscarriage

Author

Ye Cao, Wenwei Zhang, Lingyun Chen, Wen-Jing Wang, Yan Hong, Haixiao Chen, Raul E. Piña-Aguilar, Fengping Xu, Cynthia C. Morton, Zi-Jiang Chen, Karsten Kristiansen, Junhao Yan, Yuhua Shi, Jiguang Li, Jinjin Xu, Sau Wai Cheung, Chen Yuan, Huanming Yang, Qiaoling Li, Xia Zhao, Jacqueline Pui Wah Chung, Amber N. Pursley, Pei Li, Han Zhao, Yingying Qin, Ao Chen, Tak Yeung Leung, Kwong Wai Choy, Hui Jiang, Zhenjun Yang, Jianying Yuan, Yvonne K. Kwok, Yuan Jiang, Huilin Wang, Zirui Dong, Tao Ma, Lingfei Ye, Hoi Gin Wong, and Lei Zhang

Subjects

Adult, Male, 0301 basic medicine, Abortion, Habitual, Chromosomal translocation, Biology, Article, DNA sequencing, Miscarriage, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, Recurrent miscarriage, Genetics, medicine, Humans, Copy-number variation, Genetics (clinical), Retrospective Studies, Chromosome Aberrations, 030219 obstetrics & reproductive medicine, Whole Genome Sequencing, medicine.diagnostic_test, Karyotype, Prognosis, medicine.disease, 030104 developmental biology, Karyotyping, Relative risk, Female, Follow-Up Studies, Fluorescence in situ hybridization

Abstract

Recurrent miscarriage (RM) affects millions of couples globally, and half of them have no demonstrated etiology. Genome sequencing (GS) is an enhanced and novel cytogenetic tool to define the contribution of chromosomal abnormalities in human diseases. In this study we evaluated its utility in RM-affected couples. We performed low-pass GS retrospectively for 1,090 RM-affected couples, all of whom had routine chromosome analysis. A customized sequencing and interpretation pipeline was developed to identify chromosomal rearrangements and deletions/duplications with confirmation by fluorescence in situ hybridization, chromosomal microarray analysis, and PCR studies. Low-pass GS yielded results in 1,077 of 1,090 couples (98.8%) and detected 127 chromosomal abnormalities in 11.7% (126/1,077) of couples; both members of one couple were identified with inversions. Of the 126 couples, 39.7% (50/126) had received former diagnostic results by karyotyping characteristic of normal human male or female karyotypes. Low-pass GS revealed additional chromosomal abnormalities in 50 (4.0%) couples, including eight with balanced translocations and 42 inversions. Follow-up studies of these couples showed a higher miscarriage/fetal-anomaly rate of 5/10 (50%) compared to 21/93 (22.6%) in couples with normal GS, resulting in a relative risk of 2.2 (95% confidence interval, 1.1 to 4.6). In these couples, this protocol significantly increased the diagnostic yield of chromosomal abnormalities per couple (11.7%) in comparison to chromosome analysis (8.0%, chi-square test p = 0.000751). In summary, low-pass GS identified underlying chromosomal aberrations in 1 in 9 RM-affected couples, enabling identification of a subgroup of couples with increased risk of subsequent miscarriage who would benefit from a personalized intervention.

Published

2019

44. Prenatal Diagnosis: Morphology Scan and Invasive Methods

Author

Richard Kwong Wai Choy, Tak Yeung Leung

Published

2012

45. Investigation of Chromosomal Structural Abnormalities in Patients With Undiagnosed Neurodevelopmental Disorders

Author

Ye Cao, Ho Ming Luk, Yanyan Zhang, Matthew Hoi Kin Chau, Shuwen Xue, Shirley S. W. Cheng, Albert Martin Li, Josephine S. C. Chong, Tak Yeung Leung, Zirui Dong, Kwong Wai Choy, and Ivan Fai Man Lo

Subjects

Genetics, Molecular Medicine, Genetics (clinical)

Abstract

Background: Structural variations (SVs) are various types of the genomic rearrangements encompassing at least 50 nucleotides. These include unbalanced gains or losses of DNA segments (copy number changes, CNVs), balanced rearrangements (such as inversion or translocations), and complex combinations of several distinct rearrangements. SVs are known to play a significant role in contributing to human genomic disorders by disrupting the protein-coding genes or the interaction(s) with cis-regulatory elements. Recently, different types of genome sequencing-based tests have been introduced in detecting various types of SVs other than CNVs and regions with absence of heterozygosity (AOH) with clinical significance.Method: In this study, we applied the mate-pair low pass (∼4X) genome sequencing with large DNA-insert (∼5 kb) in a cohort of 100 patients with neurodevelopmental disorders who did not receive informative results from a routine CNV investigation. Read-depth-based CNV analysis and chimeric-read-pairs analysis were used for CNV and SV analyses. The region of AOH was indicated by a simultaneous decrease in the rate of heterozygous SNVs and increase in the rate of homozygous SNVs.Results: First, we reexamined the 25 previously reported CNVs among 24 cases in this cohort. The boundaries of these twenty-five CNVs including 15 duplications and 10 deletions detected were consistent with the ones indicated by the chimeric-read-pairs analysis, while the location and orientation were determined in 80% of duplications (12/15). Particularly, one duplication was involved in complex rearrangements. In addition, among all the 100 cases, 10% of them were detected with rare or complex SVs (>10 Kb), and 3% were with multiple AOH (≥5 Mb) locating in imprinting chromosomes identified. In particular, one patient with an overall value of 214.5 Mb of AOH identified on 13 autosomal chromosomes suspected parental consanguinity.Conclusion: In this study, mate-pair low-pass GS resolved a significant proportion of CNVs with inconclusive significance, and detected additional SVs and regions of AOH in patients with undiagnostic neurodevelopmental disorders. This approach complements the first-tier CNV analysis for NDDs, not only by increasing the resolution of CNV detection but also by enhancing the characterization of SVs and the discovery of potential causative regions (or genes) contributory to could be complex in composition NDDs.

Published

2021

46. Prenatal Diagnosis and Pregnancy Outcomes of Fetuses With Orofacial Cleft: A Retrospective Cohort Study in Two Centres in Hong Kong

Author

Yan Yu Li, Wing Ting Tse, Choi Wah Kong, Natalie Kwun Long Wong, Tak Yeung Leung, Kwong Wai Choy, William Wing Kee To, and Ye Cao

Subjects

Otorhinolaryngology, Oral Surgery

Abstract

Objective To evaluate the local incidence of orofacial cleft (OFC) encountered in fetal morphology scan and prenatal diagnosis, genetic etiology of fetuses with or without other structural abnormalities, and their pregnancy outcomes. Design Retrospective cohort study. Setting Two maternal fetal medicine units, tertiary hospitals, Hong Kong. Participants All pregnant women with antenatal diagnosis of fetal OFC between January 2016 and December 2020 (N = 66). Results OFC has an incidence of 0.13% among pregnancies in Hong Kong and 28.8% (19/66) were syndromic cleft that exhibited other fetal structural anomalies. There were 55 cases (84.6%) who opted for invasive prenatal diagnostic testing. Genetic defects were identified in 25.8% (17/66) of this cohort, including 14 pathogenic variants. The detection rate in the syndromic cases is 68.4% (13/19) which was significantly higher than 8.5% (4/47) among non-syndromic cases. Aneuploidies would be the most common cause, accounting for 9.1% (6/66). Chromosomal microarray analysis (CMA) provided an incremental diagnostic yield of 6.1% compared to conventional karyotyping. A total of 29 live births including 3 cases of a variant of uncertain significance and 26 cases without genetic abnormalities detected have continued pregnancy to birth. There were 87.5% (21/24) without detectable pathogenic genetic abnormality reported good long-term outcomes. The chance of OFC fetuses having a good long-term outcome was significantly higher if no genomic variant was detected ( P Conclusions Invasive prenatal tests with CMA should be offered to pregnancies with OFC regardless of the type. It has provided incremental diagnostic yield over conventional karyotyping and helped in prenatal and genetic counseling. A negative result in non-syndromic OFC favors couples to keep the pregnancy.

Published

2022

47. Clinical Implications of Promoter Hypermethylation in RASSF1A and MGMT in Retinoblastoma

Author

Kwong Wai Choy, Tom C. Lee, Kin Fai Cheung, Dorothy S.P. Fan, Kwok Wai Lo, Katherine L. Beaverson, David H. Abramson, Dennis S.C. Lam, Christopher B.O. Yu, and Chi Pui Pang

Subjects

Retinoblastoma, methylation, RASSF1A, MGMT, RB, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

We investigated the epigenetic silencing and genetic changes of the RAS-associated domain family 1A (RASSF1A) gene and the Os-methylguanine-DNA methyltransferase (MGMT) gene in retinoblastoma. We extracted DNA from microdissected tumor and normal retina tissues of the same patient in 68 retinoblastoma cases. Promoter methylation in RASSF1A and MGMT was analyzed by methylation-specific PCR, RASSF1A sequence alterations in all coding exons by direct DNA sequencing, RASSF1A expression by RT-PCR. Cell cycle staging was analyzed by flow cytometry. We detected RASSF1A promoter hypermethylation in 82% of retinoblastoma, in tumor tissues only but not in adjacent normal retinal tissue cells. There was no expression of RASSF1A transcripts in all hypermethylated samples, but RASSF1A transcripts were restored after 5-aza-2′-deoxycytidine treatment with no changes in cell cycle or apoptosis. No mutation in the RASSF1A sequence was found. MGMT hypermethylation was present in 15% of theretinoblastoma samples, the absence of MGMT hypermethylation was associated (P = .002) with retinoblastoma at advanced ReeseEllsworth tumor stage. Our results revealed a high RASSF1A hypermethylation frequency in retinoblastoma. The correlation of MGMT inactivation by promoter hypermethylation with lower-stage diseases indicated that MGMT hypermethylation provides useful prognostic information. Epigenetic mechanism plays an important role in the progression of retinoblastoma.

Published

2005

48. Epigenetic Silencing of Cellular Retinol-Binding Proteins in Nasopharyngeal Carcinoma

Author

Joseph Kwong, Kwok-Wai Lo, Lillian Shuk-Nga Chow, Ka-Fai To, Kwong-Wai Choy, Franky Leung Chan, Samuel C. Mok, and Dolly P. Huang

Subjects

CRBPIV, CRBPI, retinoid, hypermethylation, nasopharyngeal carcinoma, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Aberrant retinoid signaling in human cancers is extending from the nucleus to the cytoplasm. Recently, we have demonstrated frequent epigenetic inactivation of a retinoic acid receptor (RAR), RARβ2, in nasopharyngeal carcinoma (NPC). To further explore targets contributing to aberrant retinoid signaling in NPC, the expression of cellular retinol-binding proteins (CRBPs), cellular retinoic acid-binding proteins (CRABPs), RARs, and retinoid X receptors (RXRs) was examined. Apart from RARβ2, transcriptional silencing of two CRBPs, CRBPI and CRBPIV, was observed in NPC cell lines and xenografts. Hypermethylation of CRBPI and CRBPIV CpG islands was found to be closely correlated with the loss of expression. Treatment with the DNA methyltransferase inhibitor, 5-aza2'-deoxycytidine, resulted in reexpression of CRBPI and CRBPIV gene expression in NPC cell lines. Both CRBPI and CRBPIV hypermethylations were also observed in 43/48 (87.8%) and 26/48 (54.2%) primary NPC tumors, respectively. Here, we reported for the first time that CRBPIV was transcriptionally inactivated by promoter hypermethylation in human cancer. Simultaneous methylation of CRBPI, CRBPIV, and RARβ2 was commonly found in NPC primary tumors. Our findings implied that epigenetic disruption of the CRBPs, CRBPI and CRBPIV, is important in NPC tumorigenesis and may contribute to the loss of retinoic acid responsiveness in cancer.

Published

2005

49. Genome sequencing reveals the role of rare genomic variants in Chinese patients with symptomatic intracranial atherosclerotic disease

Author

Mengmeng Shi, Xinyi Leng, Ying Li, Zihan Chen, Ye Cao, Tiffany Chung, Bonaventure YM Ip, Vincent HL Ip, Yannie OY Soo, Florence SY Fan, Sze Ho Ma, Karen Ma, Anne Y Y Chan, Lisa WC Au, Howan Leung, Alexander Y Lau, Vincent CT Mok, Kwong Wai Choy, Zirui Dong, and Thomas W Leung

Subjects

Stroke, China, Asian People, Humans, Neurology (clinical), Genomics, Cardiology and Cardiovascular Medicine, Intracranial Arteriosclerosis

Abstract

ObjectivesThe predisposition of intracranial atherosclerotic disease (ICAD) to East Asians over Caucasians infers a genetic basis which, however, remains largely unknown. Higher prevalence of vascular risk factors (VRFs) in Chinese over Caucasian patients who had a stroke, and shared risk factors of ICAD with other stroke subtypes indicate genes related to VRFs and/or other stroke subtypes may also contribute to ICAD.MethodsUnrelated symptomatic patients with ICAD were recruited for genome sequencing (GS, 60-fold). Rare and potentially deleterious single-nucleotide variants (SNVs) and small insertions/deletions (InDels) were detected in genome-wide and correlated to genes related to VRFs and/or other stroke subtypes. Rare aneuploidies, copy number variants (CNVs) and chromosomal structural rearrangements were also investigated. Lastly, candidate genes were used for pathway and gene ontology enrichment analysis.ResultsAmong 92 patients (mean age at stroke onset 61.0±9.3 years), GS identified likely ICAD-associated rare genomic variants in 54.3% (50/92) of patients. Forty-eight patients (52.2%, 48/92) had 59 rare SNVs/InDels reported or predicted to be deleterious in genes related to VRFs and/or other stroke subtypes. None of the 59 rare variants were identified in local subjects without ICAD (n=126). 31 SNVs/InDels were related to conventional VRFs, and 28 were discovered in genes related to other stroke subtypes. Our study also showed that rare CNVs (n=7) and structural rearrangement (a balanced translocation) were potentially related to ICAD in 8.7% (8/92) of patients. Lastly, candidate genes were significantly enriched in pathways related to lipoprotein metabolism and cellular lipid catabolic process.ConclusionsOur GS study suggests a role of rare genomic variants with various variant types contributing to the development of ICAD in Chinese patients.

Published

2021

50. Consensus interpretation of the p.Met34Thr and p.Val37Ile variants in GJB2 by the ClinGen Hearing Loss Expert Panel

Author

Kwong Wai Choy, Gema Garrido, Rebecca K. Siegert, Yoel Hirsch, Andrew R. Grant, Yu Lu, Alecia Willis, Hatice Duzkale, Lisa Schimmenti, Xue Zhong Liu, Krista Moyer, Hela Azaiez, Rebecca Mar-Heyming, Richard Smith, Narasimhan Nagan, Christine Lo, Xinhua Hu, Ahmad N. Abou Tayoun, Hyunseok Kang, Sarah E. Hemphill, Cynthia C. Morton, Yan Zhang, Yen-Fu Cheng, Huijun Yuan, Kevin T. Booth, Anne Giersch, Moshe Frydman, Tatsuo Matsunaga, Jun Shen, John H. Greinwald, Tzvi Weiden, Saurav Guha, Ye Cao, Hideki Mutai, Yukun Zeng, Arti Pandya, John J. Alexander, Lina Basel-Salmon, Marina T. DiStefano, Margaret A. Kenna, Zippora Brownstein, Ignacio del Castillo, Kejian Zhang, Bella Davidov, Sami S. Amr, Minjie Luo, Karen B. Avraham, Andrea M. Oza, Mustafa Tekin, Miguel A. Moreno-Pelayo, and Heidi L. Rehm

Subjects

ClinGen, Male, Hearing loss, Hearing Loss, Sensorineural, Population, Deafness, Compound heterozygosity, Polymorphism, Single Nucleotide, Article, Connexins, Statistical analyses, otorhinolaryngologic diseases, medicine, Humans, Allele, variant classification, Hearing Loss, education, Alleles, Genetics (clinical), Genetics, education.field_of_study, incomplete penetrance, business.industry, variant interpretation, Expert consensus, medicine.disease, Penetrance, Connexin 26, Case-Control Studies, Mutation, Female, Sensorineural hearing loss, medicine.symptom, business

Abstract

PURPOSE Pathogenic variants in GJB2 are the most common cause of autosomal recessive sensorineural hearing loss. The classification of c.101T>C/p.Met34Thr and c.109G>A/p.Val37Ile in GJB2 are controversial. Therefore, an expert consensus is required for the interpretation of these two variants. METHODS The ClinGen Hearing Loss Expert Panel collected published data and shared unpublished information from contributing laboratories and clinics regarding the two variants. Functional, computational, allelic, and segregation data were also obtained. Case-control statistical analyses were performed. RESULTS The panel reviewed the synthesized information, and classified the p.Met34Thr and p.Val37Ile variants utilizing professional variant interpretation guidelines and professional judgment. We found that p.Met34Thr and p.Val37Ile are significantly overrepresented in hearing loss patients, compared to population controls. Individuals homozygous or compound heterozygous for p.Met34Thr or p.Val37Ile typically manifest mild to moderate hearing loss. Several other types of evidence also support pathogenic roles for these two variants. CONCLUSION Resolving controversies in variant classification requires coordinated effort among a panel of international multi-institutional experts to share data, standardize classification guidelines, review evidence, and reach a consensus. We concluded that p.Met34Thr and p.Val37Ile variants in GJB2 are pathogenic for autosomal recessive nonsyndromic hearing loss with variable expressivity and incomplete penetrance.

Published

2019