Your search keyword '"Tang CSM"' showing total 16 results

1. HLA-B*38:02:01 predicts carbimazole/methimazole-induced agranulocytosis

Author

Cheung, C-L, Sing, C-W, Tang, CSM, Cheng, VKF, Pirmohamed, M, Choi, C-H, Hung, C-S, Lau, EY-F, Lee, KF, Mak, MW-H, Leung, JYY, Wong, T-W, Ho, AYY, Chan, K-W, Hung, VHF, Tam, V, Siu, S-C, Pang, H-K, Wat, WZ-M, Lee, HH-Y, Chung, C-T, Hue, RS-M, Sham, P-C, Cheung, BMY, Wong, ICK, Tan, KCB, and Kung, AWC

Published

2016

2. A complementary study approach unravels novel players in the pathoetiology of Hirschsprung disease

Author

Mederer, T, Schmitteckert, S, Volz, J, Martinez, C, Roth, R, Thumberger, T, Eckstein, V, Scheuerer, J, Thoni, C, Lasitschka, F, Carstensen, L, Gunther, P, Holland-Cunz, S, Hofstra, Robert, Brosens, Erwin, Rosenfeld, JA, Schaaf, CP, Schriemer, D, Ceccherini, I, Rusmini, M, Tilghman, J, Luzon-Toro, B, Torroglosa, A, Borrego, S, Tang, CSM, Garcia-Barcelo, M, Tam, P, Paramasivam, N, Bewerunge-Hudler, M, Dalla Torre, C, Gretz, N, Rappold, GA, Romero, P, Niesler, B, Mederer, T, Schmitteckert, S, Volz, J, Martinez, C, Roth, R, Thumberger, T, Eckstein, V, Scheuerer, J, Thoni, C, Lasitschka, F, Carstensen, L, Gunther, P, Holland-Cunz, S, Hofstra, Robert, Brosens, Erwin, Rosenfeld, JA, Schaaf, CP, Schriemer, D, Ceccherini, I, Rusmini, M, Tilghman, J, Luzon-Toro, B, Torroglosa, A, Borrego, S, Tang, CSM, Garcia-Barcelo, M, Tam, P, Paramasivam, N, Bewerunge-Hudler, M, Dalla Torre, C, Gretz, N, Rappold, GA, Romero, P, and Niesler, B

Published

2020

3. Whole exome sequencing coupled with unbiased functional analysis reveals new Hirschsprung disease genes

Author

Gui, HS, Schriemer, D, Cheng, Wai, Chauhan, Rajendra, Antinolo, G, Berrios, C, Bleda, M, Brooks, Alice, Brouwer, Rutger, Burns, Alan, Cherny, SS, Dopazo, J, Eggen, BJL, Griseri, P, Jalloh, B, Le, TL, Lui, VCH, Luzon-Toro, B, Matera, I, Ngan, ESW, Pelet, A, Ruiz-Ferrer, M, Sham, PC, Shepherd, IT, So, MT, Sribudiani, Yunia, Tang, CSM, Van den Hout - van Vroonhoven, Mirjam, Zondervan - van der Linde, Herma, van Ham, Tjakko, van Ijcken, Wilfred, Verheij, J, Amiel, J, Borrego, S, Ceccherini, I, Chakravarti, A, Lyonnet, S, Tam, PKH, Garcia-Barcelo, MM, Hofstra, Robert, Gui, HS, Schriemer, D, Cheng, Wai, Chauhan, Rajendra, Antinolo, G, Berrios, C, Bleda, M, Brooks, Alice, Brouwer, Rutger, Burns, Alan, Cherny, SS, Dopazo, J, Eggen, BJL, Griseri, P, Jalloh, B, Le, TL, Lui, VCH, Luzon-Toro, B, Matera, I, Ngan, ESW, Pelet, A, Ruiz-Ferrer, M, Sham, PC, Shepherd, IT, So, MT, Sribudiani, Yunia, Tang, CSM, Van den Hout - van Vroonhoven, Mirjam, Zondervan - van der Linde, Herma, van Ham, Tjakko, van Ijcken, Wilfred, Verheij, J, Amiel, J, Borrego, S, Ceccherini, I, Chakravarti, A, Lyonnet, S, Tam, PKH, Garcia-Barcelo, MM, and Hofstra, Robert

Published

2017

4. A Structural Split in the Human Genome

Author

Tang, CSM, Epstein, RJ, Tang, CSM, and Epstein, RJ

Abstract

Background: Promoter-associated CpG islands (PCIs) mediate methylation-dependent gene silencing, yet tend to co-locate to transcriptionally active genes. To address this paradox, we used data mining to assess the behavior of PCI-positive (PCI+) genes in the human genome. Results: PCI+ genes exhibit a bimodal distribution: (1) a 'housekeeping-like' subset characterized by higher GC content and lower intron length/number, and (2) a 'pseudogene paralog' subset characterized by lower GC content and higher intron length/number (p<0.001). These subsets are functionally distinguishable, with the former gene group characterized by higher expression levels and lower evolutionary rate (p<0.001). PCI-negative (PCI-) genes exhibit higher evolutionary rate and narrower expression breadth than PCI+ genes (p<0.001), consistent with more frequent tissue-specific inactivation. Conclusions: Adaptive evolution of the human genome appears driven in part by declining transcription of a subset of PCI+ genes, predisposing to both CpG→TpA mutation and intron insertion. We propose a model of evolving biological complexity in which environmentally-selected gains or losses of PCI methylation respectively favor positive or negative selection, thus polarizing PCI+ gene structures around a genomic core of ancestral PCI- genes. © 2007 Tang, Epstein.

Published

2007

5. A narrative review of genes associated with liver fibrosis in biliary atresia.

Author

Liu F, Tang CSM, and Chung PHY

Abstract

Background and Objective: Biliary atresia (BA) is characterized by biliary inflammation and obstruction. In the later phase, liver fibrosis occurs. Although the etiology of BA is believed to be multi-factorial, genetic predisposition has been proposed to play a critical role in the pathogenesis. This review aimed to provide an updated summary of the genes that have been reported to be involved in BA-associated liver fibrosis., Methods: The review was conducted via evaluation of MalaCards (BA disease: MalaCards-research articles, drugs, genes, clinical trials) which is a universally applied website including various human disease database. The database of genes that are involved in liver fibrosis were studied., Key Content and Findings: Thirty-one genes that are associated with BA according to the disease relevance score were reviewed after further evaluations. Eleven genes ( GPT, NR1H4, TGF-B1, MMP7, CCN2, TIMP1, SPP1, ADD3, KRT7, ADD3-AS1, SOX9 ) that are specific and with a potential association with liver fibrosis were selected for detailed description. Increased expression of GPT , TGF-B1 , MMP7 , CCN2 , TIMP1 , SPP1 , ADD3 , KRT7 and ADD3-AS1 maybe associated with the development of liver fibrosis in BA patients, while the expression of NR1H4 and SOX9 are more likely to suppress liver fibrosis., Conclusions: Current scientific evidence using gene database has revealed a close association between genetic anomalies and the pathogenesis of liver fibrosis in BA. With a better understanding of these anomalies, therapy targeting these related genes may be a new therapeutic approach to alleviate liver fibrosis in BA., Competing Interests: Conflicts of Interest: All authors have completed the ICMJE uniform disclosure form (available at https://tp.amegroups.com/article/view/10.21037/tp-24-94/coif). P.H.Y.C. serves as an unpaid editorial board member of Translational Pediatrics from August 2022 to July 2024. The other authors have no conflicts of interest to declare., (2024 Translational Pediatrics. All rights reserved.)

Published

2024

6. Human Liver Organoids to Predict the Outcome of Kasai Portoenterostomy.

Author

Wai AWY, Lui VCH, Tang CSM, Wang B, Tam PKH, Wong KKY, and Chung PHY

Abstract

Background: Kasai portoenterostomy (KPE) remains the primary intervention for biliary atresia (BA), but its outcomes are highly variable. Reliable prognostic biomarkers remain elusive, complicating the management and prediction of postoperative progression., Method: Liver biopsies from BA patients taken at and after KPE (post-KPE) were used to generate organoids for RNA-sequencing analysis. Control organoids were derived from non-BA livers. Differential gene expression and enrichment analyses were performed to assess post-KPE transcriptomic changes between native liver survivors (NLS) and patients who eventually became liver transplant recipients (LTR)., Results: Organoid datasets: 70 from liver biopsies at KPE (10 patients), 112 from post-KPE livers (13 livers; 12 patients), and 47 from control livers (9 patients). At KPE, BA organoids displayed mainly hepatocyte expression, a trait notably reduced in control organoids. Similarly, post-KPE organoids from NLS revealed a significant decrease in hepatocyte expression features and an overall increase in cholangiocyte expression features. A similar hepatocyte-to-cholangiocyte expression transition was evidenced in paired liver organoids (at- and post-KPE) generated from an NLS. In contrast, post-KPE organoids from LTR maintained a high level of hepatocyte expression features., Conclusion: Our study demonstrated that an elevated expression of hepatocyte features in KPE organoids may indicate aberrant cholangiocyte development in BA livers. In contrast, a post-KPE hepatocyte-to-cholangiocyte expression transition in NLS may imply effective biliary recovery. The lack of this transition in LTR organoids indicates ongoing disease progression, highlighting the potential for organoid-based transcriptomic profiling to inform KPE success and guide BA management., Level of Evidence: Level III., Competing Interests: Conflicts of interest None., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

7. Animal and organoid models to elucidate the anti-fibrotic effect of steroid on biliary atresia.

Author

Liu F, Lui VCH, Wu Z, Blakeley PD, Tang CSM, Tam PKH, Wong KKY, and Chung PHY

Subjects

Animals, Mice, Liver pathology, Liver drug effects, Biliary Atresia, Disease Models, Animal, Organoids drug effects, Liver Cirrhosis drug therapy, Liver Cirrhosis pathology

Abstract

Purpose: We performed animal and organoid study to evaluate the anti-fibrotic effect of steroid on biliary atresia (BA) and the underlying patho-mechanism., Methods: BA animal models were created by inoculation of mice on post-natal day 1 with rhesus rotavirus (RRV). They received either 20 µl phosphate-buffered saline (PBS) or steroid from day 21 to day 34. On day 34, their serum samples were collected for hormonal markers. Necrosis, fibrosis and CK 19 expression in the liver were evaluated. Liver organoids were developed and their morphology as well as bulk RNA sequencing data were analyzed., Results: Twenty-four mice developed BA features after RRV injection and were equally divided into steroid and PBS groups. On day 34, the weight gain of steroid group increased significantly than PBS group (p < 0.0001). All mice in the PBS group developed liver fibrosis but only one mouse in the steroid group did. Serum bilirubin and liver parenchymal enzymes were significantly lower in steroid group. The morphology of liver organoids were different between the two groups. A total of 6359 differentially expressed genes were found between steroid group and PBS group., Conclusion: Based on our findings obtained from RRV-induced BA animal and organoid models, steroid has the potential to mitigate liver fibrosis in BA., (© 2024. The Author(s).)

Published

2024

8. Biliary atresia.

Author

Tam PKH, Wells RG, Tang CSM, Lui VCH, Hukkinen M, Luque CD, De Coppi P, Mack CL, Pakarinen M, and Davenport M

Subjects

Humans, Portoenterostomy, Hepatic methods, Liver Transplantation methods, Liver Transplantation statistics & numerical data, Biliary Atresia physiopathology, Biliary Atresia diagnosis, Biliary Atresia therapy, Biliary Atresia epidemiology, Biliary Atresia complications

Abstract

Biliary atresia (BA) is a progressive inflammatory fibrosclerosing disease of the biliary system and a major cause of neonatal cholestasis. It affects 1:5,000-20,000 live births, with the highest incidence in Asia. The pathogenesis is still unknown, but emerging research suggests a role for ciliary dysfunction, redox stress and hypoxia. The study of the underlying mechanisms can be conceptualized along the likely prenatal timing of an initial insult and the distinction between the injury and prenatal and postnatal responses to injury. Although still speculative, these emerging concepts, new diagnostic tools and early diagnosis might enable neoadjuvant therapy (possibly aimed at oxidative stress) before a Kasai portoenterostomy (KPE). This is particularly important, as timely KPE restores bile flow in only 50-75% of patients of whom many subsequently develop cholangitis, portal hypertension and progressive fibrosis; 60-75% of patients require liver transplantation by the age of 18 years. Early diagnosis, multidisciplinary management, centralization of surgery and optimized interventions for complications after KPE lead to better survival. Postoperative corticosteroid use has shown benefits, whereas the role of other adjuvant therapies remains to be evaluated. Continued research to better understand disease mechanisms is necessary to develop innovative treatments, including adjuvant therapies targeting the immune response, regenerative medicine approaches and new clinical tests to improve patient outcomes., (© 2024. Springer Nature Limited.)

Published

2024

9. Assessing the safety of lipid-modifying medications among Chinese adolescents: a drug-target Mendelian randomization study.

Author

Luo S, Lam HS, Chan YH, Tang CSM, He B, Kwok MK, Leung GM, Schooling CM, and Au Yeung SL

Subjects

Child, Humans, Adolescent, Aged, Proprotein Convertase 9, PCSK9 Inhibitors, Mendelian Randomization Analysis, East Asian People, Cholesterol, LDL, Hydroxymethylglutaryl-CoA Reductase Inhibitors adverse effects

Abstract

Background: With increasing hypercholesterolemia prevalence in East Asian adolescents, pharmacologic interventions (e.g., HMGCR inhibitors (statins) and PCSK9 inhibitors) may have to be considered although their longer-term safety in the general adolescent population is unclear. This study aims to investigate the longer-term safety of HMGCR inhibitors and PCSK9 inhibitors among East Asian adolescents using genetics., Methods: A drug-target Mendelian randomization study leveraging the Global Lipid Genetics Consortium (East Asian, n = 146,492) and individual-level data from Chinese participants in the Biobank clinical follow-up of Hong Kong's "Children of 1997" birth cohort (n = 3443, aged ~ 17.6 years). Safety outcomes (n = 100) included anthropometric and hematological traits, renal, liver, lung function, and other nuclear magnetic resonance metabolomics. Positive control outcomes were cholesterol markers from the "Children of 1997" birth cohort and coronary artery disease from Biobank Japan., Results: Genetic inhibition of HMGCR and PCSK9 were associated with reduction in cholesterol-related NMR metabolomics, e.g., apolipoprotein B (HMGCR: beta [95% CI], - 1.06 [- 1.52 to - 0.60]; PCSK9: - 0.93 [- 1.56 to - 0.31]) and had the expected effect on the positive control outcomes. After correcting for multiple comparisons (p-value < 0.006), genetic inhibition of HMGCR was associated with lower linoleic acid - 0.79 [- 1.25 to - 0.35]. Genetic inhibition of PCSK9 was not associated with the safety outcomes assessed., Conclusions: Statins and PCSK9 inhibitors in East Asian adolescents appeared to be safe based on the outcomes concerned. Larger studies were warranted to verify these findings. This study serves as a proof of principle study to inform the medication safety among adolescents via genetics., (© 2023. The Author(s).)

Published

2023

10. Current Understanding in the Clinical Characteristics and Molecular Mechanisms in Different Subtypes of Biliary Atresia.

Author

He L, Chung PHY, Lui VCH, Tang CSM, and Tam PKH

Subjects

Child, Humans, Infant, Portoenterostomy, Hepatic adverse effects, Biliary Atresia, Liver Transplantation adverse effects

Abstract

Biliary atresia is a severe obliterative cholangiopathy in early infancy that is by far the most common cause of surgical jaundice and the most common indicator for liver transplantation in children. With the advanced knowledge gained from different clinical trials and the development of research models, a more precise clinical classification of BA (i.e., isolated BA (IBA), cystic BA (CBA), syndromic BA (SBA), and cytomegalovirus-associated BA (CMVBA)) is proposed. Different BA subtypes have similar yet distinguishable clinical manifestations. The clinical and etiological heterogeneity leads to dramatically different prognoses; hence, treatment needs to be specific. In this study, we reviewed the clinical characteristics of different BA subtypes and revealed the molecular mechanisms of their developmental contributors. We aimed to highlight the differences among these various subtypes of BA which ultimately contribute to the development of a specific management protocol for each subtype.

Published

2022

11. Comprehensive analysis of recessive carrier status using exome and genome sequencing data in 1543 Southern Chinese.

Author

Chau JFT, Yu MHC, Chui MMC, Yeung CCW, Kwok AWC, Zhuang X, Lee R, Fung JLF, Lee M, Mak CCY, Ng NYT, Chung CCY, Chan MCY, Tsang MHY, Chan JCK, Chan KYK, Kan ASY, Chung PHY, Yang W, Lee SL, Chan GCF, Tam PKH, Lau YL, Yeung KS, Chung BHY, and Tang CSM

Abstract

Traditional carrier screening has been utilized for the detection of carriers of genetic disorders. Since a comprehensive assessment of the carrier frequencies of recessive conditions in the Southern Chinese population is not yet available, we performed a secondary analysis on the spectrum and carrier status for 315 genes causing autosomal recessive disorders in 1543 Southern Chinese individuals with next-generation sequencing data, 1116 with exome sequencing and 427 with genome sequencing data. Our data revealed that 1 in 2 people (47.8% of the population) was a carrier for one or more recessive conditions, and 1 in 12 individuals (8.30% of the population) was a carrier for treatable inherited conditions. In alignment with current American College of Obstetricians and Gynecologists (ACOG) pan-ethnic carrier recommendations, 1 in 26 individuals were identified as carriers of cystic fibrosis, thalassemia, and spinal muscular atrophy in the Southern Chinese population. When the >1% expanded carrier screening rate recommendation by ACOG was used, 11 diseases were found to meet the criteria in the Southern Chinese population. Approximately 1 in 3 individuals (35.5% of the population) were carriers of these 11 conditions. If the 1 in 200 carrier frequency threshold is used, and additional seven genes would meet the criteria, and 2 in 5 individuals (38.7% of the population) would be detected as a carrier. This study provides a comprehensive catalogue of the carrier spectrum and frequency in the Southern Chinese population and can serve as a reference for careful evaluation of the conditions to be included in expanded carrier screening for Southern Chinese people., (© 2022. The Author(s).)

Published

2022

12. Sequencing of a Chinese tetralogy of Fallot cohort reveals clustering mutations in myogenic heart progenitors.

Author

Tang CSM, Mononen M, Lam WY, Jin SC, Zhuang X, Garcia-Barcelo MM, Lin Q, Yang Y, Sahara M, Eroglu E, Chien KR, Hong H, Tam PKH, and Gruber PJ

Subjects

Asian People genetics, China epidemiology, Cluster Analysis, Gene Regulatory Networks genetics, Genetic Association Studies methods, Genetic Variation, Humans, Myocytes, Cardiac physiology, Polymorphism, Single Nucleotide, Whole Genome Sequencing methods, Embryonic Induction genetics, Heart embryology, Tetralogy of Fallot ethnology, Tetralogy of Fallot genetics

Abstract

Tetralogy of Fallot (TOF) is the most common cyanotic heart defect, yet the underlying genetic mechanisms remain poorly understood. Here, we performed whole-genome sequencing analysis on 146 nonsyndromic TOF parent-offspring trios of Chinese ethnicity. Comparison of de novo variants and recessive genotypes of this data set with data from a European cohort identified both overlapping and potentially novel gene loci and revealed differential functional enrichment between cohorts. To assess the impact of these mutations on early cardiac development, we integrated single-cell and spatial transcriptomics of early human heart development with our genetic findings. We discovered that the candidate gene expression was enriched in the myogenic progenitors of the cardiac outflow tract. Moreover, subsets of the candidate genes were found in specific gene coexpression modules along the cardiomyocyte differentiation trajectory. These integrative functional analyses help dissect the pathogenesis of TOF, revealing cellular hotspots in early heart development resulting in cardiac malformations.

Published

2022

13. Actionable secondary findings in 1116 Hong Kong Chinese based on exome sequencing data.

Author

Yu MHC, Mak CCY, Fung JLF, Lee M, Tsang MHY, Chau JFT, Chung PH, Yang W, Chan GCF, Lee SL, Lau YL, Tam PKH, Tang CSM, Yeung KS, and Chung BHY

Subjects

Adolescent, Adult, Alleles, Child, China epidemiology, Exome, Female, Genetic Variation genetics, Genome, Human genetics, Hong Kong epidemiology, Humans, Incidental Findings, Male, Middle Aged, Mutation genetics, Young Adult, Genetic Predisposition to Disease, Genetic Testing, Genomics, Exome Sequencing

Abstract

The use of exome and genome sequencing has increased rapidly nowadays. After primary analysis, further analysis can be performed to identify secondary findings that offer medical benefit for patient care. Multiple studies have been performed to evaluate secondary findings in different ethnicities. However, relevant data are limited in Chinese. Here, with the use of a cohort consisted of 1116 Hong Kong Chinese exome sequencing data, we evaluated the secondary findings in the 59 genes recommended by the American College of Medical Genetics and Genomics. Fifteen unique pathogenic or likely pathogenic variants in 17 individuals were identified, representing a frequency of 1.52% in our cohort. Although 20 individuals harboured pathogenic or likely pathogenic variants in recessive conditions, none carried bi-allelic mutations in the same gene. Our finding was in accordance with the estimation from the American College of Medical Genetics and Genomics that about 1% individuals harbour secondary findings.

Published

2021

14. Actionable pharmacogenetic variants in Hong Kong Chinese exome sequencing data and projected prescription impact in the Hong Kong population.

Author

Yu MHC, Chan MCY, Chung CCY, Li AWT, Yip CYW, Mak CCY, Chau JFT, Lee M, Fung JLF, Tsang MHY, Chan JCK, Wong WHS, Yang J, Chui WCM, Chung PHY, Yang W, Lee SL, Chan GCF, Tam PKH, Lau YL, Tang CSM, Yeung KS, and Chung BHY

Subjects

Alleles, Asian People genetics, Cohort Studies, Gene Frequency, Genotype, Hong Kong, Humans, Pharmacogenetics statistics & numerical data, Pharmacogenomic Testing methods, Pharmacogenomic Testing statistics & numerical data, Phenotype, Reproducibility of Results, Pharmacogenetics methods, Pharmacogenomic Variants genetics, Prescriptions statistics & numerical data, Exome Sequencing methods

Abstract

Preemptive pharmacogenetic testing has the potential to improve drug dosing by providing point-of-care patient genotype information. Nonetheless, its implementation in the Chinese population is limited by the lack of population-wide data. In this study, secondary analysis of exome sequencing data was conducted to study pharmacogenomics in 1116 Hong Kong Chinese. We aimed to identify the spectrum of actionable pharmacogenetic variants and rare, predicted deleterious variants that are potentially actionable in Hong Kong Chinese, and to estimate the proportion of dispensed drugs that may potentially benefit from genotype-guided prescription. The projected preemptive pharmacogenetic testing prescription impact was evaluated based on the patient prescription data of the public healthcare system in 2019, serving 7.5 million people. Twenty-nine actionable pharmacogenetic variants/ alleles were identified in our cohort. Nearly all (99.6%) subjects carried at least one actionable pharmacogenetic variant, whereas 93.5% of subjects harbored at least one rare deleterious pharmacogenetic variant. Based on the prescription data in 2019, 13.4% of the Hong Kong population was prescribed with drugs with pharmacogenetic clinical practice guideline recommendations. The total expenditure on actionable drugs was 33,520,000 USD, and it was estimated that 8,219,000 USD (24.5%) worth of drugs were prescribed to patients with an implicated actionable phenotype. Secondary use of exome sequencing data for pharmacogenetic analysis is feasible, and preemptive pharmacogenetic testing has the potential to support prescription decisions in the Hong Kong Chinese population., Competing Interests: The authors have declared that no competing interests exist.

Published

2021

15. Cancer gene mutations in congenital pulmonary airway malformation patients.

Author

Hsu JS, Zhang R, Yeung F, Tang CSM, Wong JKL, So MT, Xia H, Sham P, Tam PK, Li M, Wong KKY, and Garcia-Barcelo MM

Abstract

Background: Newborns affected with congenital pulmonary airway malformations (CPAMs) may present with severe respiratory distress or remain asymptomatic. While surgical resection is the definitive treatment for symptomatic CPAMs, prophylactic elective surgery may be recommended for asymptomatic CPAMs owing to the risk of tumour development. However, the implementation of prophylactic surgery is quite controversial on the grounds that more evidence linking CPAMs and cancer is needed. The large gap in knowledge of CPAM pathogenesis results in uncertainties and controversies in disease management. As developmental genes control postnatal cell growth and contribute to cancer development, we hypothesised that CPAMs may be underlain by germline mutations in genes governing airways development., Methods: Sequencing of the exome of 19 patients and their unaffected parents., Results: A more than expected number of mutations in cancer genes (false discovery rate q-value <5.01×10 -5 ) was observed. The co-occurrence, in the same patient, of damaging variants in genes encoding interacting proteins is intriguing, the most striking being thyroglobulin ( TG ) and its receptor, megalin ( LRP2 ). Both genes are highly relevant in lung development and cancer., Conclusions: The overall excess of mutations in cancer genes may account for the reported association of CPAMs with carcinomas and provide some evidence to argue for prophylactic surgery by some surgeons., Competing Interests: Conflict of interest: J.S. Hsu has nothing to disclose. Conflict of interest: R. Zhang has nothing to disclose. Conflict of interest: F. Yeung has nothing to disclose. Conflict of interest: C.S.M. Tang has nothing to disclose. Conflict of interest: K.K.Y. Wong has nothing to disclose. Conflict of interest: M-T. So has nothing to disclose. Conflict of interest: H. Xia has nothing to disclose. Conflict of interest: P. Sham has nothing to disclose. Conflict of interest: P.K. Tam has nothing to disclose. Conflict of interest: M. Li has nothing to disclose. Conflict of interest: J.K.L. Wong has nothing to disclose. Conflict of interest: M-M. Garcia-Barcelo has nothing to disclose.

Published

2019

16. De novo mutations in Caudal Type Homeo Box transcription Factor 2 (CDX2) in patients with persistent cloaca.

Author

Hsu JSJ, So M, Tang CSM, Karim A, Porsch RM, Wong C, Yu M, Yeung F, Xia H, Zhang R, Cherny SS, Chung PHY, Wong KKY, Sham PC, Ngo ND, Li M, Tam PKH, Lui VCH, and Garcia-Barcelo MM

Subjects

Asian People genetics, Cell Differentiation genetics, Cloaca embryology, DNA Copy Number Variations, Family, Female, Homeodomain Proteins genetics, Humans, Male, Mutation, Phenotype, Urogenital Abnormalities metabolism, Exome Sequencing, CDX2 Transcription Factor genetics, CDX2 Transcription Factor metabolism, Urogenital Abnormalities genetics

Abstract

The cloaca is an embryonic cavity that is divided into the urogenital sinus and rectum upon differentiation of the cloacal epithelium triggered by tissue-specific transcription factors including CDX2. Defective differentiation leads to persistent cloaca in humans (PC), a phenotype recapitulated in Cdx2 mutant mice. PC is linked to hypo/hyper-vitaminosis A. Although no gene has ever been identified, there is a strong evidence for a genetic contribution to PC. We applied whole-exome sequencing and copy-number-variants analyses to 21 PC patients and their unaffected parents. The damaging p.Cys132* and p.Arg237His de novo CDX2 variants were identified in two patients. These variants altered the expression of CYP26A1, a direct CDX2 target encoding the major retinoic acid (RA)-degrading enzyme. Other RA genes, including the RA-receptor alpha, were also mutated. Genes governing the development of cloaca-derived structures were recurrently mutated and over-represented in the basement-membrane components set (q-value < 1.65 × 10-6). Joint analysis of the patients' profile highlighted the extracellular matrix-receptor interaction pathway (MsigDBID: M7098, FDR: q-value < 7.16 × 10-9). This is the first evidence that PC is genetic, with genes involved in the RA metabolism at the lead. Given the CDX2 de novo variants and the role of RA, our observations could potentiate preventive measures. For the first time, a gene recapitulating PC in mouse models is found mutated in humans., (© The Author(s) 2017. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2018