Your search keyword '"Ruby, Jiang"' showing total 11 results

1. Assessing the role of placental trisomy in preeclampsia and intrauterine growth restriction

Author

Jennifer Sloan, Deborah E. McFadden, Peter von Dadelszen, Wendy P. Robinson, Maria S. Peñaherrera, Sylvie Langlois, Ruby Jiang, and Luana Avila

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Aneuploidy, Intrauterine growth restriction, Biology, Preeclampsia, 03 medical and health sciences, 0302 clinical medicine, Placenta, medicine, Neonatology, reproductive and urinary physiology, Genetics (clinical), 030304 developmental biology, Gynecology, 0303 health sciences, Pregnancy, 030219 obstetrics & reproductive medicine, Obstetrics, Obstetrics and Gynecology, medicine.disease, female genital diseases and pregnancy complications, 3. Good health, medicine.anatomical_structure, embryonic structures, Trisomy, Comparative genomic hybridization

Abstract

Objective Prenatally diagnosed confined placental trisomy is associated with increased risk for intrauterine growth restriction (IUGR) and preeclampsia. However, it is unclear how often this might underlie pregnancy complications. Our objective was to evaluate the frequency and distribution of trisomic cells in placentae ascertained for IUGR and/or preeclampsia. Method Comparative genomic hybridization was applied to two uncultured biopsies from each of 61 placentae referred with maternal preeclampsia and/or IUGR, 11 cases with elevated maternal serum hCG and/or AFP but no IUGR or preeclampsia, and 85 control placentae. Results Trisomy was observed in four placentae among the IUGR group (N = 43) but in no case of preeclampsia in the absence of IUGR (N = 18). Trisomy was observed in 1 of the 11 cases ascertained for abnormal maternal serum screen. Each of these five cases was mosaic and not all sampled sites showed the presence of trisomy. None of the 84 control placentas showed mosaic trisomy, although 1 case of nonmosaic 47,XXX was identified in this group. Conclusion In cases in which diagnosis of the cause of IUGR may provide some benefit, testing should be performed using uncultured cells from multiple placental biopsies for the accurate diagnosis of trisomy mosaicism. Copyright © 2009 John Wiley & Sons, Ltd.

Published

2009

2. MECP2promoter methylation and X chromosome inactivation in autism

Author

Ruby Jiang, Robin L Hansen, Judith A Van de Water, Isaac N. Pessah, Wendy P. Robinson, Katherine A. Patzel, Michelle R. Martin, Janine M. LaSalle, Susan E. Swanberg, Raman P. Nagarajan, Irva Hertz-Picciotto, and Dag H. Yasui

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Methyl-CpG-Binding Protein 2, Bisulfite sequencing, Epigenetics of autism, Biology, Methylation, Article, X-inactivation, MECP2, X Chromosome Inactivation, mental disorders, medicine, Humans, Epigenetics, Autistic Disorder, Genetics (clinical), DNA Primers, Genetics, Chromosomes, Human, X, Polymorphism, Genetic, General Neuroscience, Brain, medicine.disease, Molecular biology, Child, Preschool, DNA methylation, Autism, Neurology (clinical)

Abstract

Epigenetic mechanisms have been proposed to play a role in the etiology of autism. This hypothesis is supported by the discovery of increased MECP2 promoter methylation associated with decreased MeCP2 protein expression in autism male brain. To further understand the influence of female X chromosome inactivation (XCI) and neighboring methylation patterns on aberrant MECP2 promoter methylation in autism, multiple methylation analyses were peformed on brain and blood samples from individuals with autism. Bisulfite sequencing analyses of a region 0.6 kb upstream of MECP2 in brain DNA samples revealed an abrupt transition from a highly methylated region in both sexes to a region unmethylated in males and subject to XCI in females. Chromatin immunoprecipitation analysis demonstrated that the CCTC-binding factor (CTCF) bound to this transition region in neuronal cells, consistent with a chromatin boundary at the methylation transition. Male autism brain DNA samples displayed a slight increase in methylation in this transition region, suggesting a possible aberrant spreading of methylation into the MECP2 promoter in autism males across this boundary element. In addition, autistic female brain DNA samples showed evidence for aberrant MECP2 promoter methylation as an increase in the number of bisulfite sequenced clones with undefined XCI status for MECP2 but not androgen receptor (AR). To further investigate the specificity of MECP2 methylation alterations in autism, blood DNA samples from females and mothers of males with autism were also examined for XCI skewing at AR, but no significant increase in XCI skewing was observed compared to controls. These results suggest that the aberrant MECP2 methylation in autism brain DNA samples is due to locus-specific rather than global X chromosome methylation changes.

Published

2008

3. Toll-like receptor 4 polymorphisms and idiopathic chromosomally normal miscarriage

Author

Wendy P. Robinson, Aaron F. Hirschfeld, Ruby Jiang, Stuart E. Turvey, and Deborah E. McFadden

Subjects

medicine.medical_specialty, Candidate gene, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Miscarriage, Pregnancy, Internal medicine, Genotype, medicine, Humans, Amnion, Allele frequency, Fetus, Rehabilitation, Infant, Newborn, Obstetrics and Gynecology, DNA, medicine.disease, Genotype frequency, Abortion, Spontaneous, Toll-Like Receptor 4, Endocrinology, Amino Acid Substitution, Reproductive Medicine, Case-Control Studies, Aborted Fetus, Immunology, TLR4, Female, lipids (amino acids, peptides, and proteins), Chorionic Villi

Abstract

BACKGROUND: Lipopolysaccharide (LPS or endotoxin) exposure resulting from microbial invasion of the endometrium disturbs the Thl/Th2 balance at the feto-maternal interface and has been linked to the risk of idiopathic miscarriage in a range of human and animal studies. Toll-like receptor 4 (TLR4) mediates LPS signalling, and the human TLR4 gene harbours two single-nucleotide polymorphisms (SNPs) known to reduce LPS responsiveness. We hypothesized that genetic variation altering TLR4 function may influence the risk of idiopathic pregnancy loss. METHODS AND RESULTS: We examined fetal TLR4 genotypes in a case-control cohort of chromosomally normal miscarriages (n = 96) and healthy term newborns (n = 113). The allele frequencies of the Asp299Gly and Thr399Ile TLR4 SNPs were determined by quantitative PCR using DNA extracted from extraembryonic tissues and umbilical cord blood, respectively. TLR4 genotype frequencies were not significantly different between cases and controls. CONCLUSIONS: There was no association between fetal TLR4 polymorphisms, Asp299Gly and Thr399Ile, known to blunt LPS responsiveness, and the risk of idiopathic, chromosomally normal miscarriage. Nevertheless, TLR4 or perhaps other LPS-binding chaperone molecules are biologically plausible candidate genes that may alter the risk of idiopathic miscarriage.

Published

2006

4. Androgenetic/biparental mosaicism causes placental mesenchymal dysplasia

Author

Chad A. Livasy, Kathleen W. Rao, Kathleen Kaiser-Rogers, Louis Lefebvre, Ruby Jiang, Jerome Dansereau, Wendy P. Robinson, Deborah E. McFadden, and Judith Knops

Subjects

medicine.medical_specialty, Fetus, Intrauterine growth restriction, Trophoblast, Karyotype, Biology, medicine.disease, Placental Mesenchymal Dysplasia, Andrology, medicine.anatomical_structure, Endocrinology, Uniparental Isodisomy, Dysplasia, Internal medicine, Placenta, Genetics, medicine, Letter to JMG, Genetics (clinical)

Abstract

Background: Placental mesenchymal dysplasia (PMD) is a distinct syndrome of unknown aetiology that is associated with significant fetal morbidity and mortality. Intrauterine growth restriction is common, yet, paradoxically, many of the associated fetuses/newborns have been diagnosed with Beckwith-Wiedemann syndrome (BWS). Methods: We report two cases of PMD with high levels of androgenetic (complete paternal uniparental isodisomy) cells in the placenta and document, in one case, a likely androgenetic contribution to the fetus as well. Results: The same haploid paternal complement found in the androgenetic cells was present in coexisting biparental cells, suggesting origin from a single fertilisation event. Conclusions: Preferential allocation of the normal cells into the trophoblast explains the absence of trophoblast overgrowth, a key feature of this syndrome. Interestingly, the distribution of androgenetic cells appears to differ from that reported for artificially created androgenetic mouse chimeras. Androgenetic mosaicism for the first time provides an aetiology for PMD, and may be a novel mechanism for BWS and unexplained intrauterine growth restriction.

Published

2005

5. Methylation ofZNF261as an assay for determining X chromosome inactivation patterns

Author

Maria S. Peñaherrera, Ruby Jiang, Carolyn J. Brown, C. L. Beever, Sarah E. L. Baldry, Betty P.Y. Lai, and Wendy P. Robinson

Subjects

Genetics, 0303 health sciences, Methylation, Biology, Molecular biology, X-inactivation, 03 medical and health sciences, 0302 clinical medicine, Restriction fragment length polymorphism, 030217 neurology & neurosurgery, Genetics (clinical), X chromosome, 030304 developmental biology

Published

2003

6. Patterns of placental development evaluated by X chromosome inactivation profiling provide a basis to evaluate the origin of epigenetic variation

Author

Ruby Jiang, Luana Avila, Ryan K. C. Yuen, Maria S. Peñaherrera, Carolyn J. Brown, and Wendy P. Robinson

Subjects

placenta, Chorionic villus sampling, Biology, X-inactivation, Epigenesis, Genetic, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, X Chromosome Inactivation, medicine, Humans, Epigenetics, X chromosome, reproductive and urinary physiology, 030304 developmental biology, Genetics, 0303 health sciences, Reproductive Biology, 030219 obstetrics & reproductive medicine, DNA methylation, medicine.diagnostic_test, epigenetics, Rehabilitation, Infant, Newborn, Obstetrics and Gynecology, Placentation, Trophoblast, Genetic Variation, Original Articles, medicine.anatomical_structure, Reproductive Medicine, Chorionic Villi Sampling, embryonic structures, Chorionic villi, Female

Abstract

background: Inactivation of the maternally or paternally derived X chromosome (XCI) initially occurs in a random manner in early development; however as tissues form, a ‘patchiness’ will occur in terms of which X is inactivated if cells positioned near each other are clonally descended from a common precursor. Determining the relationship between skewed XCI in different tissues and in different samples from the same tissue provides a molecular assessment of the developmental history of a particular tissue that can then be used to understand how genetic and epigenetic variation arises in development. methods: XCI skewing was evaluated in and compared between amnion, chorion, trophoblast and mesenchyme using multiple sampling sites from 14 term placentae. XCI was also evaluated in chorionic villus samples obtained at multiple sites and depths from four additional term placentae. The pattern of variation was then compared with methylation variation associated with the H19/IGF2 imprinting control region (ICR); promoter regions of KISS1, PTPN6, CASP8 and APC; and LINE-1 elements. results: Mean placental level of skewing for amnion and chorion are correlated, consistent with a common developmental origin of at least a component of these membranes from inner cell mass derivatives subsequent to XCI, while trophoblast appears to be derived independently, consistent with its origin from the trophectoderm. Villus samples taken from different depths spanning the fetal to maternal side of the placenta were highly clonally related. Comparing patterns of clonal growth identified through XCI to the distribution of epigenetic variation in other genomic regions suggests that some variation arises early in development (e.g. LINE-1 methylation), whereas other variation arises predominantly after villus tree formation (e.g. methylation at H19/IGF2 ICR). conclusions: The patterns of XCI skewing are consistent with a model whereby each biopsied site of chorionic villi represents one or a few individual villus trees, each of which is clonally derived from only one or a few precursor cells. Sampling of placentae to evaluate changes associated with clinical pathology should be done with consideration of the tree-to-tree differences. A limitation of this study is the small number of placentas used and therefore placental-specific differences in variation could not be assessed.

Published

2012

7. Genome-wide mapping of imprinted differentially methylated regions by DNA methylation profiling of human placentas from triploidies

Author

Ruby Jiang, Maria S. Peñaherrera, Deborah E. McFadden, Ryan K. C. Yuen, and Wendy P. Robinson

Subjects

Genetics, 0303 health sciences, Epigenetic Process, lcsh:QH426-470, Methodology, Biology, Genome, Human genetics, 03 medical and health sciences, lcsh:Genetics, 0302 clinical medicine, Differentially methylated regions, Imprinting (psychology), Allele, Genomic imprinting, Gene, Molecular Biology, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

Background Genomic imprinting is an important epigenetic process involved in regulating placental and foetal growth. Imprinted genes are typically associated with differentially methylated regions (DMRs) whereby one of the two alleles is DNA methylated depending on the parent of origin. Identifying imprinted DMRs in humans is complicated by species- and tissue-specific differences in imprinting status and the presence of multiple regulatory regions associated with a particular gene, only some of which may be imprinted. In this study, we have taken advantage of the unbalanced parental genomic constitutions in triploidies to further characterize human DMRs associated with known imprinted genes and identify novel imprinted DMRs. Results By comparing the promoter methylation status of over 14,000 genes in human placentas from ten diandries (extra paternal haploid set) and ten digynies (extra maternal haploid set) and using 6 complete hydatidiform moles (paternal origin) and ten chromosomally normal placentas for comparison, we identified 62 genes with apparently imprinted DMRs (false discovery rate FAM50B, as well as novel imprinted DMRs associated with known imprinted genes (for example, CDKN1C and RASGRF1) can be identified by using this approach. Furthermore, we have demonstrated how comparison of DNA methylation for known imprinted genes (for example, GNAS and CDKN1C) between placentas of different gestations and other somatic tissues (brain, kidney, muscle and blood) provides a detailed analysis of specific CpG sites associated with tissue-specific imprinting and gestational age-specific methylation. Conclusions DNA methylation profiling of triploidies in different tissues and developmental ages can be a powerful and effective way to map and characterize imprinted regions in the genome.

Published

2011

8. Evaluating DNA methylation and gene expression variability in the human term placenta

Author

Ruby Jiang, D. Diego-Alvarez, Maria S. Peñaherrera, Luana Avila, Ryan K. C. Yuen, and Wendy P. Robinson

Subjects

Placenta, Adenomatous Polyposis Coli Protein, Biology, Pregnancy, Gene expression, medicine, Humans, Epigenetics, Promoter Regions, Genetic, Gene, Genetics, Regulation of gene expression, Caspase 8, Kisspeptins, Protein Tyrosine Phosphatase, Non-Receptor Type 6, Tumor Suppressor Proteins, Obstetrics and Gynecology, Methylation, DNA Methylation, Molecular biology, medicine.anatomical_structure, Reproductive Medicine, CpG site, Gene Expression Regulation, DNA methylation, CpG Islands, Female, Developmental Biology

Abstract

Obtaining representative samples from a term placenta for gene-expression studies is confounded by both within placental heterogeneity and sampling effects such as sample location and processing time. Epigenetic processes involved in the regulation of gene expression, such as DNA methylation, may show similar variability, but are less well studied. Therefore, we investigated the nature of within and between- placenta variation in gene expression and DNA methylation of genes that were chosen for being differentially expressed or methylated by cell type within the placenta. Methods: In total, two or more samples from each of 38 normal term placentae were utilized. The expression levels of CDH1, CDH11, ID2, PLAC1 and KISS1 were evaluated by real-time PCR. DNA methylation levels of LINE1 elements and CpGs within the promoter regions of KISS1, PTPN6, CASP8, and APC were similarly quantified by pyrosequencing. Results: Despite considerable sample-to-sample variability within each placenta, the within-placenta correlation for both gene expression and methylation was significant for each studied gene. Most of this variability was not due to sample location. However, between placental differences in gene expression were inflated by the dramatic effect of processing time (0e24 h) on mRNA levels, particularly for PLAC1 and KISS1 (both expressed in the apical syncytiotrophoblast). In contrast, DNA methylation levels remained relatively constant over this same time period. Conclusion: Due to extensive site-to-site variability, multiple sampled sites are needed to accurately represent a placenta for molecular studies. Furthermore, mRNA quantitation of some genes may be hampered by its rapid degradation post-delivery (and possibly perinatally) and thus processing time should be considered in such analyses. Within-placenta correlations in expression and methylation from unrelated genes raise the possibility that methylation and expression variation may potentially reflect cell composition differences between samples rather than true differences occurring at the cellular level. 2010 Elsevier Ltd. All rights reserved.

Published

2010

9. Assessing the role of placental trisomy in preeclampsia and intrauterine growth restriction

Author

Wendy P, Robinson, Maria S, Peñaherrera, Ruby, Jiang, Luana, Avila, Jennifer, Sloan, Deborah E, McFadden, Sylvie, Langlois, and Peter, von Dadelszen

Subjects

Adult, Comparative Genomic Hybridization, Fetal Growth Retardation, Mosaicism, Biopsy, Placenta, Pregnancy Outcome, Gestational Age, Trisomy, Chorionic Gonadotropin, Pre-Eclampsia, Pregnancy, Chromosomes, Human, Pair 2, Prenatal Diagnosis, Humans, Female, Genetic Predisposition to Disease, Chromosomes, Human, Pair 7

Abstract

Prenatally diagnosed confined placental trisomy is associated with increased risk for intrauterine growth restriction (IUGR) and preeclampsia. However, it is unclear how often this might underlie pregnancy complications. Our objective was to evaluate the frequency and distribution of trisomic cells in placentae ascertained for IUGR and/or preeclampsia.Comparative genomic hybridization was applied to two uncultured biopsies from each of 61 placentae referred with maternal preeclampsia and/or IUGR, 11 cases with elevated maternal serum hCG and/or AFP but no IUGR or preeclampsia, and 85 control placentae.Trisomy was observed in four placentae among the IUGR group (N = 43) but in no case of preeclampsia in the absence of IUGR (N = 18). Trisomy was observed in 1 of the 11 cases ascertained for abnormal maternal serum screen. Each of these five cases was mosaic and not all sampled sites showed the presence of trisomy. None of the 84 control placentas showed mosaic trisomy, although 1 case of nonmosaic 47,XXX was identified in this group.In cases in which diagnosis of the cause of IUGR may provide some benefit, testing should be performed using uncultured cells from multiple placental biopsies for the accurate diagnosis of trisomy mosaicism.

Published

2009

10. Methylation of ZNF261 as an assay for determining X chromosome inactivation patterns

Author

Christy, Beever, Betty P Y, Lai, Sarah E L, Baldry, Maria S, Peñaherrera, Ruby, Jiang, Wendy P, Robinson, and Carolyn J, Brown

Subjects

Dosage Compensation, Genetic, Humans, Nuclear Proteins, CpG Islands, Female, DNA Methylation

Published

2003

11. Dispermy--origin of diandric triploidy: Brief Communication

Author

Sylvie Langlois, Wendy P. Robinson, Deborah E. McFadden, and Ruby Jiang

Subjects

Genetic Markers, Male, Genetics, urogenital system, Centromere, fungi, Rehabilitation, Obstetrics and Gynecology, Biology, Polyspermy, Diploidy, Spermatozoa, Sperm, Polyploidy, Meiosis, Sperm cell, Reproductive Medicine, Fertilization, Humans, Female, Ploidy, In Situ Hybridization, Fluorescence

Abstract

Triploidy may arise from either digynic or diandric fertilizations. Errors in the second meiotic division account for most digynic triploidy while most studies have found that approximately 2/3 of diandric triploids arise as the result of dispermy and 1/3 as the result of meiotic errors giving rise to diploid sperm. Using molecular markers very close to the centromere, all 14 cases of diandric triploidy were shown to be the result of dispermy with no evidence to support a meiotic error as the origin of diandric triploids.

Published

2002