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28 results on '"Ushiki, Aki"'

1. Deletion of Pax1 scoliosis-associated regulatory elements leads to a female-biased tail abnormality.

Author

Ushiki, Aki, Sheng, Rory, Zhang, Yichi, Zhao, Jingjing, Murray, Elizabeth, Ruan, Xin, Rios, Jonathan, Wise, Carol, Ahituv, Nadav, and Nobuhara, Mai

Subjects
AIS, CP: Molecular biology, GWAS, Pax1, enhancer, scoliosis, sexual dimorphism, Animals, Female, Mice, Genetic Predisposition to Disease, Genome-Wide Association Study, Scoliosis, Tail, Transcription Factors
Abstract

Adolescent idiopathic scoliosis (AIS), a sideways curvature of the spine, is sexually dimorphic, with increased incidence in females. A genome-wide association study identified a female-specific AIS susceptibility locus near the PAX1 gene. Here, we use mouse enhancer assays, three mouse enhancer knockouts, and subsequent phenotypic analyses to characterize this region. Using mouse enhancer assays, we characterize a sequence, PEC7, which overlaps the AIS-associated variant, and find it to be active in the tail tip and intervertebral disc. Removal of PEC7 or Xe1, a known sclerotome enhancer nearby, or deletion of both sequences lead to a kinky tail phenotype only in the Xe1 and combined (Xe1+PEC7) knockouts, with only the latter showing a female sex dimorphic phenotype. Extensive phenotypic characterization of these mouse lines implicates several differentially expressed genes and estrogen signaling in the sex dimorphic bias. In summary, our work functionally characterizes an AIS-associated locus and dissects the mechanism for its sexual dimorphism.

Published
2024

2. Deletion of CTCF sites in the SHH locus alters enhancer-promoter interactions and leads to acheiropodia.

Author

Ushiki, Aki, Zhang, Yichi, Xiong, Chenling, Zhao, Jingjing, Georgakopoulos-Soares, Ilias, Kane, Lauren, Jamieson, Kirsty, Bamshad, Michael J, Nickerson, Deborah A, University of Washington Center for Mendelian Genomics, Shen, Yin, Lettice, Laura A, Silveira-Lucas, Elizabeth Lemos, Petit, Florence, and Ahituv, Nadav

Subjects
University of Washington Center for Mendelian Genomics, Extremities, Animals, Mice, Knockout, Humans, Mice, Foot Deformities, Congenital, Hand Deformities, Congenital, Disease Models, Animal, Membrane Proteins, Species Specificity, Gene Expression Regulation, Developmental, Sequence Deletion, Binding Sites, Introns, Exons, Female, Male, Hedgehog Proteins, Embryo, Mammalian, Enhancer Elements, Genetic, Promoter Regions, Genetic, Genetic Testing, Genetic Loci, Whole Genome Sequencing, CCCTC-Binding Factor, Chromatin Immunoprecipitation Sequencing, Disease Models, Animal, Embryo, Mammalian, Enhancer Elements, Genetic, Foot Deformities, Congenital, Gene Expression Regulation, Developmental, Hand Deformities, Knockout, Promoter Regions
Abstract

Acheiropodia, congenital limb truncation, is associated with homozygous deletions in the LMBR1 gene around ZRS, an enhancer regulating SHH during limb development. How these deletions lead to this phenotype is unknown. Using whole-genome sequencing, we fine-mapped the acheiropodia-associated region to 12 kb and show that it does not function as an enhancer. CTCF and RAD21 ChIP-seq together with 4C-seq and DNA FISH identify three CTCF sites within the acheiropodia-deleted region that mediate the interaction between the ZRS and the SHH promoter. This interaction is substituted with other CTCF sites centromeric to the ZRS in the disease state. Mouse knockouts of the orthologous 12 kb sequence have no apparent abnormalities, showcasing the challenges in modelling CTCF alterations in animal models due to inherent motif differences between species. Our results show that alterations in CTCF motifs can lead to a Mendelian condition due to altered enhancer-promoter interactions.

Published
2021

3. Genomic characterization of the adolescent idiopathic scoliosis-associated transcriptome and regulome.

Author

Makki, Nadja, Zhao, Jingjing, Liu, Zhaoyang, Eckalbar, Walter L, Ushiki, Aki, Khanshour, Anas M, Wu, Joe, Rios, Jonathan, Gray, Ryan S, Wise, Carol A, and Ahituv, Nadav

Subjects
Muscle, Skeletal, Spine, Humans, Scoliosis, Genetic Predisposition to Disease, Lysine, DNA-Binding Proteins, Receptors, G-Protein-Coupled, Histones, Genomics, Acetylation, Adolescent, Child, Female, Male, Genome-Wide Association Study, Transcriptome, RNA-Seq, Pediatric, Human Genome, Genetics, 2.1 Biological and endogenous factors, Musculoskeletal, Biological Sciences, Medical and Health Sciences, Genetics & Heredity
Abstract

Adolescent idiopathic scoliosis (AIS), a sideways curvature of the spine, is the most common pediatric musculoskeletal disorder, affecting ~3% of the population worldwide. However, its genetic bases and tissues of origin remain largely unknown. Several genome-wide association studies (GWAS) have implicated nucleotide variants in non-coding sequences that control genes with important roles in cartilage, muscle, bone, connective tissue and intervertebral disks (IVDs) as drivers of AIS susceptibility. Here, we set out to define the expression of AIS-associated genes and active regulatory elements by performing RNA-seq and chromatin immunoprecipitation-sequencing against H3 lysine 27 acetylation in these tissues in mouse and human. Our study highlights genetic pathways involving AIS-associated loci that regulate chondrogenesis, IVD development and connective tissue maintenance and homeostasis. In addition, we identify thousands of putative AIS-associated regulatory elements which may orchestrate tissue-specific expression in musculoskeletal tissues of the spine. Quantification of enhancer activity of several candidate regulatory elements from our study identifies three functional enhancers carrying AIS-associated GWAS SNPs at the ADGRG6 and BNC2 loci. Our findings provide a novel genome-wide catalog of AIS-relevant genes and regulatory elements and aid in the identification of novel targets for AIS causality and treatment.

Published
2021

4. The cartilage matrisome in adolescent idiopathic scoliosis

Author

Wise, Carol A, Sepich, Diane, Ushiki, Aki, Khanshour, Anas M, Kidane, Yared H, Makki, Nadja, Gurnett, Christina A, Gray, Ryan S, Rios, Jonathan J, Ahituv, Nadav, and Solnica-Krezel, Lila

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Pediatric, Pediatric Research Initiative, Genetics, Human Genome, Aetiology, 2.1 Biological and endogenous factors, Musculoskeletal, Bone quality and biomechanics, Pathogenesis, Clinical sciences
Abstract

The human spinal column is a dynamic, segmented, bony, and cartilaginous structure that protects the neurologic system and simultaneously provides balance and flexibility. Children with developmental disorders that affect the patterning or shape of the spine can be at risk of neurologic and other physiologic dysfunctions. The most common developmental disorder of the spine is scoliosis, a lateral deformity in the shape of the spinal column. Scoliosis may be part of the clinical spectrum that is observed in many developmental disorders, but typically presents as an isolated symptom in otherwise healthy adolescent children. Adolescent idiopathic scoliosis (AIS) has defied understanding in part due to its genetic complexity. Breakthroughs have come from recent genome-wide association studies (GWAS) and next generation sequencing (NGS) of human AIS cohorts, as well as investigations of animal models. These studies have identified genetic associations with determinants of cartilage biogenesis and development of the intervertebral disc (IVD). Current evidence suggests that a fraction of AIS cases may arise from variation in factors involved in the structural integrity and homeostasis of the cartilaginous extracellular matrix (ECM). Here, we review the development of the spine and spinal cartilages, the composition of the cartilage ECM, the so-called "matrisome" and its functions, and the players involved in the genetic architecture of AIS. We also propose a molecular model by which the cartilage matrisome of the IVD contributes to AIS susceptibility.

Published
2020

5. Association of genetic variation in COL11A1 with adolescent idiopathic scoliosis

Author

Yu, Hao, primary, Khanshour, Anas M, primary, Ushiki, Aki, primary, Otomo, Nao, additional, Koike, Yoshinao, additional, Einarsdottir, Elisabet, additional, Fan, Yanhui, additional, Antunes, Lilian, additional, Kidane, Yared H, additional, Cornelia, Reuel, additional, Sheng, Rory R, additional, Zhang, Yichi, additional, Pei, Jimin, additional, Grishin, Nick V, additional, Evers, Bret M, additional, Cheung, Jason Pui Yin, additional, Herring, John A, additional, Terao, Chikashi, additional, Song, You-qiang, additional, Gurnett, Christina A, additional, Gerdhem, Paul, additional, Ikegawa, Shiro, additional, Rios, Jonathan J, additional, Ahituv, Nadav, additional, and Wise, Carol A, additional

Published
2024
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6. Association of genetic variation in COL11A1 with adolescent idiopathic scoliosis

Author

Yu, Hao, primary, Khanshour, Anas M., primary, Ushiki, Aki, primary, Otomo, Nao, additional, Koike, Yoshinao, additional, Einarsdottir, Elisabet, additional, Fan, Yanhui, additional, Antunes, Lilian, additional, Kidane, Yared H., additional, Cornelia, Reuel, additional, Sheng, Rory, additional, Zhang, Yichi, additional, Pei, Jimin, additional, Grishin, Nick V., additional, Evers, Bret M., additional, Cheung, Jason Pui Yin, additional, Herring, John A., additional, Terao, Chikashi, additional, Song, You-Qiang, additional, Gurnett, Christina A., additional, Gerdhem, Paul, additional, Ikegawa, Shiro, additional, Rios, Jonathan J., additional, Ahituv, Nadav, additional, and Wise, Carol A., additional

Published
2023
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7. Association of an estrogen-sensitive Pax1-Col11a1-Mmp3 signaling axis with adolescent idiopathic scoliosis

Author

Yu, Hao, primary, Khanshour, Anas M., additional, Ushiki, Aki, additional, Otomo, Nao, additional, Koike, Yoshinao, additional, Einarsdottir, Elisabet, additional, Fan, Yanhui, additional, Antunes, Lilian, additional, Kidane, Yared H., additional, Cornelia, Reuel, additional, Sheng, Rory, additional, Zhang, Yichi, additional, Pei, Jimin, additional, Grishin, Nick V., additional, Evers, Bret M., additional, Yin Cheung, Jason Pui, additional, Herring, John A., additional, Terao, Chikashi, additional, Song, You-Qiang, additional, Gurnett, Christina A., additional, Gerdhem, Paul, additional, Ikegawa, Shiro, additional, Rios, Jonathan J., additional, Ahituv, Nadav, additional, and Wise, Carol A., additional

Published
2023
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10. Association of an estrogen-sensitive Pax1-Col11a1-Mmp3 signaling axis with adolescent idiopathic scoliosis

Author

Wise, Carol, primary, Yu, Hao, additional, Khanshour, Anas M., additional, Ushiki, Aki, additional, Otomo, Nao, additional, Koike, Yoshinao, additional, Einarsdottir, Elisabet, additional, Fan, Yanhui, additional, Antunes, Lilian, additional, Kidane, Yared H., additional, Sheng, Rory, additional, Zhang, Yichi, additional, Pei, Jimin, additional, Grishin, Nick V., additional, Evers, Bret M V., additional, Cheung, Jason Pui Yin, additional, Herring, John A., additional, Terao, Chikashi, additional, Song, You-Qiang, additional, Gurnett, Christina, additional, Gerdhem, Paul, additional, Ikegawa, Shiro, additional, Rios, Jonathan J., additional, and Ahituv, Nadav, additional

Published
2023
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12. Missense variants in collagenesis genes increase risk of adolescent idiopathic scoliosis

Author

Wise, Carol, Khanshour, Anas, Yu, Hao, Ushiki, Aki, Li, Xiao-Yan, Otomo, Nao, Koike, Yoshinao, Einarsdottir, Elisabet, Fan, Felix, Antunes, Lilian, Sheng, Rory, Zhang, Yichi, Pei, Jimin, Grishin, Nick, Evers, Bret, Cheung, Jason Pui Yin, Herring, Tony, Song, You-Qiang, Gurnett, Christina, Gerdhem, Paul, Ikegawa, Shiro, Weiss, Stephen, Ahituv, Nadav, Rios, Jonathan, Wise, Carol, Khanshour, Anas, Yu, Hao, Ushiki, Aki, Li, Xiao-Yan, Otomo, Nao, Koike, Yoshinao, Einarsdottir, Elisabet, Fan, Felix, Antunes, Lilian, Sheng, Rory, Zhang, Yichi, Pei, Jimin, Grishin, Nick, Evers, Bret, Cheung, Jason Pui Yin, Herring, Tony, Song, You-Qiang, Gurnett, Christina, Gerdhem, Paul, Ikegawa, Shiro, Weiss, Stephen, Ahituv, Nadav, and Rios, Jonathan

Abstract

QC 20230922

Published
2023

13. Integrative single-cell characterization of hypothalamus sex-differential and obesity-associated genes and regulatory elements

Author

Nguyen, Hai P., primary, Chan, Candace S.Y, additional, Cintron, Dianne Laboy, additional, Sheng, Rory, additional, Harshman, Lana, additional, Nobuhara, Mai, additional, Ushiki, Aki, additional, Biellak, Cassidy, additional, An, Kelly, additional, Gordon, Gracie M., additional, Mifsud, Francois, additional, Blake, Abbey, additional, Huang, Eric J., additional, Hemberg, Martin, additional, Vaisse, Christian, additional, and Ahituv, Nadav, additional

Published
2022
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18. Deletion of Pax1scoliosis-associated regulatory elements leads to a female-biased tail abnormality

Author

Ushiki, Aki, Sheng, Rory R., Zhang, Yichi, Zhao, Jingjing, Nobuhara, Mai, Murray, Elizabeth, Ruan, Xin, Rios, Jonathan J., Wise, Carol A., and Ahituv, Nadav

Abstract

Adolescent idiopathic scoliosis (AIS), a sideways curvature of the spine, is sexually dimorphic, with increased incidence in females. A genome-wide association study identified a female-specific AIS susceptibility locus near the PAX1gene. Here, we use mouse enhancer assays, three mouse enhancer knockouts, and subsequent phenotypic analyses to characterize this region. Using mouse enhancer assays, we characterize a sequence, PEC7, which overlaps the AIS-associated variant, and find it to be active in the tail tip and intervertebral disc. Removal of PEC7 or Xe1, a known sclerotome enhancer nearby, or deletion of both sequences lead to a kinky tail phenotype only in the Xe1 and combined (Xe1+PEC7) knockouts, with only the latter showing a female sex dimorphic phenotype. Extensive phenotypic characterization of these mouse lines implicates several differentially expressed genes and estrogen signaling in the sex dimorphic bias. In summary, our work functionally characterizes an AIS-associated locus and dissects the mechanism for its sexual dimorphism.

Published
2024
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24. A mouse renin distal enhancer is essential for blood pressure homeostasis in BAC-rescued renin-null mutant mice.

Author

Tanimoto, Keiji, Kanafusa, Sumiyo, Ushiki, Aki, Matsuzaki, Hitomi, Ishida, Junji, Sugiyama, Fumihiro, and Fukamizu, Akiyoshi

Abstract

Renin is predominantly expressed in juxtaglomerular cells in the kidney and regulates blood pressure homeostasis. To examine possible in vivo functions of a mouse distal enhancer (mdE), we generated transgenic mice (TgM) carrying either wild-type or mdE-deficient renin BACs (bacterial artificial chromosome), integrated at the identical chromosomal site. In the kidneys of the TgM, the mdE contributed 80% to basal renin promoter activity. To test for possible physiological roles for the mdE, renin BAC transgenes were used to rescue the hypotensive renin-null mice. Interestingly, renal renin expression in the TgBAC: renin-null compound mice was indistinguishable between the wild-type and mutant BAC carriers. Surprisingly, however, the plasma renin activity and angiotensin I concentration in the mdE compound mutant mice were significantly lower than the same parameters in the control mice, and the mutants were consistently hypotensive, demonstrating that blood pressure homeostasis is regulated through transcriptional cis elements controlling renin activity. [ABSTRACT FROM AUTHOR]

Published
2014
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25. Synthetic DNA fragments bearing ICR <italic>cis</italic> elements become differentially methylated and recapitulate genomic imprinting in transgenic mice.

Author

Matsuzaki, Hitomi, Okamura, Eiichi, Kuramochi, Daichi, Ushiki, Aki, Hirakawa, Katsuhiko, Fukamizu, Akiyoshi, and Tanimoto, Keiji

Subjects
DNA methylation, GENOMIC imprinting, TRANSGENIC mice, GAMETES, BACTERIOPHAGE lambda
Abstract

Background: Genomic imprinting is governed by allele-specific DNA methylation at imprinting control regions (ICRs), and the mechanism controlling its differential methylation establishment during gametogenesis has been a subject of intensive research interest. However, recent studies have reported that gamete methylation is not restricted at the ICRs, thus highlighting the significance of ICR methylation maintenance during the preimplantation period where genome-wide epigenetic reprogramming takes place. Using transgenic mice (TgM), we previously demonstrated that the H19 ICR possesses autonomous activity to acquire paternal-allele-specific DNA methylation after fertilization. Furthermore, this activity is indispensable for the maintenance of imprinted methylation at the endogenous H19 ICR during the preimplantation period. In addition, we showed that a specific 5′ fragment of the H19 ICR is required for its paternal methylation after fertilization, while CTCF and Sox-Oct motifs are essential for its maternal protection from undesirable methylation after implantation. Results: To ask whether specific cis elements are sufficient to reconstitute imprinted methylation status, we employed a TgM co-placement strategy for facilitating detection of postfertilization methylation activity and precise comparison of test sequences. Bacteriophage lambda DNA becomes highly methylated regardless of its parental origin and thus can be used as a neutral sequence bearing no inclination for differential DNA methylation. We previously showed that insertion of only CTCF and Sox-Oct binding motifs from the H19 ICR into a lambda DNA (LCb) decreased its methylation level after both paternal and maternal transmission. We therefore appended a 478-bp 5′ sequence from the H19 ICR into the LCb fragment and found that it acquired paternal-allele-specific methylation, the dynamics of which was identical to that of the H19 ICR, in TgM. Crucially, transgene expression also became imprinted. Although there are potential binding sites for ZFP57 (a candidate protein thought to control the methylation imprint) in the larger H19 ICR, they are not found in the 478-bp fragment, rendering the role of ZFP57 in postfertilization H19 ICR methylation a still open question. Conclusions: Our results demonstrate that a differentially methylated region can be reconstituted by combining the activities of specific imprinting elements and that these elements together determine the activity of a genomically imprinted region in vivo. [ABSTRACT FROM AUTHOR]

Published
2018
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26. Association of genetic variation in COL11A1 with adolescent idiopathic scoliosis.

Author

Yu H, Khanshour AM, Ushiki A, Otomo N, Koike Y, Einarsdottir E, Fan Y, Antunes L, Kidane YH, Cornelia R, Sheng R, Zhang Y, Pei J, Grishin NV, Evers BM, Cheung JPY, Herring JA, Terao C, Song YQ, Gurnett CA, Gerdhem P, Ikegawa S, Rios JJ, Ahituv N, and Wise CA

Abstract

Adolescent idiopathic scoliosis (AIS) is a common and progressive spinal deformity in children that exhibits striking sexual dimorphism, with girls at more than five-fold greater risk of severe disease compared to boys. Despite its medical impact, the molecular mechanisms that drive AIS are largely unknown. We previously defined a female-specific AIS genetic risk locus in an enhancer near the PAX1 gene. Here we sought to define the roles of PAX1 and newly-identified AIS-associated genes in the developmental mechanism of AIS. In a genetic study of 10,519 individuals with AIS and 93,238 unaffected controls, significant association was identified with a variant in COL11A1 encoding collagen (α1) XI (rs3753841; NM&#95;080629.2&#95;c.4004C>T; p.(Pro1335Leu); P=7.07e -11 , OR=1.118). Using CRISPR mutagenesis we generated Pax1 knockout mice ( Pax1 -/- ). In postnatal spines we found that PAX1 and collagen (α1) XI protein both localize within the intervertebral disc (IVD)-vertebral junction region encompassing the growth plate, with less collagen (α1) XI detected in Pax1 -/- spines compared to wildtype. By genetic targeting we found that wildtype Col11a1 expression in costal chondrocytes suppresses expression of Pax1 and of Mmp3 , encoding the matrix metalloproteinase 3 enzyme implicated in matrix remodeling. However, this suppression was abrogated in the presence of the AIS-associated COL11A1 P1335L mutant. Further, we found that either knockdown of the estrogen receptor gene Esr2 , or tamoxifen treatment, significantly altered Col11a1 and Mmp3 expression in chondrocytes. We propose a new molecular model of AIS pathogenesis wherein genetic variation and estrogen signaling increase disease susceptibility by altering a Pax1-Col11a1-Mmp3 signaling axis in spinal chondrocytes., Competing Interests: Competing interests The authors declare no competing interests.

Published
2023
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27. Deletion of Pax1 scoliosis-associated regulatory elements leads to a female-biased tail abnormality.

Author

Ushiki A, Sheng RR, Zhang Y, Zhao J, Nobuhara M, Murray E, Ruan X, Rios JJ, Wise CA, and Ahituv N

Abstract

Adolescent idiopathic scoliosis (AIS), a sideways curvature of the spine, is sexually dimorphic, with increased incidence in females. A GWAS identified a female-specific AIS susceptibility locus near the PAX1 gene. Here, we used mouse enhancer assays, three mouse enhancer knockouts and subsequent phenotypic analyses to characterize this region. Using mouse enhancer assays, we characterized a sequence, PEC7, that overlaps the AIS-associated variant, and found it to be active in the tail tip and intervertebral disc. Removal of PEC7 or Xe1, a known sclerotome enhancer nearby, and deletion of both sequences led to a kinky phenotype only in the Xe1 and combined (Xe1+PEC7) knockouts, with only the latter showing a female sex dimorphic phenotype. Extensive phenotypic characterization of these mouse lines implicated several differentially expressed genes and estrogen signaling in the sex dimorphic bias. In summary, our work functionally characterizes an AIS-associated locus and dissects the mechanism for its sexual dimorphism., Competing Interests: Competing interests NA is a cofounder and on the scientific advisory board of Regel Therapeutics and Neomer Diagnostics. NA receives funding from BioMarin Pharmaceutical Incorporate.

Published
2023
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28. De novo DNA methylation through the 5'-segment of the H19 ICR maintains its imprint during early embryogenesis.

Author

Matsuzaki H, Okamura E, Takahashi T, Ushiki A, Nakamura T, Nakano T, Hata K, Fukamizu A, and Tanimoto K

Subjects
Animals, Base Sequence, Blotting, Southern, DNA (Cytosine-5-)-Methyltransferases metabolism, DNA Methyltransferase 3A, DNA Primers genetics, Female, Insulin-Like Growth Factor II metabolism, Male, Mice, Mice, Transgenic, Molecular Sequence Data, Reverse Transcriptase Polymerase Chain Reaction, Sequence Analysis, DNA, DNA Methylation physiology, Embryonic Development physiology, Gene Expression Regulation, Developmental physiology, Genomic Imprinting physiology, RNA, Long Noncoding metabolism
Abstract

Genomic imprinting is a major monoallelic gene expression regulatory mechanism in mammals, and depends on gamete-specific DNA methylation of specialized cis-regulatory elements called imprinting control regions (ICRs). Allele-specific DNA methylation of the ICRs is faithfully maintained at the imprinted loci throughout development, even in early embryos where genomes undergo extensive epigenetic reprogramming, including DNA demethylation, to acquire totipotency. We previously found that an ectopically introduced H19 ICR fragment in transgenic mice acquired paternal allele-specific methylation in the somatic cells of offspring, whereas it was not methylated in sperm, suggesting that its gametic and postfertilization modifications were separable events. We hypothesized that this latter activity might contribute to maintenance of the methylation imprint in early embryos. Here, we demonstrate that methylation of the paternally inherited transgenic H19 ICR commences soon after fertilization in a maternal DNMT3A- and DNMT3L-dependent manner. When its germline methylation was partially obstructed by insertion of insulator sequences, the endogenous paternal H19 ICR also exhibited postfertilization methylation. Finally, we refined the responsible sequences for this activity in transgenic mice and found that deletion of the 5' segment of the endogenous paternal H19 ICR decreased its methylation after fertilization and attenuated Igf2 gene expression. These results demonstrate that this segment of the H19 ICR is essential for its de novo postfertilization DNA methylation, and that this activity contributes to the maintenance of imprinted methylation at the endogenous H19 ICR during early embryogenesis., (© 2015. Published by The Company of Biologists Ltd.)

Published
2015
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