Your search keyword '"Naoki Nariai"' showing total 25 results

1. Type 1 diabetes risk genes mediate pancreatic beta cell survival in response to proinflammatory cytokines

Author

Paola Benaglio, Han Zhu, Mei-Lin Okino, Jian Yan, Ruth Elgamal, Naoki Nariai, Elisha Beebe, Katha Korgaonkar, Yunjiang Qiu, Margaret K.R. Donovan, Joshua Chiou, Gaowei Wang, Jacklyn Newsome, Jaspreet Kaur, Michael Miller, Sebastian Preissl, Sierra Corban, Anthony Aylward, Jussi Taipale, Bing Ren, Kelly A. Frazer, Maike Sander, Kyle J. Gaulton, Department of Pathology, Biosciences, Doctoral Programme in Integrative Life Science, and Jussi Taipale / Principal Investigator

Subjects

Pediatric, accessible chromatin, type 1 diabetes, Prevention, high-throughput reporter assay, Human Genome, Diabetes, human genetics, Autoimmune Disease, Biochemistry, Genetics and Molecular Biology (miscellaneous), beta cell, CRISPR screen, Cardiovascular and Metabolic Diseases, 3121 General medicine, internal medicine and other clinical medicine, proinflammatory cytokines, gene expression, Genetics, 2.1 Biological and endogenous factors, 3111 Biomedicine, Aetiology, 3D chromatin interactions, functional genomics, Metabolic and endocrine

Abstract

Publisher Copyright: © 2022 We combined functional genomics and human genetics to investigate processes that affect type 1 diabetes (T1D) risk by mediating beta cell survival in response to proinflammatory cytokines. We mapped 38,931 cytokine-responsive candidate cis-regulatory elements (cCREs) in beta cells using ATAC-seq and snATAC-seq and linked them to target genes using co-accessibility and HiChIP. Using a genome-wide CRISPR screen in EndoC-βH1 cells, we identified 867 genes affecting cytokine-induced survival, and genes promoting survival and up-regulated in cytokines were enriched at T1D risk loci. Using SNP-SELEX, we identified 2,229 variants in cytokine-responsive cCREs altering transcription factor (TF) binding, and variants altering binding of TFs regulating stress, inflammation, and apoptosis were enriched for T1D risk. At the 16p13 locus, a fine-mapped T1D variant altering TF binding in a cytokine-induced cCRE interacted with SOCS1, which promoted survival in cytokine exposure. Our findings reveal processes and genes acting in beta cells during inflammation that modulate T1D risk.

Published

2022

2. A crowdsourced set of curated structural variants for the human genome

Author

Eric T. Dawson, Chunlin Xiao, Noah Alexander, Sree Rohit Raj Kolora, Lesley M. Chapman, Aaron M. Wenger, Christopher M. Watson, Giuseppe Narzisi, Justin M. Zook, Daniel Blankenberg, Christian Brueffer, Graeme C. Smith, Marc L. Salit, Azza Ahmed, Paul Wolujewicz, Saadlee Shehreen, Naoki Nariai, Patrick Pai, Christos Proukakis, Andrew Carroll, Garan Jones, Wayne E. Clarke, Noah Spies, Chun Shen Lim, Chapman, Lesley M [0000-0001-7413-4392], Spies, Noah [0000-0002-6759-9842], Pai, Patrick [0000-0001-5304-788X], Lim, Chun Shen [0000-0001-7015-0125], Carroll, Andrew [0000-0002-4824-6689], Narzisi, Giuseppe [0000-0003-1118-8849], Watson, Christopher M [0000-0003-2371-1844], Proukakis, Christos [0000-0001-6423-6539], Clarke, Wayne E [0000-0003-2471-0712], Dawson, Eric [0000-0001-5448-1653], Jones, Garan [0000-0002-8917-3930], Brueffer, Christian [0000-0002-3826-0989], Kolora, Sree Rohit Raj [0000-0001-7839-735X], Wolujewicz, Paul [0000-0003-2982-9448], Ahmed, Azza E [0000-0002-1358-8371], Smith, Graeme [0000-0002-7413-4998], Shehreen, Saadlee [0000-0002-4869-0747], Wenger, Aaron M [0000-0003-1183-0432], Salit, Marc [0000-0003-1624-5195], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Heredity, Computer science, Genome, Database and Informatics Methods, 0302 clinical medicine, INDEL Mutation, Heuristics, Genome Sequencing, Biology (General), Ecology, Genomics, Genetic Mapping, Tandem Repeats, Computational Theory and Mathematics, Modeling and Simulation, Sequence Analysis, Research Article, Bioinformatics, QH301-705.5, Concordance, Variant Genotypes, Computational biology, Research and Analysis Methods, Genome Complexity, DNA sequencing, Set (abstract data type), 03 medical and health sciences, Cellular and Molecular Neuroscience, Genetics, Humans, Repeated Sequences, Molecular Biology Techniques, Sequencing Techniques, Indel, Molecular Biology, Alleles, Ecology, Evolution, Behavior and Systematics, Genome, Human, Biology and Life Sciences, Computational Biology, Genome Analysis, 030104 developmental biology, Haplotypes, Genetic Loci, Genomic Structural Variation, Human genome, Sequence Alignment, 030217 neurology & neurosurgery, Reference genome

Abstract

A high quality benchmark for small variants encompassing 88 to 90% of the reference genome has been developed for seven Genome in a Bottle (GIAB) reference samples. However a reliable benchmark for large indels and structural variants (SVs) is more challenging. In this study, we manually curated 1235 SVs, which can ultimately be used to evaluate SV callers or train machine learning models. We developed a crowdsourcing app—SVCurator—to help GIAB curators manually review large indels and SVs within the human genome, and report their genotype and size accuracy. SVCurator displays images from short, long, and linked read sequencing data from the GIAB Ashkenazi Jewish Trio son [NIST RM 8391/HG002]. We asked curators to assign labels describing SV type (deletion or insertion), size accuracy, and genotype for 1235 putative insertions and deletions sampled from different size bins between 20 and 892,149 bp. ‘Expert’ curators were 93% concordant with each other, and 37 of the 61 curators had at least 78% concordance with a set of ‘expert’ curators. The curators were least concordant for complex SVs and SVs that had inaccurate breakpoints or size predictions. After filtering events with low concordance among curators, we produced high confidence labels for 935 events. The SVCurator crowdsourced labels were 94.5% concordant with the heuristic-based draft benchmark SV callset from GIAB. We found that curators can successfully evaluate putative SVs when given evidence from multiple sequencing technologies., Author summary Large genomic changes, called structural variants, can cause a variety of human diseases, but have been challenging to detect with conventional DNA sequencing methods. We are working in the Genome in a Bottle Consortium to develop authoritatively characterized genomes with benchmark structural variants that can be used by anyone to assess the accuracy of their sequencing and analysis methods. Manual curation of the sequencing reads from multiple technologies has been essential to establish benchmark variant calls. Here, we present consensus curations from a web-based platform that displays a comprehensive set of visualizations of sequencing read support for structural variants. We use the svviz visualization tool to present evidence not only for deletions but also for insertions, which have previously not been possible to curate. We derive consensus calls from the multiple curations of each variant, and we find these are highly concordant with a draft Genome in a Bottle structural variant benchmark set.

Published

2020

3. iPSCORE: A Resource of 222 iPSC Lines Enabling Functional Characterization of Genetic Variation across a Variety of Cell Types

Author

Sylvia M. Evans, Frauke Drees, Naoki Nariai, Lawrence S.B. Goldstein, Chang Zhao, Neil C. Chi, Erin N. Smith, Jonathan D. Grinstein, Olivier Harismendy, Rachel Feiring, Aitor Aguirre, Agnieszka D'Antonio-Chronowska, Eric Adler, Matteo D’Antonio, Kelly A. Frazer, William W. Greenwald, Yuriko Hishida, Fangwen Rao, Juan Carlos Izpisua Belmonte, Hiroko Matsui, Bernhard M. Schuldt, Sherin Hashem, KathyJean Farnam, Victor Borja, Paola Benaglio, Melvin Garcia, Jonathan Okubo, Franz-Josef Müller, Bradley C. Nelson, Veronica Modesto, He Li, Kenneth E. Diffenderfer, Thomas J. McGarry, Roy Williams, Margaret K.R. Donovan, Carl T. Dargitz, Gene W. Yeo, David Jakubosky, Megan Cook, Kristen Jepsen, Daniel T. O'Connor, Carl A. Miller, Christopher DeBoever, Joaquin Reyna, Athanasia D. Panopoulos, Angelo Arias, Jeanne F. Loring, and W. Travis Berggren

Subjects

0301 basic medicine, Databases, Factual, Genome-wide association study, Arrhythmias, Biochemistry, 2.1 Biological and endogenous factors, GWAS, iPSC-derived cardiomyocytes, LQT2, KCNH2, Myocytes, Cardiac, Stem Cell Research - Induced Pluripotent Stem Cell - Non-Human, Aetiology, Induced pluripotent stem cell, lcsh:QH301-705.5, Oligonucleotide Array Sequence Analysis, Genetics, lcsh:R5-920, iPSC, Continental Population Groups, Stem Cell Research - Induced Pluripotent Stem Cell - Human, High-Throughput Nucleotide Sequencing, Cell Differentiation, Single Nucleotide, Cellular Reprogramming, Phenotype, molecular traits, Multigene Family, lcsh:Medicine (General), Cardiac, Biotechnology, Resource, cardiac disease, Genotype, Clinical Sciences, Induced Pluripotent Stem Cells, NHLBI Next Gen, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Cell Line, Databases, 03 medical and health sciences, Clinical Research, Genetic variation, iPSCORE, Humans, physiological traits, Polymorphism, Allele, Genotyping, Factual, Genetic Association Studies, Genetic association, Myocytes, Stem Cell Research - Induced Pluripotent Stem Cell, Human Genome, Racial Groups, Genetic Variation, Arrhythmias, Cardiac, Cell Biology, Stem Cell Research, 030104 developmental biology, lcsh:Biology (General), Biochemistry and Cell Biology, Developmental Biology

Abstract

Summary Large-scale collections of induced pluripotent stem cells (iPSCs) could serve as powerful model systems for examining how genetic variation affects biology and disease. Here we describe the iPSCORE resource: a collection of systematically derived and characterized iPSC lines from 222 ethnically diverse individuals that allows for both familial and association-based genetic studies. iPSCORE lines are pluripotent with high genomic integrity (no or low numbers of somatic copy-number variants) as determined using high-throughput RNA-sequencing and genotyping arrays, respectively. Using iPSCs from a family of individuals, we show that iPSC-derived cardiomyocytes demonstrate gene expression patterns that cluster by genetic background, and can be used to examine variants associated with physiological and disease phenotypes. The iPSCORE collection contains representative individuals for risk and non-risk alleles for 95% of SNPs associated with human phenotypes through genome-wide association studies. Our study demonstrates the utility of iPSCORE for examining how genetic variants influence molecular and physiological traits in iPSCs and derived cell lines., Graphical Abstract, Highlights • iPSCORE: A collection of publicly available iPSCs from 222 individuals • Several multigenerational families and individuals of various ethnicities and ages • Individuals carrying risk and non-risk genotypes for 95% of GWAS SNPs • Genetic variants associated with mRNA expression in differentiated cardiomyocytes, Working as part of the NHLBI NextGen consortium, Panopoulos and colleagues report the derivation and characterization of 222 publicly available iPSCs from ethnically diverse individuals with corresponding genomic data including SNP arrays, RNA-seq, and whole-genome sequencing. This collection provides a powerful resource to investigate the function of genetic variants.

Published

2017

4. Author response: Systematic genetic analysis of the MHC region reveals mechanistic underpinnings of HLA type associations with disease

Author

Oliver Stegle, Marc Jan Bonder, Agnieszka D'Antonio-Chronowska, Matteo D’Antonio, Joaquin Reyna, Naoki Nariai, Margaret K.R. Donovan, David Jakubosky, Hiroko Matsui, and Kelly A. Frazer

Subjects

Genetics, biology, biology.protein, Human leukocyte antigen, Disease, Major histocompatibility complex, Genetic analysis

Published

2019

5. Systematic genetic analysis of the MHC region reveals mechanistic underpinnings of HLA type associations with disease

Author

Naoki Nariai, Joaquin Reyna, David Jakubosky, Matteo D’Antonio, Kelly A. Frazer, Hiroko Matsui, Margaret K.R. Donovan, Agnieszka D'Antonio-Chronowska, Marc Jan Bonder, and Oliver Stegle

Subjects

0301 basic medicine, Male, Cystic Fibrosis, Genome-wide association study, Major Histocompatibility Complex, 0302 clinical medicine, computational biology, HLA Antigens, 80 and over, 2.1 Biological and endogenous factors, genetics, RNA-Seq, HLA types, Aetiology, Biology (General), Genetics, Aged, 80 and over, General Neuroscience, eQTLs, Chromosome Mapping, systems biology, General Medicine, Single Nucleotide, Middle Aged, 3. Good health, Medicine, Female, Biotechnology, Research Article, Computational and Systems Biology, Human, Adult, Adolescent, QH301-705.5, Science, Quantitative Trait Loci, Genomics, Human leukocyte antigen, Biology, Major histocompatibility complex, Autoimmune Disease, Polymorphism, Single Nucleotide, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Young Adult, Genetic variation, genomics, Humans, Genetic Predisposition to Disease, human, Polymorphism, Alleles, Aged, General Immunology and Microbiology, Haplotype, Human Genome, Genetics and Genomics, Genetic architecture, 030104 developmental biology, Good Health and Well Being, Haplotypes, Expression quantitative trait loci, biology.protein, gene expression, Biochemistry and Cell Biology, 030217 neurology & neurosurgery, Genome-Wide Association Study

Abstract

The MHC region is highly associated with autoimmune and infectious diseases. Here we conduct an in-depth interrogation of associations between genetic variation, gene expression and disease. We create a comprehensive map of regulatory variation in the MHC region using WGS from 419 individuals to call eight-digit HLA types and RNA-seq data from matched iPSCs. Building on this regulatory map, we explored GWAS signals for 4083 traits, detecting colocalization for 180 disease loci with eQTLs. We show that eQTL analyses taking HLA type haplotypes into account have substantially greater power compared with only using single variants. We examined the association between the 8.1 ancestral haplotype and delayed colonization in Cystic Fibrosis, postulating that downregulation of RNF5 expression is the likely causal mechanism. Our study provides insights into the genetic architecture of the MHC region and pinpoints disease associations that are due to differential expression of HLA genes and non-HLA genes.

Published

2019

6. Pancreatic islet chromatin accessibility and conformation reveals distal enhancer networks of type 2 diabetes risk

Author

Nikita Kadakia, Jian Yan, Joseph Avruch, Anthony Aylward, Dana Kramer, Kelly A. Frazer, Laura Regué, Jee Yun Han, Kyle J. Gaulton, David U. Gorkin, Liliana Minichiello, Nicholas Vinckier, Maike Sander, Ning Dai, Joshua Chiou, Mei-Lin Okino, Frauke Drees, Naoki Nariai, William W. Greenwald, Allen Wang, Bing Ren, and Yunjiang Qiu

Subjects

0301 basic medicine, Epigenomics, Male, endocrine system diseases, genetic processes, Molecular Conformation, General Physics and Astronomy, Genome-wide association study, 02 engineering and technology, Inbred C57BL, Mice, Gene expression, Genetics research, 2.1 Biological and endogenous factors, Insulin, Gene Regulatory Networks, Aetiology, lcsh:Science, Mice, Knockout, Multidisciplinary, geography.geographical_feature_category, Diabetes, RNA-Binding Proteins, Middle Aged, 021001 nanoscience & nanotechnology, Islet, Chromatin, Cell biology, Transport protein, Enhancer Elements, Genetic, Female, 0210 nano-technology, Type 2, Biotechnology, Adult, endocrine system, Enhancer Elements, Knockout, Science, Quantitative Trait Loci, Biology, Chromatin structure, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Islets of Langerhans, Genetic, Diabetes Mellitus, Genetics, Animals, Humans, natural sciences, Genetic Predisposition to Disease, Enhancer, Gene, Metabolic and endocrine, Cell Nucleus, geography, Gene Expression Profiling, Human Genome, General Chemistry, Chromatin Assembly and Disassembly, Gene expression profiling, Mice, Inbred C57BL, 030104 developmental biology, Glucose, Diabetes Mellitus, Type 2, Cardiovascular and Metabolic Diseases, lcsh:Q

Abstract

Genetic variants affecting pancreatic islet enhancers are central to T2D risk, but the gene targets of islet enhancer activity are largely unknown. We generate a high-resolution map of islet chromatin loops using Hi-C assays in three islet samples and use loops to annotate target genes of islet enhancers defined using ATAC-seq and published ChIP-seq data. We identify candidate target genes for thousands of islet enhancers, and find that enhancer looping is correlated with islet-specific gene expression. We fine-map T2D risk variants affecting islet enhancers, and find that candidate target genes of these variants defined using chromatin looping and eQTL mapping are enriched in protein transport and secretion pathways. At IGF2BP2, a fine-mapped T2D variant reduces islet enhancer activity and IGF2BP2 expression, and conditional inactivation of IGF2BP2 in mouse islets impairs glucose-stimulated insulin secretion. Our findings provide a resource for studying islet enhancer function and identifying genes involved in T2D risk., Risk loci for type 2 diabetes (T2D) reside in pancreatic islet enhancers. Here, the authors generate high-resolution maps of islet chromatin conformation using Hi-C which they combine with ATAC-seq and ChIP-seq data to annotate candidate target genes of enhancers and validate IGF2BP2 activity in mouse islets.

Published

2019

7. Construction of full-length Japanese reference panel of class I HLA genes with single-molecule, real-time sequencing

Author

Nobuo Fuse, Naomi Nakai-Inagaki, Atsushi Hozawa, Akira Ono, Takahiro Mimori, Yoko Kuroki, Kazuharu Misawa, Junichi Sugawara, Sakae Saito, Naoki Nariai, Kengo Kinoshita, Shinichi Kuriyama, Jun Yasuda, Yosuke Kawai, Masao Nagasaki, Tomoko F. Shibata, Keiko Tateno, Naoko Minegishi, Kichiya Suzuki, Masayuki Yamamoto, and Fumiki Katsuoka

Subjects

0301 basic medicine, Genotype, Sequence analysis, Computational biology, Human leukocyte antigen, Biology, 030226 pharmacology & pharmacy, Article, 03 medical and health sciences, 0302 clinical medicine, Japan, Genetic variation, Genetics, Humans, Allele, Alleles, Genetic association, Pharmacology, Genome, Human, Histocompatibility Testing, Histocompatibility Antigens Class I, Genetic Variation, High-Throughput Nucleotide Sequencing, Sequence Analysis, DNA, Transplantation, 030104 developmental biology, Molecular Medicine, Single molecule real time sequencing

Abstract

Human leukocyte antigen (HLA) is a gene complex known for its exceptional diversity across populations, importance in organ and blood stem cell transplantation, and associations of specific alleles with various diseases. We constructed a Japanese reference panel of class I HLA genes (ToMMo HLA panel), comprising a distinct set of HLA-A, HLA-B, HLA-C, and HLA-H alleles, by single-molecule, real-time (SMRT) sequencing of 208 individuals included in the 1070 whole-genome Japanese reference panel (1KJPN). For high-quality allele reconstruction, we developed a novel pipeline, Primer-Separation Assembly and Refinement Pipeline (PSARP), in which the SMRT sequencing and additional short-read data were used. The panel consisted of 139 alleles, which were all extended from known IPD-IMGT/HLA sequences, contained 40 with novel variants, and captured more than 96.5% of allelic diversity in 1KJPN. These newly available sequences would be important resources for research and clinical applications including high-resolution HLA typing, genetic association studies, and analyzes of cis-regulatory elements.

Published

2017

8. Establishing the involvement of the novel gene AGBL5 in retinitis pigmentosa by whole genome sequencing

Author

John R. Heckenlively, Naoki Nariai, Kelly A. Frazer, Kari Branham, David Jakubosky, Paul A. Sieving, John Suk, Pooja Biswas, Tao Long, Michael A. Hicks, Amalio Telenti, Radha Ayyagari, He Li, Aditya A. Guru, and Hiroko Matsui

Subjects

0301 basic medicine, Male, Adolescent, Physiology, DNA Mutational Analysis, Carboxypeptidases, Biology, medicine.disease_cause, Compound heterozygosity, Genome, 03 medical and health sciences, symbols.namesake, Young Adult, Retinitis pigmentosa, Genetics, medicine, Electroretinography, Humans, Copy-number variation, Gene, Genetic Association Studies, Whole genome sequencing, Sanger sequencing, Mutation, Whole Genome Sequencing, Retinal Degeneration, General Interest, medicine.disease, Pedigree, 030104 developmental biology, symbols, Female, Retinitis Pigmentosa

Abstract

While more than 250 genes are known to cause inherited retinal degenerations (IRD), nearly 40–50% of families have the genetic basis for their disease unknown. In this study we sought to identify the underlying cause of IRD in a family by whole genome sequence (WGS) analysis. Clinical characterization including standard ophthalmic examination, fundus photography, visual field testing, electroretinography, and review of medical and family history was performed. WGS was performed on affected and unaffected family members using Illumina HiSeq X10. Sequence reads were aligned to hg19 using BWA-MEM and variant calling was performed with Genome Analysis Toolkit. The called variants were annotated with SnpEff v4.11, PolyPhen v2.2.2, and CADD v1.3. Copy number variations were called using Genome STRiP (svtoolkit 2.00.1611) and SpeedSeq software. Variants were filtered to detect rare potentially deleterious variants segregating with disease. Candidate variants were validated by dideoxy sequencing. Clinical evaluation revealed typical adolescent-onset recessive retinitis pigmentosa (arRP) in affected members. WGS identified about 4 million variants in each individual. Two rare and potentially deleterious compound heterozygous variants p.Arg281Cys and p.Arg487* were identified in the gene ATP/GTP binding protein like 5 ( AGBL5) as likely causal variants. No additional variants in IRD genes that segregated with disease were identified. Mutation analysis confirmed the segregation of these variants with the IRD in the pedigree. Homology models indicated destabilization of AGBL5 due to the p.Arg281Cys change. Our findings establish the involvement of mutations in AGBL5 in RP and validate the WGS variant filtering pipeline we designed.

Published

2016

9. Short tandem repeat number estimation from paired-end reads for multiple individuals by considering coalescent tree

Author

Yosuke Kawai, Masao Nagasaki, Kaname Kojima, Takahiro Mimori, Naoki Nariai, and Takanori Hasegawa

Subjects

0301 basic medicine, 0206 medical engineering, 02 engineering and technology, Biology, Belief propagation, Coalescent theory, 03 medical and health sciences, symbols.namesake, Genetics, Humans, Computer Simulation, Short tandem repeat, 1000 Genomes Project, Sequence, Models, Statistical, High-throughput sequencing, Genome, Human, Research, Markov chain Monte Carlo, Statistical model, Sequence Analysis, DNA, Tree (graph theory), Variable number tandem repeat, 030104 developmental biology, symbols, Algorithm, 020602 bioinformatics, Algorithms, Biotechnology, Microsatellite Repeats

Abstract

Background Two types of approaches are mainly considered for the repeat number estimation in short tandem repeat (STR) regions from high-throughput sequencing data: approaches directly counting repeat patterns included in sequence reads spanning the region and approaches based on detecting the difference between the insert size inferred from aligned paired-end reads and the actual insert size. Although the accuracy of repeat numbers estimated with the former approaches is high, the size of target STR regions is limited to the length of sequence reads. On the other hand, the latter approaches can handle STR regions longer than the length of sequence reads. However, repeat numbers estimated with the latter approaches is less accurate than those with the former approaches. Results We proposed a new statistical model named coalescentSTR that estimates repeat numbers from paired-end read distances for multiple individuals simultaneously by connecting the read generative model for each individual with their genealogy. In the model, the genealogy is represented by handling coalescent trees as hidden variables, and the summation of the hidden variables is taken on coalescent trees sampled based on phased genotypes located around a target STR region with Markov chain Monte Carlo. In the sampled coalescent trees, repeat number information from insert size data is propagated, and more accurate estimation of repeat numbers is expected for STR regions longer than the length of sequence reads. For finding the repeat numbers maximizing the likelihood of the model on the estimation of repeat numbers, we proposed a state-of-the-art belief propagation algorithm on sampled coalescent trees. Conclusions We verified the effectiveness of the proposed approach from the comparison with existing methods by using simulation datasets and real whole genome and whole exome data for HapMap individuals analyzed in the 1000 Genomes Project.

Published

2016

10. A Bayesian approach for estimating allele-specific expression from RNA-Seq data with diploid genomes

Author

Naoki Nariai, Takahiro Mimori, Kaname Kojima, Yosuke Kawai, and Masao Nagasaki

Subjects

0301 basic medicine, animal structures, Sequence analysis, Bayesian inference, Biology, Genome, RNA-Seq data, 03 medical and health sciences, Bayes' theorem, 0302 clinical medicine, Allele-specific expression, Cell Line, Tumor, Genetics, Humans, Protein Isoforms, Gene, Alleles, Comparative genomics, Genome, Human, Sequence Analysis, RNA, Proteins, Bayes Theorem, Diploidy, 030104 developmental biology, Proceedings, Gene Expression Regulation, RNA, Human genome, DNA microarray, 030217 neurology & neurosurgery, Algorithms, Reference genome, Biotechnology

Abstract

RNA-sequencing (RNA-Seq) has become a popular tool for transcriptome profiling in mammals. However, accurate estimation of allele-specific expression (ASE) based on alignments of reads to the reference genome is challenging, because it contains only one allele on a mosaic haploid genome. Even with the information of diploid genome sequences, precise alignment of reads to the correct allele is difficult because of the high-similarity between the corresponding allele sequences. We propose a Bayesian approach to estimate ASE from RNA-Seq data with diploid genome sequences. In the statistical framework, the haploid choice is modeled as a hidden variable and estimated simultaneously with isoform expression levels by variational Bayesian inference. Through the simulation data analysis, we demonstrate the effectiveness of the proposed approach in terms of identifying ASE compared to the existing approach. We also show that our approach enables better quantification of isoform expression levels compared to the existing methods, TIGAR2, RSEM and Cufflinks. In the real data analysis of the human reference lymphoblastoid cell line GM12878, some autosomal genes were identified as ASE genes, and skewed paternal X-chromosome inactivation in GM12878 was identified. The proposed method, called ASE-TIGAR, enables accurate estimation of gene expression from RNA-Seq data in an allele-specific manner. Our results show the effectiveness of utilizing personal genomic information for accurate estimation of ASE. An implementation of our method is available at http://nagasakilab.csml.org/ase-tigar .

Published

2016

11. Rare variant discovery by deep whole-genome sequencing of 1,070 Japanese individuals

Author

Rumiko Saito, Kaname Kojima, Kaoru Tsuda, Atsushi Hozawa, Yukuto Sato, Nobuo Fuse, Yosuke Kawai, Shin Ito, Shigeo Kure, Junji Yokozawa, Inaho Danjoh, Masao Nagasaki, Hideyasu Kiyomoto, Yoko Kuroki, Takahiro Mimori, Yumi Yamaguchi-Kabata, Xiaoqing Pan, Fumiki Katsuoka, Kengo Kinoshita, Naoki Nariai, Shinichi Kuriyama, Sakae Saito, Osamu Tanabe, Jun Yasuda, Masayuki Yamamoto, Naoko Minegishi, James Douglas Engel, Satoshi Nishikawa, and Nobuo Yaegashi

Subjects

Genetics, Whole genome sequencing, Multidisciplinary, Genome, Human, Haplotype, General Physics and Astronomy, Genetic Variation, General Chemistry, Biology, Genome, General Biochemistry, Genetics and Molecular Biology, Article, 3. Good health, Minor allele frequency, Asian People, Haplotypes, Genotype, Genetic variation, Humans, Human genome, Genetic association

Abstract

The Tohoku Medical Megabank Organization reports the whole-genome sequences of 1,070 healthy Japanese individuals and construction of a Japanese population reference panel (1KJPN). Here we identify through this high-coverage sequencing (32.4 × on average), 21.2 million, including 12 million novel, single-nucleotide variants (SNVs) at an estimated false discovery rate of, The Tohoku Medical Megabank Organization establishes a biobank with detailed patient health care and genome information. Here the authors analyse whole-genome sequences of 1,070 Japanese individuals, allowing them to catalogue 21 million single-nucleotide variants including 12 million novel ones.

Published

2015

12. Estimating gene regulatory networks and protein-protein interactions of Saccharomyces cerevisiae from multiple genome-wide data

Author

Satoru Miyano, Naoki Nariai, Seiya Imoto, and Yoshinori Tamada

Subjects

Statistics and Probability, Saccharomyces cerevisiae Proteins, Saccharomyces cerevisiae, Gene regulatory network, Computational biology, Biology, Biochemistry, Genome, Protein–protein interaction, Databases, Genetic, Protein Interaction Mapping, Computer Simulation, Molecular Biology, Gene, Genetics, Models, Genetic, Markov chain, Gene Expression Profiling, Chromosome Mapping, Bayesian network, biology.organism_classification, Computer Science Applications, Computational Mathematics, Gene Expression Regulation, Computational Theory and Mathematics, Algorithms, Biological network, Signal Transduction

Abstract

Motivation: Biological processes in cells are properly performed by gene regulations, signal transductions and interactions between proteins. To understand such molecular networks, we propose a statistical method to estimate gene regulatory networks and protein--protein interaction networks simultaneously from DNA microarray data, protein--protein interaction data and other genome-wide data. Results: We unify Bayesian networks and Markov networks for estimating gene regulatory networks and protein--protein interaction networks according to the reliability of each biological information source. Through the simultaneous construction of gene regulatory networks and protein--protein interaction networks of Saccharomyces cerevisiae cell cycle, we predict the role of several genes whose functions are currently unknown. By using our probabilistic model, we can detect false positives of high-throughput data, such as yeast two-hybrid data. In a genome-wide experiment, we find possible gene regulatory relationships and protein--protein interactions between large protein complexes that underlie complex regulatory mechanisms of biological processes. Contact: nariai@ims.u-tokyo.ac.jp

Published

2005

13. HLA-VBSeq: accurate HLA typing at full resolution from whole-genome sequencing data

Author

Yukuto Sato, Naoki Nariai, Yumi Yamaguchi-Kabata, Kaname Kojima, Masao Nagasaki, Yosuke Kawai, Takahiro Mimori, Jun Yasuda, and Sakae Saito

Subjects

Genotype, Human leukocyte antigen, Biology, Data sequences, Gene Frequency, HLA Antigens, Genetics, Humans, Allele, Allele frequency, Gene, Alleles, Whole genome sequencing, Internet, Polymorphism, Genetic, Genome, Human, Histocompatibility Testing, Computational Biology, High-Throughput Nucleotide Sequencing, Reproducibility of Results, Bayes Theorem, Proceedings, Primer (molecular biology), DNA microarray, Algorithms, Biotechnology

Abstract

Background Human leucocyte antigen (HLA) genes play an important role in determining the outcome of organ transplantation and are linked to many human diseases. Because of the diversity and polymorphisms of HLA loci, HLA typing at high resolution is challenging even with whole-genome sequencing data. Results We have developed a computational tool, HLA-VBSeq, to estimate the most probable HLA alleles at full (8-digit) resolution from whole-genome sequence data. HLA-VBSeq simultaneously optimizes read alignments to HLA allele sequences and abundance of reads on HLA alleles by variational Bayesian inference. We show the effectiveness of the proposed method over other methods through the analysis of predicting HLA types for HLA class I (HLA-A, -B and -C) and class II (HLA-DQA1,-DQB1 and -DRB1) loci from the simulation data of various depth of coverage, and real sequencing data of human trio samples. Conclusions HLA-VBSeq is an efficient and accurate HLA typing method using high-throughput sequencing data without the need of primer design for HLA loci. Moreover, it does not assume any prior knowledge about HLA allele frequencies, and hence HLA-VBSeq is broadly applicable to human samples obtained from a genetically diverse population.

Published

2015

14. TIGAR2: sensitive and accurate estimation of transcript isoform expression with longer RNA-Seq reads

Author

Yosuke Kawai, Yumi Yamaguchi-Kabata, Masao Nagasaki, Kaname Kojima, Naoki Nariai, Yukuto Sato, and Takahiro Mimori

Subjects

Pipeline (computing), Sequence assembly, RNA-Seq, Computational biology, Biology, Bayes' theorem, RNA Isoforms, Complementary DNA, Genetics, graphical models, Humans, RNA, Messenger, Sequence Analysis, RNA, Gene Expression Profiling, Research, Computational Biology, Genetic Variation, Bayes Theorem, Transcript isoform quantification, Gene expression profiling, DNA microarray, variational Bayesian inference, Algorithms, Software, Biotechnology, HeLa Cells

Abstract

Background High-throughput RNA sequencing (RNA-Seq) enables quantification and identification of transcripts at single-base resolution. Recently, longer sequence reads become available thanks to the development of new types of sequencing technologies as well as improvements in chemical reagents for the Next Generation Sequencers. Although several computational methods have been proposed for quantifying gene expression levels from RNA-Seq data, they are not sufficiently optimized for longer reads (e.g. > 250 bp). Results We propose TIGAR2, a statistical method for quantifying transcript isoforms from fixed and variable length RNA-Seq data. Our method models substitution, deletion, and insertion errors of sequencers based on gapped-alignments of reads to the reference cDNA sequences so that sensitive read-aligners such as Bowtie2 and BWA-MEM are effectively incorporated in our pipeline. Also, a heuristic algorithm is implemented in variational Bayesian inference for faster computation. We apply TIGAR2 to both simulation data and real data of human samples and evaluate performance of transcript quantification with TIGAR2 in comparison to existing methods. Conclusions TIGAR2 is a sensitive and accurate tool for quantifying transcript isoform abundances from RNA-Seq data. Our method performs better than existing methods for the fixed-length reads (100 bp, 250 bp, 500 bp, and 1000 bp of both single-end and paired-end) and variable-length reads, especially for reads longer than 250 bp.

Published

2015

15. Large-Scale Profiling Reveals the Influence of Genetic Variation on Gene Expression in Human Induced Pluripotent Stem Cells

Author

Bing Ren, Katrina M. Olson, David Jakubosky, Kelly A. Frazer, Erin N. Smith, Kristen Jepsen, Efren Sandoval, Naoki Nariai, Hui Huang, Angelo Arias, Paola Benaglio, Matteo D’Antonio, He Li, Hiroko Matsui, Christopher DeBoever, Agnieszka D'Antonio-Chronowska, Joaquin Reyna, Emma K. Farley, and William H. Biggs

Subjects

0301 basic medicine, Regulatory Sequences, Nucleic Acid, Medical and Health Sciences, 0302 clinical medicine, stem cell gene expression, 2.1 Biological and endogenous factors, Stem Cell Research - Induced Pluripotent Stem Cell - Non-Human, Aetiology, Induced pluripotent stem cell, Regulation of gene expression, Genetics, Stem Cell Research - Induced Pluripotent Stem Cell - Human, expression quantitative trait loci, Biological Sciences, Cellular Reprogramming, Regulatory sequence, Molecular Medicine, regulation of gene expression, Human, Biotechnology, DNA Copy Number Variations, Quantitative Trait Loci, Induced Pluripotent Stem Cells, Pair-rule gene, Biology, eQTL, Gene dosage, Article, Chromosomes, Genetic Heterogeneity, 03 medical and health sciences, Humans, Stem Cell Research - Embryonic - Human, Gene, Chromosomes, Human, X, Binding Sites, Nucleic Acid, Stem Cell Research - Induced Pluripotent Stem Cell, Gene Expression Profiling, Human Genome, Genetic Variation, Molecular Sequence Annotation, Cell Biology, Stem Cell Research, Gene expression profiling, 030104 developmental biology, Gene Expression Regulation, Expression quantitative trait loci, gene expression, stem cell genetics, Generic health relevance, Regulatory Sequences, 030217 neurology & neurosurgery, Transcription Factors, Developmental Biology

Abstract

In this study, we used whole genome sequencing and gene expression profiling of 215 human induced pluripotent stem cell (iPSC) lines from different donors to identify genetic variants associated with RNA expression for 5,746 genes. We were able to predict causal variants for these expression quantitative trait loci (eQTLs) that disrupt transcription factor binding and validated a subset of them experimentally. We also identified copy number variant (CNV) eQTLs, including some that appear to affect gene expression by altering the copy number of intergenic regulatory regions. In addition, we were able to identify effects on gene expression of rare genic CNVs and regulatory single nucleotide variants, and found that reactivation of gene expression on the X chromosome depends on gene chromosomal position. Our work highlights the value of iPSCs for genetic association analyses and provides a unique resource for investigating the genetic regulation of gene expression in pluripotent cells.

Published

2017

16. Validation of multiple single nucleotide variation calls by additional exome analysis with a semiconductor sequencer to supplement data of whole-genome sequencing of a human population

Author

Yukuto Sato, Kengo Kinoshita, Xiaoqing Pan, Masayuki Yamamoto, Inaho Danjoh, Shin Ito, Mitsuyo Matsumoto, Kaoru Tsuda, Naoki Nariai, Tomo Saito, Matsuyuki Shirota, Rumiko Saito, Satoshi Nishikawa, Junji Yokozawa, Ikuko N. Motoike, Hisaaki Kudo, Masao Nagasaki, Ichiko Nishijima, Kaname Kojima, Naoko Minegishi, Osamu Tanabe, Jun Yasuda, Kazuhiko Igarashi, Nobuo Fuse, Sakae Saito, Fumiki Katsuoka, and Yumi Yamaguchi-Kabata

Subjects

Male, Semiconductor-type sequencer, Population genetics, Population, Genomics, Biology, Polymorphism, Single Nucleotide, Deep sequencing, Single nucleotide variations, Next-generation sequencer, Human population genetics, Genetics, Humans, Exome, education, Exome sequencing, Whole genome sequencing, Whole-genome sequencing, Base Composition, education.field_of_study, Genome, Human, High-Throughput Nucleotide Sequencing, Reproducibility of Results, Sequence Analysis, DNA, SNP genotyping, Semiconductors, Female, Research Article, Biotechnology

Abstract

Background Validation of single nucleotide variations in whole-genome sequencing is critical for studying disease-related variations in large populations. A combination of different types of next-generation sequencers for analyzing individual genomes may be an efficient means of validating multiple single nucleotide variations calls simultaneously. Results Here, we analyzed 12 independent Japanese genomes using two next-generation sequencing platforms: the Illumina HiSeq 2500 platform for whole-genome sequencing (average depth 32.4×), and the Ion Proton semiconductor sequencer for whole exome sequencing (average depth 109×). Single nucleotide polymorphism (SNP) calls based on the Illumina Human Omni 2.5-8 SNP chip data were used as the reference. We compared the variant calls for the 12 samples, and found that the concordance between the two next-generation sequencing platforms varied between 83% and 97%. Conclusions Our results show the versatility and usefulness of the combination of exome sequencing with whole-genome sequencing in studies of human population genetics and demonstrate that combining data from multiple sequencing platforms is an efficient approach to validate and supplement SNP calls. Electronic supplementary material The online version of this article (doi:10.1186/1471-2164-15-673) contains supplementary material, which is available to authorized users.

Published

2014

17. SUGAR: graphical user interface-based data refiner for high-throughput DNA sequencing

Author

Naoki Nariai, Kaname Kojima, Takahiro Mimori, Masao Nagasaki, Mamoru Takahashi, Yosuke Kawai, Yukuto Sato, and Yumi Yamaguchi-Kabata

Subjects

media_common.quotation_subject, Population, MiSeq, Statistics as Topic, Detailed data, Computational biology, Biology, computer.software_genre, Computer graphics, Data cleaning, User-Computer Interface, Data sequences, Software, Genetics, Computer Graphics, Humans, Quality (business), education, Graphical user interface, media_common, education.field_of_study, business.industry, Illumina HiSeq, Computational Biology, High-Throughput Nucleotide Sequencing, Automated analysis, Sequence Analysis, DNA, High-Throughput DNA Sequencing, NGS, Data mining, business, computer, Biotechnology

Abstract

Background Next-generation sequencers (NGSs) have become one of the main tools for current biology. To obtain useful insights from the NGS data, it is essential to control low-quality portions of the data affected by technical errors such as air bubbles in sequencing fluidics. Results We develop a software SUGAR (subtile-based GUI-assisted refiner) which can handle ultra-high-throughput data with user-friendly graphical user interface (GUI) and interactive analysis capability. The SUGAR generates high-resolution quality heatmaps of the flowcell, enabling users to find possible signals of technical errors during the sequencing. The sequencing data generated from the error-affected regions of a flowcell can be selectively removed by automated analysis or GUI-assisted operations implemented in the SUGAR. The automated data-cleaning function based on sequence read quality (Phred) scores was applied to a public whole human genome sequencing data and we proved the overall mapping quality was improved. Conclusion The detailed data evaluation and cleaning enabled by SUGAR would reduce technical problems in sequence read mapping, improving subsequent variant analysis that require high-quality sequence data and mapping results. Therefore, the software will be especially useful to control the quality of variant calls to the low population cells, e.g., cancers, in a sample with technical errors of sequencing procedures.

Published

2014

18. iSVP: an integrated structural variant calling pipeline from high-throughput sequencing data

Author

Mamoru Takahashi, Takahiro Mimori, Yumi Yamaguchi-Kabata, Kaname Kojima, Masao Nagasaki, Naoki Nariai, Yukuto Sato, and Akira Ono

Subjects

Genetics, Whole genome sequencing, Time Factors, Genome, Human, Research, Applied Mathematics, Pipeline (computing), High-Throughput Nucleotide Sequencing, Genomics, Computational biology, Biology, Genome, DNA sequencing, Computer Science Applications, Structural Biology, Modelling and Simulation, Modeling and Simulation, Humans, Human genome, 1000 Genomes Project, International HapMap Project, Molecular Biology, Algorithms, Sequence Deletion

Abstract

Background: Structural variations (SVs), such as insertions, deletions, inversions, and duplications, are a common feature in human genomes, and a number of studies have reported that such SVs are associated with human diseases. Although the progress of next generation sequencing (NGS) technologies has led to the discovery of a large number of SVs, accurate and genome-wide detection of SVs remains challenging. Thus far, various calling algorithms based on NGS data have been proposed. However, their strategies are diverse and there is no tool able to detect a full range of SVs accurately. Results: We focused on evaluating the performance of existing deletion calling algorithms for various spanning ranges from low- to high-coverage simulation data. The simulation data was generated from a whole genome sequence with artificial SVs constructed based on the distribution of variants obtained from the 1000 Genomes Project. From the simulation analysis, deletion calls of various deletion sizes were obtained with each caller, and it was found that the performance was quite different according to the type of algorithms and targeting deletion size. Based on these results, we propose an integrated structural variant calling pipeline (iSVP) that combines existing methods with a newly devised filtering and merging processes. It achieved highly accurate deletion calling with >90% precision and >90% recall on the 30× read data for a broad range of size. We applied iSVP to the whole-genome sequence data of a CEU HapMap sample, and detected a large number of deletions, including notable peaks around 300 bp and 6,000 bp, which corresponded to Alus and long interspersed nuclear elements, respectively. In addition, many of the predicted deletions were highly consistent with experimentally validated ones by other studies. Conclusions: We present iSVP, a new deletion calling pipeline to obtain a genome-wide landscape of deletions in a highly accurate manner. From simulation and real data analysis, we show that iSVP is broadly applicable to human whole-genome sequencing data, which will elucidate relationships between SVs across genomes and associated diseases or biological functions.

Published

2013

19. A statistical variant calling approach from pedigree information and local haplotyping with phase informative reads

Author

Yumi Yamaguchi-Kabata, Takahiro Mimori, Masao Nagasaki, Kaname Kojima, Mamoru Takahashi, Naoki Nariai, and Yukuto Sato

Subjects

Statistics and Probability, Genotyping Techniques, Sequence analysis, Pedigree information, Computational biology, Biology, Biochemistry, Polymorphism, Single Nucleotide, Humans, Molecular Biology, Genotyping, Sequence (medicine), Genetics, Models, Statistical, Haplotype, Genetic Variation, Coverage data, Genomics, Sequence Analysis, DNA, New variant, Computer Science Applications, Pedigree, Computational Mathematics, Computational Theory and Mathematics, Haplotypes

Abstract

Motivation: Variant calling from genome-wide sequencing data is essential for the analysis of disease-causing mutations and elucidation of disease mechanisms. However, variant calling in low coverage regions is difficult due to sequence read errors and mapping errors. Hence, variant calling approaches that are robust to low coverage data are demanded. Results: We propose a new variant calling approach that considers pedigree information and haplotyping based on sequence reads spanning two or more heterozygous positions termed phase informative reads. In our approach, genotyping and haplotyping by the assignment of each read to a haplotype based on phase informative reads are simultaneously performed. Therefore, positions with low evidence for heterozygosity are rescued by phase informative reads, and such rescued positions contribute to haplotyping in a synergistic way. In addition, pedigree information supports more accurate haplotyping as well as genotyping, especially in low coverage regions. Although heterozygous positions are useful for haplotyping, homozygous positions are not informative and weaken the information from heterozygous positions, as majority of positions are homozygous. Thus, we introduce latent variables that determine zygosity at each position to filter out homozygous positions for haplotyping. In performance evaluation with a parent–offspring trio sequencing data, our approach outperforms existing approaches in accuracy on the agreement with single nucleotide polymorphism array genotyping results. Also, performance analysis considering distance between variants showed that the use of phase informative reads is effective for accurate variant calling, and further performance improvement is expected with longer sequencing data. Contact: nagasaki@megabank.tohoku.ac.jp or kojima@megabank.tohoku.ac.jp Supplementary information: Supplementary data are available at Bioinformatics online.

Published

2013

20. Pgltools: a genomic arithmetic tool suite for manipulation of Hi-C peak and other chromatin interaction data

Author

Erin N. Smith, Kelly A. Frazer, Paola Benaglio, He Li, Naoki Nariai, and William W. Greenwald

Subjects

0301 basic medicine, Source code, Paired-genomic-loci, Computer science, computer.software_genre, Genome, Biochemistry, Mathematical Sciences, 0302 clinical medicine, Structural Biology, Cross-platform, lcsh:QH301-705.5, media_common, computer.programming_language, Programming language, Applied Mathematics, Suite, High-Throughput Nucleotide Sequencing, Genomics, Biological Sciences, File format, Chromatin, Computer Science Applications, Networking and Information Technology R&D, Hi-CChIA-PET, lcsh:R858-859.7, Data mining, Biotechnology, Chromatin Immunoprecipitation, Bioinformatics, media_common.quotation_subject, lcsh:Computer applications to medicine. Medical informatics, Data type, 03 medical and health sciences, Information and Computing Sciences, Genetics, Molecular Biology, Unix, Chromatin conformation capture, Human Genome, Python (programming language), Bedtools, 030104 developmental biology, ComputingMethodologies_PATTERNRECOGNITION, lcsh:Biology (General), Tool suite, Genetic Loci, Genomic arithmetic, computer, 030217 neurology & neurosurgery, Software, Peak

Abstract

Genomic interaction studies use next-generation sequencing (NGS) to examine the interactions between two loci on the genome, with subsequent bioinformatics analyses typically including annotation, intersection, and merging of data from multiple experiments. While many file types and analysis tools exist for storing and manipulating single locus NGS data, there is currently no file standard or analysis tool suite for manipulating and storing paired-genomic-loci: the data type resulting from “genomic interaction” studies. As genomic interaction sequencing data are becoming prevalent, a standard file format and tools for working with these data conveniently and efficiently are needed. This article details a file standard and novel software tool suite for working with paired-genomic-loci data. We present the paired-genomic-loci (PGL) file standard for genomic-interactions data, and the accompanying analysis tool suite “pgltools”: a cross platform, pypy compatible python package available both as an easy-to-use UNIX package, and as a python module, for integration into pipelines of paired-genomic-loci analyses. Pgltools is a freely available, open source tool suite for manipulating paired-genomic-loci data. Source code, an in-depth manual, and a tutorial are available publicly at www.github.com/billgreenwald/pgltools , and a python module of the operations can be installed from PyPI via the PyGLtools module.

Published

2017

21. Transposon mutagenesis identifies genes that transform neural stem cells into glioma-initiating cells

Author

Naoki Nariai, Alistair G. Rust, Nancy A. Jenkins, Hideto Koso, Haruna Takeda, Neal G. Copeland, David J. Adams, Jerrold M. Ward, Masao Nagasaki, Sumiko Watanabe, Christopher Chin Kuan Yew, and Kazuko Ueno

Subjects

Transposable element, Genetics, Multidisciplinary, Brain Neoplasms, Mesenchymal stem cell, Mutagenesis (molecular biology technique), Biology, Neural stem cell, Cell biology, nervous system diseases, Transplantation, Mice, Cell Transformation, Neoplastic, Neural Stem Cells, PNAS Plus, Mutagenesis, DNA Transposable Elements, Animals, Humans, Transposon mutagenesis, Progenitor cell, Glioblastoma, Immortalised cell line

Abstract

Neural stem cells (NSCs) are considered to be the cell of origin of glioblastoma multiforme (GBM). However, the genetic alterations that transform NSCs into glioma-initiating cells remain elusive. Using a unique transposon mutagenesis strategy that mutagenizes NSCs in culture, followed by additional rounds of mutagenesis to generate tumors in vivo, we have identified genes and signaling pathways that can transform NSCs into glioma-initiating cells. Mobilization of Sleeping Beauty transposons in NSCs induced the immortalization of astroglial-like cells, which were then able to generate tumors with characteristics of the mesenchymal subtype of GBM on transplantation, consistent with a potential astroglial origin for mesenchymal GBM. Sequence analysis of transposon insertion sites from tumors and immortalized cells identified more than 200 frequently mutated genes, including human GBM-associated genes, such as Met and Nf1 , and made it possible to discriminate between genes that function during astroglial immortalization vs. later stages of tumor development. We also functionally validated five GBM candidate genes using a previously undescribed high-throughput method. Finally, we show that even clonally related tumors derived from the same immortalized line have acquired distinct combinations of genetic alterations during tumor development, suggesting that tumor formation in this model system involves competition among genetically variant cells, which is similar to the Darwinian evolutionary processes now thought to generate many human cancers. This mutagenesis strategy is faster and simpler than conventional transposon screens and can potentially be applied to any tissue stem/progenitor cells that can be grown and differentiated in vitro.

Published

2012

22. iJGVD: an integrative Japanese genome variation database based on whole-genome sequencing

Author

Masao Nagasaki, Yukuto Sato, Kaname Kojima, Minoru Tateno, Yosuke Kawai, Masayuki Yamamoto, Naoki Nariai, Jun Yasuda, Fumiki Katsuoka, and Yumi Yamaguchi-Kabata

Subjects

Genetics, Cancer genome sequencing, Whole genome sequencing, Database, Biology, computer.software_genre, Biochemistry, Genome, Genome variation, Minor allele frequency, Data Report, Molecular Biology, computer

Abstract

The integrative Japanese Genome Variation Database (iJGVD; http://ijgvd.megabank.tohoku.ac.jp/) provides genomic variation data detected by whole-genome sequencing (WGS) of Japanese individuals. Specifically, the database contains variants detected by WGS of 1,070 individuals who participated in a genome cohort study of the Tohoku Medical Megabank Project. In the first release, iJGVD includes >4,300,000 autosomal single nucleotide variants (SNVs) whose minor allele frequencies are >5.0%.

Published

2015

23. Estimating copy numbers of alleles from population-scale high-throughput sequencing data

Author

Yosuke Kawai, Kaname Kojima, Naoki Nariai, Yukuto Sato, Masao Nagasaki, Takahiro Mimori, and Yumi Yamaguchi-Kabata

Subjects

Male, DNA Copy Number Variations, Population, Locus (genetics), latent Dirichlet allocation, Biology, Biochemistry, DNA sequencing, Bayes' theorem, Structural Biology, Utah, Humans, Copy-number variation, Allele, education, Saliva, Molecular Biology, Alleles, Genetics, education.field_of_study, high-throughput sequencing data, Models, Statistical, Applied Mathematics, Haplotype, copy number variation, Computational Biology, High-Throughput Nucleotide Sequencing, Bayes Theorem, Computer Science Applications, Pedigree, Proceedings, Genetics, Population, Phenotype, Haplotypes, Amylases, Female, DNA microarray

Abstract

Background With the recent development of microarray and high-throughput sequencing (HTS) technologies, a number of studies have revealed catalogs of copy number variants (CNVs) and their association with phenotypes and complex traits. In parallel, a number of approaches to predict CNV regions and genotypes are proposed for both microarray and HTS data. However, only a few approaches focus on haplotyping of CNV loci. Results We propose a novel approach to infer copy unit alleles and their numbers in each sample simultaneously from population-scale HTS data by variational Bayesian inference on a generative probabilistic model inspired by latent Dirichlet allocation, which is a well studied model for document classification problems. In simulation studies, we evaluated concordance between inferred and true copy unit alleles for lower-, middle-, and higher-copy number dataset, in which precision and recall were ≥ 0.9 for data with mean coverage ≥ 10× per copy unit. We also applied the approach to HTS data of 1123 samples at highly variable salivary amylase gene locus and a pseudogene locus, and confirmed consistency of the estimated alleles within samples belonging to a trio of CEPH/Utah pedigree 1463 with 11 offspring. Conclusions Our proposed approach enables detailed analysis of copy number variations, such as association study between copy unit alleles and phenotypes or biological features including human diseases.

Published

2015

24. Probabilistic Protein Function Prediction from Heterogeneous Genome-Wide Data

Author

Eric D. Kolaczyk, Simon Kasif, and Naoki Nariai

Subjects

Protein domain, lcsh:Medicine, Computational biology, Biology, Cross-validation, Automation, Gene Knockout Techniques, 03 medical and health sciences, 0302 clinical medicine, Predictive Value of Tests, Protein function prediction, lcsh:Science, Critical Assessment of Function Annotation, Probability, 030304 developmental biology, Regulation of gene expression, Genetics, 0303 health sciences, Computational Biology/Systems Biology, Multidisciplinary, lcsh:R, Computational Biology, Proteins, Gene Annotation, Protein subcellular localization prediction, Phenotype, Gene Expression Regulation, lcsh:Q, 030217 neurology & neurosurgery, Research Article, Computational Biology/Genomics, DNA Damage, Genome-Wide Association Study

Abstract

Dramatic improvements in high throughput sequencing technologies have led to a staggering growth in the number of predicted genes. However, a large fraction of these newly discovered genes do not have a functional assignment. Fortunately, a variety of novel high-throughput genome-wide functional screening technologies provide important clues that shed light on gene function. The integration of heterogeneous data to predict protein function has been shown to improve the accuracy of automated gene annotation systems. In this paper, we propose and evaluate a probabilistic approach for protein function prediction that integrates protein-protein interaction (PPI) data, gene expression data, protein motif information, mutant phenotype data, and protein localization data. First, functional linkage graphs are constructed from PPI data and gene expression data, in which an edge between nodes (proteins) represents evidence for functional similarity. The assumption here is that graph neighbors are more likely to share protein function, compared to proteins that are not neighbors. The functional linkage graph model is then used in concert with protein domain, mutant phenotype and protein localization data to produce a functional prediction. Our method is applied to the functional prediction of Saccharomyces cerevisiae genes, using Gene Ontology (GO) terms as the basis of our annotation. In a cross validation study we show that the integrated model increases recall by 18%, compared to using PPI data alone at the 50% precision. We also show that the integrated predictor is significantly better than each individual predictor. However, the observed improvement vs. PPI depends on both the new source of data and the functional category to be predicted. Surprisingly, in some contexts integration hurts overall prediction accuracy. Lastly, we provide a comprehensive assignment of putative GO terms to 463 proteins that currently have no assigned function.

Published

2007

25. Identification of acquired mutations by whole-genome sequencing in GATA-2 deficiency evolving into myelodysplasia and acute leukemia

Author

Naoki Nariai, Masao Nagasaki, Takeshi Nagashima, Ryo Funayama, Hideo Harigae, Keiko Nakayama, Yoji Sasahara, Mayumi Kamata, Yasushi Onishi, Tohru Fujiwara, Noriko Fukuhara, Kaname Kojima, and Kenichi Ishizawa

Subjects

Adult, Male, DNA Mutational Analysis, Biology, medicine.disease_cause, GATA-1, GATA-2, Germline mutation, hemic and lymphatic diseases, medicine, Humans, Missense mutation, EZH2, MonoMAC, Cells, Cultured, Immunodeficiency, Genetics, Whole-genome sequencing, Mutation, Genome, Human, Myelodysplastic syndromes, GATA-2 deficiency, High-Throughput Nucleotide Sequencing, Myeloid leukemia, General Medicine, Hematology, medicine.disease, GATA2 Transcription Factor, Leukemia, Leukemia, Myeloid, Myelodysplastic Syndromes, Acute Disease, Disease Progression, Cancer research, Original Article, K562 Cells, Myelodysplastic syndrome

Abstract

Heterozygous GATA-2 germline mutations are associated with overlapping clinical manifestations termed GATA-2 deficiency, characterized by immunodeficiency and predisposition to myelodysplastic syndrome (MDS) and acute myeloid leukemia (AML). However, there is considerable clinical heterogeneity among patients, and the molecular basis for the evolution of immunodeficiency into MDS/AML remains unknown. Thus, we conducted whole-genome sequencing on a patient with a germline GATA-2 heterozygous mutation (c. 988 C > T; p. R330X), who had a history suggestive of immunodeficiency and evolved into MDS/AML. Analysis was conducted with DNA samples from leukocytes for immunodeficiency, bone marrow mononuclear cells for MDS and bone marrow-derived mesenchymal stem cells. Whereas we did not identify a candidate genomic deletion that may contribute to the evolution into MDS, a total of 280 MDS-specific nonsynonymous single nucleotide variants were identified. By narrowing down with the single nucleotide polymorphism database, the functional missense database, and NCBI information, we finally identified three candidate mutations for EZH2, HECW2 and GATA-1, which may contribute to the evolution of the disease. Electronic supplementary material The online version of this article (doi:10.1007/s00277-014-2090-4) contains supplementary material, which is available to authorized users.