Your search keyword '"CAO Han"' showing total 4 results

1. Multi-platform discovery of haplotype-resolved structural variation in human genomes.

Author

Chaisson, Mark JP, Sanders, Ashley D, Zhao, Xuefang, Malhotra, Ankit, Porubsky, David, Rausch, Tobias, Gardner, Eugene J, Rodriguez, Oscar L, Guo, Li, Collins, Ryan L, Fan, Xian, Wen, Jia, Handsaker, Robert E, Fairley, Susan, Kronenberg, Zev N, Kong, Xiangmeng, Hormozdiari, Fereydoun, Lee, Dillon, Wenger, Aaron M, Hastie, Alex R, Antaki, Danny, Anantharaman, Thomas, Audano, Peter A, Brand, Harrison, Cantsilieris, Stuart, Cao, Han, Cerveira, Eliza, Chen, Chong, Chen, Xintong, Chin, Chen-Shan, Chong, Zechen, Chuang, Nelson T, Lambert, Christine C, Church, Deanna M, Clarke, Laura, Farrell, Andrew, Flores, Joey, Galeev, Timur, Gorkin, David U, Gujral, Madhusudan, Guryev, Victor, Heaton, William Haynes, Korlach, Jonas, Kumar, Sushant, Kwon, Jee Young, Lam, Ernest T, Lee, Jong Eun, Lee, Joyce, Lee, Wan-Ping, Lee, Sau Peng, Li, Shantao, Marks, Patrick, Viaud-Martinez, Karine, Meiers, Sascha, Munson, Katherine M, Navarro, Fabio CP, Nelson, Bradley J, Nodzak, Conor, Noor, Amina, Kyriazopoulou-Panagiotopoulou, Sofia, Pang, Andy WC, Qiu, Yunjiang, Rosanio, Gabriel, Ryan, Mallory, Stütz, Adrian, Spierings, Diana CJ, Ward, Alistair, Welch, AnneMarie E, Xiao, Ming, Xu, Wei, Zhang, Chengsheng, Zhu, Qihui, Zheng-Bradley, Xiangqun, Lowy, Ernesto, Yakneen, Sergei, McCarroll, Steven, Jun, Goo, Ding, Li, Koh, Chong Lek, Ren, Bing, Flicek, Paul, Chen, Ken, Gerstein, Mark B, Kwok, Pui-Yan, Lansdorp, Peter M, Marth, Gabor T, Sebat, Jonathan, Shi, Xinghua, Bashir, Ali, Ye, Kai, Devine, Scott E, Talkowski, Michael E, Mills, Ryan E, Marschall, Tobias, Korbel, Jan O, Eichler, Evan E, and Lee, Charles

Subjects

Humans, Chromosome Mapping, Genomics, Haplotypes, Genome, Human, Algorithms, Databases, Genetic, INDEL Mutation, Genomic Structural Variation, High-Throughput Nucleotide Sequencing, Whole Genome Sequencing, Genome, Human, Databases, Genetic

Abstract

The incomplete identification of structural variants (SVs) from whole-genome sequencing data limits studies of human genetic diversity and disease association. Here, we apply a suite of long-read, short-read, strand-specific sequencing technologies, optical mapping, and variant discovery algorithms to comprehensively analyze three trios to define the full spectrum of human genetic variation in a haplotype-resolved manner. We identify 818,054 indel variants (

Published

2019

2. Genome maps across 26 human populations reveal population-specific patterns of structural variation.

Author

Levy-Sakin, Michal, Pastor, Steven, Mostovoy, Yulia, Li, Le, Leung, Alden KY, McCaffrey, Jennifer, Young, Eleanor, Lam, Ernest T, Hastie, Alex R, Wong, Karen HY, Chung, Claire YL, Ma, Walfred, Sibert, Justin, Rajagopalan, Ramakrishnan, Jin, Nana, Chow, Eugene YC, Chu, Catherine, Poon, Annie, Lin, Chin, Naguib, Ahmed, Wang, Wei-Ping, Cao, Han, Chan, Ting-Fung, Yip, Kevin Y, Xiao, Ming, and Kwok, Pui-Yan

Subjects

Chromosomes, Human, Y, Humans, Chromosome Mapping, Sequence Analysis, DNA, Computational Biology, Genomics, Phylogeny, Base Sequence, Gene Dosage, Mutation, Genome, Human, Algorithms, Female, Male, Genomic Structural Variation, Segmental Duplications, Genomic, Genetic Linkage, Chromosomes, Human, Y, Sequence Analysis, DNA, Genome, Segmental Duplications, Genomic

Abstract

Large structural variants (SVs) in the human genome are difficult to detect and study by conventional sequencing technologies. With long-range genome analysis platforms, such as optical mapping, one can identify large SVs (>2 kb) across the genome in one experiment. Analyzing optical genome maps of 154 individuals from the 26 populations sequenced in the 1000 Genomes Project, we find that phylogenetic population patterns of large SVs are similar to those of single nucleotide variations in 86% of the human genome, while ~2% of the genome has high structural complexity. We are able to characterize SVs in many intractable regions of the genome, including segmental duplications and subtelomeric, pericentromeric, and acrocentric areas. In addition, we discover ~60 Mb of non-redundant genome content missing in the reference genome sequence assembly. Our results highlight the need for a comprehensive set of alternate haplotypes from different populations to represent SV patterns in the genome.

Published

2019

3. Whole-genome mutational burden analysis of three pluripotency induction methods

Author

Bhutani, Kunal, primary, Nazor, Kristopher L., additional, Williams, Roy, additional, Tran, Ha, additional, Dai, Heng, additional, Džakula, Željko, additional, Cho, Edward H., additional, Pang, Andy W. C., additional, Rao, Mahendra, additional, Cao, Han, additional, Schork, Nicholas J., additional, and Loring, Jeanne F., additional

Published

2016

4. Genome assembly and geospatial phylogenomics of the bed bug Cimex lectularius

Author

Rosenfeld, Jeffrey A., primary, Reeves, Darryl, additional, Brugler, Mercer R., additional, Narechania, Apurva, additional, Simon, Sabrina, additional, Durrett, Russell, additional, Foox, Jonathan, additional, Shianna, Kevin, additional, Schatz, Michael C., additional, Gandara, Jorge, additional, Afshinnekoo, Ebrahim, additional, Lam, Ernest T., additional, Hastie, Alex R., additional, Chan, Saki, additional, Cao, Han, additional, Saghbini, Michael, additional, Kentsis, Alex, additional, Planet, Paul J., additional, Kholodovych, Vladyslav, additional, Tessler, Michael, additional, Baker, Richard, additional, DeSalle, Rob, additional, Sorkin, Louis N., additional, Kolokotronis, Sergios-Orestis, additional, Siddall, Mark E., additional, Amato, George, additional, and Mason, Christopher E., additional

Published

2016