Sequence-based multiscale modeling for high-throughput chromosome conformation capture (Hi-C) data analysis
In this paper, we introduce sequence-based multiscale modeling for biomolecular data analysis. We employ spectral clustering method in our modeling and reveal the difference between sequence-based global scale clustering and local scale clustering. Essentially, two types of distances, i.e., Euclidea...
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sg-ntu-dr.10356-880442023-02-28T17:00:12Z Sequence-based multiscale modeling for high-throughput chromosome conformation capture (Hi-C) data analysis Xia, Kelin Qin, Zhaohui School of Biological Sciences School of Physical and Mathematical Sciences Chromosome Data Analysis In this paper, we introduce sequence-based multiscale modeling for biomolecular data analysis. We employ spectral clustering method in our modeling and reveal the difference between sequence-based global scale clustering and local scale clustering. Essentially, two types of distances, i.e., Euclidean (or spatial) distance and genomic (or sequential) distance, can be used in data clustering. Clusters from sequence-based global scale models optimize spatial distances, meaning spatially adjacent loci are more likely to be assigned into the same cluster. Sequence-based local scale models, on the other hand, result in clusters that optimize genomic distances. That is to say, in these models, sequentially adjoining loci tend to be cluster together. We propose two sequence-based multiscale models (SeqMMs) for the study of chromosome hierarchical structures, including genomic compartments and topological associated domains (TADs). We find that genomic compartments are determined only by global scale information in the Hi-C data. The removal of all the local interactions within a band region as large as 10 Mb in genomic distance has almost no significant influence on the final compartment results. Further, in TAD analysis, we find that when the sequential scale is small, a tiny variation of diagonal band region in a contact map will result in a great change in the predicted TAD boundaries. When the scale value is larger than a threshold value, the TAD boundaries become very consistent. This threshold value is highly related to TAD sizes. By the comparison of our results with those previously obtained using a spectral clustering model, we find that our method is more robust and reliable. Finally, we demonstrate that almost all TAD boundaries from both clustering methods are local minimum of a TAD summation function. MOE (Min. of Education, S’pore) Published version 2018-03-06T09:14:29Z 2019-12-06T16:54:49Z 2018-03-06T09:14:29Z 2019-12-06T16:54:49Z 2018 Journal Article Xia, K. (2018). Sequence-based multiscale modeling for high-throughput chromosome conformation capture (Hi-C) data analysis. PLOS ONE, 13(2), e0191899-. https://hdl.handle.net/10356/88044 http://hdl.handle.net/10220/44517 10.1371/journal.pone.0191899 en PLOS ONE © 2018 The Author(s) (Public Library of Science). This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. 16 p. application/pdf |
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Chromosome Data Analysis |
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Chromosome Data Analysis Xia, Kelin Sequence-based multiscale modeling for high-throughput chromosome conformation capture (Hi-C) data analysis |
| description |
In this paper, we introduce sequence-based multiscale modeling for biomolecular data analysis. We employ spectral clustering method in our modeling and reveal the difference between sequence-based global scale clustering and local scale clustering. Essentially, two types of distances, i.e., Euclidean (or spatial) distance and genomic (or sequential) distance, can be used in data clustering. Clusters from sequence-based global scale models optimize spatial distances, meaning spatially adjacent loci are more likely to be assigned into the same cluster. Sequence-based local scale models, on the other hand, result in clusters that optimize genomic distances. That is to say, in these models, sequentially adjoining loci tend to be cluster together. We propose two sequence-based multiscale models (SeqMMs) for the study of chromosome hierarchical structures, including genomic compartments and topological associated domains (TADs). We find that genomic compartments are determined only by global scale information in the Hi-C data. The removal of all the local interactions within a band region as large as 10 Mb in genomic distance has almost no significant influence on the final compartment results. Further, in TAD analysis, we find that when the sequential scale is small, a tiny variation of diagonal band region in a contact map will result in a great change in the predicted TAD boundaries. When the scale value is larger than a threshold value, the TAD boundaries become very consistent. This threshold value is highly related to TAD sizes. By the comparison of our results with those previously obtained using a spectral clustering model, we find that our method is more robust and reliable. Finally, we demonstrate that almost all TAD boundaries from both clustering methods are local minimum of a TAD summation function. |
| author2 |
Qin, Zhaohui |
| author_facet |
Qin, Zhaohui Xia, Kelin |
| format |
Article |
| author |
Xia, Kelin |
| author_sort |
Xia, Kelin |
| title |
Sequence-based multiscale modeling for high-throughput chromosome conformation capture (Hi-C) data analysis |
| title_short |
Sequence-based multiscale modeling for high-throughput chromosome conformation capture (Hi-C) data analysis |
| title_full |
Sequence-based multiscale modeling for high-throughput chromosome conformation capture (Hi-C) data analysis |
| title_fullStr |
Sequence-based multiscale modeling for high-throughput chromosome conformation capture (Hi-C) data analysis |
| title_full_unstemmed |
Sequence-based multiscale modeling for high-throughput chromosome conformation capture (Hi-C) data analysis |
| title_sort |
sequence-based multiscale modeling for high-throughput chromosome conformation capture (hi-c) data analysis |
| publishDate |
2018 |
| url |
https://hdl.handle.net/10356/88044 http://hdl.handle.net/10220/44517 |
| _version_ |
1759853409911963648 |