MAnorm2 for quantitatively comparing groups of ChIP-seq samples

Tu, Shiqi; Li, Mushan; Tan, Fengxiang; Chen, Haojie; Xu, Jian; Waxman, David J.; Zhang, Yijing; Shao, Zongping

doi:10.1101/2020.01.07.896894

Cited by 6 publications

(13 citation statements)

References 44 publications

(39 reference statements)

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“…A count matrix and an occupancy matrix have been constructed for each data set by using MAnorm2_utils (v1.0.0) [24]. Rows and columns of both matrices corresponded .…”

Section: Input Matrices For Normalizationmentioning

confidence: 99%

“…Broad merged peaks were then divided up into consecutive bins, and narrow ones were left as they were. As for normalization, we constructed a pseudo-reference profile by averaging all the samples, and invoked the MA normalization procedure implemented in MAnorm2 [24] to normalize each sample against it (see Methods). Note also that, unless otherwise stated, each hypervariable analysis in this study targeting an individual data set has separately handled proximal and distal regions.…”

Section: Ranking Genomic Regions Based On Scaled Variancesmentioning

confidence: 99%

“…A complete statistical model specifying the null distribution of the scaled variances is required for assessing their statistical significances. We previously developed MAnorm2 for differential ChIP-seq analysis [24]. In HyperChIP, we follow the distributional theory proposed by MAnorm2 for modeling a group of ChIP-seq samples.…”

Section: Hvrsmentioning

confidence: 99%

“…A count matrix and an occupancy matrix have been constructed for each data set by using MAnorm2_utils (v1.0.0) [24]. Rows and columns of both matrices corresponded to a list of genomic regions and the related ChIP/ATAC-seq samples, respectively.…”

Section: Input Matrices For Normalizationmentioning

confidence: 99%

“…For example, sequencing count data are inherently associated with a strong dependence of signal variability on the mean signal intensity, making the ChIP/ATAC-seq signal variability of different genomic regions not directly comparable with each other. Specifically, after a logarithmic transformation, small log-counts tend to have larger variances than large log-counts [23,24]. While this mean-variability relationship has been properly accounted for in almost all the tools for calling HVGs from scRNA-seq data, several studies called hypervariable ChIP/ATAC-seq signals by ranking genomic regions based on some variability index without considering its dependence on the mean signal intensity [9,10,19,21,22].…”

Section: Introductionmentioning

confidence: 99%

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HyperChIP for identifying hypervariable signals across ChIP/ATAC-seq samples

Chen

Yuan

et al. 2021

Preprint

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With the reduction in sequencing costs, studies become prevalent that profile the chromatin landscape for tens or even hundreds of human individuals by using ChIP/ATAC-seq techniques. Identifying genomic regions with hypervariable ChIP/ATAC-seq signals across given samples is essential for such studies. In particular, the hypervariable regions (HVRs) across tumors from different patients indicate their heterogeneity and can contribute to revealing potential cancer subtypes and the associated epigenetic markers. We present HyperChIP as the first complete statistical tool for the task. HyperChIP uses scaled variances that account for the mean-variance dependence to rank genomic regions, and it increases the statistical power by diminishing the influence of true HVRs on model fitting. Applying it to a large pan-cancer ATAC-seq data set, we found that the identified HVRs not only provided a solid basis to uncover the underlying similarity structure among the involved tumor samples, but also led to the identification of transcription factors pertaining to the similarity structure when coupled with a motif-scanning analysis.

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“…A count matrix and an occupancy matrix have been constructed for each data set by using MAnorm2_utils (v1.0.0) [24]. Rows and columns of both matrices corresponded .…”

Section: Input Matrices For Normalizationmentioning

confidence: 99%

Section: Ranking Genomic Regions Based On Scaled Variancesmentioning

confidence: 99%

Section: Hvrsmentioning

confidence: 99%

Section: Input Matrices For Normalizationmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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HyperChIP for identifying hypervariable signals across ChIP/ATAC-seq samples

Chen

Yuan

et al. 2021

Preprint

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Enhancer–promoter interactions and transcription are largely maintained upon acute loss of CTCF, cohesin, WAPL or YY1

et al. 2022

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It remains unclear why acute depletion of CTCF (CCCTC-binding factor) and cohesin only marginally affects expression of most genes despite substantially perturbing three-dimensional (3D) genome folding at the level of domains and structural loops. To address this conundrum, we used high-resolution Micro-C and nascent transcript profiling in mouse embryonic stem cells. We find that enhancer–promoter (E–P) interactions are largely insensitive to acute (3-h) depletion of CTCF, cohesin or WAPL. YY1 has been proposed as a structural regulator of E–P loops, but acute YY1 depletion also had minimal effects on E–P loops, transcription and 3D genome folding. Strikingly, live-cell, single-molecule imaging revealed that cohesin depletion reduced transcription factor (TF) binding to chromatin. Thus, although CTCF, cohesin, WAPL or YY1 is not required for the short-term maintenance of most E–P interactions and gene expression, our results suggest that cohesin may facilitate TFs to search for and bind their targets more efficiently.

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Obox4promotes zygotic genome activation upon loss ofDux

Guo

Kitano

Murano

et al. 2022

Preprint

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Once fertilized, mouse zygotes rapidly proceed to zygotic genome activation (ZGA), during which long terminal repeats (LTRs) of murine endogenous retroviruses with leucine tRNA primer (MERVL) are potently activated by a conserved homeodomain-containing pioneer factor, DUX. However, Dux-knockout embryos produce fertile mice, suggesting that ZGA is redundantly driven by unknown factor(s). In the present study, we report that the multicopy mouse homeobox gene, Obox4, encodes a transcription factor that redundantly drives ZGA. OBOX4 is highly expressed in mouse 2-cell embryos. Single knockdown of Obox4 or Dux is tolerated by embryogenesis, whereas Obox4/Dux double knockdown completely compromises embryonic development. Genome-wide epigenetic profiling revealed that OBOX4 binds to MERVL LTRs as well as murine endogenous retroviruses with lysine tRNA primer (MERVK) LTRs, and mediates the deposition of active histone modifications. Our study identified OBOX4 as a pioneer factor that provides genetic redundancy to pre-implantation development.

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MAnorm2 for quantitatively comparing groups of ChIP-seq samples

Cited by 6 publications

References 44 publications

HyperChIP for identifying hypervariable signals across ChIP/ATAC-seq samples

HyperChIP for identifying hypervariable signals across ChIP/ATAC-seq samples

Enhancer–promoter interactions and transcription are largely maintained upon acute loss of CTCF, cohesin, WAPL or YY1

Obox4promotes zygotic genome activation upon loss ofDux

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