Abstract
BackgroundCurrent Hi-C technologies for chromosome conformation capture allow to understand a broad spectrum of functional interactions between genome elements. Although significant progress has been made into analysis of Hi-C data to identify biologically significant features, many questions still remain open, in particular regarding potential biological significance of various topological features that are characteristic for chromatin interaction networks.ResultsIt has been previously observed that promoter capture Hi-C (PCHi-C) interaction networks tend to separate easily into well-defined connected components that can be related to certain biological functionality, however, such evidence was based on manual analysis and was limited. Here we present a novel method for analysis of chromatin interaction networks aimed towards identifying characteristic topological features of interaction graphs and confirming their potential significance in chromatin architecture. Our method automatically identifies all connected components with an assigned significance score above a given threshold. These components can be subjected afterwards to different assessment methods for their biological role and/or significance. The method was applied to the largest PCHi-C data set available to date that contains interactions for 17 haematopoietic cell types. The results demonstrate strong evidence of well-pronounced component structure of chromatin interaction networks and provide some characterisation of this component structure. We also performed an indicative assessment of potential biological significance of identified network components with the results confirming that the network components can be related to specific biological functionality.ConclusionsThe obtained results show that the topological structure of chromatin interaction networks can be well described in terms of isolated connected components of the network and that formation of these components can be often explained by biological features of functionally related gene modules. The presented method allows automatic identification of all such components and evaluation of their significance in PCHi-C dataset for 17 haematopoietic cell types. The method can be adapted for exploration of other chromatin interaction data sets that include information about sufficiently large number of different cell types, and, in principle, also for analysis of other kinds of cell type-specific networks.
Highlights
Current Hi-C technologies for chromosome conformation capture allow to understand a broad spectrum of functional interactions between genome elements
The fact that promoter capture Hi-C (PCHi-C) interaction networks G(T) separate into comparatively small connected components was already observed by the authors in [21]
In this paper we have presented a novel algorithm for analysis of chromatin interaction networks with a goal to identify characteristic topological features of interaction graphs and to ascertain their potential significance in chromatin architecture
Summary
Current Hi-C technologies for chromosome conformation capture allow to understand a broad spectrum of functional interactions between genome elements. Most of an organism’s regulatory processes originate in its own genome, two primary categories of these processes can be delineated based on whether they are interactions primarily between regions of DNA (cisregulation) or between DNA and another molecule such as a regulatory protein (trans-regulation). Both of these forms of interaction are deeply involved in the essential mechanism underlying the action of transcription factors: the promoter-enhancer interaction (PEI). A promoter and its corresponding set of enhancers are connected with the help of activator proteins and other regulatory factors, and form a small, distinctive chromatin loop [1,2,3]
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