• 제목/요약/키워드: gene regulatory networks

검색결과 57건 처리시간 0.019초

G-Networks Based Two Layer Stochastic Modeling of Gene Regulatory Networks with Post-Translational Processes

  • Kim, Ha-Seong;Gelenbe, Erol
    • Interdisciplinary Bio Central
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    • 제3권2호
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    • pp.8.1-8.6
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    • 2011
  • Background: Thanks to the development of the mathematical/statistical reverse engineering and the high-throughput measuring biotechnology, lots of biologically meaningful genegene interaction networks have been revealed. Steady-state analysis of these systems provides an important clue to understand and to predict the systematic behaviours of the biological system. However, modeling such a complex and large-scale system is one of the challenging difficulties in systems biology. Results: We introduce a new stochastic modeling approach that can describe gene regulatory mechanisms by dividing two (DNA and protein) layers. Simple queuing system is employed to explain the DNA layer and the protein layer is modeled using G-networks which enable us to account for the post-translational protein interactions. Our method is applied to a transcription repression system and an active protein degradation system. The steady-state results suggest that the active protein degradation system is more sensitive but the transcription repression system might be more reliable than the transcription repression system. Conclusions: Our two layer stochastic model successfully describes the long-run behaviour of gene regulatory networks which consist of various mRNA/protein processes. The analytic solution of the G-networks enables us to extend our model to a large-scale system. A more reliable modeling approach could be achieved by cooperating with a real experimental study in synthetic biology.

빈발 유전자 발현 패턴과 연쇄 규칙을 이용한 유전자 조절 네트워크 구축 (Constructing Gene Regulatory Networks using Frequent Gene Expression Pattern and Chain Rules)

  • 이헌규;류근호;정두영
    • 정보처리학회논문지D
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    • 제14D권1호
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    • pp.9-20
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    • 2007
  • 유전자들의 그룹은 복잡한 상호작용들을 통해 세포의 기능이 조절되며 이러한 상호작용을 하는 유전자 그룹들을 유전자 조절 네트워크 (GRNs: Gene Regulatory Networks)라고 한다. 이전의 유전자 발현 분석 기법인 군집화와 분류는 단지 상동성에 의한 유전자들 사이의 소속을 결정하는 데에는 유용하나 분자 활동에서의 같은 클래스에서 발견되어지는 유전자들 사이의 조절 관계를 식별할 수 없다. 더욱이 유전자들이 어떻게 연관되는 지와 유전자들이 서로 어떻게 조절하는지에 대한 매커니즘의 이해가 필요하다. 따라서 이 논문에서는 시계열 마이크로어레이 데이터로부터의 유전자들의 조절 관계를 발견하기 위해서 빈발 패턴 마이닝과 연쇄 규칙을 이용한 새로운 접근법을 제안하였다. 이 기법에서는 먼저, 빈발 패턴 마이닝 적용을 위한 적절한 데이터 변환 방법을 제안하였고 FP-growth을 이용하여 유전자 발현 패턴들을 발견한다. 그런 다음, 연쇄 규칙을 이용하여 빈발한 유전자 패턴들로부터 유전자 조절 네트워크를 구축하였다. 마지막으로 제안된 기법의 검증은 공개된 유전자들의 조절 관계와 실험 결과의 일치함을 보임으로써 평가하였다.

Revealing Regulatory Networks of DNA Repair Genes in S. Cerevisiae

  • Kim, Min-Sung;Lee, Do-Heon;Yi, Gwan-Su
    • Bioinformatics and Biosystems
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    • 제2권1호
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    • pp.12-16
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    • 2007
  • DNA repair means a collection of processes that a cell identifies and corrects damage to genome sequence. The DNA repair processes are important because a genome would not be able to maintain its essential cellular functions without the processes. In this research, we make some gene regulatory networks of DNA repair in S. cerevisiae to know how each gene interacts with others. Two approaches are adapted to make the networks; Bayesian Network and ARACNE. After construction of gene regulatory networks based on the two approaches, the two networks are compared to each other to predict which genes have important roles in the DNA repair processes by finding conserved interactions and looking for hubs. In addition, each interaction between genes in the networks is validated with interaction information in S. cerevisiae genome database to support the meaning of predicted interactions in the networks.

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Inference of Gene Regulatory Networks via Boolean Networks Using Regression Coefficients

  • Kim, Ha-Seong;Choi, Ho-Sik;Lee, Jae-K.;Park, Tae-Sung
    • 한국생물정보학회:학술대회논문집
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    • 한국생물정보시스템생물학회 2005년도 BIOINFO 2005
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    • pp.339-343
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    • 2005
  • Boolean networks(BN) construction is one of the commonly used methods for building gene networks from time series microarray data. However, BN has two major drawbacks. First, it requires heavy computing times. Second, the binary transformation of the microarray data may cause a loss of information. This paper propose two methods using liner regression to construct gene regulatory networks. The first proposed method uses regression based BN variable selection method, which reduces the computing time significantly in the BN construction. The second method is the regression based network method that can flexibly incorporate the interaction of the genes using continuous gene expression data. We construct the network structure from the simulated data to compare the computing times between Boolean networks and the proposed method. The regression based network method is evaluated using a microarray data of cell cycle in Caulobacter crescentus.

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무선 센서 망에서 생체 유전자 조절 네트워크를 모방한 분산적 노드 스케줄링 기법 설계 (Design of Distributed Node Scheduling Scheme Inspired by Gene Regulatory Networks for Wireless Sensor Networks)

  • 변희정
    • 한국통신학회논문지
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    • 제40권10호
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    • pp.2054-2061
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    • 2015
  • 최근 생물학적으로 영감을 받은 모델링 기술은 단순한 현장 상호작용과 제한된 정보와 함께 이들의 강인성과 확장성, 적응성에 대해 상당한 관심을 받고 있다. 이러한 모델링 기술들 중, 유전자 조절 네트워크(Gene Regulatory Networks)(GRNs)은 세포로부터 생물학적 유기체의 발생과 자연 진화에 대한 이해에서 핵심적인 역할을 하고 있다. 본 논문은 GRN 원리를 무선 센서 네트워크 시스템에 적용하고 시간지연 요건을 충족하는 동시에 에너지 균형을 달성할 수 있는 분산화된 노드 스케쥴링 설계 기법을 제안한다. 각 센서 노드는 소비된 에너지 수준과 지연시간에 반응하여 자동으로 자신의 상태를 스케줄링하며, 이는 GRN 모델에서 영감을 받은 유전자 발현과 단백질 농도 조절 모델에 의해 제어된다. 시뮬레이션 결과는 제안된 방법이 에너지 균형뿐만 아니라 원하는 시간 지연에서 성능을 달성하고 있다는 점을 보여준다.

Reverse Engineering of a Gene Regulatory Network from Time-Series Data Using Mutual Information

  • Barman, Shohag;Kwon, Yung-Keun
    • 한국정보처리학회:학술대회논문집
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    • 한국정보처리학회 2014년도 추계학술발표대회
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    • pp.849-852
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    • 2014
  • Reverse engineering of gene regulatory network is a challenging task in computational biology. To detect a regulatory relationship among genes from time series data is called reverse engineering. Reverse engineering helps to discover the architecture of the underlying gene regulatory network. Besides, it insights into the disease process, biological process and drug discovery. There are many statistical approaches available for reverse engineering of gene regulatory network. In our paper, we propose pairwise mutual information for the reverse engineering of a gene regulatory network from time series data. Firstly, we create random boolean networks by the well-known $Erd{\ddot{o}}s-R{\acute{e}}nyi$ model. Secondly, we generate artificial time series data from that network. Then, we calculate pairwise mutual information for predicting the network. We implement of our system on java platform. To visualize the random boolean network graphically we use cytoscape plugins 2.8.0.

CONSTRUCTING GENE REGULATORY NETWORK USING FREQUENT GENE EXPRESSION PATTERN MINING AND CHAIN RULES

  • Park, Hong-Kyu;Lee, Heon-Gyu;Cho, Kyung-Hwan;Ryu, Keun-Ho
    • 대한원격탐사학회:학술대회논문집
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    • 대한원격탐사학회 2006년도 Proceedings of ISRS 2006 PORSEC Volume II
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    • pp.623-626
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    • 2006
  • Group of genes controls the functioning of a cell by complex interactions. These interacting gene groups are called Gene Regulatory Networks (GRNs). Two previous data mining approaches, clustering and classification have been used to analyze gene expression data. While these mining tools are useful for determining membership of genes by homology, they don't identify the regulatory relationships among genes found in the same class of molecular actions. Furthermore, we need to understand the mechanism of how genes relate and how they regulate one another. In order to detect regulatory relationships among genes from time-series Microarray data, we propose a novel approach using frequent pattern mining and chain rule. In this approach, we propose a method for transforming gene expression data to make suitable for frequent pattern mining, and detect gene expression patterns applying FP-growth algorithm. And then, we construct gene regulatory network from frequent gene patterns using chain rule. Finally, we validated our proposed method by showing that our experimental results are consistent with published results.

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Review of Biological Network Data and Its Applications

  • Yu, Donghyeon;Kim, MinSoo;Xiao, Guanghua;Hwang, Tae Hyun
    • Genomics & Informatics
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    • 제11권4호
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    • pp.200-210
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    • 2013
  • Studying biological networks, such as protein-protein interactions, is key to understanding complex biological activities. Various types of large-scale biological datasets have been collected and analyzed with high-throughput technologies, including DNA microarray, next-generation sequencing, and the two-hybrid screening system, for this purpose. In this review, we focus on network-based approaches that help in understanding biological systems and identifying biological functions. Accordingly, this paper covers two major topics in network biology: reconstruction of gene regulatory networks and network-based applications, including protein function prediction, disease gene prioritization, and network-based genome-wide association study.

Inferring candidate regulatory networks in human breast cancer cells

  • Jung, Ju-Hyun;Lee, Do-Heon
    • Bioinformatics and Biosystems
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    • 제2권1호
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    • pp.24-27
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    • 2007
  • Human cell regulatory mechanism is one of suspicious problems among biologists. Here we tried to uncover the human breast cancer cell regulatory mechanism from gene expression data (Marc J. Van de vijver, et. al., 2002) using a module network algorithm which is suggested by Segal, et. al.(2003) Finally, we derived a module network which consists of 50 modules and 10 tree depths. Moreover, to validate this candidate network, we applied a GO enrichment test and known transcription factor-target relationships from Transfac(R) (V. Matys, et. al, 2006) and HPRD database (Peri, S. et al., 2003).

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An integrated Bayesian network framework for reconstructing representative genetic regulatory networks.

  • Lee, Phil-Hyoun;Lee, Do-Heon;Lee, Kwang-Hyung
    • 한국생물정보학회:학술대회논문집
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    • 한국생물정보시스템생물학회 2003년도 제2차 연례학술대회 발표논문집
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    • pp.164-169
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    • 2003
  • In this paper, we propose the integrated Bayesian network framework to reconstruct genetic regulatory networks from genome expression data. The proposed model overcomes the dimensionality problem of multivariate analysis by building coherent sub-networks from confined gene clusters and combining these networks via intermediary points. Gene Shaving algorithm is used to cluster genes that share a common function or co-regulation. Retrieved clusters incorporate prior biological knowledge such as Gene Ontology, pathway, and protein protein interaction information for extracting other related genes. With these extended gene list, system builds genetic sub-networks using Bayesian network with MDL score and Sparse Candidate algorithm. Identifying functional modules of genes is done by not only microarray data itself but also well-proved biological knowledge. This integrated approach can improve there liability of a network in that false relations due to the lack of data can be reduced. Another advantage is the decreased computational complexity by constrained gene sets. To evaluate the proposed system, S. Cerevisiae cell cycle data [1] is applied. The result analysis presents new hypotheses about novel genetic interactions as well as typical relationships known by previous researches [2].

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