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Protein localization as a principal feature of the etiology and comorbidity of genetic diseases

Author:: Park, Solip Yang, Jae-Seong Shin, Young-Eun Park, Juyong Jang, Sung Key Kim, Sanguk
Journal:: MOLECULAR SYSTEMS BIOLOGY
Issue Date:: 2011
Abstract(summary):: Proteins targeting the same subcellular localization tend to participate in mutual protein-protein interactions (PPIs) and are often functionally associated. Here, we investigated the relationship between disease-associated proteins and their subcellular localizations, based on the assumption that protein pairs associated with phenotypically similar diseases are more likely to be connected via subcellular localization. The spatial constraints from subcellular localization significantly strengthened the disease associations of the proteins connected by subcellular localizations. In particular, certain disease types were more prevalent in specific subcellular localizations. We analyzed the enrichment of disease phenotypes within subcellular localizations, and found that there exists a significant correlation between disease classes and subcellular localizations. Furthermore, we found that two diseases displayed high comorbidity when disease-associated proteins were connected via subcellular localization. We newly explained 7584 disease pairs by using the context of protein subcellular localization, which had not been identified using shared genes or PPIs only. Our result establishes a direct correlation between protein subcellular localization and disease association, and helps to understand the mechanism of human disease progression. Molecular Systems Biology 7: 494; published online 24 May 2011; doi: 10.1038/msb.2011.29

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References

No genotype left untreated[J]. NATURE GENETICS,2004:429---430.
Botstein, D, Risch, N. Discovering genotypes underlying human phenotypes: past successes for mendelian disease, future approaches for complex disease[J]. NATURE GENETICS,2003:228---237.
Su, AI, Wiltshire, T, Batalov, S, Lapp, H, Ching, KA, Block, D, Zhang, J, Soden, R, Hayakawa, M, Kreiman, G, Cooke, MP, Walker, JR, Hogenesch, JB. A gene atlas of the mouse and human protein-encoding transcriptomes[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA,2004:6062---6067.
Olpin, SE. Implications of impaired ketogenesis in fatty acid oxidation disorders[J]. PROSTAGLANDINS LEUKOTRIENES AND ESSENTIAL FATTY ACIDS,2004:293---308.
Winter, EE, Goodstadt, L, Ponting, CP. Elevated rates of protein secretion, evolution, and disease among tissue-specific genes[J]. GENOME RESEARCH,2004:54---61.
Koot, BGP, Houwen, R, Pot, DJ, Nauta, J. Congenital analbuminaemia: biochemical and clinical implications. A case report and literature review[J]. EUROPEAN JOURNAL OF PEDIATRICS,2004:664---670.
Broeckel, U, Schork, NJ. Identifying genes and genetic variation underlying human diseases and complex phenotypes via recombination mapping[J]. JOURNAL OF PHYSIOLOGY-LONDON,2004:40---45.
Bodenreider, O. The Unified Medical Language System (UMLS): integrating biomedical terminology[J]. NUCLEIC ACIDS RESEARCH,2004:D267---D270.
Szafron, D, Lu, P, Greiner, R, Wishart, DS, Poulin, B, Eisner, R, Lu, Z, Anvik, J, Macdonell, C, Fyshe, A, Meeuwis, D. Proteome Analyst: custom predictions with explanations in a web-based tool for high-throughput proteome annotations[J]. NUCLEIC ACIDS RESEARCH,2004:W365---W371.
Kau, TR, Way, JC, Silver, PA. Nuclear transport and cancer: From mechanism to intervention[J]. NATURE REVIEWS CANCER,2004:106---117.

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Chi, Sang-Mun, Dougu Nam. WegoLoc: accurate prediction of protein subcellular localization using weighted Gene Ontology terms[J]. BIOINFORMATICS,2012:1028---1030.
Park, Solip, Yang, Jae-Seong, Kim, Jinho, Shin, Young-Eun, Hwang, Jihye, Park, Juyong, Jang, Sung Key, Kim, Sanguk. Evolutionary history of human disease genes reveals phenotypic connections and comorbidity among genetic diseases[J]. SCIENTIFIC REPORTS,2012
Yang, Jae-Seong, Kim, Jinho, Park, Solip, Jeon, Jouhyun, Shin, Young-Eun, Kim, Sanguk. Spatial and functional organization of mitochondrial protein network[J]. SCIENTIFIC REPORTS,2013
Furlong, Laura I.. Human diseases through the lens of network biology[J]. TRENDS IN GENETICS,2013:150---159.
Psychiatric comorbidity and causal disease models[J]. Preventive Medicine,2013:748---752.
Nuclear tropomyosin and troponin in striated muscle: new roles in a new locale?[J]. Journal of Muscle Research and Cell Motility,2013:275---284.
Mass-spectrometry-based spatial proteomics data analysis using pRoloc and pRolocdata[J]. Bioinformatics (Oxford),2014:1322---1324.
Human Proteins with Target Sites of Multiple Post-Translational Modification Types Are More Prone to Be Involved in Disease[J]. Journal of Proteome Research,2014:2735---2748.
Inference of dynamic networks using time-course data[J]. Briefings in Bioinformatics,2014:212---228.
Insights into pathophysiology of dystropy through the analysis of gene networks: an example of bronchial asthma and tuberculosis[J]. Immunogenetics,2014:457---465.

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