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A comprehensive interaction study provides a potential domain interaction network of human death domain superfamily proteins
Authors:Wei Zhou  Naoe Kaneko  Tomoya Nakagita  Hiroyuki Takeda  Junya Masumoto
Affiliation:1.Department of Analytical Pathology, Ehime University Graduate School of Medicine, Toon, Ehime Japan ;2.Division of Proteo-Drug-Discovery Sciences, Ehime University Proteo-Science Center, Matsuyama, Ehime Japan ;3.Division of Pathology, Ehime University Proteo-Science Center, Toon, Ehime Japan
Abstract:Human death domain superfamily proteins (DDSPs) play important roles in many signaling pathways involved in cell death and inflammation. Disruption or constitutive activation of these DDSP interactions due to inherited gene mutations is closely related to immunodeficiency and/or autoinflammatory diseases; however, responsible gene mutations have not been found in phenotypical diagnosis of these diseases. In this study, we comprehensively investigated the interactions of death-fold domains to explore the signaling network mediated by human DDSPs. We obtained 116 domains of DDSPs and conducted a domain–domain interaction assay of 13,924 reactions in duplicate using amplified luminescent proximity homogeneous assay. The data were mostly consistent with previously reported interactions. We also found new possible interactions, including an interaction between the caspase recruitment domain (CARD) of CARD10 and the tandem CARD–CARD domain of NOD2, which was confirmed by reciprocal co-immunoprecipitation. This study enables prediction of the interaction network of human DDSPs, sheds light on pathogenic mechanisms, and will facilitate identification of drug targets for treatment of immunodeficiency and autoinflammatory diseases.Subject terms: Cell death and immune response, Rheumatic diseases
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