Title of article :
Nod2-Nodosome in a Cell-Free System: Implications in Pathogenesis and Drug Discovery for Blau Syndrome and Early-Onset Sarcoidosis
Author/Authors :
Iwasaki, Tomoyuki Department of Pathology - Ehime University Proteo-Science Center and Graduate School of Medicine - Shitsukawa 454 - Toon - Ehime 791-0295 - Japan , Kaneko, Naoe Department of Pathology - Ehime University Proteo-Science Center and Graduate School of Medicine - Shitsukawa 454 - Toon - Ehime 791-0295 - Japan , Ito, Yuki Department of Pathology - Ehime University Proteo-Science Center and Graduate School of Medicine - Shitsukawa 454 - Toon - Ehime 791-0295 - Japan , Takeda, Hiroyuki Division of Cell-Free Sciences - Ehime University Proteo-Science Center - Bunkyocho 3 - Matsuyama - Ehime 790-8577 - Japan , Sawasaki, Tatsuya Division of Cell-Free Sciences - Ehime University Proteo-Science Center - Bunkyocho 3 - Matsuyama - Ehime 790-8577 - Japan , Heike, Toshio Department of Pediatrics - Kyoto University Graduate School of Medicine - Shogoin Kawaramachi 54 - Kyoto 606-8507 - Japan , Migita, Kiyoshi Clinical Research Center - Nagasaki Medical Center - Kubara 2-1001-1 - Omura - Nagasaki 856-8562 - Japan , Agematsu, Kazunaga Department of Infection and Host Defense - Shinshu University Graduate School of Medicine - Asahi 3-1-1, Matsumoto - Nagano 390-8621 - Japan , Kawakami, Atsushi Unit of Translational Medicine - Department of Immunology and Rheumatology - Nagasaki University Graduate School of Biomedical Sciences - Medicine - Sakamoto 1-7-1 - Nagasaki 852-8501 - Japan , Morikawa, Shinnosuke Department of Pathology - Ehime University Proteo-Science Center and Graduate School of Medicine - Shitsukawa 454 - Toon - Ehime 791-0295 - Japan , Mokuda, Sho Department of Pathology - Ehime University Proteo-Science Center and Graduate School of Medicine - Shitsukawa 454 - Toon - Ehime 791-0295 - Japan , Kurata, Mie Department of Pathology - Ehime University Proteo-Science Center and Graduate School of Medicine - Shitsukawa 454 - Toon - Ehime 791-0295 - Japan , Masumoto, Junya Department of Pathology - Ehime University Proteo-Science Center and Graduate School of Medicine - Shitsukawa 454 - Toon - Ehime 791-0295 - Japan
Pages :
7
From page :
1
To page :
7
Abstract :
Nucleotide-binding oligomerization domain-containing protein (Nod) 2 is an intracellular pattern recognition receptor, which recognizes muramyl dipeptide (N-Acetylmuramyl-L-Alanyl-D-Isoglutamine: MDP), a bacterial peptidoglycan component, and makes a NF-𝜅B-activating complex called nodosome with adaptor protein RICK (RIP2/RIPK2). Nod2 mutants are associated with the autoinflammatory diseases, Blau syndrome (BS)/early-onset sarcoidosis (EOS). For drug discovery of BS/EOS, we tried to develop Nod2-nodosome in a cell-free system. FLAG-tagged RICK, biotinylated-Nod2, and BS/EOS-associated Nod2 mutants were synthesized, and proximity signals between FLAG-tagged and biotinylated proteins were detected by amplified luminescent proximity homogeneous assay (ALPHA). Upon incubation with MDP, the ALPHA signal of interaction between Nod2-WT and RICK was increased in a dose-dependent manner. The ALPHA signal of interaction between RICK and the BS/EOS-associated Nod2 mutants was more significantly increased than Nod2-WT. Notably, the ALPHA signal between Nod2-WT and RICK was increased upon incubation with MDP, but not when incubated with the same concentrations, L-alanine, D-isoglutamic acid, or the MDP-D-isoform. Thus, we successfully developed Nod2-nodosome in a cell-free system reflecting its function in vivo, and it can be useful for screening Nod2-nodosome-targeted therapeutic molecules for BS/EOS and granulomatous inflammatory diseases.
Keywords :
Nod2-Nodosome , Cell-Free System , Pathogenesis , Drug Discovery , Blau Syndrome , Early-Onset Sarcoidosis
Journal title :
The Scientific World Journal
Serial Year :
2016
Full Text URL :
Record number :
2610917
Link To Document :
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