Your search keyword '"20399041"' showing total 8 results

1. Structural insights into the agonists binding and receptor selectivity of human histamine H₄ receptor

Author

50721883, 00734469, 00422410, 20399041, 60452330, Im, Dohyun, Kishikawa, Jun-ichi, Shiimura, Yuki, Hisano, Hiromi, Ito, Akane, Fujita-Fujiharu, Yoko, Sugita, Yukihiko, Noda, Takeshi, Kato, Takayuki, Asada, Hidetsugu, Iwata, So, 50721883, 00734469, 00422410, 20399041, 60452330, Im, Dohyun, Kishikawa, Jun-ichi, Shiimura, Yuki, Hisano, Hiromi, Ito, Akane, Fujita-Fujiharu, Yoko, Sugita, Yukihiko, Noda, Takeshi, Kato, Takayuki, Asada, Hidetsugu, and Iwata, So

Abstract

Histamine is a biogenic amine that participates in allergic and inflammatory processes by stimulating histamine receptors. The histamine H₄ receptor (H₄R) is a potential therapeutic target for chronic inflammatory diseases such as asthma and atopic dermatitis. Here, we show the cryo-electron microscopy structures of the H₄R-Gq complex bound with an endogenous agonist histamine or the selective agonist imetit bound in the orthosteric binding pocket. The structures demonstrate binding mode of histamine agonists and that the subtype-selective agonist binding causes conformational changes in Phe344[7.39], which, in turn, form the “aromatic slot”. The results provide insights into the molecular underpinnings of the agonism of H₄R and subtype selectivity of histamine receptors, and show that the H₄R structures may be valuable in rational drug design of drugs targeting the H₄R.

Published

2023

2. Endogenous agonist–bound S1PR3 structure reveals determinants of G protein–subtype bias

Author

20399041, 20600505, 60452330, 10208423, Maeda, Shintaro, Shiimura, Yuki, Asada, Hidetsugu, Hirata, Kunio, Luo, Fangjia, Nango, Eriko, Tanaka, Nobuo, Toyomoto, Masayasu, Inoue, Asuka, Aoki, Junken, Iwata, So, Hagiwara, Masatoshi, 20399041, 20600505, 60452330, 10208423, Maeda, Shintaro, Shiimura, Yuki, Asada, Hidetsugu, Hirata, Kunio, Luo, Fangjia, Nango, Eriko, Tanaka, Nobuo, Toyomoto, Masayasu, Inoue, Asuka, Aoki, Junken, Iwata, So, and Hagiwara, Masatoshi

Abstract

Sphingosine-1-phosphate (S1P) regulates numerous important physiological functions, including immune response and vascular integrity, via its cognate receptors (S1PR1 to S1PR5); however, it remains unclear how S1P activates S1PRs upon binding. Here, we determined the crystal structure of the active human S1PR3 in complex with its natural agonist S1P at 3.2-Å resolution. S1P exhibits an unbent conformation in the long tunnel, which penetrates through the receptor obliquely. Compared with the inactive S1PR1 structure, four residues surrounding the alkyl tail of S1P (the “quartet core”) exhibit orchestrating rotamer changes that accommodate the moiety, thereby inducing an active conformation. In addition, we reveal that the quartet core determines G protein selectivity of S1PR3. These results offer insight into the structural basis of activation and biased signaling in G protein–coupled receptors and will help the design of biased ligands for optimized therapeutics.

Published

2021

3. Structure of the dopamine D2 receptor in complex with the antipsychotic drug spiperone

Author

50721883, 20399041, 10314246, 60452330, 90391979, Im, Dohyun, Inoue, Asuka, Fujiwara, Takaaki, Nakane, Takanori, Yamanaka, Yasuaki, Uemura, Tomoko, Mori, Chihiro, Shiimura, Yuki, Kimura Terakado, Kanako, Asada, Hidetsugu, Nomura, Norimichi, Tanaka, Tomoyuki, Yamashita, Ayumi, Nango, Eriko, Tono, Kensuke, Kadji, Francois Marie Ngako, Aoki, Junken, Iwata, So, Shimamura, Tatsuro, 50721883, 20399041, 10314246, 60452330, 90391979, Im, Dohyun, Inoue, Asuka, Fujiwara, Takaaki, Nakane, Takanori, Yamanaka, Yasuaki, Uemura, Tomoko, Mori, Chihiro, Shiimura, Yuki, Kimura Terakado, Kanako, Asada, Hidetsugu, Nomura, Norimichi, Tanaka, Tomoyuki, Yamashita, Ayumi, Nango, Eriko, Tono, Kensuke, Kadji, Francois Marie Ngako, Aoki, Junken, Iwata, So, and Shimamura, Tatsuro

Abstract

In addition to the serotonin 5-HT2A receptor (5-HT2AR), the dopamine D2 receptor (D2R) is a key therapeutic target of antipsychotics for the treatment of schizophrenia. The inactive state structures of D2R have been described in complex with the inverse agonists risperidone (D2Rris) and haloperidol (D2Rhal). Here we describe the structure of human D2R in complex with spiperone (D2Rspi). In D2Rspi, the conformation of the extracellular loop (ECL) 2, which composes the ligand-binding pocket, was substantially different from those in D2Rris and D2Rhal, demonstrating that ECL2 in D2R is highly dynamic. Moreover, D2Rspi exhibited an extended binding pocket to accommodate spiperone’s phenyl ring, which probably contributes to the selectivity of spiperone to D2R and 5-HT2AR. Together with D2Rris and D2Rhal, the structural information of D2Rspi should be of value for designing novel antipsychotics with improved safety and efficacy.

Published

2020

4. Proteoliposome-based Selection of a Recombinant Antibody Fragment Against the Human M2 Muscarinic Acetylcholine Receptor.

Author

20399041, 90391979, 60452330, 10314246, Suharni, Nomura, Yayoi, Arakawa, Takatoshi, Hino, Tomoya, Abe, Hitomi, Nakada-Nakura, Yoshiko, Sato, Yumi, Iwanari, Hiroko, Shiroishi, Mitsunori, Asada, Hidetsugu, Shimamura, Tatsuro, Murata, Takeshi, Kobayashi, Takuya, Hamakubo, Takao, Iwata, So, Nomura, Norimichi, 20399041, 90391979, 60452330, 10314246, Suharni, Nomura, Yayoi, Arakawa, Takatoshi, Hino, Tomoya, Abe, Hitomi, Nakada-Nakura, Yoshiko, Sato, Yumi, Iwanari, Hiroko, Shiroishi, Mitsunori, Asada, Hidetsugu, Shimamura, Tatsuro, Murata, Takeshi, Kobayashi, Takuya, Hamakubo, Takao, Iwata, So, and Nomura, Norimichi

Abstract

The development of antibodies against human G-protein-coupled receptors (GPCRs) has achieved limited success, which has mainly been attributed to their low stability in a detergent-solubilized state. We herein describe a method that can generally be applied to the selection of phage display libraries with human GPCRs reconstituted in liposomes. A key feature of this approach is the production of biotinylated proteoliposomes that can be immobilized on the surface of streptavidin-coupled microplates or paramagnetic beads and used as a binding target for antibodies. As an example, we isolated a single chain Fv fragment from an immune phage library that specifically binds to the human M2 muscarinic acetylcholine receptor with nanomolar affinity. The selected antibody fragment recognized the GPCR in both detergent-solubilized and membrane-embedded forms, which suggests that it may be a potentially valuable tool for structural and functional studies of the GPCR. The use of proteoliposomes as immunogens and screening bait will facilitate the application of phage display to this difficult class of membrane proteins.

Published

2014

5. Structure of the human M2 muscarinic acetylcholine receptor bound to an antagonist

Author

20399041, 20311730, Haga, Kazuko, Kruse, Andrew C., Asada, Hidetsugu, Yurugi-Kobayashi, Takami, Shiroishi, Mitsunori, Zhang, Cheng, Weis, William I., Okada, Tetsuji, Kobilka, Brian K., Haga, Tatsuya, Kobayashi, Takuya, 20399041, 20311730, Haga, Kazuko, Kruse, Andrew C., Asada, Hidetsugu, Yurugi-Kobayashi, Takami, Shiroishi, Mitsunori, Zhang, Cheng, Weis, William I., Okada, Tetsuji, Kobilka, Brian K., Haga, Tatsuya, and Kobayashi, Takuya

Abstract

The parasympathetic branch of the autonomic nervous system regulates the activity ofmultiple organ systems.Muscarinic receptors are G-protein-coupled receptors that mediate the response to acetylcholine released from parasympathetic nerves1–5. Their role in the unconscious regulation of organ and central nervous system function makes them potential therapeutic targets for a broad spectrum of diseases. The M2 muscarinic acetylcholine receptor (M2 receptor) is essential for the physiological control of cardiovascular function through activation of G-protein-coupled inwardly rectifying potassiumchannels, and is of particular interest because of its extensive pharmacological characterization with both orthosteric and allosteric ligands.Herewe report the structure of the antagonistbound humanM2 receptor, the first human acetylcholine receptor to be characterized structurally, to our knowledge. The antagonist 3-quinuclidinyl-benzilate binds in the middle of a long aqueous channel extending approximately two-thirds through the membrane. The orthosteric binding pocket is formed by amino acids that are identical in all five muscarinic receptor subtypes, and shares structural homology with other functionally unrelated acetylcholine binding proteins from different species. A layer of tyrosine residues forms an aromatic cap restricting dissociation of the bound ligand. A binding site for allosteric ligands has been mapped to residues at the entrance to the binding pocket near this aromatic cap. The structure of the M2 receptor provides insights into the challenges of developing subtype-selective ligands for muscarinic receptors and their propensity for allosteric regulation.

Published

2012

6. Cysteine-to-serine shuffling using a Saccharomyces cerevisiae expression system improves protein secretion: case of a nonglycosylated mutant of miraculin, a taste-modifying protein.

Author

20399041, 90391979, 60452330, 20311730, Ito, Keisuke, Sugawara, Taishi, Koizumi, Ayako, Nakajima, Ken-ichiro, Shimizu-Ibuka, Akiko, Shiroishi, Mitsunori, Asada, Hidetsugu, Yurugi-Kobayashi, Takami, Shimamura, Tatsuro, Asakura, Tomiko, Misaka, Takumi, Iwata, So, Kobayashi, Takuya, Abe, Keiko, 20399041, 90391979, 60452330, 20311730, Ito, Keisuke, Sugawara, Taishi, Koizumi, Ayako, Nakajima, Ken-ichiro, Shimizu-Ibuka, Akiko, Shiroishi, Mitsunori, Asada, Hidetsugu, Yurugi-Kobayashi, Takami, Shimamura, Tatsuro, Asakura, Tomiko, Misaka, Takumi, Iwata, So, Kobayashi, Takuya, and Abe, Keiko

Abstract

PURPOSE OF WORK: Soluble protein expression is an important first step during various types of protein studies. Here, we present the screening strategy of secretable mutant. The strategy aimed to identify those cysteine residues that provoke protein misfolding in the heterologous expression system. Intentional mutagenesis studies should consider the size of the library and the time required for expression screening. Here, we proposed a cysteine-to-serine shuffling mutation strategy (CS shuffling) using a Saccharomyces cerevisiae expression system. This strategy of site-directed shuffling mutagenesis of cysteine-to-serine residues aims to identify the cysteine residues that cause protein misfolding in heterologous expression. In the case of a nonglycosylated mutant of the taste-modifying protein miraculin (MCL), which was used here as a model protein, 25% of all constructs obtained from CS shuffling expressed MCL mutant, and serine mutations were found at Cys47 or Cys92, which are involved in the formation of the disulfide bond. This indicates that these residues had the potential to provoke protein misfolding via incorrect disulfide bonding. The CS shuffling can be performed using a small library and within one week, and is an effective screening strategy of soluble protein expression.

Published

2011

7. Cloning, expression and purification of the anion exchanger 1 homologue from the basidiomycete Phanerochaete chrysosporium.

Author

90391979, 20399041, 10314246, 60452330, 20311730, Tokuda, Natsuko, Igarashi, Kiyohiko, Shimamura, Tatsuro, Yurugi-Kobayashi, Takami, Shiroishi, Mitsunori, Ito, Keisuke, Sugawara, Taishi, Asada, Hidetsugu, Murata, Takeshi, Nomura, Norimichi, Iwata, So, Kobayashi, Takuya, 90391979, 20399041, 10314246, 60452330, 20311730, Tokuda, Natsuko, Igarashi, Kiyohiko, Shimamura, Tatsuro, Yurugi-Kobayashi, Takami, Shiroishi, Mitsunori, Ito, Keisuke, Sugawara, Taishi, Asada, Hidetsugu, Murata, Takeshi, Nomura, Norimichi, Iwata, So, and Kobayashi, Takuya

Published

2011

8. Bulky high-mannose-type N-glycan blocks the taste-modifying activity of miraculin.

Author

20399041, 90391979, 60452330, 20311730, Ito, Keisuke, Sugawara, Taishi, Koizumi, Ayako, Nakajima, Ken-Ichiro, Shimizu-Ibuka, Akiko, Shiroishi, Mitsunori, Asada, Hidetsugu, Yurugi-Kobayashi, Takami, Shimamura, Tatsuro, Asakura, Tomiko, Masuda, Katsuyoshi, Ishiguro, Masaji, Misaka, Takumi, Iwata, So, Kobayashi, Takuya, Abe, Keiko, 20399041, 90391979, 60452330, 20311730, Ito, Keisuke, Sugawara, Taishi, Koizumi, Ayako, Nakajima, Ken-Ichiro, Shimizu-Ibuka, Akiko, Shiroishi, Mitsunori, Asada, Hidetsugu, Yurugi-Kobayashi, Takami, Shimamura, Tatsuro, Asakura, Tomiko, Masuda, Katsuyoshi, Ishiguro, Masaji, Misaka, Takumi, Iwata, So, Kobayashi, Takuya, and Abe, Keiko

Abstract

BACKGROUND: Miraculin (MCL) is a taste-modifying protein that converts sourness into sweetness. The molecular mechanism underlying the taste-modifying action of MCL is unknown. METHODS: Here, a yeast expression system for MCL was constructed to accelerate analysis of its structure-function relationships. The Saccharomyces cerevisiae expression system has advantages as a high-throughput analysis system, but compared to other hosts it is characterized by a relatively low level of recombinant protein expression. To alleviate this weakness, in this study we optimized the codon usage and signal-sequence as the first step. Recombinant MCL (rMCL) was expressed and purified, and the sensory taste was analyzed. RESULTS: As a result, a 2 mg/l yield of rMCL was successfully obtained. Although sensory taste evaluation showed that rMCL was flat in taste under all the pH conditions employed, taste-modifying activity similar to that of native MCL was recovered after deglycosylation. Mutagenetic analysis revealed that the N-glycan attached to Asn42 was bulky in rMCL. CONCLUSIONS: The high-mannose-type N-glycan attached in yeast blocks the taste-modifying activity of rMCL. GENERAL SIGNIFICANCE: The bulky N-glycan attached to Asn42 may cause steric hindrance in the interaction between active residues and the sweet taste receptor hT1R2/hT1R3.

Published

2010