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Structural basis for hepatitis B virus restriction by a viral receptor homologue
by
Mifune, Junki
, Watashi, Koichi
, Ikeguchi, Mitsunori
, Umezawa, Haruka
, Kusunoki, Atsuto
, Tame, Jeremy R. H.
, Yamamoto, Kenichiro
, Kobayashi, Chisa
, Park, Sam-Yong
, Takeuchi, Junko S.
, Morita, Takeshi
, Nomura, Norimichi
, Muramatsu, Masamichi
, Ishimoto, Naito
, Ekimoto, Toru
, Iwata, So
, Park, Jae-Hyun
, Shionoya, Kaho
in
101/28
/ 13/109
/ 14/34
/ 631/326/596/1550
/ 631/535/1258/1259
/ Animals
/ Bile acids
/ Bile Acids and Salts - chemistry
/ Bile Acids and Salts - metabolism
/ Binding
/ Cryoelectron Microscopy
/ Electron microscopy
/ Embedding
/ Hepatitis
/ Hepatitis B
/ Hepatitis B - virology
/ Hepatitis B Surface Antigens - chemistry
/ Hepatitis B Surface Antigens - genetics
/ Hepatitis B Surface Antigens - metabolism
/ Hepatitis B virus - chemistry
/ Hepatitis B virus - genetics
/ Hepatitis B virus - metabolism
/ Hepatitis B virus - ultrastructure
/ Humanities and Social Sciences
/ Humans
/ Models, Molecular
/ Molecular chains
/ Molecular structure
/ multidisciplinary
/ Mutation
/ Organic Anion Transporters, Sodium-Dependent - chemistry
/ Organic Anion Transporters, Sodium-Dependent - genetics
/ Organic Anion Transporters, Sodium-Dependent - metabolism
/ Protein Binding
/ Protein Precursors
/ Protein structure
/ Receptors
/ Receptors, Virus - chemistry
/ Receptors, Virus - metabolism
/ Science
/ Science (multidisciplinary)
/ Steric hindrance
/ Structure-function relationships
/ Symporters - chemistry
/ Symporters - genetics
/ Symporters - metabolism
/ Symporters - ultrastructure
/ Viruses
2024
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Structural basis for hepatitis B virus restriction by a viral receptor homologue
by
Mifune, Junki
, Watashi, Koichi
, Ikeguchi, Mitsunori
, Umezawa, Haruka
, Kusunoki, Atsuto
, Tame, Jeremy R. H.
, Yamamoto, Kenichiro
, Kobayashi, Chisa
, Park, Sam-Yong
, Takeuchi, Junko S.
, Morita, Takeshi
, Nomura, Norimichi
, Muramatsu, Masamichi
, Ishimoto, Naito
, Ekimoto, Toru
, Iwata, So
, Park, Jae-Hyun
, Shionoya, Kaho
in
101/28
/ 13/109
/ 14/34
/ 631/326/596/1550
/ 631/535/1258/1259
/ Animals
/ Bile acids
/ Bile Acids and Salts - chemistry
/ Bile Acids and Salts - metabolism
/ Binding
/ Cryoelectron Microscopy
/ Electron microscopy
/ Embedding
/ Hepatitis
/ Hepatitis B
/ Hepatitis B - virology
/ Hepatitis B Surface Antigens - chemistry
/ Hepatitis B Surface Antigens - genetics
/ Hepatitis B Surface Antigens - metabolism
/ Hepatitis B virus - chemistry
/ Hepatitis B virus - genetics
/ Hepatitis B virus - metabolism
/ Hepatitis B virus - ultrastructure
/ Humanities and Social Sciences
/ Humans
/ Models, Molecular
/ Molecular chains
/ Molecular structure
/ multidisciplinary
/ Mutation
/ Organic Anion Transporters, Sodium-Dependent - chemistry
/ Organic Anion Transporters, Sodium-Dependent - genetics
/ Organic Anion Transporters, Sodium-Dependent - metabolism
/ Protein Binding
/ Protein Precursors
/ Protein structure
/ Receptors
/ Receptors, Virus - chemistry
/ Receptors, Virus - metabolism
/ Science
/ Science (multidisciplinary)
/ Steric hindrance
/ Structure-function relationships
/ Symporters - chemistry
/ Symporters - genetics
/ Symporters - metabolism
/ Symporters - ultrastructure
/ Viruses
2024
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Structural basis for hepatitis B virus restriction by a viral receptor homologue
by
Mifune, Junki
, Watashi, Koichi
, Ikeguchi, Mitsunori
, Umezawa, Haruka
, Kusunoki, Atsuto
, Tame, Jeremy R. H.
, Yamamoto, Kenichiro
, Kobayashi, Chisa
, Park, Sam-Yong
, Takeuchi, Junko S.
, Morita, Takeshi
, Nomura, Norimichi
, Muramatsu, Masamichi
, Ishimoto, Naito
, Ekimoto, Toru
, Iwata, So
, Park, Jae-Hyun
, Shionoya, Kaho
in
101/28
/ 13/109
/ 14/34
/ 631/326/596/1550
/ 631/535/1258/1259
/ Animals
/ Bile acids
/ Bile Acids and Salts - chemistry
/ Bile Acids and Salts - metabolism
/ Binding
/ Cryoelectron Microscopy
/ Electron microscopy
/ Embedding
/ Hepatitis
/ Hepatitis B
/ Hepatitis B - virology
/ Hepatitis B Surface Antigens - chemistry
/ Hepatitis B Surface Antigens - genetics
/ Hepatitis B Surface Antigens - metabolism
/ Hepatitis B virus - chemistry
/ Hepatitis B virus - genetics
/ Hepatitis B virus - metabolism
/ Hepatitis B virus - ultrastructure
/ Humanities and Social Sciences
/ Humans
/ Models, Molecular
/ Molecular chains
/ Molecular structure
/ multidisciplinary
/ Mutation
/ Organic Anion Transporters, Sodium-Dependent - chemistry
/ Organic Anion Transporters, Sodium-Dependent - genetics
/ Organic Anion Transporters, Sodium-Dependent - metabolism
/ Protein Binding
/ Protein Precursors
/ Protein structure
/ Receptors
/ Receptors, Virus - chemistry
/ Receptors, Virus - metabolism
/ Science
/ Science (multidisciplinary)
/ Steric hindrance
/ Structure-function relationships
/ Symporters - chemistry
/ Symporters - genetics
/ Symporters - metabolism
/ Symporters - ultrastructure
/ Viruses
2024
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Structural basis for hepatitis B virus restriction by a viral receptor homologue
Journal Article
Structural basis for hepatitis B virus restriction by a viral receptor homologue
2024
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Overview
Macaque restricts hepatitis B virus (HBV) infection because its receptor homologue, NTCP (mNTCP), cannot bind preS1 on viral surface. To reveal how mNTCP loses the viral receptor function, we here solve the cryo-electron microscopy structure of mNTCP. Superposing on the human NTCP (hNTCP)-preS1 complex structure shows that Arg158 of mNTCP causes steric clash to prevent preS1 from embedding onto the bile acid tunnel of NTCP. Cell-based mutation analysis confirms that only Gly158 permitted preS1 binding, in contrast to robust bile acid transport among mutations. As the second determinant, Asn86 on the extracellular surface of mNTCP shows less capacity to restrain preS1 from dynamic fluctuation than Lys86 of hNTCP, resulting in unstable preS1 binding. Additionally, presence of long-chain conjugated-bile acids in the tunnel induces steric hindrance with preS1 through their tailed-chain. This study presents structural basis in which multiple sites in mNTCP constitute a molecular barrier to strictly restrict HBV.
Here the authors look at why macaque is non-susceptible to hepatitis B virus by focusing on the protein structure of the host receptor homolog. They show that macaque-derived host receptor homolog has multiple structural defects against virus binding.
Publisher
Nature Publishing Group UK,Nature Publishing Group,Nature Portfolio
Subject
/ 13/109
/ 14/34
/ Animals
/ Bile Acids and Salts - chemistry
/ Bile Acids and Salts - metabolism
/ Binding
/ Hepatitis B Surface Antigens - chemistry
/ Hepatitis B Surface Antigens - genetics
/ Hepatitis B Surface Antigens - metabolism
/ Hepatitis B virus - chemistry
/ Hepatitis B virus - genetics
/ Hepatitis B virus - metabolism
/ Hepatitis B virus - ultrastructure
/ Humanities and Social Sciences
/ Humans
/ Mutation
/ Organic Anion Transporters, Sodium-Dependent - chemistry
/ Organic Anion Transporters, Sodium-Dependent - genetics
/ Organic Anion Transporters, Sodium-Dependent - metabolism
/ Receptors, Virus - chemistry
/ Receptors, Virus - metabolism
/ Science
/ Structure-function relationships
/ Viruses
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