PDB-6x2c: SARS-CoV-2 u1S2q All Down RBD State Spike Protein Trimer

基本情報

• 登録情報: データベース: PDB / ID: 6x2c
• タイトル: SARS-CoV-2 u1S2q All Down RBD State Spike Protein Trimer
• 要素: Spike glycoproteinスパイクタンパク質
• キーワード: VIRAL PROTEIN (ウイルスタンパク質) / Trimer

機能・相同性

分子機能:

Maturation of spike protein / viral translation / Translation of Structural Proteins / Virion Assembly and Release / host cell surface / host extracellular space / suppression by virus of host tetherin activity / Induction of Cell-Cell Fusion / structural constituent of virion / host cell endoplasmic reticulum-Golgi intermediate compartment membrane / entry receptor-mediated virion attachment to host cell / receptor-mediated endocytosis of virus by host cell / Attachment and Entry / membrane fusion / positive regulation of viral entry into host cell / receptor-mediated virion attachment to host cell / receptor ligand activity / host cell surface receptor binding / fusion of virus membrane with host plasma membrane / fusion of virus membrane with host endosome membrane / エンベロープ (ウイルス) / symbiont-mediated suppression of host type I interferon-mediated signaling pathway / virion attachment to host cell / SARS-CoV-2 activates/modulates innate and adaptive immune responses / host cell plasma membrane / virion membrane / 生体膜 / identical protein binding / 細胞膜

ドメイン・相同性:

Spike (S) protein S1 subunit, receptor-binding domain, SARS-CoV-2 / Spike (S) protein S1 subunit, N-terminal domain, SARS-CoV-like / Betacoronavirus spike (S) glycoprotein S1 subunit N-terminal (NTD) domain profile. / Spike glycoprotein, N-terminal domain superfamily / Betacoronavirus spike (S) glycoprotein S1 subunit C-terminal (CTD) domain profile. / Spike glycoprotein, betacoronavirus / Spike (S) protein S1 subunit, receptor-binding domain, betacoronavirus / Spike S1 subunit, receptor binding domain superfamily, betacoronavirus / Betacoronavirus spike glycoprotein S1, receptor binding / Spike glycoprotein S1, N-terminal domain, betacoronavirus-like / Betacoronavirus-like spike glycoprotein S1, N-terminal / Spike glycoprotein S2, coronavirus, heptad repeat 1 / Spike glycoprotein S2, coronavirus, heptad repeat 2 / Coronavirus spike (S) glycoprotein S2 subunit heptad repeat 2 (HR2) region profile. / Coronavirus spike (S) glycoprotein S2 subunit heptad repeat 1 (HR1) region profile. / Spike glycoprotein S2 superfamily, coronavirus / Spike glycoprotein S2, coronavirus / Coronavirus spike glycoprotein S2 / Coronavirus spike glycoprotein S1, C-terminal / Coronavirus spike glycoprotein S1, C-terminal

構成要素:

スパイクタンパク質

• 生物種: Severe acute respiratory syndrome coronavirus 2 (SARSコロナウイルス2)
• 手法: 電子顕微鏡法 / 単粒子再構成法 / クライオ電子顕微鏡法 / 解像度: 3.2 Å
• データ登録者: Henderson, R. / Acharya, P.

資金援助

米国, 5件

組織	認可番号	国
National Institutes of Health/National Institute of General Medical Sciences (NIH/NIGMS)	U24 GM129539	米国
Other private	SF349247	米国
National Institutes of Health/National Institute Of Allergy and Infectious Diseases (NIH/NIAID)	UM1 AI100645	米国
National Institutes of Health/National Institute Of Allergy and Infectious Diseases (NIH/NIAID)	UM1 AI44371	米国
National Institutes of Health/National Institute of Environmental Health Sciences (NIH/NIEHS)	ZIC ES103326	米国

引用

ジャーナル: Nat Struct Mol Biol / 年: 2020
タイトル: Controlling the SARS-CoV-2 spike glycoprotein conformation.
著者: Rory Henderson / Robert J Edwards / Katayoun Mansouri / Katarzyna Janowska / Victoria Stalls / Sophie M C Gobeil / Megan Kopp / Dapeng Li / Rob Parks / Allen L Hsu / Mario J Borgnia / Barton F Haynes / Priyamvada Acharya /
要旨: The coronavirus (CoV) spike (S) protein, involved in viral-host cell fusion, is the primary immunogenic target for virus neutralization and the current focus of many vaccine design efforts. The highly flexible S-protein, with its mobile domains, presents a moving target to the immune system. Here, to better understand S-protein mobility, we implemented a structure-based vector analysis of available β-CoV S-protein structures. Despite an overall similarity in domain organization, we found that S-proteins from different β-CoVs display distinct configurations. Based on this analysis, we developed two soluble ectodomain constructs for the SARS-CoV-2 S-protein, in which the highly immunogenic and mobile receptor binding domain (RBD) is either locked in the all-RBDs 'down' position or adopts 'up' state conformations more readily than the wild-type S-protein. These results demonstrate that the conformation of the S-protein can be controlled via rational design and can provide a framework for the development of engineered CoV S-proteins for vaccine applications.

#1: ジャーナル: bioRxiv / 年: 2020
タイトル: Controlling the SARS-CoV-2 Spike Glycoprotein Conformation.
著者: Rory Henderson / Robert J Edwards / Katayoun Mansouri / Katarzyna Janowska / Victoria Stalls / Sophie Gobeil / Megan Kopp / Allen Hsu / Mario Borgnia / Rob Parks / Barton F Haynes / Priyamvada Acharya /
要旨: The coronavirus (CoV) viral host cell fusion spike (S) protein is the primary immunogenic target for virus neutralization and the current focus of many vaccine design efforts. The highly flexible S-protein, with its mobile domains, presents a moving target to the immune system. Here, to better understand S-protein mobility, we implemented a structure-based vector analysis of available β-CoV S-protein structures. We found that despite overall similarity in domain organization, different β-CoV strains display distinct S-protein configurations. Based on this analysis, we developed two soluble ectodomain constructs in which the highly immunogenic and mobile receptor binding domain (RBD) is locked in either the all-RBDs 'down' position or is induced to display a previously unobserved in SARS-CoV-2 2-RBDs 'up' configuration. These results demonstrate that the conformation of the S-protein can be controlled via rational design and provide a framework for the development of engineered coronavirus spike proteins for vaccine applications.

履歴

登録	2020年5月20日	登録サイト: RCSB / 処理サイト: RCSB
改定 1.0	2020年5月27日	Provider: repository / タイプ: Initial release
改定 1.1	2020年6月24日	Group: Database references / カテゴリ: citation / citation_author Item: _citation.country / _citation.journal_abbrev / _citation.journal_id_CSD / _citation.pdbx_database_id_DOI / _citation.pdbx_database_id_PubMed / _citation.title / _citation.year / _citation_author.name
改定 1.2	2020年7月29日	Group: Data collection / Structure summary / カテゴリ: em_entity_assembly / em_software Item: _em_entity_assembly.name / _em_software.category / _em_software.fitting_id / _em_software.imaging_id
改定 1.3	2020年9月30日	Group: Database references / カテゴリ: citation / citation_author
改定 1.4	2020年10月21日	Group: Database references / カテゴリ: citation / citation_author Item: _citation.journal_volume / _citation.page_first / _citation.page_last / _citation_author.identifier_ORCID
改定 2.0	2021年7月7日	Group: Advisory / Atomic model / Data collection / Derived calculations / Structure summary カテゴリ: atom_site / em_entity_assembly / em_software / pdbx_poly_seq_scheme / pdbx_struct_assembly_prop / pdbx_struct_sheet_hbond / pdbx_unobs_or_zero_occ_residues / pdbx_validate_peptide_omega / pdbx_validate_planes / pdbx_validate_rmsd_angle / pdbx_validate_torsion / struct_conf / struct_conn / struct_sheet / struct_sheet_order / struct_sheet_range Item: _em_entity_assembly.name / _em_software.category / _pdbx_poly_seq_scheme.auth_mon_id / _pdbx_poly_seq_scheme.auth_seq_num / _pdbx_poly_seq_scheme.pdb_mon_id / _struct_conn.pdbx_dist_value / _struct_sheet_range.beg_auth_asym_id / _struct_sheet_range.beg_auth_comp_id / _struct_sheet_range.beg_auth_seq_id / _struct_sheet_range.beg_label_asym_id / _struct_sheet_range.beg_label_comp_id / _struct_sheet_range.beg_label_seq_id / _struct_sheet_range.end_auth_asym_id / _struct_sheet_range.end_auth_comp_id / _struct_sheet_range.end_auth_seq_id / _struct_sheet_range.end_label_asym_id / _struct_sheet_range.end_label_comp_id / _struct_sheet_range.end_label_seq_id / _struct_sheet_range.id / _struct_sheet_range.sheet_id 解説: Model orientation/position / Provider: author / タイプ: Coordinate replacement

集合体

登録構造単位

A: Spike glycoprotein

B: Spike glycoprotein

C: Spike glycoprotein

概要:

• 422 kDa, 3 ポリマー

構成要素の詳細:

	分子量 (理論値)	分子数
合計 (水以外)	422,371	3
ポリマ－	422,371	3
非ポリマー	0	0
水	0

1

概要:

• 登録構造と同一
• 登録者が定義した集合体

対称操作:

タイプ	名称	対称操作	数
identity operation	1_555		1

要素

#1: タンパク質

A B C Spike glycoprotein / スパイクタンパク質 / S glycoprotein / E2 / Peplomer protein

詳細:

分子量: 140790.453 Da / 分子数: 3 / 断片: ectodomain (UNP residues 16-1208) / 変異: F855Y+N856I+A570L+T572I / 由来タイプ: 組換発現
由来: (組換発現) Severe acute respiratory syndrome coronavirus 2 (SARSコロナウイルス2)
遺伝子: S, 2 / 発現宿主: Homo sapiens (ヒト) / 参照: UniProt: P0DTC2

実験情報

実験

• 実験: 手法: 電子顕微鏡法
• EM実験: 試料の集合状態: PARTICLE / ３次元再構成法: 単粒子再構成法

試料調製

• 構成要素: 名称: Severe acute respiratory syndrome coronavirus 2SARSコロナウイルス2; タイプ: VIRUS / Entity ID: all / 由来: RECOMBINANT
• 由来(天然): 生物種: Severe acute respiratory syndrome coronavirus 2 (SARSコロナウイルス2)
• 由来(組換発現): 生物種: Homo sapiens (ヒト)
• ウイルスについての詳細: 中空か: NO / エンベロープを持つか: YES / 単離: OTHER / タイプ: VIRION
• 緩衝液: pH: 7.4
• 試料: 包埋: NO / シャドウイング: NO / 染色: NO / 凍結: YES
• 試料支持: 詳細: unspecified
• 急速凍結: 凍結剤: ETHANE

電子顕微鏡撮影

• 実験機器: モデル: Titan Krios / 画像提供: FEI Company
• 顕微鏡: モデル: FEI TITAN KRIOS
• 電子銃: 電子線源: FIELD EMISSION GUN / 加速電圧: 300 kV / 照射モード: FLOOD BEAM
• 電子レンズ: モード: BRIGHT FIELDBright-field microscopy
• 撮影: 電子線照射量: 68.82 e/Ų / フィルム・検出器のモデル: GATAN K3 (6k x 4k)

解析

• CTF補正: タイプ: PHASE FLIPPING AND AMPLITUDE CORRECTION
• 3次元再構成: 解像度: 3.2 Å / 解像度の算出法: FSC 0.143 CUT-OFF / 粒子像の数: 192430 / 対称性のタイプ: POINT