PDB-7bh9: SARS-CoV-2 RBD-62 in complex with ACE2 peptidase domain

基本情報

• 登録情報: データベース: PDB / ID: 7bh9
• タイトル: SARS-CoV-2 RBD-62 in complex with ACE2 peptidase domain

要素

• Angiotensin-converting enzyme 2
• Spike protein S1

• キーワード: VIRUS / In vitro evolution / Complex / receptor binding domain

機能・相同性

分子機能:

positive regulation of amino acid transport / angiotensin-converting enzyme 2 / positive regulation of L-proline import across plasma membrane / 加水分解酵素; プロテアーゼ; ペプチド結合加水分解酵素; 金属プロテアーゼ / angiotensin-mediated drinking behavior / regulation of systemic arterial blood pressure by renin-angiotensin / positive regulation of gap junction assembly / tryptophan transport / regulation of cardiac conduction / maternal process involved in female pregnancy / peptidyl-dipeptidase activity / regulation of vasoconstriction / transporter activator activity / Metabolism of Angiotensinogen to Angiotensins / carboxypeptidase activity / angiotensin maturation / Attachment and Entry / receptor-mediated endocytosis of virus by host cell / metallocarboxypeptidase activity / viral life cycle / positive regulation of cardiac muscle contraction / regulation of cytokine production / blood vessel diameter maintenance / negative regulation of smooth muscle cell proliferation / brush border membrane / negative regulation of ERK1 and ERK2 cascade / endocytic vesicle membrane / positive regulation of reactive oxygen species metabolic process / metallopeptidase activity / regulation of cell population proliferation / virus receptor activity / regulation of inflammatory response / endopeptidase activity / symbiont-mediated disruption of host tissue / Maturation of spike protein / Translation of Structural Proteins / Virion Assembly and Release / host cell surface / viral translation / host extracellular space / symbiont-mediated-mediated suppression of host tetherin activity / Potential therapeutics for SARS / Induction of Cell-Cell Fusion / structural constituent of virion / entry receptor-mediated virion attachment to host cell / membrane fusion / Attachment and Entry / host cell endoplasmic reticulum-Golgi intermediate compartment membrane / positive regulation of viral entry into host cell / receptor-mediated virion attachment to host cell / host cell surface receptor binding / cilium / symbiont-mediated suppression of host innate immune response / apical plasma membrane / membrane raft / receptor ligand activity / endocytosis involved in viral entry into host cell / endoplasmic reticulum lumen / fusion of virus membrane with host plasma membrane / fusion of virus membrane with host endosome membrane / viral envelope / symbiont entry into host cell / virion attachment to host cell / SARS-CoV-2 activates/modulates innate and adaptive immune responses / host cell plasma membrane / virion membrane / cell surface / negative regulation of transcription by RNA polymerase II / extracellular space / extracellular exosome / extracellular region / zinc ion binding / identical protein binding / membrane / plasma membrane

ドメイン・相同性:

Collectrin domain / Renal amino acid transporter / Collectrin-like domain profile. / Peptidase M2, peptidyl-dipeptidase A / Angiotensin-converting enzyme / Peptidase family M2 domain profile. / Neutral zinc metallopeptidases, zinc-binding region signature. / Spike (S) protein S1 subunit, receptor-binding domain, SARS-CoV-2 / Spike (S) protein S1 subunit, N-terminal domain, SARS-CoV-like / Coronavirus spike glycoprotein S1, C-terminal / Coronavirus spike glycoprotein S1, C-terminal / Spike glycoprotein, betacoronavirus / Spike glycoprotein, N-terminal domain superfamily / Betacoronavirus spike (S) glycoprotein S1 subunit N-terminal (NTD) domain profile. / Betacoronavirus spike (S) glycoprotein S1 subunit C-terminal (CTD) domain profile. / 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 1 (HR1) region profile. / Coronavirus spike (S) glycoprotein S2 subunit heptad repeat 2 (HR2) region profile. / Spike glycoprotein S2 superfamily, coronavirus / Spike glycoprotein S2, coronavirus / Coronavirus spike glycoprotein S2

構成要素:

Spike glycoprotein / Angiotensin-converting enzyme 2

• 生物種: Homo sapiens (ヒト); Severe acute respiratory syndrome coronavirus 2 (ウイルス)
• 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: 2.9 Å
• データ登録者: Elad, N. / Dym, O. / Zahradnik, J. / Schreiber, G.

資金援助

イスラエル, 2件

組織	認可番号	国
Israel Science Foundation	3814/19	イスラエル
Israel Science Foundation	1268/18	イスラエル

• 引用: ジャーナル: Nat Microbiol / 年: 2021; タイトル: SARS-CoV-2 variant prediction and antiviral drug design are enabled by RBD in vitro evolution.; 著者: Jiří Zahradník / Shir Marciano / Maya Shemesh / Eyal Zoler / Daniel Harari / Jeanne Chiaravalli / Björn Meyer / Yinon Rudich / Chunlin Li / Ira Marton / Orly Dym / Nadav Elad / Mark G Lewis / Hanne Andersen / Matthew Gagne / Robert A Seder / Daniel C Douek / Gideon Schreiber / ; 要旨: SARS-CoV-2 variants of interest and concern will continue to emerge for the duration of the COVID-19 pandemic. To map mutations in the receptor-binding domain (RBD) of the spike protein that affect binding to angiotensin-converting enzyme 2 (ACE2), the receptor for SARS-CoV-2, we applied in vitro evolution to affinity-mature the RBD. Multiple rounds of random mutagenic libraries of the RBD were sorted against decreasing concentrations of ACE2, resulting in the selection of higher affinity RBD binders. We found that mutations present in more transmissible viruses (S477N, E484K and N501Y) were preferentially selected in our high-throughput screen. Evolved RBD mutants include prominently the amino acid substitutions found in the RBDs of B.1.620, B.1.1.7 (Alpha), B1.351 (Beta) and P.1 (Gamma) variants. Moreover, the incidence of RBD mutations in the population as presented in the GISAID database (April 2021) is positively correlated with increased binding affinity to ACE2. Further in vitro evolution increased binding by 1,000-fold and identified mutations that may be more infectious if they evolve in the circulating viral population, for example, Q498R is epistatic to N501Y. We show that our high-affinity variant RBD-62 can be used as a drug to inhibit infection with SARS-CoV-2 and variants Alpha, Beta and Gamma in vitro. In a model of SARS-CoV-2 challenge in hamster, RBD-62 significantly reduced clinical disease when administered before or after infection. A 2.9 Å cryo-electron microscopy structure of the high-affinity complex of RBD-62 and ACE2, including all rapidly spreading mutations, provides a structural basis for future drug and vaccine development and for in silico evaluation of known antibodies.

履歴

登録	2021年1月11日	登録サイト: PDBE / 処理サイト: PDBE
改定 1.0	2021年2月17日	Provider: repository / タイプ: Initial release
改定 1.1	2021年3月10日	Group: Database references / Source and taxonomy / Structure summary カテゴリ: entity / entity_name_com / entity_src_gen / struct / struct_ref / struct_ref_seq / struct_ref_seq_dif Item: _entity.pdbx_description / _entity_src_gen.gene_src_common_name / _entity_src_gen.pdbx_gene_src_gene / _struct.pdbx_descriptor / _struct_ref.db_code / _struct_ref.pdbx_db_accession / _struct_ref.pdbx_seq_one_letter_code / _struct_ref_seq.pdbx_db_accession
改定 1.2	2021年9月1日	Group: Database references / カテゴリ: citation / citation_author / database_2 Item: _citation.country / _citation.journal_abbrev / _citation.journal_id_CSD / _citation.journal_id_ISSN / _citation.pdbx_database_id_DOI / _citation.pdbx_database_id_PubMed / _citation.title / _citation.year / _database_2.pdbx_DOI / _database_2.pdbx_database_accession
改定 1.3	2021年9月22日	Group: Data collection / Database references カテゴリ: citation / citation_author / em_admin / pdbx_database_proc Item: _citation.journal_volume / _citation.page_first / _citation.page_last / _citation_author.identifier_ORCID / _em_admin.last_update
改定 1.4	2024年10月9日	Group: Data collection / Refinement description / Structure summary カテゴリ: chem_comp_atom / chem_comp_bond / em_3d_fitting_list / em_admin / pdbx_entry_details / pdbx_initial_refinement_model / pdbx_modification_feature Item: _em_3d_fitting_list.accession_code / _em_3d_fitting_list.initial_refinement_model_id / _em_3d_fitting_list.source_name / _em_3d_fitting_list.type / _em_admin.last_update / _pdbx_entry_details.has_protein_modification

集合体

登録構造単位

A: Angiotensin-converting enzyme 2

E: Spike protein S1

ヘテロ分子

概要:

• 94.2 kDa, 2 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)	94,249	6
ポリマ－	93,520	2
非ポリマー	729	4
水	0	0

1

概要:

• 登録構造と同一
• 登録者・ソフトウェアが定義した集合体
• 根拠: gel filtration

対称操作:

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

計算値:

Buried area	2470 Å2
ΔGint	-25 kcal/mol
Surface area	32800 Å2
手法	PISA

要素

#1: タンパク質

A Angiotensin-converting enzyme 2 / Angiotensin-converting enzyme homolog / ACEH / Angiotensin-converting enzyme-related carboxypeptidase / ACE-related carboxypeptidase / Metalloprotease MPROT15

詳細:

分子量: 70486.039 Da / 分子数: 1 / 由来タイプ: 組換発現 / 由来: (組換発現) Homo sapiens (ヒト) / 遺伝子: ACE2, UNQ868/PRO1885 / 発現宿主: Homo sapiens (ヒト)
参照: UniProt: Q9BYF1, angiotensin-converting enzyme 2, 加水分解酵素; プロテアーゼ; ペプチド結合加水分解酵素; 金属プロテアーゼ

#2: タンパク質

E Spike protein S1

詳細:

分子量: 23033.965 Da / 分子数: 1 / 由来タイプ: 組換発現 / 詳細: SARS-CoV-2 receptor binding domain
由来: (組換発現) Severe acute respiratory syndrome coronavirus 2 (ウイルス)
遺伝子: S, 2 / 発現宿主: Homo sapiens (ヒト) / 参照: UniProt: P0DTC2

#3: 化合物

A-901 ChemComp-ZN / ZINC ION

詳細:

分子量: 65.409 Da / 分子数: 1 / 由来タイプ: 合成 / 式: Zn / タイプ: SUBJECT OF INVESTIGATION

#4: 糖

A-902 A-903 A-904 ChemComp-NAG / 2-acetamido-2-deoxy-beta-D-glucopyranose / N-acetyl-beta-D-glucosamine / 2-acetamido-2-deoxy-beta-D-glucose / 2-acetamido-2-deoxy-D-glucose / 2-acetamido-2-deoxy-glucose / N-ACETYL-D-GLUCOSAMINE / N-アセチル-β-D-グルコサミン

詳細:

タイプ: D-saccharide, beta linking / 分子量: 221.208 Da / 分子数: 3 / 由来タイプ: 合成 / 式: C₈H₁₅NO₆ / タイプ: SUBJECT OF INVESTIGATION

識別子:

識別子	タイプ	プログラム
DGlcpNAcb	CONDENSED IUPAC CARBOHYDRATE SYMBOL	GMML 1.0
N-acetyl-b-D-glucopyranosamine	COMMON NAME	GMML 1.0
b-D-GlcpNAc	IUPAC CARBOHYDRATE SYMBOL	PDB-CARE 1.0
GlcNAc	SNFG CARBOHYDRATE SYMBOL	GMML 1.0

• 研究の焦点であるリガンドがあるか: Y
• Has protein modification: Y

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

ID	名称	タイプ	Entity ID	Parent-ID	由来
1	SARS-CoV-2 RBD-62 in complex with ACE2 peptidase domain	COMPLEX	#1-#2	0	RECOMBINANT
2	ACE2 extracellular peptidase domain	COMPLEX	#1	1	RECOMBINANT
3	SARS-CoV-2 receptor binding domain	COMPLEX	#2	1	RECOMBINANT

• 分子量: 実験値: NO

由来(天然)

ID	Entity assembly-ID	生物種	Ncbi tax-ID
1	2	Homo sapiens (ヒト)	9606
2	3	Severe acute respiratory syndrome coronavirus 2 (ウイルス)	2697049

由来(組換発現)

ID	Entity assembly-ID	生物種	Ncbi tax-ID
1	2	Homo sapiens (ヒト)	9606
2	3	Homo sapiens (ヒト)	9606

• 緩衝液: pH: 7.2
• 試料: 濃度: 3.5 mg/ml / 包埋: NO / シャドウイング: NO / 染色: NO / 凍結: YES
• 試料支持: グリッドの材料: GOLD / グリッドのサイズ: 300 divisions/in. / グリッドのタイプ: UltrAuFoil R1.2/1.3
• 急速凍結: 装置: FEI VITROBOT MARK IV / 凍結剤: ETHANE / 湿度: 100 % / 凍結前の試料温度: 277 K

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: TFS 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 FIELD / 倍率（公称値）: 165000 X / 倍率（補正後）: 94518 X / Cs: 2.7 mm / C2レンズ絞り径: 70 µm / アライメント法: COMA FREE
• 試料ホルダ: 凍結剤: NITROGEN; 試料ホルダーモデル: FEI TITAN KRIOS AUTOGRID HOLDER
• 撮影: 平均露光時間: 1.214 sec. / 電子線照射量: 70 e/Ų / フィルム・検出器のモデル: GATAN K3 (6k x 4k) / 撮影したグリッド数: 2 / 実像数: 4470

解析

• ソフトウェア: 名称: PHENIX / バージョン: 1.15.2_3472: / 分類: 精密化

EMソフトウェア

ID	名称	バージョン	カテゴリ
2	SerialEM	3.9	画像取得
4	cryoSPARC	3.0.1	CTF補正
7	PHENIX		モデルフィッティング
9	cryoSPARC	3.0.1	初期オイラー角割当
10	cryoSPARC	3.0.1	最終オイラー角割当
11	cryoSPARC	3.0.1	分類
12	cryoSPARC	3.0.1	３次元再構成
13	PHENIX		モデル精密化

• CTF補正: タイプ: PHASE FLIPPING AND AMPLITUDE CORRECTION
• 対称性: 点対称性: C₁ (非対称)
• 3次元再構成: 解像度: 2.9 Å / 解像度の算出法: FSC 0.143 CUT-OFF / 粒子像の数: 164636 / 対称性のタイプ: POINT
• 原子モデル構築: プロトコル: FLEXIBLE FIT / 空間: REAL

原子モデル構築

PDB-ID: 6M0J

6m0j

Accession code: 6M0J / Source name: PDB / タイプ: experimental model

拘束条件

Refine-ID	タイプ	Dev ideal	数
ELECTRON MICROSCOPY	f_bond_d	0.007	6038
ELECTRON MICROSCOPY	f_angle_d	0.673	8205
ELECTRON MICROSCOPY	f_dihedral_angle_d	9.025	3508
ELECTRON MICROSCOPY	f_chiral_restr	0.047	871
ELECTRON MICROSCOPY	f_plane_restr	0.004	1050