EMDB-46645: Focused map of Cryo-EM structure of Ubiquitin C-degron bound to K...

基本情報

登録情報

データベース: EMDB / ID: EMD-46645

• タイトル: Focused map of Cryo-EM structure of Ubiquitin C-degron bound to KLHDC10-EloB/C

試料

• 複合体: Trapped ARIH1-diUB-CRL2-KLHDC10 complex
  • タンパク質・ペプチド: Kelch domain-containing protein 10
  • タンパク質・ペプチド: Elongin-B
  • タンパク質・ペプチド: Elongin-C
  • タンパク質・ペプチド: Ubiquitin-C

• キーワード: KLHDC10 / ubiquitin / E3 / Cullin-RING / C-Degron / LIGASE

機能・相同性

分子機能:

positive regulation of stress-activated MAPK cascade / ubiquitin-dependent protein catabolic process via the C-end degron rule pathway / target-directed miRNA degradation / VCB complex / elongin complex / Cul5-RING ubiquitin ligase complex / Cul2-RING ubiquitin ligase complex / Pausing and recovery of Tat-mediated HIV elongation / Tat-mediated HIV elongation arrest and recovery / HIV elongation arrest and recovery / Pausing and recovery of HIV elongation / Tat-mediated elongation of the HIV-1 transcript / ubiquitin-like ligase-substrate adaptor activity / Formation of HIV-1 elongation complex containing HIV-1 Tat / Formation of HIV elongation complex in the absence of HIV Tat / RNA Polymerase II Transcription Elongation / Formation of RNA Pol II elongation complex / Maturation of protein E / Maturation of protein E / ER Quality Control Compartment (ERQC) / RNA Polymerase II Pre-transcription Events / Myoclonic epilepsy of Lafora / rescue of stalled ribosome / FLT3 signaling by CBL mutants / Prevention of phagosomal-lysosomal fusion / IRAK2 mediated activation of TAK1 complex / Alpha-protein kinase 1 signaling pathway / Glycogen synthesis / IRAK1 recruits IKK complex / IRAK1 recruits IKK complex upon TLR7/8 or 9 stimulation / Membrane binding and targetting of GAG proteins / Endosomal Sorting Complex Required For Transport (ESCRT) / Regulation of TBK1, IKKε (IKBKE)-mediated activation of IRF3, IRF7 / Negative regulation of FLT3 / PTK6 Regulates RTKs and Their Effectors AKT1 and DOK1 / Regulation of TBK1, IKKε-mediated activation of IRF3, IRF7 upon TLR3 ligation / IRAK2 mediated activation of TAK1 complex upon TLR7/8 or 9 stimulation / Constitutive Signaling by NOTCH1 HD Domain Mutants / NOTCH2 Activation and Transmission of Signal to the Nucleus / TICAM1,TRAF6-dependent induction of TAK1 complex / TICAM1-dependent activation of IRF3/IRF7 / APC/C:Cdc20 mediated degradation of Cyclin B / Regulation of FZD by ubiquitination / Downregulation of ERBB4 signaling / APC-Cdc20 mediated degradation of Nek2A / p75NTR recruits signalling complexes / InlA-mediated entry of Listeria monocytogenes into host cells / TRAF6 mediated IRF7 activation in TLR7/8 or 9 signaling / TRAF6-mediated induction of TAK1 complex within TLR4 complex / Regulation of pyruvate metabolism / Regulation of innate immune responses to cytosolic DNA / NF-kB is activated and signals survival / Downregulation of ERBB2:ERBB3 signaling / Pexophagy / NRIF signals cell death from the nucleus / VLDLR internalisation and degradation / Regulation of PTEN localization / Activated NOTCH1 Transmits Signal to the Nucleus / Synthesis of active ubiquitin: roles of E1 and E2 enzymes / Regulation of BACH1 activity / MAP3K8 (TPL2)-dependent MAPK1/3 activation / TICAM1, RIP1-mediated IKK complex recruitment / Translesion synthesis by REV1 / Activation of IRF3, IRF7 mediated by TBK1, IKKε (IKBKE) / Translesion synthesis by POLK / InlB-mediated entry of Listeria monocytogenes into host cell / Downregulation of TGF-beta receptor signaling / Josephin domain DUBs / JNK (c-Jun kinases) phosphorylation and activation mediated by activated human TAK1 / Regulation of activated PAK-2p34 by proteasome mediated degradation / IKK complex recruitment mediated by RIP1 / Translesion synthesis by POLI / Gap-filling DNA repair synthesis and ligation in GG-NER / transcription corepressor binding / PINK1-PRKN Mediated Mitophagy / TGF-beta receptor signaling in EMT (epithelial to mesenchymal transition) / TNFR1-induced NF-kappa-B signaling pathway / Autodegradation of Cdh1 by Cdh1:APC/C / APC/C:Cdc20 mediated degradation of Securin / N-glycan trimming in the ER and Calnexin/Calreticulin cycle / TCF dependent signaling in response to WNT / Asymmetric localization of PCP proteins / Regulation of NF-kappa B signaling / Ubiquitin-dependent degradation of Cyclin D / SCF-beta-TrCP mediated degradation of Emi1 / NIK-->noncanonical NF-kB signaling / activated TAK1 mediates p38 MAPK activation / Negative regulators of DDX58/IFIH1 signaling / TNFR2 non-canonical NF-kB pathway / AUF1 (hnRNP D0) binds and destabilizes mRNA / transcription initiation at RNA polymerase II promoter / Regulation of signaling by CBL / TP53 Regulates Transcription of DNA Repair Genes / NOTCH3 Activation and Transmission of Signal to the Nucleus / Vpu mediated degradation of CD4 / Assembly of the pre-replicative complex / Ubiquitin-Mediated Degradation of Phosphorylated Cdc25A / Deactivation of the beta-catenin transactivating complex / Degradation of DVL / Negative regulation of FGFR3 signaling

ドメイン・相同性:

: / Galactose oxidase, central domain / KLHDC2/KLHL20/DRC7 Kelch-repeats domain / Kelch / Kelch repeat type 1 / Elongin-C / Elongin B / Kelch-type beta propeller / S-phase kinase-associated protein 1-like / SKP1 component, POZ domain / Skp1 family, tetramerisation domain / Found in Skp1 protein family / SKP1/BTB/POZ domain superfamily / : / Ubiquitin domain signature. / Ubiquitin conserved site / Ubiquitin domain / Ubiquitin family / Ubiquitin homologues / Ubiquitin domain profile. / Ubiquitin-like domain / Ubiquitin-like domain superfamily

構成要素:

Polyubiquitin-C / Elongin-C / Elongin-B / Kelch domain-containing protein 10

• 生物種: Homo sapiens (ヒト)
• 手法: 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: Chittori S / Scott DC / Schulman BA

資金援助

米国, 1件

Organization	Grant number	国
National Institutes of Health/National Cancer Institute (NIH/NCI)	5R01CA247365	米国

• 引用: ジャーナル: Nat Commun / 年: 2024; タイトル: Structural basis for C-degron selectivity across KLHDCX family E3 ubiquitin ligases.; 著者: Daniel C Scott / Sagar Chittori / Nicholas Purser / Moeko T King / Samuel A Maiwald / Kelly Churion / Amanda Nourse / Chan Lee / Joao A Paulo / Darcie J Miller / Stephen J Elledge / J Wade Harper / Gary Kleiger / Brenda A Schulman / ; 要旨: Specificity of the ubiquitin-proteasome system depends on E3 ligase-substrate interactions. Many such pairings depend on E3 ligases binding to peptide-like sequences - termed N- or C-degrons - at the termini of substrates. However, our knowledge of structural features distinguishing closely related C-degron substrate-E3 pairings is limited. Here, by systematically comparing ubiquitylation activities towards a suite of common model substrates, and defining interactions by biochemistry, crystallography, and cryo-EM, we reveal principles of C-degron recognition across the KLHDCX family of Cullin-RING ligases (CRLs). First, a motif common across these E3 ligases anchors a substrate's C-terminus. However, distinct locations of this C-terminus anchor motif in different blades of the KLHDC2, KLHDC3, and KLHDC10 β-propellers establishes distinct relative positioning and molecular environments for substrate C-termini. Second, our structural data show KLHDC3 has a pre-formed pocket establishing preference for an Arg or Gln preceding a C-terminal Gly, whereas conformational malleability contributes to KLHDC10's recognition of varying features adjacent to substrate C-termini. Finally, additional non-consensus interactions, mediated by C-degron binding grooves and/or by distal propeller surfaces and substrate globular domains, can substantially impact substrate binding and ubiquitylatability. Overall, the data reveal combinatorial mechanisms determining specificity and plasticity of substrate recognition by KLDCX-family C-degron E3 ligases.

履歴

登録	2024年8月19日	-
ヘッダ(付随情報) 公開	2024年11月20日	-
マップ公開	2024年11月20日	-
更新	2025年2月5日	-
現状	2025年2月5日	処理サイト: RCSB / 状態: 公開

マップ

• ファイル: ダウンロード / ファイル: emd_46645.map.gz / 形式: CCP4 / 大きさ: 178 MB / タイプ: IMAGE STORED AS FLOATING POINT NUMBER (4 BYTES)
• ボクセルのサイズ: X=Y=Z: 1.297 Å

密度

表面レベル	登録者による: 0.202
最小 - 最大	-0.48354346 - 1.1814079
平均 (標準偏差)	-0.0007011356 (±0.010655936)

• 対称性: 空間群: 1

詳細

EMDB XML:

マップ形状	Axis order X Y Z Origin 0 0 0 サイズ 360 360 360 Spacing 360 360 360
セル	A=B=C: 466.92 Å α=β=γ: 90.0 °

添付データ

ハーフマップ: #2

• ファイル: emd_46645_half_map_1.map

ハーフマップ: #1

• ファイル: emd_46645_half_map_2.map

試料の構成要素

全体 : Trapped ARIH1-diUB-CRL2-KLHDC10 complex

• 全体: 名称: Trapped ARIH1-diUB-CRL2-KLHDC10 complex

要素

• 複合体: Trapped ARIH1-diUB-CRL2-KLHDC10 complex
  • タンパク質・ペプチド: Kelch domain-containing protein 10
  • タンパク質・ペプチド: Elongin-B
  • タンパク質・ペプチド: Elongin-C
  • タンパク質・ペプチド: Ubiquitin-C

超分子 #1: Trapped ARIH1-diUB-CRL2-KLHDC10 complex

• 超分子: 名称: Trapped ARIH1-diUB-CRL2-KLHDC10 complex / タイプ: complex / ID: 1 / 親要素: 0 / 含まれる分子: all

分子 #1: Kelch domain-containing protein 10

• 分子: 名称: Kelch domain-containing protein 10 / タイプ: protein_or_peptide / ID: 1 / コピー数: 1 / 光学異性体: LEVO
• 由来(天然): 生物種: Homo sapiens (ヒト)
• 分子量: 理論値: 45.745375 KDa
• 組換発現: 生物種: Trichoplusia ni (イラクサキンウワバ)

配列

文字列:

QLNRFVQLSG RPHLPGKKKI RWDPVRRRFI QSCPIIRIPN RFLRGHRPPP ARSGHRCVAD NTNLYVFGGY NPDYDESGGP DNEDYPLFR ELWRYHFATG VWHQMGTDGY MPRELASMSL VLHGNNLLVF GGTGIPFGES NGNDVHVCNV KYKRWALLSC R GKKPSRIY GQAMAIINGS LYVFGGTTGY IYSTDLHKLD LNTREWTQLK PNNLSCDLPE ERYRHEIAHD GQRIYILGGG TS WTAYSLN KIHAYNLETN AWEEIATKPH EKIGFPAARR CHSCVQIKND VFICGGYNGE VILGDIWKLN LQTFQWVKLP ATM PEPVYF HCAAVTPAGC MYIHGGVVNI HENKRTGSLF KIWLVVPSLL ELAWEKLLAA FPNLANLSRT QLLHLGLTQG LIER LK

UniProtKB: Kelch domain-containing protein 10

分子 #2: Elongin-B

• 分子: 名称: Elongin-B / タイプ: protein_or_peptide / ID: 2 / コピー数: 1 / 光学異性体: LEVO
• 由来(天然): 生物種: Homo sapiens (ヒト)
• 分子量: 理論値: 13.147781 KDa
• 組換発現: 生物種: Trichoplusia ni (イラクサキンウワバ)

配列

文字列:

MDVFLMIRRH KTTIFTDAKE SSTVFELKRI VEGILKRPPD EQRLYKDDQL LDDGKTLGEC GFTSQTARPQ APATVGLAFR ADDTFEALC IEPFSSPPEL PDVMKPQDSG SSANEQAVQ

UniProtKB: Elongin-B

分子 #3: Elongin-C

• 分子: 名称: Elongin-C / タイプ: protein_or_peptide / ID: 3 / コピー数: 1 / 光学異性体: LEVO
• 由来(天然): 生物種: Homo sapiens (ヒト)
• 分子量: 理論値: 12.485135 KDa
• 組換発現: 生物種: Trichoplusia ni (イラクサキンウワバ)

配列

文字列:

MDGEEKTYGG CEGPDAMYVK LISSDGHEFI VKREHALTSG TIKAMLSGPG QFAENETNEV NFREIPSHVL SKVCMYFTYK VRYTNSSTE IPEFPIAPEI ALELLMAANF LDC

UniProtKB: Elongin-C

分子 #4: Ubiquitin-C

• 分子: 名称: Ubiquitin-C / タイプ: protein_or_peptide / ID: 4 / コピー数: 1 / 光学異性体: LEVO
• 由来(天然): 生物種: Homo sapiens (ヒト)
• 分子量: 理論値: 8.550794 KDa
• 組換発現: 生物種: Escherichia coli (大腸菌)

配列

文字列:

MQIFVKTLTG KTITLEVEPS DTIENVKAKI QDKEGIPPDQ QRLIFAGCQL EDGRTLSDYN IQKESTLHLV LRLRGG

UniProtKB: Polyubiquitin-C

実験情報

構造解析

• 手法: クライオ電子顕微鏡法
• 解析: 単粒子再構成法
• 試料の集合状態: particle

試料調製

• 濃度: 0.8 mg/mL
• 緩衝液: pH: 7.5
• 凍結: 凍結剤: ETHANE / 装置: FEI VITROBOT MARK IV

電子顕微鏡法

• 顕微鏡: FEI TITAN KRIOS
• 撮影: フィルム・検出器のモデル: GATAN K3 BIOQUANTUM (6k x 4k); 実像数: 13395 / 平均電子線量: 40.0 e/Ų
• 電子線: 加速電圧: 300 kV / 電子線源: FIELD EMISSION GUN
• 電子光学系: 照射モード: FLOOD BEAM / 撮影モード: BRIGHT FIELD / 最大 デフォーカス（公称値）: 2.25 µm / 最小 デフォーカス（公称値）: 0.6 µm / 倍率（公称値）: 130000
• 実験機器: モデル: Titan Krios / 画像提供: FEI Company

画像解析

• 初期モデル: モデルのタイプ: INSILICO MODEL
• 最終 再構成: 想定した対称性 - 点群: C₁ (非対称) / 解像度のタイプ: BY AUTHOR / 解像度: 3.2 Å / 解像度の算出法: FSC 0.143 CUT-OFF / 使用した粒子像数: 234648
• 初期 角度割当: タイプ: MAXIMUM LIKELIHOOD
• 最終 角度割当: タイプ: MAXIMUM LIKELIHOOD