PDB-2kms: Combined high- and low-resolution techniques reveal compact struc...

基本情報

• 登録情報: データベース: PDB / ID: 2kms
• タイトル: Combined high- and low-resolution techniques reveal compact structure in central portion of factor H despite long inter-modular linkers
• 要素: Complement factor H
• キーワード: IMMUNE SYSTEM / compact structure / limited interdomain flexibility / Age-related macular degeneration / Alternative splicing / Complement alternate pathway / Disease mutation / Disulfide bond / Glycoprotein / Immune response / Innate immunity / Polymorphism / Secreted / Sushi

機能・相同性

分子機能:

regulation of complement activation, alternative pathway / symbiont cell surface / regulation of complement-dependent cytotoxicity / complement component C3b binding / regulation of complement activation / heparan sulfate proteoglycan binding / serine-type endopeptidase complex / complement activation / complement activation, alternative pathway / Regulation of Complement cascade / heparin binding / blood microparticle / proteolysis / extracellular space / extracellular exosome / extracellular region / identical protein binding

ドメイン・相同性:

: / Complement Module, domain 1 / Complement Module; domain 1 / Sushi repeat (SCR repeat) / Domain abundant in complement control proteins; SUSHI repeat; short complement-like repeat (SCR) / Sushi/SCR/CCP domain / Sushi/CCP/SCR domain profile. / Sushi/SCR/CCP superfamily / Ribbon / Mainly Beta

構成要素:

Complement factor H

• 生物種: Homo sapiens (ヒト)
• 手法: 溶液NMR / simulated annealing
• Model details: lowest energy, model 1
• データ登録者: Schmidt, C.Q. / Herbert, A.P. / Guariento, M. / Mertens, H.D.T. / Soares, D.C. / Uhrin, D. / Rowe, A.J. / Svergun, D.I. / Barlow, P.N.
• 引用: ジャーナル: J Mol Biol / 年: 2010; タイトル: The central portion of factor H (modules 10-15) is compact and contains a structurally deviant CCP module.; 著者: Christoph Q Schmidt / Andrew P Herbert / Haydyn D T Mertens / Mara Guariento / Dinesh C Soares / Dusan Uhrin / Arthur J Rowe / Dmitri I Svergun / Paul N Barlow / ; 要旨: The first eight and the last two of 20 complement control protein (CCP) modules within complement factor H (fH) encompass binding sites for C3b and polyanionic carbohydrates. These binding sites cooperate self-surface selectively to prevent C3b amplification, thus minimising complement-mediated damage to host. Intervening fH CCPs, apparently devoid of such recognition sites, are proposed to play a structural role. One suggestion is that the generally small CCPs 10-15, connected by longer-than-average linkers, act as a flexible tether between the two functional ends of fH; another is that the long linkers induce a 180 degrees bend in the middle of fH. To test these hypotheses, we determined the NMR-derived structure of fH12-13 consisting of module 12, shown here to have an archetypal CCP structure, and module 13, which is uniquely short and features a laterally protruding helix-like insertion that contributes to a prominent electropositive patch. The unusually long fH12-13 linker is not flexible. It packs between the two CCPs that are not folded back on each other but form a shallow vee shape; analytical ultracentrifugation and X-ray scattering supported this finding. These two techniques additionally indicate that flanking modules (within fH11-14 and fH10-15) are at least as rigid and tilted relative to neighbours as are CCPs 12 and 13 with respect to one another. Tilts between successive modules are not unidirectional; their principal axes trace a zigzag path. In one of two arrangements for CCPs 10-15 that fit well with scattering data, CCP 14 is folded back onto CCP 13. In conclusion, fH10-15 forms neither a flexible tether nor a smooth bend. Rather, it is compact and has embedded within it a CCP module (CCP 13) that appears to be highly specialised given both its deviant structure and its striking surface charge distribution. A passive, purely structural role for this central portion of fH is unlikely.

履歴

登録	2009年8月4日	登録サイト: BMRB / 処理サイト: PDBJ
改定 1.0	2009年11月3日	Provider: repository / タイプ: Initial release
改定 1.1	2011年7月13日	Group: Version format compliance
改定 1.2	2020年2月26日	Group: Data collection / Database references / Derived calculations / Other カテゴリ: database_2 / pdbx_database_status / pdbx_nmr_software / pdbx_nmr_spectrometer / pdbx_struct_assembly / pdbx_struct_oper_list Item: _pdbx_database_status.status_code_cs / _pdbx_nmr_software.name / _pdbx_nmr_spectrometer.model
改定 1.3	2024年11月13日	Group: Data collection / Database references / Structure summary カテゴリ: chem_comp_atom / chem_comp_bond / database_2 / pdbx_entry_details / pdbx_modification_feature Item: _database_2.pdbx_DOI / _database_2.pdbx_database_accession

集合体

登録構造単位

A: Complement factor H

概要:

• 13.3 kDa, 1 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)	13,262	1
ポリマ－	13,262	1
非ポリマー	0	0
水	0	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

NMR アンサンブル

	データ	基準
コンフォーマー数 (登録 / 計算)	20 / 100	structures with the lowest energy
代表モデル	モデル #1	lowest energy

要素

#1: タンパク質

A Complement factor H / H factor 1

詳細:

分子量: 13262.045 Da / 分子数: 1 / 断片: Sushi domain, residues 690-804 / 由来タイプ: 組換発現 / 由来: (組換発現) Homo sapiens (ヒト) / 遺伝子: CFH, HF, HF1, HF2 / 発現宿主: Pichia pastoris (菌類) / 株 (発現宿主): KM71H / 参照: UniProt: P08603

• Has protein modification: Y

実験情報

実験

• 実験: 手法: 溶液NMR

NMR実験

Conditions-ID	Experiment-ID	Solution-ID	タイプ
1	1	1	2D 1H-15N HSQC
1	2	1	2D 1H-13C HSQC
1	3	1	3D CBCA(CO)NH
1	4	1	3D HN(CA)CB
1	5	1	3D HBHA(CO)NH
1	6	1	3D H(CCO)NH
1	7	1	3D (H)CCH-TOCSY
1	8	1	3D HNCO
1	9	1	3D HNCA
1	10	1	3D C(CO)NH
1	11	1	3D 1H-15N TOCSY
1	12	1	3D 1H-13C NOESY
1	13	1	3D 1H-15N NOESY
1	14	1	3D CBCANH

試料調製

• 詳細: 内容: 20mM potassium phosphate-1, 93% H2O/7% D2O / 溶媒系: 93% H2O/7% D2O
• 試料: 濃度: 20 mM / 構成要素: potassium phosphate-1
• 試料状態: イオン強度: 20 / pH: 6.6 / 圧: ambient / 温度: 298 K

NMR測定

NMRスペクトロメーター

タイプ	製造業者	モデル	磁場強度 (MHz)	Spectrometer-ID
Bruker Avance	Bruker	AVANCE	800	1
Bruker Avance	Bruker	AVANCE	600	2

解析

NMR software

名称	バージョン	開発者	分類
CNS	1.2	Brunger, Adams, Clore, Gros, Nilges and Read	精密化
CYANA	2.1	Guntert, Mumenthaler and Wuthrich	精密化
CYANA	2.1	Guntert, Mumenthaler and Wuthrich	構造決定
MOLMOL		Koradi, Billeter and Wuthrich	データ解析
Azara		Boucher	解析
ProcheckNMR		Laskowski and MacArthur	データ解析
TopSpin		Bruker Biospin	collection
WHAT IF		Vriend	データ解析

• 精密化: 手法: simulated annealing / ソフトェア番号: 1 ; 詳細: Cyana used first to calculate the structures followed by refinement in explicit water in CNS.
• 代表構造: 選択基準: lowest energy
• NMRアンサンブル: コンフォーマー選択の基準: structures with the lowest energy; 計算したコンフォーマーの数: 100 / 登録したコンフォーマーの数: 20 / 代表コンフォーマー: 1