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6W4F

NMR-driven structure of KRAS4B-GDP homodimer on a lipid bilayer nanodisc

6W4F の概要
エントリーDOI10.2210/pdb6w4f/pdb
NMR情報BMRB: 30735
分子名称Apolipoprotein A-I, GTPase KRas, 1,2-DIOLEOYL-SN-GLYCERO-3-PHOSPHOCHOLINE, ... (6 entities in total)
機能のキーワードgtpase, nanodisc, oncoprotein
由来する生物種Homo sapiens (Human)
詳細
タンパク質・核酸の鎖数4
化学式量合計152473.95
構造登録者
Lee, K.,Fang, Z.,Enomoto, M.,Gasmi-Seabrook, G.M.,Zheng, L.,Marshall, C.B.,Ikura, M. (登録日: 2020-03-10, 公開日: 2020-04-29, 最終更新日: 2024-05-15)
主引用文献Lee, K.Y.,Fang, Z.,Enomoto, M.,Gasmi-Seabrook, G.,Zheng, L.,Koide, S.,Ikura, M.,Marshall, C.B.
Two Distinct Structures of Membrane-Associated Homodimers of GTP- and GDP-Bound KRAS4B Revealed by Paramagnetic Relaxation Enhancement.
Angew.Chem.Int.Ed.Engl., 59:11037-11045, 2020
Cited by
PubMed Abstract: KRAS homo-dimerization has been implicated in the activation of RAF kinases, however, the mechanism and structural basis remain elusive. We developed a system to study KRAS dimerization on nanodiscs using paramagnetic relaxation enhancement (PRE) NMR spectroscopy, and determined distinct structures of membrane-anchored KRAS dimers in the active GTP- and inactive GDP-loaded states. Both dimerize through an α4-α5 interface, but the relative orientation of the protomers and their contacts differ substantially. Dimerization of KRAS-GTP, stabilized by electrostatic interactions between R135 and E168, favors an orientation on the membrane that promotes accessibility of the effector-binding site. Remarkably, "cross"-dimerization between GTP- and GDP-bound KRAS molecules is unfavorable. These models provide a platform to elucidate the structural basis of RAF activation by RAS and to develop inhibitors that can disrupt the KRAS dimerization. The methodology is applicable to many other farnesylated small GTPases.
PubMed: 32227412
DOI: 10.1002/anie.202001758
主引用文献が同じPDBエントリー
実験手法
SOLUTION NMR
構造検証レポート
Validation report summary of 6w4f
検証レポート(詳細版)ダウンロードをダウンロード

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件を2024-10-30に公開中

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