EMDB/PDB/SASBDBから引用されている文献のデータベース

キーワード
構造解析手法	All X線回折 NMR 電子顕微鏡小角散乱中性子線回折線維回折粉末回折赤外分光 EPR FRET 理論モデルハイブリッド
著者・登録者
ジャーナル
IF	>30 >20 >10 >5 all

タイトル	Structure and Genome Release Mechanism of the Human Cardiovirus Saffold Virus 3.
ジャーナル・号・ページ	J Virol, Vol. 90, Issue 17, Page 7628-7639, Year 2016
掲載日	2016年9月1日
著者	Edukondalu Mullapudi / Jiří Nováček / Lenka Pálková / Pavel Kulich / A Michael Lindberg / Frank J M van Kuppeveld / Pavel Plevka /
PubMed 要旨	In order to initiate an infection, viruses need to deliver their genomes into cells. This involves uncoating the genome and transporting it to the cytoplasm. The process of genome delivery is not ...In order to initiate an infection, viruses need to deliver their genomes into cells. This involves uncoating the genome and transporting it to the cytoplasm. The process of genome delivery is not well understood for nonenveloped viruses. We address this gap in our current knowledge by studying the uncoating of the nonenveloped human cardiovirus Saffold virus 3 (SAFV-3) of the family Picornaviridae SAFVs cause diseases ranging from gastrointestinal disorders to meningitis. We present a structure of a native SAFV-3 virion determined to 2.5 Å by X-ray crystallography and an 11-Å-resolution cryo-electron microscopy reconstruction of an "altered" particle that is primed for genome release. The altered particles are expanded relative to the native virus and contain pores in the capsid that might serve as channels for the release of VP4 subunits, N termini of VP1, and the RNA genome. Unlike in the related enteroviruses, pores in SAFV-3 are located roughly between the icosahedral 3- and 5-fold axes at an interface formed by two VP1 and one VP3 subunit. Furthermore, in native conditions many cardioviruses contain a disulfide bond formed by cysteines that are separated by just one residue. The disulfide bond is located in a surface loop of VP3. We determined the structure of the SAFV-3 virion in which the disulfide bonds are reduced. Disruption of the bond had minimal effect on the structure of the loop, but it increased the stability and decreased the infectivity of the virus. Therefore, compounds specifically disrupting or binding to the disulfide bond might limit SAFV infection. IMPORTANCE: A capsid assembled from viral proteins protects the virus genome during transmission from one cell to another. However, when a virus enters a cell the virus genome has to be released from the capsid in order to initiate infection. This process is not well understood for nonenveloped viruses. We address this gap in our current knowledge by studying the genome release of Human Saffold virus 3 Saffold viruses cause diseases ranging from gastrointestinal disorders to meningitis. We show that before the genome is released, the Saffold virus 3 particle expands, and holes form in the previously compact capsid. These holes serve as channels for the release of the genome and small capsid proteins VP4 that in related enteroviruses facilitate subsequent transport of the virus genome into the cell cytoplasm.
リンク	J Virol / PubMed:27279624 / PubMed Central
手法	EM (単粒子) / X線回折
解像度	2.5 - 10.6 Å
構造データ	3097 5a8f EMDB-3097, PDB-5a8f: Structure and genome release mechanism of human cardiovirus Saffold virus-3 手法: EM (単粒子) / 解像度: 10.6 Å PDB-5cfc: Crystal Structure of Human Cardiovirus SAFV-3 手法: X-RAY DIFFRACTION / 解像度: 2.5 Å PDB-5cfd: Crystal Structure of DTT treated Human Cardiovirus SAFV-3 手法: X-RAY DIFFRACTION / 解像度: 2.5 Å
化合物	ChemComp-HOH: WATER / 水
由来	saffold virus (ウイルス)
キーワード	VIRAL PROTEIN (ウイルスタンパク質) / SAFFOLD / VIRUS (ウイルス) / CARDIOVIRUS / PICORNAVIRALES (ピコルナウイルス目) / A / ALTERED / VIRION (ウイルス) / PARTICLE (粒子) / CAPSID (カプシド) / GENOME (ゲノム) / RNA (リボ核酸) / SSRNA (リボ核酸) / saffold virus / pathogen (病原体) / DTT