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首页> 外文期刊>Protein Science: A Publication of the Protein Society >Backbone (15)N relaxation analysis of the N-terminal domain of the HTLV-I capsid protein and comparison with the capsid protein of HIV-1.
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Backbone (15)N relaxation analysis of the N-terminal domain of the HTLV-I capsid protein and comparison with the capsid protein of HIV-1.

机译:HTLV-1衣壳蛋白N末端结构域的骨干(15)N松弛分析,并与HIV-1衣壳蛋白进行比较。

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摘要

Human T-cell leukemia virus type 1 (HTLV-I) is an oncogenic retrovirus that exhibits specific tropism for human T-cells. The capsid (CA) proteins of retroviruses share highly conserved secondary and tertiary structures. However, they can form quaternary structures (assembled cores) that are conical (e.g., the lentivirus subgroup, including HIV) or spherical (e.g., the oncovirus subgroup, including HTLV). The intrinsic features that drive these differences are not understood. So far, only structural studies have been used as a basis for comparison. Dynamics may play a role in particle formation. High-resolution nuclear magnetic resonance (NMR) (15)N relaxation data (T(1), T(1rho), and NOE) have been used to characterize the backbone dynamics of the N-terminal domain (NTD) of the oncovirus HTLV-I and to compare with the CA NTD of HIV-1. Large variations in the (15)N heteronuclear NOEs and transversal relaxation rates for individual residues are consistent with the bundle RMSD of the previously calculatedNMR structures. The beta-hairpin and CyP-A loop exhibit different mobility in HTLV-I and HIV-1. The overall hydrodynamic property of the HTLV-I capsid NTD is quite distinct from the HIV-1.
机译:1型人类T细胞白血病病毒(HTLV-1)是致癌性逆转录病毒,对人类T细胞表现出特定的嗜性。逆转录病毒的衣壳蛋白(CA)具有高度保守的二级和三级结构。然而,它们可以形成圆锥形(例如,包括HIV的慢病毒亚组)或球形(例如,包括HTLV的癌病毒亚组)的四级结构(组装的核)。导致这些差异的内在特征尚不清楚。到目前为止,仅将结构研究用作比较的基础。动力学可能在颗粒形成中起作用。高分辨率核磁共振(NMR)(15)N弛豫数据(T(1),T(1rho)和NOE)已用于表征瘤病毒HTLV的N末端域(NTD)的骨干动力学-I并与HIV-1的CA NTD进行比较。 (15)N异核NOE的巨大变化和单个残基的横向弛豫速率与先前计算的NMR结构的束RMSD一致。 β-发夹和CyP-A环在HTLV-1和HIV-1中表现出不同的迁移率。 HTLV-1衣壳NTD的总体流体力学性质与HIV-1完全不同。

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