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噬菌体φ29蛋白p6处于单体-二聚体平衡状态,在体内发现的毫摩尔浓度下会转变为更高的缔合状态。

Phage phi29 protein p6 is in a monomer-dimer equilibrium that shifts to higher association states at the millimolar concentrations found in vivo.

作者信息

Abril A M, Salas M, Andreu J M, Hermoso J M, Rivas G

机构信息

Centro de Biología Molecular "Severo Ochoa" (CSIC-UAM), Universidad Autónoma, Cantoblanco, 28049 Madrid, Spain.

出版信息

Biochemistry. 1997 Sep 30;36(39):11901-8. doi: 10.1021/bi970994e.

DOI:10.1021/bi970994e
PMID:9305983
Abstract

Protein p6 from Bacillus subtilis phage phi29 (Mr = 11 800) binds in vitro to DNA forming a large nucleoprotein complex in which the DNA wraps a multimeric protein core. The high intracellular abundance of protein p6 together with its ability to bind the whole phi29 DNA in vitro strongly suggests that it plays a role in viral genome organization. We have determined by sedimentation equilibrium analysis that protein p6 (1-100 microM range), in the absence of DNA, is in a monomer-dimer equilibrium, with an association constant (K2) of approximately 2 x 10(5) M-1. The intracellular concentration of protein p6 (approximately 1 mM) was estimated measuring the number of copies per cell (7 x 10(5)) and the cell volume (1 x 10(-15) L). At concentrations around 1 mM, protein p6 associates into oligomers. This self-association behavior is compatible with a dimer-hexamer model (K2,6 = 3.2 x 10(8) M-2) or with an isodesmic association of the dimer (K = 950 M-1), because the apparent weight-average molecular mass (Mw,a) does not reach saturation at the highest protein concentrations. The sedimentation coefficients of protein p6 monomer and dimer were 1.4 and 2.0, respectively, compatible with translational frictional ratios (f/fo) of 1.15 and 1.30, which slightly deviate from the hydrodynamics of a rigid globular protein. Taking together these results and considering the structure of the nucleoprotein complex, we speculate that the observed oligomers of protein p6 could mimic a scaffold on which DNA folds to form the nucleoprotein complex in vivo.

摘要

来自枯草芽孢杆菌噬菌体phi29的p6蛋白(分子量 = 11800)在体外与DNA结合,形成一个大型核蛋白复合物,其中DNA环绕着一个多聚体蛋白核心。p6蛋白在细胞内的高丰度及其在体外结合整个phi29 DNA的能力强烈表明它在病毒基因组组织中发挥作用。我们通过沉降平衡分析确定,在没有DNA的情况下,p6蛋白(浓度范围为1 - 100 microM)处于单体 - 二聚体平衡状态,缔合常数(K2)约为2×10⁵ M⁻¹。通过测量每个细胞中的拷贝数(7×10⁵)和细胞体积(1×10⁻¹⁵ L),估算出p6蛋白在细胞内的浓度约为1 mM。在浓度约为1 mM时,p6蛋白缔合成寡聚体。这种自缔合行为与二聚体 - 六聚体模型(K2,6 = 3.2×10⁸ M⁻²)或二聚体的等距缔合(K = 950 M⁻¹)相符,因为在最高蛋白浓度下,表观重均分子量(Mw,a)并未达到饱和。p6蛋白单体和二聚体的沉降系数分别为1.4和2.0,与平移摩擦比(f/fo)1.15和1.30相符,这与刚性球状蛋白的流体动力学略有偏差。综合这些结果并考虑核蛋白复合物的结构,我们推测观察到的p6蛋白寡聚体可能模拟了一个支架,DNA在其上折叠以在体内形成核蛋白复合物。

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