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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Spontaneous insertion of gene 9 minor coat protein of bacteriophage M13 in model membranes
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Spontaneous insertion of gene 9 minor coat protein of bacteriophage M13 in model membranes

机译:在模型膜中自发插入噬菌体M13的基因9次要外壳蛋白

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摘要

Gene 9 minor coat protein from bacteriophage M13 is known to be located in the inner membrane after phage infection of Escherichia coli. The way of insertion of this small protein (32 amino acids) into membranes is still unknown. Here we show that the protein is able to insert in monolayers. The limiting surface pressure of 35 mN/m for 1,2-dioleoyl-sn-glycero-3-phosphocholine and 1,2-dioleoyl-sn-glycero-3-phosphoglycerol lipid systems indicates that this spontaneous insertion can also occur in vivo. By carboxyfluorescein leakage experiments of vesicles it is demonstrated that protein monomers, or at least small aggregates, are more effective in releasing carboxyfluorescein than highly aggregated protein. The final orientation of the protein in the bilayer after insertion was addressed by proteinase K digestion, thereby making use of the unique C-terminal location of the antigenic binding site. After insertion the C-terminus is still available for the enzymatic digestion, while the N-terminus is not. This leads to the overall conclusion that the protein is able to insert spontaneously into membranes without the need of any machinery or transmembrane gradient, with the positively charged C-terminus remaining on the outside. The orientation after insertion of gene 9 protein is in agreement with the 'positive inside rule'.
机译:已知来自噬菌体M13的基因9次要外壳蛋白位于大肠杆菌噬菌体感染后的内膜中。这种小蛋白质(32个氨基酸)插入膜的方式仍然未知。在这里,我们表明该蛋白质能够插入单层。 1,2-二油酰基-sn-甘油-3-磷酸胆碱和1,2-二油酰基-sn-甘油-3-磷酸甘油脂质系统的极限表面压力为35 mN / m,表明这种自发插入也可以在体内发生。通过囊泡的羧基荧光素泄漏实验表明,蛋白质单体或至少小聚集体比高度聚集的蛋白质更有效地释放羧基荧光素。插入后双层中蛋白质的最终取向通过蛋白酶K消化来解决,从而利用抗原结合位点的独特的C末端位置。插入后,C末端仍可用于酶消化,而N末端则不可。这导致了总的结论,即该蛋白质能够自发插入膜中,而无需任何机械或跨膜梯度作用,带正电的C末端保留在外部。插入基因9蛋白后的方向与“阳性内部规则”一致。

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