White Mark Andrew, Mast Natalia, Bjorkhem Ingemar, Johnson Eric F, Stout C David, Pikuleva Irina A
Sealy Center for Structural and Molecular Biophysics, UTMB Galveston, TX 77555, USA.
Acta Crystallogr D Biol Crystallogr. 2008 May;64(Pt 5):487-95. doi: 10.1107/S0907444908004046. Epub 2008 Apr 19.
Human cytochrome P450 46A1 (CYP46A1) is one of the key enzymes in cholesterol homeostasis in the brain. The crystallization and heavy-atom structure solution of an active truncated CYP46A1 in complex with the high-affinity substrate analogue cholesterol-3-sulfate (CH-3S) is reported. The 2.6 angstroms structure of CYP46A1-CH-3S was solved using both anion and cation heavy-atom salts. In addition to the native anomalous signal from the haem iron, an NaI anion halide salt derivative and a complementary CsCl alkali-metal cation salt derivative were used. The general implications of the use of halide and alkali-metal quick soaks are discussed. The importance of using isoionic strength buffers, the titration of heavy-atom salts into different ionic species and the role of concentration are considered. It was observed that cation/anion-binding sites will occasionally overlap, which could negatively impact upon mixed RbBr soaks used for multiple anomalous scatterer MAD (MMAD). The use of complementary cation and anion heavy-atom salt derivatives is a convenient and powerful tool for MIR(AS) structure solution.
人细胞色素P450 46A1(CYP46A1)是大脑胆固醇稳态中的关键酶之一。本文报道了一种活性截短型CYP46A1与高亲和力底物类似物胆固醇-3-硫酸盐(CH-3S)复合物的结晶及重原子结构解析。利用阴离子和阳离子重原子盐解析了CYP46A1-CH-3S的2.6埃结构。除了血红素铁的天然异常信号外,还使用了碘化钠阴离子卤化物盐衍生物和互补的氯化铯碱金属阳离子盐衍生物。讨论了使用卤化物和碱金属快速浸泡的一般意义。考虑了使用等离子强度缓冲液、将重原子盐滴定到不同离子种类中的重要性以及浓度的作用。观察到阳离子/阴离子结合位点偶尔会重叠,这可能会对用于多异常散射体MAD(MMAD)的混合溴化铷浸泡产生负面影响。使用互补的阳离子和阴离子重原子盐衍生物是用于MIR(AS)结构解析的便捷而强大的工具。
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