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StAR-related lipid transfer domain protein 5 binds primary bile acids

机译:与StAR相关的脂质转移域蛋白5结合初级胆汁酸

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摘要

Steroidogenic acute regulatory-related lipid transfer (START) domain proteins are involved in the nonvesicular intracellular transport of lipids and sterols. The STARD1 (STARD1 and STARD3) and STARD4 subfamilies (STARD4–6) have an internal cavity large enough to accommodate sterols. To provide a deeper understanding on the structural biology of this domain, the binding of sterols to STARD5, a member of the STARD4 subfamily, was monitored. The SAR by NMR [1H-15N heteronuclear single-quantum coherence (HSQC)] approach, complemented by circular dichroism (CD) and isothermal titration calorimetry (ITC), was used. Titration of STARD5 with cholic (CA) and chenodeoxycholic acid (CDCA), ligands of the farnesoid X receptor (FXR), leads to drastic perturbation of the 1H-15N HSQC spectra and the identification of the residues in contact with those ligands. The most perturbed residues in presence of ligands are lining the internal cavity of the protein. Ka values of 1.8·10−4 M−1 and 6.3·104 M−1 were measured for CA and CDCA, respectively. This is the first report of a START domain protein in complex with a sterol ligand. Our original findings indicate that STARD5 may be involved in the transport of bile acids rather than cholesterol.
机译:类固醇激素相关的急性调节相关脂质转移(START)结构域蛋白参与脂质和固醇的非囊泡细胞内转运。 STARD1(STARD1和STARD3)和STARD4子家族(STARD4-6)的内部腔体足够容纳甾醇。为了提供对该结构域的结构生物学的更深入的了解,对固醇与STARD4亚家族成员STARD5的结合进行了监测。通过NMR [ 1 H- 15 N异核单量子相干(HSQC)]方法合成的SAR,辅以圆二色性(CD)和等温滴定量热(ITC),被使用了。用法尼醇X受体(FXR)的配体胆酸(CA)和鹅去氧胆酸(CDCA)滴定STARD5会导致对 1 H- 15 N的剧烈扰动HSQC光谱以及与这些配体接触的残基的鉴定。在配体存在的情况下,最易受干扰的残基排列在蛋白质的内腔中。测量的Ka值为1.8·10− 4 M -1 和6.3·10 4 M -1 CA和CDCA分别。这是START结构域蛋白与固醇配体复合的首次报道。我们最初的发现表明STARD5可能参与胆汁酸而不是胆固醇的运输。

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