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Crystal structure of botulinum neurotoxin type G light chain: Serotype divergence in substrate recognition

机译:肉毒杆菌神经毒素G型轻链的晶体结构:底物识别中的血清型差异。

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The seven serotypes (A-G) of botulinum neurotoxins (BoNTs) block neurotransmitter release through their specific proteolysis of one of the three proteins of the soluble N-ethylmaleimide-sensitive-factor attachment protein receptor (SNARE) complex. BoNTs have stringent substrate specificities that are unique for metalloprotease in that they require exceptionally long substrates (1). To understand the molecular reasons for the unique specificities of the BoNTs, we determined the crystal structure of the catalytic light chain (LC) of Clostridium botulinum neurotoxin type G (BoNT/G-LC) at 2.35 angstrom resolution. The structure of BoNT/G-LC reveals a C-terminal beta-sheet that is critical for LC oligomerization and is unlike that seen in the other LC structures. Its structural comparison with thermolysin and the available pool of LC structures reveals important serotype differences that are likely to be involved in substrate recognition of the P1' residue. In addition, structural and sequence analyses have identified a potential exosite of BoNT/G-LC that recognizes a SNARE recognition motif of VAMP.
机译:肉毒杆菌神经毒素(BoNT)的7种血清型(A-G)通过可溶性N-乙基马来酰亚胺敏感因子附着蛋白受体(SNARE)三种蛋白质之一的特异性蛋白水解作用来阻断神经递质的释放。 BoNT具有严格的底物特异性,是金属蛋白酶所特有的,因为它们需要极长的底物(1)。为了了解BoNTs独特特异性的分子原因,我们在2.35埃分辨率下确定了G型肉毒梭菌神经毒素催化性轻链(LC)的晶体结构(BoNT / G-LC)。 BoNT / G-LC的结构揭示了一个C端β-折叠,此折叠对于LC的低聚反应至关重要,与其他LC结构不同。它与嗜热菌蛋白酶的结构比较和可用的LC结构池揭示了重要的血清型差异,这些差异可能与底物识别P1'残基有关。此外,结构和序列分析已鉴定出识别VAMP的SNARE识别基序的BoNT / G-LC潜在异位。

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