Atg13 N 端结构域的形态及其功能:招募 PtdIns 3-kinase 所需的 HORMA 结构域。
What the N-terminal domain of Atg13 looks like and what it does: a HORMA fold required for PtdIns 3-kinase recruitment.
机构信息
Laboratory of Molecular Biology; National Institute of Diabetes and Digestive and Kidney Diseases; National Institutes of Health; Bethesda, MD USA.
出版信息
Autophagy. 2013 Jul;9(7):1112-4. doi: 10.4161/auto.24896. Epub 2013 May 2.
Atg13 is a subunit of the Atg1 complex that is involved in autophagy. The middle and C-terminal regions of Atg13 are intrinsically disordered and rich in regulatory phosphorylation sites. Thus far, there have been no structural data for any part of Atg13, and no function assigned to its N-terminal domain. We crystallized this domain, and found that it has a HORMA (Hop1, Rev7, Mad2) fold. We showed that the Atg13 HORMA domain is required for autophagy and for recruitment of the phosphatidylinositol (PtdIns) 3-kinase subunit Atg14, but is not required for Atg1 interaction or Atg13 recruitment to the PAS. The HORMA domain of Atg13 is similar to the closed conformation of the spindle checkpoint protein Mad2. A pair of conserved arginines was identified in the structure, and tested functionally in yeast. These residues are important for autophagy, as mutations abrogate autophagy and block Atg14 recruitment. The location of these Arg residues in the structure suggests that the Atg13 HORMA domain could act as a phosphorylation-dependent conformational switch.
Atg13 是参与自噬的 Atg1 复合物的一个亚基。Atg13 的中部和 C 末端区域是固有无序的,富含调节性磷酸化位点。到目前为止,还没有 Atg13 的任何部分的结构数据,也没有为其 N 端结构域分配功能。我们对这个结构域进行了结晶,并发现它具有 HORMA(Hop1、Rev7、Mad2)折叠结构。我们表明,Atg13 的 HORMA 结构域对于自噬和磷酸肌醇(PtdIns)3-激酶亚基 Atg14 的募集是必需的,但对于 Atg1 相互作用或 Atg13 募集到 PAS 是不需要的。Atg13 的 HORMA 结构域与纺锤体检查点蛋白 Mad2 的封闭构象相似。在结构中鉴定出一对保守的精氨酸,并在酵母中进行了功能测试。这些残基对于自噬很重要,因为突变会阻断自噬并阻止 Atg14 的募集。这些 Arg 残基在结构中的位置表明,Atg13 的 HORMA 结构域可以作为一种依赖于磷酸化的构象开关。
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