Zamora-Caballero Sara, Šiaučiunaite-Gaubard Lina, Bravo Jeronimo
Department of Genomics and Proteomics, Instituto de Biomedicina de Valencia - CSIC, Jaime Roig 11, 46010 Valencia, Spain.
Acta Crystallogr F Struct Biol Commun. 2015 Jun;71(Pt 6):684-7. doi: 10.1107/S2053230X15006457. Epub 2015 May 20.
Acidic leucine-rich nuclear phosphoprotein 32A (PP32A) is a tumour suppressor whose expression is altered in many cancers. It is an apoptotic enhancer that stimulates apoptosome-mediated caspase activation and also forms part of a complex involved in caspase-independent apoptosis (the SET complex). Crystals of a fragment of human PP32A corresponding to the leucine-rich repeat domain, a widespread motif suitable for protein-protein interactions, have been obtained. The structure has been refined to 1.56 Å resolution. This domain was previously solved at 2.4 and 2.69 Å resolution (PDB entries 2je0 and 2je1, respectively). The new high-resolution structure shows some differences from previous models: there is a small displacement in the turn connecting the first α-helix (α1) to the first β-strand (β1), which slightly changes the position of α1 in the structure. The shift in the turn is observed in the context of a new crystal packing unrelated to those of previous structures.
富含酸性亮氨酸的核磷蛋白32A(PP32A)是一种肿瘤抑制因子,其表达在多种癌症中发生改变。它是一种凋亡增强剂,可刺激凋亡小体介导的半胱天冬酶激活,也是参与非半胱天冬酶依赖性凋亡的复合物(SET复合物)的一部分。已获得与富含亮氨酸重复结构域相对应的人PP32A片段的晶体,该结构域是一种广泛存在的适用于蛋白质-蛋白质相互作用的基序。结构已精修至1.56 Å分辨率。该结构域先前分别以2.4 Å和2.69 Å分辨率解析(分别为PDB条目2je0和2je1)。新的高分辨率结构与先前模型存在一些差异:连接第一个α螺旋(α1)和第一个β链(β1)的转角处有一个小位移,这略微改变了α1在结构中的位置。在与先前结构无关的新晶体堆积情况下观察到了转角处的位移。
