pThe serine/threonine PP-1c (protein phosphatase-1 catalytic subunit) is regulated by association with multiple regulatory subunits. Human ASPPs (apoptosis-stimulating proteins of p53) comprise three family members: ASPP1, ASPP2 and iASPP (inhibitory ASPP), which is uniquely overexpressed in many cancers. While ASPP2 and iASPP are known to bind PP-1c, we now identify novel and distinct molecular interactions that allow all three ASPPs to bind differentially to PP-1c isoforms and p53. iASPP lacks a PP-1c-binding RVXF motif; however, we show it interacts with PP-1c via a RARL sequence with a iK/isubd/sub value of 26 nM. Molecular modelling and mutagenesis of PP-1c–ASPP protein complexes identified two additional modes of interaction. First, two positively charged residues, Lyssup260/sup and Argsup261/sup on PP-1c, interact with all ASPP family members. Secondly, the C-terminus of the PP-1c α, β and γ isoforms contain a type-2 SH3 (Src homology 3) poly-proline motif (PxxPxR), which binds directly to the SH3 domains of ASPP1, ASPP2 and iASPP. In PP-1cγ this comprises residues 309–314 (PVTPPR). When the Px(T)PxR motif is deleted or mutated via insertion of a phosphorylation site mimic (T311D), PP-1c fails to bind to all three ASPP proteins. Overall, we provide the first direct evidence for PP-1c binding via its C-terminus to an SH3 protein domain./p
展开▼
机译:>丝氨酸/苏氨酸PP-1c(蛋白磷酸酶1催化亚基)受多个调节亚基的调节。人ASPP(p53的促凋亡蛋白)包含三个家族成员:ASPP1,ASPP2和iASPP(抑制性ASPP),在许多癌症中均过表达。虽然已知ASPP2和iASPP可以结合PP-1c,但我们现在确定了新颖而独特的分子相互作用,该相互作用使所有三个ASPP都可以差异性地结合到PP-1c同工型和p53。 iASPP缺少结合PP-1c的RVXF基序;但是,我们显示了它通过具有 K d 值为26nM的RARL序列与PP-1c相互作用。 PP-1c–ASPP蛋白复合物的分子建模和诱变确定了两种其他相互作用方式。首先,PP-1c上两个带正电荷的残基Lys 260 和Arg 261 与所有ASPP家族成员相互作用。其次,PP-1cα,β和γ亚型的C末端包含2型SH3(Src同源性3)多脯氨酸基序(PxxPxR),其直接与ASPP1,ASPP2和iASPP的SH3域结合。在PP-1cγ中,它包含残基309-314(PVTPPR)。当通过插入磷酸化位点模拟物(T311D)删除或突变Px(T)PxR基序时,PP-1c无法结合所有三个ASPP蛋白。总体而言,我们为PP-1c通过其C末端与SH3蛋白结构域的结合提供了直接的直接证据。
展开▼
