Ramirez-Espain Ximena, Ruiz Lidia, Martin-Malpartida Pau, Oschkinat Hartmut, Macias Maria J
Institute for Research in Biomedicine-Protein NMR group, and the Institució catalana de recerca i estudis avançats ICREA, Barcelona Science Park, Josep Samitier 1-5, E-08028 Barcelona, Spain.
J Mol Biol. 2007 Nov 9;373(5):1255-68. doi: 10.1016/j.jmb.2007.08.052. Epub 2007 Aug 29.
Formin homology 1 (FH1), is a long proline-rich region of formins, shown to bind to five WW containing proteins named formin binding proteins (FBPs). FH1 has several potential binding regions but only the PPLPx motif and its interaction with FBP11WW1 has been characterized structurally. To detect whether additional motifs exist in FH1, we synthesized five peptides and investigated their interaction with FBP28WW2, FBP11WW1 and FBP11WW2 domains. Peptides of sequence PTPPPLPP (positive control), PPPLIPPPP and PPLIPPPP (new motifs) interact with the domains with micromolar affinity. We observed that FBP28WW2 and FBP11WW2 behave differently from FBP11WW1 in terms of motif selection and affinity, since they prefer a doubly interrupted proline stretch of sequence PPLIPP. We determined the NMR structure of three complexes involving the FBP28WW2 domain and the three ligands. Depending on the peptide under study, the domain interacts with two proline residues accommodated in either the XP or the XP2 groove. This difference represents a one-turn displacement of the domain along the ligand sequence. To understand what drives this behavior, we performed further structural studies with the FBP11WW1 and a mutant of FBP28WW2 mimicking the XP2 groove of FBP11WW1. Our observations suggest that the nature of the XP2 groove and the balance of flexibility/rigidity around loop 1 of the domain contribute to the selection of the final ligand positioning in fully independent domains. Additionally, we analyzed the binding of a double WW domain region, FBP11WW1-2, to a long stretch of FH1 using fluorescence spectroscopy and NMR titrations. With this we show that the presence of two consecutive WW domains may also influence the selection of the binding mode, particularly if both domains can interact with consecutive motifs in the ligand. Our results represent the first observation of protein-ligand recognition where a pair of WW and two consecutive motifs in a ligand participate simultaneously.
formin同源结构域1(FH1)是formin的一个富含脯氨酸的长区域,已证明它能与5种含WW结构域的蛋白结合,这些蛋白被称为formin结合蛋白(FBP)。FH1有几个潜在的结合区域,但只有PPLPx基序及其与FBP11WW1的相互作用在结构上得到了表征。为了检测FH1中是否存在其他基序,我们合成了5种肽,并研究了它们与FBP28WW2、FBP11WW1和FBP11WW2结构域的相互作用。序列为PTPPPLPP(阳性对照)、PPPLIPPPP和PPLIPPPP(新基序)的肽以微摩尔亲和力与这些结构域相互作用。我们观察到,在基序选择和亲和力方面,FBP28WW2和FBP11WW2与FBP11WW1的行为不同,因为它们更喜欢序列为PPLIPP的双间断脯氨酸延伸。我们确定了涉及FBP28WW2结构域和三种配体的三种复合物的核磁共振结构。根据所研究的肽,该结构域与容纳在XP或XP2凹槽中的两个脯氨酸残基相互作用。这种差异代表了该结构域沿配体序列的一圈位移。为了理解驱动这种行为的原因,我们用FBP11WW1和模拟FBP11WW1的XP2凹槽的FBP28WW2突变体进行了进一步的结构研究。我们的观察结果表明,XP2凹槽的性质以及该结构域环1周围的灵活性/刚性平衡有助于在完全独立的结构域中选择最终的配体定位。此外,我们使用荧光光谱和核磁共振滴定分析了双WW结构域区域FBP11WW1-2与一段长FH1的结合。由此我们表明,两个连续的WW结构域的存在也可能影响结合模式的选择,特别是如果两个结构域都能与配体中的连续基序相互作用。我们的结果代表了首次观察到蛋白质-配体识别中,一对WW结构域和配体中的两个连续基序同时参与的情况。
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