Dipartimento di Scienze Biochimiche "A. Rossi Fanelli," Sapienza Università di Roma, Laboratory affiliated with Istituto Pasteur Italia-Fondazione Cenci Bolognetti, Piazzale Aldo Moro 5, 00185 Roma, Italy.
Istituto di Biologia e Patologia Molecolari, CNR, Piazzale Aldo Moro 5, 00185 Roma, Italy.
J Biol Chem. 2019 Oct 25;294(43):15593-15603. doi: 10.1074/jbc.RA119.009697. Epub 2019 Sep 4.
In , the synthesis of pyridoxal 5'-phosphate (PLP), the catalytically active form of vitamin B, takes place through the so-called deoxyxylulose 5-phosphate-dependent pathway, whose last step is pyridoxine 5'-phosphate (PNP) oxidation to PLP, catalyzed by the FMN-dependent enzyme PNP oxidase (PNPOx). This enzyme plays a pivotal role in controlling intracellular homeostasis and bioavailability of PLP. PNPOx has been proposed to undergo product inhibition resulting from PLP binding at the active site. PLP has also been reported to bind tightly at a secondary site, apparently without causing PNPOx inhibition. The possible location of this secondary site has been indicated by crystallographic studies as two symmetric surface pockets present on the PNPOx homodimer, but this site has never been verified by other experimental means. Here, we demonstrate, through kinetic measurements, that PLP inhibition is actually of a mixed-type nature and results from binding of this vitamer at an allosteric site. This interpretation was confirmed by the characterization of a mutated PNPOx form, in which substrate binding at the active site is heavily hampered but PLP binding is preserved. Structural and functional connections between the active site and the allosteric site were indicated by equilibrium binding experiments, which revealed different PLP-binding stoichiometries with WT and mutant PNPOx forms. These observations open up new horizons on the mechanisms that regulate PNPOx, which may have commonalities with the mechanisms regulating human PNPOx, whose crucial role in vitamin B metabolism and epilepsy is well-known.
在 中,维生素 B 的催化活性形式吡哆醛 5'-磷酸(PLP)的合成通过所谓的依赖脱氧木酮糖 5-磷酸途径进行,其最后一步是吡哆醇 5'-磷酸(PNP)氧化为 PLP,由 FMN 依赖性酶 PNP 氧化酶(PNPOx)催化。该酶在控制细胞内 PLP 的内稳态和生物利用度方面起着关键作用。有人提出,PNPOx 会因 PLP 结合在活性部位而发生产物抑制。据报道,PLP 也会紧密结合在一个次要部位,显然不会导致 PNPOx 抑制。晶体学研究表明,这个次要部位可能位于 PNPOx 同源二聚体上的两个对称表面口袋中,但该部位从未通过其他实验手段得到证实。在这里,我们通过动力学测量证明,PLP 抑制实际上是一种混合类型的抑制,是由于该变体结合在别构部位。通过对一种突变的 PNPOx 形式的表征证实了这一解释,在这种形式中,活性部位的底物结合受到严重阻碍,但 PLP 结合得以保留。平衡结合实验表明了活性部位和别构部位之间的结构和功能联系,该实验揭示了 WT 和突变 PNPOx 形式与 PLP 的不同结合化学计量。这些观察结果为调节 PNPOx 的机制开辟了新的视野,这些机制可能与调节人类 PNPOx 的机制具有共同性,而人类 PNPOx 在维生素 B 代谢和癫痫中的关键作用是众所周知的。
