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关于丙酮酸和果糖 6-磷酸同时激活根癌农杆菌 ADP-葡萄糖焦磷酸化酶。

On the simultaneous activation of Agrobacterium tumefaciens ADP-glucose pyrophosphorylase by pyruvate and fructose 6-phosphate.

机构信息

Instituto de Agrobiotecnología Del Litoral, UNL, CONICET, FBCB, Colectora Ruta Nacional 168 Km 0, 3000, Santa Fe, Argentina; Department of Chemistry and Biochemistry, Loyola University Chicago, 1068 W. Sheridan Rd., Chicago, IL, 60660, USA.

Instituto de Agrobiotecnología Del Litoral, UNL, CONICET, FBCB, Colectora Ruta Nacional 168 Km 0, 3000, Santa Fe, Argentina.

出版信息

Biochimie. 2020 Apr-May;171-172:23-30. doi: 10.1016/j.biochi.2020.01.012. Epub 2020 Jan 31.

DOI:10.1016/j.biochi.2020.01.012
PMID:32014504
Abstract

Bacterial ADP-glucose pyrophosphorylases are allosterically regulated by metabolites that are key intermediates of central pathways in the respective microorganism. Pyruvate (Pyr) and fructose 6-phosphate (Fru6P) activate the enzyme from Agrobacterium tumefaciens by increasing V about 10- and 20-fold, respectively. Here, we studied the combined effect of both metabolites on the enzyme activation. Our results support a model in which there is a synergistic binding of these two activators to two distinct sites and that each activator leads the enzyme to distinct active forms with different properties. In presence of both activators, Pyr had a catalytically dominant effect over Fru6P determining the active conformational state. By mutagenesis we obtained enzyme variants still sensitive to Pyr activation, but in which the allosteric signal by Fru6P was disrupted. This indicated that the activation mechanism for each effector was not the same. The ability for this enzyme to have more than one allosteric activator site, active forms, and allosteric signaling mechanisms is critical to expand the evolvability of its regulation. These synergistic interactions between allosteric activators may represent a feature in other allosteric enzymes.

摘要

细菌 ADP-葡萄糖焦磷酸化酶受代谢物的变构调节,这些代谢物是相应微生物中心途径的关键中间产物。丙酮酸 (Pyr) 和果糖 6-磷酸 (Fru6P) 通过分别将酶的 V 增加约 10 倍和 20 倍来激活来自根瘤农杆菌的酶。在这里,我们研究了这两种代谢物对酶激活的协同作用。我们的研究结果支持这样一种模型,即这两种激活剂协同结合到两个不同的位点,并且每个激活剂使酶具有不同性质的不同活性形式。在存在两种激活剂的情况下,Pyr 对 Fru6P 具有催化主导作用,决定了活性构象状态。通过突变,我们获得了仍然对 Pyr 激活敏感但 Fru6P 的变构信号被破坏的酶变体。这表明每个效应物的激活机制并不相同。该酶具有多个变构激活剂结合位点、活性形式和变构信号机制的能力,对于扩大其调节的可进化性至关重要。这种变构激活剂之间的协同相互作用可能是其他变构酶的一个特征。

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