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P(II)介导的 2-氧戊二酸感应破坏 Amt-GlnK 复合物的机制。

Mechanism of disruption of the Amt-GlnK complex by P(II)-mediated sensing of 2-oxoglutarate.

机构信息

Institut für organische Chemie und Biochemie, Albert-Ludwigs-Universität Freiburg, Freiburg, Germany.

出版信息

PLoS One. 2011;6(10):e26327. doi: 10.1371/journal.pone.0026327. Epub 2011 Oct 19.

Abstract

GlnK proteins regulate the active uptake of ammonium by Amt transport proteins by inserting their regulatory T-loops into the transport channels of the Amt trimer and physically blocking substrate passage. They sense the cellular nitrogen status through 2-oxoglutarate, and the energy level of the cell by binding both ATP and ADP with different affinities. The hyperthermophilic euryarchaeon Archaeoglobus fulgidus possesses three Amt proteins, each encoded in an operon with a GlnK ortholog. One of these proteins, GlnK2 was recently found to be incapable of binding 2-OG, and in order to understand the implications of this finding we conducted a detailed structural and functional analysis of a second GlnK protein from A. fulgidus, GlnK3. Contrary to Af-GlnK2 this protein was able to bind both ATP/2-OG and ADP to yield inactive and functional states, respectively. Due to the thermostable nature of the protein we could observe the exact positioning of the notoriously flexible T-loops and explain the binding behavior of GlnK proteins to their interaction partner, the Amt proteins. A thermodynamic analysis of these binding events using microcalorimetry evaluated by microstate modeling revealed significant differences in binding cooperativity compared to other characterized P(II) proteins, underlining the diversity and adaptability of this class of regulatory signaling proteins.

摘要

GlnK 蛋白通过将其调节 T 环插入 Amt 转运蛋白的转运通道,物理阻断底物通道,从而调节铵的主动摄取。它们通过 2-氧戊二酸感应细胞的氮状态,通过结合不同亲和力的 ATP 和 ADP 来感应细胞的能量水平。超嗜热古菌 Archaeoglobus fulgidus 拥有三种 Amt 蛋白,每种蛋白都与 GlnK 同源物在操纵子中编码。最近发现其中一种蛋白 GlnK2 不能结合 2-OG,为了了解这一发现的意义,我们对 A. fulgidus 的第二种 GlnK 蛋白 GlnK3 进行了详细的结构和功能分析。与 Af-GlnK2 不同,该蛋白能够分别结合 ATP/2-OG 和 ADP,产生无活性和有活性的状态。由于该蛋白的热稳定性,我们可以观察到臭名昭著的灵活 T 环的精确定位,并解释 GlnK 蛋白与其相互作用伙伴 Amt 蛋白的结合行为。使用微态模型进行微热量法的热力学分析评估这些结合事件表明,与其他表征的 P(II)蛋白相比,结合协同性存在显著差异,突出了这类调节信号蛋白的多样性和适应性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5823/3198391/f1f02f83f362/pone.0026327.g001.jpg

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