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系统分析社会变形虫 Dd 中 γ-氨基丁酸(GABA)代谢和功能。

Systematic analysis of γ-aminobutyric acid (GABA) metabolism and function in the social amoeba Dictyostelium discoideum.

机构信息

Department of Biological Sciences, Vanderbilt University, Nashville, Tennessee 37232, USA.

出版信息

J Biol Chem. 2013 May 24;288(21):15280-90. doi: 10.1074/jbc.M112.427047. Epub 2013 Apr 2.

Abstract

While GABA has been suggested to regulate spore encapsulation in the social amoeba Dictyostelium discoideum, the metabolic profile and other potential functions of GABA during development remain unclear. In this study, we investigated the homeostasis of GABA metabolism by disrupting genes related to GABA metabolism and signaling. Extracellular levels of GABA are tightly regulated during early development, and GABA is generated by the glutamate decarboxylase, GadB, during growth and in early development. However, overexpression of the prespore-specific homologue, GadA, in the presence of GadB reduces production of extracellular GABA. Perturbation of extracellular GABA levels delays the process of aggregation. Cytosolic GABA is degraded by the GABA transaminase, GabT, in the mitochondria. Disruption of a putative vesicular GABA transporter (vGAT) homologue DdvGAT reduces secreted GABA. We identified the GABAB receptor-like family member GrlB as the major GABA receptor during early development, and either disruption or overexpression of GrlB delays aggregation. This delay is likely the result of an abolished pre-starvation response and late expression of several "early" developmental genes. Distinct genes are employed for GABA generation during sporulation. During sporulation, GadA alone is required for generating GABA and DdvGAT is likely responsible for GABA secretion. GrlE but not GrlB is the GABA receptor during late development.

摘要

虽然 GABA 被认为可以调节变形虫 Dictyostelium discoideum 的孢子包裹,但 GABA 在发育过程中的代谢谱和其他潜在功能仍不清楚。在这项研究中,我们通过干扰与 GABA 代谢和信号相关的基因来研究 GABA 代谢的动态平衡。在早期发育过程中,GABA 的细胞外水平受到严格调控,GABA 在生长和早期发育过程中由谷氨酸脱羧酶 GadB 产生。然而,在存在 GadB 的情况下过表达孢子特异性同源物 GadA 会减少细胞外 GABA 的产生。干扰细胞外 GABA 水平会延迟聚集过程。细胞质 GABA 被线粒体中的 GABA 转氨酶 GabT 降解。破坏推定的囊泡 GABA 转运体(vGAT)同源物 DdvGAT 会减少分泌的 GABA。我们鉴定出 GABAB 受体样家族成员 GrlB 是早期发育过程中的主要 GABA 受体,无论是 GrlB 的破坏还是过表达都会延迟聚集。这种延迟可能是由于饥饿前反应的消失和几个“早期”发育基因的晚期表达所致。在孢子形成过程中使用了不同的基因来产生 GABA。在孢子形成过程中,仅 GadA 就足以产生 GABA,而 DdvGAT 可能负责 GABA 的分泌。在晚期发育过程中,GrlE 而不是 GrlB 是 GABA 受体。

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