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Domain Contributions to Signaling Specificity Differences Between Ras-Guanine Nucleotide Releasing Factor (Ras-GRF) 1 and Ras-GRF2

机译:Ras-鸟嘌呤核苷酸释放因子(Ras-GRF)1和Ras-GRF2之间的信号特异性差异的域贡献。

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摘要

Ras-GRF1 (GRF1) and Ras-GRF2 (GRF2) constitute a family of similar calcium sensors that regulate synaptic plasticity. They are both guanine exchange factors that contain a very similar set of functional domains, including N-terminal pleckstrin homology, coiled-coil, and calmodulin-binding IQ domains and C-terminal Dbl homology Rac-activating domains, Ras-exchange motifs, and CDC25 Ras-activating domains. Nevertheless, they regulate different forms of synaptic plasticity. Although both GRF proteins transduce calcium signals emanating from NMDA-type glutamate receptors in the CA1 region of the hippocampus, GRF1 promotes LTD, whereas GRF2 promotes θ-burst stimulation-induced LTP (TBS-LTP). GRF1 can also mediate high frequency stimulation-induced LTP (HFS-LTP) in mice over 2-months of age, which involves calcium-permeable AMPA-type glutamate receptors. To add to our understanding of how proteins with similar domains can have different functions, WT and various chimeras between GRF1 and GRF2 proteins were tested for their abilities to reconstitute defective LTP and/or LTD in the CA1 hippocampus of Grf1/Grf2 double knock-out mice. These studies revealed a critical role for the GRF2 CDC25 domain in the induction of TBS-LTP by GRF proteins. In contrast, the N-terminal pleckstrin homology and/or coiled-coil domains of GRF1 are key to the induction of HFS-LTP by GRF proteins. Finally, the IQ motif of GRF1 determines whether a GRF protein can induce LTD. Overall, these findings show that for the three forms of synaptic plasticity that are regulated by GRF proteins in the CA1 hippocampus, specificity is encoded in only one or two domains, and a different set of domains for each form of synaptic plasticity.
机译:Ras-GRF1(GRF1)和Ras-GRF2(GRF2)构成了一系列调节突触可塑性的类似钙传感器。它们都是鸟嘌呤交换因子,它们包含一组非常相似的功能域,包括N末端pleckstrin同源性,卷曲螺旋和结合钙调蛋白的IQ域以及C末端Dbl同源性Rac激活域,Ras交换基序和CDC25 Ras激活域。然而,它们调节不同形式的突触可塑性。尽管这两种GRF蛋白都转导海马CA1区NMDA型谷氨酸受体产生的钙信号,但GRF1促进LTD,而GRF2促进θ爆发刺激诱导的LTP(TBS-LTP)。 GRF1还可以介导两个月以上的小鼠中的高频刺激诱导的LTP(HFS-LTP),这涉及钙可渗透的AMPA型谷氨酸受体。为了加深我们对具有相似结构域的蛋白质如何具有不同功能的理解,测试了WT和GRF1与GRF2蛋白之间的各种嵌合体重组Grf1 / Grf2双敲除CA1海马中缺陷LTP和/或LTD的能力。老鼠。这些研究揭示了GRF2 CDC25结构域在GRF蛋白诱导TBS-LTP中的关键作用。相反,GRF1的N末端pleckstrin同源性和/或卷曲螺旋结构域是GRF蛋白诱导HFS-LTP的关键。最后,GRF1的IQ基序决定了GRF蛋白是否可以诱导LTD。总体而言,这些发现表明,对于CA1海马中由GRF蛋白调节的三种形式的突触可塑性,特异性仅在一个或两个域中编码,而每种形式的突触可塑性都具有一组不同的域。

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