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The neuronal RNA binding protein Nova-1 recognizes specific RNA targets in vitro and in vivo.

机译:神经元RNA结合蛋白Nova-1在体外和体内都能识别特定的RNA靶标。

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Nova-1, an autoantigen in paraneoplastic opsoclonus myoclonus ataxia (POMA), a disorder associated with breast cancer and motor dysfunction, is a neuron-specific nuclear RNA binding protein. We have identified in vivo Nova-1 RNA ligands by combining affinity-elution-based RNA selection with protein-RNA immunoprecipitation. Starting with a pool of approximately 10(15) random 52-mer RNAs, we identified long stem-loop RNA ligands that bind to Nova-1 with high affinity (Kd of approximately 2 nM). The loop region of these RNAs harbors a approximately 15-bp pyrimidine-rich element [UCAU(N)(0-2)]3 which is essential for Nova-1 binding. Mutagenesis studies defined the third KH domain of Nova-1 and the [UCAU(N)(0-2)]3 element as necessary for in vitro binding. Consensus [UCAU (N)(0-2)], elements were identified in two neuronal pre-mRNAs, one encoding the inhibitory glycine receptor alpha2 (GlyR alpha2) and a second encoding Nova-1 itself. Nova-1 protein binds these RNAs with high affinity and specificity in vitro, and this binding can be blocked by POMA antisera. Moreover, both Nova-1 and GlyR alpha2 pre-mRNAs specifically coimmunoprecipitated with Nova-1 protein from brain extracts. Thus, Nova-1 functions as a sequence-specific nuclear RNA binding protein in vivo; disruption of the specific interaction between Nova-1 and GlyR alpha2 pre-mRNA may underlie the motor dysfunction seen in POMA.
机译:Nova-1是一种与乳腺癌和运动功能障碍有关的副肿瘤性肌阵挛性共济失调(POMA)的自身抗原,是一种神经元特异性核RNA结合蛋白。我们已经通过结合基于亲和洗脱的RNA选择与蛋白质RNA免疫沉淀来鉴定体内Nova-1 RNA配体。从大约10(15)个随机的52-mer RNA池开始,我们鉴定了以高亲和力(Kd约为2 nM)结合Nova-1的长茎环RNA配体。这些RNA的环区包含大约15 bp的富含嘧啶的元件[UCAU(N)(0-2)] 3,这对于Nova-1结合至关重要。诱变研究确定了Nova-1的第三个KH结构域和[UCAU(N)(0-2)] 3元件是体外结合所必需的。共识[UCAU(N)(0-2)],在两个神经元前mRNA中鉴定出元件,一个编码抑制性甘氨酸受体α2(GlyR alpha2),第二个编码Nova-1本身。 Nova-1蛋白在体外以高亲和力和特异性结合这些RNA,并且这种结合可以被POMA抗血清阻断。此外,Nova-1和GlyR alpha2 pre-mRNA均与脑提取物中的Nova-1蛋白特异性免疫共沉淀。因此,Nova-1在体内起序列特异性核RNA结合蛋白的作用。 Nova-1和GlyR alpha2 pre-mRNA之间特异性相互作用的破坏可能是POMA中所见的运动功能障碍的基础。

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