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Single-stranded DNA binding proteins are required for LIM complexes to induce transcriptionally active chromatin and specify spinal neuronal identities

机译:LIM复合物需要单链DNA结合蛋白来诱导转录活性染色质并指定脊髓神经元身份

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摘要

LIM homeodomain factors regulate the development of many cell types. However, transcriptional coactivators that mediate their developmental function remain poorly defined. To address these, we examined how two related NLI-dependent LIM complexes, which govern the development of spinal motor neurons and V2a interneurons, activate the transcription in the embryonic spinal cord. We found that single-stranded DNA-binding proteins are recruited to these LIM complexes via NLI, and enhance their transcriptional activation potential. Ssdp1 and Ssdp2 (Ssdp1/2) are highly expressed in the neural tube and promote motor neuron differentiation in the embryonic spinal cord and P19 stem cells. Inhibition of Ssdp1/2 activity in mouse and chick embryos suppresses the generation of motor neurons and V2a interneurons. Furthermore, Ssdp1/2 recruit histone-modifying enzymes to the motor neuron-specifying LIM complex and trigger acetylation and lysine 4 trimethylation of histone H3, which are well-established chromatin marks for active transcription. Our results suggest that Ssdp1/2 function as crucial transcriptional coactivators for LIM complexes to specify spinal neuronal identities during development.
机译:LIM同源域因子调节许多细胞类型的发育。但是,介导其发育功能的转录共激活因子仍然定义不清。为了解决这些问题,我们研究了两个相关的NLI依赖性LIM复合物(它们控制着脊髓运动神经元和V2a interneurons的发育)如何激活胚胎脊髓中的转录。我们发现单链DNA结合蛋白通过NLI被募集到这些LIM复合物中,并增强其转录激活潜力。 Ssdp1和Ssdp2(Ssdp1 / 2)在神经管中高度表达,并促进胚胎脊髓和P19干细胞中的运动神经元分化。抑制小鼠和雏鸡胚胎中Ssdp1 / 2活性可抑制运动神经元和V2a中间神经元的生成。此外,Ssdp1 / 2将组蛋白修饰酶募集到特定于运动神经元的LIM复合体,并触发组蛋白H3的乙酰化和赖氨酸4三甲基化,这是用于主动转录的成熟染色质标记。我们的结果表明,Ssdp1 / 2作为LIM复合体在发育过程中指定脊髓神经元身份的关键转录共激活因子。

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