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VPAC2 receptor agonist BAY 55-9837 increases SMN protein levels and moderates disease phenotype in severe spinal muscular atrophy mouse models

机译：在严重的脊髓性肌萎缩症小鼠模型中，VPAC2受体激动剂BAY 55-9837可提高SMN蛋白水平并缓解疾病表型

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Abstract Background Spinal Muscular Atrophy (SMA) is one of the most common inherited causes of infant death and is caused by the loss of functional survival motor neuron (SMN) protein due to mutations or deletion in the SMN1 gene. One of the treatment strategies for SMA is to induce the expression of the protein from the homologous SMN2 gene, a rescuing paralog for SMA. Methods and results Here we demonstrate the promise of pharmacological modulation of SMN2 gene by BAY 55-9837, an agonist of the vasoactive intestinal peptide receptor 2 (VPAC2), a member of G protein coupled receptor family. Treatment with BAY 55-9837 lead to induction of SMN protein levels via activation of MAPK14 or p38 pathway in vitro. Importantly, BAY 55-9837 also ameliorated disease phenotype in severe SMA mouse models. Conclusion Our findings suggest the VPAC2 pathway is a potential SMA therapeutic target.

机译：摘要背景脊髓性肌萎缩症（SMA）是婴儿死亡的最常见遗传原因之一，其原因是SMN1基因突变或缺失导致功能性生存运动神经元（SMN）蛋白丧失。 SMA的治疗策略之一是从同源SMN2基因（SMA的拯救旁系）诱导蛋白质表达。方法和结果在这里，我们证明了BAY 55-9837是G蛋白偶联受体家族成员之一的血管活性肠肽受体2（VPAC2）的激动剂对SMN2基因的药理调节作用。用BAY 55-9837处理可通过激活MAPK14或p38途径体外诱导SMN蛋白水平的诱导。重要的是，BAY 55-9837还改善了严重SMA小鼠模型中的疾病表型。结论我们的发现表明VPAC2途径是潜在的SMA治疗靶标。

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Hadwen, Jeremiah; MacKenzie, Duncan; Shamim, Fahad; Mongeon, Kevin; Holcik, Martin; MacKenzie, Alex; Farooq, Faraz;
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1. VPAC2 receptor agonist BAY 55-9837 increases SMN protein levels and moderates disease phenotype in severe spinal muscular atrophy mouse models [J] . Jeremiah Hadwen, Duncan MacKenzie, Fahad Shamim, Orphanet journal of rare diseases . 2014,第2期

机译：在严重的脊髓性肌萎缩症小鼠模型中，VPAC2受体激动剂BAY 55-9837可提高SMN蛋白水平并缓解疾病表型
2. Increasing SMN levels using the histone deacetylase inhibitor SAHA ameliorates defects in skeletal muscle microvasculature in a mouse model of severe spinal muscular atrophy [J] . SomersE., RiesslandM., SchremlJ., Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences . 2013,第Null期

机译：使用组蛋白脱乙酰基酶抑制剂SAHA提高SMN水平可改善严重脊髓性肌萎缩症小鼠模型中骨骼肌微血管的缺陷
3. Postsymptomatic restoration of SMN rescues the disease phenotype in a mouse model of severe spinal muscular atrophy [J] . Cathleen M. Lutz, Shingo Kariya, Sunita Patruni, The journal of clinical investigation . 2011,第8期

机译：SMN的症状后恢复可挽救严重脊髓性肌肉萎缩症小鼠模型的疾病表型
4. The Smn-independent beneficial effects of trichostatin A on an intermediate mouse model of spinal muscular atrophy. [D] . Yazdani, Armin. 2014

机译：曲古抑菌素A对脊髓性肌萎缩症的中级小鼠模型的Smn依赖性有益作用。
5. VPAC2 receptor agonist BAY 55-9837 increases SMN protein levels and moderates disease phenotype in severe spinal muscular atrophy mouse models [O] . Jeremiah Hadwen, Duncan MacKenzie, Fahad Shamim, 2014

机译：在严重的脊髓性肌萎缩症小鼠模型中VPAC2受体激动剂BAY 55-9837可提高SMN蛋白水平并缓解疾病表型
6. VPAC2 receptor agonist BAY 55-9837 increases SMN protein levels and moderates disease phenotype in severe spinal muscular atrophy mouse models [O] . Jeremiah Hadwen, Duncan MacKenzie, Fahad Shamim, 2014

机译：在严重的脊髓性肌萎缩症小鼠模型中，VPAC2受体激动剂BAY 55-9837可提高SMN蛋白水平并缓解疾病表型

VPAC2 receptor agonist BAY 55-9837 increases SMN protein levels and moderates disease phenotype in severe spinal muscular atrophy mouse models

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