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国家自然科学基金(30770676)

作品数:2 被引量:2H指数:1
相关作者:张敬美白波更多>>
相关机构:泰山医学院更多>>
发文基金:国家自然科学基金山东省自然科学基金山东省科技攻关计划更多>>
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Construction of the Subtracted cDNA Library of Striatal Neurons Treated with Long-term Morphine被引量:1
2011年
Objective To construct a morphine tolerance model in primarily cultured striatal neurons, and screen the differentially expressed genes in this model using suppression subtractive hybridization (SSH). Methods Sbtracted cDNA libraries were constructed using SSH from normal primarily cultured striatal neurons and long-term morphine treated striatal neurons (10^-5 mol/L for 72 hours). To check reliability of the cell culture model, RT-PCR was performed to detect the cAMP-responsive element-binding protein (CREB) mRNA expression. The subtracted clones were prescreened by PCR. The clones containing inserted fragments from forward libraries were sequenced and submitted to GenBank for homology analysis. And the expression levels of genes of interest were confirmed by RT-PCR. Results CREB mRNA expression showed a significant increase in morphine treated striatal neurons (62.85± 1.98) compared with normal striatal neurons (28.43 ± 1.46, P〈0.01). Thirty-six clones containing inserted fragments were randomly chosen for sequence analysis. And the 36 clones showed homology with 19 known genes and 2 novel genes. The expression of 2 novel genes, mitochondrial carrier homolog 1 (Mtchl ; 96.81±2.04 vs. 44.20±1.31, P〈0.01) and thyrnoma viral proto-oncogene 1 (Akt1 ; 122.10±2.17 vs 50.11±2.01, P〈0.01), showed a significant increase in morphine-treated striatal neurons compared with normal striatal neurons. Conclusions A reliable differential cDNA library of striatal neurons treated with long-term morphine is constructed. Mtchl and Aktl might be the candidate genes for the development of morphine tolerance.
Bo BaiHai-qing LiuJing ChenYa-lin LiHui DuHai LuPeng-li Yu
关键词:NEURON
Apelin系统的生物学特性及其作用机制被引量:1
2008年
血管紧张素受体AT-1相关的受体蛋白(APJ)是G蛋白耦联受体(GPCRs)成员之一。APJ及其内源性配体Apelin(APJ endogenous ligand)在中枢和外周广泛分布,在心血管系统、内分泌系统及免疫系统等都有重要的的生物学效应。Apelin系统已经成为新药研制非常有意义的靶点。
张敬美白波
关键词:G蛋白耦联受体APELIN
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