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首页> 外文期刊>European Journal of Pharmacology: An International Journal >Screening for novel lead compounds increasing insulin expression in medullary thymic epithelial cells
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Screening for novel lead compounds increasing insulin expression in medullary thymic epithelial cells

机译:筛选新型的增加髓质胸腺上皮细胞胰岛素表达的先导化合物

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Insulin expression in the thymus has been implicated in regulating the negative selection of autoreactive T cells and in mediating the central immune tolerance to pancreatic beta-cells. Thymic insulin expression modulation might be an important drug target for preventing type 1 diabetes. We performed a high-throughput screening to identify compounds with such activity. A reporter plasmid was constructed with the human insulin promoter sequence including a short allele of the upstream variable number tandem repeat (VNTR) sequence (32 repeats), subcloned into the pGL4.17 vector. The plasmid was stably transfected into an insulin-transcribing medullary thymic epithelial cell (mTEC) line. Primary high-throughput screening assays were carried out by stimulating with candidate compounds for 24 h, and the activity of luciferase was measured. Positive compounds were further validated by real-time PCR. Of 19,707 compounds, we identified one compound that could enhance mTEC insulin expression, as confirmed by real-time PCR. We also observed that transfection with the autoimmune regulator (AIRE) increased endogenous AIRE expression in mTECs. Our insulin-VNTRI-promoter reporter system is consistent with the insulin expression regulation in mTECs, and one compound that was identified could increase insulin expression in mTECs. A positive feedback effect of AIRE in mTECS was observed. Whether these efforts in murine thymus cells apply to humans remains to be determined.
机译:胸腺中的胰岛素表达与调节自身反应性T细胞的阴性选择以及介导对胰腺β细胞的中枢免疫耐受有关。胸腺胰岛素表达调节可能是预防1型糖尿病的重要药物靶标。我们进行了高通量筛选,以鉴定具有这种活性的化合物。用人胰岛素启动子序列构建报告质粒,所述人胰岛素启动子序列包括亚克隆入pGL4.17载体的上游可变数目串联重复序列(VNTR)序列(32个重复序列)的短等位基因。将该质粒稳定转染到转录胰岛素的髓样胸腺上皮细胞(mTEC)系中。通过用候选化合物刺激24 h进行主要的高通量筛选测定,并测量荧光素酶的活性。阳性化合物通过实时PCR进一步验证。实时PCR证实,在19,707种化合物中,我们鉴定了一种可以增强mTEC胰岛素表达的化合物。我们还观察到用自身免疫调节剂(AIRE)转染增加了mTECs中的内源性AIRE表达。我们的胰岛素-VNTRI-启动子报告系统与mTECs中的胰岛素表达调节一致,一种已鉴定的化合物可以增加mTECs中的胰岛素表达。观察到AIRE在mTECS中具有正反馈作用。这些在小鼠胸腺细胞中的作用是否适用于人类仍有待确定。

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