Exploring the utility of organo-polyoxometalate hybrids to inhibit SOX transcription factors

IF 4 Q2 CELL & TISSUE ENGINEERING

Cell Regeneration Pub Date : 2014-01-01 DOI:10.1186/2045-9769-3-10

Kamesh Narasimhan , Kevin Micoine , Emmanuel Lacôte , Serge Thorimbert , Edwin Cheung , Bernold Hasenknopf , Ralf Jauch

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引用次数: 10

Abstract

Background

SOX transcription factors constitute an attractive target class for intervention with small molecules as they play a prominent role in the field of regenerative biomedicine and cancer biology. However, rationally engineering specific inhibitors that interfere with transcription factor DNA interfaces continues to be a monumental challenge in the field of transcription factor chemical biology. Polyoxometalates (POMs) are inorganic compounds that were previously shown to target the high-mobility group (HMG) of SOX proteins at nanomolar concentrations. In continuation of this work, we carried out an assessment of the selectivity of a panel of newly synthesized organo-polyoxometalate hybrids in targeting different transcription factor families to enable the usage of polyoxometalates as specific SOX transcription factor drugs.

Results

The residual DNA-binding activities of 15 different transcription factors were measured after treatment with a panel of diverse polyoxometalates. Polyoxometalates belonging to the Dawson structural class were found to be more potent inhibitors than the Keggin class. Further, organically modified Dawson polyoxometalates were found to be the most potent in inhibiting transcription factor DNA binding activity. The size of the polyoxometalates and its derivitization were found to be the key determinants of their potency.

Conclusion

Polyoxometalates are highly potent, nanomolar range inhibitors of the DNA binding activity of the Sox-HMG family. However, binding assays involving a limited subset of structurally diverse polyoxometalates revealed a low selectivity profile against different transcription factor families. Further progress in achieving selectivity and deciphering structure-activity relationship of POMs require the identification of POM binding sites on transcription factors using elaborate approaches like X-ray crystallography and multidimensional NMR. In summary, our report reaffirms that transcription factors are challenging molecular architectures and that future polyoxometalate chemistry must consider further modification strategies, to address the substantial challenges involved in achieving target selectivity.

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探索有机多金属氧酸盐杂合体抑制SOX转录因子的效用

sox转录因子在再生生物医学和癌症生物学领域发挥着重要作用，是小分子干预的一个有吸引力的靶标类。然而，合理设计干扰转录因子DNA界面的特异性抑制剂仍然是转录因子化学生物学领域的巨大挑战。多金属氧酸盐(pom)是一种无机化合物，以前被证明可以在纳摩尔浓度下靶向SOX蛋白的高迁移基团(HMG)。在这项工作的继续，我们进行了一组新合成的有机多金属氧酸盐杂合体的选择性评估，以针对不同的转录因子家族，使多金属氧酸盐作为特异性SOX转录因子药物的使用。结果用不同的多金属氧酸盐处理后，测定了15种不同转录因子的剩余dna结合活性。道森结构类的多金属氧酸盐被发现是比凯金结构类更有效的抑制剂。此外，有机修饰的道森多金属氧酸酯在抑制转录因子DNA结合活性方面效果最好。发现多金属氧酸盐的大小及其衍生化是其效力的关键决定因素。结论多金属氧酸盐对Sox-HMG家族的DNA结合活性具有纳米摩尔范围的抑制作用。然而，涉及结构多样化多金属氧酸盐的有限子集的结合分析显示，对不同转录因子家族的选择性较低。在实现POM的选择性和破译结构-活性关系方面的进一步进展需要使用x射线晶体学和多维核磁共振等复杂方法识别转录因子上的POM结合位点。总之，我们的报告重申了转录因子是具有挑战性的分子结构，未来的多金属氧酸盐化学必须考虑进一步的修饰策略，以解决实现目标选择性所涉及的实质性挑战。

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来源期刊

Cell Regeneration Biochemistry, Genetics and Molecular Biology-Cell Biology

CiteScore

5.80

自引率

0.00%

发文量

审稿时长

35 days

期刊介绍： Cell Regeneration aims to provide a worldwide platform for researches on stem cells and regenerative biology to develop basic science and to foster its clinical translation in medicine. Cell Regeneration welcomes reports on novel discoveries, theories, methods, technologies, and products in the field of stem cells and regenerative research, the journal is interested, but not limited to the following topics: ◎ Embryonic stem cells ◎ Induced pluripotent stem cells ◎ Tissue-specific stem cells ◎ Tissue or organ regeneration ◎ Methodology ◎ Biomaterials and regeneration ◎ Clinical translation or application in medicine