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ATP 非依赖型生物发光报告基因变体以改善活体成像。

ATP-Independent Bioluminescent Reporter Variants To Improve in Vivo Imaging.

机构信息

Center for Membrane and Cell Physiology, Department of Molecular Physiology and Biological Physics, Department of Chemistry, and the UVA Cancer Center , University of Virginia , 1340 Jefferson Park Avenue , Charlottesville , Virginia 22908 , United States.

出版信息

ACS Chem Biol. 2019 May 17;14(5):959-965. doi: 10.1021/acschembio.9b00150. Epub 2019 Apr 17.

Abstract

Coelenterazine (CTZ)-utilizing marine luciferases and their derivatives have attracted significant attention because of their ATP-independency, fast enzymatic turnover, and high bioluminescence brightness. However, marine luciferases typically emit blue photons and their substrates, including CTZ and the recently developed diphenylterazine (DTZ), have poor water solubility, hindering their in vivo applications. Herein, we report a family of pyridyl CTZ and DTZ analogs that exhibit spectrally shifted emission and improved water solubility. Through directed evolution, we engineered a LumiLuc luciferase with broad substrate specificity. In the presence of corresponding pyridyl substrates (i.e., pyCTZ, 6pyDTZ, or 8pyDTZ), LumiLuc generates highly bright blue, teal, or yellow bioluminescence. We compared our LumiLuc-8pyDTZ pair with several benchmark reporters in a tumor xenograft mouse model. Our new pair, which does not need organic cosolvents for in vivo administration, surpasses other reporters by detecting early tumors. We further fused LumiLuc to a red fluorescent protein, resulting in a LumiScarlet reporter with further red-shifted emission and enhanced tissue penetration. LumiScarlet-8pyDTZ was comparable to Akaluc-AkaLumine, the brightest ATP-dependent luciferase-luciferin pair, for detecting cells in deep tissues of mice. In summary, we have engineered a new family of ATP-independent bioluminescent reporters, which will have broad applications because of their ATP-independency, excellent biocompatibility, and superior in vivo sensitivity.

摘要

腔肠素(CTZ)-利用海洋荧光素酶及其衍生物因其不依赖于 ATP、快速酶转化和高生物发光亮度而引起了广泛关注。然而,海洋荧光素酶通常发射蓝光,其底物,包括 CTZ 和最近开发的二苯基四嗪(DTZ),水溶性差,限制了它们的体内应用。在此,我们报告了一系列吡啶 CTZ 和 DTZ 类似物,它们具有光谱位移发射和改善的水溶性。通过定向进化,我们设计了一种具有广泛底物特异性的 LumiLuc 荧光素酶。在相应的吡啶底物(即 pyCTZ、6pyDTZ 或 8pyDTZ)存在下,LumiLuc 产生高亮度的蓝色、蓝绿色或黄色生物发光。我们在肿瘤异种移植小鼠模型中比较了我们的 LumiLuc-8pyDTZ 对与几种基准报告基因。我们的新对,不需要有机共溶剂用于体内给药,通过检测早期肿瘤超过其他报告基因。我们进一步将 LumiLuc 融合到红色荧光蛋白中,得到具有进一步红移发射和增强组织穿透性的 LumiScarlet 报告基因。LumiScarlet-8pyDTZ 在检测小鼠深层组织中的细胞时与最亮的 ATP 依赖性荧光素酶-荧光素对 Akaluc-AkaLumine 相当。总之,我们已经设计了一种新的 ATP 非依赖性生物发光报告基因家族,由于其不依赖于 ATP、优异的生物相容性和优越的体内灵敏度,它们将具有广泛的应用。

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