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Small near-infrared photochromic protein for photoacoustic multi-contrast imaging and detection of protein interactions in vivo

机译:小型近红外光致变色蛋白用于光声多对比度成像和体内蛋白相互作用的检测

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摘要

Photoacoustic (PA) computed tomography (PACT) benefits from genetically encoded probes with photochromic behavior, which dramatically increase detection sensitivity and specificity through photoswitching and differential imaging. Starting with a DrBphP bacterial phytochrome, we have engineered a near-infrared photochromic probe, DrBphP-PCM, which is superior to the full-length RpBphP1 phytochrome previously used in differential PACT. DrBphP-PCM has a smaller size, better folding, and higher photoswitching contrast. We have imaged both DrBphP-PCM and RpBphP1 simultaneously on the basis of their unique signal decay characteristics, using a reversibly switchable single-impulse panoramic PACT (RS-SIP-PACT) with a single wavelength excitation. The simple structural organization of DrBphP-PCM allows engineering a bimolecular PA complementation reporter, a split version of DrBphP-PCM, termed DrSplit. DrSplit enables PA detection of protein–protein interactions in deep-seated mouse tumors and livers, achieving 125-µm spatial resolution and 530-cell sensitivity in vivo. The combination of RS-SIP-PACT with DrBphP-PCM and DrSplit holds great potential for noninvasive multi-contrast deep-tissue functional imaging.
机译:光声(PA)计算机断层扫描(PACT)受益于具有光致变色行为的基因编码探针,该探针通过光开关和差分成像显着提高了检测灵敏度和特异性。从DrBphP细菌植物色素开始,我们设计了一种近红外光致变色探针DrBphP-PCM,它优于以前在差异PACT中使用的全长RpBphP1植物色素。 DrBphP-PCM具有更小的尺寸,更好的折叠和更高的光开关对比度。我们已经使用可逆切换的单脉冲全景PACT(RS-SIP-PACT)和单波长激励,根据它们独特的信号衰减特性同时对DrBphP-PCM和RpBphP1进行了成像。 DrBphP-PCM的简单结构组织允许工程化双分子PA互补报告基因,即DrBphP-PCM的分离版本,称为DrSplit。 DrSplit支持PA检测深部小鼠肿瘤和肝脏中蛋白质之间的相互作用,从而在体内实现125 µm的空间分辨率和530细胞敏感性。 RS-SIP-PACT与DrBphP-PCM和DrSplit的结合在无创多对比度深层组织功能成像方面具有巨大潜力。

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