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Emission spectra of bioluminescent reporters and interaction with mammalian tissue determine the sensitivity of detection in vivo

机译:生物发光报告分子的发射光谱以及与哺乳动物组织的相互作用决定了体内检测的敏感性

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In vivo bioluminescence imaging depends on light emitted by luciferases in the body overcoming the effect of tissue attenuation. Understanding this relationship is essential for detection and quantification of signal. We have studied four codon optimized luciferases with different emission spectra, including enzymes from firefly (FLuc), click beetle (CBGr68, CBRed) and Renilla reniformins (hRLuc). At 25℃, the in vitro λ_(max) of these reporters are 578, 543, 615, and 480 nm, respectively; at body temperature, 37℃, the brightness increases and the firefly enzyme demonstrates a 34-nm spectral red shift. Spectral shifts and attenuation due to tissue effects were evaluated using a series of 20-nm bandpass filters and a cooled charge-coupled device (CCD) camera. Attenuation increased and the spectra of emitted light was red shifted for signals originating from deeper within the body relative to superficial origins. The tissue attenuation of signals from CBGr68 and hRLuc was greater than from those of Fluc and CBRed. To further probe tissue effects, broad spectral emitters were created through gene fusions between CBGr68 and CBRed. These resulted in enzymes with broader emission spectra, featuring two peaks whose intensities are differentially affected by temperature and tissue depth. These spectral measurement data allow for improved understanding of how these reporters can be used in vivo and what they can reveal about biological processes in living subjects.
机译:体内生物发光成像取决于体内萤光素酶所发出的光,从而克服了组织衰减的影响。了解这种关系对于检测和量化信号至关重要。我们研究了四种具有不同发射光谱的经密码子优化的荧光素酶,包括萤火虫(FLuc),点击甲虫(CBGr68,CBRed)和海肾Renniformins(hRLuc)的酶。在25℃下,这些报告基因的体外λ_(max)分别为578、543、615和480 nm。在37℃的体温下,亮度增加,萤火虫酶显示出34 nm的光谱红移。使用一系列20 nm带通滤光片和冷却的电荷耦合器件(CCD)摄像机评估了由于组织效应引起的光谱偏移和衰减。相对于表面起源,从体内更深处发出的信号衰减增加,并且发射光的光谱发生红移。来自CBGr68和hRLuc的信号的组织衰减大于来自Fluc和CBRed的信号。为了进一步探测组织效应,通过CBGr68和CBRed之间的基因融合产生了广谱发射体。这些产生的酶具有更宽的发射光谱,具有两个峰,其强度受温度和组织深度的影响不同。这些光谱测量数据有助于更好地了解这些报道分子如何在体内使用,以及它们可以揭示活体受试者的生物学过程。

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