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近红外比率探针带有自毁间隔基,可快速灵敏地检测碱性磷酸酶活性,并实现体内成像。

Near-infrared ratiometric probe with a self-immolative spacer for rapid and sensitive detection of alkaline phosphatase activity and imaging in vivo.

机构信息

College of Science, China Agricultural University, Beijing, 100193, PR China.

College of Science, China Agricultural University, Beijing, 100193, PR China.

出版信息

Anal Chim Acta. 2020 Jan 15;1094:113-121. doi: 10.1016/j.aca.2019.10.001. Epub 2019 Oct 7.

DOI:10.1016/j.aca.2019.10.001
PMID:31761037
Abstract

Alkaline phosphatase (ALP), an enzyme that catalyzes the hydrolysis of phosphate groups, is closely associated with many diseases, including bone disease, prostate cancer, and diabetes. Thus, new assays for ALP detection in live cells are needed to better understand its role in related biological processes. In this study, we constructed a novel near-infrared ratiometric fluorescent probe for detecting ALP activity with high sensitivity. The probe uses a new self-immolative mechanism that can achieve a rapid response (within 10 min) to ALP, detected as a spectral shift (from 580 to 650 nm). This method effectively avoids issues related to instrument variability, and the near-infrared fluorescence emission (650 nm) makes it more suitable for biological detection. Moreover, the high sensitivity (14-fold enhancement of the fluorescence ratio F/F) and low detection limit (0.89 U L) for ALP allows the probe to be adapted to complex biological environments. The assay was successfully performed using serum samples with a linear range of ALP of up to 150 U L. We used the developed probe to detect and image endogenous ALP in cells with satisfactory results, and we successfully used the probes to detect changes in endogenous ALP levels in zebrafish caused by drug-induced organ damage.

摘要

碱性磷酸酶(ALP)是一种能够催化磷酸基团水解的酶,与许多疾病密切相关,包括骨骼疾病、前列腺癌和糖尿病。因此,需要新的方法来检测活细胞中的 ALP 以更好地理解其在相关生物过程中的作用。在本研究中,我们构建了一种新型的近红外比率荧光探针,用于高灵敏度检测 ALP 活性。该探针使用了一种新的自消毁机制,可以快速响应 ALP(在 10 分钟内),表现为光谱位移(从 580nm 到 650nm)。这种方法有效地避免了与仪器变化相关的问题,并且近红外荧光发射(650nm)使其更适合生物检测。此外,ALP 的高灵敏度(荧光比 F/F 增强 14 倍)和低检测限(0.89 U/L)允许探针适应复杂的生物环境。该检测方法在血清样本中成功进行,ALP 的线性范围高达 150 U/L。我们使用开发的探针成功地检测和成像了细胞内的内源性 ALP,并且成功地使用探针检测了药物引起的器官损伤导致的斑马鱼内源性 ALP 水平的变化。

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