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利用红色荧光探针快速检测二肽基肽酶 4 和对氨苯甲酰基-L-精氨酸-β-萘酰胺酶活性以实现肺癌的快速成像。

Rapid imaging of lung cancer using a red fluorescent probe to detect dipeptidyl peptidase 4 and puromycin-sensitive aminopeptidase activities.

机构信息

Laboratory of Chemical Biology and Molecular Imaging, Graduate School of Medicine, The University of Tokyo, Tokyo, Japan.

Department of Thoracic Surgery, Graduate School of Medicine, The University of Tokyo, Tokyo, Japan.

出版信息

Sci Rep. 2022 Jun 1;12(1):9100. doi: 10.1038/s41598-022-12665-9.

Abstract

Rapid identification of lung-cancer micro-lesions is becoming increasingly important to improve the outcome of surgery by accurately defining the tumor/normal tissue margins and detecting tiny tumors, especially for patients with low lung function and early-stage cancer. The purpose of this study is to select and validate the best red fluorescent probe for rapid diagnosis of lung cancer by screening a library of 400 red fluorescent probes based on 2-methyl silicon rhodamine (2MeSiR) as the fluorescent scaffold, as well as to identify the target enzymes that activate the selected probe, and to confirm their expression in cancer cells. The selected probe, glutamine-alanine-2-methyl silicon rhodamine (QA-2MeSiR), showed 96.3% sensitivity and 85.2% specificity for visualization of lung cancer in surgically resected specimens within 10 min. In order to further reduce the background fluorescence while retaining the same side-chain structure, we modified QA-2MeSiR to obtain glutamine-alanine-2-methoxy silicon rhodamine (QA-2OMeSiR). This probe rapidly visualized even borderline lesions. Dipeptidyl peptidase 4 and puromycin-sensitive aminopeptidase were identified as enzymes mediating the cleavage and consequent fluorescence activation of QA-2OMeSiR, and it was confirmed that both enzymes are expressed in lung cancer. QA-2OMeSiR is a promising candidate for clinical application.

摘要

快速识别肺癌微病变对于提高手术效果变得越来越重要,其可以通过准确界定肿瘤/正常组织边界和检测微小肿瘤来实现,这对于肺功能低下和早期癌症患者尤为重要。本研究旨在通过筛选基于 2-甲基硅罗丹明(2MeSiR)的 400 种红色荧光探针库,选择和验证用于快速诊断肺癌的最佳红色荧光探针,确定激活所选探针的靶酶,并确认它们在癌细胞中的表达。选择的探针谷氨酰胺-丙氨酸-2-甲基硅罗丹明(QA-2MeSiR)在 10 分钟内对手术切除标本中的肺癌进行可视化,其灵敏度为 96.3%,特异性为 85.2%。为了在保留相同侧链结构的同时进一步降低背景荧光,我们对 QA-2MeSiR 进行了修饰,得到谷氨酰胺-丙氨酸-2-甲氧基硅罗丹明(QA-2OMeSiR)。该探针能快速可视化边界病变。二肽基肽酶 4 和嘌呤霉素敏感氨肽酶被鉴定为介导 QA-2OMeSiR 切割和随后荧光激活的酶,并且证实这两种酶均在肺癌中表达。QA-2OMeSiR 是一种很有前途的临床应用候选物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c4be/9160295/5cbea9903830/41598_2022_12665_Fig1_HTML.jpg

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