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Integrin Facilitates the Internalization of TAT Peptide Conjugated to RGD Motif in Model Lipid Membranes.整合素促进 RGD 基序肽与 TAT 肽的内化在模型脂质膜中。
Chembiochem. 2024 Jan 15;25(2):e202300642. doi: 10.1002/cbic.202300642. Epub 2023 Nov 23.
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Biomacromolecules. 2023 Nov 13;24(11):4890-4900. doi: 10.1021/acs.biomac.3c00603. Epub 2023 Oct 20.
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Engineered Histidine-Rich Peptides Enhance Endosomal Escape for Antibody-Targeted Intracellular Delivery of Functional Proteins.工程化组氨酸丰富肽增强抗体靶向细胞内递呈功能性蛋白的内体逃逸。
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Evaluation of the effect of a cell penetrating peptide (TAT) towards tailoring the targeting efficacy and tumor uptake of porphyrin.评估细胞穿透肽(TAT)对定制卟啉靶向功效和肿瘤摄取的影响。
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细胞穿透肽功能的体内研究:在肿瘤中的积累及作为特异性正电子发射断层显像(PET)探针的潜力

In Vivo Interrogation of Cell-Penetrating Peptide Function: Accumulation in Tumors and the Potential as a Specific PET Probe.

作者信息

Si Zhan, Tian Lulu, Zhou Hongxin, Lin Jiasheng, Zhou Jun

机构信息

Department of Nuclear Medicine, Zhongshan Hospital, Fudan University, Shanghai 200032, China.

Institute of Nuclear Medicine, Fudan University, Shanghai 200032, China.

出版信息

Bioconjug Chem. 2025 May 21;36(5):1088-1097. doi: 10.1021/acs.bioconjchem.5c00128. Epub 2025 Apr 9.

DOI:10.1021/acs.bioconjchem.5c00128
PMID:40202497
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12101444/
Abstract

We aimed to evaluate the biodistribution and specificity of Ga-DOTA-TAT and RHO-TAT using MGC-803 and HT-29 tumor cells as well as tumor-xenografted nude mice and to demonstrate its application in positron emission tomography (PET) imaging. The in vitro evaluation of Ga-DOTA-TAT was assessed in MGC-803 and HT-29 cell lines, and the in vivo evaluation of Ga-DOTA-TAT was also performed in mice bearing MGC-803 or HT-29 tumors, respectively. Fluorescence microscopy was also employed to evaluate the specificity of RHO-TAT in vitro in MGC-803 and HT-29 cells as well as ex vivo in tumor slices of the corresponding tumor models. The in vivo imaging differences between Ga-DOTA-TAT and F-FDG in MGC-803 and HT-29 tumors were also studied. The biodistribution and micro-PET results demonstrated significant uptake of Ga-DOTA-TAT in non-FDG-avid MGC-803 tumors, whereas there was negligible uptake in FDG-avid HT-29 tumors. RHO-TAT showed superior fluorescence microscopy imaging effects in MGC-803 cells and tumor slices but not in HT-29 cells and tumor slices, which were consistent with the in vivo results. Ga-DOTA-TAT combined with F-FDG can be applied noninvasively in cancers with PET imaging for potential patient selection and stratification. We demonstrated a higher binding of Ga-DOTA-TAT and RHO-TAT to MGC-803 cells as well as to non-FDG-avid MGC-803 xenografted tumors and a lower binding to HT-29 cells and FDG-avid xenografted tumors. These results suggest that TAT has the potential to be a ligand for targeting certain tumors.

摘要

我们旨在以MGC - 803和HT - 29肿瘤细胞以及肿瘤异种移植裸鼠为研究对象,评估Ga - DOTA - TAT和RHO - TAT的生物分布及特异性,并展示其在正电子发射断层扫描(PET)成像中的应用。在MGC - 803和HT - 29细胞系中对Ga - DOTA - TAT进行体外评估,同时也分别在携带MGC - 803或HT - 29肿瘤的小鼠体内对Ga - DOTA - TAT进行评估。还采用荧光显微镜在体外评估MGC - 803和HT - 29细胞中RHO - TAT的特异性,以及在相应肿瘤模型的肿瘤切片中进行离体评估。此外,还研究了Ga - DOTA - TAT和F - FDG在MGC - 803和HT - 29肿瘤中的体内成像差异。生物分布和微型PET结果表明,Ga - DOTA - TAT在非FDG摄取型MGC - 803肿瘤中有显著摄取,而在FDG摄取型HT - 29肿瘤中的摄取可忽略不计。RHO - TAT在MGC - 803细胞和肿瘤切片中显示出优异的荧光显微镜成像效果,但在HT - 29细胞和肿瘤切片中则不然,这与体内结果一致。Ga - DOTA - TAT联合F - FDG可通过PET成像在癌症中进行无创应用,用于潜在的患者选择和分层。我们证明了Ga - DOTA - TAT和RHO - TAT与MGC - 803细胞以及非FDG摄取型MGC - 803异种移植肿瘤的结合力较高,而与HT - 29细胞和FDG摄取型异种移植肿瘤的结合力较低。这些结果表明,TAT有潜力成为靶向某些肿瘤的配体。