Elucidation and Structural Modeling of CD71 as a Molecular Target for Cell-Specific Aptamer Binding

化学 转铁蛋白受体 胰腺癌 转铁蛋白 适体 癌症 癌细胞 抗体 癌症研究 恶性肿瘤 生物化学 分子生物学 生物 遗传学
作者
Xiaoqiu Wu,Honglin Liu,Dongmei Han,Bo Peng,Hui Zhang,Lin Zhang,Jianglin Li,Jing Liu,Cheng Cui,Senbiao Fang,Min Li,Mao Ye,Weihong Tan
出处
期刊:Journal of the American Chemical Society [American Chemical Society]
卷期号:141 (27): 10760-10769 被引量:131
标识
DOI:10.1021/jacs.9b03720
摘要

Pancreatic cancer is a highly lethal malignancy associated with tissues of the pancreas. Early diagnosis and effective treatment are crucial to improving the survival rate of patients with pancreatic cancer. In a previous study, we employed the cell-SELEX strategy to obtain an ssDNA aptamer termed XQ-2d with high binding affinity for pancreatic cancer. Here, we first identify CD71 as the XQ-2d-binding target. We found that knockdown of CD71 abolished the binding of XQ-2d and that the binding affinity of XQ-2d is associated with membrane-bound CD71, rather than total CD71 levels. Competitive analysis revealed that XQ-2d shares the same binding site on CD71 with transferrin (Tf), but not anti-CD71 antibody. We then used a surface energy transfer (SET) nanoruler to measure the distance between the binding sites of XQ-2d and anti-CD71 antibody, and it was about 15 nm. Furthermore, we did molecular dynamics simulation to clarify that the spatial structure of XQ-2d and Tf competitively binding to CD71. We also engineered XQ-2d-mediated targeted therapy for pancreatic cancer, using an XQ-2d-based complex for loading doxorubicin (Dox). Because CD71 is overexpressed not only in pancreatic cancer but also in a variety of tumors, our work provides a systematic novel way of studying a potential biomarker and also promising tools for cancer diagnosis and therapy, opening new doors for effective cancer theranostics.
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