Nanoparticles targeting extra domain B of fibronectin-specific to the atherosclerotic lesion types III, IV, and V-enhance plaque detection and cargo delivery

Extra domain B of fibronectin (FN-EDB) is upregulated in the extracellular matrix during tissue remodeling and has been postulated as a potential biomarker for atherosclerosis, yet no systematic test for FN-EDB in plaques has been reported. We hypothesized that FN-EDB expression would intensify in a...

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Detalles Bibliográficos
Autores principales: Yu, Mikyung, Ortega, Carleena A., Si, Kevin, Molinaro, Roberto, Schoen, Frederick J., Leitao, Renata F. C., Xu, Xiaoding, Mahmoudi, Morteza, Ahn, Suyeon, Liu, Jerry, Saw, Phei Er, Lee, In-Hyun, Brayner, Mirna M. B., Lotfi, Azita, Shi, Jinjun, Libby, Peter, Jon, Sangyong, Farokhzad, Omid C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2018
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6299428/
https://www.ncbi.nlm.nih.gov/pubmed/30613278
http://dx.doi.org/10.7150/thno.24365
Descripción
Sumario:Extra domain B of fibronectin (FN-EDB) is upregulated in the extracellular matrix during tissue remodeling and has been postulated as a potential biomarker for atherosclerosis, yet no systematic test for FN-EDB in plaques has been reported. We hypothesized that FN-EDB expression would intensify in advanced plaques. Furthermore, engineering of FN-EDB-targeted nanoparticles (NPs) could enable imaging/diagnosis and local delivery of payloads to plaques. Methods: The amount of FN-EDB in human atherosclerotic and normal arteries (ages: 40 to 85 years) was assessed by histological staining and quantification using an FN-EDB-specific aptide (APT(FN-EDB)). FN-EDB-specific NPs that could serve as MRI beacons were constructed by immobilizing APT(FN-EDB) on the NP surface containing DTPA[Gd]. MRI visualized APT(FN-EDB)-[Gd]NPs administered to atherosclerotic apolipoprotein E-deficient mice in the brachiocephalic arteries. Analysis of the ascending-to-descending thoracic aortas and the aortic roots of the mice permitted quantitation of Gd, FN-EDB, and APT(FN-EDB)-[Gd]NPs. Cyanine, a model small molecule drug, was used to study the biodistribution and pharmacokinetics of APT(FN-EDB)-NPs to evaluate their utility for drug delivery. Results: Atherosclerotic tissues had significantly greater FN-EDB-positive areas than normal arteries (P < 0.001). This signal pertained particularly to Type III (P < 0.01), IV (P < 0.01), and V lesions (P < 0.001) rather than Type I and II lesions (AHA classification). FN-EDB expression was positively correlated with macrophage accumulation and neoangiogenesis. Quantitative analysis of T1-weighted images of atherosclerotic mice revealed substantial APT(FN-EDB)-[Gd]NPs accumulation in plaques compared to control NPs, conventional MRI contrast agent (Gd-DTPA) or accumulation in wild-type C57BL/6J mice. Additionally, the APT(FN-EDB)-NPs significantly prolonged the blood-circulation time (t(1/2): ~ 6 h) of a model drug and increased its accumulation in plaques (6.9-fold higher accumulation vs. free drug). Conclusions: Our findings demonstrate augmented FN-EDB expression in Type III, IV, and V atheromata and that APT(FN-EDB)-NPs could serve as a platform for identifying and/or delivering agents locally to a subset of atherosclerotic plaques.

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