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LDL-mimetic lipid nanoparticles prepared by surface KAT ligation for in vivo MRI of atherosclerosis

Low-density lipoprotein (LDL)-mimetic lipid nanoparticles (LNPs), decorated with MRI contrast agents and fluorescent dyes, were prepared by the covalent attachment of apolipoprotein-mimetic peptide (P), Gd(iii)-chelate (Gd), and sulforhodamine B (R) moieties on the LNP surface. The functionalized LN...

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Autores principales: Fracassi, Alessandro, Cao, Jianbo, Yoshizawa-Sugata, Naoko, Tóth, Éva, Archer, Corey, Gröninger, Olivier, Ricciotti, Emanuela, Tang, Soon Yew, Handschin, Stephan, Bourgeois, Jean-Pascal, Ray, Ankita, Liosi, Korinne, Oriana, Sean, Stark, Wendelin, Masai, Hisao, Zhou, Rong, Yamakoshi, Yoko
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society of Chemistry 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8162946/
https://www.ncbi.nlm.nih.gov/pubmed/34094421
http://dx.doi.org/10.1039/d0sc04106h
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author Fracassi, Alessandro
Cao, Jianbo
Yoshizawa-Sugata, Naoko
Tóth, Éva
Archer, Corey
Gröninger, Olivier
Ricciotti, Emanuela
Tang, Soon Yew
Handschin, Stephan
Bourgeois, Jean-Pascal
Ray, Ankita
Liosi, Korinne
Oriana, Sean
Stark, Wendelin
Masai, Hisao
Zhou, Rong
Yamakoshi, Yoko
author_facet Fracassi, Alessandro
Cao, Jianbo
Yoshizawa-Sugata, Naoko
Tóth, Éva
Archer, Corey
Gröninger, Olivier
Ricciotti, Emanuela
Tang, Soon Yew
Handschin, Stephan
Bourgeois, Jean-Pascal
Ray, Ankita
Liosi, Korinne
Oriana, Sean
Stark, Wendelin
Masai, Hisao
Zhou, Rong
Yamakoshi, Yoko
author_sort Fracassi, Alessandro
collection PubMed
description Low-density lipoprotein (LDL)-mimetic lipid nanoparticles (LNPs), decorated with MRI contrast agents and fluorescent dyes, were prepared by the covalent attachment of apolipoprotein-mimetic peptide (P), Gd(iii)-chelate (Gd), and sulforhodamine B (R) moieties on the LNP surface. The functionalized LNPs were prepared using the amide-forming potassium acyltrifluoroborate (KAT) ligation reaction. The KAT groups on the surface of LNPs were allowed to react with the corresponding hydroxylamine (HA) derivatives of P and Gd to provide bi-functionalized LNPs (PGd-LNP). The reaction proceeded with excellent yields, as observed by ICP-MS (for B and Gd amounts) and MALDI-TOF-MS data, and did not alter the morphology of the LNPs (mean diameter: ca. 50 nm), as shown by DLS and cryoTEM analyses. With the help of the efficient KAT ligation, a high payload of Gd(iii)-chelate on the PGd-LNP surface (ca. 2800 Gd atoms per LNP) was successfully achieved and provided a high r(1) relaxivity (r(1) = 22.0 s(−1) mM(−1) at 1.4 T/60 MHz and 25 °C; r(1) = 8.2 s(−1) mM(−1) at 9.4 T/400 MHz and 37 °C). This bi-functionalized PGd-LNP was administered to three atherosclerotic apoE(−/−) mice to reveal the clear enhancement of atherosclerotic plaques in the brachiocephalic artery (BA) by MRI, in good agreement with the high accumulation of Gd in the aortic arch as shown by ICP-MS. The parallel in vivo MRI and ex vivo studies of whole mouse cryo-imaging were performed using triply functionalized LNPs with P, Gd, and R (PGdR-LNP). The clear presence of atherosclerotic plaques in BA was observed by ex vivo bright field cryo-imaging, and they were also observed by high emission fluorescent imaging. These directly corresponded to the enhanced tissue in the in vivo MRI of the identical mouse.
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spelling pubmed-81629462021-06-04 LDL-mimetic lipid nanoparticles prepared by surface KAT ligation for in vivo MRI of atherosclerosis Fracassi, Alessandro Cao, Jianbo Yoshizawa-Sugata, Naoko Tóth, Éva Archer, Corey Gröninger, Olivier Ricciotti, Emanuela Tang, Soon Yew Handschin, Stephan Bourgeois, Jean-Pascal Ray, Ankita Liosi, Korinne Oriana, Sean Stark, Wendelin Masai, Hisao Zhou, Rong Yamakoshi, Yoko Chem Sci Chemistry Low-density lipoprotein (LDL)-mimetic lipid nanoparticles (LNPs), decorated with MRI contrast agents and fluorescent dyes, were prepared by the covalent attachment of apolipoprotein-mimetic peptide (P), Gd(iii)-chelate (Gd), and sulforhodamine B (R) moieties on the LNP surface. The functionalized LNPs were prepared using the amide-forming potassium acyltrifluoroborate (KAT) ligation reaction. The KAT groups on the surface of LNPs were allowed to react with the corresponding hydroxylamine (HA) derivatives of P and Gd to provide bi-functionalized LNPs (PGd-LNP). The reaction proceeded with excellent yields, as observed by ICP-MS (for B and Gd amounts) and MALDI-TOF-MS data, and did not alter the morphology of the LNPs (mean diameter: ca. 50 nm), as shown by DLS and cryoTEM analyses. With the help of the efficient KAT ligation, a high payload of Gd(iii)-chelate on the PGd-LNP surface (ca. 2800 Gd atoms per LNP) was successfully achieved and provided a high r(1) relaxivity (r(1) = 22.0 s(−1) mM(−1) at 1.4 T/60 MHz and 25 °C; r(1) = 8.2 s(−1) mM(−1) at 9.4 T/400 MHz and 37 °C). This bi-functionalized PGd-LNP was administered to three atherosclerotic apoE(−/−) mice to reveal the clear enhancement of atherosclerotic plaques in the brachiocephalic artery (BA) by MRI, in good agreement with the high accumulation of Gd in the aortic arch as shown by ICP-MS. The parallel in vivo MRI and ex vivo studies of whole mouse cryo-imaging were performed using triply functionalized LNPs with P, Gd, and R (PGdR-LNP). The clear presence of atherosclerotic plaques in BA was observed by ex vivo bright field cryo-imaging, and they were also observed by high emission fluorescent imaging. These directly corresponded to the enhanced tissue in the in vivo MRI of the identical mouse. The Royal Society of Chemistry 2020-10-07 /pmc/articles/PMC8162946/ /pubmed/34094421 http://dx.doi.org/10.1039/d0sc04106h Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by-nc/3.0/
spellingShingle Chemistry
Fracassi, Alessandro
Cao, Jianbo
Yoshizawa-Sugata, Naoko
Tóth, Éva
Archer, Corey
Gröninger, Olivier
Ricciotti, Emanuela
Tang, Soon Yew
Handschin, Stephan
Bourgeois, Jean-Pascal
Ray, Ankita
Liosi, Korinne
Oriana, Sean
Stark, Wendelin
Masai, Hisao
Zhou, Rong
Yamakoshi, Yoko
LDL-mimetic lipid nanoparticles prepared by surface KAT ligation for in vivo MRI of atherosclerosis
title LDL-mimetic lipid nanoparticles prepared by surface KAT ligation for in vivo MRI of atherosclerosis
title_full LDL-mimetic lipid nanoparticles prepared by surface KAT ligation for in vivo MRI of atherosclerosis
title_fullStr LDL-mimetic lipid nanoparticles prepared by surface KAT ligation for in vivo MRI of atherosclerosis
title_full_unstemmed LDL-mimetic lipid nanoparticles prepared by surface KAT ligation for in vivo MRI of atherosclerosis
title_short LDL-mimetic lipid nanoparticles prepared by surface KAT ligation for in vivo MRI of atherosclerosis
title_sort ldl-mimetic lipid nanoparticles prepared by surface kat ligation for in vivo mri of atherosclerosis
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8162946/
https://www.ncbi.nlm.nih.gov/pubmed/34094421
http://dx.doi.org/10.1039/d0sc04106h
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