Tumor Targeting by αvβ3-Integrin-Specific Lipid Nanoparticles Occurs via Phagocyte Hitchhiking

Alexandros Marios Sofias; Yohana C. Toner; Anu E. Meerwaldt; Mandy M.T. van Leent; Georgios Soultanidis; Mattijs Elschot; Haruki Gonai; Kristin Grendstad; Åsmund Flobak; Ulrike Neckmann; Camilla Wolowczyk; Elizabeth L. Fisher; Thomas Reiner; Catharina de Lange Davies; Geir Bjørkøy; Abraham J.P. Teunissen; Jordi Ochando; Carlos Pérez-Medina; Willem J.M. Mulder; Sjoerd Hak

doi:10.1021/acsnano.9b08693

Tumor Targeting by α_vβ₃-Integrin-Specific Lipid Nanoparticles Occurs via Phagocyte Hitchhiking

Alexandros Marios Sofias (Corresponding author), Yohana C. Toner, Anu E. Meerwaldt, Mandy M.T. van Leent, Georgios Soultanidis, Mattijs Elschot, Haruki Gonai, Kristin Grendstad, Åsmund Flobak, Ulrike Neckmann, Camilla Wolowczyk, Elizabeth L. Fisher, Thomas Reiner, Catharina de Lange Davies, Geir Bjørkøy, Abraham J.P. Teunissen, Jordi Ochando, Carlos Pérez-Medina, Willem J.M. Mulder, Sjoerd Hak (Corresponding author)

Research output: Contribution to journal › Article › Academic › peer-review

85 Citations (Scopus)

Abstract

Although the first nanomedicine was clinically approved more than two decades ago, nanoparticles' (NP) in vivo behavior is complex and the immune system's role in their application remains elusive. At present, only passive-targeting nanoformulations have been clinically approved, while more complicated active-targeting strategies typically fail to advance from the early clinical phase stage. This absence of clinical translation is, among others, due to the very limited understanding for in vivo targeting mechanisms. Dynamic in vivo phenomena such as NPs' real-time targeting kinetics and phagocytes' contribution to active NP targeting remain largely unexplored. To better understand in vivo targeting, monitoring NP accumulation and distribution at complementary levels of spatial and temporal resolution is imperative. Here, we integrate in vivo positron emission tomography/computed tomography imaging with intravital microscopy and flow cytometric analyses to study αvβ3-integrin-targeted cyclic arginine-glycine-aspartate decorated liposomes and oil-in-water nanoemulsions in tumor mouse models. We observed that ligand-mediated accumulation in cancerous lesions is multifaceted and identified "NP hitchhiking" with phagocytes to contribute considerably to this intricate process. We anticipate that this understanding can facilitate rational improvement of nanomedicine applications and that immune cell-NP interactions can be harnessed to develop clinically viable nanomedicine-based immunotherapies.

Original language	English
Pages (from-to)	7832-7846
Number of pages	15
Journal	ACS Nano
Volume	14
Issue number	7
DOIs	https://doi.org/10.1021/acsnano.9b08693
Publication status	Published - 28 Jul 2020

Funding

Central Norway Regional Health Authority “Helse Midt-Norge Funding numbers: 90284100 Funding numbers: 90262100

Funders	Funder number
National Institutes of Health	P30 CA00574
National Cancer Institute	R01CA220234
American Heart Association	16SDG31390007
Norges Forskningsråd	230788/F20

Keywords

cyclic RGD nanoparticles
immune cell hitchhiking
intravital microscopy
nanomedicine
neutrophils
positron emission tomography/computed tomography imaging
Integrin alphaV
Neoplasms/drug therapy
Lipids
Integrin alphaVbeta3
Nanoparticles
Phagocytes
Animals
Mice

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1021/acsnano.9b08693

Cite this

Sofias, A. M., Toner, Y. C., Meerwaldt, A. E., van Leent, M. M. T., Soultanidis, G., Elschot, M., Gonai, H., Grendstad, K., Flobak, Å., Neckmann, U., Wolowczyk, C., Fisher, E. L., Reiner, T., de Lange Davies, C., Bjørkøy, G., Teunissen, A. J. P., Ochando, J., Pérez-Medina, C., Mulder, W. J. M., & Hak, S. (2020). Tumor Targeting by α_vβ₃-Integrin-Specific Lipid Nanoparticles Occurs via Phagocyte Hitchhiking. ACS Nano, 14(7), 7832-7846. https://doi.org/10.1021/acsnano.9b08693

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abstract = "Although the first nanomedicine was clinically approved more than two decades ago, nanoparticles' (NP) in vivo behavior is complex and the immune system's role in their application remains elusive. At present, only passive-targeting nanoformulations have been clinically approved, while more complicated active-targeting strategies typically fail to advance from the early clinical phase stage. This absence of clinical translation is, among others, due to the very limited understanding for in vivo targeting mechanisms. Dynamic in vivo phenomena such as NPs' real-time targeting kinetics and phagocytes' contribution to active NP targeting remain largely unexplored. To better understand in vivo targeting, monitoring NP accumulation and distribution at complementary levels of spatial and temporal resolution is imperative. Here, we integrate in vivo positron emission tomography/computed tomography imaging with intravital microscopy and flow cytometric analyses to study αvβ3-integrin-targeted cyclic arginine-glycine-aspartate decorated liposomes and oil-in-water nanoemulsions in tumor mouse models. We observed that ligand-mediated accumulation in cancerous lesions is multifaceted and identified {"}NP hitchhiking{"} with phagocytes to contribute considerably to this intricate process. We anticipate that this understanding can facilitate rational improvement of nanomedicine applications and that immune cell-NP interactions can be harnessed to develop clinically viable nanomedicine-based immunotherapies.",

keywords = "cyclic RGD nanoparticles, immune cell hitchhiking, intravital microscopy, nanomedicine, neutrophils, positron emission tomography/computed tomography imaging, Integrin alphaV, Neoplasms/drug therapy, Lipids, Integrin alphaVbeta3, Nanoparticles, Phagocytes, Animals, Mice",

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year = "2020",

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Sofias, AM, Toner, YC, Meerwaldt, AE, van Leent, MMT, Soultanidis, G, Elschot, M, Gonai, H, Grendstad, K, Flobak, Å, Neckmann, U, Wolowczyk, C, Fisher, EL, Reiner, T, de Lange Davies, C, Bjørkøy, G, Teunissen, AJP, Ochando, J, Pérez-Medina, C, Mulder, WJM & Hak, S 2020, 'Tumor Targeting by α_vβ₃-Integrin-Specific Lipid Nanoparticles Occurs via Phagocyte Hitchhiking', ACS Nano, vol. 14, no. 7, pp. 7832-7846. https://doi.org/10.1021/acsnano.9b08693

TY - JOUR

T1 - Tumor Targeting by αvβ3-Integrin-Specific Lipid Nanoparticles Occurs via Phagocyte Hitchhiking

AU - Sofias, Alexandros Marios

AU - Toner, Yohana C.

AU - Meerwaldt, Anu E.

AU - van Leent, Mandy M.T.

AU - Soultanidis, Georgios

AU - Elschot, Mattijs

AU - Gonai, Haruki

AU - Grendstad, Kristin

AU - Flobak, Åsmund

AU - Neckmann, Ulrike

AU - Wolowczyk, Camilla

AU - Fisher, Elizabeth L.

AU - Reiner, Thomas

AU - de Lange Davies, Catharina

AU - Bjørkøy, Geir

AU - Teunissen, Abraham J.P.

AU - Ochando, Jordi

AU - Pérez-Medina, Carlos

AU - Mulder, Willem J.M.

AU - Hak, Sjoerd

PY - 2020/7/28

Y1 - 2020/7/28

N2 - Although the first nanomedicine was clinically approved more than two decades ago, nanoparticles' (NP) in vivo behavior is complex and the immune system's role in their application remains elusive. At present, only passive-targeting nanoformulations have been clinically approved, while more complicated active-targeting strategies typically fail to advance from the early clinical phase stage. This absence of clinical translation is, among others, due to the very limited understanding for in vivo targeting mechanisms. Dynamic in vivo phenomena such as NPs' real-time targeting kinetics and phagocytes' contribution to active NP targeting remain largely unexplored. To better understand in vivo targeting, monitoring NP accumulation and distribution at complementary levels of spatial and temporal resolution is imperative. Here, we integrate in vivo positron emission tomography/computed tomography imaging with intravital microscopy and flow cytometric analyses to study αvβ3-integrin-targeted cyclic arginine-glycine-aspartate decorated liposomes and oil-in-water nanoemulsions in tumor mouse models. We observed that ligand-mediated accumulation in cancerous lesions is multifaceted and identified "NP hitchhiking" with phagocytes to contribute considerably to this intricate process. We anticipate that this understanding can facilitate rational improvement of nanomedicine applications and that immune cell-NP interactions can be harnessed to develop clinically viable nanomedicine-based immunotherapies.

AB - Although the first nanomedicine was clinically approved more than two decades ago, nanoparticles' (NP) in vivo behavior is complex and the immune system's role in their application remains elusive. At present, only passive-targeting nanoformulations have been clinically approved, while more complicated active-targeting strategies typically fail to advance from the early clinical phase stage. This absence of clinical translation is, among others, due to the very limited understanding for in vivo targeting mechanisms. Dynamic in vivo phenomena such as NPs' real-time targeting kinetics and phagocytes' contribution to active NP targeting remain largely unexplored. To better understand in vivo targeting, monitoring NP accumulation and distribution at complementary levels of spatial and temporal resolution is imperative. Here, we integrate in vivo positron emission tomography/computed tomography imaging with intravital microscopy and flow cytometric analyses to study αvβ3-integrin-targeted cyclic arginine-glycine-aspartate decorated liposomes and oil-in-water nanoemulsions in tumor mouse models. We observed that ligand-mediated accumulation in cancerous lesions is multifaceted and identified "NP hitchhiking" with phagocytes to contribute considerably to this intricate process. We anticipate that this understanding can facilitate rational improvement of nanomedicine applications and that immune cell-NP interactions can be harnessed to develop clinically viable nanomedicine-based immunotherapies.

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KW - nanomedicine

KW - neutrophils

KW - positron emission tomography/computed tomography imaging

KW - Integrin alphaV

KW - Neoplasms/drug therapy

KW - Lipids

KW - Integrin alphaVbeta3

KW - Nanoparticles

KW - Phagocytes

KW - Animals

KW - Mice

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