Delayed alveolar clearance of nanoparticles through control of coating composition and interaction with lung surfactant protein A

Susana Carregal-Romero; Hugo Groult; Olga Cañadas; Noelia A-Gonzalez; Ana Victoria Lechuga-Vieco; Belén García-Fojeda; Fernando Herranz; Juan Pellico; Andrés Hidalgo; Cristina Casals; Jesús Ruiz-Cabello

doi:10.1016/j.msec.2021.112551

Delayed alveolar clearance of nanoparticles through control of coating composition and interaction with lung surfactant protein A

Susana Carregal-Romero
, Hugo Groult
, Olga Cañadas
, Noelia A-Gonzalez
, Ana Victoria Lechuga-Vieco
, Belén García-Fojeda
, Fernando Herranz
, Juan Pellico
, Andrés Hidalgo
, Cristina Casals
, Jesús Ruiz-Cabello

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

17 Scopus citations

Abstract

The coating composition of nanomedicines is one of the main features in determining the medicines' fate, clearance, and immunoresponse in the body. To highlight the coatings' impact in pulmonary administration, two micellar superparamagnetic iron oxide nanoparticles (SPION) were compared. These nanoparticles are similar in size and charge but have different coatings: either phosphatidylcholine (PC-SPION) or bovine serum albumin (BSA-SPION). The aim of the study was to increase the understanding of the nano-bio interaction with the cellular and non-cellular components of the lung and underline valuable coatings either for local lung-targeted drug delivery in theranostic application or patient-friendly route systemic administration. PC-SPION and BSA-SPION were deposited in the alveoli by in vivo instillation and, despite the complexity of imaging the lung, SPION were macroscopically visualized by MRI. Impressively, PC-SPION were retained within the lungs for at least a week, while BSA-SPION were cleared more rapidly. The different lung residence times were confirmed by histological analysis and supported by a flow cytometry analysis of the SPION interactions with different myeloid cell populations. To further comprehend the way in which these nanoformulations interact with lung components at the molecular level, we used fluorescence spectroscopy, turbidity measurements, and dynamic light scattering to evaluate the interactions of the two SPION with surfactant protein A (SP-A), a key protein in setting up the nanoparticle behavior in the alveolar fluid. We found that SP-A induced aggregation of PC-SPION, but not BSA-SPION, which likely caused PC-SPION retention in the lung without inducing inflammation. In conclusion, the two SPION show different outcomes from interaction with SP-A leading to distinctive fate in the lung. PC-SPION hold great promise as imaging and theranostic agents when prolonged pulmonary drug delivery is required.

Original language	English
Article number	112551
Journal	Biomaterials Advances
Volume	134
DOIs	https://doi.org/10.1016/j.msec.2021.112551
State	Published - Mar 2022
Externally published	Yes

Keywords

Lung clearance
Magnetic resonance imaging
Micellar superparamagnetic iron oxide nanoparticles
Pulmonary administration
Surfactant protein A

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10.1016/j.msec.2021.112551

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Carregal-Romero, S., Groult, H., Cañadas, O., A-Gonzalez, N., Lechuga-Vieco, A. V., García-Fojeda, B., Herranz, F., Pellico, J., Hidalgo, A., Casals, C., & Ruiz-Cabello, J. (2022). Delayed alveolar clearance of nanoparticles through control of coating composition and interaction with lung surfactant protein A. Biomaterials Advances, 134, Article 112551. https://doi.org/10.1016/j.msec.2021.112551

@article{9ac31a28c983470b9c386e9cffa400b9,

title = "Delayed alveolar clearance of nanoparticles through control of coating composition and interaction with lung surfactant protein A",

abstract = "The coating composition of nanomedicines is one of the main features in determining the medicines' fate, clearance, and immunoresponse in the body. To highlight the coatings' impact in pulmonary administration, two micellar superparamagnetic iron oxide nanoparticles (SPION) were compared. These nanoparticles are similar in size and charge but have different coatings: either phosphatidylcholine (PC-SPION) or bovine serum albumin (BSA-SPION). The aim of the study was to increase the understanding of the nano-bio interaction with the cellular and non-cellular components of the lung and underline valuable coatings either for local lung-targeted drug delivery in theranostic application or patient-friendly route systemic administration. PC-SPION and BSA-SPION were deposited in the alveoli by in vivo instillation and, despite the complexity of imaging the lung, SPION were macroscopically visualized by MRI. Impressively, PC-SPION were retained within the lungs for at least a week, while BSA-SPION were cleared more rapidly. The different lung residence times were confirmed by histological analysis and supported by a flow cytometry analysis of the SPION interactions with different myeloid cell populations. To further comprehend the way in which these nanoformulations interact with lung components at the molecular level, we used fluorescence spectroscopy, turbidity measurements, and dynamic light scattering to evaluate the interactions of the two SPION with surfactant protein A (SP-A), a key protein in setting up the nanoparticle behavior in the alveolar fluid. We found that SP-A induced aggregation of PC-SPION, but not BSA-SPION, which likely caused PC-SPION retention in the lung without inducing inflammation. In conclusion, the two SPION show different outcomes from interaction with SP-A leading to distinctive fate in the lung. PC-SPION hold great promise as imaging and theranostic agents when prolonged pulmonary drug delivery is required.",

keywords = "Lung clearance, Magnetic resonance imaging, Micellar superparamagnetic iron oxide nanoparticles, Pulmonary administration, Surfactant protein A",

author = "Susana Carregal-Romero and Hugo Groult and Olga Ca{\~n}adas and Noelia A-Gonzalez and Lechuga-Vieco, \{Ana Victoria\} and Bel{\'e}n Garc{\'i}a-Fojeda and Fernando Herranz and Juan Pellico and Andr{\'e}s Hidalgo and Cristina Casals and Jes{\'u}s Ruiz-Cabello",

note = "Publisher Copyright: {\textcopyright} 2021 The Authors",

year = "2022",

month = mar,

doi = "10.1016/j.msec.2021.112551",

language = "English",

volume = "134",

journal = "Biomaterials Advances",

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Carregal-Romero, S, Groult, H, Cañadas, O, A-Gonzalez, N, Lechuga-Vieco, AV, García-Fojeda, B, Herranz, F, Pellico, J, Hidalgo, A, Casals, C & Ruiz-Cabello, J 2022, 'Delayed alveolar clearance of nanoparticles through control of coating composition and interaction with lung surfactant protein A', Biomaterials Advances, vol. 134, 112551. https://doi.org/10.1016/j.msec.2021.112551

TY - JOUR

T1 - Delayed alveolar clearance of nanoparticles through control of coating composition and interaction with lung surfactant protein A

AU - Carregal-Romero, Susana

AU - Groult, Hugo

AU - Cañadas, Olga

AU - A-Gonzalez, Noelia

AU - Lechuga-Vieco, Ana Victoria

AU - García-Fojeda, Belén

AU - Herranz, Fernando

AU - Pellico, Juan

AU - Hidalgo, Andrés

AU - Casals, Cristina

AU - Ruiz-Cabello, Jesús

PY - 2022/3

Y1 - 2022/3

N2 - The coating composition of nanomedicines is one of the main features in determining the medicines' fate, clearance, and immunoresponse in the body. To highlight the coatings' impact in pulmonary administration, two micellar superparamagnetic iron oxide nanoparticles (SPION) were compared. These nanoparticles are similar in size and charge but have different coatings: either phosphatidylcholine (PC-SPION) or bovine serum albumin (BSA-SPION). The aim of the study was to increase the understanding of the nano-bio interaction with the cellular and non-cellular components of the lung and underline valuable coatings either for local lung-targeted drug delivery in theranostic application or patient-friendly route systemic administration. PC-SPION and BSA-SPION were deposited in the alveoli by in vivo instillation and, despite the complexity of imaging the lung, SPION were macroscopically visualized by MRI. Impressively, PC-SPION were retained within the lungs for at least a week, while BSA-SPION were cleared more rapidly. The different lung residence times were confirmed by histological analysis and supported by a flow cytometry analysis of the SPION interactions with different myeloid cell populations. To further comprehend the way in which these nanoformulations interact with lung components at the molecular level, we used fluorescence spectroscopy, turbidity measurements, and dynamic light scattering to evaluate the interactions of the two SPION with surfactant protein A (SP-A), a key protein in setting up the nanoparticle behavior in the alveolar fluid. We found that SP-A induced aggregation of PC-SPION, but not BSA-SPION, which likely caused PC-SPION retention in the lung without inducing inflammation. In conclusion, the two SPION show different outcomes from interaction with SP-A leading to distinctive fate in the lung. PC-SPION hold great promise as imaging and theranostic agents when prolonged pulmonary drug delivery is required.

AB - The coating composition of nanomedicines is one of the main features in determining the medicines' fate, clearance, and immunoresponse in the body. To highlight the coatings' impact in pulmonary administration, two micellar superparamagnetic iron oxide nanoparticles (SPION) were compared. These nanoparticles are similar in size and charge but have different coatings: either phosphatidylcholine (PC-SPION) or bovine serum albumin (BSA-SPION). The aim of the study was to increase the understanding of the nano-bio interaction with the cellular and non-cellular components of the lung and underline valuable coatings either for local lung-targeted drug delivery in theranostic application or patient-friendly route systemic administration. PC-SPION and BSA-SPION were deposited in the alveoli by in vivo instillation and, despite the complexity of imaging the lung, SPION were macroscopically visualized by MRI. Impressively, PC-SPION were retained within the lungs for at least a week, while BSA-SPION were cleared more rapidly. The different lung residence times were confirmed by histological analysis and supported by a flow cytometry analysis of the SPION interactions with different myeloid cell populations. To further comprehend the way in which these nanoformulations interact with lung components at the molecular level, we used fluorescence spectroscopy, turbidity measurements, and dynamic light scattering to evaluate the interactions of the two SPION with surfactant protein A (SP-A), a key protein in setting up the nanoparticle behavior in the alveolar fluid. We found that SP-A induced aggregation of PC-SPION, but not BSA-SPION, which likely caused PC-SPION retention in the lung without inducing inflammation. In conclusion, the two SPION show different outcomes from interaction with SP-A leading to distinctive fate in the lung. PC-SPION hold great promise as imaging and theranostic agents when prolonged pulmonary drug delivery is required.

KW - Lung clearance

KW - Magnetic resonance imaging

KW - Micellar superparamagnetic iron oxide nanoparticles

KW - Pulmonary administration

KW - Surfactant protein A

UR - https://www.scopus.com/pages/publications/85214073161

U2 - 10.1016/j.msec.2021.112551

DO - 10.1016/j.msec.2021.112551

M3 - Article

AN - SCOPUS:85214073161

SN - 2772-9508

VL - 134

JO - Biomaterials Advances

JF - Biomaterials Advances

M1 - 112551

ER -

Delayed alveolar clearance of nanoparticles through control of coating composition and interaction with lung surfactant protein A

Abstract

Keywords

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