Multifunctional magneto-plasmonic nanoparticles (MP-NPs) are attracting increasing interest for biomedical applications due to their dual magnetic and optical properties. However, existing synthesis protocols for MP-NPs could be limited by harsh conditions or lengthy, complex procedures. These limitations can hinder the development of nanosystems that work effectively in biological dispersion. In this work, we present a flexible nanoplatform for capture and probe applications, based on MP-NPs and bioorthogonal plasmonic nanoparticles (AuNPs). This system enables efficient cell sorting and surface-enhanced Raman scattering (SERS) detection in complex biological media under dynamic conditions. Magnetic Fe₃O₄ nanoclusters were synthesized using a scalable, aqueous Massart-based protocol. These structures were then densely decorated with electrostatically assembled AuNPs, producing magnetically responsive and plasmonically active nanocomposites with high aqueous stability. A polyethylene glycol (PEG) derivative was used for surface functionalization, improving colloidal stability and enabling broad bio-recognition capability. To enhance detection sensitivity and shift the optical response into the near-infrared (NIR) range, bioorthogonal Raman-active gold nanostars (AuNSts) were integrated into a sandwich configuration with the MP-NPs. The system demonstrated selective sorting and sensitive SERS-based identification of cell subpopulation within a heterogeneous sample. Additionally, the integration of the MP-NPs assay into a 3D-printed microfluidic device allowed controlled nanoparticles manipulation using external magnets, enhancing magnetic separation, hot-spots generation, and assay reusability. Overall, these MP-NPs platform combines scalable synthesis, tunable colloidal and surface properties, and compatibility with microfluidic systems. This work lays the foundation for advanced biosensing approaches in lab-on-chip formats for clinical diagnostics and targeted analysis of rare cell populations.
Scalable synthesis of self-assembled magneto-plasmonic core-satellite nanoparticles for microfluidic sorting and bioorthogonal sensing of targeted cells
Feregotto, G.;Muzzi, B.;Pavone, F. S.;Calamai, M.;Capitini, C.;Dallari, C.;Credi, C.
2025
Abstract
Multifunctional magneto-plasmonic nanoparticles (MP-NPs) are attracting increasing interest for biomedical applications due to their dual magnetic and optical properties. However, existing synthesis protocols for MP-NPs could be limited by harsh conditions or lengthy, complex procedures. These limitations can hinder the development of nanosystems that work effectively in biological dispersion. In this work, we present a flexible nanoplatform for capture and probe applications, based on MP-NPs and bioorthogonal plasmonic nanoparticles (AuNPs). This system enables efficient cell sorting and surface-enhanced Raman scattering (SERS) detection in complex biological media under dynamic conditions. Magnetic Fe₃O₄ nanoclusters were synthesized using a scalable, aqueous Massart-based protocol. These structures were then densely decorated with electrostatically assembled AuNPs, producing magnetically responsive and plasmonically active nanocomposites with high aqueous stability. A polyethylene glycol (PEG) derivative was used for surface functionalization, improving colloidal stability and enabling broad bio-recognition capability. To enhance detection sensitivity and shift the optical response into the near-infrared (NIR) range, bioorthogonal Raman-active gold nanostars (AuNSts) were integrated into a sandwich configuration with the MP-NPs. The system demonstrated selective sorting and sensitive SERS-based identification of cell subpopulation within a heterogeneous sample. Additionally, the integration of the MP-NPs assay into a 3D-printed microfluidic device allowed controlled nanoparticles manipulation using external magnets, enhancing magnetic separation, hot-spots generation, and assay reusability. Overall, these MP-NPs platform combines scalable synthesis, tunable colloidal and surface properties, and compatibility with microfluidic systems. This work lays the foundation for advanced biosensing approaches in lab-on-chip formats for clinical diagnostics and targeted analysis of rare cell populations.| File | Dimensione | Formato | |
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Colloids and Surfaces B Biointerfaces 256 (2025) 115040.pdf
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1-s2.0-S0927776525005478-mmc1.pdf
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