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The Effect of Substrate Properties on Cellular Behavior and Nanoparticle Uptake in Human Fibroblasts and Epithelial Cells

Nanomaterials 2024 12 citations ? Citation count from OpenAlex, updated daily. May differ slightly from the publisher's own count. Score: 60 ? 0–100 AI score estimating relevance to the microplastics field. Papers below 30 are filtered from public browse.
Mauro Sousa de Almeida, Alke Petri‐Fink Aaron Lee, Barbara Rothen‐Rutishauser, Alke Petri‐Fink Alke Petri‐Fink Barbara Rothen‐Rutishauser, Alke Petri‐Fink Barbara Rothen‐Rutishauser, Barbara Rothen‐Rutishauser, Barbara Rothen‐Rutishauser, Barbara Rothen‐Rutishauser, Barbara Rothen‐Rutishauser, Barbara Rothen‐Rutishauser, Fabian Itel, Barbara Rothen‐Rutishauser, Alke Petri‐Fink Alke Petri‐Fink Alke Petri‐Fink Barbara Rothen‐Rutishauser, Barbara Rothen‐Rutishauser, Katharina Maniura‐Weber, Alke Petri‐Fink Barbara Rothen‐Rutishauser, Alke Petri‐Fink Alke Petri‐Fink Alke Petri‐Fink Alke Petri‐Fink Alke Petri‐Fink Barbara Rothen‐Rutishauser, Alke Petri‐Fink Barbara Rothen‐Rutishauser, Barbara Rothen‐Rutishauser, Barbara Rothen‐Rutishauser, Alke Petri‐Fink Barbara Rothen‐Rutishauser, Fabian Itel, Alke Petri‐Fink Barbara Rothen‐Rutishauser, Barbara Rothen‐Rutishauser, Barbara Rothen‐Rutishauser, Alke Petri‐Fink Barbara Rothen‐Rutishauser, Alke Petri‐Fink Alke Petri‐Fink Barbara Rothen‐Rutishauser, Alke Petri‐Fink

Summary

Researchers found that the physical properties of the surface cells grow on significantly affects how they take up nanoparticles, with lung fibroblast cells on soft, flexible surfaces absorbing over three times more silica nanoparticles than cells on rigid surfaces. This finding is important for understanding microplastic health effects because it suggests that nanoparticle uptake in the body depends on the tissue environment, not just the particles themselves. Cells in soft tissues like the lungs may be more vulnerable to nanoplastic absorption than lab tests on rigid surfaces would predict.

Polymers
Study Type In vivo

The delivery of nanomedicines into cells holds enormous therapeutic potential; however little is known regarding how the extracellular matrix (ECM) can influence cell-nanoparticle (NP) interactions. Changes in ECM organization and composition occur in several pathophysiological states, including fibrosis and tumorigenesis, and may contribute to disease progression. We show that the physical characteristics of cellular substrates, that more closely resemble the ECM in vivo, can influence cell behavior and the subsequent uptake of NPs. Electrospinning was used to create two different substrates made of soft polyurethane (PU) with aligned and non-aligned nanofibers to recapitulate the ECM in two different states. To investigate the impact of cell-substrate interaction, A549 lung epithelial cells and MRC-5 lung fibroblasts were cultured on soft PU membranes with different alignments and compared against stiff tissue culture plastic (TCP)/glass. Both cell types could attach and grow on both PU membranes with no signs of cytotoxicity but with increased cytokine release compared with cells on the TCP. The uptake of silica NPs increased more than three-fold in fibroblasts but not in epithelial cells cultured on both membranes. This study demonstrates that cell-matrix interaction is substrate and cell-type dependent and highlights the importance of considering the ECM and tissue mechanical properties when designing NPs for effective cell targeting and treatment.

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