The detrimental invasiveness of glioma cells controlled by gadolinium chelate-coated gold nanoparticles.


Journal

Nanoscale
ISSN: 2040-3372
Titre abrégé: Nanoscale
Pays: England
ID NLM: 101525249

Informations de publication

Date de publication:
27 May 2021
Historique:
pubmed: 13 5 2021
medline: 1 6 2021
entrez: 12 5 2021
Statut: ppublish

Résumé

Glioblastoma are characterized by an invasive phenotype, which is thought to be responsible for recurrences and the short overall survival of patients. In the last decade, the promising potential of ultrasmall gadolinium chelate-coated gold nanoparticles (namely Au@DTDTPA(Gd)) was evidenced for image-guided radiotherapy in brain tumors. Considering the threat posed by invasiveness properties of glioma cells, we were interested in further investigating the biological effects of Au@DTDTPA(Gd) by examining their impact on GBM cell migration and invasion. In our work, exposure of U251 glioma cells to Au@DTDTPA(Gd) led to high accumulation of gold nanoparticles, that were mainly diffusely distributed in the cytoplasm of the tumor cells. Experiments pointed out a significant decrease in glioma cell invasiveness when exposed to nanoparticles. As the proteolysis activities were not directly affected by the intracytoplasmic accumulation of Au@DTDTPA(Gd), the anti-invasive effect cannot be attributed to matrix remodeling impairment. Rather, Au@DTDTPA(Gd) nanoparticles affected the intrinsic biomechanical properties of U251 glioma cells, such as cell stiffness, adhesion and generated traction forces, and significantly reduced the formation of protrusions, thus exerting an inhibitory effect on their migration capacities. Consistently, analysis of talin-1 expression and membrane expression of beta 1 integrin evoke the stabilization of focal adhesion plaques in the presence of nanoparticles. Taken together, our results highlight the interest in Au@DTDTPA(Gd) nanoparticles for the therapeutic management of astrocytic tumors, not only as a radio-enhancing agent but also by reducing the invasive potential of glioma cells.

Identifiants

pubmed: 33977943
doi: 10.1039/d0nr08936b
doi:

Substances chimiques

Gold 7440-57-5
Gadolinium AU0V1LM3JT

Types de publication

Journal Article

Langues

eng

Sous-ensembles de citation

IM

Pagination

9236-9251

Auteurs

Maxime Durand (M)

Université de Lorraine, CNRS, CRAN, F-54000 Nancy, France. sophie.pinel@univ-lorraine.fr.

Elodie Lelievre (E)

Université de Reims-Champagne-Ardennes, UMR CNRS/URCA 7369, MEDyC, F-51100 Reims, France. jerome.devy@univ-reims.fr.

Alicia Chateau (A)

Université de Lorraine, CNRS, CRAN, F-54000 Nancy, France. sophie.pinel@univ-lorraine.fr.

Alexandre Berquand (A)

Université de Reims-Champagne-Ardennes, EA 4682, F-51100 Reims, France.

Gautier Laurent (G)

Université Bourgogne Franche-Comté, UMR CNRS 6213-UBFC, UTINAM, F-25000 Besançon, France.

Philippe Carl (P)

Université de Strasbourg, CNRS UMR 7021 - Strasbourg, France.

Stéphane Roux (S)

Université Bourgogne Franche-Comté, UMR CNRS 6213-UBFC, UTINAM, F-25000 Besançon, France.

Lise Chazee (L)

Université de Reims-Champagne-Ardennes, UMR CNRS/URCA 7369, MEDyC, F-51100 Reims, France. jerome.devy@univ-reims.fr.

Rana Bazzi (R)

Université Bourgogne Franche-Comté, UMR CNRS 6213-UBFC, UTINAM, F-25000 Besançon, France.

Frederic Eghiaian (F)

Abberior Instruments GmbH, F-13008 Marseille, France.

Justine Jubreaux (J)

Université de Lorraine, CNRS, CRAN, F-54000 Nancy, France. sophie.pinel@univ-lorraine.fr.

Philippe Ronde (P)

Université de Strasbourg, CNRS UMR 7021 - Strasbourg, France.

Muriel Barberi-Heyob (M)

Université de Lorraine, CNRS, CRAN, F-54000 Nancy, France. sophie.pinel@univ-lorraine.fr.

Pascal Chastagner (P)

Université de Lorraine, CNRS, CRAN, F-54000 Nancy, France. sophie.pinel@univ-lorraine.fr.

Jérôme Devy (J)

Université de Reims-Champagne-Ardennes, UMR CNRS/URCA 7369, MEDyC, F-51100 Reims, France. jerome.devy@univ-reims.fr.

Sophie Pinel (S)

Université de Lorraine, CNRS, CRAN, F-54000 Nancy, France. sophie.pinel@univ-lorraine.fr.

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Classifications MeSH