Functionalized Gold Nanoclusters Promote Stress Response in COS‐7 Cells

Author:

Linklater Denver P.1ORCID,Le Guével Xavier2,Kosyer Erim1,Rubanov Sergey3,Bryant Gary1,Hanssen Eric3,Baulin Vladimir A.4,Pereiro Eva5,Perera Palalle G.Tharushi1,Wandiyanto Jason V.6,Angulo Ana7,Juodkazis Saulius6,Ivanova Elena P.1

Affiliation:

1. STEM College School of Science RMIT University Melbourne VIC 3000 Australia

2. Cancer Targets and Experimental Therapeutics Institute for Advanced Biosciences University of Grenoble Alpes 38700 La Tronche France

3. Ian Holmes Imaging Centre Bio21 University of Melbourne Parkville 3052 VIC Australia

4. Departament de Química Física i Inorgànica Universitat Rovira i Virgili C/Marcel.lí Domingo s/n 43007 Tarragona Spain

5. MISTRAL Beamline-Experiments Division ALBA Synchrotron Light Source Cerdanyola del Vallès 08290 Barcelona Spain

6. Optical Sciences Centre Swinburne University of Technology Hawthorn VIC 3122 Australia

7. Immunology Unit Department of Biomedical Sciences Faculty of Medicine and Health Sciences University of Barcelona, Institut d’Investigacions Biomèdiques August Pi i Sunyer Barcelona Spain

Abstract

Ultrasmall gold nanoclusters (AuNC) show great promise for application in theranostics due to their unique optical and physicochemical properties; however, the associated nanotoxicology concerns need to be carefully considered because of their high diffusion across the cellular barrier. Herein, new insights into the role of surface modification of 2 nm AuNC on their toxicity with impact on the metabolism of COS‐7 fibroblast‐like cells are revealed. AuNCs are chemically modified with either a monodentate‐thiolated molecule (AuNC‐MHA) or a modified‐bidentate sulfobetaine zwitterionic molecule (AuNC‐ZwBuEt). Uptake and localization inside fibroblasts and the resultant influence on cell ultrastructure are carefully evaluated using scanning transmission electron microscopy (STEM) and cryo‐soft‐X‐ray tomography (cryo‐SXT). At concentrations of ≥25 μg Au mL−1, AuNC‐ZwBuEt are cytotoxic toward COS‐7 cells and are observed to cross the nuclear membrane. Cryo‐SXT analysis shows that fibroblasts develop an acute stress response in the form of swollen mitochondria, nuclear membrane blebbing, and large cytoplasmic vacuoles as early as 1 h postexposure. By contrast, AuNC‐MHA are not cytotoxic toward COS‐7 cells. Endosomal escape and translocation of the AuNC‐ZwBuEt into the nucleus and other organelles may be the cause for the observed cytotoxicity and highlight the need for further study of metal nanocluster‐cell interactions.

Publisher

Wiley

Subject

General Medicine

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