Visible Pulsed Laser-Assisted Selective Killing of Cancer Cells with PVP-Capped Plasmonic Gold Nanostars

Author:

Mishra Aniket1,Inaam Rafia1,Okamoto Shunya1,Shibata Takayuki12ORCID,Santra Tuhin Subhra3ORCID,Nagai Moeto12ORCID

Affiliation:

1. Department of Mechanical Engineering, Toyohashi University of Technology, Toyohashi 441-8580, Japan

2. Institute for Research on Next-Generation Semiconductor and Sensing Science (IRES2), Toyohashi University of Technology, Toyohashi 441-8580, Japan

3. Department of Engineering Design, Indian Institute of Technology Madras, Chennai 600036, India

Abstract

A new generation of nanoscale photosensitizer agents has improved photothermal capabilities, which has increased the impact of photothermal treatments (PTTs) in cancer therapy. Gold nanostars (GNS) are promising for more efficient and less invasive PTTs than gold nanoparticles. However, the combination of GNS and visible pulsed lasers remains unexplored. This article reports the use of a 532 nm nanosecond pulse laser and polyvinylpyrrolidone (PVP)-capped GNS to kill cancer cells with location-specific exposure. Biocompatible GNS were synthesized via a simple method and were characterized under FESEM, UV–visible spectroscopy, XRD analysis, and particle size analysis. GNS were incubated over a layer of cancer cells that were grown in a glass Petri dish. A nanosecond pulsed laser was irradiated on the cell layer, and cell death was verified via propidium iodide (PI) staining. We assessed the effectiveness of single-pulse spot irradiation and multiple-pulse laser scanning irradiation in inducing cell death. Since the site of cell killing can be accurately chosen with a nanosecond pulse laser, this technique will help minimize damage to the cells around the target cells.

Funder

JSPS KAKENHI

Nitto Foundation for Science Promotion

Foundation of Public Interest of Tatematsu

Amano Institute of Technology

Publisher

MDPI AG

Subject

Electrical and Electronic Engineering,Mechanical Engineering,Control and Systems Engineering

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