Zero-valent iron based nanoparticles selectively inhibit cancerous cells through mitochondria-mediated autophagy

Dar Bin Shieh; Li Xing Yang; Wei Ting Lee; Kuang Jing Huang; Ya Na Wu; Wu Chou Su; Don Hwang Chen; Benjamin Tsang

doi:10.1109/NANO.2017.8117431

Zero-valent iron based nanoparticles selectively inhibit cancerous cells through mitochondria-mediated autophagy

Dar Bin Shieh, Li Xing Yang, Wei Ting Lee, Kuang Jing Huang, Ya Na Wu, Wu Chou Su, Don Hwang Chen, Benjamin Tsang

Research output: Chapter in Book/Report/Conference proceeding › Conference contribution

2 Citations (Scopus)

Abstract

How to improve the selectivity and efficacy of anticancer agents and to reduce side effects has always been a big challenge in clinical cancer therapy. Chemotherapeutic agents are usually toxic to both cancer and normal tissues, thus rendering compromised overall clinical outcome. Here we developed zero-valent iron nanoparticles (ZVI NPs) that exhibited selectivity toward higher toxicity to most cancerous cells thus opening a new era of anti-cancer therapy or adjuvant therapy through a novel molecular signaling pathway. We used head-and-neck cancer (HNC) cells and ovarian cancer (OVCA) cells to test the anti-cancer properties of ZVI NPs. The ZVI NPs served as a strong reactive oxygen species (ROS) inducer and caused irreversible mitochondria membrane potential lost in sensitive cancer cells that lead to cancer cell autophagy and growth suppression, while not significantly affect normal cell population. Further, the cytotoxicity of the ZVI NPs is highly depended on its redox state as oxidation of the NPs upon aging reduced their cytotoxic potency. In vivo study revealed a dose dependent tumor size reduction in tumor-bearing mice model without significant weight loss and pathological signs. These results suggest that ZVI NPs may serve as a new class of anticancer agent for a wide spectra of neoplastic diseases.

Original language	English
Title of host publication	2017 IEEE 17th International Conference on Nanotechnology, NANO 2017
Publisher	Institute of Electrical and Electronics Engineers Inc.
Pages	168-170
Number of pages	3
ISBN (Electronic)	9781509030286
DOIs	https://doi.org/10.1109/NANO.2017.8117431
Publication status	Published - 2017 Nov 21
Event	17th IEEE International Conference on Nanotechnology, NANO 2017 - Pittsburgh, United States Duration: 2017 Jul 25 → 2017 Jul 28

Publication series

Name	2017 IEEE 17th International Conference on Nanotechnology, NANO 2017

Other

Other	17th IEEE International Conference on Nanotechnology, NANO 2017
Country/Territory	United States
City	Pittsburgh
Period	17-07-25 → 17-07-28

All Science Journal Classification (ASJC) codes

Electronic, Optical and Magnetic Materials
Surfaces, Coatings and Films
Electrical and Electronic Engineering

Access to Document

10.1109/NANO.2017.8117431

Cite this

Shieh, D. B., Yang, L. X., Lee, W. T., Huang, K. J., Wu, Y. N., Su, W. C., Chen, D. H., & Tsang, B. (2017). Zero-valent iron based nanoparticles selectively inhibit cancerous cells through mitochondria-mediated autophagy. In 2017 IEEE 17th International Conference on Nanotechnology, NANO 2017 (pp. 168-170). Article 8117431 (2017 IEEE 17th International Conference on Nanotechnology, NANO 2017). Institute of Electrical and Electronics Engineers Inc.. https://doi.org/10.1109/NANO.2017.8117431

Shieh, Dar Bin ; Yang, Li Xing ; Lee, Wei Ting et al. / Zero-valent iron based nanoparticles selectively inhibit cancerous cells through mitochondria-mediated autophagy. 2017 IEEE 17th International Conference on Nanotechnology, NANO 2017. Institute of Electrical and Electronics Engineers Inc., 2017. pp. 168-170 (2017 IEEE 17th International Conference on Nanotechnology, NANO 2017).

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title = "Zero-valent iron based nanoparticles selectively inhibit cancerous cells through mitochondria-mediated autophagy",

abstract = "How to improve the selectivity and efficacy of anticancer agents and to reduce side effects has always been a big challenge in clinical cancer therapy. Chemotherapeutic agents are usually toxic to both cancer and normal tissues, thus rendering compromised overall clinical outcome. Here we developed zero-valent iron nanoparticles (ZVI NPs) that exhibited selectivity toward higher toxicity to most cancerous cells thus opening a new era of anti-cancer therapy or adjuvant therapy through a novel molecular signaling pathway. We used head-and-neck cancer (HNC) cells and ovarian cancer (OVCA) cells to test the anti-cancer properties of ZVI NPs. The ZVI NPs served as a strong reactive oxygen species (ROS) inducer and caused irreversible mitochondria membrane potential lost in sensitive cancer cells that lead to cancer cell autophagy and growth suppression, while not significantly affect normal cell population. Further, the cytotoxicity of the ZVI NPs is highly depended on its redox state as oxidation of the NPs upon aging reduced their cytotoxic potency. In vivo study revealed a dose dependent tumor size reduction in tumor-bearing mice model without significant weight loss and pathological signs. These results suggest that ZVI NPs may serve as a new class of anticancer agent for a wide spectra of neoplastic diseases.",

author = "Shieh, {Dar Bin} and Yang, {Li Xing} and Lee, {Wei Ting} and Huang, {Kuang Jing} and Wu, {Ya Na} and Su, {Wu Chou} and Chen, {Don Hwang} and Benjamin Tsang",

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doi = "10.1109/NANO.2017.8117431",

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Shieh, DB, Yang, LX, Lee, WT, Huang, KJ, Wu, YN, Su, WC , Chen, DH & Tsang, B 2017, Zero-valent iron based nanoparticles selectively inhibit cancerous cells through mitochondria-mediated autophagy. in 2017 IEEE 17th International Conference on Nanotechnology, NANO 2017., 8117431, 2017 IEEE 17th International Conference on Nanotechnology, NANO 2017, Institute of Electrical and Electronics Engineers Inc., pp. 168-170, 17th IEEE International Conference on Nanotechnology, NANO 2017, Pittsburgh, United States, 17-07-25. https://doi.org/10.1109/NANO.2017.8117431

Zero-valent iron based nanoparticles selectively inhibit cancerous cells through mitochondria-mediated autophagy. / Shieh, Dar Bin; Yang, Li Xing; Lee, Wei Ting et al.
2017 IEEE 17th International Conference on Nanotechnology, NANO 2017. Institute of Electrical and Electronics Engineers Inc., 2017. p. 168-170 8117431 (2017 IEEE 17th International Conference on Nanotechnology, NANO 2017).

Research output: Chapter in Book/Report/Conference proceeding › Conference contribution

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AU - Shieh, Dar Bin

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AU - Lee, Wei Ting

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AU - Wu, Ya Na

AU - Su, Wu Chou

AU - Chen, Don Hwang

AU - Tsang, Benjamin

PY - 2017/11/21

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N2 - How to improve the selectivity and efficacy of anticancer agents and to reduce side effects has always been a big challenge in clinical cancer therapy. Chemotherapeutic agents are usually toxic to both cancer and normal tissues, thus rendering compromised overall clinical outcome. Here we developed zero-valent iron nanoparticles (ZVI NPs) that exhibited selectivity toward higher toxicity to most cancerous cells thus opening a new era of anti-cancer therapy or adjuvant therapy through a novel molecular signaling pathway. We used head-and-neck cancer (HNC) cells and ovarian cancer (OVCA) cells to test the anti-cancer properties of ZVI NPs. The ZVI NPs served as a strong reactive oxygen species (ROS) inducer and caused irreversible mitochondria membrane potential lost in sensitive cancer cells that lead to cancer cell autophagy and growth suppression, while not significantly affect normal cell population. Further, the cytotoxicity of the ZVI NPs is highly depended on its redox state as oxidation of the NPs upon aging reduced their cytotoxic potency. In vivo study revealed a dose dependent tumor size reduction in tumor-bearing mice model without significant weight loss and pathological signs. These results suggest that ZVI NPs may serve as a new class of anticancer agent for a wide spectra of neoplastic diseases.

AB - How to improve the selectivity and efficacy of anticancer agents and to reduce side effects has always been a big challenge in clinical cancer therapy. Chemotherapeutic agents are usually toxic to both cancer and normal tissues, thus rendering compromised overall clinical outcome. Here we developed zero-valent iron nanoparticles (ZVI NPs) that exhibited selectivity toward higher toxicity to most cancerous cells thus opening a new era of anti-cancer therapy or adjuvant therapy through a novel molecular signaling pathway. We used head-and-neck cancer (HNC) cells and ovarian cancer (OVCA) cells to test the anti-cancer properties of ZVI NPs. The ZVI NPs served as a strong reactive oxygen species (ROS) inducer and caused irreversible mitochondria membrane potential lost in sensitive cancer cells that lead to cancer cell autophagy and growth suppression, while not significantly affect normal cell population. Further, the cytotoxicity of the ZVI NPs is highly depended on its redox state as oxidation of the NPs upon aging reduced their cytotoxic potency. In vivo study revealed a dose dependent tumor size reduction in tumor-bearing mice model without significant weight loss and pathological signs. These results suggest that ZVI NPs may serve as a new class of anticancer agent for a wide spectra of neoplastic diseases.

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Shieh DB, Yang LX, Lee WT, Huang KJ, Wu YN, Su WC et al. Zero-valent iron based nanoparticles selectively inhibit cancerous cells through mitochondria-mediated autophagy. In 2017 IEEE 17th International Conference on Nanotechnology, NANO 2017. Institute of Electrical and Electronics Engineers Inc. 2017. p. 168-170. 8117431. (2017 IEEE 17th International Conference on Nanotechnology, NANO 2017). doi: 10.1109/NANO.2017.8117431

Zero-valent iron based nanoparticles selectively inhibit cancerous cells through mitochondria-mediated autophagy

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