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      Monitoring the dynamics of hemeoxygenase-1 activation in head and neck cancer cells in real-time using plasmonically enhanced Raman spectroscopy†

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          Abstract

          Real-time monitoring of the dynamics of pharmacologically generated HO-1 in mammalian cells by using plasmonically enhanced Raman spectroscopy (PERS).

          Abstract

          We report for the first time the usage of plasmonically enhanced Raman spectroscopy (PERS) to directly monitor the dynamics of pharmacologically generated hemeoxygenase-1 (HO-1) by evaluating the kinetics of formation of carbon monoxide (CO), one of the metabolites of HO-1 activation, in live cells during cisplatin treatment. Being an endogenous signaling molecule, CO plays an important role in cancer regression. Many aspects of HO-1's and CO's functions in biology are still unclear largely due to the lack of technological tools for the real-time monitoring of their dynamics in live cells and tissues. In this study, we found that, together with nuclear region-targeted gold nanocubes (AuNCs), cisplatin treatment can dramatically trigger the activation of HO-1 and thereby the rate and production of CO in mammalian cells in a dose-dependent manner. Though quantitative molecular data revealed that a lower concentration of cisplatin up-regulates HO-1 expression in cancer cells, PERS data suggest that it poorly facilitates the activation of HO-1 and thereby the production of CO. However, at a higher dose, cisplatin along with AuNCs could significantly enhance the activation of HO-1 in cancer cells, which could be probed in real-time by monitoring the CO generation by using PERS. Under the same conditions, the rate of formation of CO in healthy cells was relatively higher in comparison to the cancer cells. Additionally, molecular data revealed that AuNCs have the potential to suppress the up-regulation of HO-1 in cancer cells during cisplatin treatment at a lower concentration. As up-regulation of HO-1 has a significant role in cell adaptation to oxidative stress in cancer cells, the ability of AuNCs in suppressing the HO-1 overexpression will have a remarkable impact in the development of nanoformulations for combination cancer therapy. This exploratory study demonstrates the unique possibilities of PERS in the real-time monitoring of endogenously generated CO and thereby the dynamics of HO-1 in live cells, which could expedite our understanding of the signaling action of CO and HO-1 in cancer progression.

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          Author and article information

          Journal
          Chem Sci
          Chem Sci
          Chemical Science
          Royal Society of Chemistry
          2041-6520
          2041-6539
          22 March 2019
          14 May 2019
          : 10
          : 18
          : 4876-4882
          Affiliations
          [a ] Laser Dynamics Laboratory , School of Chemistry and Biochemistry , Georgia Institute of Technology , Atlanta , Georgia 30332 , USA . Email: melsayed@ 123456gatech.edu
          [b ] Georgia State University , Department of Biology , Atlanta , GA , USA
          Author information
          http://orcid.org/0000-0002-8337-9591
          http://orcid.org/0000-0002-7674-8424
          Article
          c9sc00093c
          10.1039/c9sc00093c
          6520930
          8d201000-2196-4306-a065-b913d473593b
          This journal is © The Royal Society of Chemistry 2019

          This article is freely available. This article is licensed under a Creative Commons Attribution Non Commercial 3.0 Unported Licence (CC BY-NC 3.0)

          History
          : 7 January 2019
          : 21 March 2019
          Categories
          Chemistry

          Notes

          †Electronic supplementary information (ESI) available: TEM image of AuNCs, extinction spectra of AuNCs, additional PERS data, and dark field images, in silico analysis of HO-1 expression. See DOI: 10.1039/c9sc00093c


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