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Anticancer efficacité de la thérapie photodynamique avec Lung Cancer-ciblée Nanoparticules

Published: December 01, 2016
doi:
10.3791/54865
, ,
1Department of Thoracic and Cardiovascular Surgery,Seoul National University Bundang Hospital, 2College of Pharmacy,Kangwon National University, 3Department of Thoracic and Cardiovascular Surgery,Seoul National University College of Medicine

Summary

Photodynamic therapy (PDT) is an alternative choice for lung cancer treatment. To increase the therapeutic effect of PDT, lung cancer-targeted nanoparticles combined with chemotherapy were developed. Both in vitro and in vivo anticancer efficacies of PDT with prepared nanoparticles were evaluated.

Abstract

Photodynamic therapy (PDT) is a non-invasive and non-surgical method representing an attractive alternative choice for lung cancer treatment. Photosensitizers selectively accumulate in tumor tissue and lead to tumor cell death in the presence of oxygen and the proper wavelength of light.

To increase the therapeutic effect of PDT, we developed both photosensitizer- and anticancer agent-loaded lung cancer-targeted nanoparticles. Both enhanced permeability and retention (EPR) effect-based passive targeting and hyaluronic-acid-CD44 interaction-based active targeting were applied. CD44 is a well-known hyaluronic acid receptor that is often introduced as a biomarker of non-small cell lung cancer.

In addition, a combination of PDT and chemotherapy is adopted in the present study. This combination concept may increase anticancer therapeutic effects and reduce adverse reactions.

We chose hypocrellin B (HB) as a novel photosensitizer in this study. It has been reported that HB causes higher anticancer efficacy of PDT compared to hematoporphyrin derivatives1. Paclitaxel was selected as the anticancer drug since it has proven to be a potential treatment for lung cancer2.

The antitumor efficacies of photosensitizer (HB) solution, photosensitizer encapsulated hyaluronic acid-ceramide nanoparticles (HB-NPs), and both photosensitizer- and anticancer agent (paclitaxel)-encapsulated hyaluronic acid-ceramide nanoparticles (HB-P-NPs) after PDT were compared both in vitro and in vivo. The in vitro phototoxicity in A549 (human lung adenocarcinoma) cells and the in vivo antitumor efficacy in A549 tumor-bearing mice were evaluated.

The HB-P-NP treatment group showed the most effective anticancer effect after PDT. In conclusion, the HB-P-NPs prepared in the present study represent a potential and novel photosensitizer delivery system in treating lung cancer with PDT.

Introduction

Photodynamic therapy (PDT) is composed of three major factors: photosensitizers, light, and oxygen. PDT is reported as a promising treatment for various cancers3. When the photosensitizers are administered into the cancer patient, they selectively accumulate in the tumor tissues. When the proper wavelength of light is applied, the highly reactive singlet oxygen and other free radicals lead to tumor cell damage4.

Lung cancer was introduced as one of the first applications for PDT in the early 1980s5. PDT provides several advantages in treating lung cancer. Since PDT is a non-invasive and non-surgical treatment, it is an attractive alternative choice for the patients in whom surgical resection is inappropriate.

There have been many challenges to enhance the cancer-targeting efficacy of the photosensitizers. Increasing photosensitizer accumulation in cancer sites and decreasing accumulation in normal tissues are the identical goals for the cancer-targeting studies. A variety of targeted drug delivery systems, such as polymers, liposomes, and nanoparticles are adopted as photosensitizer carriers6-8. In our previous studies, nanoparticles effectively increased the cancer-targeting abilities of the photosensitizers9,10. Nanoparticles are ideal cancer-targeting carriers since they possess both passive and active targeting abilities. The leaky tumor vessels provide opportunity for nano-sized carriers to accumulate easily in tumors, which is well-known as the enhanced permeability and retention (EPR) effect11,12. The interaction between the nanoparticles and the specific receptors on cancer cells enables active cancer targeting. In this study, we prepared hyaluronic acid-based nanoparticles to interact with CD44, the major hyaluronic acid receptor that is overexpressed on lung cancer cells13.

To maximize the anticancer efficacy, a combination of PDT and chemotherapy is adopted in the present study. This combination concept may permit an increased therapeutic effect. Furthermore, decreased doses of both the photosensitizer and the anticancer drug can diminish adverse effects. We selected hypocrellin B (HB) as a novel photosensitizer in the present study. HB is isolated from Chinese medicinal fungus Hypocrella bambuase. Shang et al. reported that HB-based PDT possesses a higher anticancer efficacy when compared to hematoporphyrin derivative-based PDT1. Paclitaxel was selected as the anticancer drug since it has proven to be a potential treatment for various cancers, including lung cancer2.

Herein, we compared the anticancer efficacies of photosensitizer (hypocrellin B, HB) solution, photosensitizer-encapsulated hyaluronic acid-ceramide nanoparticles (HB-NPs), and both photosensitizer- and anticancer agent (paclitaxel)-encapsulated hyaluronic acid-ceramide nanoparticles (HB-P-NPs) after PDT. The in vitro phototoxicity in A549 (human lung adenocarcinoma) cells and the in vivo antitumor efficacy in A549 tumor-bearing mice were evaluated.

Protocol

NOTE: Tous les protocoles d'études animales ont été approuvés par le soin et l'utilisation des animaux Comité institutionnel de l'hôpital Bundang Université nationale de Séoul (BA1308-134 / 072-01). 1. Synthèse de l'Acide Hyaluronique-céramide (HACE) Solubiliser 12,21 mmol d'acide hyaluronique (HA) oligomère et 9,77 mmol de tétra n – butylammonium hydroxyde (TBA) dans 60 ml d'eau distillée deux fois (DDW). On agite pendant 30 min. Pour synthétis…

Representative Results

Nous avons préparé deux HB-NPs et HB-P-NPs avec les techniques mentionnées ci-dessus. Les diamètres moyens de HB-NPs et HB-P-NPs étaient 220,9 ± 3,2 nm et 211,9 ± 1,6 nm, respectivement. La viabilité cellulaire des cellules A549 après 4 heures d'incubation avec du PBS, NPs vides, HB-NPs et HB-P-NPs suivie d' une irradiation de lumière (0 à 16 J / cm 2) est représentée sur la figure 1.</s…

Discussion

L'étape la plus critique dans cette étude est de choisir les conditions de laser appropriés: longueur d'onde, la puissance et le temps d'irradiation. La longueur d'onde appropriée de lumière appropriée pour le photosensibilisateur spécifique est nécessaire pour la PDT. Nous avons utilisé un laser 630-nm qui était approprié pour hypocrelline B. La puissance de sortie est un autre facteur important, qui a été fixé à 400 mW / cm 2 sur la base de nombreuses études pilotes. Puissanc…

Divulgazioni

The authors have nothing to disclose.

Acknowledgements

Cette étude a été soutenue par aucune subvention. 14-2014-017 du Fonds pour la recherche SNUBH.

Les auteurs remercient J. Patrick Barron, professeur émérite, Université de médecine de Tokyo et professeur adjoint, Hôpital Bundang Université nationale de Séoul pour sa pro bono édition de ce manuscrit.

Materials

oligo hyaluronic acid Bioland Co., Ltd. _
DS-Y30 (ceramide 3B; mainly N-oleoyl-phytosphingosine) Doosan Biotech Co., Ltd. _
adipic acid dihydrazide Sigma Aldrich A0638
N-(3-dimethylaminopropyl)-N′-ethylcarbodiimide Sigma Aldrich 39391
4-(chloromethyl)benzoyl chloride Sigma Aldrich 270784
Tween 80 Tokyo Chemical Industry Co., Ltd. T0546
syringe filter Sartorius Stedim Biotech GmbH 17762 15 mm, RC, PP, 0.45 µm
triethylamine Sigma Aldrich T0886
Mini-GeBAflex tubes Gene Bio-Application Ltd. D070-12-100
Paclitaxel Taihua Corporations _
RPMI-1640 Gibco Life Technologies, Inc. 11875
Penicillin–streptomycin Gibco Life Technologies, Inc. 15070
Fetal bovine serum Gibco Life Technologies, Inc. 16140071
Celite (Filter agent) Sigma Aldrich 6858 See step 1.4
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Riferimenti

  1. Shang, L., Zhou, N., Gu, Y., Liu, F., Zeng, J. Comparative study on killing effect of esophageal cancer cell line between hypocrellin B-photodynamic therapy and hematoporphyrin derivative-photodynamic therapy. Chin J Cancer Prev Treat. 12, 1139-1142 (2005).
  2. Huisman, C., et al. Paclitaxel triggers cell death primarily via caspase-independent routes in the non-small cell lung cancer cell line NCI-H460. Clin Cancer Res. 8 (2), 596-606 (2002).
  3. Dolmans, D. E., Fukumura, D., Jain, R. K. Photodynamic therapy for cancer. Nat Rev Cancer. 3 (5), 380-387 (2003).
  4. Pass, H. I. Photodynamic therapy in oncology: mechanisms and clinical use. J Natl Cancer Inst. 85 (6), 443-456 (1993).
  5. Sutedja, T. G., Postmus, P. E. Photodynamic therapy in lung cancer. A review . J. Photochem. Photobiol. 36 (2), 199-204 (1996).
  6. Peng, C. L., Shieh, M. J., Tsai, M. H., Chang, C. C., Lai, P. S. Self-assembled star-shaped chlorin-core poly(epsilon-caprolactone)-poly(ethylene glycol) diblock copolymer micelles for dual chemo-photodynamic therapies. Biomaterials. 29 (26), 3599-3608 (2008).
  7. Chen, B., Pogue, B. W., Hasan, T. Liposomal delivery of photosensitising agents. Expert Opin Drug Deliv. 2 (3), 477-487 (2005).
  8. Lee, S. J., et al. Comparative study of photosensitizer loaded and conjugated glycol chitosan nanoparticles for cancer therapy. J Control Release. 152 (1), 21-29 (2011).
  9. Chang, J. E., et al. Anticancer efficacy of photodynamic therapy with hematoporphyrin-modified, doxorubicin-loaded nanoparticles in liver cancer. J. Photochem. Photobiol. 140, 49-56 (2014).
  10. Chang, J. E., Cho, H. J., Yi, E., Kim, D. D., Jheon, S. Hypocrellin B and paclitaxel-encapsulated hyaluronic acid-ceramide nanoparticles for targeted photodynamic therapy in lung cancer. J. Photochem. Photobiol. 158, 113-121 (2016).
  11. Wang, A. Z., Langer, R., Farokhzad, O. C. Nanoparticle delivery of cancer drugs. Annu. Rev. Med. 63, 185-198 (2012).
  12. Matsumura, Y., Maeda, H. A new concept for macromolecular therapeutics in cancer chemotherapy: mechanism of tumoritropic accumulation of proteins and the antitumor agent smancs. Cancer Res. 46 (12 Pt 1), 6387-6392 (1986).
  13. Penno, M. B., et al. Expression of CD44 in human lung tumors. Cancer Res. 54 (5), 1381-1387 (1994).
  14. Wilkins, R., Kutzner, B., Truong, M., Sanchez-Dardon, J., McLean, J. Analysis of radiation-induced apoptosis in human lymphocytes: Flow cytometry using Annexin V and propidium iodide versus the neutral comet assay. Cytometry. 48 (1), 14-19 (2002).
  15. Bannas, P., et al. Validation of nanobody and antibody based in vivo tumor xenograft NIRF-imaging experiments in mice using ex vivo flow cytometry and microscopy. J Vis Exp. (98), e52462 (2015).
  16. Fischer, A. H., Jacobson, K. A., Rose, J., Zeller, R. Hematoxylin and eosin staining of tissue and cell sections. Cold Spring Harbor Protocols. (5), (2008).
  17. Lam, S. Photodynamic therapy of lung cancer. Semin Oncol. 21 (6 Suppl 15), 15-19 (1994).
  18. Simone, C. B., et al. Photodynamic therapy for the treatment of non-small cell lung cancer. J Thorac Dis. 4 (1), 63-75 (2012).

Tags

Keywords: Photodynamic TherapyLung CancerNanoparticlesPhotosensitizerAnticancer DrugHyaluronic Acid-ceramideA549 Cell LineIn VitroIn VivoTuberculosisUlcersDermatology
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Chang, J., Cho, H., Jheon, S. Anticancer Efficacy of Photodynamic Therapy with Lung Cancer-Targeted Nanoparticles. J. Vis. Exp. (118), e54865, doi:10.3791/54865 (2016).
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