A magnetic vehicle realized tumor cell-targeted radiotherapy using low-dose radiation

A magnetic vehicle realized tumor cell-targeted radiotherapy using low-dose radiation

Radiotherapy, a common cancer treatment, often adversely affects the surrounding healthy tissue and/or cells. Some tumor tissue-focused radiation therapies have been developed to lower radiation-induced lesion formation; however, achieving tumor cell-targeted radiotherapy (i.e., precisely focusing t...

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Veröffentlicht in:Journal of controlled release 2016-03, Vol.226, p.182-192
Hauptverfasser: Chen, Hsiao-Ping, Tung, Fu-I, Chen, Ming-Hong, Liu, Tse-Ying
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Chitosan - analogs & derivatives
Chitosan - chemistry
Chlorin e6
Drug Delivery Systems
Drug vehicle
Female
Ferric Compounds - chemistry
Folic Acid - chemistry
HeLa Cells
Humans
Magnetic guidance
Magnets - chemistry
Mice, Nude
Micelles
Neoplasms - pathology
Neoplasms - radiotherapy
Porphyrins - administration & dosage
Porphyrins - therapeutic use
Radiation-Sensitizing Agents - administration & dosage
Radiation-Sensitizing Agents - therapeutic use
Targeted delivery
Tumor cell-targeted radiotherapy
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Zusammenfassung:Radiotherapy, a common cancer treatment, often adversely affects the surrounding healthy tissue and/or cells. Some tumor tissue-focused radiation therapies have been developed to lower radiation-induced lesion formation; however, achieving tumor cell-targeted radiotherapy (i.e., precisely focusing the radiation efficacy to tumor cells) remains a challenge. In the present study, we developed a novel tumor cell-targeted radiotherapy, named targeted sensitization-enhanced radiotherapy (TSER), that exploits tumor-specific folic acid-conjugated carboxymethyl lauryl chitosan/superparamagnetic iron oxide (FA-CLC/SPIO) micelles to effectively deliver chlorin e6 (Ce6, a sonosensitizer) to mitochondria of HeLa cells under magnetic guidance. For the in vitro tests, the sensitization of Ce6 induced by ultrasound, that could weaken the radiation resistant ability of tumor cells, occurred only in Ce6-internalizing tumor cells. Therefore, low-dose X-ray irradiation, that was not harmful to normal cells, could exert high tumor cell-specific killing ability. The ratio of viable normal cells to tumor cells was increased considerably, from 7.8 (at 24h) to 97.1 (at 72h), after they had received TSER treatment. Our data suggest that TSER treatment significantly weakens tumor cells, resulting in decreased viability in vitro as well as decreased in vivo subcutaneous tumor growth in nude mice, while the adverse effects were minimal. Taken together, TSER treatment appears to be an effective, clinically feasible tumor cell-targeted radiotherapy that can solve the problems of traditional radiotherapy and photodynamic therapy. A newly proposed tumor-cell targeted radiotherapy, Ce6 was effectively delivered to mitochondria and subsequently sensitized by ultrasound to lower radiation resistance, was employed to maximize the destruction of tumor cells and minimize the harm to normal cells with the use of low dose of therapeutic agent and radiation. [Display omitted]
ISSN:0168-3659
1873-4995
DOI:10.1016/j.jconrel.2016.02.025