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激光-ICG 光热疗法联合多柔比星化疗对卵巢癌细胞的影响。

Combined effects of laser-ICG photothermotherapy and doxorubicin chemotherapy on ovarian cancer cells.

机构信息

Department of Biomedical Engineering, Florida International University, 10555 West Flagler Street, Miami, FL 33174, USA.

出版信息

J Photochem Photobiol B. 2009 Dec 2;97(3):138-44. doi: 10.1016/j.jphotobiol.2009.09.001. Epub 2009 Sep 11.

Abstract

Doxorubicin (DOX) is an anthracycline antibiotic widely used in cancer chemotherapy. Its use is limited by cardiac toxicity and drug resistance. Hyperthermia can aid the functionality of DOX, but current hyperthermia delivery methods are hard to apply selectively and locally. The slow temperature increase associated with the external heating may lead to thermal tolerance in cancer cells. The FDA approved dye indocynine green (ICG) has been demonstrated to absorb near-infrared (NIR) light at 808 nm (ideal for tissue penetration) and emit the energy as heat, making it an ideal agent for localized hyperthermia with a rapid rate of temperature increase. The purpose of this study was to investigate the in vitro cytotoxic effect of combined chemotherapy and hyperthermia to a DOX resistant ovarian cancer cell line (SKOV-3). The effect of two different heating methods, ICG induced rapid rate heating and an incubator induced slow rate heating, were compared. All the experiments were conducted in 96-well plates. Cells were subjected to different concentrations of DOX and 60 min 43 degrees C incubation or 5 microM of ICG with 1 min 808 nm NIR laser. SRB assay was used to measure cell proliferation. ICG itself without laser irradiation was not toxic to SKOV-3 cells. The two types of hyperthermia individually produced similar cytotoxicity. DOX by itself was toxic with an IC(50) value of about 5 microM. Hyperthermia in combination with DOX achieved significantly greater cell killing/growth inhibition at all DOX concentrations compared to DOX alone. A subadditive cytotoxic effect was observed by combining DOX and 60 min 43 degrees C incubation which lead to a lowered DOX IC(50) value of about 1 microM. This value was even lower with 1 min laser-ICG photothermotherapy (0.1 microM) and, though not statistically significant, a synergistic effect may exist between DOX and laser-ICG photothermotherapy. The rate of heating may have an effect on chemotherapy-hyperthermia interaction. In conclusion, the combination of photothermal therapy and chemotherapy may provide a valuable tool for cancer treatment with minimized side effect.

摘要

多柔比星(DOX)是一种广泛用于癌症化疗的蒽环类抗生素。其应用受到心脏毒性和耐药性的限制。热疗可以增强 DOX 的功能,但目前的热疗输送方法难以选择性和局部应用。与外部加热相关的缓慢升温可能导致癌细胞产生热耐受性。美国食品和药物管理局批准的染料吲哚青绿(ICG)已被证明在 808nm 处吸收近红外(NIR)光(适合组织穿透)并将能量作为热量释放,使其成为具有快速升温率的局部热疗的理想试剂。本研究旨在研究联合化疗和热疗对 DOX 耐药卵巢癌细胞系(SKOV-3)的体外细胞毒性作用。比较了两种不同的加热方法,即 ICG 诱导的快速升温法和孵育箱诱导的缓慢升温法。所有实验均在 96 孔板中进行。细胞分别接受不同浓度的 DOX 和 60 分钟 43°C 孵育或 5μM 的 ICG 与 1 分钟 808nm NIR 激光。SRB 测定法用于测量细胞增殖。没有激光照射的 ICG 本身对 SKOV-3 细胞没有毒性。两种类型的热疗单独使用时具有相似的细胞毒性。DOX 本身具有毒性,IC50 值约为 5μM。与单独使用 DOX 相比,DOX 联合热疗在所有 DOX 浓度下均能显著增强细胞杀伤/生长抑制作用。联合 DOX 和 60 分钟 43°C 孵育可观察到亚相加细胞毒性作用,导致 DOX IC50 值降低至约 1μM。使用 1 分钟激光-ICG 光热疗法(0.1μM)时,该值甚至更低,尽管统计学意义不显著,但 DOX 和激光-ICG 光热疗法之间可能存在协同作用。加热速率可能会影响化疗-热疗相互作用。总之,光热疗法与化疗相结合可能为癌症治疗提供一种有价值的工具,同时最大限度地减少副作用。

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