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热疗对恶性肿瘤的影响。

Effects of hyperthermia in a malignant tumor.

作者信息

Fajardo L F, Egbert B, Marmor J, Hahn G M

出版信息

Cancer. 1980 Feb;45(3):613-23. doi: 10.1002/1097-0142(19800201)45:3<613::aid-cncr2820450331>3.0.co;2-e.

DOI:10.1002/1097-0142(19800201)45:3<613::aid-cncr2820450331>3.0.co;2-e
PMID:7353209
Abstract

The mechanisms of immediate and delayed tumor cell killing by hyperthermia were investigated in EMT-6 neoplasms implanted in BALB/cKa mice. Radiofrequency electromagnetic fields were used to achieve a curative local dose of 44 degrees C for 30 minutes. The tumors were sampled sequentially, during and after heat therapy, and studied by light and elecron microscopy. Assays for cell survival, including cell cultures, were performed at various times after completion of therapy. Focal cytoplasmic swelling, rupture of the plasma membrane and peripheral migration of heterochromatin were observed 5 minutes after initiation of therapy and led to cytoplasmic fragmentation by the end of the treatment period (30 minutes). Necrosis of most cells occurred 2--6 hours after the end of treatment. At 48 hours, there were no recognizable tumor cells. A scar replaced the tumor bed 14 days later. Viable (clonogenic) tumor cells were still 2% of control levels at the end of therapy and then progressively decreased to 0.0003% at 48 hours, confirming the morphologic observations and indicating that factors other than the direct effect of heat on tumor cells contributed to complete tumor eradication. Our findings, coupled with previous studies, suggest that the immediate heat induced necrosis in this tumor occurs through the mechanisms of physical changes in the plasma membrane. The delayed (post-therapy) cell death is likely due to modifications in the environment of the tumor bed.

摘要

在植入BALB/cKa小鼠体内的EMT-6肿瘤中,研究了热疗对肿瘤细胞的即时和延迟杀伤机制。使用射频电磁场将局部治疗剂量提高到44摄氏度并持续30分钟以达到治愈效果。在热疗期间及热疗后,对肿瘤进行连续取样,并通过光学显微镜和电子显微镜进行研究。在治疗完成后的不同时间进行细胞存活检测,包括细胞培养。治疗开始5分钟后,观察到局灶性细胞质肿胀、质膜破裂和异染色质向周边迁移,到治疗期结束(30分钟)时导致细胞质碎片化。大多数细胞在治疗结束后2至6小时发生坏死。48小时后,已无法识别出肿瘤细胞。14天后,肿瘤床被瘢痕取代。治疗结束时,存活(克隆形成)的肿瘤细胞仍为对照水平的2%,然后在48小时时逐渐降至0.0003%,这证实了形态学观察结果,并表明除了热对肿瘤细胞的直接作用外,其他因素也有助于完全消除肿瘤。我们的研究结果与先前的研究相结合,表明该肿瘤中热诱导的即时坏死是通过质膜的物理变化机制发生的。延迟(治疗后)细胞死亡可能是由于肿瘤床环境的改变。

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Effects of hyperthermia in a malignant tumor.热疗对恶性肿瘤的影响。
Cancer. 1980 Feb;45(3):613-23. doi: 10.1002/1097-0142(19800201)45:3<613::aid-cncr2820450331>3.0.co;2-e.
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