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使用单-L-天冬酰胺基二氢卟吩e6的光动力疗法对血管收缩、血管渗漏及肿瘤反应的影响。

Effects of photodynamic therapy using mono-L-aspartyl chlorin e6 on vessel constriction, vessel leakage, and tumor response.

作者信息

McMahon K S, Wieman T J, Moore P H, Fingar V H

机构信息

Department of Surgery, University of Louisville, Kentucky 40292.

出版信息

Cancer Res. 1994 Oct 15;54(20):5374-9.

PMID:7923168
Abstract

The effect of photodynamic therapy using mono-L-aspartyl chlorin e6 (NPe6) on both direct cytotoxicity and vascular damage was examined. Sprague-Dawley rats bearing chondrosarcoma tumor were given i.v. injections of 5 or 10 mg/kg NPe6 and exposed to 135-J/cm2 664-nm laser light either 4 or 24h after NPe6 injection. The percentage of viable tumor cells was estimated either immediately after the completion of light treatment or 24 h after treatment using a 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide assay. Measurements of arteriole constriction and venule leakage in normal cremaster tissues were made during and 1 h after the light treatment. Tumor response was evaluated for the 4 different NPe6 dose and time combinations. Both direct tumor cytotoxicity and vascular stasis were observed during light treatment. Vessel leakage did not occur. Blood flow stasis was a result of platelet aggregation and the mechanical obstruction of flow rather than vessel constriction. The magnitude of direct cytotoxicity and vascular response was dependent on both the amount of NPe6 delivered and the delay between injection and light treatment. Tumor cure was found in animals either when given high NPe6 doses or when treated early after NPe6 injection. Treatment regimens which maximized the effect of both vascular stasis and direct tumor cytotoxicity were found to produce the best tumor response. Dose combinations which produced vascular stasis with minimal early cytotoxicity did not result in cure. The combined mechanisms of damage after photodynamic therapy using NPe6 suggests that this photosensitizer may have specific advantages for clinical use and provides a benchmark for the development of new photosensitizers.

摘要

研究了使用单-L-天冬氨酸氯啉e6(NPe6)的光动力疗法对直接细胞毒性和血管损伤的影响。给患有软骨肉瘤肿瘤的Sprague-Dawley大鼠静脉注射5或10mg/kg的NPe6,并在注射NPe6后4或24小时暴露于135-J/cm2 664-nm激光下。在光疗完成后立即或治疗后24小时,使用3-(4,5-二甲基噻唑-2-基)-2,5-二苯基四氮唑溴盐测定法估计存活肿瘤细胞的百分比。在光疗期间和光疗后1小时,对正常提睾肌组织中的小动脉收缩和小静脉渗漏进行测量。评估了4种不同NPe6剂量和时间组合的肿瘤反应。在光疗期间观察到了直接肿瘤细胞毒性和血管淤滞。未发生血管渗漏。血流淤滞是血小板聚集和血流机械阻塞的结果,而非血管收缩。直接细胞毒性和血管反应的程度取决于所递送的NPe6的量以及注射与光疗之间的延迟。当给予高剂量NPe6或在注射NPe6后早期进行治疗时,在动物中发现了肿瘤治愈情况。发现使血管淤滞和直接肿瘤细胞毒性的效果最大化的治疗方案产生了最佳的肿瘤反应。产生血管淤滞且早期细胞毒性最小的剂量组合并未导致治愈。使用NPe6的光动力疗法后的联合损伤机制表明,这种光敏剂可能具有临床应用的特定优势,并为新型光敏剂的开发提供了一个基准。

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