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本文引用的文献

1
Blood flow changes in transplanted mouse tumours and skin after mild hyperthermia.轻度热疗后移植小鼠肿瘤和皮肤的血流变化
Br J Radiol. 1983 Jul;56(667):477-82. doi: 10.1259/0007-1285-56-667-477.
2
A study of the effects of prior heat treatment on the skin reaction of mouse feet after heat alone or combined with X-rays: influence of misonidazole.一项关于预先热处理对单独热刺激或热与X射线联合刺激后小鼠足部皮肤反应的影响的研究:米索硝唑的作用
Radiother Oncol. 1984 Aug;2(2):159-70. doi: 10.1016/s0167-8140(84)80052-3.
3
Alterations in rubidium-86 extraction in normal mouse tissues after irradiation. An estimate of long-term blood flow changes in kidney, lung, liver, skin and muscle.照射后正常小鼠组织中铷 - 86摄取的变化。对肾脏、肺、肝脏、皮肤和肌肉中长期血流变化的估计。
Radiat Res. 1973 Jan;53(1):88-101.
4
Dose-response relationships for photodynamic injury to murine skin.光动力对小鼠皮肤损伤的剂量-反应关系。
Br J Radiol. 1986 Mar;59(699):257-61. doi: 10.1259/0007-1285-59-699-257.
5
Destruction of rat mammary tumor and normal tissue microcirculation by hematoporphyrin derivative photoradiation observed in vivo in sandwich observation chambers.在夹心观察室中对大鼠进行体内观察,发现血卟啉衍生物光辐射可破坏大鼠乳腺肿瘤及正常组织的微循环。
Cancer Res. 1986 May;46(5):2532-40.
6
Effect of multiple heatings on the blood flow in RIF-1 tumours, skin and muscle of C3H mice.
Int J Hyperthermia. 1987 Nov-Dec;3(6):535-45. doi: 10.3109/02656738709140426.
7
Vascular function and the probability of skin necrosis after photodynamic therapy: an experimental study.光动力治疗后血管功能与皮肤坏死概率:一项实验研究
Br J Cancer. 1988 May;57(5):451-4. doi: 10.1038/bjc.1988.105.
8
The effect of fractionation of light treatment on necrosis and vascular function of normal skin following photodynamic therapy.光动力疗法后光治疗分次照射对正常皮肤坏死及血管功能的影响。
Br J Cancer. 1988 Sep;58(3):301-5. doi: 10.1038/bjc.1988.208.
9
Interaction of interstitial photodynamic therapy and interstitial hyperthermia in a rat rhabdomyosarcoma--a pilot study.大鼠横纹肌肉瘤中间质光动力疗法与间质热疗的相互作用——一项初步研究
Int J Radiat Oncol Biol Phys. 1988 Jan;14(1):139-45. doi: 10.1016/0360-3016(88)90061-2.
10
Hyperthermic potentiation of photodynamic therapy employing Photofrin I and II: comparison of results using three animal tumor models.
Lasers Surg Med. 1987;7(1):12-22. doi: 10.1002/lsm.1900070104.

单独及联合应用热疗和光动力疗法后小鼠皮肤的血管功能和组织损伤

Vascular function and tissue injury in murine skin following hyperthermia and photodynamic therapy, alone and in combination.

作者信息

Moore J V, West C M, Haylett A K

机构信息

Paterson Institute for Cancer Research (Cancer Research Campaign), Christie Hospital (NHS) Trust, Manchester, UK.

出版信息

Br J Cancer. 1992 Dec;66(6):1037-43. doi: 10.1038/bjc.1992.406.

DOI:10.1038/bjc.1992.406
PMID:1457342
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1978046/
Abstract

The murine tail has been used as a model for injury to skin when hyperthermia (HT) and photodynamic therapy (PDT) using haematoporphyrin derivative, are used in combination. Skin injury by either agent alone was quantitated by the probability of tail necrosis as a function of dose of agent. 'Tolerance' doses of each modality were given and changes in skin vascular function were measured by the rate of clearance of 133Xenon. This was promptly inhibited but restored to normal by 7 days. The absolute numbers of hypodermal vessels of different sizes were measured in tail cross-sections and capillary numbers were found to be greatly reduced between 1 and 7 days, and restored to normal by 21-28 days. When a tolerance dose of PDT was followed at 1, 7, 21 and 28 days by test doses of HT, or vice versa, marked enhancements in probability of necrosis were observed when the interval was 1 or 7 days (Enhancement ratio (ER)PDT-HT = 1.5 and ERHT-PDT = 1.8). Prolonging the interval between modalities to 21-28 days spared the tissue (ERHT-PDT/21 DAYS = 1.1; ERPDT-HT/28 DAYS = 1.0). Close temporal apposition of PDT and HT, such as has been advocated to improve tumour control, may also increase injury to normal tissue through vascular effects common to both.

摘要

当联合使用热疗(HT)和使用血卟啉衍生物的光动力疗法(PDT)时,小鼠尾巴已被用作皮肤损伤的模型。单独使用任何一种药物引起的皮肤损伤,都通过尾巴坏死的概率作为药物剂量的函数来定量。给予每种治疗方式的“耐受”剂量,并通过133氙的清除率来测量皮肤血管功能的变化。这种变化立即受到抑制,但在7天时恢复正常。在尾巴横切面上测量不同大小的皮下血管的绝对数量,发现毛细血管数量在1至7天之间大幅减少,并在21至28天恢复正常。当在1、7、21和28天给予PDT耐受剂量后,接着给予HT测试剂量,反之亦然,当间隔为1或7天时,观察到坏死概率有显著提高(增强比(ER)PDT-HT = 1.5,ERHT-PDT = 1.8)。将两种治疗方式之间的间隔延长至21至28天可使组织免受损伤(ERHT-PDT/21天 = 1.1;ERPDT-HT/28天 = 1.0)。PDT和HT在时间上紧密相邻,如为改善肿瘤控制所提倡的那样,也可能通过两者共有的血管效应增加对正常组织的损伤。