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用作光动力治疗可移植性N-2-氟烯丙基-N'-(4-羟丁基)亚硝脲(FANFT)诱导的膀胱肿瘤光敏剂的紫红素衍生物的剂量反应分析。

A dose response analysis of purpurin derivatives used as photosensitizers for the photodynamic treatment of transplantable FANFT induced urothelial tumors.

作者信息

Selman S H, Garbo G M, Keck R W, Kreimer-Birnbaum M, Morgan A R

出版信息

J Urol. 1987 Jun;137(6):1255-7. doi: 10.1016/s0022-5347(17)44476-4.

DOI:10.1016/s0022-5347(17)44476-4
PMID:3586170
Abstract

Rats engrafted with transplantable N-[4-(5-nitro-2-furyl)-2-thiazolyl] formamide (FANFT) induced urothelial tumors were treated with purpurin derivatives and red light (greater than 590 nm., 360 joules/cm.2). Treated and control tumors were harvested 12 days after treatment and dry weights compared. At doses of 5.0 micrograms./gm. and 2.5 micrograms./gm. body weight, the purpurins designated NT1 and NT2, when combined with light, caused statistically significant (p less than 0.02) tumor regression when compared to light shielded controls. At 1.0 micrograms./gm. body weight, NT1 and light also induced significant tumor regression (p less than 0.02). Purpurins, which have strong absorption bands above 650 nm. and can be synthesized with a high degree of purity, appear to have potential as photosensitizers for photodynamic therapy.

摘要

将可移植的N-[4-(5-硝基-2-呋喃基)-2-噻唑基]甲酰胺(FANFT)诱导的尿路上皮肿瘤移植到大鼠体内,然后用紫红素衍生物和红光(大于590纳米,360焦耳/平方厘米)进行治疗。治疗12天后收集治疗组和对照组的肿瘤并比较干重。在剂量为5.0微克/克和2.5微克/克体重时,名为NT1和NT2的紫红素与光联合使用时,与遮光对照组相比,导致肿瘤出现具有统计学意义(p小于0.02)的消退。在剂量为1.0微克/克体重时,NT1与光联合使用也诱导了显著的肿瘤消退(p小于0.02)。紫红素在650纳米以上有强吸收带,并且能够以高纯度合成,似乎有潜力作为光动力疗法的光敏剂。

相似文献

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A dose response analysis of purpurin derivatives used as photosensitizers for the photodynamic treatment of transplantable FANFT induced urothelial tumors.用作光动力治疗可移植性N-2-氟烯丙基-N'-(4-羟丁基)亚硝脲(FANFT)诱导的膀胱肿瘤光敏剂的紫红素衍生物的剂量反应分析。
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引用本文的文献

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Current status of photodynamic therapy in oncology.光动力疗法在肿瘤学中的现状
Drugs. 1994 Oct;48(4):510-27. doi: 10.2165/00003495-199448040-00003.
2
Hydroporphyrins of the meso-tetra(hydroxyphenyl)porphyrin series as tumour photosensitizers.中-四(羟苯基)卟啉系列的氢卟啉作为肿瘤光敏剂
Biochem J. 1989 Jul 1;261(1):277-80. doi: 10.1042/bj2610277.