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竹红菌素B及其衍生物作为癌症光动力治疗敏化剂的临床前评估:进展更新

Preclinical assessment of hypocrellin B and hypocrellin B derivatives as sensitizers for photodynamic therapy of cancer: progress update.

作者信息

Miller G G, Brown K, Ballangrud A M, Barajas O, Xiao Z, Tulip J, Lown J W, Leithoff J M, Allalunis-Turner M J, Mehta R D, Moore R B

机构信息

Department of Surgery, University of Alberta, Edmonton, Canada.

出版信息

Photochem Photobiol. 1997 Apr;65(4):714-22. doi: 10.1111/j.1751-1097.1997.tb01915.x.

Abstract

Hypocrellins are perylenequinone pigments with substantial absorption in the red spectral region and high singlet oxygen yield. They are available in pure monomeric form and may be derivatized to optimize properties of red light absorption, tissue biodistribution and toxicity. In vitro screening of synthetic derivatives of the naturally occurring compound, hypocrellin B (HB), for optimal properties of cyto-(dark) toxicity and phototoxicity resulted in selection of three compounds for preclinical evaluation: HBEA-R1 (ethanolaminated HB), HBBA-R2 (butylaminated HB) and HBDP-R1 [2-(N,N-dimethylamino)-propylamine-HB]. Extinction coefficients at 630 nm (epsilon 630) are 6230, 6190 and 4800, respectively; and 1O2 quantum yields, phi, 0.60, 0.32 and 0.42. Intracellular uptake is essentially complete within 2 h (HBEA-R1, HBBA-R2) and 20 h (HBDP-R1). Greatest uptake is associated with lysosomes and Golgi. The HBEA-R1 and HBBA-R2 elicit phototoxicity in vitro primarily via the type II mechanism, with some type I activity under stringently hypoxic conditions. Transcutaneous phototherapy with HBEA-R1 permanently ablates EMT6/Ed tumors growing in the flanks of Balb/c mice, with minimal cutaneous effects. The HBBA-R2 does not elicit mutagenic activity in strains TA98 and TA100 of Salmonella typhimurium. Further development of selected hypocrellin derivatives as photosensitizers for photodynamic therapy is warranted.

摘要

竹红菌素是苝醌类色素,在红色光谱区域有大量吸收且单线态氧产率高。它们有纯单体形式,可进行衍生化以优化红光吸收、组织生物分布和毒性等特性。对天然存在的化合物竹红菌素B(HB)的合成衍生物进行体外筛选,以寻找细胞(暗)毒性和光毒性的最佳特性,结果选择了三种化合物进行临床前评估:HBEA-R1(乙醇胺化HB)、HBBA-R2(丁胺化HB)和HBDP-R1 [2-(N,N-二甲基氨基)-丙胺-HB]。在630 nm处的消光系数(ε630)分别为6230、6190和4800;单线态氧量子产率φ分别为0.60、0.32和0.42。细胞内摄取在2小时内(HBEA-R1、HBBA-R2)和20小时内(HBDP-R1)基本完成。最大摄取量与溶酶体和高尔基体有关。HBEA-R1和HBBA-R2在体外主要通过II型机制引发光毒性,在严格缺氧条件下有一些I型活性。用HBEA-R1进行经皮光疗可永久消除Balb/c小鼠侧腹生长的EMT6/Ed肿瘤,皮肤影响最小。HBBA-R2在鼠伤寒沙门氏菌TA98和TA100菌株中不引发诱变活性。有必要进一步开发选定的竹红菌素衍生物作为光动力疗法的光敏剂。

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