Boyle R W, Rousseau J, Kudrevich S V, Obochi M, van Lier J E
MRC Group in the Radiation Sciences, Faculty of Medicine, Université de Sherbrooke, Québec, Canada.
Br J Cancer. 1996 Jan;73(1):49-53. doi: 10.1038/bjc.1996.9.
Hexadecafluorinated zinc phthalocyanine (ZnPcF16), an analogue of zinc phthalocyanine (ZnPc) in which all hydrogen atoms have been substituted by fluorine, was prepared as a single isomeric product via the condensation of tetrafluorophthalonitrile with zinc acetate. Fluorination renders the ZnPc soluble in most common solvents. The photodynamic properties and pharmacokinetics of the ZnPcF16 were evaluated in EMT-6 tumour-bearing Balb/c mice using 65Zn-radiolabelled analogues. Both dyes, administered i.v. at 1 mumol kg-1 as Cremophor emulsions, revealed good tumour uptake [approximately 8-9 per cent of the injected dose per g tissue (%IDg-1)] at 24 h post injection (p.i.), with the fluorinated dye reaching higher concentrations (approximately 11%IDg-1) at 48 h p.i. and subsequently higher tumour-blood ratios due to rapid blood clearance. ZnPcF16 at a dose of 5 mumol kg-1 (4.3 mg kg-1) induced complete tumour regression after phototherapy (24 h p.i., 650-700 nm band, 360 J cm-2, 200 mW cm-1). At a dose of 2 mumol kg-1 and phototherapy at 24 h p.i., the tumour volume doubling time increased to 11 days vs 6 days for the control tumours. A similar tumour growth delay was observed when phototherapy was conducted at 48 h or 72 h after dye injection implying that tumour response correlates with tumour dye concentrations rather than serum concentrations. As a result of its low solubility, the administered dose of ZnPc was limited to 1 mumol kg-1 and at this drug level significant tumour response was only observed when the dye was solubilised as the pyridinium salt. Isolation of the neoplastic cells after in vivo dye administration and in vitro exposure to red light followed by a colony formation assay showed that the ZnPcF16 exhibited a 1-2 order of magnitude higher potential for direct cell killing as compared with Photofrin and about a five times lower efficiency than ZnPc. However, all three photosensitisers induced complete occlusion of tumour vasculature immediately after PDT, suggesting that tumour regression mainly resulted from vascular stasis. The ZnPcF16 offers several advantages over ZnPc for clinical applications, including improved solubility in most solvents, resulting in facilitated drug formation, favourable pharmacokinetics as well as the potential use in fluorine magnetic resonance (F-MR) imaging.
十六氟代锌酞菁(ZnPcF16)是锌酞菁(ZnPc)的类似物,其中所有氢原子均被氟取代,它是通过四氟邻苯二甲腈与醋酸锌缩合制备而成的单一异构体产物。氟化使ZnPc可溶于大多数常见溶剂。使用65Zn放射性标记的类似物在荷EMT - 6肿瘤的Balb/c小鼠中评估了ZnPcF16的光动力特性和药代动力学。两种染料均以1 μmol kg-1的剂量作为聚氧乙烯蓖麻油乳剂静脉注射,在注射后24小时(p.i.)显示出良好的肿瘤摄取[约为每克组织注射剂量的8 - 9%(%IDg-1)],氟化染料在注射后48小时达到更高浓度(约11%IDg-1),随后由于血液快速清除而具有更高的肿瘤 - 血液比。剂量为5 μmol kg-1(4.3 mg kg-1)的ZnPcF16在光疗后(注射后24小时,650 - 700 nm波段,360 J cm-2,200 mW cm-1)诱导肿瘤完全消退。在注射后24小时给予2 μmol kg-1的剂量并进行光疗时,肿瘤体积倍增时间增加到11天,而对照肿瘤为6天。当在染料注射后48小时或72小时进行光疗时,观察到类似的肿瘤生长延迟,这意味着肿瘤反应与肿瘤染料浓度而非血清浓度相关。由于其低溶解度,ZnPc的给药剂量限制为1 μmol kg-1,在此药物水平下,仅当染料以吡啶盐形式溶解时才观察到显著的肿瘤反应。在体内给予染料并在体外暴露于红光后分离肿瘤细胞,随后进行集落形成试验表明,与Photofrin相比,ZnPcF16的直接细胞杀伤潜力高1 - 2个数量级,且效率比ZnPc低约五倍。然而,所有三种光敏剂在光动力疗法(PDT)后立即诱导肿瘤血管完全闭塞,这表明肿瘤消退主要是由于血管淤滞。与ZnPc相比,ZnPcF16在临床应用中具有几个优点,包括在大多数溶剂中溶解度提高,从而便于药物制剂的制备,有利的药代动力学以及在氟磁共振(F - MR)成像中的潜在应用。
