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新型前列腺癌局部光动力疗法:脂质体包封的羟基铝酞菁。

Novel topical photodynamic therapy of prostate carcinoma using hydroxy-aluminum phthalocyanine entrapped in liposomes.

机构信息

Charles University in Prague, Third Faculty of Medicine, Prague, Czech Republic.

出版信息

Anticancer Res. 2013 Apr;33(4):1563-8.

PMID:23564798
Abstract

BACKGROUND

Clinically-approved anticancer photodynamic therapy (PDT) is now extensively studied for various cancer diagnoses. We focused on the treatment efficacy of topical administration of hydroxy-aluminum phthalocyanine (AlOH-PC) entrapped in liposomes against in vivo models of prostate carcinomas.

MATERIALS AND METHODS

LNCaP and PC3 cells were subcutaneously injected into the right flank of athymic nude mice. Mice with grown tumours were used for in vivo efficacy studies. Firstly, we applied different doses of AlOH-PC to less aggressive LNCaP tumours to determine the effective dose. In later studies, we focused on more aggressive prostate tumours (PC3) using doses of liposomal-AlOH-PC gel formulation. Topical application of photosensitizers was followed by PDT irradiation (600-700 nm, 635 nm peak). Tumour growth was measured three times-a-week.

RESULTS

Comparison of PDT of aggressive PC3 and less aggressive LNCaP prostate carcinomas showed that both tumour types are sensitive and treatable by liposomal formulation of AlOH-PC. For LNCaP tumours the efficient dose (100% experimental animals cured, n=8/8) was 4.5 mg/ml of AlOH-PC in the gel. Whereas, in the case of PC3 carcinomas, a dose of 4 mg/ml significantly postponed tumour growth, but no animals were cured (n=0/8); a sufficient curative dose (100% mice cured, n=8/8) was 6 mg/ml of AlOH-PC in the gel.

CONCLUSION

Liposomal AlOH-PC gel has potential for effective PDT of prostate carcinomas.

摘要

背景

临床上批准的抗癌光动力疗法(PDT)现在广泛用于各种癌症的诊断。我们专注于局部应用羟铝酞菁(AlOH-PC)包封在脂质体中对前列腺癌体内模型的治疗效果。

材料和方法

LNCaP 和 PC3 细胞被皮下注射到裸鼠的右侧侧腹。生长肿瘤的小鼠用于体内疗效研究。首先,我们将不同剂量的 AlOH-PC 应用于侵袭性较低的 LNCaP 肿瘤,以确定有效剂量。在后来的研究中,我们使用脂质体 AlOH-PC 凝胶制剂的剂量,专注于侵袭性更强的前列腺肿瘤(PC3)。光敏剂的局部应用后进行 PDT 照射(600-700nm,635nm 峰)。每周三次测量肿瘤生长情况。

结果

比较侵袭性 PC3 和侵袭性较低的 LNCaP 前列腺癌的 PDT 结果表明,这两种肿瘤类型都对脂质体制剂的 AlOH-PC 敏感且可治疗。对于 LNCaP 肿瘤,有效剂量(100%实验动物治愈,n=8/8)为凝胶中 4.5mg/ml 的 AlOH-PC。然而,在 PC3 癌的情况下,4mg/ml 的剂量显著推迟了肿瘤生长,但没有动物治愈(n=0/8);足够的治愈剂量(100%小鼠治愈,n=8/8)为凝胶中 6mg/ml 的 AlOH-PC。

结论

脂质体 AlOH-PC 凝胶具有有效治疗前列腺癌的 PDT 潜力。

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