环磷酰胺增强5-氨基乙酰丙酸光动力疗法。

Cancer biochemistry biophysics Pub Date : 1998-06-01
A Casas, H Fukuda, A M Batlle
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引用次数: 0

摘要

我们利用实验室开发的体内外模型研究了5-氨基乙酰丙酸(ALA)光动力疗法(PDT)与抗肿瘤药物联合使用的疗效。选择烷基化剂环磷酰胺(CY)是因为有证据表明该药物具有致卟啉的性质。携带可移植乳腺腺癌的雄性BALB/c小鼠分别给予35 mg de CY/kg wt和9 mg/kg wt瘤内注射。在最后一次注射CY后16、22和40小时处死动物,取2 mg肿瘤外植体在含有0.6 mM ALA的培养基中孵育2小时;然后用氦氖激光照射。然后分别在正常小鼠的左右两侧皮下注射1 mm3的辐照组织和未辐照组织。肿瘤植入后第10天肿瘤生长情况确定治疗效果。在本实验条件下,在末次注射后40小时再用CY处理外植体,其效果可提高30%。同时测定了注射小鼠肝脏和肿瘤等组织中卟啉的含量;与未注射CY的小鼠相比,CY i.p.注射后40和22小时,除了肿瘤和肝脏略有增加外,其他任何组织均未见变化。这些结果表明,未来的治疗应鼓励结合ALA内源性形成的卟啉和环磷酰胺等抗肿瘤药物的肿瘤定位特性。
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Potentiation of the 5-aminolevulinic acid-based photodynamic therapy with cyclophosphamide.

We have investigated the efficacy of the Photodynamic Therapy (PDT) from 5-aminolevulinic acid (ALA) in combination with an antineoplastic agent using an in vitro-in vivo model developed in our laboratory. The alkylant cyclophosphamide (CY) was chosen because there is evidence of the porphyrinogenic properties of this drug. Male BALB/c mice bearing a transplantable mammary adenoarcinoma were given two doses of 35 mg de CY/kg wt. i.p. and 9 mg/kg wt intratumorally. At 16, 22 and 40 hrs after the last injection of CY the animals were sacrificed and explants of 2 mg of tumor were incubated 2 hrs in a medium containing 0.6 mM ALA; and then irradiated with a He-Ne laser. Innocula of 1 mm3 of irradiated and non-irradiated tissue were then injected subcutaneously under the right and left flanks of a normal mouse, respectively. The efficacy of the treatment was determined following the growth of the tumor from day 10 after tumor implantation. Under the present conditions a 30% increased efficacy was observed in the case of the explants treated with CY 40 hrs after the last i.p. injection. Porphyrins in the liver and tumor and other tissues of the injected mice were also determined; except for a slight increase in tumor and liver, 40 and 22 hrs after CY i.p. injection respectively, no other changes were observed in any tissue, as compared with not CY treated mice. These results indicate that future treatment, combining the tumor localizing properties of endogenously formed porphyrins from ALA and antineoplasic drugs such as cyclophosphamide, should be encouraged.

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