[Distribution studies of alpha-L-arabinofuranosidase already unstable at pH 7.0 (37 degrees C) in tumor-bearing mice in connection with its possible use to enhance the selectivity of the chemotherapy of malignant tumors].

Archiv fur Geschwulstforschung Pub Date : 1990-01-01
G Butschak, B Schulze, A Küster, T Niederhausen, U Niemeyer, A Graffi
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Abstract

Graffi et al. (1-3) had proposed the use of exogenous enzymes to toxify inactive transport forms of cancerostatic substances. For this purpose, the pH difference between normal tissues and the tumor was to be exploited, which can be essentially increased by the application of glucose and inorganic phosphate (5-7). Earlier studies using alpha-L-arabinofuranosidase obtained from Aspergillus niger have shown that the selectivity of tumor chemotherapy can be increased in this way (4). The alpha-L-arabinofuranosidases known to date are stabile in a wide pH range (9). However, in some moulds we found pH-labile enzymes of this kind that become irreversibly inactivated in the weakly alkaline or neutral pH range (10, 11). Studies on the distribution of the activity of a pH-labile alpha-L-arabinofuranosidase from Glomerella myabana in tumor-bearing mice have shown that this enzyme is rapidly eliminated from the organism, in contrast to the pH-stable alpha-L-arabinofuranosidase from A. niger. Apart from its excretion via kidney and liver, of importance is the inactivation of the enzyme in the normal tissues. The additional application of glucose strongly increased the activity of this enzyme both in the tumor and in normal tissues (12). By injecting alkaline solutions, stronger inactivation in normal tissues than in the tumor was achieved (13). In the present paper, distribution of an alpha-L-arabinofuranosidase from Fusarium species I 50 (11), inactive already at pH 7.0 (37 degrees C), was studied in tumor-bearing mice. The activity of this enzyme could be enriched under various conditions in the tumor, and especially favorable proved to be the additional application of a combination of glucose and inorganic phosphate. Under these conditions, a higher activity than in the tumor was demonstrable only in the kidney, which can possibly be eliminated in larger experimental animals by diuretics or an appropriate alkaline administration. The investigations have shown that the pH-labile alpha-L-arabinofuranosidases, especially those of Fusarium sp., due to their pharmacokinetic behavior are better suited for use in our therapy concept than the hitherto employed enzyme from A. niger. More recently, Tietze (16) has proposed a similar therapy concept, in which also the glucose-increased pH difference between tumor and normal tissue using tumor-own enzymes, exogenous enzymes as well as transport forms of cancerostatic agents spontaneously hydrolysing under weakly acidic pH conditions is to be exploited.

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[在pH 7.0(37℃)时已经不稳定的α - l -阿拉伯糖醛酸苷酶在荷瘤小鼠体内的分布研究,其可能用于增强恶性肿瘤化疗的选择性]。
Graffi等人(1-3)提出使用外源性酶来毒害无活性的抑癌物质的运输形式。为此,要利用正常组织和肿瘤之间的pH值差异,通过葡萄糖和无机磷酸盐的应用基本上可以增加pH值差异(5-7)。早期使用从黑曲霉中获得的α -l -阿拉伯糖醛酸苷酶的研究表明,肿瘤化疗的选择性可以通过这种方式增加(4)。迄今已知的α -l -阿拉伯糖醛酸苷酶在很宽的pH范围内是稳定的(9)。然而,在一些霉菌中,我们发现这种pH不稳定的酶在弱碱性或中性pH范围内会不可逆地失活(10,11)。对myabana肾小球中ph不稳定的α -l -阿拉伯糖醛酸苷酶在荷瘤小鼠体内的活性分布的研究表明,该酶能迅速从机体中消除,而与此相反的是来自a . niger的ph稳定的α -l -阿拉伯糖醛酸苷酶。除了通过肾脏和肝脏排泄外,重要的是正常组织中酶的失活。葡萄糖的额外应用大大增加了肿瘤和正常组织中这种酶的活性(12)。通过注射碱性溶液,在正常组织中的失活比在肿瘤中的失活更强(13)。本文研究了在pH 7.0(37℃)条件下失活的镰刀菌I 50(11)中α - l -阿拉伯糖醛酸苷酶在荷瘤小鼠中的分布。该酶的活性可以在肿瘤的各种条件下得到增强,特别是在葡萄糖和无机磷酸盐的联合应用中被证明是特别有利的。在这些条件下,仅在肾脏中表现出比肿瘤中更高的活性,在较大的实验动物中可能通过利尿剂或适当的碱性管理来消除。研究表明,ph不稳定的α -l -阿拉伯糖苷酶,特别是镰刀菌属的α -l -阿拉伯糖苷酶,由于其药代动力学行为,比迄今为止使用的黑曲霉酶更适合用于我们的治疗概念。最近,Tietze(16)提出了一个类似的治疗概念,即利用肿瘤自身的酶、外源性酶以及在弱酸性pH条件下自发水解的抑癌剂的转运形式,利用肿瘤与正常组织之间葡萄糖升高的pH差异。
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