Interferon counteracts pyrimidinone-induced hyporeactivity and the combined treatment has antitumor effect in mice.

Gan Pub Date : 1984-07-01
T Oku, J Imanishi, T Kishida
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Abstract

A potent interferon (IFN) inducer, 2-amino-5-bromo-6-phenyl-4-pyrimidinone (ABPP), induced hyporeactivity in mice, and so IFN induced by subsequently administered ABPP was reduced even 120 hr after the first administration of ABPP. This hyporeactivity was counteracted by the injection of IFN (10,000 IU or more) 3 hr before the subsequent administrations of ABPP. Since the injection of more than 5,000 IU/mouse of IFN 3 hr before an administration of ABPP enhanced the circulating IFN titer, the priming effect in vivo by IFN may result in the reduction of hyporeactivity. Administrations of ABPP (200 mg/kg or 500 mg/kg) at intervals of 2 days and the injection of IFN (25,000 IU/mouse) 3 hr before each administration of ABPP to neuroblastoma-bearing A/J mice reduced the mortality and completely cured 40% of the mice in each combined therapy group. These results suggest that the combined use of the IFN inducer with IFN may be available for patients with neoplasm or viral infection.

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干扰素可抵消嘧啶诱导的小鼠低反应性,联合治疗具有抗肿瘤作用。
一种有效的干扰素(IFN)诱导剂,2-氨基-5-溴-6-苯基-4-嘧啶酮(ABPP),诱导小鼠反应性降低,因此,随后给药的ABPP诱导的IFN甚至在第一次给药120小时后也减少了。这种低反应性可通过在随后给药ABPP前3小时注射IFN (10,000 IU或更多)来抵消。由于在给药前3小时注射超过5000 IU/小鼠的IFN可增强循环IFN滴度,IFN在体内的启动效应可能导致低反应性的减少。每隔2天给药ABPP (200 mg/kg或500 mg/kg),并在每次给药ABPP前3小时注射IFN (25,000 IU/只),降低了A/J神经母细胞瘤小鼠的死亡率,并在每个联合治疗组中完全治愈了40%的小鼠。这些结果表明,IFN诱导剂与IFN联合使用可能适用于肿瘤或病毒感染患者。
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