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盐酸替洛隆:一种口服干扰素诱导剂。

Tilorone hydrochloride: an oral interferon-inducing agent.

作者信息

Stringfellow D A, Glasgow L A

出版信息

Antimicrob Agents Chemother. 1972 Aug;2(2):73-8. doi: 10.1128/AAC.2.2.73.

Abstract

Tilorone hydrochloride characteristically induces an unusually delayed and prolonged interferon response not commonly associated with other synthetic inducers. Maximum circulating interferon levels of 8,000 to 10,000 units/ml were detected 12 hr postinoculation and persisted for up to 30 hr after administration of tilorone. The fact that both oral and intraperitoneal injections of tilorone induce a similar response suggests that this delay is not based on the time required for adsorption from the gastrointestinal tract. In vitro, tilorone failed to induce detectable levels of interferon in either mouse peritoneal lymphocyte or macrophage cell cultures. Furthermore, interferon production could not be detected in the upper gastrointestinal tract after oral administration of tilorone. The striking suppression of interferon production in X-irradiated mice suggested that lymphatic tissue may be a source of interferon in response to tilorone. This concept was not supported, however, by experiments utilizing antilymphocyte serum (ALS). Tilorone induced comparable levels of interferon in both ALS-treated and control animals which had received normal serum, even though the ALS-treated mice had decreased spleen weights and peripheral lymphocyte counts. These data suggest that a radiosensitive cell population other than lymphocytes may be an important factor in the capacity of the host to produce interferon in response to tilorone. Mice which received repeated injections of tilorone developed a severe state of hyporeactivity. The degree of hyporeactivity was particularly striking when compared to that induced by polyinosinic acid:polycytidylic acid and emphasizes one of the major obstacles confronting interferon inducers as chemotherapeutic agents.

摘要

盐酸替洛隆的特点是能诱导出异常延迟且持久的干扰素反应,这与其他合成诱导剂通常引发的反应不同。接种后12小时可检测到循环中干扰素的最高水平为8000至10000单位/毫升,且在给予替洛隆后可持续长达30小时。口服和腹腔注射替洛隆均诱导出相似反应,这一事实表明这种延迟并非基于从胃肠道吸收所需的时间。在体外,替洛隆在小鼠腹腔淋巴细胞或巨噬细胞培养物中均未能诱导出可检测到的干扰素水平。此外,口服替洛隆后在上消化道中未检测到干扰素产生。X射线照射小鼠后干扰素产生受到显著抑制,这表明淋巴组织可能是对替洛隆产生反应时干扰素的一个来源。然而,使用抗淋巴细胞血清(ALS)的实验并不支持这一概念。尽管接受ALS处理的小鼠脾脏重量和外周淋巴细胞计数减少,但替洛隆在接受ALS处理的动物和接受正常血清的对照动物中诱导出了相当水平的干扰素。这些数据表明,淋巴细胞以外的对辐射敏感的细胞群体可能是宿主对替洛隆产生干扰素能力的一个重要因素。反复注射替洛隆的小鼠会出现严重的低反应状态。与聚肌苷酸:聚胞苷酸诱导的低反应程度相比,这种低反应程度尤为显著,这也凸显了干扰素诱导剂作为化疗药物所面临的主要障碍之一。

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