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精神活性吩噻嗪类药物硫利达嗪与天然多肽巴曲酶联合使用对其抗肿瘤活性及后肢麻痹的体内作用。

In vivo effects of the association of the psychoactive phenotiazine thioridazine on antitumor activity and hind limb paralysis induced by the native polypeptide crotamine.

作者信息

Porta Lucas C, Campeiro Joana D, Papa Giovanna B, Oliveira Eduardo B, Godinho Rosely O, Rodrigues Tiago, Hayashi Mirian A F

机构信息

Departamento de Farmacologia, Escola Paulista de Medicina (EPM), Universidade Federal de São Paulo (UNIFESP), SP, Brazil.

Departamento de Bioquímica e Imunologia, Universidade de São Paulo (USP-RP), Ribeirão Preto, Brazil.

出版信息

Toxicon. 2020 Oct 15;185:64-71. doi: 10.1016/j.toxicon.2020.06.017. Epub 2020 Jul 2.

DOI:10.1016/j.toxicon.2020.06.017
PMID:32621838
Abstract

Crotamine is a cationic polypeptide composed by 42 amino acid residues with several pharmacological and biological properties, including the selective ability to enter and kill actively proliferating tumour cells, which led us to propose its use as a theranostic agent for cancer therapy. At the moment, the improvement of crotamine antitumoral efficacy by association with chemotherapeutic adjuvants is envisioned. In the present work, we evaluated the association of crotamine with the antitumoral adjuvant phenotiazine thioridazine (THD). In spite of the clear efficacy of these both compounds as anticancer agents in long-term in vivo treatment of animal model bearing implanted xenograph melanoma tumor, the expected mutual potentiation of the antitumor effects was not observed here. Moreover, this association revealed for the first time the influence of THD on crotamine ability to trigger the hind limb paralysis in mice, and this discovery may represent the first report suggesting the potential involvement of the CNS in the action of this snake polypeptide on the skeletal muscle paralysis, which was classically believed to be essentially limited to a direct action in peripheral tissues as the skeletal muscle. This is also supported by the observed ability of crotamine to potentiate the sedative effects of THD which action was consistently demonstrated to be based on its central action. The better characterization of crotamine properties in CNS may certainly bring important insights for the knowledge needed to pave the way toward the use of this molecule as a theranostic compound in human diseases as cancer.

摘要

巴豆毒素是一种由42个氨基酸残基组成的阳离子多肽,具有多种药理和生物学特性,包括进入并杀死活跃增殖的肿瘤细胞的选择性能力,这促使我们提出将其用作癌症治疗的治疗诊断剂。目前,设想通过与化疗佐剂联合来提高巴豆毒素的抗肿瘤疗效。在本研究中,我们评估了巴豆毒素与抗肿瘤佐剂吩噻嗪硫利达嗪(THD)的联合。尽管这两种化合物作为抗癌剂在长期体内治疗植入异种移植黑色素瘤肿瘤的动物模型中具有明显疗效,但在此未观察到预期的抗肿瘤作用的相互增强。此外,这种联合首次揭示了THD对巴豆毒素引发小鼠后肢麻痹能力的影响,这一发现可能代表了第一份报告,表明中枢神经系统可能参与了这种蛇多肽对骨骼肌麻痹的作用,传统上认为这种作用主要限于在周围组织如骨骼肌中的直接作用。巴豆毒素增强THD镇静作用的观察能力也支持了这一点,THD的作用一直被证明是基于其中枢作用。更好地表征巴豆毒素在中枢神经系统中的特性肯定会为将该分子用作人类疾病如癌症的治疗诊断化合物所需的知识带来重要见解。

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In vivo effects of the association of the psychoactive phenotiazine thioridazine on antitumor activity and hind limb paralysis induced by the native polypeptide crotamine.精神活性吩噻嗪类药物硫利达嗪与天然多肽巴曲酶联合使用对其抗肿瘤活性及后肢麻痹的体内作用。
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Crotamine inhibits preferentially fast-twitching muscles but is inactive on sodium channels.克罗塔明优先抑制快肌,但对钠通道无作用。
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