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酚类黑色素前体为设计黑色素瘤抗肿瘤药物提供了一种合理的方法。

Phenolic melanin precursors provide a rational approach to the design of antitumor agents for melanoma.

作者信息

Jimbow K, Miura T, Ito S, Ishikawa K

机构信息

Division of Dermatology and Cutaneous Sciences, University of Alberta, Edmonton, Canada.

出版信息

Pigment Cell Res. 1989 Jan-Feb;2(1):34-9. doi: 10.1111/j.1600-0749.1989.tb00155.x.

Abstract

A unique biological property of the melanocyte, melanin synthesis may permit a rational approach to design agents for better management of malignant melanoma. This in vivo and in vitro study examined the selective melanocytotoxicity and antimelanoma effects of phenolic compounds, cysteinylphenol (CP), cysteaminylphenol (CAP), and related compounds, and found (1) that both 4-S-CP and 4-S-CAP are melanin precursors, (2) that 4-S-CAP possesses a marked depigmenting potency with selective destruction of melanocytes in black follicles, and (3) a significant inhibition in the protein synthesis and tumor growth of B16 melanoma. Importantly, a whole body autoradiography indicated that these phenolic melanin precursors are selectively incorporated into melanoma tissues after i.p. administration.

摘要

黑色素细胞的独特生物学特性——黑色素合成,可能为设计更好地治疗恶性黑色素瘤的药物提供合理方法。这项体内和体外研究考察了酚类化合物、半胱氨酰苯酚(CP)、半胱胺基苯酚(CAP)及相关化合物的选择性黑素细胞毒性和抗黑素瘤作用,发现:(1)4-S-CP和4-S-CAP均为黑色素前体;(2)4-S-CAP具有显著的色素脱失效力,可选择性破坏黑色毛囊中的黑素细胞;(3)对B16黑色素瘤的蛋白质合成和肿瘤生长有显著抑制作用。重要的是,全身放射自显影表明,这些酚类黑色素前体经腹腔注射后可选择性地掺入黑色素瘤组织。

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