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[黑色素前体在恶性黑色素瘤实验性化疗中的应用]

[Utilization of melanin precursors for experimental chemotherapy of malignant melanoma].

作者信息

Jimbow K, Miura S, Ito Y, Kasuga T, Ito S

出版信息

Gan To Kagaku Ryoho. 1984 Oct;11(10):2125-32.

PMID:6435538
Abstract

Melanin synthesis is a metabolic pathway unique and specific to melanocytes. It occurs by conversion of tyrosine to dopa and dopaquinone in the presence of tyrosinase. It is highly accelerated in malignant melanoma with a marked increase of tyrosinase activity. This study summarizes the recent progress in experimental chemotherapeutic approaches to malignant melanoma by utilizing melanin precursors, and presents our current results. Our studies indicated (a) that hydroquinone and 4-isopropylcatechol are selectively toxic to melanocytes and melanoma cells, (b) that their actions are mediated through tyrosinase, and (c) that dopa is selectively and highly incorporated into melanoma cells and melanocytes depending on the tyrosinase activity. In addition, our new compounds, i.e., 4-S-cysteinylphenol and 4-S-cysteaminylphenol were highly toxic to melanoma cells, increasing the life span of B16 melanoma bearing mice and decreasing melanoma growth in C57 BL mice. Other synthetic compounds, e.g., cysteinylcatechols and their devivatives, were, however, not toxic to melanoma cells. 4-S-cysteinylphenol and 4-S-cysteaminylphenol appeared to exert their cytotoxicity through the action of tyrosinase present in melanoma cells, thus providing a kind of "guided missile" approach to melanoma chemotherapy.

摘要

黑色素合成是黑素细胞特有的代谢途径。它通过在酪氨酸酶存在的情况下将酪氨酸转化为多巴和多巴醌而发生。在恶性黑色素瘤中,由于酪氨酸酶活性显著增加,黑色素合成会高度加速。本研究总结了利用黑色素前体对恶性黑色素瘤进行实验性化疗方法的最新进展,并展示了我们目前的研究结果。我们的研究表明:(a)对苯二酚和4 - 异丙基邻苯二酚对黑素细胞和黑色素瘤细胞具有选择性毒性;(b)它们的作用是通过酪氨酸酶介导的;(c)多巴根据酪氨酸酶活性选择性地并高度地被黑色素瘤细胞和黑素细胞摄取。此外,我们的新化合物,即4 - S - 半胱氨酰苯酚和4 - S - 半胱胺基苯酚对黑色素瘤细胞具有高度毒性,可延长荷B16黑色素瘤小鼠的寿命,并减少C57 BL小鼠体内黑色素瘤的生长。然而,其他合成化合物,如半胱氨酰儿茶酚及其衍生物,对黑色素瘤细胞没有毒性。4 - S - 半胱氨酰苯酚和4 - S - 半胱胺基苯酚似乎通过黑色素瘤细胞中存在的酪氨酸酶的作用发挥其细胞毒性,从而为黑色素瘤化疗提供了一种“制导导弹”方法。

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