Comparative Study of the Effects of Curcuminoids and Tetrahydrocurcuminoids on Melanogenesis: Role of the Methoxy Groups

S. Goenka
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Abstract

Curcuminoids are naturally occurring yellow-colored compounds that, when hydrogenated to remove their conjugated double bond, become colorless and are referred to as tetrahydrocurcuminoids. Curcuminoids consist of pure curcumin (PC) in major amounts and demethoxycurcumin (DC) and bisdemethoxycurcumin (BDC) in minor amounts. Tetrahydrocurcuminoids similarly consist mainly of tetrahydrocurcumin (THC), along with minor amounts of tetrahydrodemethoxycurcumin (THDC) and tetrahydrobisdemethoxycurcumin (THBDC). Previous studies have shown the inhibitory effects of PC, DC, and BDC on melanin production, but there are contradictory findings about THC. In addition, there are currently no reports on the effects of THDC and THBDC on melanogenesis. Our previous report described that, in contrast to PC, which suppressed melanin production, THC stimulated melanin production in B16F10 and MNT-1 cells; this effect was ascribed to the loss of the conjugated heptadiene moiety of PC. However, whether this finding can be generalized to the two curcumin derivatives (DC and BDC), such that THDC and THBDC might also stimulate melanogenesis, has not been addressed. Herein, a comparative study of six curcumin derivatives (PC, DC, BDC, THC, THDC, and THBDC) was undertaken to identify their effects on melanogenesis with the goal of elucidating the structure–activity relationships (SARs) focused on assessing the two regions of the parent curcumins’ structure: (i) the hydrogenation of the two double bonds bridging the phenyl rings to the β-diketone moiety, and (ii) the effect of the ortho-methoxy substituent (-OCH3) on the two phenyl rings. To determine the direct effects of the six compounds, antioxidant activity and tyrosinase activity were assessed in cell-free systems before cellular experiments utilizing the B16F10 mouse melanoma cells, MNT-1 human melanoma cells, and primary cells. Evaluations were made on cytotoxicity, melanin concentration, and cellular tyrosinase activity. The results showed that BDC inhibited melanogenesis in B16F10 and MNT-1 cells. However, it was ineffective in primary human melanocytes, while THBDC continued to exhibit anti-melanogenic capacity in normal human melanocytes. Moreover, these findings provide a novel perspective into the role of the methoxy groups of PC on the biological effects of melanogenesis and also confirm that the removal of the conjugated double bonds abolishes the anti-melanogenic capacity of PC and DC only, but not BDC, as THBDC maintained anti-melanogenic activity that was greater than BDC. However, the outcome is contingent upon the specific kind of cell involved. To the best of our knowledge, this work presents novel findings indicating that the anti-melanogenic capacity of the colored BDC is not only intact but enhanced after its hydrogenation as observed in THBDC. The findings show potential for using colorless THBDC as a pharmacological candidate to diminish the increased pigmentation characteristic of skin hyperpigmentation disorders. Future pharmacological therapeutics that incorporate pure THBDC or THBDC-enriched extracts, which retain both a colorless appearance and potent anti-melanogenic activity, can be applied to compounds for anti-melanoma therapeutics where the demand for nontoxic novel molecules is desired for established efficacies.
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姜黄素和四氢姜黄素对黑色素生成作用的比较研究:甲氧基的作用
姜黄素是天然存在的黄色化合物,氢化去除共轭双键后会变成无色,被称为四氢姜黄素。姜黄素主要包括纯姜黄素(PC),以及少量的去甲氧基姜黄素(DC)和双去甲氧基姜黄素(BDC)。四氢姜黄素同样主要包括四氢姜黄素(THC),以及少量的四氢去甲氧基姜黄素(THDC)和四氢双去甲氧基姜黄素(THBDC)。以往的研究表明 PC、DC 和 BDC 对黑色素的生成有抑制作用,但关于 THC 的研究结果却相互矛盾。此外,目前还没有关于 THDC 和 THBDC 对黑色素生成的影响的报告。我们之前的报告指出,与抑制黑色素生成的 PC 不同,THC 可刺激 B16F10 和 MNT-1 细胞中黑色素的生成;这一效应可归因于 PC 中共轭庚二烯分子的缺失。然而,这一发现是否可以推广到两种姜黄素衍生物(DC 和 BDC),从而使 THDC 和 THBDC 也能刺激黑色素生成,这一问题尚未解决。在此,我们对六种姜黄素衍生物(PC、DC、BDC、THC、THDC 和 THBDC)进行了比较研究,以确定它们对黑色素生成的影响,目的是阐明结构-活性关系(SARs),重点评估姜黄素母体结构的两个区域:(i)连接苯基环与β-二酮分子的两个双键的氢化,以及(ii)两个苯基环上的原位甲氧基取代基(-OCH3)的影响。为了确定这六种化合物的直接作用,在利用 B16F10 小鼠黑色素瘤细胞、MNT-1 人类黑色素瘤细胞和原代细胞进行细胞实验之前,先在无细胞系统中评估了抗氧化活性和酪氨酸酶活性。对细胞毒性、黑色素浓度和细胞酪氨酸酶活性进行了评估。结果表明,BDC 能抑制 B16F10 和 MNT-1 细胞的黑色素生成。然而,它对原代人类黑色素细胞无效,而 THBDC 在正常人类黑色素细胞中继续表现出抗黑色素生成的能力。此外,这些发现为了解 PC 的甲氧基基团对黑色素生成的生物效应的作用提供了一个新的视角,同时也证实了去除共轭双键后,仅 PC 和 DC 的抗黑色素生成能力会减弱,而 BDC 的抗黑色素生成能力不会减弱,因为 THBDC 的抗黑色素生成活性高于 BDC。然而,结果取决于所涉及的特定细胞种类。据我们所知,这项工作提出了新的发现,表明有色 BDC 的抗黑色素生成能力不仅完好无损,而且在氢化后还会增强,正如在 THBDC 中观察到的那样。研究结果表明,无色的 THBDC 有可能作为一种药理候选物质,用于减少皮肤色素沉着症所特有的色素增加。纯 THBDC 或 THBDC 富集提取物既保持了无色外观,又具有强大的抗黑色素生成活性,未来可将其应用于抗黑色素瘤疗法的化合物中,因为这种疗法需要无毒的新型分子来达到既定的疗效。
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