Takamatsu Kayo, Takano Atsushi, Yakushiji Nobumasa, Morishita Ken-ichi, Matsuura Nobuyasu, Makishima Makoto, Ali Hamed Ismail, Akaho Eiichi, Tai Akihiro, Sasaki Kenji, Kakuta Hiroki
Okayama University Graduate School of Medicine, Dentistry and Pharmaceutical Sciences, 1-1-1, Tsushima-Naka, Okayama 700-8530, Japan.
ChemMedChem. 2008 Mar;3(3):454-60. doi: 10.1002/cmdc.200700265.
Retinoid X receptor agonists (RXR agonists, rexinoids) are interesting candidates for the treatment of cancers such as tamoxifen-resistant breast cancer and taxol-resistant lung cancer. However, well-known RXR agonists possess a strong lipophilic character. In addition, although RXR has three subtypes, no subtype-selective RXR agonists are known. Thus we aimed to produce less-lipophilic and subtype-selective RXR agonists. By designing sulfonamide-type RXR agonists, 4-[N-methanesulfonyl-N-(5,5,8,8-tetramethyl-5,6,7,8-tetrahydro-2-naphthyl)amino]benzoic acid (8 a) was found to prefer RXRalpha over RXRbeta and RXRgamma, although the potency is less than the potencies of well-known RXR pan-agonists. Moreover, our results suggest that the reduction of lipophilicity at the hydrophobic interaction region of RXR agonists enables production of RXR subtype preference. Our finding will be useful for the creation of more potent and less-lipophilic subtype-selective RXR agonists aimed at the reduction of undesirable side effects.
维甲酸X受体激动剂(RXR激动剂,视黄酸类化合物)是治疗诸如抗他莫昔芬乳腺癌和抗紫杉醇肺癌等癌症的有吸引力的候选药物。然而,众所周知的RXR激动剂具有很强的亲脂性。此外,尽管RXR有三种亚型,但尚无亚型选择性的RXR激动剂。因此,我们旨在制备亲脂性较低且具有亚型选择性的RXR激动剂。通过设计磺酰胺型RXR激动剂,发现4-[N-甲磺酰基-N-(5,5,8,8-四甲基-5,6,7,8-四氢-2-萘基)氨基]苯甲酸(8a)对RXRα的偏好高于RXRβ和RXRγ,尽管其效力低于众所周知的RXR泛激动剂。此外,我们的结果表明,降低RXR激动剂疏水相互作用区域的亲脂性能够产生RXR亚型偏好性。我们的发现将有助于开发更有效且亲脂性更低的亚型选择性RXR激动剂,以减少不良副作用。
