So Po-Lin, Fujimoto Michele A, Epstein Ervin H
Children's Hospital Oakland Research Institute, 5700 Martin Luther King Jr. Way, Oakland, CA 94609, USA.
Mol Cancer Ther. 2008 May;7(5):1275-84. doi: 10.1158/1535-7163.MCT-07-2043.
Basal cell carcinoma (BCC) is the most common human cancer. Patients with basal cell nevus syndrome (Gorlin syndrome) are highly susceptible to developing many BCCs as a result of a constitutive inactivating mutation in one allele of PATCHED 1, which encodes a tumor suppressor that is a major inhibitor of Hedgehog signaling. Dysregulated Hedgehog signaling is a common feature of both hereditary and sporadic BCCs. Recently, we showed remarkable anti-BCC chemopreventive efficacy of tazarotene, a retinoid with retinoic acid receptor (RAR) beta/gamma specificity, in Ptch1+/- mice when treatment was commenced before carcinogenic insults. In this study, we assessed whether the effect of tazarotene against BCC carcinogenesis is sustained after its withdrawal and whether tazarotene is effective against preexisting microscopic BCC lesions. We found that BCCs did not reappear for at least 5 months after topical drug treatment was stopped and that already developed, microscopic BCCs were susceptible to tazarotene inhibition. In vitro, tazarotene inhibited a murine BCC keratinocyte cell line, ASZ001, suggesting that its effect in vivo is by direct action on the actual tumor cells. Down-regulation of Gli1, a target gene of Hedgehog signaling and up-regulation of CRABPII, a target gene of retinoid signaling, were observed with tazarotene treatment. Finally, we investigated the effects of topical applications of other retinoid-related compounds on BCC tumorigenesis in vivo. Tazarotene was the most effective of the preparations studied, and its effect most likely was mediated by RARgamma activation. Furthermore, inhibition of basal RAR signaling in the skin promoted BCC carcinogenesis, suggesting that endogenous RAR signaling restrains BCC growth.
基底细胞癌(BCC)是人类最常见的癌症。患有基底细胞痣综合征(Gorlin综合征)的患者由于patched 1基因一个等位基因的组成性失活突变,极易发生多发性基底细胞癌,patched 1基因编码一种肿瘤抑制因子,是刺猬信号通路的主要抑制剂。刺猬信号通路失调是遗传性和散发性基底细胞癌的共同特征。最近,我们发现,在致癌损伤之前开始治疗时,他扎罗汀(一种对维甲酸受体(RAR)β/γ具有特异性的维甲酸)在Ptch1+/-小鼠中具有显著的抗基底细胞癌化学预防功效。在本研究中,我们评估了他扎罗汀停用后其对基底细胞癌致癌作用的影响是否持续,以及他扎罗汀对已存在的微小基底细胞癌病变是否有效。我们发现,局部药物治疗停止后,基底细胞癌至少5个月未复发,并且已经形成的微小基底细胞癌易受他扎罗汀抑制。在体外,他扎罗汀抑制了小鼠基底细胞癌细胞系ASZ001,这表明其在体内的作用是通过对实际肿瘤细胞的直接作用实现的。他扎罗汀治疗可观察到刺猬信号通路的靶基因Gli1下调以及维甲酸信号通路的靶基因CRABPII上调。最后,我们研究了其他维甲酸相关化合物局部应用对基底细胞癌体内肿瘤发生的影响。他扎罗汀是所研究制剂中最有效的,其作用很可能是由RARγ激活介导的。此外,皮肤中基础RAR信号的抑制促进了基底细胞癌的发生,这表明内源性RAR信号抑制基底细胞癌的生长。