Pemrick S M, Lucas D A, Grippo J F
Department of Toxicology and Pathology, Hoffman-La Roche, Nutley, NJ 07110.
Leukemia. 1994 Nov;8(11):1797-806.
The retinoid receptors belong to a large superfamily of ligand-inducible transcription factors that include the steroid, vitamin D and thyroid hormone receptors, the peroxisome proliferator-activated receptor, the insect edysteroid receptor, and a number of orphan receptors whose ligands are unknown. All nuclear receptors have several well-characterized structural domains, including a conserved DNA-binding domain, and a ligand binding domain at the carboxyl terminus of the receptor. The RAR and RXR classes of nuclear retinoic acid receptors are each composed of alpha, beta and gamma subtypes with more than one isoform for each receptor subtype. Data from many investigators suggest there are RAR- and RXR-dependent gene pathways, and that the individual receptor subtypes may control distinct gene expression patterns. In addition, RXR has been found to heterodimerize with other nuclear receptors to form active transcriptional complexes, which influence the activity of a variety of gene pathways important in growth and differentiation. As a result, retinoids have been useful clinical agents in Dermatology and Oncology. However, upon prolonged exposure to retinoic acid, resistance to retinoids has often been encountered both in the clinical setting and in long-term cell culture (HL60R and RAC65 cells). In the latter case, retinoid resistance has been associated with a mutation in the RAR gene which transcribes a RAR receptor truncated at the C-terminal end. These mutated RAR receptors exhibit a reduced affinity for retinoic acid while retaining the ability to bind to a retinoic acid response element on DNA. As a result, these mutant receptors exhibit dominant-negative activity by binding to the DNA without activating transcription and by competing with other receptors for sites on the response element. In fact, dominant-negative activity may be very important in the development of many neoplastic diseases, including acute promyelocytic leukemia (APL), where a t(15;17) chromosomal translocation fuses the PML gene to the RAR gene, to produce a PML-RAR fusion protein in large excess in the cell. However, retinoid resistance in the patient is most probably the result of pharmacokinetic problems, whereby, with continuous retinoid treatment, the plasma levels of retinoic acid gradually decrease to below that required to maintain differentiation of leukemic cells in vivo. A major challenge for drug discovery is to design a drug which circumvents these pharmacokinetic problems either by designing novel drug delivery systems or by employing retinoids which do not bind to CRABP, such as 9-c-RA.(ABSTRACT TRUNCATED AT 400 WORDS)
维甲酸受体属于一个大型的配体诱导转录因子超家族,其中包括类固醇、维生素D和甲状腺激素受体、过氧化物酶体增殖物激活受体、昆虫蜕皮甾体受体,以及一些配体未知的孤儿受体。所有核受体都有几个特征明确的结构域,包括一个保守的DNA结合结构域,以及位于受体羧基末端的配体结合结构域。核视黄酸受体的RAR和RXR类别各自由α、β和γ亚型组成,每个受体亚型有不止一种异构体。许多研究人员的数据表明存在RAR和RXR依赖性基因途径,并且各个受体亚型可能控制不同的基因表达模式。此外,已发现RXR与其他核受体异源二聚化以形成活性转录复合物,这会影响生长和分化中重要的多种基因途径的活性。因此,维甲酸在皮肤病学和肿瘤学中一直是有用的临床药物。然而,在长期暴露于维甲酸后,在临床环境和长期细胞培养(HL60R和RAC65细胞)中经常会遇到对维甲酸的耐药性。在后一种情况下,维甲酸耐药性与RAR基因的突变有关,该基因转录出在C末端截短的RAR受体。这些突变的RAR受体对维甲酸的亲和力降低,同时保留了与DNA上的维甲酸反应元件结合的能力。结果,这些突变受体通过结合DNA而不激活转录并通过与其他受体竞争反应元件上的位点而表现出显性负性活性。事实上,显性负性活性在许多肿瘤性疾病的发展中可能非常重要,包括急性早幼粒细胞白血病(APL),其中t(15;17)染色体易位将PML基因与RAR基因融合,在细胞中大量产生PML-RAR融合蛋白。然而,患者对维甲酸的耐药性很可能是药代动力学问题的结果,即随着维甲酸的持续治疗,维甲酸的血浆水平逐渐降低至低于维持体内白血病细胞分化所需的水平。药物研发的一个主要挑战是设计一种药物,通过设计新型药物递送系统或使用不与CRABP结合的维甲酸(如9-c-RA)来规避这些药代动力学问题。(摘要截断于400字)
