Willhite C C, Dawson M I, Reichert U
State of California, Berkeley 94710, USA.
Drug Metab Rev. 1996 Feb-May;28(1-2):105-19. doi: 10.3109/03602539608993994.
Retinoid mechanism of action is dependent upon interaction with the retinoid nuclear RAR and RXR subfamilies of receptors. Study of ligands selective for the different receptors or which modify that interaction may provide insight into which receptors play roles in or contribute to retinoid teratogenesis. The retinoids considered here include in the RAR alpha-selective arylcarboxamidobenzoic acid CD 336 (Am580), the RAR beta/gamma-selective naphthalenecarboxylic acid CD 135 and the adamantyl-phenylcarboxamidobenzoic acid CD 394, the RAR-selective tetrahydrotetra-methylanthracenylbenzoic acid (TTAB) SRI 3961, the carboxyphenylretinamide SRI 7167-67, and the RXR-selective diarylisopropylidene SR 11217. CD 135 has a 3-fold higher affinity for RAR beta when compared with RAR gamma, whereas CD 394 has a 3-fold higher affinity for RAR gamma when compared with RAR beta. A separate investigation into potential amelioration of retinoid teratogenesis by concomitant administration of the cyclohexanetrione (Ro 31-0521) was also conducted. When pregnant hamsters were given an oral bolus of CD 336 or CD 135 during the early primitive streak stage of gestation, these retinoids proved 60-100 times more potent teratogens than all-trans-retinoic acid. Intubation of CD 394 resulted in production of terata similar to that seen after an equivalent dose of all-trans-retinoic acid. Administration of SRI 3961 found this compound 8000 times more potent than all-trans-retinoic acid, while SRI 7167-67 failed to show any evidence for developmental toxicity even after exposure to 105 mg/kg. Studies with the RXR-selective SR 11217 found it to be far less potent than all-trans-retinoic acid. These data point to the conclusion that those retinoids which have no affinity for retinoid nuclear receptors also have little potential for induction of developmental toxicity at doses which do not also provoke maternal intoxication. Comparing in vitro transcriptional activation of wild-type human RAR for the supertoxic TTNBP (Ro 13-7410) and TTAB (SRI 3961) with their relative teratogenic potency in hamster found that the more toxic congener also had the lower in vitro EC50 transactivation value (at ratios approximating their differential toxicities measured as administered dose). The RAR beta/gamma-selective CD 135 (TTNN) was not as efficient as TTNBP (Ro 13-7410) or TTAB (SRI 3961) in hRAR transactivation and CD 135 was less toxic than either Ro 13-7410 or SRI 3961. Although the RXR-selective SR 11217 failed to elicit terata after moderate doses, malformations consistent with those induced by high doses of retinoic acid could be produced following a single large bolus of SR 11217. Under the conditions here, simultaneous administration of Ro 31-0521 with all-trans-retinoic acid appeared to reduce the total percentage of abnormal fetuses seen after exposure to retinoic acid alone, but fetal body weights remained depressed and the numbers of dead embryos remained elevated, suggesting only limited influence of the cyclohexanetrione on retinoid developmental toxicity.
维甲酸的作用机制取决于其与维甲酸核受体RAR和RXR亚家族的相互作用。对不同受体具有选择性或能改变这种相互作用的配体进行研究,可能有助于深入了解哪些受体在维甲酸致畸过程中发挥作用或有影响。本文所涉及的维甲酸包括对RARα有选择性的芳基羧酰胺苯甲酸CD 336(Am580)、对RARβ/γ有选择性的萘甲酸CD 135和金刚烷基苯基羧酰胺苯甲酸CD 394、对RAR有选择性的四氢四甲基蒽基苯甲酸(TTAB)SRI 3961、羧基苯基维甲酰胺SRI 7167 - 67以及对RXR有选择性的二芳基异丙叉物SR 11217。与RARγ相比,CD 135对RARβ的亲和力高3倍;而与RARβ相比,CD 394对RARγ的亲和力高3倍。还进行了一项单独研究,探究同时给予环己三酮(Ro 31 - 0521)对维甲酸致畸作用的潜在改善情况。在妊娠早期原条期给怀孕仓鼠口服大剂量的CD 336或CD 135,结果显示这些维甲酸的致畸效力比全反式维甲酸高60 - 100倍。插管给予CD 394产生的畸形与给予等量全反式维甲酸后所见相似。给予SRI 3961发现该化合物的效力比全反式维甲酸高八千倍,而SRI 7167 - 67即使在暴露于105 mg/kg后也未显示出任何发育毒性的证据。对RXR有选择性的SR 11217的研究发现,其效力远低于全反式维甲酸。这些数据表明,那些对维甲酸核受体没有亲和力的维甲酸,在不引起母体中毒的剂量下,诱导发育毒性的可能性也很小。比较超毒性的TTNBP(Ro 13 - 7410)和TTAB(SRI 3961)对野生型人RAR的体外转录激活与其在仓鼠体内的相对致畸效力,发现毒性更强的同系物在体外的EC50转录激活值也更低(其比例近似于以给药剂量衡量的差异毒性)。RARβ/γ有选择性的CD 135(TTNN)在激活人RAR方面不如TTNBP(Ro 13 - 7410)或TTAB(SRI 3961)有效,且CD 135的毒性低于Ro 13 - 7410或SRI 3961。尽管中等剂量的RXR有选择性的SR 11217未引发畸形,但单次大剂量给予SR 11217后可产生与高剂量维甲酸诱导的畸形一致的畸形。在本文所述条件下,同时给予Ro 31 - 0521和全反式维甲酸似乎可降低单独暴露于维甲酸后出现的异常胎儿的总百分比,但胎儿体重仍较低,死胎数量仍较高,这表明环己三酮对维甲酸发育毒性的影响有限。
