Delatour P, Benoit E, Bourdin M, Gobron M, Moysan F
Département de Toxicologie Métabolique, Ecole Nationale Vétérinaire de Lyon.
Bull Acad Natl Med. 1993 Mar;177(3):515-26; discussion 526-7.
After the administration of racemic ketoprofen and carprofen to man, both enantiomers of each compound exhibit similar plasma profiles. This contrasts with the rat where the active S(+) enantiomer is predominant. For carprofen, regardless of the route of administration, the R(-) enantiomer is predominant in the plasma of all investigated animal species. The S(+)/R(-) ratio of the "areas under the curves" during the time course of the kinetics, is: 0.60 in dogs, 0.53 in Yucatan micro-pigs, 0.48 in mini-goats, 0.67 in calves and 0.19 in horses. For ketoprofen, the S(+) enantiomer is predominant in dogs, cats and horses, with ratios of 30.3, 5.3 and 1.5, respectively, while R(-) is the predominant enantiomer in sheep. The interpretation of these inter-species differences can be supported by experimental evidence, however some informations are lacking and additional investigation is required. In the case of ketoprofen where S(+) is predominant in rats, dogs and horses, the metabolic chiral inversion from R(-) to S(+), which has been demonstrated in rats, may also take place in the latter two species. In addition, the well documented stereoselective clearance of the glucuronides, possibly in favour of the enantiomer S(+), may explain the lower body clearance of the R(-) enantiomer in sheep. For carprofen, no metabolic chiral inversion was shown in rats and dogs after administration of each enantiomer individually, but for this compound, stereoselective clearance of glucuronides has been demonstrated which may support the idea of a plasma concentration shift of the enantiomeric proportions vs time in favour of the R(-) enantiomer. Regardless of the possible biological mechanisms which are responsible for these inter-species differences, the existence of these differences gives rise to at least two important issues: The choice of animal species which can be used in the research of drugs destined for human therapeutics: the most pertinent animal species will be the one which demonstrates an enantiomeric plasma profile closest to that observed in man. The present data show that the ideal animal species from this respect has still to be identified. For application in veterinary therapeutics, a careful balance must be established between the requirement of favourable bioavailability of the active S(+) enantiomer and the potential of any possible chiral inversion of R(-) to generate hybrid molecules in meat and milk which in turn may lead to residues, the toxicity of which to the human consumer is still unknown.
给人体施用消旋酮洛芬和卡洛芬后,每种化合物的两种对映体都呈现出相似的血浆浓度曲线。这与大鼠的情况形成对比,在大鼠中活性S(+)对映体占主导。对于卡洛芬,无论给药途径如何,在所有研究的动物物种血浆中R(-)对映体占主导。在动力学过程中,“曲线下面积”的S(+)/R(-)比值在犬中为0.60,在尤卡坦微型猪中为0.53,在小型山羊中为0.48,在犊牛中为0.67,在马中为0.19。对于酮洛芬,S(+)对映体在犬、猫和马中占主导,比值分别为30.3、5.3和1.5,而R(-)是绵羊中的主要对映体。这些种间差异的解释可以得到实验证据的支持,然而仍缺乏一些信息,需要进一步研究。在大鼠、犬和马中S(+)占主导的酮洛芬情况下,已在大鼠中证实的从R(-)到S(+)的代谢手性转化,在后两个物种中也可能发生。此外,有充分记录的葡糖醛酸苷的立体选择性清除,可能有利于S(+)对映体,这可以解释绵羊中R(-)对映体较低的体内清除率。对于卡洛芬,单独施用每种对映体后,在大鼠和犬中未显示代谢手性转化,但对于该化合物,已证实葡糖醛酸苷的立体选择性清除,这可能支持对映体比例随时间向有利于R(-)对映体的血浆浓度变化的观点。无论导致这些种间差异的可能生物学机制如何,这些差异的存在至少引发了两个重要问题:在用于人类治疗药物研究的动物物种选择方面:最相关的动物物种将是其对映体血浆浓度曲线最接近在人体中观察到的曲线的物种。目前的数据表明,在这方面理想的动物物种仍有待确定。对于兽医治疗应用,必须在活性S(+)对映体良好的生物利用度要求与R(-)任何可能的手性转化产生肉和奶中混合分子的可能性之间建立谨慎的平衡,这些混合分子进而可能导致残留物,其对人类消费者的毒性仍然未知。
