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右美沙芬试验用于评估肺癌的先天性易感性。

Dextromethorphan test for evaluation of congenital predisposition to lung cancer.

作者信息

Puchetti V, Faccini G B, Micciolo R, Ghimenton F, Bertrand C, Zatti N

机构信息

Clinica Chirurgica, Ospedale Policlinico, Verona, Italy.

出版信息

Chest. 1994 Feb;105(2):449-53. doi: 10.1378/chest.105.2.449.

Abstract

We report the results of an investigation conducted in 992 healthy control subjects (854 adults and 138 adolescents) and in 116 subjects with lung cancer (LC) for the purpose of detecting those individuals with a possible genetic predisposition to lung cancer. The test consists of the oral administration of 64 mumol of dextromethorphan (DMP) with collection of urine samples over the following 8-h period and urine assay of the drug (DMP) and its main metabolite, dextrorphan (DOP). The ratio of the urinary concentrations of DMP to those of DOP is called the metabolic ratio (DMP/DOP) and is inversely proportional to the DMP demethylation rate. The pattern of the metabolic ratio (Log10 DMP/DOP) allowed, using a maximum likelihood approach, the identification of three subpopulations in the 854 control subjects (adults): (1) probable homozygous extensive metabolizers with Log10 DMP/DOP < -1.74 (73.1 percent); (2) probable heterozygous intermediate metabolizers with Log10 DMP/DOP in the -1.74 to -0.40 range (22.3 percent); and (3) probable homozygous poor metabolizers with Log10 DMP/DOP > -0.4 (4.6 percent). Most of the patients with LC (89 percent) were probable homozygous extensive metabolizers. As the latter have a cancer risk that is 2.54-fold greater than that of intermediate metabolizers (95 percent confidence interval [CI]: 1.37 to 4.73) and 7.43-fold greater than that of poor metabolizers (95 percent CI: 1.01 to 54.5), their identification by means of the DMP test may be particularly useful for subjects exposed to environmental and occupational carcinogens. The phenotype test used is similar to that of the debrisoquin test, but presents the advantage that DMP is a widely used, harmless drug with a faster and simpler urinary assay procedure.

摘要

我们报告了一项针对992名健康对照者(854名成年人和138名青少年)以及116名肺癌(LC)患者进行的调查结果,目的是检测那些可能具有肺癌遗传易感性的个体。该检测包括口服64微摩尔右美沙芬(DMP),并在随后的8小时内收集尿液样本,同时对尿液中的药物(DMP)及其主要代谢物右啡烷(DOP)进行检测。尿液中DMP浓度与DOP浓度的比值称为代谢比值(DMP/DOP),它与DMP脱甲基化速率成反比。利用最大似然法,根据代谢比值(Log10 DMP/DOP)的模式,在854名对照者(成年人)中识别出了三个亚群:(1)Log10 DMP/DOP < -1.74的可能纯合广泛代谢者(73.1%);(2)Log10 DMP/DOP在-1.74至-0.40范围内的可能杂合中间代谢者(22.3%);以及(3)Log10 DMP/DOP > -0.4的可能纯合慢代谢者(4.6%)。大多数肺癌患者(89%)为可能的纯合广泛代谢者。由于后者患癌风险比中间代谢者高2.54倍(95%置信区间[CI]:1.37至4.73),比慢代谢者高7.43倍(95% CI:1.01至54.5),因此通过DMP检测识别出他们对于暴露于环境和职业致癌物的个体可能特别有用。所使用的表型检测与异喹胍检测类似,但具有DMP是一种广泛使用的无害药物且尿液检测程序更快、更简单的优点。

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