首页> 外文期刊>The Journal of Urology >Solid phase assay of urine cystine supersaturation in the presence of cystine binding drugs.
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Solid phase assay of urine cystine supersaturation in the presence of cystine binding drugs.

机译:在胱氨酸结合药物存在下尿中胱氨酸过饱和的固相分析。

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PURPOSE: We report a new kind of assay system for urine cystine supersaturation that is accurate in the presence of cystine binding thiol drugs. We measured the molar ratio of cystine dissolved per mole of drug. MATERIALS AND METHODS: Measured amounts of cystine crystals were incubated in buffer or urine for 48 hours with stirring. The solid phase remaining was pelleted by centrifugation, extracted into a high pH buffer and measured. D-penicillamine, tiopronin and captopril were added to determine their effect on solid phase dissolution. RESULTS: Total cystine calculated from urine and solid measurements closely matched the amounts of cystine weighed in, meaning that the assay system successfully recovered the total cystine from the 2 phases. Each drug dissolved solid cystine in a specific and fixed proportion to its molar concentration in the range of 0.2 to 0.4 mM. dissolution per mM. of drug. Solution measurements were not a reliable gauge to the actual amounts of cystine dissolved. CONCLUSIONS: Changes in solid phase cystine accurately reflect buffer or urine supersaturation when thiol drugs are present. The solid phase assay is a technically straightforward and reliable way of assessing cystine movement into and out of urine that avoids complexity of measurement and distortions of assay systems by drugs. This assay enables one to assess the level of drug effect and the need for a change in dosing.
机译:目的:我们报告了一种新型的尿液胱氨酸过饱和度测定系统,该系统在与胱氨酸结合的硫醇药物存在下是准确的。我们测量了每摩尔药物溶解的胱氨酸的摩尔比。材料与方法:在搅拌下,将测定量的胱氨酸晶体在缓冲液或尿液中孵育48小时。剩余的固相通过离心沉淀,提取到高pH缓冲液中并进行测量。加入D-青霉胺,硫普罗宁和卡托普利以确定它们对固相溶解的影响。结果:从尿液和固体中测得的总胱氨酸与称量的胱氨酸量非常匹配,这意味着该分析系统成功地从两个阶段中回收了总胱氨酸。每种药物以特定且固定的比例溶解固体胱氨酸,其摩尔浓度范围为0.2至0.4 mM。每毫米溶解。毒品。溶液测量值不是衡量胱氨酸实际溶解量的可靠指标。结论:当存在硫醇药物时,固相胱氨酸的变化准确地反映了缓冲液或尿液的过饱和。固相测定是评估胱氨酸进入尿中和从尿中移出的技术上简单,可靠的方法,可避免测量的复杂性和药物对测定系统的扭曲。这种测定使人们能够评估药物作用水平和改变剂量的需要。

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