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稳定铜同位素(65Cu)在肝豆状核变性鉴别诊断中的应用。

Use of a stable copper isotope (65Cu) in the differential diagnosis of Wilson's disease.

作者信息

Lyon T D, Fell G S, Gaffney D, McGaw B A, Russell R I, Park R H, Beattie A D, Curry G, Crofton R J, Gunn I

机构信息

Institute of Biochemistry, Royal Infirmary, Glasgow, U.K.

出版信息

Clin Sci (Lond). 1995 Jun;88(6):727-32. doi: 10.1042/cs0880727.

Abstract
  1. 65Cu/63Cu stable-isotope ratios have been measured in blood serum after oral administration of the stable isotope 65Cu. The incorporation of the isotope into the plasma protein pool was followed at various times for up to 3 days. The resulting patterns of enrichment in healthy control subjects, in Wilson's disease patients and in heterozygotes for the Wilson's disease gene, were similar in appearance to those found by others using copper radioactive isotopes. After an initially high enrichment at 2 h after dosage, the Wilson's disease cases, in contrast to the control subjects, did not show a secondary rise in isotope enrichment of the plasma pool after 72 h, demonstrating a failure to incorporate copper into caeruloplasmin. The Wilson's disease heterozygotes had variable degrees of impairment of isotope incorporation, not always distinguished from those of control subjects. 2. The stability of the isotope also permits the copper tracer to be followed for a longer period. Ten healthy subjects were studied for over 40 days, allowing the biological half-time of an oral dose of copper to be determined (median 18.5 days, 95% confidence interval 14-26 days). Known heterozygotes for the Wilson's disease gene were found to have a significantly increased biological half-time for removal of copper from the plasma pool (median 43 days, 95% confidence interval 32-77 days). 3. The incorporation of 65 Cu in patients with diseases of the liver (other than Wilson's disease) was found to be similar to that in control subjects, aiding differential diagnosis.
摘要
  1. 口服稳定同位素⁶⁵Cu后,测定了血清中的⁶⁵Cu/⁶³Cu稳定同位素比率。在长达3天的不同时间点追踪该同位素掺入血浆蛋白池的情况。健康对照受试者、威尔逊病患者以及威尔逊病基因杂合子中所得到的富集模式,在外观上与其他人使用铜放射性同位素所发现的模式相似。与对照受试者相比,威尔逊病患者在给药后2小时最初有较高的富集,但在72小时后血浆池中的同位素富集未出现二次升高,这表明未能将铜掺入铜蓝蛋白。威尔逊病杂合子的同位素掺入受损程度各异,并不总是能与对照受试者区分开来。2. 该同位素的稳定性还使得能够对铜示踪剂进行更长时间的追踪。对10名健康受试者进行了超过40天的研究,从而确定口服铜剂量的生物半衰期(中位数18.5天,95%置信区间14 - 26天)。已发现已知的威尔逊病基因杂合子从血浆池中清除铜的生物半衰期显著延长(中位数43天,95%置信区间32 - 77天)。3. 发现肝脏疾病(威尔逊病除外)患者中⁶⁵Cu的掺入情况与对照受试者相似,有助于鉴别诊断。

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