转铁蛋白饱和度和不饱和铁结合能力的生物学变异性。
Biological variability of transferrin saturation and unsaturated iron-binding capacity.
作者信息
Adams Paul C, Reboussin David M, Press Richard D, Barton James C, Acton Ronald T, Moses Godfrey C, Leiendecker-Foster Catherine, McLaren Gordon D, Dawkins Fitzroy W, Gordeuk Victor R, Lovato Laura, Eckfeldt John H
机构信息
Department of Medicine, University Hospital, London, Ontario, Canada.
出版信息
Am J Med. 2007 Nov;120(11):999.e1-7. doi: 10.1016/j.amjmed.2007.02.027.
BACKGROUND
Transferrin saturation is widely considered the preferred screening test for hemochromatosis. Unsaturated iron-binding capacity has similar performance at lower cost. However, the within-person biological variability of both these tests may limit their ability at commonly used cut points to detect HFE C282Y homozygous patients.
METHODS
The Hemochromatosis and Iron Overload Screening Study screened 101,168 primary care participants for iron overload using transferrin saturation, unsaturated iron-binding capacity, ferritin, and HFE C282Y and H63D genotyping. Transferrin saturation and unsaturated iron-binding capacity were performed at initial screening and again when selected participants and controls returned for a clinical examination several months later. A missed case was defined as a C282Y homozygote who had transferrin saturation below the cut point (45% for women, 50% for men) or unsaturated iron-binding capacity above the cut point (150 micromol/L for women, 125 micromol/L for men) at the initial screening or the clinical examination, or both, regardless of serum ferritin.
RESULTS
There were 209 C282Y previously undiagnosed homozygotes with transferrin saturation and unsaturated iron-binding capacity testing performed at the initial screening and clinical examination. Sixty-eight C282Y homozygotes (33%) would have been missed at these transferrin saturation cut points (19 men, 49 women; median serum ferritin level of 170 microg/L; first and third quartiles, 50 and 474 microg/L), and 58 homozygotes (28%) would have been missed at the unsaturated iron-binding capacity cut points (20 men, 38 women; median serum ferritin level of 168 microg/L; first and third quartiles, 38 and 454 microg/L). There was no advantage to using fasting samples.
CONCLUSIONS
The within-person biological variability of transferrin saturation and unsaturated iron-binding capacity limits their usefulness as an initial screening test for expressing C282Y homozygotes.
背景
转铁蛋白饱和度被广泛认为是血色素沉着症的首选筛查试验。不饱和铁结合能力具有相似的性能且成本更低。然而,这两种检测方法在个体内部的生物学变异性可能会限制它们在常用切点时检测HFE C282Y纯合子患者的能力。
方法
血色素沉着症和铁过载筛查研究使用转铁蛋白饱和度、不饱和铁结合能力、铁蛋白以及HFE C282Y和H63D基因分型对101168名初级保健参与者进行铁过载筛查。转铁蛋白饱和度和不饱和铁结合能力在初次筛查时进行检测,当部分选定的参与者和对照组几个月后返回进行临床检查时再次检测。漏诊病例定义为在初次筛查或临床检查时,或两者均出现转铁蛋白饱和度低于切点(女性为45%,男性为50%)或不饱和铁结合能力高于切点(女性为150微摩尔/升,男性为125微摩尔/升)的C282Y纯合子,无论血清铁蛋白水平如何。
结果
在初次筛查和临床检查时对转铁蛋白饱和度和不饱和铁结合能力进行检测,共有209例先前未诊断出的C282Y纯合子。在这些转铁蛋白饱和度切点时,68例C282Y纯合子(33%)会被漏诊(19名男性,49名女性;血清铁蛋白水平中位数为170微克/升;第一和第三四分位数分别为50和474微克/升),在不饱和铁结合能力切点时,58例纯合子(28%)会被漏诊(20名男性,38名女性;血清铁蛋白水平中位数为168微克/升;第一和第三四分位数分别为38和454微克/升)。使用空腹样本并无优势。
结论
转铁蛋白饱和度和不饱和铁结合能力在个体内部的生物学变异性限制了它们作为筛查C282Y纯合子初始检测方法的效用。
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