Heilmann Romy M, Ruaux Craig G, Burgener Iwan A, Hern Jennifer D, Suchodolski Jan S, Steiner Jörg M
Department of Small Animal Clinical Sciences, College of Veterinary Medicine and Biomedical Sciences, Gastrointestinal Laboratory, Texas A&M University, College Station, TX 77843-4474, USA.
Vet Clin Pathol. 2013 Jun;42(2):190-5. doi: 10.1111/vcp.12039. Epub 2013 Apr 23.
A chronic loss of canine α1 -proteinase inhibitor (cα1 -PI) into the gastrointestinal (GI) tract could change the systemic proteinase-proteinase inhibitor balance. Serum cα1 -PI concentrations have not been studied in dogs with well-defined GI diseases.
To further evaluate serum cα1 -PI concentrations in dogs with GI diseases, the objectives of this study were to (1) analytically validate a previously developed fecal cα1 -PI immunoassay to determine serum concentrations, (2) determine a population-based reference interval (RI) and assess the clinical utility, (3) determine stability of serum cα1 -PI, (4) determine the intra-individual variation in healthy dogs, and (5) determine the clinically relevant magnitude of change of serum cα1 -PI.
Prestudy validation of the (125) I-cα1 -PI immunoassay included linearity, spiking recovery, and intra- and inter-assay precision. A RI was calculated with samples of healthy dogs. Stability at -20°C was tested on 36 samples. Intra-individual variation was assessed using samples collected from 11 healthy dogs over a 12-week period.
The cα1 -PI radioimmunoassay (RIA) was linear, accurate, precise, and reproducible. Serum cα1 -PI decreased by 11% after one year at -20°C. Analytical, intra-individual, inter-individual, and total variation were 6.4, 9.9, 9.0, and 25.3%, respectively. The RI for serum cα1 -PI was 732-1802 mg/L (n = 87); there were no differences between sex and age groups. The index of individuality was 1.31. As analytical variation was > ½ inter-individual variation, the minimum critical difference was not determined.
The results of this study provide the basis for further evaluating serum cα1 -PI in dogs with GI disease. Using a population-based RI for serum cα1 -PI appears to be appropriate.
犬α1 -蛋白酶抑制剂(cα1 -PI)长期流失至胃肠道可能会改变全身蛋白酶-蛋白酶抑制剂平衡。血清cα1 -PI浓度尚未在患有明确胃肠道疾病的犬中进行研究。
为进一步评估患有胃肠道疾病犬的血清cα1 -PI浓度,本研究的目的是:(1)分析验证先前开发的粪便cα1 -PI免疫测定法以测定血清浓度;(2)确定基于群体的参考区间(RI)并评估临床实用性;(3)确定血清cα1 -PI的稳定性;(4)确定健康犬的个体内变异;(5)确定血清cα1 -PI临床上相关的变化幅度。
(125)I-cα1 -PI免疫测定法的预研究验证包括线性、加标回收率以及批内和批间精密度。用健康犬的样本计算参考区间。在36个样本上测试了-20°C下的稳定性。使用11只健康犬在12周内采集的样本评估个体内变异。
cα1 -PI放射免疫测定法(RIA)具有线性、准确性、精密度和可重复性。血清cα1 -PI在-20°C下保存一年后下降了11%。分析变异、个体内变异、个体间变异和总变异分别为6.4%、9.9%、9.0%和25.3%。血清cα1 -PI的参考区间为732 - 1802 mg/L(n = 87);性别和年龄组之间无差异。个体指数为1.31。由于分析变异>个体间变异的一半,因此未确定最小临界差异。
本研究结果为进一步评估患有胃肠道疾病犬的血清cα1 -PI提供了依据。使用基于群体的血清cα1 -PI参考区间似乎是合适的。
