Modified throughput ninhydrin method for the qualitative assessment of dietary protein absorption in pig plasma.

IF 2.5 Q3 BIOCHEMICAL RESEARCH METHODS
Biology Methods and Protocols Pub Date : 2024-10-25 eCollection Date: 2024-01-01 DOI:10.1093/biomethods/bpae078
Kateryna Pierzynowska, Kamil Zaworski, Piotr Wychowański, Janine Donaldson, Jarosław Woliński, Drucy Borowitz, Robert Gallotto, Stefan Pierzynowski
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Abstract

Protein maldigestion and malabsorption lead to malnutrition and are a feature of exocrine pancreatic insufficiency (EPI). Although it is the current standard, measurement of nitrogen in stool to assess protease activity is indirect. Up to 80% of hydrolysed proteins appear in blood in the form of peptides, so we developed a method to measure peptide-derived amino acids in plasma as a relevant measure of proteolysis, verified its accuracy, precision, and linearity, and validated it in a porcine model. We modified a ninhydrin method. Large proteins were eliminated from plasma with 10 kDa-cut-off centrifugal filters. Free and total amino acids were measured in permeate before and after its hydrolysis. Peptide-derived amino acids were quantified by subtracting free amino acids from total amino acids. We verified the method in vitro and by comparing results in healthy and EPI pigs. The accuracy of the analysis was close to 100%, with excellent precision (mean relative standard deviation for low, medium, and high amino acid levels = 0.88%) and with stringent linearity (r2  = 0.986, %RE = 5.23). The high-throughput ninhydrin method detected levels of peptide-derived amino acids in vivo with maximal changes seen approximately 2 hours postprandially in young pigs. The AUC and Cmax were significantly higher in healthy compared to EPI pigs (P = .0026 and P = .0037, respectively). The high-throughput ninhydrin method is a sensitive, reliable, and practical method for the estimation of dietary peptide-derived amino acids. This assay endpoint could serve as a direct biomarker of protein digestion and absorption.

用于定性评估猪血浆中日粮蛋白质吸收的改良吞吐量茚三酮法。
蛋白质消化不良和吸收不良会导致营养不良,是胰腺外分泌功能不全(EPI)的一个特征。测量粪便中的氮来评估蛋白酶活性虽然是目前的标准,但却是间接的。高达 80% 的水解蛋白以肽的形式出现在血液中,因此我们开发了一种测量血浆中肽衍生氨基酸的方法,作为蛋白水解的相关测量指标,验证了该方法的准确性、精确性和线性,并在猪模型中进行了验证。我们改进了茚三酮法。用 10 kDa 截断离心过滤器去除血浆中的大分子蛋白质。在水解前后测量渗透液中的游离氨基酸和总氨基酸。通过从氨基酸总量中减去游离氨基酸来量化肽衍生氨基酸。我们在体外验证了这种方法,并比较了健康猪和 EPI 猪的结果。分析的准确度接近 100%,具有极高的精确度(低、中、高氨基酸水平的平均相对标准偏差 = 0.88%)和严格的线性度(r2 = 0.986,%RE = 5.23)。高通量茚三酮法检测体内肽源氨基酸水平,幼猪餐后约 2 小时变化最大。健康猪的 AUC 和 Cmax 明显高于 EPI 猪(P = .0026 和 P = .0037)。高通量茚三酮法是一种灵敏、可靠、实用的膳食肽源氨基酸测定方法。该检测终点可作为蛋白质消化和吸收的直接生物标志物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Biology Methods and Protocols
Biology Methods and Protocols Agricultural and Biological Sciences-Agricultural and Biological Sciences (all)
CiteScore
3.80
自引率
2.80%
发文量
28
审稿时长
19 weeks
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