Correlation between Olink and SomaScan proteomics platforms in adults with a Fontan circulation

IF 0.8 Q4 CARDIAC & CARDIOVASCULAR SYSTEMS
Ismael Z. Assi , Michael J. Landzberg , Kristian C. Becker , David Renaud , Fernando Baraona Reyes , David M. Leone , Mark Benson , Miriam Michel , Robert E. Gerszten , Alexander R. Opotowsky
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Abstract

Background

High-throughput proteomics platforms using aptamers (SomaScan) or proximity extension assay (Olink) provide novel opportunities for improving diagnostic and risk stratification tools in cardiovascular diseases, including understudied congenital heart diseases. The correlation between these proteomics approaches has not yet been studied among individuals with a Fontan circulation.

Objective

The correlation of plasma protein measurements between SomaScan and Olink platforms was evaluated in adults with a Fontan circulation.

Methods

We measured 491 proteins in plasma of 71 adults with a Fontan circulation using Olink and SomaScan. Missing Olink measurements (0.13%, 47/34,861) were imputed using non-parametric imputation. Spearman's rank correlation coefficient for absolute values of protein expression between platforms was calculated. Protein correlation frequencies were compared to 3 cohorts reported in the literature using Pearson's Chi-squared test of independence.

Results

Overall, protein correlations between Olink and SomaScan measurements were moderately strong for most proteins, (rho > 0.4 for 57.2%), but with substantial variability (median correlation = 0.457, IQR = 0.538). The distribution of protein correlations was qualitatively similar to published literature in non-Fontan cohorts. Both Olink and SomaScan identified proteins with sex-based differences; both identified differences in myostatin and leptin, but each identified additional nonoverlapping sexually dimorphic proteins (n = 14 Olink, n = 5 SomaScan).

Conclusions

In adults with a Fontan circulation, correlations between plasma proteins measured by Olink and SomaScan varied widely, approximately in line with prior reports in other populations. While these tools may be uniquely useful to generate hypotheses, specifically regarding potential molecular mechanisms, more definitive inference requires independent validation.

Abstract Image

成人Fontan循环患者中Olink和SomaScan蛋白组学平台的相关性
使用适体(SomaScan)或邻近扩展测定(Olink)的高通量蛋白质组学平台为改善心血管疾病(包括未充分研究的先天性心脏病)的诊断和风险分层工具提供了新的机会。这些蛋白质组学方法之间的相关性尚未在Fontan循环个体中进行研究。目的评价成人Fontan循环患者血浆蛋白水平与SomaScan和Olink平台的相关性。方法应用Olink和SomaScan检测了71例Fontan循环成人血浆中的491种蛋白。缺失的Olink测量值(0.13%,47/34,861)使用非参数估算。计算平台间蛋白表达绝对值的Spearman秩相关系数。使用Pearson卡方独立性检验将蛋白相关频率与文献中报道的3个队列进行比较。结果总的来说,对于大多数蛋白质,Olink和SomaScan测量之间的蛋白质相关性中等强,(rho >;0.4为57.2%),但存在显著的可变性(中位相关= 0.457,IQR = 0.538)。在非fontan队列中,蛋白质相关性的分布在质量上与已发表的文献相似。Olink和SomaScan都鉴定出了基于性别差异的蛋白质;两者都发现了肌肉生长抑制素和瘦素的差异,但都发现了额外的非重叠性二态蛋白(n = 14 Olink, n = 5 SomaScan)。结论:在Fontan循环的成年人中,Olink和SomaScan测定的血浆蛋白之间的相关性差异很大,与先前在其他人群中的报道大致一致。虽然这些工具可能是唯一有用的产生假设,特别是关于潜在的分子机制,更明确的推断需要独立的验证。
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
International journal of cardiology. Congenital heart disease
International journal of cardiology. Congenital heart disease Cardiology and Cardiovascular Medicine
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83 days
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