Altered microheterogeneity at several N-glycosylation sites in OPSCC in constant protein expression conditions

IF 2.5 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Amy Dickinson, Sakari Joenväärä, Tiialotta Tohmola, Jutta Renkonen, Petri Mattila, Timo Carpén, Antti Mäkitie, Suvi Silén
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Abstract

Protein glycosylation responds sensitively to disease states. It is implicated in every hallmark of cancer and has recently started to be considered as a hallmark itself. Changes in N-glycosylation microheterogeneity are more dramatic than those of protein expression due to the non-template nature of protein glycosylation. This enables their potential use in serum-based diagnostics. Here, we perform glycopeptidomics on serum from patients with oropharyngeal squamous cell carcinoma (OPSCC), compared to controls and comparing between cancers based on etiology (human papilloma virus- positive or negative). Using MS2, we then targeted glycoforms, significantly different between the groups, to identify their glycopeptide compositions. Simultaneously we investigate the same serum proteins, comparing whether N-glycosylation changes reflect protein-level changes. Significant glycoforms were identified from proteins such as alpha-1-antitrypsin (SERPINA1), haptoglobin, and different immunoglobulins. SERPINA1 had glycovariance at 2 N-glycosylation sites, that were up to 35 times more abundant in even early-stage OPSCCs, despite minimal differences between SERPINA1 protein levels between groups. Some identified glycoforms' fold changes (FCs) were in line with serum protein level FCs, others were less abundant in early-stage cancers but with great variance in higher-stage cancers, such as on immunoglobulin heavy constant gamma 2, despite no change in protein levels. Such findings indicate that glycovariant analysis might be more beneficial than proteomic analysis, which is yet to be fruitful in the search for biomarkers. Highly sensitive glycopeptide changes could potentially be used in the future for cancer screening. Additionally, characterizing the glycopeptide changes in OPSCC is valuable in the search for potential therapeutic targets.

Abstract Image

恒定蛋白表达条件下 OPSCC 中多个 N-糖基化位点的微异质性改变
蛋白质糖基化对疾病状态反应敏感。它与癌症的每一个特征都有关联,最近它本身也开始被认为是一种特征。由于蛋白质糖基化的非模板性,N-糖基化微异质性的变化比蛋白质表达的变化更剧烈。这使它们有可能用于基于血清的诊断。在这里,我们对口咽鳞状细胞癌(OPSCC)患者的血清进行了糖肽组学研究,与对照组进行了比较,并根据病因(人类乳头状瘤病毒阳性或阴性)对不同癌症进行了比较。然后,我们利用 MS2,针对组间差异显著的糖型,确定它们的糖肽组成。同时,我们对相同的血清蛋白进行研究,比较 N-糖基化的变化是否反映了蛋白质水平的变化。我们从α-1-抗胰蛋白酶(SERPINA1)、隐球蛋白和不同的免疫球蛋白等蛋白质中发现了重要的糖型。SERPINA1在2个N-糖基化位点上存在糖变异,在早期OPSCC中的含量甚至高达35倍,尽管不同组间的SERPINA1蛋白水平差异极小。一些已发现的糖基化形式的折叠变化(FC)与血清蛋白水平的折叠变化一致,而另一些糖基化形式在早期癌症中含量较低,但在晚期癌症中却有很大差异,如免疫球蛋白重常数γ2上的糖基化形式,尽管蛋白质水平没有变化。这些发现表明,糖变异分析可能比蛋白质组分析更有益,而蛋白质组分析在寻找生物标记物方面尚未取得成果。高灵敏度的糖肽变化有可能在未来用于癌症筛查。此外,确定 OPSCC 中糖肽变化的特征对于寻找潜在的治疗靶点也很有价值。
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来源期刊
FASEB bioAdvances
FASEB bioAdvances Multiple-
CiteScore
5.40
自引率
3.70%
发文量
56
审稿时长
10 weeks
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