Jonas Bergquist, Gökhan Baykut, Maria Bergquist, Matthias Witt, Franz-Josef Mayer, Doan Baykut
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However, in order to fully exploit and also validate these findings there is a definite need for unambiguous identification of the differences between different etiologies at molecular level. In this study, samples representative for the aortic valve disease and coronary heart disease were prepared, tryptically digested, and analyzed using an FT-ICR MS that allowed collision-induced dissociation (CID) of selected classifier masses. By using the fragment spectra, proteins were identified by database searches. For comparison and further validation, classifier masses were also fragmented and analyzed using HPLC-/Matrix-assisted laser desorption ionization (MALDI) time-of-flight/time-of-flight (TOF/TOF) mass spectrometry. Desmin and lumican precursor were examples of proteins found in aortic samples at higher abundances than in coronary samples. Similarly, adenylate kinase isoenzyme was found in coronary samples at a higher abundance. 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Right atrial appendages from 10 patients with hemodynamically significant isolated aortic valve disease and from 10 patients with isolated symptomatic coronary heart disease were collected during elective cardiac surgery. As presented in an earlier study by our group (Baykut et al., 2006), both disease forms showed clearly different pattern distribution characteristics. Interesting enough, the classification patterns could be used for correctly sorting unknown test samples in their correct categories. However, in order to fully exploit and also validate these findings there is a definite need for unambiguous identification of the differences between different etiologies at molecular level. In this study, samples representative for the aortic valve disease and coronary heart disease were prepared, tryptically digested, and analyzed using an FT-ICR MS that allowed collision-induced dissociation (CID) of selected classifier masses. 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引用次数: 5
摘要
采用高效液相色谱(HPLC)/傅立叶变换离子回旋共振质谱(FT-ICR MS)研究了两种不同病因心力衰竭心肌组织的蛋白质组学特征。本文收集了10例有血流动力学意义的孤立性主动脉瓣疾病患者和10例孤立性症状性冠心病患者在择期心脏手术中的右心房附件。正如我们小组早期的一项研究(Baykut et al., 2006)所述,这两种疾病表现出明显不同的模式分布特征。有趣的是,分类模式可以用于将未知测试样本正确地分类到正确的类别中。然而,为了充分利用和验证这些发现,明确需要在分子水平上明确识别不同病因之间的差异。在本研究中,制备了具有代表性的主动脉瓣疾病和冠心病样本,进行了胰消化,并使用FT-ICR MS进行了分析,该MS允许对选定的分类块进行碰撞诱导解离(CID)。利用片段光谱,通过数据库检索对蛋白质进行鉴定。为了比较和进一步验证,分类器质量也被碎片化,并使用高效液相色谱/基质辅助激光解吸电离(MALDI)飞行时间/飞行时间(TOF/TOF)质谱法进行分析。Desmin和lumican前体是在主动脉样本中发现的比在冠状动脉样本中丰度更高的蛋白质的例子。同样,在冠状动脉样品中发现腺苷酸激酶同工酶的丰度较高。所描述的方法也可用于寻找用于诊断目的的血浆或血清中的特定生物标志物。
Human myocardial protein pattern reveals cardiac diseases.
Proteomic profiles of myocardial tissue in two different etiologies of heart failure were investigated using high performance liquid chromatography (HPLC)/Fourier transform ion cyclotron resonance mass spectrometry (FT-ICR MS). Right atrial appendages from 10 patients with hemodynamically significant isolated aortic valve disease and from 10 patients with isolated symptomatic coronary heart disease were collected during elective cardiac surgery. As presented in an earlier study by our group (Baykut et al., 2006), both disease forms showed clearly different pattern distribution characteristics. Interesting enough, the classification patterns could be used for correctly sorting unknown test samples in their correct categories. However, in order to fully exploit and also validate these findings there is a definite need for unambiguous identification of the differences between different etiologies at molecular level. In this study, samples representative for the aortic valve disease and coronary heart disease were prepared, tryptically digested, and analyzed using an FT-ICR MS that allowed collision-induced dissociation (CID) of selected classifier masses. By using the fragment spectra, proteins were identified by database searches. For comparison and further validation, classifier masses were also fragmented and analyzed using HPLC-/Matrix-assisted laser desorption ionization (MALDI) time-of-flight/time-of-flight (TOF/TOF) mass spectrometry. Desmin and lumican precursor were examples of proteins found in aortic samples at higher abundances than in coronary samples. Similarly, adenylate kinase isoenzyme was found in coronary samples at a higher abundance. The described methodology could also be feasible in search for specific biomarkers in plasma or serum for diagnostic purposes.