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缺血性心脏病伴收缩功能障碍患者中金属蛋白酶的失调。

Dysregulation of metalloproteins in ischemic heart disease patients with systolic dysfunction.

机构信息

H.E.J. Research Institute of Chemistry, International Center for Chemical and Biological Sciences, University of Karachi, Karachi 75270, Pakistan.

Department of Biological and Biomedical Sciences, Agha Khan University, Karachi 74800, Pakistan.

出版信息

Int J Biol Macromol. 2023 Mar 31;232:123435. doi: 10.1016/j.ijbiomac.2023.123435. Epub 2023 Jan 28.

Abstract

Ischemic heart disease (IHD) is the leading cause of mortality worldwide. Metalloproteins have been linked to human health and diseases. The molecular functions of metalloproteins in IHD is not well understood and require further exploration. The objective of this study was to find out the role of metalloproteins in the pericardial fluid of IHD patients having normal (EF > 45) and impaired (EF < 45) left ventricular ejection fraction (LVEF). IHD patients were grouped into two categories: LVEF<45 (n = 12) and LVEF >45 (n = 33). Pooled samples of pericardial fluid were fractionated by using ZOOM-isoelectric focusing (IEF) followed by further processing using one-dimensional gel electrophoresis (1D SDS-PAGE) and filter-aided sample preparation (FASP). Tryptic peptides of each fraction and differential bands were then analyzed by nano-LC-ESI-MS/MS. Protein identification was performed through a Mascot search engine using NCBI-Prot and SwissProt databases. A total of 1082 proteins including 154 metalloproteins were identified. In the differential bands, 60 metalloproteins were identified, while 115 metalloproteins were identified in all ZOOM-IEF fractions. Twelve differentially expressed metalloproteins were selected in the intense bands according to their molecular weight (MW) and isoelectric point (pI). The 12 differentially expressed metalloprotein includes ceruloplasmin, Prothrombin, Vitamin K-dependent protein, Fibulin-1, Ribosomal protein S6 kinase alpha-6, nidogen, partial, Serum albumin, Hemopexin, C-reactive protein, Serum amyloid P-component, and Intelectin-1 protein which were all up-regulated while serotransferrin is the only metalloprotein that was down-regulated in impaired (LVEF<45) group. Among the metalloproteins, Zn-binding proteins are 36.5 % followed by Ca-binging 32.2 %, and Fe-binging 12.2 %. KEGG, pathway analysis revealed the association of ceruloplasmin and serotransferrin with the ferroptosis pathway. In conclusion, 154 metalloproteins were identified of them the Zn-binding protein followed by Ca-binding and Fe-binding proteins were the most abundant metalloproteins. The two metalloproteins, the Cu-binding protein ceruloplasmin, and Fe-binding protein serotransferrin are involved in the ferroptosis pathway, an iron-dependent form of regulated cell death that has been linked to cardiac pathology, especially in IHD patients having impaired systolic (LVEF<45) dysfunction. However, further research is required to validate these findings.

摘要

缺血性心脏病 (IHD) 是全球死亡的主要原因。金属蛋白与人类健康和疾病有关。金属蛋白在 IHD 中的分子功能尚不清楚,需要进一步探索。本研究的目的是探讨金属蛋白在左心室射血分数正常 (EF>45) 和受损 (EF<45) 的 IHD 患者的心包液中的作用。将 IHD 患者分为两组:LVEF<45(n=12)和 LVEF>45(n=33)。使用 ZOOM-等电聚焦 (IEF) 对心包液进行分组,然后使用一维凝胶电泳 (1D SDS-PAGE) 和过滤辅助样品制备 (FASP) 进一步处理。然后通过纳升 LC-ESI-MS/MS 分析每个馏分的胰蛋白酶肽和差异带。通过 NCBI-Prot 和 SwissProt 数据库使用 Mascot 搜索引擎进行蛋白质鉴定。共鉴定了 1082 种蛋白质,包括 154 种金属蛋白。在差异带中,鉴定出 60 种金属蛋白,而在所有 ZOOM-IEF 馏分中鉴定出 115 种金属蛋白。根据分子量 (MW) 和等电点 (pI),在强带中选择了 12 种差异表达的金属蛋白。根据分子量 (MW) 和等电点 (pI),在强带中选择了 12 种差异表达的金属蛋白。根据分子量 (MW) 和等电点 (pI),在强带中选择了 12 种差异表达的金属蛋白。根据分子量 (MW) 和等电点 (pI),在强带中选择了 12 种差异表达的金属蛋白。根据分子量 (MW) 和等电点 (pI),在强带中选择了 12 种差异表达的金属蛋白。根据分子量 (MW) 和等电点 (pI),在强带中选择了 12 种差异表达的金属蛋白。根据分子量 (MW) 和等电点 (pI),在强带中选择了 12 种差异表达的金属蛋白。根据分子量 (MW) 和等电点 (pI),在强带中选择了 12 种差异表达的金属蛋白。根据分子量 (MW) 和等电点 (pI),在强带中选择了 12 种差异表达的金属蛋白。根据分子量 (MW) 和等电点 (pI),在强带中选择了 12 种差异表达的金属蛋白。根据分子量 (MW) 和等电点 (pI),在强带中选择了 12 种差异表达的金属蛋白。在强烈的带中,选择了 12 种差异表达的金属蛋白,根据其分子量 (MW) 和等电点 (pI)。在差异表达的金属蛋白中,有 12 种金属蛋白被鉴定出来,包括铜结合蛋白 ceruloplasmin 和铁结合蛋白转铁蛋白。ceruloplasmin 和 serotransferrin 与 ferroptosis 途径相关。结论:共鉴定了 154 种金属蛋白,其中锌结合蛋白最多,其次是钙结合蛋白和铁结合蛋白。两种金属蛋白,铜结合蛋白 ceruloplasmin 和铁结合蛋白转铁蛋白,参与铁依赖性的细胞死亡形式,与心脏病理学有关,特别是在左心室射血分数受损 (LVEF<45) 功能障碍的 IHD 患者中。然而,需要进一步的研究来验证这些发现。

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