首页> 外文期刊>Taiwan Veterinary Journal >TELETHONIN AS AN EARLY IMMUNOHISTOCHEMICAL MARKER IN LIGATION-INDUCED ISCHEMIC MYOCARDIAL INJURY
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TELETHONIN AS AN EARLY IMMUNOHISTOCHEMICAL MARKER IN LIGATION-INDUCED ISCHEMIC MYOCARDIAL INJURY

机译:Telethonin作为结扎诱导的缺血性心肌损伤的早期免疫组织化学标志物

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In this study, acute myocardial injuries or necrosis were experimentally induced in calves and pigs by ligation of either the left anterior descending coronary artery or left circumflex branch for 30min without reperfusion. Various antibodies directed to structural and functional proteins of the sarcomere, as well as activated proteinases, were employed in immunohistochemistry to compare for their potentials to detect early myocardial injury. For comparison, the histological criteria (designated as “Method A”) of cardiomyocyte necrosis such as nuclear pyknosis, sarcoplasmic fragmentation, flocculation, and/or the presence of a contraction band, and inflammatory infiltration were also scored. Additional criteria (designated “Method B”) of changes in late reversible stage of cell injury such as irregular nuclear shape or hyperchromasia, sarcomplasmic hypereosinophilia with either swelling or atrophy in diameter, and perinuclear vacuolation likely of swollen organelles, were also scored. In this setting, telethonin (T-cap), cardiac troponin I (cTnI), the current gold standard, and Method B, were superior to others in detecting ligation-induced ischemic injury. Other markers were either less specific, or less sensitive, or inconclusive for the current application. In conclusion, telethonin may serve as an early immunohistochemical marker in ligation-induced ischemic myocardial injury due to a combination of biomechanical stress, hypoxia, and possibly additional factor as matrix metalloproteinase activation.
机译:在这项研究中,通过连接左前期下降冠状动脉或左侧环形分支30min而无需再灌注,通过连接急性心肌损伤或坏死在犊牛和猪中进行实验诱导。免疫组织化学中使用针对Sarcomere的结构和功能蛋白以及活化的蛋白酶的各种抗体,以比较它们潜在检测早期心肌损伤的潜力。为了比较,还评分了心肌细胞坏死的组织学标准(指定为“方法A”),例如核细胞坏死,肌肉肌肉片段,絮凝和/或收缩带的存在,以及炎症浸润。还评分了诸如不规则的核形状或高速瘤细胞损伤或高速瘤细胞患者的细胞损伤的后期可逆阶段的变化的附加标准(指定的“方法B”)。在该设置中,Telethonin(T-Cap),心肌肌钙蛋白I(CTNI),目前的金标准和方法B,优于检测结扎诱导的缺血性损伤的其他。其他标记对于目前申请的特异性或更少的敏感性或不确定或不确定。总之,由于生物力学应力,缺氧和可能额外因素作为基质金属蛋白酶活化,即可作为结扎诱导的缺血性心肌损伤的早期免疫组化标志物。

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