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64^Cu-bis(thiosemicarbazone) Complexes for Delineating Myocardial Hypoxia

机译:用于描述心肌缺氧的64 ^ Cu-双(thiosemicarbazone)配合物

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摘要

Coronary artery disease and coronary microvascular disease, as well as acute myocardial infarction and adverse remodelling are often characterised by tissue hypoxia. They benefit from the earliest possible diagnosis and treatment. Positron Emission Tomography (PET) is a highly sensitive technique capable of non-invasively imaging the biochemistry of the body, with the capacity to track biochemical changes over time. In this project, we aim to characterise a series of novel PET imaging agents able to identify and characterise hypoxic myocardium with a view to optimising the treatment of a range of cardiovascular diseases. Bisthiosemicarbazone (BTSC) ligands readily chelate positron emitting copper isotopes, and have been demonstrated to selectively accumulate in hypoxic tissue in vitro, in vivo, and in isolated perfused hearts. While the lead compound Cu-ATSM has been widely investigated, a library of related Cu-BTSC complexes exist which may have better pharmacokinetics and selectivity for application in cardiology. We employed isolated ventricular myocytes and isolated perfused hearts to screen a number of 64Cu-labelled BTSC complexes, to assess their hypoxia selectivity and accumulation in cardiac tissue. For this purpose we developed a novel incubation chamber for maintaining isolated cardiomyocytes under hypoxic conditions. We also developed a novel gamma radiation detector array comprising three Na/1 y-detectors, for monitoring the flow of radioactivity through isolated perfused hearts in real-time. We have demonstrated the hypoxia selective accumulation of 6 Cu-ATSM in adult rat ventricular myocytes (ARVM) incubated under hypoxic conditions. Using isolated perfused hearts we demonstrated that all 64Cu-BTSC readily accumulate within cardiac tissue in an oxygen-dependent manner.We have demonstrated the hypoxia selective accumulation of 64Cu-ATSM in adult rat ventricular myocytes (ARVM) incubated under hypoxic conditions. Using isolated perfused hearts we demonstrated that all 64Cu-BTSC readily accumulate within cardiac tissue in an oxygen-dependent manner. We also identified a relationship between the structure of Cu-BTSCs and their tissue retention, with lower molecular weight complexes providing the greatest hypoxic to oxygenated tissue contrast. In doing this we have identified two complexes, Cu-ATS and Cu-CTS, which could potentially supersede Cu-ATSM as the agent of choice for imaging the hypoxic myocardium.
机译:冠状动脉疾病和冠状动脉微血管疾病以及急性心肌梗塞和不良重塑通常以组织缺氧为特征。他们受益于最早的诊断和治疗。正电子发射断层扫描(PET)是一种高度敏感的技术,能够对人体的生物化学进行非侵入性成像,并具有随时间推移追踪生物化学变化的能力。在该项目中,我们旨在表征一系列能够识别和表征缺氧心肌的新型PET显像剂,以优化一系列心血管疾病的治疗。双硫半脲(BTSC)配体容易螯合发射正电子的铜同位素,并已证明在体外,体内和离体的灌注心脏中选择性地积聚在低氧组织中。尽管对铅化合物Cu-ATSM进行了广泛研究,但存在相关的Cu-BTSC复合物库,该库可能具有更好的药代动力学和选择性,可用于心脏病学。我们采用离体的心室心肌细胞和离体的灌注心脏来筛选许多64Cu标记的BTSC复合物,以评估它们的缺氧选择性和在心脏组织中的蓄积。为了这个目的,我们开发了一种新型的培养箱,用于在缺氧条件下维持分离的心肌细胞。我们还开发了包括三个Na / 1 y探测器的新型伽马辐射探测器阵列,用于实时监测通过孤立的灌注心脏的放射流。我们已经证明了在缺氧条件下培养的成年大鼠心室肌细胞(ARVM)中6 Cu-ATSM的低氧选择性积累。使用孤立的灌注心脏,我们证明了所有64Cu-BTSC都容易以氧气依赖的方式在心脏组织中蓄积。我们已经证明了在缺氧条件下培养的成年大鼠心室肌细胞(ARVM)中64Cu-ATSM的低氧选择性积累。使用孤立的灌注心脏,我们证明了所有64Cu-BTSC都容易以氧依赖性方式在心脏组织内蓄积。我们还确定了Cu-BTSCs的结构与其组织保留之间的关系,其中较低分子量的复合物可提供最大程度的低氧至氧合的组织对比。在此过程中,我们确定了两种复合物Cu-ATS和Cu-CTS,它们有可能取代Cu-ATSM,成为低氧心肌成像的首选药物。

著录项

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    Handley Maxwell;

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  • 年度 2012
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  • 原文格式 PDF
  • 正文语种 eng
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