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Metabolism of synthetic anaplerotic nutrients in pig heart.

机译:猪心脏中合成的前卫营养素的代谢。

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摘要

Nearly every enzymatic step required for the mitochondrial beta-oxidation of saturated and unsaturated fatty acids has been associated with an inherited metabolic disorder. The current treatment involves providing the majority of dietary fat as medium even-chain triglycerides for long-chain fatty acid oxidation disorders (FOD) or restricting dietary fat for medium- and short-chain FOD. In many cases, this treatment does not prevent the progressive deterioration of cardiac, muscular and/or retinal function. An initial clinical trial, replacing trioctanoin (medium even-chain triglyceride) in the diet by triheptanoin (medium odd-chain triglyceride), has demonstrated rapid and major clinical improvements in the treatment of long-chain FOD. The beneficial effects of triheptanoin have been ascribed to the anaplerotic property of pentanoate which is oxidized to propionyl-CoA and acetyl-CoA.; Current limitations of FOD therapy are: (i) there is no parenteral form to treat acute decompensation episodes and (ii) triheptanoin therapy is not suitable for medium-chain FOD. Pentanoate is a potentially better anaplerotic treatment for FOD because it can be used for all FOD. The goal of my study is to investigate the cardiac metabolism of pentanoate and beta-ketopentanoate (BKP), which might be used to treat acute decompensation episodes in FOD patients.; Two series of experiments using a live pig heart model and labeled substrates characterized the metabolism of pentanoate: (i) [1-13C]pentanoate (assessing the contribution of pentanoate to energy metabolism) and (ii) [3,4,5- 13C3]pentanoate and beta-keto[3,4,5-13C 3]pentanoate (assessing the efficiency as anaplerotic substrates). In the concentration range investigated (up to 1.5 mM), there was no alteration in cardiovascular parameters observed. I measured the labeling of the propionyl-CoA pathway using gas chromatography-mass spectrometry methods. The calculated total anaplerosis (enrichment ratio M3 succinyl-CoA/M3 propionyl-CoA) from pentanoate and BKP ranged from 6-10% of the citric acid cycle flux. This study paves the way to the preclinical testing of anaplerotic compounds in animal models of FOD before clinical trials are planned.
机译:饱和和不饱和脂肪酸的线粒体β-氧化所需的几乎每个酶促步骤都与遗传性代谢紊乱有关。目前的治疗方法包括为中链长链脂肪酸氧化紊乱(FOD)提供大部分膳食脂肪,以中链均匀甘油三酸酯为食,或为中链和短链FOD提供限制膳食脂肪。在许多情况下,这种治疗不能防止心脏,肌肉和/或视网膜功能的逐步恶化。一项初步的临床试验用三庚酸(中链奇数甘油三酯)代替了饮食中的三辛酸(中链甘油三酯),已证明在治疗长链FOD方面有快速而重大的临床改进。三庚酸的有益作用归因于戊酸酯的抗血管紧张作用,戊酸酯被氧化成丙酰-CoA和乙酰-CoA。 FOD治疗的当前局限性是:(i)没有肠胃外形式可以治疗急性代偿失调发作;(ii)三庚酸治疗不适用于中链FOD。戊酸可能是一种更好的FOD补血疗法,因为它可以用于所有FOD。我的研究目标是研究戊酸酯和β-酮戊酸酯(BKP)的心脏代谢,这些代谢可用于治疗FOD患者的急性代偿失调。使用活猪心脏模型和标记底物进行的两个系列实验表征了戊酸的代谢:(i)[1-13C]戊酸(评估戊酸对能量代谢的贡献)和(ii)[3,4,5- 13C3戊酸]和β-酮[3,4,5-13C 3]戊酸(评估其作为抗动脉粥样硬化底物的效率)。在所研究的浓度范围内(最高1.5 mM),没有观察到心血管参数的变化。我使用气相色谱-质谱法测量了丙酰辅酶A途径的标记。从戊酸酯和BKP计算得出的总动脉异常(富集比为M3琥珀酰-CoA / M3丙酰-CoA)占柠檬酸循环通量的6-10%。这项研究为在计划临床试验之前在FOD动物模型中进行抗动脉粥样硬化化合物的临床前测试铺平了道路。

著录项

  • 作者

    Yu, Lynn.;

  • 作者单位

    Case Western Reserve University (Health Sciences).;

  • 授予单位 Case Western Reserve University (Health Sciences).;
  • 学科 Health Sciences Nutrition.; Biology Physiology.
  • 学位 Ph.D.
  • 年度 2006
  • 页码 169 p.
  • 总页数 169
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 预防医学、卫生学;
  • 关键词

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