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亨廷顿病患者和转基因大鼠具有相似的分解代谢前血清代谢物特征
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作者 Underwood B.R. Broadhurst D. +2 位作者 dunn w.b. D.C. Rubinsztein 赵天智 《世界核心医学期刊文摘(神经病学分册)》 2006年第9期32-33,共2页
There has been considerable progress recently towards developing therapeutic strategies for Huntington’s disease (HD), with several compounds showing beneficial effects in transgenic mouse models. However, human tria... There has been considerable progress recently towards developing therapeutic strategies for Huntington’s disease (HD), with several compounds showing beneficial effects in transgenic mouse models. However, human trials in HD are difficult, costly and time-consuming due to the slow disease course, insidious onset and patient-to-patient variability. Identification of molecular biomarkers associated with disease progression will aid the development of effective therapies by allowing further validation of animal models and by providing hopefully more sensitive measures of disease progression. Here, we apply metabolic profiling by gas chromatography-time-of-flight-mass spectrometry to serum samples from human HD patients and a transgenic mouse model in a hypothesis-generating search for disease biomarkers. We observed clear differences in metabolic profiles between transgenic mice and wild-type littermates, with a trend for similar differences in human patients and control subjects. Thus, the metabolites responsible for distinguishing transgenic mice also comprised a metabolic signature tentatively associated with the human disease. The candidate biomarkers composing this HD-associated metabolic signature in mouse and humans are indicative of a change to a pro-catabolic phenotype in early HD preceding symptom onset, with changes in various markers of fatty acid breakdown (including glycerol and malonate) and also in certain aliphatic amino acids. Our data raise the prospect of a robust molecular definition of progression of HD prior to symptom onset, and if validated in a genuinely prospective fashion these biomarker trajectories could facilitate the development of useful therapies for this disease. 展开更多
关键词 转基因大鼠模型 血清样本 代谢物 分子生物学标记物 分解代谢 相似 病患 疾病进展
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