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用于线粒体疾病临床试验的小鼠研究:哈林顿鼠的高脂肪饮食。

Mouse studies to shape clinical trials for mitochondrial diseases: high fat diet in Harlequin mice.

机构信息

INSERM, U676, Paris, France.

出版信息

PLoS One. 2011;6(12):e28823. doi: 10.1371/journal.pone.0028823. Epub 2011 Dec 13.

Abstract

BACKGROUND

Therapeutic options in human mitochondrial oxidative phosphorylation (OXPHOS) diseases have been poorly evaluated mostly because of the scarcity of cohorts and the inter-individual variability of disease progression. Thus, while a high fat diet (HFD) is often recommended, data regarding efficacy are limited. Our objectives were 1) to determine our ability to evaluate therapeutic options in the Harlequin OXPHOS complex I (CI)-deficient mice, in the context of a mitochondrial disease with human hallmarks and 2) to assess the effects of a HFD.

METHODS AND FINDINGS

Before launching long and expensive animal studies, we showed that palmitate afforded long-term death-protection in 3 CI-mutant human fibroblasts cell lines. We next demonstrated that using the Harlequin mouse, it was possible to draw solid conclusions on the efficacy of a 5-month-HFD on neurodegenerative symptoms. Moreover, we could identify a group of highly responsive animals, echoing the high variability of the disease progression in Harlequin mice.

CONCLUSIONS

These results suggest that a reduced number of patients with identical genetic disease should be sufficient to reach firm conclusions as far as the potential existence of responders and non responders is recognized. They also positively prefigure HFD-trials in OXPHOS-deficient patients.

摘要

背景

人类线粒体氧化磷酸化(OXPHOS)疾病的治疗选择评估效果不佳,主要是因为疾病进展的个体间变异性和队列稀少。因此,尽管经常推荐高脂肪饮食(HFD),但关于疗效的数据有限。我们的目标是 1)确定我们在具有人类特征的线粒体疾病背景下评估 Harlequin OXPHOS 复合物 I(CI)缺陷型小鼠治疗选择的能力,2)评估 HFD 的影响。

方法和发现

在开展长期和昂贵的动物研究之前,我们表明棕榈酸在 3 种 CI 突变的人类成纤维细胞系中可提供长期的死亡保护。我们接下来证明,使用 Harlequin 小鼠,可以就 HFD 对神经退行性症状的 5 个月疗效得出可靠结论。此外,我们可以鉴定出一组高度敏感的动物,与 Harlequin 小鼠疾病进展的高度变异性相呼应。

结论

这些结果表明,只要认识到存在应答者和无应答者,具有相同遗传疾病的患者数量减少,就应该足以得出坚定的结论。它们还积极预示着 OXPHOS 缺陷患者的 HFD 试验。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ffb4/3236768/e9589a726e33/pone.0028823.g001.jpg

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