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首页> 外文期刊>Nature reviews. Neurology >Neuroimaging in frontotemporal lobar degeneration - Predicting molecular pathology
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Neuroimaging in frontotemporal lobar degeneration - Predicting molecular pathology

机译:额颞叶变性的神经影像学-预测分子病理学

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Frontotemporal lobar degeneration (FTLD) encompasses a group of diseases characterized by neuronal loss and gliosis of the frontal and temporal lobes. Almost all cases of FTLD can be classified into three categories on the basis of deposition of one of three abnormal proteins: the microtubule-associated protein tau, TAR DNA-binding protein 43, or fused in sarcoma. The specific diagnoses within each of these three categories are further differentiated by the distribution and morphological appearance of the protein-containing inclusions. Future treatments are likely to target these abnormal proteins; the clinical challenge, therefore, is to be able to predict molecular pathology during life. Clinical diagnosis alone has had variable success in helping to predict pathology, and is particularly poor in the diagnosis of behavioral variant frontotemporal dementia, which can be associated with all three abnormal proteins. Consequently, other biomarkers of disease are needed. This Review highlights how patterns of atrophy assessed on MRI demonstrate neuroanatomical signatures of the individual FTLD pathologies, independent of clinical phenotype. The roles of these patterns of atrophy as biomarkers of disease, and their potential to help predict pathology during life in patients with FTLD, are also discussed.
机译:额颞叶变性(FTLD)涵盖了一组以额叶和颞叶神经元丢失和神经胶质细胞增生为特征的疾病。根据三种异常蛋白之一的沉积,几乎所有FTLD病例都可以分为三类:微管相关蛋白tau,TAR DNA结合蛋白43或融合在肉瘤中。通过包含蛋白质的内含物的分布和形态外观,进一步区分了这三类中的特定诊断。未来的治疗可能针对这些异常蛋白。因此,临床上的挑战是能够预测生命中的分子病理。单独的临床诊断在帮助预测病理方面取得了成功,并且在行为变异额颞痴呆的诊断方面特别差,后者可能与所有三种异常蛋白有关。因此,需要其他疾病的生物标记。这篇综述着重介绍了在MRI上评估的萎缩模式如何显示单个FTLD病理的神经解剖学特征,而与临床表型无关。还讨论了这些萎缩模式作为疾病的生物标志物的作用,以及它们在预测FTLD患者生命过程中有助于预测病理学的潜力。

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