| 论文题目: | Dysfunction of microtubule-associated proteins of MAP2/tau family in prion disease |
|---|---|
| 作者: | Zhang, J; Dong, XP |
| 联系作者: | Dong, XP |
| 刊物名称: | PRION |
| 期: | 4 |
| 卷: | 6 |
| 页: | 334-338 |
| 年份: | 2012 |
| 影响因子: | 2.85 |
| 论文下载: | 下载地址 |
| 摘要: | The aggregation of PrPSc is thought to be crucial for the neuropathology of prion diseases. A growing body of evidence demonstrates that the perturbation of the microtubule network contributes to PrPSc-mediated neuro-degeneration. Microtubules are a component of the cytoskeleton and play a central role in organelle transport, axonal elongation and cellular architecture in neurons. The polymerization, stabilization, arrangement of microtubules can be modulated by interactions with a series of microtubule-associated proteins (MAPs). Recent studies have proposed the abnormal alterations of two major microtubule-associated proteins, tau and MAP2, in the brain tissues of naturally occurred and experimental human and animal prion diseases. Increased total tau protein and hyper-phosphorylation of tau at multiple residues are observed at the terminal stage of prion disease. The abnormal aggregation of tau protein disturbs its binding ability to microtubules and affects the microtubule dynamic. Significantly downregulated MAP2 is detected in the brain tissues of scrapie-infected hamsters and PrP106-126 treated cells, which corresponds well with the remarkably low levels of tubulin. In conclusion, dysfunction of MAP2/tau family leads to disruption of microtubule structure and impairment of axonal transport, and eventually triggers apoptosis in neurons, which becomes an essential pathway for prion to induce the neuropathology. |
京公网安备 11010502044263号