TDP43 的细胞质聚集以及与 rTg4510 小鼠 tauopathy 模型中 tau 和 α-synuclein 积累的地形相关性。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-10-01 DOI:10.1093/jnen/nlae063
Yutaro Nakayama, James K Chambers, Yuta Takaichi, Kazuyuki Uchida
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引用次数: 0

摘要

在TDP43蛋白病患者中,磷酸化TDP43(p-TDP43)会在神经元的细胞质中积聚。p-TDP43在tauopathy和α-synucleinopathy患者中的积累也有报道。我们研究了过量表达人类突变型tau(P301L)并表现出高磷酸化tau(hp-tau)和磷酸化αSyn(p-αSyn)积累的rTg4510小鼠大脑中p-TDP43积累的时空变化。免疫组化结果显示,在神经元的细胞质中发现了p-TDP43聚集体,并且随着年龄的增长而增加。p-TDP43 聚集细胞的数量与 hp-tau 和 p-αSyn 聚集细胞的数量呈明显的正相关。多西环素治疗抑制了人类突变体 tau(P301L)的表达,减少了 p-TDP43、hp-tau 和 p-αSyn 的聚集。在hp-tau和p-αSyn高度聚集的区域发现了抗蛋白酶K的p-TDP43聚集体。对沙可糖不溶性部分进行的 Western 印迹显示了单体 TDP43 和 p-TDP43 的条带。这些结果表明,小鼠p-TDP43的积累与rTg4510小鼠大脑中人类突变体tau(P301L)的积累有关。hp-tau和p-αSyn的积累可能会促进对蛋白酶K有抗性的sarkosyl-不溶性p-TDP43聚集。
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Cytoplasmic aggregation of TDP43 and topographic correlation with tau and α-synuclein accumulation in the rTg4510 mouse model of tauopathy.

In patients with TDP43 proteinopathy, phosphorylated TDP43 (p-TDP43) accumulates in the cytoplasm of neurons. The accumulation of p-TDP43 has also been reported in patients with tauopathy and α-synucleinopathy. We investigated spatiotemporal changes in p-TDP43 accumulation in the brains of rTg4510 mice that overexpressed human mutant tau (P301L) and exhibited hyperphosphorylated tau (hp-tau) and phosphorylated αSyn (p-αSyn) accumulation. Immunohistochemically, p-TDP43 aggregates were observed in the cytoplasm of neurons, which increased with age. A significant positive correlation was observed between the number of cells with p-TDP43 aggregates and hp-tau and p-αSyn aggregates. Suppression of the human mutant tau (P301L) expression by doxycycline treatment reduces the accumulation of p-TDP43, hp-tau, and p-αSyn. Proteinase K-resistant p-TDP43 aggregates were found in regions with high hp-tau, and p-αSyn accumulation. Western blotting of the sarkosyl-insoluble fraction revealed bands of monomeric TDP43 and p-TDP43. These results indicate that the accumulation of mouse p-TDP43 is associated with the accumulation of human mutant tau (P301L) in rTg4510 mouse brains. The accumulation of hp-tau and p-αSyn may promote sarkosyl-insoluble p-TDP43 aggregates that are resistant to proteinase K. The synergistic effects of tau, TDP43, and αSyn may be involved in the pathology of proteinopathies, leading to the accumulation of multiple abnormal proteins.

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CiteScore
7.20
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4.30%
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567
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