Patricia F. Kao, Yun-Ru Chen, Xiao-Bo Liu, Charles DeCarli, William W. Seeley, Lee-Way Jin

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Patricia F. Kao, Yun-Ru Chen, Xiao-Bo Liu, Charles DeCarli, William W. Seeley, Lee-Way Jin

机译：Patricia F. K熬, Y UN-Ru Chen, ξ奥-B OL IU, Charles Dec AR里, William W. Seeley, Lee-way jin

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Objective: The proteinaceous inclusions in TDP-43 proteinopathies such as frontotemporal lobar degeneration (FTLD)-TDP are made of high-molecular-weight aggregates of TDP-43. These aggregates have not been classified as amyloids, as prior amyloid staining results were not conclusive. Here we used a specific TDP-43 amyloid oligomer antibody called TDP-O to determine the presence and abundance of TDP-43 oligomers among different subtypes of FTLD-TDP as well as in hippocampal sclerosis (HS), which represents a non-FTLD pathology with TDP-43 inclusions. Methods: Postmortem tissue from the hippocampus and anterior orbital gyrus from 54 prospectively assessed and diagnosed subjects was used for immunostaining with TDP-O. Electron microscopy was used to assess the subcellular locations of TDP-O-decorated structures. Results: TDP-43 inclusions staining with TDP-O were present in FTLD-TDP and were most conspicuous for FTLD-TDP type C, the subtype seen in most patients with semantic variant primary progressive aphasia. TDP-O immunoreactiv-ity was absent in the hippocampus of HS patients despite abundant TDP-43 inclusions. Ultrastructurally, TDP-43 oligomers resided in granular or tubular structures, frequently in close proximity to, but not within, neuronal lysosomes. Interpretation: TDP-43 forms amyloid oligomers in the human brain, which may cause neurotoxicity in a manner similar to other amyloid oligomers. Oligomer formation may contribute to the conformational heterogeneity of TDP-43 aggregates and mark the different properties of TDP-43 inclusions between FTLD-TDP and HS.

机译：目的：TDP-43蛋白质病等蛋白质夹杂物，如额发射叶片退化（FTLD）-TDP的TDP-43的高分子量聚集体制成。这些聚集体尚未被归类为淀粉样蛋白，因为先前的淀粉样蛋白染色结果并未确定。在这里，我们使用称为TDP-O的特异性TDP-43淀粉样蛋白低聚物抗体，以确定FTLD-TDP的不同亚型的TDP-43低聚物的存在和丰度以及在海马硬化症（HS）中，这代表非FTLD病理学使用TDP-43夹杂物。方法：从54个前瞻性评估和诊断受试者中来自海马和前眶上转毒的后术组织用于用TDP-O免疫染色。电子显微镜用于评估TDP-O装饰结构的亚细胞位置。结果：TDP-43夹杂物在FTLD-TDP中存在染色，对FTLD-TDP型C，大多数患者中患者最显着，大多数患有语义变异的初级进步性失语症。尽管有丰富的TDP-43夹杂物，但HS患者的海马缺乏TDP-O免疫反应性ITY。超微结构的上，TDP-43寡聚体留在颗粒状或管状结构中，经常密切接近，但不在内核溶酶体内。解释：TDP-43在人脑中形成淀粉样蛋白低聚物，这可能以类似于其他淀粉样蛋白低聚物的方式引起神经毒性。低聚物形成可有助于TDP-43聚集体的构象异质性，并标记FTLD-TDP和HS之间的TDP-43夹杂物的不同性质。

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《Annals of neurology》 |2015年第2期|共11页
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Patricia F. Kao, Yun-Ru Chen, Xiao-Bo Liu, Charles DeCarli, William W. Seeley, Lee-Way Jin

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