Dysregulation of the ALS-associated gene TDP-43 leads to neuronal death and degeneration in mice
Lionel M. Igaz, … , John Q. Trojanowski, Virginia M.-Y. Lee
Lionel M. Igaz, … , John Q. Trojanowski, Virginia M.-Y. Lee
Published January 4, 2011
Citation Information: J Clin Invest. 2011;121(2):726-738. https://doi.org/10.1172/JCI44867.
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Dysregulation of the ALS-associated gene TDP-43 leads to neuronal death and degeneration in mice

Abstract

Amyotrophic lateral sclerosis (ALS) and frontotemporal lobar degeneration (FTLD) are characterized by cytoplasmic protein aggregates in the brain and spinal cord that include TAR-DNA binding protein 43 (TDP-43). TDP-43 is normally localized in the nucleus with roles in the regulation of gene expression, and pathological cytoplasmic aggregates are associated with depletion of nuclear protein. Here, we generated transgenic mice expressing human TDP-43 with a defective nuclear localization signal in the forebrain (hTDP-43-ΔNLS), and compared them with mice expressing WT hTDP-43 (hTDP-43-WT) to determine the effects of mislocalized cytoplasmic TDP-43 on neuronal viability. Expression of either hTDP-43-ΔNLS or hTDP-43-WT led to neuron loss in selectively vulnerable forebrain regions, corticospinal tract degeneration, and motor spasticity recapitulating key aspects of FTLD and primary lateral sclerosis. Only rare cytoplasmic phosphorylated and ubiquitinated TDP-43 inclusions were seen in hTDP-43-ΔNLS mice, suggesting that cytoplasmic inclusions were not required to induce neuronal death. Instead, neurodegeneration in hTDP-43 and hTDP-43-ΔNLS–expressing neurons was accompanied by a dramatic downregulation of the endogenous mouse TDP-43. Moreover, mice expressing hTDP-43-ΔNLS exhibited profound changes in gene expression in cortical neurons. Our data suggest that perturbation of endogenous nuclear TDP-43 results in loss of normal TDP-43 function(s) and gene regulatory pathways, culminating in degeneration of selectively vulnerable affected neurons.

Authors

Lionel M. Igaz, Linda K. Kwong, Edward B. Lee, Alice Chen-Plotkin, Eric Swanson, Travis Unger, Joe Malunda, Yan Xu, Matthew J. Winton, John Q. Trojanowski, Virginia M.-Y. Lee

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Figure 4

TDP-43 aggregates are phosphorylated and ubiquitinated in tTA/TDP-ΔNLS mice.

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TDP-43 aggregates are phosphorylated and ubiquitinated in tTA/TDP-ΔNLS m...
(AH) TDP-43 aggregates in cortex and hippocampus of tTA/TDP-ΔNLS mice. IHC of cortex from tTA/TDP-ΔNLS4 (A) and tTA/TDP-ΔNLS19 mice (B) at 1 month off Dox with p409/410 TDP-43 antibody shows relatively few aggregates in tTA/TDP-ΔNLS4 mice and higher number of inclusions in tTA/TDP-ΔNLS19 mice. Inclusions in the DG (CE) and cortex (FH) of tTA/TDP-ΔNLS19 mice 1 week off DOX were immunopositive for p409/410 TDP-43 (C and F), p403/404 TDP-43 (D and G), and ubiquitin (Ub) (E and H) antibodies. (IN) Colocalization of pathologic epitopes in TDP-43 aggregates. IF staining with antibodies to ubiquitin (green) and p409/410 TDP-43 (red) demonstrated extensive colocalization within pathological cytoplasmic aggregates (arrows) in cortex (IN) from tTA/TDP-ΔNLS19 mice 1 week off Dox. Scale bars: 50 μm (A and B); 20 μm (CE).