Mutant huntingtin impairs immune cell migration in Huntington disease
Wanda Kwan, Ulrike Träger, Dimitrios Davalos, Austin Chou, Jill Bouchard, Ralph Andre, Aaron Miller, Andreas Weiss, Flaviano Giorgini, Christine Cheah, Thomas Möller, Nephi Stella, Katerina Akassoglou, Sarah J. Tabrizi, Paul J. Muchowski
Wanda Kwan, Ulrike Träger, Dimitrios Davalos, Austin Chou, Jill Bouchard, Ralph Andre, Aaron Miller, Andreas Weiss, Flaviano Giorgini, Christine Cheah, Thomas Möller, Nephi Stella, Katerina Akassoglou, Sarah J. Tabrizi, Paul J. Muchowski
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Research Article Neuroscience

Mutant huntingtin impairs immune cell migration in Huntington disease

Abstract

In Huntington disease (HD), immune cells are activated before symptoms arise; however, it is unclear how the expression of mutant huntingtin (htt) compromises the normal functions of immune cells. Here we report that primary microglia from early postnatal HD mice were profoundly impaired in their migration to chemotactic stimuli, and expression of a mutant htt fragment in microglial cell lines was sufficient to reproduce these deficits. Microglia expressing mutant htt had a retarded response to a laser-induced brain injury in vivo. Leukocyte recruitment was defective upon induction of peritonitis in HD mice at early disease stages and was normalized upon genetic deletion of mutant htt in immune cells. Migration was also strongly impaired in peripheral immune cells from pre-manifest human HD patients. Defective actin remodeling in immune cells expressing mutant htt likely contributed to their migration deficit. Our results suggest that these functional changes may contribute to immune dysfunction and neurodegeneration in HD, and may have implications for other polyglutamine expansion diseases in which mutant proteins are ubiquitously expressed.

Authors

Wanda Kwan, Ulrike Träger, Dimitrios Davalos, Austin Chou, Jill Bouchard, Ralph Andre, Aaron Miller, Andreas Weiss, Flaviano Giorgini, Christine Cheah, Thomas Möller, Nephi Stella, Katerina Akassoglou, Sarah J. Tabrizi, Paul J. Muchowski

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Figure 5

Severe impairment in migration of monocytes and macrophages isolated from HD patients.

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Severe impairment in migration of monocytes and macrophages isolated fro...
(A) Monocytes and (B) macrophages were isolated or derived from blood samples of presymptomatic HD patients, HD patients with early and moderate/advanced symptoms, and age-matched controls and assayed for migration using a Transwell approach. Cells from HD patients have significantly impaired migration relative to the control upon stimulation with ATP (100 μM), C5a (10 nM), and MCP-1 (50 ng/ml). Results are normalized to control basal levels. Values are mean ± SEM. n > 4 patient samples. *P < 0.05, **P < 0.01 (2-way ANOVA, Bonferroni post hoc test), #P < 0.001.