Inhibition of polyglutamine aggregation in R6/2 HD brain slices - Complex dose-response profiles

D L Smith; R Portier; B Woodman; E Hockly; A Mahal; W E Klunk; X J Li; E Wanker; K D Murray; G P Bates

doi:10.1006/nbdi.2001.0438

Inhibition of polyglutamine aggregation in R6/2 HD brain slices - Complex dose-response profiles

D L Smith, R Portier, B Woodman, E Hockly, A Mahal, W E Klunk, X J Li, E Wanker, K D Murray, G P Bates

Research output: Contribution to journal › Article › peer-review

65 Citations (Scopus)

Abstract

Huntington's disease (HD) is a late onset neurodegenerative disorder caused by a CAG/polyglutamine (polyQ) repeat expansion. PolyQ aggregates can be detected in the nuclei and processes of neurons in HD patients and mouse models prior to the onset of symptoms. The misfolding and aggregation pathway is an important therapeutic target. To better test the efficacy of aggregation inhibitors, we have developed an organotypic slice culture system. We show here that the formation of polyQ aggregates in hippocampal slices established from the R6/2 mouse follows the same prescribed sequence as occurs in vivo. Using this assay, we show that Congo red and chrysamine G can modulate aggregate formation, but show complex dose-response curves. Oral administration of creatine has been shown to delay the onset of all aspects of the phenotype and neuropathology in R6/2 mice. We show here that creatine can similarly inhibit aggregate formation in the slice culture assay. (C) 2001 Elsevier Science.

Original language	English
Pages (from-to)	1017 - 1026
Number of pages	10
Journal	Neurobiology of Disease
Volume	8
Issue number	6
DOIs	https://doi.org/10.1006/nbdi.2001.0438
Publication status	Published - 2001

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abstract = "Huntington's disease (HD) is a late onset neurodegenerative disorder caused by a CAG/polyglutamine (polyQ) repeat expansion. PolyQ aggregates can be detected in the nuclei and processes of neurons in HD patients and mouse models prior to the onset of symptoms. The misfolding and aggregation pathway is an important therapeutic target. To better test the efficacy of aggregation inhibitors, we have developed an organotypic slice culture system. We show here that the formation of polyQ aggregates in hippocampal slices established from the R6/2 mouse follows the same prescribed sequence as occurs in vivo. Using this assay, we show that Congo red and chrysamine G can modulate aggregate formation, but show complex dose-response curves. Oral administration of creatine has been shown to delay the onset of all aspects of the phenotype and neuropathology in R6/2 mice. We show here that creatine can similarly inhibit aggregate formation in the slice culture assay. (C) 2001 Elsevier Science.",

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AU - Portier, R

AU - Woodman, B

AU - Hockly, E

AU - Mahal, A

AU - Klunk, W E

AU - Li, X J

AU - Wanker, E

AU - Murray, K D

AU - Bates, G P

PY - 2001

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AB - Huntington's disease (HD) is a late onset neurodegenerative disorder caused by a CAG/polyglutamine (polyQ) repeat expansion. PolyQ aggregates can be detected in the nuclei and processes of neurons in HD patients and mouse models prior to the onset of symptoms. The misfolding and aggregation pathway is an important therapeutic target. To better test the efficacy of aggregation inhibitors, we have developed an organotypic slice culture system. We show here that the formation of polyQ aggregates in hippocampal slices established from the R6/2 mouse follows the same prescribed sequence as occurs in vivo. Using this assay, we show that Congo red and chrysamine G can modulate aggregate formation, but show complex dose-response curves. Oral administration of creatine has been shown to delay the onset of all aspects of the phenotype and neuropathology in R6/2 mice. We show here that creatine can similarly inhibit aggregate formation in the slice culture assay. (C) 2001 Elsevier Science.

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Inhibition of polyglutamine aggregation in R6/2 HD brain slices - Complex dose-response profiles

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