Caspase Cleavage of Mutant Huntingtin Precedes Neurodegeneration in Huntington's Disease

Wellington, Cheryl L.; Ellerby, Lisa M.; Gutekunst, Claire‐Anne; Rogers, Danny H.; Warby, Simon C.; Graham, Rona K.; Loubser, Odell; Raamsdonk, Jeremy M. Van; Singaraja, Roshni R.; Yang, Yuzhou; Gafni, Juliette; Bredesen, Dale E.; Hersch, Steven M.; Leavitt, Blair R.; Roy, Sophie; Nicholson, Donald W.; Hayden, Michael R.

doi:10.1523/jneurosci.22-18-07862.2002

Cited by 344 publications

(251 citation statements)

References 48 publications

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“…Our results demonstrate that Htt is cleaved by caspase-2 only at the 552 site when probed with antibodies that detect caspasecleaved Htt fragments (neospecific antibodies to cleavage sites at 513 and 552) (Figure 1d). 31 These results indicate that, in vitro, caspase-2 cleaves Htt at amino acid 552 and correlates with our recent results demonstrating that Htt is also cleaved in vivo at the D552 caspase consensus site in pyramidal cortical neurons of YAC72 mice and HD brains. 31 However, these results do not necessarily explain how this cleavage event is initiated in vivo.…”

Section: Hd Is Specifically Cleaved By Caspase-2 At Caspase Consensussupporting

confidence: 90%

“…BDNF levels are directed regulated by wild-type Htt and are reduced in HD transgenic mice and HD patient brains. 33 We find that caspase-2 cleaves Htt selectively at amino acid 552, which is the Htt caspase cleavage product detected in vivo both in early-grade HD postmortem tissue and in YAC transgenic mice expression mutant Htt, 31 and further that Htt directly interacts with specific caspases to form a cell-death complex. We found that caspase-2, -6, and -7 recruit Htt in an apoptosome-like complex.…”

Section: Introductionmentioning

confidence: 74%

“…Evidence for region-specific cleavage of Htt in vivo comes from studies of YAC transgenic mice expressing mutant full-length huntingtin (YAC72). In this model, N-terminal fragments of Htt are clearly found in the medium spiny neurons of the striatum 30 and cortex, 31 but not in other regions of the brain unaffected in HD. These results suggest that cleavage of Htt by caspases and other proteases such as calpains 32 may produce toxic fragments.…”

Section: Introductionmentioning

confidence: 80%

“…36 However, in vivo, we found that Htt is specifically cleaved at a caspase consensus site at amino acid 552 in pyramidal cortical neurons, while the caspase consensus site at amino acid 513 does not appear to be utilized. 31 Since caspase-3 cleaves at both D513 and D552, we further evaluated the specificity of caspases in cleaving Htt. Here, we show that Htt is also cleaved by caspase-2, -7, and -8 ( Figure 1b).…”

Section: Hd Is Specifically Cleaved By Caspase-2 At Caspase Consensusmentioning

confidence: 99%

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Specific caspase interactions and amplification are involved in selective neuronal vulnerability in Huntington's disease

et al. 2004

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Huntington's disease (HD) is an autosomal dominant progressive neurodegenerative disorder resulting in selective neuronal loss and dysfunction in the striatum and cortex. The molecular pathways leading to the selectivity of neuronal cell death in HD are poorly understood. Proteolytic processing of full-length mutant huntingtin (Htt) and subsequent events may play an important role in the selective neuronal cell death found in this disease. Despite the identification of Htt as a substrate for caspases, it is not known which caspase(s) cleaves Htt in vivo or whether regional expression of caspases contribute to selective neuronal cells loss. Here, we evaluate whether specific caspases are involved in cell death induced by mutant Htt and if this correlates with our recent finding that Htt is cleaved in vivo at the caspase consensus site 552. We find that caspase-2 cleaves Htt selectively at amino acid 552. Further, Htt recruits caspase-2 into an apoptosome-like complex. Binding of caspase-2 to Htt is polyglutamine repeat-length dependent, and therefore may serve as a critical initiation step in HD cell death. This hypothesis is supported by the requirement of caspase-2 for the death of mouse primary striatal cells derived from HD transgenic mice expressing full-length Htt (YAC72). Expression of catalytically inactive (dominant-negative) forms of caspase-2, caspase-7, and to some extent caspase-6, reduced the cell death of YAC72 primary striatal cells, while the catalytically inactive forms of caspase-3, -8, and -9 did not. Histological analysis of post-mortem human brain tissue and YAC72 mice revealed activation of caspases and enhanced caspase-2 immunoreactivity in medium spiny neurons of the striatum and the cortical projection neurons when compared to controls. Further, upregulation of caspase-2 correlates directly with decreased levels of brain-derived neurotrophic factor in the cortex and striatum of 3-month YAC72 transgenic mice and therefore suggests that these changes are early events in HD pathogenesis. These data support the involvement of caspase-2 in the selective neuronal cell death associated with HD in the striatum and cortex.

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Section: Hd Is Specifically Cleaved By Caspase-2 At Caspase Consensussupporting

confidence: 90%

Section: Introductionmentioning

confidence: 74%

Section: Introductionmentioning

confidence: 80%

Section: Hd Is Specifically Cleaved By Caspase-2 At Caspase Consensusmentioning

confidence: 99%

See 2 more Smart Citations

Specific caspase interactions and amplification are involved in selective neuronal vulnerability in Huntington's disease

et al. 2004

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“…10 The decreased apoptosis observed in the brain suggested a critical role for caspase 3 in the development of the central nervous system. Caspase 3 has also been implicated in cell death following a number of neurodegenerative insults including global ischaemia, 12,13 focal ischaemia, [14][15][16][17][18][19] transient ischaemia of the spinal cord, 20 neonatal cerebral hypoxia-ischaemia, [21][22][23] traumatic brain injury, [24][25][26] Alzheimer's disease, [27][28][29] Huntington's disease, [30][31][32] and Parkinson's disease. [33][34][35][36][37] It was therefore hypothesized that overexpression of caspase 3 may sensitize the animal to normal (physiological) apoptotic processes that occur during development and natural ageing and confer particular susceptibility to neurodegenerative insults.…”

Section: Introductionmentioning

confidence: 99%

Mice overexpressing human caspase 3 appear phenotypically normal but exhibit increased apoptosis and larger lesion volumes in response to transient focal cerebral ischaemia

et al. 2004

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Caspase 3 activation has been implicated in cell death following a number of neurodegenerative insults. To determine whether caspase genes can affect the susceptibility of cells to neurodegeneration, a transgenic mouse line was created, expressing human caspase 3 under control of its own promoter. The human gene was regulated by the murine homeostatic machinery and human procaspase 3 was expressed in the same tissues as mouse caspase 3. These novel transgenic mice appeared phenotypically and developmentally normal and survived in excess of 2 years. Behavioural assessment using the 5-choice serial reaction time task found no differences from wild-type littermates. Caspase activity was found to be tightly regulated under physiological conditions, however, significantly larger lesions were obtained when transgenic mice were subjected to focal cerebral ischaemia/reperfusion injury compared to wildtype littermates. These data demonstrate that mice overexpressing human caspase 3 are essentially normal, however, they have increased susceptibility to degenerative insults.

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Triplet Repeat Diseases

Guyenet

Spada

2006

Encyclopedia of Molecular Cell Biology and Molecular Medicine

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Caspase Cleavage of Mutant Huntingtin Precedes Neurodegeneration in Huntington's Disease

Cited by 344 publications

References 48 publications

Specific caspase interactions and amplification are involved in selective neuronal vulnerability in Huntington's disease

Specific caspase interactions and amplification are involved in selective neuronal vulnerability in Huntington's disease

Mice overexpressing human caspase 3 appear phenotypically normal but exhibit increased apoptosis and larger lesion volumes in response to transient focal cerebral ischaemia

Triplet Repeat Diseases

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