Caspase-8 Is Required for Cell Death Induced by Expanded Polyglutamine Repeats

Sánchez, Ignasi Marco; Xu, Chi-jie; Juo, Peter; Kakizaka, Akira; Blenis, John; Yuan, Junying

doi:10.1016/s0896-6273(00)80716-3

Cited by 392 publications

(229 citation statements)

References 45 publications

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“…This finding may also explain the apparent differences between the report that a polyglutamine tract demonstrates interaction with caspase-8 38 and our failure to identify caspase-8 interaction with fulllength Htt (or to identify caspase-8 requirement in Htt-induced striatal neuronal cell death).…”

Section: Caspase-2 Involvement In Hd E Hermel Et Alcontrasting

confidence: 71%

“…Our results differ from an earlier report using primary culture because we use the full-length Htt construct while they used a Htt-derived fragment mostly composed of polyglutamine repeats. 38 Using a primary culture model where full-length Htt is expressed is more relevant for evaluating the early events in HD disease pathogenesis and proteolysis. Next, we examined whether coexpression of catalytically inactive forms of caspase-2 (C303A), caspase-3 (C163A), caspase-6 (C163A), caspase-7 (C186A), caspase-8 (C360A), or caspase-9 (C287A) inhibit cell death induced by Htt138 in striatal neurons.…”

Section: Inhibition Of Htt-induced Polyglutamine Repeatdependent Cellmentioning

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: Caspase-2 Involvement In Hd E Hermel Et Alcontrasting

confidence: 71%

Section: Inhibition Of Htt-induced Polyglutamine Repeatdependent Cellmentioning

confidence: 99%

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) results from an aberrant expansion of CAG repeats, which is translated into a polyglutamine repeat in the Huntingtin protein (Htt), which is a substrate for caspase-3. Cytosolic aggregates of polyglutamine repeat proteins may recruit procaspase 8, resulting in the activation of caspase -8 (48). Thus caspases play an important role in mediating cell death in human neurodegenerative diseases.Amyotrophic lateral sclerosis (ALS) is associated with death of motor neurons in the spinal cord and brain due to mutations in the gene encoding CuZnSoD .…”

Section: Apoptosis and Human Diseasementioning

confidence: 99%

Apoptosis in health and disease and modulation of apoptosis for therapy: An overview

Singh

2007

Indian J Clin Biochem

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“…Examination of post-mortem tissue has implicated caspases in multiple neurodegenerative diseases. Cleaved caspases have been detected in AD (caspases 3, 6, and 9; Chan et al, 1999;LeBlanc et al, 1999;Stadelmann et al, 1999;Lu et al, 2000), in ALS (caspases 1 and 3; Pasinelli et al, 1998), in Parkinson's disease (PD; caspases 3, 8, and 9; Anglade et al, 1997;Jeon et al, 1999;Viswanath et al, 2001), in ischemia (caspases 1 and 3; Love et al, 2000), and Huntington's disease (HD; caspases 1 and 8; Sanchez et al, 1999). Such findings are correlative, in that it is almost impossible to identify definitively causal factors of disease in end-stage brain.…”

Section: Death Pathways In Neurodegenerative Diseasesmentioning

confidence: 99%

“…In PD models, both the extrinsic and the intrinsic pathways have been implicated in studies using pseudosusbstrate inhibitors (Viswanath et al, 2001) and immunocytochemistry of cleaved caspase 3 (Jeon et al, 1999). For HD, the extrinsic pathway has been proposed to be necessary (Sanchez et al, 1999). Overexpression of dominantnegative caspase 1 delays disease in the mouse model of ALS (Friedlander et al, 1997) and in a model of ischemia (Friedlander et al, 1997).…”

Section: Death Pathways In Neurodegenerative Diseasesmentioning

confidence: 99%

Caspases on the brain

Troy

Salvesen

2002

J of Neuroscience Research

106

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The basic mechanisms that underlie neurodegenerative diseases are unknown. Loss of function of specific regions of the brain is due to incapacitation of cells that constitute those regions. Cells can simply stop functioning normally (neurons may cease to transmit signals), or they may die. There is now evidence that the pathology of several neurodegenerative diseases is due to inappropriate apoptosis. This being the case, an understanding of the mediators of apoptosis, their identities, and their role in orchestrating death would be a vital step toward remedying the diseases. The central components of apoptotic pathways, proteases of the caspase family, are present in latent forms in all nucleated cells. Their activity is balanced by specific activation and inactivation events, and the molecular and biochemical controls have been well established in vitro and in model transformed cell lines. In this Mini‐Review, we consider the current status of the basic control mechanisms and how these may be subverted during neurodegeneration. © 2002 Wiley‐Liss, Inc.

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Caspase-8 Is Required for Cell Death Induced by Expanded Polyglutamine Repeats

Cited by 392 publications

References 45 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

Apoptosis in health and disease and modulation of apoptosis for therapy: An overview

Caspases on the brain

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