Human Molecular Genetics
 2000
DOI: 10.1093/hmg/9.14.2175
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Huntingtin's WW domain partners in Huntington's disease post-mortem brain fulfill genetic criteria for direct involvement in Huntington's disease pathogenesis

Lucius A. Passani
1
,
Mark T. Bedford
2
,
Peter W. Faber
3
et al.

Abstract: An elongated glutamine tract in mutant huntingtin initiates Huntington's disease (HD) pathogenesis via a novel structural property that displays neuronal selectivity, glutamine progressivity and dominance over the normal protein based on genetic criteria. As this mechanism is likely to involve a deleterious protein interaction, we have assessed the major class of huntingtin interactors comprising three WW domain proteins. These are revealed to be related spliceosome proteins (HYPA/FBP-11 and HYPC) and a transc… Show more

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Cited by 89 publications
(63 citation statements)
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“…Another interesting set of GO categories populated by upregulated genes was categories associated with RNA splicing/RNA processing. This is particularly intriguing given that mutant and wild-type huntingtin have been reported to have differential affinities for WW-domain proteins involved in RNA splicing (Passani et al, 2000).…”
Section: Transcriptomic Effects Of Lentiviral Expression Are Polyglutmentioning
confidence: 99%

Dysregulation of Gene Expression in Primary Neuron Models of Huntington's Disease Shows That Polyglutamine-Related Effects on the Striatal Transcriptome May Not Be Dependent on Brain Circuitry

Runne1,
Régulier2,
Kuhn3
et al. 2008
J. Neurosci.
88
5
91
0
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“…Another interesting set of GO categories populated by upregulated genes was categories associated with RNA splicing/RNA processing. This is particularly intriguing given that mutant and wild-type huntingtin have been reported to have differential affinities for WW-domain proteins involved in RNA splicing (Passani et al, 2000).…”
Section: Transcriptomic Effects Of Lentiviral Expression Are Polyglutmentioning
confidence: 99%

Dysregulation of Gene Expression in Primary Neuron Models of Huntington's Disease Shows That Polyglutamine-Related Effects on the Striatal Transcriptome May Not Be Dependent on Brain Circuitry

Runne1,
Régulier2,
Kuhn3
et al. 2008
J. Neurosci.
88
5
91
0
View full textAdd to dashboardCite
“…Based on the Prp40 data, PRPF40A and PRPF40B are thought to participate in early spliceosome assembly, but their functions remain unknown. Notably, PRPF40B has been implicated in the pathogenesis of neurological disorders, including Huntington's disease and Rett syndrome (Faber et al 1998;Passani et al 2000;Buschdorf and Strätling 2004). Moreover, mutations in spliceosome components involved in splice site recognition have been recently detected in myelodysplastic syndrome (MDS), a group of disorders that lead to myeloid leukemia (Papaemmanuil et al 2011;Yoshida et al 2011).…”
Section: Introductionmentioning
confidence: 99%

Prp40 pre-mRNA processing factor 40 homolog B (PRPF40B) associates with SF1 and U2AF65and modulates alternative pre-mRNA splicing in vivo

Becerra1,
Montes2,
Hernández-Munaín
3
et al. 2015
RNA
32
3
45
2
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“…The role of mutant htt aggregates in cell death is controversial, because the presence of aggregates does not consistently correlate with cell death (Saudou et al, 1998;Sisodia 1998;Kim et al, 1999;Kuemmerle et al, 1999). A soluble, nonaggregated, mutant htt might contribute to neurodegeneration by engaging in abnormal protein interactions (Bao et al, 1996;Sittler et al, 1998;Passani et al, 2000;Gervais et al, 2002). Oligomers of mutant htt expressed from exon 1 form spheroids and protofibrils as intermediates (prefibrillar forms) during fibril assembly (Poirier et al, 2002).…”
Section: Introductionmentioning
confidence: 99%

Huntingtin Bodies Sequester Vesicle-Associated Proteins by a Polyproline-Dependent Interaction

Qin1,
Wang2,
Sapp3
et al. 2004
J. Neurosci.
152
8
124
0
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