Haploinsufficiency at the  -synuclein gene underlies phenotypic severity in familial Parkinson's disease

Kobayashi, Hirokazu; Krüger, Rejko; Μarkopoulou, Κaterina; Wszołek, Zbigniew K.; Chase, Bruce A.; Taka, Hikaru; Mineki, Reiko; Murayama, Kimie; Rieß, Olaf; Mizuno, Yoshikuni; Hattori, Nobutaka

doi:10.1093/brain/awg010

Cited by 41 publications

(28 citation statements)

References 21 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…When translated, these lead to the missense mutations Ala53Thr and Ala30Pro, respectively. Recently, reduced mRNA expression of the G209A allele was reported in a Greek-American family [23]. Very recently, we reported that the mRNA expression of the mutant G88C and G209A alleles of the α-synuclein gene is significantly reduced relative to the wild-type allele in lymphoblastoid cell lines established from affected heterozygotes, who had mutations of either G88C or G209A alleles, with a severe clinical phenotype.…”

Section: Snca (α-Synuclein)mentioning

confidence: 79%

Familial Parkinson?s disease: a hint to elucidate the mechanisms of nigral degeneration

Kobayashi

Sasaki-Hatano

Sato

et al. 2003

Journal of Neurology

View full text Add to dashboard Cite

In the majority of patients with Parkinson's disease (PD), it is now clear that genetic factors contribute to the pathogenesis of PD, although the contribution of genetic and environmental factors remains to be elucidated. The contribution of genetic factors to the pathogenesis of PD is supported by the demonstration of the high concordance in twins, increased risk among relatives of PD patients in case control and family studies, and the existence of familial PD based on single gene defects. Recently, several genes have been mapped and identified in patients with familial PD (FPD). alpha-Synuclein is involved in a rare dominant form of familial PD with dopa responsive parkinsonian features and Lewy body positive pathology. In contrast, parkin is responsible for autosomal recessive form of earlyonset PD with Lewy body-negative pathology. This form is identified with world-wide distribution among patients with young-onset PD. Furthermore, ubiquitin carboxy terminal hydrolase L1 (UCHL1) gene is responsible for an autosomal dominant form of typical PD, although only a single family has so far been identified with a mutation of this gene. In addition, DJ-1 has been identified as a causative gene for PARK7, a recessive form of familial PD. Now, a total of five causative genes including NR4A2 have been identified, and others such as PARK3, -4, -6, -8, -9, -10 have been mapped as hereditary forms of familial PD. The presence of different loci or different causative genes indicates that PD is not a single entity but a highly heterogeneous disorder. However, the functions of causative genes may share a common pathway such as an ubiquitin-proteasome pathway. Thus, identification and elucidation of the causative genes should enhance our understanding of the pathogenesis of not only familial PD, but also sporadic PD.

show abstract

Section: Snca (α-Synuclein)mentioning

confidence: 79%

Familial Parkinson?s disease: a hint to elucidate the mechanisms of nigral degeneration

Kobayashi

Sasaki-Hatano

Sato

et al. 2003

Journal of Neurology

View full text Add to dashboard Cite

show abstract

“…Independent reports on other patients [Kobayashi et al, 2003;Markopoulou et al, 1999] have previously shown that expression of the same SNCA allele as well as of the allele for the p.Ala30Pro mutation, was either absent or significantly reduced. This raises the question how common such monoallelic SCNA expression is; studies on this issue will provide important insights, however, they are complicated, because nucleotide variations in the coding sequence of the gene are rare.…”

Section: Discussionmentioning

confidence: 93%

“…Surprisingly, the p.Ala53Thr and p.Ala30Pro alleles were found to be silenced to different degrees, compared to the expression of the normal counterpart in the same patient, in various cases [Kobayashi et al, 2003;Markopoulou et al, 1999]. This interallelic variation of expression, unexpected on the basis of the nature of these mutations, could cause a decrease in alphasynuclein protein in these patients and lead the authors to conclude that a haploinsufficiency effect exists associated with the clinical severity of the disease.…”

Section: Introductionmentioning

confidence: 94%

Allelic imbalance of expression and epigenetic regulation within the alpha-synuclein wild-type and p.Ala53Thr alleles in Parkinson disease

et al. 2010

View full text Add to dashboard Cite

Genetic alterations in the alpha-synuclein (SNCA) gene have been implicated in Parkinson Disease (PD), including point mutations, gene multiplications, and sequence variations within the promoter. Such alterations may be involved in pathology through structural changes or overexpression of the protein leading to protein aggregation, as well as through impaired gene expression. It is, therefore, of importance to specify the parameters that regulate SNCA expression in its normal and mutated state. We studied the expression of SNCA alleles in a lymphoblastoid cell line and in the blood cells of a patient heterozygous for p.Ala53Thr, the first mutation to be implicated in PD pathogenesis. Here, we provide evidence that: (1) SNCA shows monoallelic expression in this patient, (2) epigenetic silencing of the mutated allele involves histone modifications but not DNA methylation, and (3) steady-state mRNA levels deriving from the normal SNCA allele in this patient exceed those of the two normal SNCA alleles combined, in matching, control individuals. An imbalanced SNCA expression in this patient is thus documented, with silencing of the p.Ala53Thr allele and upregulation of the wild-type-allele. This phenomenon is demonstrated for a first time in the SNCA gene, and may have important implications for PD pathogenesis.

show abstract

“…Posttranscriptional regulation of a-synuclein can also occur through endogenous micro RNAs, which bind to the 3 0 end of the gene (Junn et al 2009;Doxakis 2010). A particularly interesting twist to the effects of familial point mutations in SNCA has been provided by a series of studies that, somewhat counterintuitively, suggest that the expression of the mutant alleles is suppressed, especially in cases with prolonged disease (Markopoulou et al 1999;Kobayashi et al 2003), through a mechanism that may involve histone modifications (Voutsinas et al 2010). Remarkably, Voutsinas et al (2010) found that the WT allele is induced in a compensatory fashion, and that the total level of SNCA messenger RNA (mRNA) exceeds that of controls, suggesting that total SNCA levels, rather than the presence of the A53T mutant, are responsible for the disease in these cases.…”

Section: Gain-of-function and Accumulation Of A-synucleinmentioning

confidence: 99%

-Synuclein in Parkinson's Disease

Stefanis¹

2011

Cold Spring Harbor Perspectives in Medicine

1,076

732

View full text Add to dashboard Cite

Haploinsufficiency at the -synuclein gene underlies phenotypic severity in familial Parkinson's disease

Cited by 41 publications

References 21 publications

Familial Parkinson?s disease: a hint to elucidate the mechanisms of nigral degeneration

Familial Parkinson?s disease: a hint to elucidate the mechanisms of nigral degeneration

Allelic imbalance of expression and epigenetic regulation within the alpha-synuclein wild-type and p.Ala53Thr alleles in Parkinson disease

-Synuclein in Parkinson's Disease

Contact Info

Product

Resources

About