Genome-wide Linkage Analysis of a Parkinsonian-Pyramidal Syndrome Pedigree by 500 K SNP Arrays

Shojaee, Seyedmehdi; Sina, Farzad; Banihosseini, Setareh Sadat; Kazemi, Mohammad; Kalhor, Reza; Shahidi, Gholam Ali; Fakhrai-Rad, Hossein; Ronaghi, Mostafa; Elahi, Elahe

doi:10.1016/j.ajhg.2008.05.005

Cited by 218 publications

(200 citation statements)

References 38 publications

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“…A homozygous mutation in the FBXO7 gene was identified in an Iranian family with early-onset autosomal recessive parkinsonism and pyramidal tract signs [180]. Another homozygous mutation and a compound heterozygous mutation were found in Italian and Dutch families with similar phenotypes [261].…”

Section: Park15mentioning

confidence: 94%

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Epidemiology and etiology of Parkinson’s disease: a review of the evidence

et al. 2011

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Section: Park15mentioning

confidence: 94%

“…To date (2010), 11 genes and an additional 3 genetic loci have been associated with PD [168][169][170][171][172][173][174][175][176][177][178][179][180][181][182][183][184]; two additional loci await to be confirmed [185,186]. The PD genes and loci are described in Table 4.…”

Section: Genes and Loci In Familial Pdmentioning

confidence: 99%

Epidemiology and etiology of Parkinson’s disease: a review of the evidence

et al. 2011

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“…Fbxo7 had a nuclear localization in a percentage of biopsies from human colon cancer samples, and yet, interestingly, data presented here indicated a different localization defect in PD. Homozygous inheritance of an R378G allele of Fbxo7 causes an atypical PD (9,11), and finding that this pathogenic point mutation, located outside of the FBD, severely compromised Skp1 binding was surprising. Moreover, in agreement with our model for the role of Skp1 binding in nuclear retention, R378G did not accumulate in the nucleus and was more cytoplasmic than the WT protein.…”

Section: Discussionmentioning

confidence: 99%

“…Autosomal recessive mutations in FBXO7 have been identified as causing an early-onset Parkinsonian disease (9,11), and Fbxo7 has also been found to be highly expressed in human malignancies (10). We cloned Fbxo7 in a yeast two hybrid screen for proteins interacting with viral D-type cyclins (10).…”

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confidence: 99%

A Competitive Binding Mechanism between Skp1 and Exportin 1 (CRM1) Controls the Localization of a Subset of F-box Proteins

Nelson

Laman

2011

Journal of Biological Chemistry

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SCF-type E3 ubiquitin ligases are crucial regulators of cell cycle progression. As the F-box protein is the substrate-specifying subunit of this family of ligases, their availability dictates the timing and the location of the ubiquitination of substrates. We report here our investigation into the regulation of the localization of F-box proteins, in particular Fbxo7, whose mislocalization is associated with human disease. We identified a motif in Fbxo7 that we have characterized as a functional leucine-rich nuclear export sequence (NES), and which allowed binding to the nuclear export protein, exportin 1 (CRM1). Unusually, the NES was embedded within the F-box domain, which is bound by Skp1 and enables the F-box protein to form part of an E3 ubiquitin ligase. The NES of Fbxo7 controlled its localization and was conserved in Fbxo7 homologues in other species. Skp1 binding prevented Fbxo7 from contacting CRM1. We propose that this competitive binding allowed Fbxo7 to accumulate within the nucleus starting at the G1/S transition. More than ten other F-box proteins also contain an NES at the same location in their F-box domains, indicating that this competitive binding mechanism may contribute to the regulation of a sixth of the known F-box proteins.

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“…Additionally, Cytochrome P450 (CYP), and in particular CYP2D6, which has polymorphic expression, and which is expressed in neurons and in the gut has a different expression in PD patients, where it has been found preponderantly as CYP2D6*4 allele [267] CYP2D6 acts as a 25-hydroxylase, which is able to convert vitamin D3 into 25OHD, being the key enzyme to determine a deficiency of vitamin D. In mouse MPTP treated model (inducing PD phenotype), Singh et al [268] reported the strong expression of the animal ortholog of CYP2D6, CYP2D22. Very interestingly, CYP2D loci are located on chromosome 22 where many genes related to PD are segregated [269][270][271]. It seems surprising that deletion of chromosome 22q11 was reported to be associated to PD [271] but also with a reduced serum calcium and a reduced level of vitamin D [272].…”

Section: Vitamin D Deficiency and Neurodegenerative Diseasesmentioning

confidence: 99%

Vitamin D in Neurological Diseases: A Rationale for a Pathogenic Impact

Moretti

Morelli

Caruso

2018

Preprint

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It is widely known that vitamin D receptors have been found in neurons and glial cells and their highest expression is in the hippocampus, hypothalamus, thalamus and subcortical grey nuclei, and substantia nigra. The vitamin D helps the regulation of neurotrophin, neural differentiation and maturation, through the control operation of growing factors synthesis (ie NGF and GDNF), the trafficking of the septo-hyppocampal pathway, and the control of the synthesis process of different neuromodulators (such as Ach, DA, and GABA).Based on these assumptions, we have written this review in order to summarize the potential role of vitamin D in neurological pathologies. The work could be titanic, and might result very fuzzy and even incoherent, if we would not have conjectured to taper our first intentions and devoted our interests towards three mainstreams: demyelinating pathologies, vascular syndromes and neurodegeneration.Due to the lack of effective therapeutic options, a part from the disease modifying strategies, the role of different risk factors should be investigated in neurology, as far as their correction may lead to the improvement of the cerebral conditions.We have explored the relationships between the gene-environmental influence and long term vitamin D deficiency, as a risk factor for the development of different types of neurological disorders, along with the role and the rationale of therapeutic trials with vitamin D implementation. Peer-reviewed version available at Int. J. Mol. Sci. 2018, 19, 2245 doi:10.3390/ijms19082245 3 SEARCH STRATEGY AND SELECTION CRITERIAWe searched MEDLINE using the search terms: "vitamin D central nervous system" , both "vitamin D" and "central nervous system"; "vitamin D immune system/response", both "vitamin D" and "immune system" or "immune response"; "vitamin D multiple sclerosis risk", both "vitamin D" and "multiple sclerosis risk"; "vitamin D multiple sclerosis relapse", both "vitamin D" and "multiple sclerosis relapse"; "vitamin D multiple sclerosis magnetic resonance imaging", both "vitamin D" and "multiple sclerosis magnetic resonance imaging"; "vitamin D multiple sclerosis disability", both "vitamin D" and "multiple sclerosis disability"; "vitamin D supplementation/therapy/treatment multiple sclerosis", both "vitamin D supplementation" or "vitamin D therapy" or "vitamin D treatment" and "multiple sclerosis"; "vascular dementia", both as -vascular-and -dementia-, "subcortical vascular dementia", both assubcortical-and -dementia-, "Alzheimer's disease", "pathogenesis neurodegeneration" "amyloid", "cholinergic afferents", "arteriolosclerosis", "cerebral flow regulation", "stroke". Publications were selected mostly form the past 20years, but did not exclude frequently referenced and highly regarded older publications. . Congress abstracts and isolated case reports were not considered. We searched the reference lists of articles identified by this search strategy and selected those we judged relevant. Review articles and book chapters are cited to provide with ...

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Genome-wide Linkage Analysis of a Parkinsonian-Pyramidal Syndrome Pedigree by 500 K SNP Arrays

Cited by 218 publications

References 38 publications

Epidemiology and etiology of Parkinson’s disease: a review of the evidence

Epidemiology and etiology of Parkinson’s disease: a review of the evidence

A Competitive Binding Mechanism between Skp1 and Exportin 1 (CRM1) Controls the Localization of a Subset of F-box Proteins

Vitamin D in Neurological Diseases: A Rationale for a Pathogenic Impact

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