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Query: UMLS:C0013421 (
dystonia
)
8,418
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
X-linked
dystonia
-parkinsonism (XDP) is a movement disorder endemic to the Philippines. The disease locus,
DYT3
, has been mapped to Xq13.1. In a search for the causative gene, we performed genomic sequencing analysis, followed by expression analysis of XDP brain tissues. We found a disease-specific SVA (short interspersed nuclear element, variable number of tandem repeats, and Alu composite) retrotransposon insertion in an intron of the TATA-binding protein-associated factor 1 gene (TAF1), which encodes the largest component of the TFIID complex, and significantly decreased expression levels of TAF1 and the dopamine receptor D2 gene (DRD2) in the caudate nucleus. We also identified an abnormal pattern of DNA methylation in the retrotransposon in the genome from the patient's caudate, which could account for decreased expression of TAF1. Our findings suggest that the reduced neuron-specific expression of the TAF1 gene is associated with XDP.
...
PMID:Reduced neuron-specific expression of the TAF1 gene is associated with X-linked dystonia-parkinsonism. 1766 93
X-linked recessive
dystonia
-parkinsonism (
XDP
;
DYT3
; Lubag) is an adult-onset disorder that manifests severe and progressive
dystonia
with a high frequency of generalization. In search for the anatomical basis for
dystonia
, we performed postmortem analyses of the functional anatomy of the basal ganglia based on the striatal compartments (i.e., the striosomes and matrix compartment) in
XDP
. Our study showed that in the
XDP
neostriatum, the matrix compartment is relatively spared in a mosaic pattern, whereas the striosomes are severely depleted. In view of the three-pathway basal ganglia model, we postulate that the disproportionate involvement of neostriatal compartments and their efferent projections may underlie the manifestation of
dystonia
in patients with
XDP
. This study is the first to show specific basal ganglia pathology that could explain the genesis of
dystonia
in human heredodegenerative movement disorders, suggesting that
dystonia
may result from an imbalance in the activity between the striosomal and matrix pathways.
...
PMID:[A pathomechanism for the genesis of dystonia: striatal compartments and hypothesized model of basal ganglia circuits]. 1743 34
X-Linked
Dystonia
-Parkinsonism (
XDP
or "Lubag") is a progressive neurodegenerative disorder unique to the Island of Panay in the Philippines. Imaging and autopsy studies have suggested involvement of the caudate and putamen in late stages. Because the clinical presentation of patients with
XDP
resembles that of patients with Parkinson disease or
dystonia
, it is reasonable to predict the neuropsychological profile might be similar; however, the neuropsychological profile of a
XDP
patient has not previously been published. We present the neuropsychological findings of a 67-year-old gentleman with a 10-year history of
XDP
who presented with parkinsonian and dystonic symptoms. He was evaluated for suitability for deep brain stimulation surgery. Neuropsychological findings demonstrated diffuse impairment involving memory, visuospatial, language, and executive functioning.
...
PMID:Neuropsychological profile of a Filipino gentleman with X-linked dystonia-parkinsonism: a case report of Lubag disease. 1860 12
X-linked
dystonia
-parkinsonism (
XDP
,
DYT3
), endemic in the Philippine island of Panay, is characterized by the clinical onset with
dystonia
followed by parkinsonism. We found a 35-year-old American male patient, originally from Panay with typical
XDP
, has a 2-year history of parkinsonism,
dystonia
, and tremor. Ancestral
DYT3
haplotype and disease-specific SVA (short interspersed nuclear element, variable number of tandem repeats, and Alu composite) retrotransposon insertion were identified in the
DYT3
proband and two female unaffected family members. No mutation(s) and expression changes in peripheral blood lymphocytes were observed in the TATA-binding protein-associated factor 1 gene (TAF1) or the chemokine CXC motif receptor 3 gene (CXCR3) of the proband or other
DYT3
carriers. These findings indicate blood DNA test has a diagnostic utility and implications for genetic counseling in families with
DYT3
. In contrast, TAF1 and CXCR3 gene expression in peripheral blood lymphocytes is not a suitable surrogate disease marker for
DYT3
.
...
PMID:Genetic study of an American family with DYT3 dystonia (lubag). 1895 44
Presently, 17 distinct monogenic primary dystonias referred to as dystonias 1- 4, 5a,b, 6-8, 10-13 and 15-18 (loci DYT 1-4, 5a,b, 6-8, 10-13, 15-18) have been recognized. Twelve forms are inherited as autosomal dominant, four as autosomal recessive and one as an X-linked recessive trait. Three additional autosomal dominant forms (DYT9, DYT19 and DYT20) might exist based on linkage mapping to regions apparently different from, yet in close proximity to or overlapping with the known loci DYT18, DYT10 and DYT8. Clinically, this group of movement disorders includes pure dystonias and
dystonia
plus syndromes. In addition, dyskinesias (paroxysmal dystonias), although phenotypically distinct from classical dystonias, are discussed within this group. In pure dystonias,
dystonia
is occasionally accompanied by tremor. In
dystonia
plus syndromes,
dystonia
as the prominent sign concurs with other movement abnormalities such as myoclonus and parkinsonism. In the dyskinesias,
dystonia
occurs as a paroxysmal sign in association with other movement anomalies and sometimes seizures. While gross neuropathological changes are absent in most primary dystonias, including the paroxysmal forms, striking morphological alterations are found in some, such as in the X-linked
dystonia
-parkinsonism syndrome (
DYT3
). Neuropathological findings at the microscopic level have also been reported in several cases of
dystonia
1 and 5, both of which were previously thought to be morphologically normal. One locus, DYT14 had been erroneously assigned, by linkage mapping, in a family with
dystonia
5. There are two forms of
dystonia
5, one autosomal dominant and one autosomal recessive. These forms are designated here as
dystonia
5a and
dystonia
5b (DYT5a, DYT5b), respectively. The disease gene has been identified in 10 primary dystonias, seven autosomal dominant (TOR1A/DYT1, GCH1/DYT5a, THAP1/DYT6, PNKD1/MR-1/DYT8, SGCE/DYT11, ATP1A3/DYT12 and SLC2A1/DYT18), two autosomal recessive (TH/DYT5b and PRKRA/DYT16) and one X-chromosomal recessive (TAF1/
DYT3
). This article summarizes all known aspects on each of the monogenic primary dystonias, including phenotype, neuropathology, imaging, inheritance, mapping, molecular genetics, molecular pathology, animal models and treatment. Suggestions for the diagnostic procedure in primary dystonias are given. Although much is now known about the molecular basis of primary dystonias, treatment of patients is still mainly symptomatic. The only exceptions are dystonias 5a and 5b with their excellent long-term response to L-dopa substitution.
...
PMID:The monogenic primary dystonias. 1957 24
THAP1 is a sequence-specific DNA binding factor that regulates cell proliferation through modulation of target genes such as the cell cycle-specific gene RRM1. Mutations in the THAP1 DNA binding domain, an atypical zinc finger (THAP-zf), have recently been found to cause DYT6
dystonia
, a neurological disease characterized by twisting movements and abnormal postures. In this study, we report that THAP1 shares sequence characteristics, in vivo expression patterns and protein partners with THAP3, another THAP-zf protein. Proteomic analyses identified HCF-1, a potent transcriptional coactivator and cell cycle regulator, and O-GlcNAc transferase (OGT), the enzyme that catalyzes the addition of O-GlcNAc, as major cellular partners of THAP3. THAP3 interacts with HCF-1 through a consensus HCF-1-binding motif (HBM), a motif that is also present in THAP1. Accordingly, THAP1 was found to bind HCF-1 in vitro and to associate with HCF-1 and OGT in vivo. THAP1 and THAP3 belong to a large family of HCF-1 binding factors since seven other members of the human THAP-zf protein family were identified, which harbor evolutionary conserved HBMs and bind to HCF-1. Chromatin immunoprecipitation (ChIP) assays and RNA interference experiments showed that endogenous THAP1 mediates the recruitment of HCF-1 to the RRM1 promoter during endothelial cell proliferation and that HCF-1 is essential for transcriptional activation of RRM1. Together, our findings suggest HCF-1 is an important cofactor for THAP1. Interestingly, our results also provide an unexpected link between DYT6 and
DYT3
(X-linked
dystonia
-parkinsonism) dystonias because the gene encoding the THAP1/DYT6 protein partner OGT maps within the
DYT3
critical region on Xq13.1.
...
PMID:The THAP-zinc finger protein THAP1 associates with coactivator HCF-1 and O-GlcNAc transferase: a link between DYT6 and DYT3 dystonias. 2020 Jan 53
The list of genetic causes of syndromes of
dystonia
parkinsonism grows constantly. As a consequence, the diagnosis becomes more and more challenging for the clinician. Here, we summarize the important causes of
dystonia
parkinsonism including autosomal-dominant, recessive, and x-linked forms. We cover dopa-responsive dystonia, Wilson's disease, Parkin-, PINK1-, and DJ-1-associated parkinsonism (PARK2, 6, and 7), x-linked
dystonia
-parkinsonism/Lubag (
DYT3
), rapid-onset
dystonia
-parkinsonism (DYT12) and DYT16
dystonia
, the syndromes of Neurodegeneration with Brain Iron Accumulation (NBIA) including pantothenate kinase (PANK2)- and PLA2G6 (PARK14)-associated neurodegeneration, neuroferritinopathy, Kufor-Rakeb disease (PARK9) and the recently described SENDA syndrome; FBXO7-associated neurodegeneration (PARK15), autosomal-recessive spastic paraplegia with a thin corpus callosum (SPG11), and
dystonia
parkinsonism due to mutations in the SLC6A3 gene encoding the dopamine transporter. They have in common that in all these syndromes there may be a combination of dystonic and parkinsonian features, which may be complicated by pyramidal tract involvement. The aim of this review is to familiarize the clinician with the phenotypes of these disorders.
...
PMID:Rare causes of dystonia parkinsonism. 2069 31
Sex-linked
dystonia
parkinsonism (
XDP
,
DYT3
, "Lubag") is an adult-onset, progressive, debilitating movement disorder first described in Filipino males from Panay Islands in 1975.
XDP
manifests predominantly as torsion dystonia, later combined with or sometimes replaced with parkinsonism. Within the Island of Panay, the prevalence rate is highest in the province of Capiz, where 1:4000 men suffer from the disorder. There is a high degree of penetrance and generalization. While women often serve as carriers,
XDP
is not limited to men. An updated
XDP
Philippine registry (as of January 2010) has identified 505 cases, with 500 males and 5 females. While some report that females may carry a milder form of the disorder, in our experience, both sexes generally follow a similar progressive clinical course.
...
PMID:The unique phenomenology of sex-linked dystonia parkinsonism (XDP, DYT3, "Lubag"). 2104 75
The neuron-specific isoform of the TAF1 gene (N-TAF1) is thought to be involved in the pathogenesis of
DYT3
dystonia
, which leads to progressive neurodegeneration in the striatum. To determine the expression pattern of N-TAF1 transcripts, we developed a specific monoclonal antibody against the N-TAF1 protein. Here we show that in the rat brain, N-TAF1 protein appears as a nuclear protein within subsets of neurons in multiple brain regions. Of particular interest is that in the striatum, the nuclei possessing N-TAF1 protein are largely within medium spiny neurons, and they are distributed preferentially, though not exclusively, in the striosome compartment. The compartmental preference and cell type-selective distribution of N-TAF1 protein in the striatum are strikingly similar to the patterns of neuronal loss in the striatum of
DYT3
patients. Our findings suggest that the distribution of N-TAF1 protein could represent a key molecular characteristic contributing to the pattern of striatal degeneration in
DYT3
dystonia
.
...
PMID:Identification and localization of a neuron-specific isoform of TAF1 in rat brain: implications for neuropathology of DYT3 dystonia. 2161 29
By family-based screening, first Fuchs and then many other authors showed that mutations in THAP1 (THAP [thanatos-associated protein] domain-containing, apoptosis-associated protein 1) account for a substantial proportion of familial, early-onset, nonfocal, primary
dystonia
cases (DYT6
dystonia
). THAP1 is the first transcriptional factor involved in primary
dystonia
and the hypothesis of a transcriptional deregulation, which was primarily proposed for the X-linked
dystonia
-parkinsonism (
DYT3
dystonia
), provided thus a new way to investigate the possible mechanism underlying the development of
dystonic movements
. Currently, 56 families present with a THAP1 mutation; however, no genotype/phenotype relationship has been found. Therefore, we carried out a systematic review of the literature on the THAP1 gene to colligate all reported patients with a specific THAP1 mutation and the associated clinical signs in order to describe the broad phenotypic continuum of this disorder. To facilitate the comparison of the identified mutations, we created a Locus-Specific Database (UMD-THAP1 LSDB) available at http://www.umd.be/THAP1/. Currently, the database lists 56 probands and 43 relatives with the associated clinical phenotype when available. The identification of a larger number of THAP1 mutations and collection of high-quality clinical information for each described mutation through international collaborative effort will help investigating the structure-function and genotype-phenotype correlations in DYT6
dystonia
.
...
PMID:DYT6 dystonia: review of the literature and creation of the UMD Locus-Specific Database (LSDB) for mutations in the THAP1 gene. 2179 5
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