Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: UMLS:C0013421 (
dystonia
)
8,418
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Linkage of the Huntington's disease gene to chromosome 4 in 1983 marked the birth of modern genetics in movement disorders. The discovery that an expanded trinucleotide DNA repeat was central to the mechanism of this disease has been repeated over and over in a growing list of inherited ataxias. In 1997, a different mutation and genetic mechanism was discovered in a severe type of generalized primary torsion dystonia - Oppenheim's
dystonia
. Before this, only the genetic cause for rare metabolic dystonias was known, notably dopa-responsive (Segawa's)
dystonia
. In the same year, from the identification of mutation in the alpha-synuclein gene in rare pedigrees with autosomal dominant parkinsonism, arose the concept that Parkinson's disease may be part of a broader group of 'synucleinopathies', in which there is a fundamental defect in protein processing. In the following year, mutations in autosomal recessive juvenile onset parkinsonism were found in a gene called '
parkin
'. Parkin mutations are a more common cause of parkinsonism than the rare alpha-synuclein mutations, particularly in young-onset disease. However, a most important understanding, occurring in the last year, has been the relationship between the
parkin
gene product, alpha-synuclein and abnormal protein degradation in the cell. A unified theory of neuronal death in Parkinson's disease is emerging, pointing to potential new therapies in the future.
...
PMID:Genetics of movement disorders: an abbreviated overview. 1237 57
Mutations in the
parkin
gene, PARK2, are a common cause of parkinsonism in familial as well as isolated cases with an age of onset <40 years and should be considered in the diagnostic work up of young-onset parkinsonism. We report a detailed clinical evaluation of a personal series of 24 patients with mutations in the
parkin
gene. The clinical presentation of most cases was broadly comparable to that of previous descriptions of autosomal recessive early-onset or juvenile parkinsonism and young-onset Parkinson's disease and also had similarities with phenotypes of dopa-responsive dystonia. However, our only case with consanguineous parents had an age of onset of 54 years. We report three new phenotypes at presentation: cervical
dystonia
; autonomic dysfunction and peripheral neuropathy; and pure exercise-induced
dystonia
. We emphasize a number of clinical features that can be seen in
parkin
disease: focal
dystonia
; early instability; freezing; festination or retropulsion; concurrent autonomic failure; dramatic response to anticholinergics; early or atypical L-dopa-induced dyskinesias; exquisite sensitivity to small doses of L-dopa; and recurrent psychosis, even taking L-dopa alone. We also report behavioural disorder prior to the onset of parkinsonism. Some relatives carrying a single
parkin
mutation without extrapyramidal symptoms or signs also had psychiatric symptoms that might be related to their carrier status.
...
PMID:Parkin disease: a phenotypic study of a large case series. 1276 48
Autosomal recessive juvenile parkinsonism (ARJP/PARK2) is a distinct clinical and genetic entity characterized by early-onset levodopa-responsive parkinsonism, foot
dystonia
, sleep benefit, and hyperactive tendon reflexes. We report a patient with genetically confirmed ARJP, who showed mild sensory disturbance and diminished deep tendon reflexes in the advanced stage. Nerve conduction studies revealed a sensory dominant neuropathy, which has not been described in ARJP. We suggest that peripheral neuropathy may occur in patients with advanced ARJP due to the loss of
parkin
protein function, although the function of
parkin
in the peripheral nervous system remains to be clarified.
...
PMID:Sensory neuropathy in autosomal recessive juvenile parkinsonism (PARK2). 1278
Parkin gene mutations have been detected in families with early-onset autosomal recessive parkinsonism. We report a novel heterozygous 40 base pair deletion in exon 3 of the
parkin
gene that increases the susceptibility of carriers to develop parkinsonism/
dystonia
and manifests remarkable variability in regard to age of onset and phenotype in a single family. After identifying the new mutation in the proband of this kindred, family members were contacted and evaluated by a movement disorders specialist using standardized protocols and prospectively set diagnostic criteria. Importantly, examining physicians and family members were blinded to the genetic testing. Five affected members in two generations carried the
parkin
mutation. The proband and one of his brothers had disease onset at 24 years of age while another brother had disease at age 44. One exhibited multi-focal
dystonia
and parkinsonism of 17 years duration, another suffered a unilateral slowly progressive parkinsonism over 13 years while the third suffered
dystonia
-parkinsonism of recent onset. A sibling pair in the preceding generation had mild previously undiagnosed parkinsonism. Clinicians should be aware that patients carrying a
parkin
gene mutation may present with
dystonia
-parkinsonism or very subtle parkinsonism with a markedly varied age of onset.
...
PMID:Marked variation in clinical presentation and age of onset in a family with a heterozygous parkin mutation. 1281 54
To establish phenotype-genotype correlations in early-onset parkinsonism, we have compared the phenotype of a large series of 146 patients with and 250 patients without
parkin
mutations. Although no single sign distinguished the groups, patients with mutations had significantly earlier and more symmetrical onset,
dystonia
more often at onset and hyperreflexia, slower progression of the disease, and a tendency toward a greater response to levodopa despite lower doses. After forward stepwise multiple logistic regression analysis,
dystonia
at onset and brisk reflexes were not longer significantly different but were correlated with age at onset rather than the presence of the
parkin
mutation. Age at onset in carriers of
parkin
mutations varied as did the rate of progression of the disease: the younger the age at onset the slower the evolution. The genotype influenced the phenotype: carriers of at least one missense mutation had a higher United Parkinson's Disease Rating Scale motor score than those carrying two truncating mutations. The localization of the mutations was also important because missense mutations in functional domains of
parkin
resulted in earlier onset. Patients with a single heterozygous mutation had significantly later and more asymmetrical onset and more frequent levodopa-induced fluctuations and
dystonia
than patients with two mutations.
...
PMID:How much phenotypic variation can be attributed to parkin genotype? 1289 70
Despite clinical and genetic complexity of
dystonia
, knowledge of primary torsion dystonia and
dystonia
-plus syndromes was recently expanded. Part of the category of primary
dystonia
includes genetic forms (DYT1, DYT6, DYT13). The DYTI mutation, with predominant limbs (95p. 100) and neck and trunk (25-35p. 100) involvement accounts for about 80p. 100 of the early onset cases in the Ashkenazi population and of 16-53p. 100 in the non- Ashkenazi population. The
dystonia
-plus group is defined by the association of parkinsonism (dopa-responsive-
dystonia
and rapid-onset
dystonia
-parkinsonism) or myoclonus (myoclonus-
dystonia
). Dopa-responsive-
dystonia
is a heterogeneous group with several causes (GCH1 mutations, compound mutations in GCH1, mutations in TH gene, or in 6-PTS gene). Differential diagnosis could be juvenile parkinsonism (
parkin
mutations). Epsilon-sarcoglycan mutation accounts for a sub-group of myoclonus-
dystonia
, but other genes are still unidentified. The vast majority of
dystonia
are sporadic and still unexplained. Functional imaging may bring new insights in disease mechanisms. Because of phenotypic overlaps, within
dystonia
, new classifications based on functional markers may emerge.
...
PMID:Dystonia: phenotypes and genotypes. 1462 53
Paroxysmal exercise-induced
dystonia
can occur with Parkinson's disease (PD), and in rare cases, this can also be the presenting symptom. We report on 2 second cousins (no known consanguinity) who presented with paroxysmal exercise-induced
dystonia
who later developed clinical features of PD. Although autosomal recessive inheritance was suggested, and the dystonic features further suggest
parkin
as a possible cause, sequencing for
parkin
mutations was negative and this family may represent a genetic variant of PD. Further genotype-phenotype studies in this and similar families may give clues to pre-symptomatic symptoms in PD and may reflect a particular phenotype of interest for genetics studies in the future.
...
PMID:Exercise-induced dystonia as a preceding symptom of familial Parkinson's disease. 1497 84
Early-onset autosomal recessive parkinsonism is associated with
parkin
gene mutations. Different
parkin
mutations occur in many ethnic backgrounds; however, the phenotype may vary. We studied 102 young-onset (age at onset <60 years) Parkinson's disease (PD) patients. From 102 patients, 40 with early-onset PD (<45 years at symptomatic onset) were selected for clinical assessment and
parkin
gene molecular analysis for duplications/deletions and point mutations. We identified
parkin
mutations in 7 of 40 early-onset patients; including novel compound heterozygotes and potential splice site changes. The mean age at onset in the 7
parkin
mutation-positive patients was 33 +/- 9 years (age range, 18-42 years), marginally lower than that of the 33
parkin
-negative early-onset patients, 38 +/- 7 years (age range, 17-45 years). A family history of PD was present in 4 of 7 patients with
parkin
mutations, compared with 6 of 33 early-onset
parkin
-negative patients. Overall,
parkin
mutations were found in 4 of 10 patients with a positive family history and 3 of 30 patients without a family history of PD. Patients with
parkin
mutations had more
dystonia
, dyskinesia, and sleep benefit compared with
parkin
-negative patients. We subsequently identified a single point mutation among the 62 young-onset (age at onset 45 to <60 years). Mutations in the
parkin
gene may account for approximately 17% of early-onset (age at onset <45 years) parkinsonism in Ireland, in agreement with previous European studies.
...
PMID:Parkinson's disease in Ireland: clinical presentation and genetic heterogeneity in patients with parkin mutations. 1519 7
Two homozygous mutations in the PINK1 gene, encoding a mitochondrial putative protein kinase, recently have been identified in families with PARK6-linked, autosomal recessive early-onset parkinsonism (AREP). Here, we describe a novel homozygous mutation (1573_1574 insTTAG) identified in an AREP patient, which causes a frameshift and truncation at the C-terminus of the PINK1 protein, outside the kinase catalytic domain. The clinical phenotype includes early-onset (28 years) parkinsonism, foot
dystonia
at onset, good levodopa response, slow progression, early levodopa-induced dyskinesias, and sleep benefit, thereby resembling closely
parkin
-related disease. These findings confirm that recessive mutations in PINK1 cause early-onset parkinsonism and expand the associated clinical phenotype.
...
PMID:Homozygous PINK1 C-terminus mutation causing early-onset parkinsonism. 1534 71
Autosomal recessive juvenile parkinsonism (AR-JP, PARK2) is characterized by an early onset parkinsonism, often presenting with
dystonia
as an early feature. Mutations in Parkin are a relatively common cause of AR-JP and are estimated to be present in approximately 30% of familial young onset Parkinson disease (PD) [Abbas et al. (1999); Hum Mol Genet 8:567-574]. These mutations include exon rearrangements (deletions and duplications), point mutations, and small deletions. Similar genomic mutations have been described in unrelated patients, thereby indicating independent mutational events or ancient founder effects. We have identified homozygous deletion mutations of exon 4 in Parkin in two unrelated families, one from Brazil and the other from Turkey [Dogu et al. (2004); Mov Dis 9:812-816; Khan et al., Mov Dis, in press]. We have performed molecular analysis of the deletion breakpoints and this data indicates these mutations originated independently. We present here data demonstrating that the mutation responsible for disease in the Brazilian kindred consists of two separate deletions (1,069 and 1,750 bp) surrounding and including exon 4. The deletion removing
parkin
exon 4 identified in the Turkish family extended 156,203 bp. In addition to demonstrating that disease in these families is not caused by a single founder mutation, these data show that there is no common fragile site between these mutational events.
...
PMID:Defining the ends of Parkin exon 4 deletions in two different families with Parkinson's disease. 1563 62
<< Previous
1
2
3
4
Next >>
