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ND12161
LCL
from
B-Lymphocyte
Description:
AMYOTROPHIC LATERAL SCLEROSIS 1; ALS1
ALS PANEL; LOWER-LIMB ONSET
ALS PANEL; LOWER-LIMB ONSET; PROBABLE AND POSSIBLE ALS
Affected:
Yes
Gender:
Male
Age:
55
YR
(At Sampling)
Sample Description
Overview
Characterizations
Phenotypic Data
Publications
External Links
Images
Culture Protocols
Overview
Repository
NINDS Repository
Subcollection
Motor Neuron Disease
Biopsy Source
Peripheral vein
Cell Type
B-Lymphocyte
Tissue Type
Blood
Transformant
Epstein-Barr Virus
Sample Source
LCL from B-Lymphocyte
Race
White
Subject Type
case-spouse
Family Type
NUCLEAR FAMILIES - ONE AFFECTED
Ethnicity
Not Hispanic/Latino
Country of Origin
USA
Family Member
1
Family History
N
Relation to Proband
proband
Species
Homo
sapiens
Common Name
Human
Characterizations
Gene
C9ORF72
Chromosomal Location
9p21
Allelic Variant 1
614260.0001
; FRONTOTEMPORAL DEMENTIA AND/OR AMYOTROPHIC LATERAL SCLEROSIS
Identified Mutation
(GGGGCC)n EXPANSION
; DeJesus-Hernandez et al. (2011) identified a polymorphic hexanucleotide repeat (GGGGCC) located between the noncoding exons 1a and 1b of the C9ORF72 gene. The maximum size of the repeat in healthy controls was 23 units, whereas it was expanded in members of a large family with frontotemporal dementia and/or anyotrophic lateral sclerosis mapping to chromosome 9p21 (FTDALS; 105550) (Boxer et al., 2011). Affected individuals had expanded repeat units ranging from 700 to 1,600. Further analysis identified this expanded hexanucleotide repeat in 16 (61.5%) of a series of 26 families with the disorder, as well as in 11.7% of familial FTD and 23.5% of familial ALS from 3 patient series. Sporadic cases with the expansion were also identified. Overall, 75 (10.4%) of 722 unrelated patients with FTD, ALS, or both were found to carry an expanded GGGGCC repeat, and DeJesus-Hernandez et al. (2011) concluded that it is the most common genetic abnormality in FTD/ALS. Longer repeats were associated with the A allele at SNP rs3849942, which marked a disease haplotype. The expanded repeat is located in the promoter region of C9ORF72 transcript variant 1 and in intron 1 of transcript variants 2 and 3. Tissue from affected individuals showed reduced or absent mRNA levels of C9ORF72 variants 1 and 3 compared to nonrepeat carriers, consistent with a loss-of-function mechanism. However, protein levels of these variants were similar to controls, and analysis of patient frontal cortex and spinal cord tissue showed that the transcribed expanded GGGGCC repeat formed nuclear RNA foci, suggesting a gain-of-function mechanism. Simultaneously and independently, Renton et al. (2011) identified the GGGGCC expanded repeat as a cause of FTD/ALS in families reported by Pearson et al. (2011) and Mok et al. (2011). The expanded repeat was also found in 46.4% of Finnish familial ALS cases and in 21% of sporadic cases. PCR assays showed that Finnish controls had between 0 and 22 repeats. FISH studies showed that the expansion in a family from Wales (Pearson et al., 2011) was at least 250 repeats. In addition, an expanded repeat was found in 102 (38.1%) of 268 familial ALS probands of European origin. Real-time RT-PCR analysis of expression in frontal cortex tissue from patients and controls did not detect conclusive changes in RNA levels and produced inconsistent results. Nevertheless, Renton et al. (2011) postulated that a disruption in RNA metabolism likely underlies this disorder.
Phenotypic Data
Demographic Data
Relation to Proband
proband
Age at Sampling
55 YR
Gender
Male
Age of Onset(If not a control)
52 YR
Age at Diagnosis(If not a control)
53 YR
Hispanic or Latino/Not Hispanic or Latino
Not Hispanic/Latino
Racial Category
White
Country
USA
Diagnosed By
No Data
Data Elements
Clinical Element Type: Motor Neuron Disorders
(Baseline)
Longitudinal Data
Is this data Longitudinal (Follow-Up) Data?
yes
no
Family History
ALS/other MND
present
absent
unknown
Parkinson's disease
present
absent
unknown
Alzheimer's disease
present
absent
unknown
Other dementia
present
absent
unknown
Other neurodegenerative disease
present
absent
unknown
Medical History
Alzheimer's disease
present
absent
Ataxia
present
absent
Autism
present
absent
Bipolar (manic-depressive)
present
absent
Brain aneurysm
present
absent
Cancer
present
absent
Dementia
Alzheimer's
Dementia
absent
Depression
present
absent
Diabetes
present
absent
Dystonia
present
absent
Epilepsy
present
absent
Heart disease
present
absent
Hypertension
present
absent
Multiple sclerosis
present
absent
Muscle disease
present
absent
Parkinson's
present
absent
Schizophrenia
present
absent
Suicide/Attempt
present
absent
Stroke
present
absent
Primary Clinical Diagnosis
Primary clinical diagnosis
ALS
Secondary Neurological Diagnosis
Secondary neurological diagnoses
Frontotemporal dementia
Other (specify)
Not Applicable
Site of Symptom Onset
site of symptom onset
Limb-lower
Treatment
Current treatment
Riluzole
PEG
NIPPV
Tracheotomy
Assisted Ventilation > 23 hours
Other (specify)
No Treatment
Signs Supporting Diagnosis
Upper Motor Neuron Signs-Bulbar
definite
indeterminate
absent
not tested
Upper Motor Neuron Signs-Cervical/upper limbs
definite
indeterminate
absent
not tested
Upper Motor Neuron Signs-Thoracic/chest
definite
indeterminate
absent
not tested
Upper Motor Neuron Signs-Lumbosacral/lower limbs
definite
indeterminate
absent
not tested
Lower Motor Neuron Signs-Bulbar
definite
indeterminate
absent
not tested
Lower Motor Neuron Signs-Cervical/upper limbs
definite
indeterminate
absent
not tested
Lower Motor Neuron Signs-Thoracic/chest
definite
indeterminate
absent
not tested
Lower Motor Neuron Signs-Lumbosacral/lower limbs
definite
indeterminate
absent
not tested
EMG Studies
Bulbar
acute denervation
chronic denervation
negative
not examined
acute/chronic denervation
Cervical/upper limbs
acute denervation
chronic denervation
negative
not examined
acute/chronic denervation
Thoracic/chest
acute denervation
chronic denervation
negative
not examined
acute/chronic denervation
Lumbosacral/lower limbs
acute denervation
chronic denervation
negative
not examined
acute/chronic denervation
Genetics
SOD-1 mutation
No Data
Other mutation
present
absent
unknown
Notes:
C9ORF72: (GGGGCC)N EXPANSION
Atypical Features of ALS/MND
Atypical features of ALS/MND
sensory
autonomic
cerebellar
cognitive
Parkinsonian
sphincter
ocular
other
Optional data
Current ALSFRS-R
No Data
FVC
No Data
smoking history
No Data
years smoking
No Data
Handedness
No Data
Publications
Abramzon Y, Johnson JO, Scholz SW, Taylor JP, Brunetti M, Calvo A, Mandrioli J, Benatar M, Mora G, Restagno G, ChiĆ² A, Traynor BJ
, Valosin-containing protein (VCP) mutations in sporadic amyotrophic lateral sclerosis Neurobiology of aging33:2231.e1-6 2012
PubMed ID:
22572540
External Links
NCBI GTR
105400 AMYOTROPHIC LATERAL SCLEROSIS 1; ALS1
OMIM
105400 AMYOTROPHIC LATERAL SCLEROSIS 1; ALS1
Omim Description
ALS
AMYOTROPHIC LATERAL SCLEROSIS
AMYOTROPHIC LATERAL SCLEROSIS, TYPE 1; ALS1
dbGaP Link
phs000101.v5.p1
Images
View
pedigree
Culture Protocols
Split Ratio (Frequency)
1:3 (4 Days)
Temperature
37 C
Percent CO2
5%
Percent O2
AMBIENT
Medium
Roswell Park Memorial Institute Medium 1640 with 2mM L-glutamine or equivalent
Serum
15% fetal bovine serum Not Inactivated
Substrate
None specified
Subcultivation Method
dilution - add fresh medium
Supplement
-
Pricing
Commercial:
$0.00
USD
Academic &
Non-profit:
$0.00
USD
Add to Cart
How to Order
Ordering Instructions
MTA / Assurance Form
Statement of Research Intent Form
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