Description:
NEUROPATHY, HEREDITARY SENSORY AND AUTONOMIC, TYPE III; HSAN3
INHIBITOR OF KAPPA LIGHT POLYPEPTIDE GENE ENHANCER IN B CELLS, KINASE-COMPLEX ASSOCIATED PROTEIN; IKBKAP
Repository
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NIGMS Human Genetic Cell Repository
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Subcollection |
Heritable Diseases |
Class |
Disorders of the Nervous System |
Quantity |
25 µg |
Quantitation Method |
Please see our FAQ |
Biopsy Source
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Peripheral vein
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Cell Type
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B-Lymphocyte
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Tissue Type
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Blood
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Transformant
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Epstein-Barr Virus
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Sample Source
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DNA from LCL
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Race
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White
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Ethnicity
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ASHKENAZI
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Family Member
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1
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Relation to Proband
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proband
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Confirmation
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Clinical summary/Case history
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Species
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Homo sapiens
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Common Name
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Human
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Remarks
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IDENTIFICATION OF SPECIES OF ORIGIN |
Species of Origin Confirmed by Nucleoside Phosphorylase, Glucose-6-Phosphate Dehydrogenase, and Lactate Dehydrogenase Isoenzyme Electrophoresis |
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GENE MAPPING & DOSAGE STUDIES - Y CHROMOSOME |
PCR analysis of DNA from this cell culture gave a negative result with a primer for Yq11, DYS227. |
|
Gene |
IKBKAP |
Chromosomal Location |
9q31 |
Allelic Variant 1 |
603722.0001; FAMILIAL DYSAUTONOMIA |
Identified Mutation |
c.2204+6T>C (IVS20+6T>C); Slaugenhaupt et al. (2001) found that more than 99.5% of disease alleles causing familial dysautonomia (223900) in Ashkenazi Jewish individuals carried a donor splice site mutation (IVS20+6T-C) which leads to deletion of exon 20 from mRNA. Haplotype analyses were consistent with a common founder. Anderson et al. (2001) identified the same mutation in Ashkenazi Jewish patients with familial dysautonomia. |
|
Gene |
IKBKAP |
Chromosomal Location |
9q31 |
Allelic Variant 2 |
603722.0001; FAMILIAL DYSAUTONOMIA |
Identified Mutation |
c.2204+6T>C (IVS20+6T>C); Slaugenhaupt et al. (2001) found that more than 99.5% of disease alleles causing familial dysautonomia (223900) in Ashkenazi Jewish individuals carried a donor splice site mutation (IVS20+6T-C) which leads to deletion of exon 20 from mRNA. Haplotype analyses were consistent with a common founder. Anderson et al. (2001) identified the same mutation in Ashkenazi Jewish patients with familial dysautonomia. |
Remarks |
Clinically affected; alacrima; no corneal problems; color blindness; strabismus; mild left exotropia; no depth perception; recurrent Staphylococcal pneumonias; cyanotic nailbeds; chronic interstitial fibrosis noted on chext x-ray; kyphoscoliosis; epidural hematoma with surgical removal and subsequent seizure disorder; vomiting crises during premenstrual week but vomiting resolved with initiation of Ovral 21; postural hypotension; recurrent otitis media during infancy; absent right corneal reflex; almost no appreciation of "sharp" on face; vibration sense slighlty decreased in all extremities; complete absence of pain sensation in right leg; azotemia; evidence of progressive renal insufficiency; only one of four odors identified; affected brother is GM09297; unaffected siblings are GM09298, GM09302; mother is GM09764; donor subject is homozygous for the 2507+6T>C mutation in the IKBKAP gene; this donor splice site mutation (IVS20+6T>C) leads to deletion of exon 20 from the mRNA |
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