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DHPLC can be used to detect low-level mutations in amyotrophic lateral sclerosis. | LitMetric

DHPLC can be used to detect low-level mutations in amyotrophic lateral sclerosis.

Amyotroph Lateral Scler

Department of Molecular and Clinical Genetics, Royal Prince Alfred Hospital, Sydney, Australia.

Published: August 2010

AI Article Synopsis

Article Abstract

Somatic mutations have been suggested as a cause of sporadic amyotrophic lateral sclerosis (SALS). These mutations can be difficult to detect since they may involve only a small percentage of cells within the tissue, so we devised a method to detect low mutation levels in brain DNA. Different proportions of a known SOD1 mutation were prepared to determine the sensitivity of DHPLC. The fraction containing the mutant signal was collected and re-amplified ('enriched') to increase sensitivity and to dideoxy sequence the mutation. The combined technique was used to screen all exons and the promoter of SOD1 in 23 SALS brains. DHPLC could detect a known SOD1 mutation in 5% of a sample of brain tissue. Using our enrichment technique doubled the height of the mutant sequencing signal, which allowed identification of an unknown mutation in 10% of brain tissue. No SOD1 mutations were found in the SALS brains using this technique. In conclusion, combining DHPLC and sequencing doubles the sensitivity of sequencing alone and can detect low levels of known and unknown mutations in brain DNA. No SALS SOD1 somatic mutations were detected, but DHPLC would be useful in looking for somatic mutations in other SALS candidate genes.

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Source
http://dx.doi.org/10.3109/17482960802572699DOI Listing

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