AI Article Synopsis
- The report focuses on two Indian brothers and a Chinese patient who experience somatic reversion of harmful mutations in the WAS gene, which affects immune function.
- Both Indian siblings inherited a specific deletion mutation from their mother that caused a frameshift, but also presented a second deletion variant that restored the gene’s reading frame.
- The Chinese patient had a novel duplication mutation leading to a frameshift and was found to have both mutated and normal sequences in different blood cell types, with the reversion occurring selectively in T lymphocytes.
Article Abstract
This report describes two brothers from India and a Chinese patient with somatic reversion of an inherited deleterious mutation in the WAS gene. Both the Indian siblings had inherited a single nucleotide deletion causing a frameshift mutation (c.1190del, p.Pro397Argfs*48) (variant 1: marked in blue) from the mother. Another variant (variant 2: marked in red), a 12-nucleotide deletion at position 1188-1199 (c.1188_1199del, p.P401_P404del) was also found, which resulted in restoration of the frame and subsequent rescue of the protein sequence. DNA sequencing from buccal mucosal cells revealed only the inherited variant (variant 1), while no reversion mutation was identified in the mucosal cells. Similarly, the Chinese patient was found to have a novel germline 14-base duplication (ACGAAAATGCTTGG) c.120_132 + 1dup (variant 1). This resulted in abolishment of the original splice junction coupled with the creation of a new junction 14 bases 3' and a frameshift mutation with predicted protein truncation p. Thr45Aspfs*. DNA from the patient's PBMC showed co-existence of wild-type and mutated sequences, but only the mutant was present in the buccal cells. Genomic and mRNA analysis of the isolated CD3+ T lymphocytes, CD3- mononuclear cells, and EBV-transformed B lymphocytes indicated that the reverant variant (germline variant was restored to wild-type sequence) were selectively found in CD3+ T lymphocytes.
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| http://dx.doi.org/10.1111/sji.13408 | DOI Listing |
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