| Literature DB >> 35001352 |
Yu Nee Lee1, Amit Nahum2,3, Ori Toker4, Arnon Broides5,2, Atar Lev1, Amos J Simon1, Orli Megged6, Oded Shamriz7,8, Yuval Tal8, Raz Somech1.
Abstract
X-linked agammaglobulinemia (XLA) is caused by mutations in the Bruton tyrosine kinase) BTK) gene. Affected patients have severely reduced amounts of circulating B cells. Patients with atypical XLA may have residual circulating B cells, and there are few studies exploring these cells' repertoire. We aimed to study the B cell repertoire of a novel hypomorphic mutation in the BTK gene, using the next generation sequencing (NGS) technology. Clinical data was collected from our clinical records. Real-time PCR was used to determine KREC copies, and NGS was used to determine the immunoglobulin (Ig) heavy chain (IgH) repertoire diversity. Both patients had a relatively mild clinical and laboratory phenotype, residual BTK protein expression, and the same novel mutation in the BTK gene, c.1841 T > C, p. L614P. Signal-joint kappa-deleting recombination excision circles (sj-KREC) for both patients were completely absent reflecting lack of naïve B cells. The intron RSS-Kde coding joints (cj) were significantly reduced, reflecting residual replicating B cells. NGS displayed restricted IgH repertoire with highly uneven distribution of clones, especially for Pt2. We report a novel BTK mutation, c.1841 T > C (p. L614P) that is associated with a relatively mild phenotype. We conclude that the IgH repertoire in atypical XLA is restricted with highly uneven distribution of clones. This phenomenon may be explained by extremely reduced to non-existent levels of BTK in B cells. This report sheds further light on atypical cases of XLA.Entities:
Keywords: Agammaglobulinemia; BTK; IgH repertoire diversity; KREC; XLA
Mesh:
Substances:
Year: 2022 PMID: 35001352 DOI: 10.1007/s12026-022-09263-2
Source DB: PubMed Journal: Immunol Res ISSN: 0257-277X Impact factor: 2.829