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Prisijungti
Nustatymai
International Journal of Hematology 2015-Mar

Mutations in Bruton's tyrosine kinase impair IgA responses.

Straipsnius versti gali tik registruoti vartotojai
Prisijungti Registracija
Nuoroda įrašoma į mainų sritį
Noriko Mitsuiki
Xi Yang
Sophinus J W Bartol
Christina Grosserichter-Wagener
Yoshiyuki Kosaka
Hidetoshi Takada
Kohsuke Imai
Hirokazu Kanegane
Shuki Mizutani
Mirjam van der Burg
STRAIPSNIS: 25589397
DOI: 10.1007/s12185-015-1732-1
BioSeek: 25589397

Raktažodžiai

phospholipase

tyrosine

primary immunodeficiency diseases

agammaglobulinemia

dysgammaglobulinemia

Santrauka

X-linked agammaglobulinemia (XLA) is a primary immunodeficiency caused by mutations in Bruton's tyrosine kinase (BTK), and is characterized by markedly decreased numbers of blood B cells and an absence of all immunoglobulin isotypes. We performed whole exome sequencing in a male pediatric patient with dysgammaglobulinemia with IgA deficiency. Genetic analysis revealed a BTK missense mutation (Thr316Ala). To investigate whether a BTK mutation underlay this antibody deficiency with marked decrease of IgA in this patient, we performed functional analyses of B cells and phagocytes, and molecular analyses of somatic hypermutation and class switch recombination. The BTK missense mutation resulted in B cells with reduced BTK and high IgM expression. Equal proportions of CD19(low) and CD19(normal) fractions were observed, and both included naïve and memory B cells. Calcium influx and phospholipase Cγ2 phosphorylation upon IgM stimulation were marginally impaired in CD19(low), but not in CD19(+) B cells. Similar to XLA patients, IgA transcripts showed low SHM levels, whereas IgG transcripts were hardly affected. Our analyses suggest that the BTK mutation likely underlies the disease in this case, and that hypomorphic BTK mutations can result in normal circulating B cell numbers, but specifically impair IgA responses.

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