Deficiencies of Bruton's tyrosine kinase (Btk) have been implicated in the pathogenesis of human X-linked agammaglobulinemia (XLA). The distinctive phenotype observed in B-cell deficiency indicates the crucial role of Btk in B-cell development. This report describes a nationwide study of Btk deficiency in Japan, covering 51 XLA patients (35 independent families). Along with the identification of mutations, the resulting protein products were characterized by an in vitro kinase assay and a Western blot analysis. Thirty-one of the families were found to have mutations in the coding region of Btk. Although mutations were not found in the cDNA of 4 families, the Btk transcripts of these patients were greatly reduced. The identification of several novel missense mutations, in combination with the result of other studies, clarified the presence of two (missense) mutation hot spots, one in the SH1 and the other in the PH domain. The absence of kinase activity seen in 32 of the families underscored the importance of Btk protein analysis as a diagnostic indicator of XLA. The protein analysis also clarified the different effects of missense mutations on kinase activity and protein stability.
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July 15, 1996
Identification of Bruton's tyrosine kinase (Btk) gene mutations and characterization of the derived proteins in 35 X-linked agammaglobulinemia families: a nationwide study of Btk deficiency in Japan
S Hashimoto,
S Hashimoto
Department of Medicine III, Osaka University Medical School, Japan.
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S Tsukada,
S Tsukada
Department of Medicine III, Osaka University Medical School, Japan.
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M Matsushita,
M Matsushita
Department of Medicine III, Osaka University Medical School, Japan.
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T Miyawaki,
T Miyawaki
Department of Medicine III, Osaka University Medical School, Japan.
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Y Niida,
Y Niida
Department of Medicine III, Osaka University Medical School, Japan.
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A Yachie,
A Yachie
Department of Medicine III, Osaka University Medical School, Japan.
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S Kobayashi,
S Kobayashi
Department of Medicine III, Osaka University Medical School, Japan.
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T Iwata,
T Iwata
Department of Medicine III, Osaka University Medical School, Japan.
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H Hayakawa,
H Hayakawa
Department of Medicine III, Osaka University Medical School, Japan.
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H Matsuoka,
H Matsuoka
Department of Medicine III, Osaka University Medical School, Japan.
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I Tsuge,
I Tsuge
Department of Medicine III, Osaka University Medical School, Japan.
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T Yamadori,
T Yamadori
Department of Medicine III, Osaka University Medical School, Japan.
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T Kunikata,
T Kunikata
Department of Medicine III, Osaka University Medical School, Japan.
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S Arai,
S Arai
Department of Medicine III, Osaka University Medical School, Japan.
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K Yoshizaki,
K Yoshizaki
Department of Medicine III, Osaka University Medical School, Japan.
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N Taniguchi,
N Taniguchi
Department of Medicine III, Osaka University Medical School, Japan.
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T Kishimoto
T Kishimoto
Department of Medicine III, Osaka University Medical School, Japan.
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Blood (1996) 88 (2): 561–573.
Citation
S Hashimoto, S Tsukada, M Matsushita, T Miyawaki, Y Niida, A Yachie, S Kobayashi, T Iwata, H Hayakawa, H Matsuoka, I Tsuge, T Yamadori, T Kunikata, S Arai, K Yoshizaki, N Taniguchi, T Kishimoto; Identification of Bruton's tyrosine kinase (Btk) gene mutations and characterization of the derived proteins in 35 X-linked agammaglobulinemia families: a nationwide study of Btk deficiency in Japan. Blood 1996; 88 (2): 561–573. doi: https://doi.org/10.1182/blood.V88.2.561.bloodjournal882561
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July 15 1996
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