A subject with a novel type I bare lymphocyte syndrome has tapasin deficiency due to deletion of 4 exons by Alu-mediated recombination.

نویسندگان

  • Toshio Yabe
  • Sumiyo Kawamura
  • Masako Sato
  • Koichi Kashiwase
  • Hidenori Tanaka
  • Yoshihide Ishikawa
  • Yoji Asao
  • Junko Oyama
  • Kazuma Tsuruta
  • Katsushi Tokunaga
  • Kenji Tadokoro
  • Takeo Juji
چکیده

HLA class I expression depends on the formation of a peptide-loading complex composed of class I heavy chain; beta(2)-microglobulin; the transporter associated with antigen processing (TAP); and tapasin, which links TAP to the heavy chain. Defects in TAP result in a class I deficiency called the type I bare lymphocyte syndrome (BLS). In the present study, we examined a subject with a novel type I BLS who does not exhibit apparent TAP abnormalities but who has a tapasin defect. The subject's TAPASIN gene has a 7.4-kilobase deletion between introns 3 and 7; an Alu repeat-mediated unequal homologous recombination may be the cause of the deletion. No tapasin polypeptide was detected in the subject's cells. The cell surface class I expression level in tapasin-deficient cells was markedly reduced but the reduction was not as profound as in TAP-deficient cells. These results suggest that tapasin deficiency is another cause of type I BLS.

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Brief report A subject with a novel type I bare lymphocyte syndrome has tapasin deficiency due to deletion of 4 exons by Alu-mediated recombination

HLA class I expression depends on the formation of a peptide-loading complex composed of class I heavy chain; 2microglobulin; the transporter associated with antigen processing (TAP); and tapasin, which links TAP to the heavy chain. Defects in TAP result in a class I deficiency called the type I bare lymphocyte syndrome (BLS). In the present study, we examined a subject with a novel type I BLS ...

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عنوان ژورنال:
  • Blood

دوره 100 4  شماره 

صفحات  -

تاریخ انتشار 2002