Functional significance of the Fas molecule in naive lymphocytes.

نویسندگان

  • S Senju
  • I Negishi
  • N Motoyama
  • F Wang
  • K Nakayama
  • P J Lucas
  • S Hatakeyama
  • Q Zhang
  • S Yonehara
  • D Y Loh
چکیده

The Fas molecule mediates apoptotic signal in many cell types. Mouse mutations (lpr, lprcg, gld), which impair the function of Fas, cause spontaneous autoimmune disease. We generated Fas-deficient (Fas-/-) mice by homologous recombination. In embryonic stem cells Fas-/- mice developed lpr-like disease, confirming that the abnormality of Fas is causal in the lpr phenotype. We also made Fas-/- chimeric mice composed of a mixture of Fas+/+ and Fas-/- cells. The chimeric mice also showed the lpr phenotype. In Fas-/-, chimeric mice, the Fas-deficient population expanded progressively among mature T and B lymphocytes. The expansion of Fas-deficient lymphocytes occurred at the naive, pre-primed, lymphocyte stage. These results suggest that the Fas molecule functions not only after antigenic stimulation, as previously hypothesized, but also at the naive lymphocyte stage.

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عنوان ژورنال:
  • International immunology

دوره 8 3  شماره 

صفحات  -

تاریخ انتشار 1996