A CONSERVED EPITOPE ON H+,K+-ADENOSINE TRIPHOSPHATASE OF PARIETAL-CELLS DISCERNED BY A MURINE GASTRITOGENIC T-CELL CLONE

被引：58

作者：

NISHIO, A

HOSONO, M

WATANABE, Y

SAKAI, M

OKUMA, M

MASUDA, T

机构：

[1] KYOTO UNIV, FAC MED, INST IMMUNOL, DEPT IMMUNOBIOL, SAKYO KU, KYOTO 606, JAPAN

[2] KYOTO UNIV, FAC MED, DEPT INTERNAL MED 1, KYOTO, JAPAN

[3] KYOTO UNIV, FAC PHARMACEUT SCI, CHEST DIS RES INST, DEPT IMMUNOL, KYOTO, JAPAN

[4] KYOTO UNIV, FAC MED, DEPT GASTROENTEROL ENDOSCOPY, KYOTO, JAPAN

来源：

GASTROENTEROLOGY | 1994年 / 107卷 / 05期

关键词：

D O I：

10.1016/0016-5085(94)90543-6

中图分类号：

R57 [消化系及腹部疾病];

学科分类号：

摘要：

Background/Aims: H+,K+-adenosine triphosphatase (H+,K+-ATPase) of parietal cells is an organ-specific enzyme recognized by autoantibodies found in human and murine autoimmune gastritis (AIG). Murine AIG can be induced in BALB/c mice by thymectomy 3 days after birth and is a T cell-mediated disease. This study examined the specificity of T cells that cause AIG and the role of H+,K+-ATPase in this disease. Methods: From an AIG mouse, a gastritogenic T-cell clone (II-6) was established, and its reactivity to synthetic peptides of H+,K+-ATPase was tested. Results: II-6 cells are CD4(+), V beta 14+, and interferon gamma producers. Adoptive transfer of II-6 cells to syngeneic nude mice resulted in AIG without the production of autoantibodies to parietal cells. The II-6 cells were responsive not only to murine but also to human and porcine parietal cells. Their proliferation was also induced by amino acids 891-905 (alpha(891)) and 892-906 (alpha(892)) of the alpha subunit of porcine and human H+,K+-ATPase, respectively. Conclusions: The T-cell response to a single epitope of H+,K+-Pase, the amino acid sequence of which is conserved among at least three mammals tested, is sufficient to cause AIG. Autoantibodies to parietal cells are not detected in these AIG mice.

引用

页码：1408 / 1414

页数：7

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