Mast cells are protective against snake venom sarafotoxins that belong to the endothelin (ET) peptide family. The molecular mechanism underlying this recently recognized innate defense pathway is unknown, but secretory granule proteases have been invoked. To specifically disrupt a single protease function without affecting expression of other proteases, we have generated a mouse mutant selectively lacking mast cell carboxypeptidase A (Mc-cpa) activity. Using this mutant, we have now identified Mc-cpa as the essential protective mast cell enzyme. Mass spectrometry of peptide substrates after cleavage by normal or mutant mast cells showed that removal of a single amino acid, the C-terminal tryptophan, from ET and sarafotoxin by Mc-cpa is the principle molecular mechanism underlying this very rapid mast cell response. Mast cell proteases can also cleave ET and sarafotoxin internally, but such “nicking” is not protective because intramolecular disulfide bridges maintain peptide function. We conclude that mast cells attack ET and sarafotoxin exactly at the structure required for toxicity, and hence sarafotoxins could not “evade” Mc-cpa's substrate specificity without loss of toxicity.
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29 October 2007
Article|
October 08 2007
Molecular mechanism of mast cell–mediated innate defense against endothelin and snake venom sarafotoxin
Lars A. Schneider,
Lars A. Schneider
1Institute for Immunology
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Susan M. Schlenner,
Susan M. Schlenner
1Institute for Immunology
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Thorsten B. Feyerabend,
Thorsten B. Feyerabend
1Institute for Immunology
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Markus Wunderlin,
Markus Wunderlin
2Section for Mass Spectrometry, Institute for Organic Chemistry II, University of Ulm, D-89081 Ulm, Germany
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Hans-Reimer Rodewald
Hans-Reimer Rodewald
1Institute for Immunology
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Lars A. Schneider
1Institute for Immunology
Susan M. Schlenner
1Institute for Immunology
Thorsten B. Feyerabend
1Institute for Immunology
Markus Wunderlin
2Section for Mass Spectrometry, Institute for Organic Chemistry II, University of Ulm, D-89081 Ulm, Germany
Hans-Reimer Rodewald
1Institute for Immunology
CORRESPONDENCE H.R. Rodewald: [email protected]
Abbreviations used: ET, endothelin; Mc-cpa, mast cell carboxypeptidase A; Mcp, mast cell protease; PEC, peritoneal exudate cell; S6b, sarafotoxin 6b.
L.A. Schneider, S.M. Schlenner, and T.B. Feyerabend contributed equally to this paper.
Received:
June 21 2007
Accepted:
September 17 2007
Online ISSN: 1540-9538
Print ISSN: 0022-1007
The Rockefeller University Press
2007
J Exp Med (2007) 204 (11): 2629–2639.
Article history
Received:
June 21 2007
Accepted:
September 17 2007
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Citation
Lars A. Schneider, Susan M. Schlenner, Thorsten B. Feyerabend, Markus Wunderlin, Hans-Reimer Rodewald; Molecular mechanism of mast cell–mediated innate defense against endothelin and snake venom sarafotoxin . J Exp Med 29 October 2007; 204 (11): 2629–2639. doi: https://doi.org/10.1084/jem.20071262
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