1f0c

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1f0c, resolution 2.26Å

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STRUCTURE OF THE VIRAL SERPIN CRMA

Overview

BACKGROUND: Cowpox virus expresses the serpin CrmA (cytokine response, modifier A) in order to avoid inflammatory and apoptotic responses of, infected host cells. The targets of CrmA are members of the caspase family, of proteases that either initiate the extrinsic pathway of apoptosis, (caspases 8 and 10) or trigger activation of the pro-inflammatory, cytokines interleukin-1beta and interleukin-18 (caspase 1). RESULTS: We, have determined the structure of a cleaved form of CrmA to 2.26 A, resolution. CrmA has the typical fold of a cleaved serpin, even though it, lacks the N-terminal half of the A helix, the entire D helix, and a, portion of the E helix that are present in all other known serpins. The, reactive-site loop of CrmA was mutated to contain the optimal substrate, recognition sequence for caspase 3; however, the mutation only marginally, increased the ability of CrmA to inhibit caspase 3. Superposition of the, reactive-site loop of alpha1-proteinase inhibitor on the cleaved CrmA, structure provides a model for virgin CrmA that can be docked to caspase, 1, but not to caspase 3. CONCLUSIONS: CrmA exemplifies viral economy, selective pressure having resulted in a 'minimal' serpin that lacks the, regions not needed for structural integrity or inhibitory activity. The, docking model provides an explanation for the selectivity of CrmA. Our, demonstration that engineering optimal substrate recognition sequences, into the CrmA reactive-site loop fails to generate a good caspase 3, inhibitor is consistent with the docking model.

About this Structure

1F0C is a Protein complex structure of sequences from Cow pox virus with DTT as ligand. Full crystallographic information is available from OCA.

Reference

Crystal structure of the apoptotic suppressor CrmA in its cleaved form., Renatus M, Zhou Q, Stennicke HR, Snipas SJ, Turk D, Bankston LA, Liddington RC, Salvesen GS, Structure. 2000 Jul 15;8(7):789-97. PMID:10903953

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