A Phenylalanine Clamp Catalyzes Protein Translocation Through the Anthrax Toxin Pore

Bryan A. Krantz; Roman A. Melnyk; Sen Zhang; Stephen Juris; D. Borden Lacy; Zhengyan Wu; Alan Finkelstein; R. John Collier

doi:10.1126/science.1113380

A Phenylalanine Clamp Catalyzes Protein Translocation Through the Anthrax Toxin Pore

Bryan A. Krantz(Albert Einstein College of Medicine), Roman A. Melnyk(Albert Einstein College of Medicine), Sen Zhang(Albert Einstein College of Medicine), Stephen Juris(Albert Einstein College of Medicine), D. Borden Lacy(Albert Einstein College of Medicine), Zhengyan Wu(Albert Einstein College of Medicine), Alan Finkelstein(Albert Einstein College of Medicine), R. John Collier(Albert Einstein College of Medicine)

Science

July 28, 2005

10.1126/science.1113380

Cited by 298Open Access

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Abstract

The protective antigen component of anthrax toxin forms a homoheptameric pore in the endosomal membrane, creating a narrow passageway for the enzymatic components of the toxin to enter the cytosol. We found that, during conversion of the heptameric precursor to the pore, the seven phenylalanine-427 residues converged within the lumen, generating a radially symmetric heptad of solvent-exposed aromatic rings. This "phi-clamp" structure was required for protein translocation and comprised the major conductance-blocking site for hydrophobic drugs and model cations. We conclude that the phi clamp serves a chaperone-like function, interacting with hydrophobic sequences presented by the protein substrate as it unfolds during translocation.

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