Publications by authors named "N E Tumer"
Shiga toxins are the main virulence factors of Shiga toxin producing (STEC) and . There is no effective therapy to counter the disease caused by these toxins. The A1 subunits of Shiga toxins bind the C-termini of ribosomal P-stalk proteins to depurinate the sarcin/ricin loop.
View Article and Find Full Text PDFRicin is one of the most toxic substances known and a type B biothreat agent. Shiga toxins (Stxs) produced by E. coli (STEC) and Shigella dysenteriae are foodborne pathogens.
View Article and Find Full Text PDFRicin is a potent plant toxin that targets the eukaryotic ribosome by depurinating an adenine from the sarcin-ricin loop (SRL), a highly conserved stem-loop of the rRNA. As a category-B agent for bioterrorism it is a prime target for therapeutic intervention with antibodies and enzyme blocking inhibitors since no effective therapy exists for ricin. Ricin toxin A subunit (RTA) depurinates the SRL by binding to the P-stalk proteins at a remote site.
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- Shiga toxin 2a (Stx2a) is linked to hemolytic uremic syndrome, which causes kidney failure in children, by inhibiting protein synthesis in cells.
- The study identifies the minimal sequence of the ribosomal P-stalk proteins needed for Stx2A1's binding and its inhibitory effectiveness, focusing on the importance of the last eight amino acids.
- Researchers presented the X-ray crystal structure of Stx2A1 alone and with the P-stalk, revealing that specific contacts are crucial for Stx2A1's activity, highlighting the distinct interaction requirements among different ribosome-inactivating proteins.
Ricin, a category-B agent for bioterrorism, and Shiga toxins (Stxs), which cause food poisoning bind to the ribosomal P-stalk to depurinate the sarcin/ricin loop. No effective therapy exists for ricin or Stx intoxication. Ribosome binding sites of the toxins have not been targeted by small molecules.
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