This study reveals that a novel antibacterial toxin from Yersinia kristensenii shares a common structural fold with RNase A and possesses the superfamily's characteristic ribonuclease activity. Homologs of this toxin are associated with diverse secretion systems in both Gram-negative and Gram-positive bacteria, suggesting that RNase A-like toxins are commonly deployed in inter-bacterial competition. Contact-dependent growth inhibition (CDI) is a toxin-delivery platform that is distributed widely amongst proteobacteria and is particularly common in pathogens. There is substantial functional and structural diversity observed between CDI toxin/immunity protein pairs, and these systems are important mediators of inter-cellular competition and self/nonself recognition in bacteria. Antibacterial toxin secretion systems are ubiquitous in nature and are beginning to inspire the development of “next generation” antimicrobial therapies.

Telomeres are special structures at the ends of linear chromosomes. Maintenance of functional telomeres is essential for genome stability, and dysregulation of telomere synthesis is one of the hallmarks of cancer. Human telomeres consist of several kilobases of repeated DNA sequences, terminating in a 3’ single-strand Grich DNA overhang. The overhang is synthesized by telomerase, which is often regarded as the essential regulator of overhang length. Here, the laboratory of Carolyn M. Price laboratory reports that filling-in of the recessed, C-rich strand is as important as the for maintaining human telomere length as telomerase itself. They mutated CTC1, a subunit of a multiprotein complex that aids in synthesis of the C-rich strand. Loss of CTC1 leads to gradual telomere shortening, akin to what is observed in cells that lack telomerase. In the absence of CTC1, telomerase continues to extend the G-rich DNA overhang, but the elongated overhang cannot be converted to double-stranded D ...

Toxin-antitoxin systems become activated in bacteria under stress conditions and enable bacterial cells to survive episodes of stress including antibiotic challenges. This phenomenon is called persistence and contributes to the difficulties in treating relapsing, chronic and biofilm producing bacterial infections. This paper shows how the ratio of CcdB toxin to CcdA antitoxin determines transcriptional regulation of the ccdAB module. Depending on the exact ratio, CcdA can combine with CcdB and multiple low-affinity binding sites on operator DNA to form helical assemblies of alternating chains of CcdA and CcdB dimers that cover the operator and repress transcription of the ccdAB operon; alternatively, the two proteins can form DNA-free heterohexamers that relieve repression. The study uncovers an unusual mechanism of transcriptional regulation and helps to better understand the features of toxin-antitoxin systems.