Scientific Report Human TLR8 senses UR/URR motifs in bacterial and mitochondrial RNA

نویسندگان

  • Anne Krüger
  • Marina Oldenburg
  • Chiranjeevi Chebrolu
  • Daniela Beisser
  • Julia Kolter
  • Anna M Sigmund
  • Jörg Steinmann
  • Simon Schäfer
  • Hubertus Hochrein
  • Sven Rahmann
  • Hermann Wagner
  • Philipp Henneke
  • Veit Hornung
  • Jan Buer
  • Carsten J Kirschning
چکیده

Toll-like receptor (TLR) 13 and TLR2 are the major sensors of Gram-positive bacteria in mice. TLR13 recognizes Sa19, a specific 23S ribosomal (r) RNA-derived fragment and bacterial modification of Sa19 ablates binding to TLR13, and to antibiotics such as erythromycin. Similarly, RNase A-treated Staphylococcus aureus activate human peripheral blood mononuclear cells (PBMCs) only via TLR2, implying single-stranded (ss) RNA as major stimulant. Here, we identify human TLR8 as functional TLR13 equivalent that promiscuously senses ssRNA. Accordingly, Sa19 and mitochondrial (mt) 16S rRNA sequence-derived oligoribonucleotides (ORNs) stimulate PBMCs in a MyD88-dependent manner. These ORNs, as well as S. aureus-, Escherichia coli-, and mt-RNA, also activate differentiated human monocytoid THP-1 cells, provided they express TLR8. Moreover, Unc93b1 / and Tlr8 / -THP-1 cells are refractory, while endogenous and ectopically expressed TLR8 confers responsiveness in a UR/URR RNA ligand consensus motif-dependent manner. If TLR8 function is inhibited by suppression of lysosomal function, antibiotic treatment efficiently blocks bacteria-driven inflammatory responses in infected human whole blood cultures. Sepsis therapy might thus benefit from interfering with TLR8 function.

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Human TLR8 senses UR/URR motifs in bacterial and mitochondrial RNA

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تاریخ انتشار 2015