![NA sensing by TLR7, TLR8 and TLR9. The liganded dimers of the extracellular domains of simian TLR7 [Protein Data Bank (PDB) ID: 5GMF], human TLR8 (PDB ID: 4R07) and horse TLR9 (PDB ID: 3WPC). TLR7 interacts with guanosine and the tri-ribonucleotide UUU. TLR8 binds to uridine and the di-nucleotide UG. TLR9 interacts with the ODN CpG. The figures were prepared with CueMol (http://www.cuemol.org). m_dxy01601.jpeg?Expires=1520598193&Signa](https://oup.silverchair-cdn.com/oup/backfile/Content_public/Journal/intimm/30/2/10.1093_intimm_dxy016/1/m_dxy01601.jpeg?Expires=1520598193&Signature=YCF1xIAupSNrCRn-yMYVU3aWfbsWlXHY4Gp70ZqYKgMBapYkqAoB~BWF8ZW1LMw~j7Nq9Ms~N4Fd0MX~u~o64M-pAwNCA6faD0lrS7Vj4USLW~K-4Z9JjcEKeZ6QO6eP1WWXe1ja2B6VUc0RglgpoqaFGEPRVxz5~ipsaxR9~0RXud3mjjU5gk8RdG24h965KesCfbFVHMZQfLufvmA-FEKJEDeJvoP7w63CXPWpv10d6mmKGvzWR4jIh-mKGP~WlGXm-MzYYVj2kFsHY4jgtZ5SQ2BCOBS5zb9FijMskf2p3qQ-XidA5ZeFfeT2PfpFdPGjbjelQQVHteKLyk7kng__&Key-Pair-Id=APKAIUCZBIA4LVPAVW3Q)
Abstract
Nucleic acid (NA)-sensing Toll-like receptors (TLRs) respond to DNA/RNA derived from pathogens and dead cells. Structural studies have revealed a variety of molecular mechanisms by which TLRs sense NAs. Double-stranded RNA and single-stranded DNA directly bind to TLR3 and TLR9, respectively, whereas TLR7 and TLR8 bind to nucleosides and oligoribonucleotides derived from RNAs. Activation of ligand-bound TLRs is influenced by the functional status of TLRs. Proteolytic cleavage of NA-sensing TLRs enables ligand-dependent TLR dimerization. Trafficking of ligand-activated TLRs in endosomal and lysosomal compartments is requisite for production of type I interferons. Activation of NA-sensing TLRs is required for the control of viruses such as herpes simplex virus and endogenous retroviruses. On the other hand, excessive activation of NA-sensing TLRs drives disease progression in a variety of inflammatory diseases including systemic lupus erythematosus, heart failure, arthritis and non-alcoholic steatohepatitis. NA-sensing TLRs are targets for therapeutic intervention in these diseases. We here focus on our recent progresses in our understanding of NA-sensing TLRs.
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