%0 Journal Article %1 SilasiMansat:2015eb %A Silasi-Mansat, Robert %A Zhu, Hua %A Georgescu, Constantin %A Popescu, Narcis %A Keshari, Ravi S %A Peer, Glenn %A Lupu, Cristina %A Taylor, Fletcher B. %A Pereira, Heloise Anne %A Kinasewitz, Gary %A Lambris, John D. %A Lupu, Florea %D 2015 %J Journal of cellular and molecular medicine %K imported %N 11 %P 2549--2563 %R 10.1111/jcmm.12667 %T Complement inhibition decreases early fibrogenic events in the lung of septic baboons. %U http://eutils.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&id=26337158&retmode=ref&cmd=prlinks %V 19 %X Acute respiratory distress syndrome (ARDS) induced by severe sepsis can trigger persistent inflammation and fibrosis. We have shown that experimental sepsis in baboons recapitulates ARDS progression in humans, including chronic inflammation and long-lasting fibrosis in the lung. Complement activation products may contribute to the fibroproliferative response, suggesting that complement inhibitors are potential therapeutic agents. We have been suggested that treatment of septic baboons with compstatin, a C3 convertase inhibitor protects against ARDS-induced fibroproliferation. Baboons challenged with 10(9) cfu/kg (LD50) live E. coli by intravenous infusion were treated or not with compstatin at the time of challenge or 5 hrs thereafter. Changes in the fibroproliferative response at 24 hrs post-challenge were analysed at both transcript and protein levels. Gene expression analysis showed that sepsis induced fibrotic responses in the lung as early as 24 hrs post-bacterial challenge. Immunochemical and biochemical analysis revealed enhanced collagen synthesis, induction of profibrotic factors and increased cell recruitment and proliferation. Specific inhibition of complement with compstatin down-regulated sepsis-induced fibrosis genes, including transforming growth factor-beta (TGF-$\beta$), connective tissue growth factor (CTGF), tissue inhibitor of metalloproteinase 1 (TIMP1), various collagens and chemokines responsible for fibrocyte recruitment (e.g. chemokine (C-C motif) ligand 2 (CCL2) and 12 (CCL12)). Compstatin decreased the accumulation of myofibroblasts and proliferating cells, reduced the production of fibrosis mediators (TGF-$\beta$, phospho-Smad-2 and CTGF) and inhibited collagen deposition. Our data demonstrate that complement inhibition effectively attenuates collagen deposition and fibrotic responses in the lung after severe sepsis. Inhibiting complement could prove an attractive strategy for preventing sepsis-induced fibrosis of the lung.

@article{SilasiMansat:2015eb, abstract = {Acute respiratory distress syndrome (ARDS) induced by severe sepsis can trigger persistent inflammation and fibrosis. We have shown that experimental sepsis in baboons recapitulates ARDS progression in humans, including chronic inflammation and long-lasting fibrosis in the lung. Complement activation products may contribute to the fibroproliferative response, suggesting that complement inhibitors are potential therapeutic agents. We have been suggested that treatment of septic baboons with compstatin, a C3 convertase inhibitor protects against ARDS-induced fibroproliferation. Baboons challenged with 10(9) cfu/kg (LD50) live E. coli by intravenous infusion were treated or not with compstatin at the time of challenge or 5 hrs thereafter. Changes in the fibroproliferative response at 24 hrs post-challenge were analysed at both transcript and protein levels. Gene expression analysis showed that sepsis induced fibrotic responses in the lung as early as 24 hrs post-bacterial challenge. Immunochemical and biochemical analysis revealed enhanced collagen synthesis, induction of profibrotic factors and increased cell recruitment and proliferation. Specific inhibition of complement with compstatin down-regulated sepsis-induced fibrosis genes, including transforming growth factor-beta (TGF-$\beta$), connective tissue growth factor (CTGF), tissue inhibitor of metalloproteinase 1 (TIMP1), various collagens and chemokines responsible for fibrocyte recruitment (e.g. chemokine (C-C motif) ligand 2 (CCL2) and 12 (CCL12)). Compstatin decreased the accumulation of myofibroblasts and proliferating cells, reduced the production of fibrosis mediators (TGF-$\beta$, phospho-Smad-2 and CTGF) and inhibited collagen deposition. Our data demonstrate that complement inhibition effectively attenuates collagen deposition and fibrotic responses in the lung after severe sepsis. Inhibiting complement could prove an attractive strategy for preventing sepsis-induced fibrosis of the lung.}, added-at = {2017-12-08T05:18:19.000+0100}, affiliation = {Programs in Cardiovascular Biology, Oklahoma Medical Research Foundation, Oklahoma City, OK, USA.}, author = {Silasi-Mansat, Robert and Zhu, Hua and Georgescu, Constantin and Popescu, Narcis and Keshari, Ravi S and Peer, Glenn and Lupu, Cristina and Taylor, Fletcher B. and Pereira, Heloise Anne and Kinasewitz, Gary and Lambris, John D. and Lupu, Florea}, biburl = {https://www.bibsonomy.org/bibtex/204f9ba63e466c15955050bfc7cc2e8b4/lambris}, date-added = {2017-12-08T03:20:43GMT}, date-modified = {2017-12-08T04:17:02GMT}, doi = {10.1111/jcmm.12667}, interhash = {0c512d04f8b0e7d4e51c54eb0ae6236d}, intrahash = {04f9ba63e466c15955050bfc7cc2e8b4}, journal = {Journal of cellular and molecular medicine}, keywords = {imported}, language = {English}, month = nov, number = 11, pages = {2549--2563}, pmcid = {PMC4627561}, pmid = {26337158}, rating = {0}, timestamp = {2017-12-08T05:18:19.000+0100}, title = {{Complement inhibition decreases early fibrogenic events in the lung of septic baboons.}}, uri = {\url{papers3://publication/doi/10.1111/jcmm.12667}}, url = {http://eutils.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&id=26337158&retmode=ref&cmd=prlinks}, volume = 19, year = 2015 }