Drug repurposing screen identifies Foxo1-dependent angiopoietin-2 regulation in sepsis
CC Ghosh, K Thamm, AV Berghelli… - Critical care …, 2015 - journals.lww.com
CC Ghosh, K Thamm, AV Berghelli, C Schrimpf, MR Maski, T Abid, KE Milam, A Rajakumar…
Critical care medicine, 2015•journals.lww.comObjective: The recent withdrawal of a targeted sepsis therapy has diminished
pharmaceutical enthusiasm for developing novel drugs for the treatment of sepsis.
Angiopoietin-2 is an endothelial-derived protein that potentiates vascular inflammation and
leakage and may be involved in sepsis pathogenesis. We screened approved compounds
for putative inhibitors of angiopoietin-2 production and investigated underlying molecular
mechanisms. Design: Laboratory and animal research plus prospective placebo-controlled …
pharmaceutical enthusiasm for developing novel drugs for the treatment of sepsis.
Angiopoietin-2 is an endothelial-derived protein that potentiates vascular inflammation and
leakage and may be involved in sepsis pathogenesis. We screened approved compounds
for putative inhibitors of angiopoietin-2 production and investigated underlying molecular
mechanisms. Design: Laboratory and animal research plus prospective placebo-controlled …
Abstract
Objective:
The recent withdrawal of a targeted sepsis therapy has diminished pharmaceutical enthusiasm for developing novel drugs for the treatment of sepsis. Angiopoietin-2 is an endothelial-derived protein that potentiates vascular inflammation and leakage and may be involved in sepsis pathogenesis. We screened approved compounds for putative inhibitors of angiopoietin-2 production and investigated underlying molecular mechanisms.
Design:
Laboratory and animal research plus prospective placebo-controlled randomized controlled trial (NCT00529139) and retrospective analysis (NCT00676897).
Setting:
Research laboratories of Hannover Medical School and Harvard Medical School.
Patients:
Septic patients/C57Bl/6 mice and human endothelial cells.
Interventions:
Food and Drug Administration–approved library screening.
Measurements and Main Results:
In a cell-based screen of more than 650 Food and Drug Administration–approved compounds, we identified multiple members of the 3-hydroxy-3-methyl-glutaryl-CoA reductase inhibitor drug class (referred to as statins) that suppressed angiopoietin-2. Simvastatin inhibited 3-hydroxy-3-methyl-glutaryl-CoA reductase, which in turn activated PI3K-kinase. Downstream of this signaling, PI3K-dependent phosphorylation of the transcription factor Foxo1 at key amino acids inhibited its ability to shuttle to the nucleus and bind cis-elements in the angiopoietin-2 promoter. In septic mice, transient inhibition of angiopoietin-2 expression by liposomal siRNA in vivo improved absolute survival by 50%. Simvastatin had a similar effect, but the combination of angiopoietin-2 siRNA and simvastatin showed no additive benefit. To verify the link between statins and angiopoietin-2 in humans, we performed a pilot matched case-control study and a small randomized placebo-controlled trial demonstrating beneficial effects on angiopoietin-2.
Conclusions:
3-hydroxy-3-methyl-glutaryl-CoA reductase inhibitors may operate through a novel Foxo1-angiopoietin-2 mechanism to suppress de novo production of angiopoietin-2 and thereby ameliorate manifestations of sepsis. Given angiopoietin-2’s dual role as a biomarker and candidate disease mediator, early serum angiopoietin-2 measurement may serve as a stratification tool for future trials of drugs targeting vascular leakage.
Lippincott Williams & Wilkins