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An engineered bacterial therapeutic lowers urinary oxalate in preclinical models and in silico simulations of enteric hyperoxaluria
Authors:David Lubkowicz  Nicholas G Horvath  Michael J James  Pasquale Cantarella  Lauren Renaud  Christopher G Bergeron  Ron B Shmueli  Cami Anderson  Jian&#x;Rong Gao  Caroline B Kurtz  Mylene Perreault  Mark R Charbonneau  Vincent M Isabella  David L Hava
Institution:1. Synlogic Therapeutics, Cambridge MA, USA
Abstract:Enteric hyperoxaluria (EH) is a metabolic disease caused by excessive absorption of dietary oxalate leading to the formation of chronic kidney stones and kidney failure. There are no approved pharmaceutical treatments for EH. SYNB8802 is an engineered bacterial therapeutic designed to consume oxalate in the gut and lower urinary oxalate as a potential treatment for EH. Oral administration of SYNB8802 leads to significantly decreased urinary oxalate excretion in healthy mice and non‐human primates, demonstrating the strain''s ability to consume oxalate in vivo. A mathematical modeling framework was constructed that combines in vitro and in vivo preclinical data to predict the effects of SYNB8802 administration on urinary oxalate excretion in humans. Simulations of SYNB8802 administration predict a clinically meaningful lowering of urinary oxalate excretion in healthy volunteers and EH patients. Together, these findings suggest that SYNB8802 is a promising treatment for EH.
Keywords:engineered bacteria  enteric hyperoxaluria    in silico modeling  oxalate  synthetic biology
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