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An engineered ligand trap inhibits leukemia inhibitory factor as pancreatic cancer treatment strategy

Commun Biol. 2021-04; 
Sean A Hunter, Brianna J McIntosh, Yu Shi, R Andres Parra Sperberg, Chie Funatogawa, Louai Labanieh, Erin Soon, Hannah C Wastyk, Nishant Mehta, Catherine Carter, Tony Hunter, Jennifer R Cochran
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Proteins, Expression, Isolation and Analysis Samples were boiled for 10 min before they were loaded onto a 15-well, 4–20% Expressplus PAGE gel (M42015, GenScript) Get A Quote

摘要

Leukemia inhibitory factor (LIF), a cytokine secreted by stromal myofibroblasts and tumor cells, has recently been highlighted to promote tumor progression in pancreatic and other cancers through KRAS-driven cell signaling. We engineered a high affinity soluble human LIF receptor (LIFR) decoy that sequesters human LIF and inhibits its signaling as a therapeutic strategy. This engineered 'ligand trap', fused to an antibody Fc-domain, has ~50-fold increased affinity (~20 pM) and improved LIF inhibition compared to wild-type LIFR-Fc, potently blocks LIF-mediated effects in pancreatic cancer cells, and slows the growth of pancreatic cancer xenograft tumors. These results, and the lack of apparent toxicity observe... More

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