A lymphatic-absorbed multi-targeted kinase inhibitor for myelofibrosis therapy.
Brian D RossYoungsoon JangAmanda WeltonChristopher A BonhamDilrukshika S W PalagamaKevin HeistJagadish BoppisettiKasun P ImaduwageTanner H RobisonLeah R KingEdward Z ZhangCyrus AmirfazliKathryn E LukerWinston Y LeeGary D LukerThomas L ChenevertMarcian E Van DortPublished in: Nature communications (2022)
Activation of compensatory signaling nodes in cancer often requires combination therapies that are frequently plagued by dose-limiting toxicities. Intestinal lymphatic drug absorption is seldom explored, although reduced toxicity and sustained drug levels would be anticipated to improve systemic bioavailability. A potent orally bioavailable multi-functional kinase inhibitor (LP-182) is described with intrinsic lymphatic partitioning for the combined targeting of phosphoinositide 3-kinase (PI3K) and mitogen-activated protein kinase (MAPK) signaling pathways without observable toxicity. We demonstrate selectivity and therapeutic efficacy through reduction of downstream kinase activation, amelioration of disease phenotypes, and improved survival in animal models of myelofibrosis. Our further characterization of synthetic and physiochemical properties for small molecule lymphatic uptake will support continued advancements in lymphatropic therapy for altering disease trajectories of a myriad of human disease indications.
Keyphrases
- lymph node
- small molecule
- signaling pathway
- oxidative stress
- endothelial cells
- protein kinase
- tyrosine kinase
- cancer therapy
- papillary thyroid
- pi k akt
- stem cells
- young adults
- epithelial mesenchymal transition
- bone marrow
- induced apoptosis
- neoadjuvant chemotherapy
- replacement therapy
- electronic health record
- smoking cessation
- oxide nanoparticles