Disruption of podocyte cytoskeletal biomechanics by dasatinib leads to nephrotoxicity.
Rhodora C CalizoSmiti BhattacharyaJohan G C van HasseltChengguo WeiJenny S WongRobert J WienerXuhua GeNicholas J WongJia-Jye LeeChristina M CuttittaGomathi JayaramanVivienne H AuWilliam JanssenTong LiuHong LiFadi SalemEdgar A JaimesBarbara MurphyKirk N CampbellEvren U AzelogluPublished in: Nature communications (2019)
Nephrotoxicity is a critical adverse event that leads to discontinuation of kinase inhibitor (KI) treatment. Here we show, through meta-analyses of FDA Adverse Event Reporting System, that dasatinib is associated with high risk for glomerular toxicity that is uncoupled from hypertension, suggesting a direct link between dasatinib and podocytes. We further investigate the cellular effects of dasatinib and other comparable KIs with varying risks of nephrotoxicity. Dasatinib treated podocytes show significant changes in focal adhesions, actin cytoskeleton, and morphology that are not observed with other KIs. We use phosphoproteomics and kinome profiling to identify the molecular mechanisms of dasatinib-induced injury to the actin cytoskeleton, and atomic force microscopy to quantify impairment to cellular biomechanics. Furthermore, chronic administration of dasatinib in mice causes reversible glomerular dysfunction, loss of stress fibers, and foot process effacement. We conclude that dasatinib induces nephrotoxicity through altered podocyte actin cytoskeleton, leading to injurious cellular biomechanics.
Keyphrases
- high glucose
- chronic myeloid leukemia
- diabetic nephropathy
- drug induced
- atomic force microscopy
- endothelial cells
- systematic review
- randomized controlled trial
- type diabetes
- lymph node
- radiation therapy
- cell migration
- emergency department
- high speed
- adipose tissue
- adverse drug
- rectal cancer
- risk assessment
- climate change
- human health
- replacement therapy
- finite element analysis
- heat stress