Abstract

It is being increasingly recognized that multiple pathways contribute to necrotic cell death in a highly regulated fashion and are amenable to specific interventions. Processes that have been implicated include necrotic cell death related to development of the mitochondrial permeability transition (MPT) regulated by cyclophilin D (CypD), necroptosis mediated by receptor-interacting protein kinases 1 and 3 (RIPK1 and RIPK3) and sensitive to inhibition by necrostatin-1, and pyroptosis resulting from activation of caspases 1 and 11. The ultimate downstream event required for several of the necrotic, immunogenic processes is glycine-sensitive opening of a plasma membrane channel. Preliminary studies for this proposal show that an additional pathway of iron-mediated cell death termed 'ferroptosis' may account for the iron-related cell injury involved in several common and clinically relevant forms of acute kidney injury (AKI). Ferroptosis is subject to modulation by novel small molecule inhibitors that emerged from chemical library screening, ferrostatins, as well as by other lipophilic antioxidants and by inhibition of NADPH oxidase. The objectives of this proposal are to further investigate and clarify the mechanisms of ferroptosis and its expression in freshly isolated kidney proximal tubules ex vivo, its impact on AKI in vivo, and its interactions with necroptosis and cyclophilin D pathways of regulated necrosis to address the hypothesis that regulated necrosis resulting from additive effects of ferroptosis, induction of the MPT mediated by CypD, and necroptosis contributes to tubule cell killing during AKI and is a target for pharmacological intervention. Studies will utilie tubules from rabbits and mice subjected to injury ex vivo and in vivo models of mouse AKI along with pharmacologic modulators and mutant mice deficient in CypD or RIPK3, newly developed mice deficient in both CypD+RIPK3 or caspase+RIPK3, and mice deficient in NADPH oxidase 4. Tubules isolated by collagenase digestion will be subjected to oxidant and iron-induced injury by tert-butylhydroperoxide or by hydroxyquinoline plus ferrous ammonium sulfate, or to hypoxia/reoxygenation. Lethal membrane damage will be quantitated as the final endpoint, and, at time points preceding that damage, measurements of ATP, mitochondrial membrane potential, reactive oxygen species production, and lipid peroxidation will be made to assess the mechanisms of this injury and its modification by ferrostatins, pharmacologic inhibitors of the MPT and necroptosis, and absence of pathway proteins. AKI will be produced in vivo by glycerol-induced rhabdomyolysis, clamp ischemia, or cisplatin followed by assessment of renal function and structural changes. These studies will further elucidate the role of newly characterized forms of regulated necrosis during AKI and provide insight into approaches for ameliorating them and the organ failure that results.

Public Health Relevance

Acute kidney injury is a common cause of illness and death in hospitalized VA patients that greatly increases the cost of care. Many of its forms are characterized by a type of cell death termed necrosis. Although the end appearance of the cells has a common pattern, the processes at the cellular level leading to it have proven to be complex and subject to multiple types of regulation that were previously unsuspected. However, this provides new possibilities for prevention and treatment of the tissue damage and organ failure. The proposed studies will address three processes (ferroptosis, mitochondrial permeability transition, and necroptosis) for which there is new evidence of strong involvement in cell death during acute kidney injury. The work will assess their contributions individually and in combination and will test promising approaches for alleviating them.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Veterans Affairs (VA)
Type
Non-HHS Research Projects (I01)
Project #
1I01BX002367-01A1
Application #
8735503
Study Section
Nephrology (NEPH)
Project Start
2014-10-01
Project End
2018-09-30
Budget Start
2014-10-01
Budget End
2015-09-30
Support Year
1
Fiscal Year
2015
Total Cost
Indirect Cost

  Institution

Name
Veterans Health Administration
Department
Type
DUNS #
096318480
City
Ann Arbor
State
MI
Country
United States
Zip Code
48105

  Publications

von Mässenhausen, Anne; Tonnus, Wulf; Himmerkus, Nina et al. (2018) Phenytoin inhibits necroptosis. Cell Death Dis 9:359
Venkatachalam, Manjeri A; Weinberg, Joel M (2017) Pericytes Preserve Capillary Integrity to Prevent Kidney Hypoxia. J Am Soc Nephrol 28:717-719
Bienholz, Anja; Reis, Jonas; Sanli, Pinar et al. (2017) Citrate shows protective effects on cardiovascular and renal function in ischemia-induced acute kidney injury. BMC Nephrol 18:130
Lan, Rongpei; Geng, Hui; Singha, Prajjal K et al. (2016) Mitochondrial Pathology and Glycolytic Shift during Proximal Tubule Atrophy after Ischemic AKI. J Am Soc Nephrol 27:3356-3367
Sas, Kelli M; Kayampilly, Pradeep; Byun, Jaeman et al. (2016) Tissue-specific metabolic reprogramming drives nutrient flux in diabetic complications. JCI Insight 1:e86976
Weinberg, Joel M; Bienholz, Anja; Venkatachalam, M A (2016) The role of glycine in regulated cell death. Cell Mol Life Sci 73:2285-308
Venkatachalam, Manjeri A; Weinberg, Joel M; Kriz, Wilhelm et al. (2015) Failed Tubule Recovery, AKI-CKD Transition, and Kidney Disease Progression. J Am Soc Nephrol 26:1765-76
Linkermann, Andreas; Skouta, Rachid; Himmerkus, Nina et al. (2014) Synchronized renal tubular cell death involves ferroptosis. Proc Natl Acad Sci U S A 111:16836-41
Yusof, M Sukeri M; Wong, Sze Ting; Yamin, Bohari M (2011) 1-(Biphenyl-4-ylcarbon-yl)-3-(4-nitro-phen-yl)thio-urea. Acta Crystallogr Sect E Struct Rep Online 67:o2483