Peroxisome proliferator-activated receptor gamma agonist ELB00824 suppresses oxaliplatin-induced pain, neuronal hypersensitivity, and oxidative stress

Morgan Zhang; Min Hu; Sascha R A Alles; Marena A Montera; Ian Adams; Maria D Santi; Kenji Inoue; Nguyen Huu Tu; Karin N Westlund; Yi Ye

doi:10.1016/j.neuropharm.2022.109233

Peroxisome proliferator-activated receptor gamma agonist ELB00824 suppresses oxaliplatin-induced pain, neuronal hypersensitivity, and oxidative stress

Neuropharmacology. 2022 Nov 1:218:109233. doi: 10.1016/j.neuropharm.2022.109233. Epub 2022 Aug 22.

Authors

Morgan Zhang¹, Min Hu², Sascha R A Alles³, Marena A Montera³, Ian Adams³, Maria D Santi⁴, Kenji Inoue⁴, Nguyen Huu Tu⁴, Karin N Westlund³, Yi Ye⁵

Affiliations

¹ Bluestone Center for Clinical Research, New York University College of Dentistry, 421 First Avenue, 233W, New York, NY, 10010, USA; Department of Molecular Pathobiology, New York University College of Dentistry, 345 E. 24th street, New York, NY, 10010, USA; USA Elixiria Biotech Inc, Hartsdale, NY, 10530, USA; Shanghai Elixiria Biotech Co. Ltd, 578 Yingkou Road, Yangpu District, Shanghai, 200433, China.
² Shanghai Elixiria Biotech Co. Ltd, 578 Yingkou Road, Yangpu District, Shanghai, 200433, China.
³ Department of Anesthesiology & Critical Care Medicine, MSC10 6000, 2211 Lomas Blvd. NE, University of New Mexico Health Sciences Center, Albuquerque, NM, 87131, USA.
⁴ Bluestone Center for Clinical Research, New York University College of Dentistry, 421 First Avenue, 233W, New York, NY, 10010, USA; Department of Molecular Pathobiology, New York University College of Dentistry, 345 E. 24th street, New York, NY, 10010, USA.
⁵ Bluestone Center for Clinical Research, New York University College of Dentistry, 421 First Avenue, 233W, New York, NY, 10010, USA; Department of Molecular Pathobiology, New York University College of Dentistry, 345 E. 24th street, New York, NY, 10010, USA. Electronic address: yy22@nyu.edu.

Abstract

Chemotherapy-induced neuropathic pain (CINP) is a debilitating and difficult-to-treat side effect of chemotherapeutic drugs. CINP is marked with oxidative stress and neuronal hypersensitivities. The peroxisome proliferator-activated receptor gamma (PPARγ) is a transcription factor that regulates genes involved in oxidative stress and inflammation. We hypothesize that PPARγ agonists are protective against CIPN by reducing oxidative stress and inhibiting neuronal hypersensitivities. To test our hypothesis, acute or chronic CIPN was introduced by short or long-term treatment of oxaliplatin in BALB/c mice. CIPN mice were treated with either a novel blood-brain barrier (BBB) penetrable PPARγ agonist ELB00824, or a BBB non-penetrable PPARγ agonist pioglitazone, or vehicle. Cold allodynia, mechanical allodynia, motor coordination, sedation and addiction were measured with dry ice, von Frey filaments, beam-walking tests, and conditioned place preference, respectively. Oxidative stress was accessed by measuring byproducts of protein oxidation (carbonyl and 3-Nitrotyrosine) and lipid peroxidation [Thiobarbituric acid reactive substances (TBARS)], as wells as gene expression of Cat, Sod2, Ppargc1a. The effects of ELB00824 on nociceptor excitability were measured using whole-cell electrophysiology of isolated dorsal root ganglion neurons. Preemptive ELB00824, but not pioglitazone, reduced oxaliplatin-induced cold and mechanical allodynia and oxidative stress. ELB0824 suppressed oxaliplatin-induced firing in IB4^- neurons. ELB00824 did not cause motor discoordination or sedation/addiction or reduce the antineoplastic activity of oxaliplatin (measured with an MTS-based cell proliferation assay) in a human colon cancer cell line (HCT116) and a human oral cancer cell line (HSC-3). Our results demonstrated that ELB00824 prevents oxaliplatin-induced pain, likely via inhibiting neuronal hypersensitivities and oxidative stress.

Keywords: Chemotherapy-induced neuropathy; Neuropathic pain; Non-addictive; Oxaliplatin; Oxidative stress; PPAR.

MeSH terms

Animals
Antineoplastic Agents*
Humans
Hyperalgesia / chemically induced
Hyperalgesia / drug therapy
Hyperalgesia / prevention & control
Hypersensitivity* / drug therapy
Mice
Neuralgia* / chemically induced
Neuralgia* / drug therapy
Neuralgia* / prevention & control
Neurons / metabolism
Oxaliplatin
Oxidative Stress
PPAR gamma / metabolism

Substances

Antineoplastic Agents
PPAR gamma
Oxaliplatin

Abstract

MeSH terms

Substances

Grants and funding