Renal biomarker changes associated with hyaline droplet nephropathy in rats are time and potentially compound dependent

David A Brott; Patricia Bentley; Murali V P Nadella; Dale Thurman; Jim Fikes; Letitia Cheatham; Frank McGrath; Wenli Luo; Lewis B Kinter

doi:10.1016/j.tox.2012.11.003

Renal biomarker changes associated with hyaline droplet nephropathy in rats are time and potentially compound dependent

Toxicology. 2013 Jan 7:303:133-8. doi: 10.1016/j.tox.2012.11.003. Epub 2012 Nov 14.

Authors

David A Brott¹, Patricia Bentley, Murali V P Nadella, Dale Thurman, Jim Fikes, Letitia Cheatham, Frank McGrath, Wenli Luo, Lewis B Kinter

Affiliation

¹ Global Safety Assessment, AstraZeneca Pharmaceuticals, Wilmington, DE 19850, USA. david.brott@astrazeneca.com

PMID: 23159986
DOI: 10.1016/j.tox.2012.11.003

Abstract

Alpha 2u-globulin mediated hyaline droplet nephropathy (HDN) is a male rat specific lesion induced when a compound or metabolite binds to alpha 2u-globulin. The objective of this study was to investigate if the newer and more sensitive renal biomarkers would be altered with HDN as well as be able to distinguish between HDN and oxidative stress-induced kidney injury. Rats were dosed orally for 7 days to determine (1) if HDN (induced by 2-propanol or D-limonene) altered the newer renal biomarkers and not BUN or creatinine, (2) if renal biomarkers could distinguish between HDN and oxidative stress-induced kidney injury (induced by potassium bromate), (3) sensitivity of HDN-induced renal biomarker changes relative to D-limonene dose, and (4) reversibility of HDN and renal biomarkers, using vehicle or 300 mg/kg/day D-limonene with 7 days of dosing and necropsies scheduled over the period of Days 8-85. HDN-induced renal biomarker changes in male rats were potentially compound specific: (1) 2-propanol induced mild HDN without increased renal biomarkers, (2) potassium bromate induced moderate HDN with increased clusterin, and (3) D-limonene induced marked HDN with increased αGST, μGST and albumin. Administration of potassium bromate did not result in oxidative stress-induced kidney injury, based on histopathology and renal biomarkers creatinine and BUN. The compound D-limonene induced a dose dependent increase in HDN severity and renal biomarker changes without altering BUN, creatinine or NAG: (1) minimal induction of HDN and no altered biomarkers at 10 mg/kg/day, (2) mild induction of HDN with increased αGST and μGST at 50 mg/kg/day and (3) marked induction of HDN with increased αGST, μGST and albumin at 300 mg/kg/day. HDN induced by D-limonene was reversible, but with a variable renal biomarker pattern over time: Day 8 there was increased αGST, μGST and albumin; on Day 15 increased clusterin, albumin and Kim-1. In summary, HDN altered the newer and more sensitive renal biomarkers in a time and possibly compound dependent manner.

MeSH terms

1-Propanol / administration & dosage
1-Propanol / toxicity
Alpha-Globulins / metabolism*
Animals
Biomarkers / metabolism
Blood Urea Nitrogen
Bromates / toxicity
Creatinine / metabolism
Cyclohexenes / administration & dosage
Cyclohexenes / toxicity
Dose-Response Relationship, Drug
Female
Hyalin / metabolism*
Kidney Diseases / diagnosis
Kidney Diseases / pathology*
Limonene
Male
Oxidative Stress*
Rats
Rats, Wistar
Severity of Illness Index
Terpenes / administration & dosage
Terpenes / toxicity
Time Factors

Substances

Alpha-Globulins
Biomarkers
Bromates
Cyclohexenes
Terpenes
alpha 2u globulin
potassium bromate
1-Propanol
Limonene
Creatinine