Nephron number determines susceptibility to renal mass reduction-induced CKD in Lewis and Fisher 344 rats: implications for development of experimentally induced chronic allograft nephropathy

doi:10.1093/ndt/gfn112

NDT Advance Access originally published online on March 10, 2008
Nephrology Dialysis Transplantation 2008 23(8):2492-2495; doi:10.1093/ndt/gfn112

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Nephron number determines susceptibility to renal mass reduction-induced CKD in Lewis and Fisher 344 rats: implications for development of experimentally induced chronic allograft nephropathy

Attila J. Szabo¹, Veronika Muller², Gin-Fu Chen³, Lennie J. Samsell⁴, Aaron Erdely⁵ and Chris Baylis³

¹ Department of Pediatrics ² Department of Pulmonology, Semmelweis University, Budapest, Hungary ³ Department of Physiology and Functional Genomics and Department of Medicine, University of Florida, Gainesville, FL ⁴ Department of Pediatrics, West Virginia University ⁵ Toxicology and Molecular Biology Branch, National Institute of Occupational Safety and Health, Morgantown, West Virginia, USA

Correspondence and offprint requests to: Chris Baylis, Department of Physiology and Functional Genomics and Department of Medicine, 1600 SW Archer Road, Room M554, University of Florida, PO Box 100274, Gainesville, FL 36210, USA. Tel: +1-352-392-7869; Fax: +1-352-392-7935; E-mail: baylisc{at}ufl.edu

Abstract

Background. The Fisher 344 (F344) rat kidney transplanted toa Lewis rat recipient is a common model of chronic renal allograftnephropathy (CAN); however, CAN does not develop when the Lewiskidney is grafted into a F344 recipient. In this study we investigatedwhether a difference in nephron number/glomerular volume existsbetween the strains that could contribute to a greater susceptibilityto development of kidney disease in the F344.

Methods. Separate animals, male F344 and Lewis rats, were subjectedto either sham surgery or right uni-nephrectomy and infarctionof 2/3 of the left kidney, to produce a 5/6 ablation/infarctioninjury (5/6 A/I). Serial urinary protein excretions were measured,a terminal 24-h creatinine clearance was obtained and rats werekilled 11 weeks after surgery and kidneys were harvestedfor pathology. Glomerular volumes were measured in the shamcontrols of each strain. Glomerular number was counted in separate,normal rats of each strain.

Results. The normal F344 had $~$ 30% fewer glomeruli than Lewisrats that were larger in volume. The sham F344 had similar creatinineclearance and glomerular structure to the Lewis shams, althoughBP and urine protein excretion were higher. After 5/6 A/I theF344 developed more severe proteinuria and structural kidneydamage. When factored for kidney weight, the F344 rats exhibiteda greater compensatory hyperfiltration in response to 5/6 A/I,compared to Lewis.

Conclusions. The F344 strain is more vulnerable to developmentof progressive kidney damage due to 5/6 A/I, compared to theLewis. This is likely due to the lower nephron number/greaterglomerular volume of the F344 that may also account for thegreater susceptibility to CAN exhibited by this strain.

Keywords: creatinine clearance; 5/6 renal ablation/infarction; glomerulosclerosis; proteinuria; rat strain

Received for publication: 3. 8.07
Accepted in revised form: 7. 2.08

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