Megalin Knockout Reduces SGLT2 Expression and Sensitizes to Western Diet-induced Kidney Injury

Author:

Youm Elynna B12,Shipman Katherine E1ORCID,Albalawy Wafaa N12,Vandevender Amber M3,Sipula Ian J3,Rbaibi Youssef1,Marciszyn Allison E1,Lashway Jared A3,Brown Emma E1,Bondi Corry B1,Boyd-Shiwarski Cary R1,Tan Roderick J1,Jurczak Michael J3ORCID,Weisz Ora A1

Affiliation:

1. Renal-Electrolyte Division, University of Pittsburgh School of Medicine , Pittsburgh, PA 15261 , USA

2. Department of Human Genetics, University of Pittsburgh School of Public Health , Pittsburgh, PA 15261 , USA

3. Division of Endocrinology and Metabolism, Department of Medicine, University of Pittsburgh School of Medicine , Pittsburgh, PA 15261 , USA

Abstract

Abstract Megalin (Lrp2) is a multiligand receptor that drives endocytic flux in the kidney proximal tubule (PT) and is necessary for the recovery of albumin and other filtered proteins that escape the glomerular filtration barrier. Studies in our lab have shown that knockout (KO) of Lrp2 in opossum PT cells leads to a dramatic reduction in sodium–glucose co-transporter 2 (SGLT2) transcript and protein levels, as well as differential expression of genes involved in mitochondrial and metabolic function. SGLT2 transcript levels are reduced more modestly in Lrp2 KO mice. Here, we investigated the effects of Lrp2 KO on kidney function and health in mice fed regular chow (RC) or a Western-style diet (WD) high in fat and refined sugar. Despite a modest reduction in SGLT2 expression, Lrp2 KO mice on either diet showed increased glucose tolerance compared to control mice. Moreover, Lrp2 KO mice were protected against WD-induced fat gain. Surprisingly, renal function in male Lrp2 KO mice on WD was compromised, and the mice exhibited significant kidney injury compared with control mice on WD. Female Lrp2 KO mice were less susceptible to WD-induced kidney injury than male Lrp2 KO. Together, our findings reveal both positive and negative contributions of megalin expression to metabolic health, and highlight a megalin-mediated sex-dependent response to injury following WD.

Funder

NIH

Dialysis Clinic, Inc.

Publisher

Oxford University Press (OUP)

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