Abstract

We reported previously that overexpression of heterogeneous nuclear ribonucleoprotein F (Hnrnpf) in renal proximal tubular cells (RPTCs) suppresses angiotensinogen (Agt) expression, and attenuates systemic hypertension and renal injury in diabetic Hnrnpf-transgenic (Tg) mice. We thus hypothesized that deletion of Hnrnpf in the renal proximal tubules (RPT) of mice would worsen systemic hypertension and kidney injury, perhaps revealing novel mechanism(s). Tubule-specific Hnrnpf knockout (KO) mice were generated by crossbreeding Pax8-Cre mice with floxed Hnrnpf mice on a C57BL/6 background. Both male and female KO mice exhibited elevated systolic blood pressure, increased urinary albumin/creatinine ratio, tubulo-interstitial fibrosis and glycosuria without changes in blood glucose or glomerular filtration rate compared with control littermates. However, glycosuria disappeared in male KO mice at the age of 12 weeks, while female KO mice had persistent glycosuria. Agt expression was elevated, whereas sodium-glucose co-transporter 2 (Sglt2) expression was down-regulated in RPTs of both male and female KO mice as compared to control littermates. In vitro, KO of HNRNPF in human RPTCs (HK-2) by CRISPR gRNA up-regulated AGT and down-regulated SGLT2 expression. The Sglt2 inhibitor canagliflozin treatment had no effect on Agt and Sglt2 expression in HK-2 and in RPTCs of wild-type mice but induced glycosuria. Our results demonstrate that Hnrnpf plays a role in the development of hypertension and glycosuria through modulation of renal Agt and Sglt2 expression in mice, respectively.

Highlights

  • We report that tubule-specific (Pax8) heterogeneous nuclear ribonucleoprotein F (Hnrnpf) KO leads to elevated SBP and kidney injury via up-regulation of Agt and down-regulation of Sglt[2] expression in renal proximal tubular cells (RPTCs) in both sexes and results in glycosuria in a sex-dependent manner

  • LoxP sites were inserted to flank exon 4 of mouse Hnrnpf gene (Gene ID: 98758) which is localized on chromosome 6

  • Hnrnpf mRNA was barely detectable in renal proximal tubules (RPT) of both male and female KO mice at 8 and 24 weeks of age

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Summary

Introduction

We generated tubule-specific Hnrnpf KO mice by employing the Pax8-Cre/lox system[17] and monitored the development of phenotype in both male and female mice. We report that tubule-specific (Pax8) Hnrnpf KO leads to elevated SBP and kidney injury via up-regulation of Agt and down-regulation of Sglt[2] expression in RPTCs in both sexes and results in glycosuria in a sex-dependent manner. KO of HNRNPF by CRISPR gRNA confirmed the up-regulation and down-regulation of AGT and SGLT2 expression in human RPTCs (HK-2), respectively. Treatment with canagliflozin (an inhibitor of Sglt2) had no effect on Agt and Sglt[2] expression in HK-2 and in RPTCs of wild-type mice, whereas it induced glycosuria

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Conclusion

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