citations

                    Adrenomedullin-RAMP2 system suppresses ER stress-induced tubule cell death and is involved in kidney protection.
                

Authors:

Uetake R1, Sakurai T1, Kamiyoshi A1, Ichikawa-Shindo Y1, Kawate H1, Iesato Y1, Yoshizawa T1, Koyama T1, Yang L1, Toriyama Y1, Yamauchi A1, Igarashi K1, Tanaka M1, Kuwabara T2, Mori K3, Yanagita M4, Mukoyama M2, Shindo T1.

In:

Source: PLoS ONE
Publication Date: (2014)
Issue: 9(2): e87667

Research Area:

Basic Research

Cells used in publication:

Renal proximal tubule cells (RPTEC), human: Species: human; Tissue Origin: kidney

Culture Media:

Renal Epithelial Cell Growth Medium

Experiment

Abstract

Various bioactive peptides have been implicated in the homeostasis of organs and tissues. Adrenomedullin (AM) is a peptide with various bioactivities. AM-receptor, calcitonin-receptor-like receptor (CLR) associates with one of the subtypes of the accessory proteins, RAMPs. Among the RAMP subisoforms, only RAMP2 knockout mice (-/-) reproduce the phenotype of embryonic lethality of AM-/-, illustrating the importance of the AM-RAMP2-signaling system. Although AM and RAMP2 are abundantly expressed in kidney, their function there remains largely unknown. We used genetically modified mice to assess the pathophysiological functions of the AM-RAMP2 system. RAMP2+/- mice and their wild-type littermates were used in a streptozotocin (STZ)-induced renal injury model. The effect of STZ on glomeruli did not differ between the 2 types of mice. On the other hand, damage to the proximal urinary tubules was greater in RAMP2+/-. Tubular injury in RAMP2+/- was resistant to correction of blood glucose by insulin administration. We examined the effect of STZ on human renal proximal tubule epithelial cells (RPTECs), which express glucose transporter 2 (GLUT2), the glucose transporter that specifically takes up STZ. STZ activated the endoplasmic reticulum (ER) stress sensor protein kinase RNA-like endoplasmic reticulum kinase (PERK). AM suppressed PERK activation, its downstream signaling, and CCAAT/enhancer-binding homologous protein (CHOP)-induced cell death. We confirmed that the tubular damage was caused by ER stress-induced cell death using tunicamycin (TUN), which directly evokes ER stress. In RAMP2+/- kidneys, TUN caused severe injury with enhanced ER stress. In wild-type mice, TUN-induced tubular damage was reversed by AM administration. On the other hand, in RAMP2+/-, the rescue effect of exogenous AM was lost. These results indicate that the AM-RAMP2 system suppresses ER stress-induced tubule cell death, thereby exerting a protective effect on kidney. The AM-RAMP2 system thus has the potential to serve as a therapeutic target in kidney disease

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