Neuropilin‐1 regulates renin synthesis in juxtaglomerular cells

Author:

Shen Yunzhu1,Lotenberg Kenza1,Zaworski Jeremy1,Broeker Katharina A.‐E.2ORCID,Vasseur Florence3,Louedec Liliane1ORCID,Placier Sandrine1ORCID,Frère Perrine1,Verpont Marie‐Christine1,Galichon Pierre1ORCID,Buob David1,Hadchouel Juliette1ORCID,Terzi Fabiola3,Chatziantoniou Christos1,Calmont Amélie1ORCID

Affiliation:

1. Sorbonne Université, INSERM, Unité mixte de Recherche 1155, Kidney Research Centre, Hôpital Tenon Paris France

2. Institut für Physiologie Universität Regensburg Regensburg Germany

3. Institut Necker Enfants Malades, Growth and Signalling departement Université Paris Cité, INSERM U1151, CNRS UMR 8253 Paris France

Abstract

AbstractRenin is the key enzyme of the systemic renin–angiotensin–aldosterone system, which plays an essential role in regulating blood pressure and maintaining electrolyte and extracellular volume homeostasis. Renin is mainly produced and secreted by specialized juxtaglomerular (JG) cells in the kidney. In the present study, we report for the first time that the conserved transmembrane receptor neuropilin‐1 (NRP1) participates in the development of JG cells and plays a key role in renin production. We used the myelin protein zero‐Cre (P0‐Cre) to abrogate Nrp1 constitutively in P0‐Cre lineage‐labelled cells of the kidney. We found that the P0‐Cre precursor cells differentiate into renin‐producing JG cells. We employed a lineage‐tracing strategy combined with RNAscope quantification and metabolic studies to reveal a cell‐autonomous role for NRP1 in JG cell function. Nrp1‐deficient animals displayed abnormal levels of tissue renin expression and failed to adapt properly to a homeostatic challenge to sodium balance. These findings provide new insights into cell fate decisions and cellular plasticity operating in P0‐Cre–expressing precursors and identify NRP1 as a novel key regulator of JG cell maturation. imageKey points Renin is a centrepiece of the renin–angiotensin–aldosterone system and is produced by specialized juxtaglomerular cells (JG) of the kidney. Neuropilin‐1 (NRP1) is a conserved membrane‐bound receptor that regulates vascular and neuronal development, cancer aggressiveness and fibrosis progression. We used conditional mutagenesis and lineage tracing to show that NRP1 is expressed in JG cells where it regulates their function. Cell‐specific Nrp1 knockout mice present with renin paucity in JG cells and struggle to adapt to a homeostatic challenge to sodium balance. The results support the versatility of renin‐producing cells in the kidney and may open new avenues for therapeutic approaches.

Funder

Agence Nationale de la Recherche

Publisher

Wiley

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