Interaction of the sorting nexin 25 homologue Snazarus with Rab11 balances endocytic and secretory transport and maintains the ultrafiltration diaphragm in nephrocytes

Maruzs, Tamás ✉ [Maruzs, Tamás (genetika), author] Institute of Genetics; Feil-Börcsök, Dalma* [Feil-Börcsök, Dalma (genetika), author] Institute of Genetics; Lakatos, Enikő [Lakatos, Enikő (genetika), author] Institute of Genetics; Juhász, Gábor; Blastyák, András [Blastyák, András (genetika), author] Institute of Genetics; Hargitai, Dávid [Hargitai, Dávid (Sejtbiológia), author] Department of Anatomy, Cell and Developmental B... (ELTE / ELU FoS / Bio_I); Jean, Steve; Lőrincz, Péter [Lőrincz, Péter (Sejtbiológia), author] Department of Anatomy, Cell and Developmental B... (ELTE / ELU FoS / Bio_I); Juhász, Gábor ✉ [Juhász, Gábor (Sejtbiológia), author] Institute of Genetics; Department of Anatomy, Cell and Developmental B... (ELTE / ELU FoS / Bio_I)

English Article (Journal Article) Scientific
Published: MOLECULAR BIOLOGY OF THE CELL 1059-1524 1939-4586 34 (9) Paper: 0421 , 14 p. 2023
  • SJR Scopus - Cell Biology: Q1
Proper balance of exocytosis and endocytosis is important for the maintenance of plasma membrane lipid and protein homeostasis. This is especially critical in human podocytes and the podocyte-like Drosophila nephrocytes that both use a delicate diaphragm system with evolutionarily conserved components for ultrafiltration. Here we show that the sorting nexin 25 homolog Snazarus (Snz) binds to Rab11 and localizes to Rab11-positive recycling endosomes in Drosophila nephrocytes, unlike in fat cells where it is present in plasma membrane/lipid droplet/ER contact sites. Loss of Snz leads to redistribution of Rab11 vesicles from the cell periphery and increases endocytic activity in nephrocytes. These changes are accompanied by defects in diaphragm protein distribution that resemble those seen in Rab11 gain-of-function cells. Of note, co-overexpression of Snz rescues diaphragm defects in Rab11 overexpressing cells, whereas snz knockdown in Rab11 overexpressing nephrocytes or simultaneous knockdown of snz and tbc1d8b encoding a Rab11 GAP lead to massive expansion of the lacunar system that contains mislocalized diaphragm components: Sns and Pyd/ZO-1. We find that loss of Snz enhances while its overexpression impairs secretion, which, together with genetic epistasis analyses, suggest that Snz counteracts Rab11 to maintain the diaphragm via setting the proper balance of exocytosis and endocytosis.
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2025-01-16 02:45