ERM proteins regulate the shape and number of Endoplasmic Reticulum–Plasma Membrane Junctions in neurons

Endoplasmic Reticulum (ER) - Plasma Membrane (PM) Junctions (EPJs) are specialized contact sites between ER membrane and the inner leaflet of PM. These junctions are critical for lipid exchange and Ca²⁺signaling. In excitable cells like neurons and muscle, EPJs further modulate membrane excitability by regulating Ca²⁺homeostasis. The mechanisms controlling EPJ abundance and morphology remain poorly understood. Usingin vivofluorescence imaging and electron microscopy ofC. elegansneurons, we showed that EPJs form discrete, patch-like structures distributed across the soma. Through a forward genetics screen, we identified two conserved ERM (Ezrin-Radixin-Moesin) proteins, FRM-4 and FRM-1, as key regulators of EPJ shape and abundance. Both proteins localize to EPJs and exhibit liquid-liquid phase separation properties (LLPS).in vitro, purified FRM-4 binds to FRM-1, and together bundle filamentous actin. However, their presence in LLPS condensates and actin-bundling activity are mutually exclusive.In vivo, F-actin cables surround—but do not penetrate—EPJs, where FRM proteins are enriched as phase-separated condensates. Loss of FRM-4, FRM-1, or disruption of F-actin led to increased mobility of EPJs that fused into fewer but enlarged junctions. Together, our findings demonstrate that FRM-4 and FRM-1 control EPJ morphology by organizing peri-junctional F-actin networks, thereby restricting EPJ mobility and fusion.