Actin cross-linking organizes basal body patterning through anomalous diffusion transitions

doi:10.64898/2026.05.14.725088

Actin cross-linking organizes basal body patterning through anomalous diffusion transitions

2026 · doi:10.64898/2026.05.14.725088

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This study reveals how actin cross-linking governs basal body organization by inducing transitions between anomalous diffusion states, influencing their spatial patterning.

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The study investigated how actin dynamics regulate spatial patterning of hundreds of centriole-derived basal bodies on the apical surface of multiciliated cells in developing Xenopus laevis embryos. Using high-resolution quantitative confocal and high-speed TIRF imaging alongside theoretical modeling, the authors found that basal body trajectories undergo time-resolved transitions between diffusive and anomalous motion, with distinct dynamic regimes correlating with apical surface expansion. They report that early actin remodeling disperses basal bodies by creating a permissive low-confinement environment, whereas later increased actin cross-linking forms a dense meshwork that constrains movement and promotes uniform basal body spacing; disrupting α-actinin-1 impairs the actin meshwork, weakens confinement, and disrupts regular spatial patterning. The paper does not explicitly discuss endometriosis or adenomyosis; it was included in the corpus via a keyword match in the upstream search index.

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Abstract Subcellular protein complexes and organelles exhibit diverse dynamic behaviors that reflect the mechanical constraints and organization of the intracellular environment. Although some structures follow classical Brownian motion, many display anomalous dynamics, including subdiffusion and superdiffusion, driven by viscoelasticity, molecular crowding, and cytoskeletal interactions. Transitions between these regimes are increasingly recognized as critical for subcellular organization, yet how they are regulated and influence pattern formation remains unclear. Here, we investigate the spatial arrangement of cilia on the apical surface of multiciliated cells (MCCs) in developing Xenopus laevis embryos, where coordinated ciliary beating depends on the precise organization of hundreds of centriole-derived basal bodies (BBs). Using quantitative confocal, high-resolution and high-speed TIRF imaging together with theoretical modeling, we show that BB trajectories undergo time-resolved transitions between diffusive and anomalous motion, with distinct regimes that correlate with apical surface expansion. During the early stages, actin remodeling facilitates the dispersal of BBs by providing a permissive, low-confinement environment. As development progresses, the actin network becomes increasingly cross-linked, forming a dense meshwork that constrains BB movement and promotes uniform spacing across the apical domain. Disruption of α-actinin-1, a major actin cross-linking protein, impairs the integrity of the apical actin meshwork, weakens BB confinement, and disrupts regular spatial patterning, ultimately compromising the spatial arrangement of BBs required for proper cilia alignment. Together, we show that progressive apical actin cross-linking coordinates BB positioning and regulates their dynamic state, guiding the shift from diffusive to confined motion. This transition in dynamics enables the emergence of a uniform BB pattern, which in turn ensures the aligned deployment of motile cilia necessary for effective directional fluid flow. Competing Interest Statement The authors have declared no competing interest.

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