AI Article Synopsis

  • The self-organization of cells is crucial for healthy tissue development, and cytonemes facilitate long-distance signaling between cells.
  • Myosin XV, an unconventional myosin, plays a key role in regulating the dynamics of these cytonemes during sensory bristle patterning in fruit flies.
  • Loss of Myosin XV results in longer and more numerous cytonemes that disrupt signaling between cells, indicating that Myosin XV negatively regulates their formation to ensure effective Notch signaling.

Article Abstract

The self-organization of cells during development is essential for the formation of healthy tissues and requires the coordination of cell activities at local scales. Cytonemes, or signaling filopodia, are dynamic actin-based cellular protrusions that allow cells to engage in contact mediated signaling at a distance. While signaling filopodia have been shown to support several signaling paradigms during development, less is understood about how these protrusions are regulated. We investigated the role of the plus-end directed, unconventional MyTH4-FERM myosins in regulating signaling filopodia during sensory bristle patterning on the dorsal thorax of the fruit fly Drosophila melanogaster. We found that Myosin XV is required for regulating signaling filopodia dynamics and, as a consequence, lateral inhibition more broadly throughout the patterning epithelium. We found that Myosin XV is required for limiting the length and number of signaling filopodia generated by bristle precursor cells. Cells with additional and longer signaling filopodia due to loss of Myosin XV are not signaling competent, due to altered levels of Delta ligand and Notch receptor along their lengths. We conclude that Myosin XV acts to negatively regulate signaling filopodia, as well as promote the ability of signaling filopodia to engage in long-range Notch signaling. Since Myosin XV isoforms are present across several vertebrate and invertebrate systems, this may have significance for other long-range signaling mechanisms.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10767839PMC
http://dx.doi.org/10.1016/j.ydbio.2023.11.002DOI Listing

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