Neuronal migration prevents spatial competition in retinal morphogenesis.
Mauricio Rocha-MartinsElisa NerliJenny KretzschmarMartin WeigertJaroslav IchaEugene W MyersCaren NordenPublished in: Nature (2023)
The concomitant occurrence of tissue growth and organization is a hallmark of organismal development 1-3 . This often means that proliferating and differentiating cells are found at the same time in a continuously changing tissue environment. How cells adapt to architectural changes to prevent spatial interference remains unclear. Here, to understand how cell movements that are key for growth and organization are orchestrated, we study the emergence of photoreceptor neurons that occur during the peak of retinal growth, using zebrafish, human tissue and human organoids. Quantitative imaging reveals that successful retinal morphogenesis depends on the active bidirectional translocation of photoreceptors, leading to a transient transfer of the entire cell population away from the apical proliferative zone. This pattern of migration is driven by cytoskeletal machineries that differ depending on the direction: microtubules are exclusively required for basal translocation, whereas actomyosin is involved in apical movement. Blocking the basal translocation of photoreceptors induces apical congestion, which hampers the apical divisions of progenitor cells and leads to secondary defects in lamination. Thus, photoreceptor migration is crucial to prevent competition for space, and to allow concurrent tissue growth and lamination. This shows that neuronal migration, in addition to its canonical role in cell positioning 4 , can be involved in coordinating morphogenesis.
Keyphrases
- induced apoptosis
- single cell
- optical coherence tomography
- endothelial cells
- diabetic retinopathy
- cell therapy
- high resolution
- cell cycle arrest
- induced pluripotent stem cells
- cerebral ischemia
- spinal cord
- magnetic resonance imaging
- spinal cord injury
- squamous cell carcinoma
- signaling pathway
- oxidative stress
- mass spectrometry
- stem cells
- mesenchymal stem cells
- cell proliferation
- endoplasmic reticulum stress
- contrast enhanced
- pluripotent stem cells