Astrocyte morphogenesis requires self-recognition.
S Lawrence ZipurskyJohn LeeAlina SergeevaGoran AhlsenSeetha MannepalliFabiana BahnaKerry GoodmanBaljit S KhakhJoshua WeinerLawrence ShapiroBarry HonigPublished in: Research square (2024)
Self-recognition is a fundamental cellular process across evolution and forms the basis of neuronal self-avoidance1-4. Clustered protocadherins (Pcdh), comprising a large family of isoform-specific homophilic recognition molecules, play a pivotal role in neuronal self-avoidance required for mammalian brain development5-7. The probabilistic expression of different Pcdh isoforms confers unique identities upon neurons and forms the basis for neuronal processes to discriminate between self and non-self5,6,8. Whether this self-recognition mechanism exists in astrocytes, the other predominant cell type of the brain, remains unknown. Here, we report that a specific isoform in the Pcdhγ cluster, γC3, is highly enriched in human and murine astrocytes. Through genetic manipulation, we demonstrate that γC3 acts autonomously to regulate astrocyte morphogenesis in the mouse visual cortex. To determine if γC3 proteins act by promoting recognition between processes of the same astrocyte, we generated pairs of γC3 chimeric proteins capable of heterophilic binding to each other, but incapable of homophilic binding. Co-expressing complementary heterophilic binding isoform pairs in the same γC3 null astrocyte restored normal morphology. By contrast, chimeric γC3 proteins individually expressed in single γC3 null mutant astrocytes did not. These data establish that self-recognition is essential for astrocyte development in the mammalian brain and that, by contrast to neuronal self-recognition, a single Pcdh isoform is both necessary and sufficient for this process.
Keyphrases
- cerebral ischemia
- resting state
- white matter
- magnetic resonance
- cell therapy
- endothelial cells
- machine learning
- functional connectivity
- spinal cord
- stem cells
- multiple sclerosis
- binding protein
- spinal cord injury
- computed tomography
- contrast enhanced
- subarachnoid hemorrhage
- genome wide
- transcription factor
- electronic health record