Clonal relations in the mouse brain revealed by single-cell and spatial transcriptomics

Ratz, Michael; Berlin, Leonie von; Larsson, Ludvig; Martin, Marcel; Westholm, Jakub Orzechowski; Manno, Gioele La; Lundeberg, Joakim; Frisén, Jonas

doi:10.1038/s41593-022-01011-x

Cited by 71 publications

(64 citation statements)

References 66 publications

(87 reference statements)

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“…Our findings indicate that some individual microglia undergo mass expansion as evidenced by the clouds of sparse-labelled microglia at P30. This finding is in line with a recent study where in vivo barcoding was used to track clonal expansion of various cell types, including microglia, within the embryonic brain (Ratz et al, 2022). In line with our findings, this study showed that expanded microglial progenitors span anatomical niches in an almost continuum (Ratz et al, 2022).…”

Section: Discussionsupporting

confidence: 90%

“…This finding is in line with a recent study where in vivo barcoding was used to track clonal expansion of various cell types, including microglia, within the embryonic brain (Ratz et al, 2022). In line with our findings, this study showed that expanded microglial progenitors span anatomical niches in an almost continuum (Ratz et al, 2022). Here we examined the changes in the spatial distribution of sparsely labelled microglia, which were highly clustered during embryonic development in comparison to adulthood, when the labelled microglia were more randomly distributed with a lower NND in line with the formation of the mosaic similar to the trends observed in the total PU.1 + population.…”

Section: Discussionsupporting

confidence: 90%

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Microglial colonisation of the developing brain is facilitated by clonal expansion of highly proliferative progenitors and follows an allometric scaling

Barry-Carroll

Greulich

Marshall

et al. 2022

Preprint

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Microglia are the resident immune cells of the brain and arise from yolk sac-derived macrophages during early embryogenesis. On entering the brain, microglia undergo in situ proliferation and eventually colonise the entire brain by the second and third postnatal weeks in mice. However, the intricate dynamics of their developmental expansion remain unclear. Here, we examine and characterise the proliferative dynamics of microglia during embryonic and postnatal development. Using complementary fate-mapping techniques, we demonstrate that the developmental colonisation of the brain by microglia is facilitated by clonal expansion of highly proliferative microglial progenitors that occupy spatial niches throughout the brain. We also find that the distribution of microglia switches from a clustered to a random pattern between embryonic and late postnatal development. Moreover, the developmental increase in microglia follows the proportional growth of the brain in an allometric manner with the density of microglia eventually stabilising when the mosaic distribution has been established. Overall, our findings offer insight into how the competition for space acts as a driving force for microglial colonisation by clonal expansion during development.

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Section: Discussionsupporting

confidence: 90%

Section: Discussionsupporting

confidence: 90%

Microglial colonisation of the developing brain is facilitated by clonal expansion of highly proliferative progenitors and follows an allometric scaling

Barry-Carroll

Greulich

Marshall

et al. 2022

Preprint

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“…Timelapse microscopy studies conducted in cerebral organoids have demonstrated that the characteristic behaviors of radial glia subtypes are recapitulated in organoids [ 95 , 96 ], as well as their capacity to differentiate via direct and indirect neurogenesis [ 97 ]. In addition to timelapse microscopy, technologies that enable multiplexed tracking of cell lineage at high-throughput using single cell transcriptomics can be applied to cerebral organoids [ 98 , 99 ] and primary tissue [ 79 , 100 , 101 ]. Examining mechanisms underlying human brain development using brain organoids will critically depend on rigorous benchmarking of the differentiation trajectories of neural progenitor cells.…”

Section: Benchmarking Against Primary Tissuementioning

confidence: 99%

Cerebral Organoids as an Experimental Platform for Human Neurogenomics

Nowakowski

Salama

2022

Cells

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The cerebral cortex forms early in development according to a series of heritable neurodevelopmental instructions. Despite deep evolutionary conservation of the cerebral cortex and its foundational six-layered architecture, significant variations in cortical size and folding can be found across mammals, including a disproportionate expansion of the prefrontal cortex in humans. Yet our mechanistic understanding of neurodevelopmental processes is derived overwhelmingly from rodent models, which fail to capture many human-enriched features of cortical development. With the advent of pluripotent stem cells and technologies for differentiating three-dimensional cultures of neural tissue in vitro, cerebral organoids have emerged as an experimental platform that recapitulates several hallmarks of human brain development. In this review, we discuss the merits and limitations of cerebral organoids as experimental models of the developing human brain. We highlight innovations in technology development that seek to increase its fidelity to brain development in vivo and discuss recent efforts to use cerebral organoids to study regeneration and brain evolution as well as to develop neurological and neuropsychiatric disease models.

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“…Spatial omics technologies map out organizational structures of cells along with their genomics, transcriptomics, proteomics and epigenomics profiles, providing powerful tools for deciphering mechanisms of functional and spatial arrangements in normal development and disease pathology (Larsson et al 2021;Longo et al 2021;Marx 2021;Deng et al 2022;Dhainaut et al 2022;Ratz et al 2022;Zhao et al 2022). The collection of available approaches provides a wide spectrum of throughput and spatial resolution.…”

Section: Introductionmentioning

confidence: 99%

Scalable and model-free detection of spatial patterns and colocalization

2022

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The expeditious growth in spatial omics technologies enable profiling genome-wide molecular events at molecular and single-cell resolution, highlighting a need for fast and reliable methods to characterize spatial patterns. We developed SpaGene, a model-free method to discover spatial patterns rapidly in large scale spatial omics studies. Analyzing simulation and a variety of spatial resolved transcriptomics data demonstrated that SpaGene is more powerful and scalable than existing methods. Spatial expression patterns by SpaGene reconstructed unobserved tissue structures. SpaGene also successfully discovered ligand-receptor interactions through their colocalization.

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Clonal relations in the mouse brain revealed by single-cell and spatial transcriptomics

Cited by 71 publications

References 66 publications

Microglial colonisation of the developing brain is facilitated by clonal expansion of highly proliferative progenitors and follows an allometric scaling

Microglial colonisation of the developing brain is facilitated by clonal expansion of highly proliferative progenitors and follows an allometric scaling

Cerebral Organoids as an Experimental Platform for Human Neurogenomics

Scalable and model-free detection of spatial patterns and colocalization

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