A human-specific enhancer fine-tunes radial glia potency and corticogenesis

Liu, Jing; Mosti, Federica; Zhao, Hanzhi T.; Sotelo-Fonseca, Jesus E.; Escobar-Tomlienovich, Carla F.; Lollis, Davoneshia; Musso, Camila M.; Mao, Yiwei; Massri, Abdull J.; Doll, Hannah M.; Sousa, Andre M.; Wray, Gregory A.; Schmidt, Ewoud; Silver, Debra L.

doi:10.1101/2024.04.10.588953

Cited by 1 publication

(3 citation statements)

References 75 publications

(128 reference statements)

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“…Determining the specific traits that HARs and HGEs influenced ultimately requires genetic models, such as humanized mice or cerebral organoids, in which their effects on neurodevelopment and function can be measured. A small number of HARs and HGEs have been shown to drive changes in gene expression and regulation in humanized mouse models, as well as developmental phenotypes including changes in radial glial self-renewal that lead to an increased number of neurons in the cortex 12,15,24 . These studies all share two advantages: first, strong evidence that the HAR or HGE encoded human-specific regulatory activity in a particular tissue, developmental time point or cell type; and second, a clear understanding of the identity and biological function of the likely gene targets.…”

Section: Discussionmentioning

confidence: 99%

“…Multiple studies support that HARs include transcriptional enhancers with human-specific activity 10,11 . HARs have been shown to drive changes in gene expression in genetically modified mouse models [12][13][14][15] , while massively parallel reporter assays (MPRAs) comparing HARs with their non-human primate orthologs have identified HARs that exhibit species-specific changes in enhancer activity [16][17][18] . Targeted perturbations and large-scale CRISPR proliferation screens have also been used to link HARs to changes in gene expression and neural stem cell phenotypes 19,20 .…”

Section: Introductionmentioning

confidence: 99%

“…HARs and HGEs may drive changes in gene expression via two non-exclusive mechanisms. First, HARs, HGEs and their chimpanzee orthologs may target conserved sets of orthologous genes in each species, with HARs and HGEs acting to alter expression of those genes in human [12][13][14][15]24 . Alternatively, it has been suggested HARs may have gained new gene targets in human neurodevelopment, a phenomenon referred to as enhancer hijacking 7 .…”

Section: Introductionmentioning

confidence: 99%

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Resolving the three-dimensional interactome of Human Accelerated Regions during human and chimpanzee neurodevelopment

Pal,

Noble,

Morales

et al. 2024

Preprint

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Human Accelerated Regions (HARs) are highly conserved across species but exhibit a significant excess of human-specific sequence changes, suggesting they may have gained novel functions in human evolution. HARs include transcriptional enhancers with human-specific activity and have been implicated in the evolution of the human brain. However, our understanding of how HARs contributed to uniquely human features of the brain is hindered by a lack of insight into the genes and pathways that HARs regulate. It is unclear whether HARs acted by altering the expression of gene targets conserved between HARs and their chimpanzee orthologs or by gaining new gene targets in human, a mechanism termed enhancer hijacking. We generated a high-resolution map of chromatin interactions for 1,590 HARs and their orthologs in human and chimpanzee neural stem cells (NSCs) to comprehensively identify gene targets in both species. HARs and their chimpanzee orthologs targeted a conserved set of 2,963 genes enriched for neurodevelopmental processes including neurogenesis and synaptic transmission. Changes in HAR enhancer activity were correlated with changes in conserved gene target expression. Conserved targets were enriched among genes differentially expressed between human and chimpanzee NSCs or between human and non-human primate developing and adult brain. Species-specific HAR gene targets did not converge on known biological functions and were not significantly enriched among differentially expressed genes, suggesting that HARs did not alter gene expression via enhancer hijacking. HAR gene targets, including differentially expressed targets, also showed cell type-specific expression patterns in the developing human brain, including outer radial glia, which are hypothesized to contribute to human cortical expansion. Our findings support that HARs influenced human brain evolution by altering the expression of conserved gene targets and provide the means to functionally link HARs with novel human brain features.

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Section: Discussionmentioning

confidence: 99%