Literature DB >> 36074851

Human TKTL1 implies greater neurogenesis in frontal neocortex of modern humans than Neanderthals.

Lei Xing1, Takashi Namba1, Nereo Kalebic1, Anneline Pinson1, Jula Peters1, Christina Eugster Oegema1, Sofia Traikov1, Katrin Reppe1, Stephan Riesenberg2, Tomislav Maricic2, Razvan Derihaci3, Pauline Wimberger3, Svante Pääbo2, Wieland B Huttner1.   

Abstract

Neanderthal brains were similar in size to those of modern humans. We sought to investigate potential differences in neurogenesis during neocortex development. Modern human transketolase-like 1 (TKTL1) differs from Neanderthal TKTL1 by a lysine-to-arginine amino acid substitution. Using overexpression in developing mouse and ferret neocortex, knockout in fetal human neocortical tissue, and genome-edited cerebral organoids, we found that the modern human variant, hTKTL1, but not the Neanderthal variant, increases the abundance of basal radial glia (bRG) but not that of intermediate progenitors (bIPs). bRG generate more neocortical neurons than bIPs. The hTKTL1 effect requires the pentose phosphate pathway and fatty acid synthesis. Inhibition of these metabolic pathways reduces bRG abundance in fetal human neocortical tissue. Our data suggest that neocortical neurogenesis in modern humans differs from that in Neanderthals.

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Year:  2022        PMID: 36074851     DOI: 10.1126/science.abl6422

Source DB:  PubMed          Journal:  Science        ISSN: 0036-8075            Impact factor:   63.714


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