Engineering of human brain organoids with a functional vascular-like system

Human cortical organoids (hCOs), derived from human embryonic stem cells (hESCs), provide a platform to study human brain development and diseases in complex three-dimensional tissue. However, current hCOs lack microvasculature, resulting in limited oxygen and nutrient delivery to the inner-most par...

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Veröffentlicht in:Nature methods 2019-11, Vol.16 (11), p.1169-1175
Hauptverfasser: Cakir, Bilal, Xiang, Yangfei, Tanaka, Yoshiaki, Kural, Mehmet H., Parent, Maxime, Kang, Young-Jin, Chapeton, Kayley, Patterson, Benjamin, Yuan, Yifan, He, Chang-Shun, Raredon, Micha Sam B., Dengelegi, Jake, Kim, Kun-Yong, Sun, Pingnan, Zhong, Mei, Lee, Sangho, Patra, Prabir, Hyder, Fahmeed, Niklason, Laura E., Lee, Sang-Hun, Yoon, Young-Sup, Park, In-Hyun
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Sprache:eng
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Zusammenfassung:Human cortical organoids (hCOs), derived from human embryonic stem cells (hESCs), provide a platform to study human brain development and diseases in complex three-dimensional tissue. However, current hCOs lack microvasculature, resulting in limited oxygen and nutrient delivery to the inner-most parts of hCOs. We engineered hESCs to ectopically express human ETS variant 2 ( ETV2 ). ETV2 -expressing cells in hCOs contributed to forming a complex vascular-like network in hCOs. Importantly, the presence of vasculature-like structures resulted in enhanced functional maturation of organoids. We found that vascularized hCOs (vhCOs) acquired several blood-brain barrier characteristics, including an increase in the expression of tight junctions, nutrient transporters and trans-endothelial electrical resistance. Finally, ETV2 -induced endothelium supported the formation of perfused blood vessels in vivo. These vhCOs form vasculature-like structures that resemble the vasculature in early prenatal brain, and they present a robust model to study brain disease in vitro. Expression of ETV2 in human cortical organoids induces the formation of vascular-like networks, which reduces cell death within organoids and increases their functional maturation.
ISSN:1548-7091
1548-7105
DOI:10.1038/s41592-019-0586-5