Hyperactive FOXO1 results in lack of tip stalk identity and deficient microvascular regeneration during kidney injury

Loss of the microvascular (MV) network results in tissue ischemia, loss of tissue function, and is a hallmark of chronic diseases. The incorporation of a functional vascular network with that of the host remains a challenge to utilizing engineered tissues in clinically relevant therapies. We showed...

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Published inBiomaterials Vol. 141; pp. 314 - 329
Main Authors Dang, Lan T.H., Aburatani, Takahide, Marsh, Graham A., Johnson, Bryce G., Alimperti, Stella, Yoon, Christine J., Huang, Angela, Szak, Suzanne, Nakagawa, Naoki, Gomez, Ivan, Ren, Shuyu, Read, Sarah K., Sparages, Chris, Aplin, Alfred C., Nicosia, Roberto F., Chen, Chris, Ligresti, Giovanni, Duffield, Jeremy S.
Format Journal Article
LanguageEnglish
Published Netherlands Elsevier Ltd 01.10.2017
Subjects
Angiogenesis
FOXO1
Microfluidics
Vascular rarefaction
Vascular regeneration
VEGF
Angiogenesis
Vascular rarefaction
Vascular regeneration
VEGF
FOXO1
Microfluidics
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Summary:Loss of the microvascular (MV) network results in tissue ischemia, loss of tissue function, and is a hallmark of chronic diseases. The incorporation of a functional vascular network with that of the host remains a challenge to utilizing engineered tissues in clinically relevant therapies. We showed that vascular-bed-specific endothelial cells (ECs) exhibit differing angiogenic capacities, with kidney microvascular endothelial cells (MVECs) being the most deficient, and sought to explore the underlying mechanism. Constitutive activation of the phosphatase PTEN in kidney MVECs resulted in impaired PI3K/AKT activity in response to vascular endothelial growth factor (VEGF). Suppression of PTEN in vivo resulted in microvascular regeneration, but was insufficient to improve tissue function. Promoter analysis of the differentially regulated genes in KMVECs suggests that the transcription factor FOXO1 is highly active and RNAseq analysis revealed that hyperactive FOXO1 inhibits VEGF-Notch-dependent tip-cell formation by direct and indirect inhibition of DLL4 expression in response to VEGF. Inhibition of FOXO1 enhanced angiogenesis in human bio-engineered capillaries, and resulted in microvascular regeneration and improved function in mouse models of injury-repair. [Display omitted]
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Co-corresponding authors
Current Address: Department of Cardiovascular Research, Daiichi-Sankyo, Japan
ISSN:0142-9612
1878-5905
DOI:10.1016/j.biomaterials.2017.07.010