Etv2 and Fli1b Function Together as Key Regulators of Vasculogenesis and Angiogenesis

Craig, Michael P.; Grajevskaja, Viktorija; Liao, Hsin Kai; Balciuniene, Jorune; Ekker, Stephen C.; Park, Joo Seop; Essner, Jeffrey J.; Balciunas, Darius; Sumanas, Saulius

doi:10.1161/atvbaha.114.304768

Cited by 58 publications

(70 citation statements)

References 50 publications

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“…There are multiple ETS family members, but of these ETS-1 and ERG are highly expressed in the vasculature and have been shown to be regulated by VEGF signaling [27, 28]. The FOXO family of transcription factors has been implicated in metabolism, proliferation and longevity in endothelial cells [29, 30].…”

Section: Introductionmentioning

confidence: 99%

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

et al. 2017

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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.

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Section: Introductionmentioning

confidence: 99%

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

et al. 2017

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“…Despite dramatic defects in early vasculogenesis, vascular development partially recovers even in etv2 null mutant zebrafish embryos at later stages, and only aberrant angiogenesis is observed during later stages. This later recovery is mediated by related ETS transcription factors such as Fli1b which functions redundantly with Etv2 during later stages of vasculogenesis and during angiogenesis [10]. Overexpression of Etv2 results in dramatic expansion of hemangioblast and vascular endothelial marker expression in either zebrafish or Xenopus embryos, demonstrating that a single transcription factor is sufficient to induce vascular endothelial fate in different cell types [18, 21].…”

Section: Ets Factors In Vascular Developmentmentioning

confidence: 99%

“…In contrast, a separate study demonstrated that Flk1:Cre; Etv2 conditional mouse knockout embryos displayed disorganized vasculature and reduced hematopoietic progenitors cells and died at 10.5 [11]. Conditional Etv2 knockdown in zebrafish embryos using photoactivatable caging strand hybridized to a morpholino also demonstrated lack of vascular phenotype when Etv2 function is inhibited at 18-somite or later stages after the initial vasculature has formed [10, 22, 36]. However, recent studies show that Etv2 functions redundantly with other ETS transcription factors during later angiogenesis stages [10], which may explain the absence of the phenotype in mouse Flk1:Cre conditional Etv2-knockout embryos.…”

Section: Ets Factors In Vascular Developmentmentioning

confidence: 99%

“…Conditional Etv2 knockdown in zebrafish embryos using photoactivatable caging strand hybridized to a morpholino also demonstrated lack of vascular phenotype when Etv2 function is inhibited at 18-somite or later stages after the initial vasculature has formed [10, 22, 36]. However, recent studies show that Etv2 functions redundantly with other ETS transcription factors during later angiogenesis stages [10], which may explain the absence of the phenotype in mouse Flk1:Cre conditional Etv2-knockout embryos. Inducible Etv2 inactivation at the 18-somite stage resulted in angiogenic defects in fli1b −/− zebrafish mutant embryos, which otherwise were phenotypically normal (Fig.…”

Section: Ets Factors In Vascular Developmentmentioning

confidence: 99%

“…However, runt-related transcription factor 1 ( runx1 ) expression was not rescued by Fli1a unless it was co-injected with scl -α and scl -β mRNAs, suggesting that Fli1a is insufficient to initiate hematopoietic stem cell (HSC) specification, but that it is capable of mediating the endothelial program [43]. However, in two separate studies, Fli1a overexpression failed to induce vascular endothelial markers in zebrafish embryos [10, 42]. Rather, Fli1a likely plays an important later role in the maintenance of the endothelial lineage.…”

Section: Ets Factors In Vascular Developmentmentioning

confidence: 99%

See 2 more Smart Citations

ETS transcription factors in embryonic vascular development

Craig

Sumanas

2016

Angiogenesis

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At least thirteen ETS-domain transcription factors are expressed during embryonic hematopoietic or vascular development and potentially function in the formation and maintenance of the embryonic vasculature or blood lineages. This review summarizes our current understanding of the specific roles played by ETS factors in vasculogenesis and angiogenesis and the implications of functional redundancies between them.

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Transcriptional control of blood cell emergence

et al. 2019

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The haematopoietic system is established during embryonic life through a series of developmental steps that culminates with the generation of haematopoietic stem cells. Characterisation of the transcriptional network that regulates blood cell emergence has led to the identification of transcription factors essential for this process. Among the many factors wired within this complex regulatory network, ETV2, SCL and RUNX1 are the central components. All three factors are absolutely required for blood cell generation, each one controlling a precise step of specification from the mesoderm germ layer to fully functional blood progenitors. Insight into the transcriptional control of blood cell emergence has been used for devising protocols to generate blood cells de novo, either through reprogramming of somatic cells or through forward programming of pluripotent stem cells. Interestingly, the physiological process of blood cell generation and its laboratory‐engineered counterpart have very little in common.

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Etv2 and Fli1b Function Together as Key Regulators of Vasculogenesis and Angiogenesis

Cited by 58 publications

References 50 publications

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

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

ETS transcription factors in embryonic vascular development

Transcriptional control of blood cell emergence

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