BACH family members regulate angiogenesis and lymphangiogenesis by modulating VEGFC expression

Cohen, Batya; Tempelhof, Hanoch; Raz, Tal; Oren, Roni; Nicenboim, Julian; Bochner, Filip; Even, Ron; Jelinski, Adam; Ben‐Dor, Shifra; Addadi, Yoseph; Golani, Ofra; Lazar, Shlomi; Yaniv, Karina; Neeman, Michal

doi:10.1101/2019.12.13.876268

Cited by 4 publications

(8 citation statements)

References 103 publications

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“…Cell-cycle arrest in dorsal PCV ECs is VegfC/VegfR3 dependent During embryonic development, venous and lymphatic ECs sprout from the CV in response to Vegfc-Vegfr3 signaling (Petrova and Koh, 2018;Semo et al, 2016). In zebrafish, Vegfc is ex-pressed in the hypochord and the DA (Cohen et al, 2020;Covassin et al, 2006;Hogan et al, 2009b), whereas its receptor, Flt4, is expressed in PCV ECs, including those in lymphatic and venous sprouts. Mutations in either vegfc or flt4 lead to a block in sprouting of lymphatic and venous ECs from the PCV and a failure to develop a functional lymphatic system, along with defective arteriovenous remodeling of ISVs (Covassin et al, 2006;van Impel et al, 2014;Siekmann and Lawson, 2007).…”

Section: Ecs Sprout From the Pcv In G1 Phasementioning

confidence: 99%

VEGFC/FLT4-induced cell-cycle arrest mediates sprouting and differentiation of venous and lymphatic endothelial cells

et al. 2021

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Section: Ecs Sprout From the Pcv In G1 Phasementioning

confidence: 99%

VEGFC/FLT4-induced cell-cycle arrest mediates sprouting and differentiation of venous and lymphatic endothelial cells

et al. 2021

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“…In parallel to indirect regulation of Vegfc by SOX7, our study identified putative VEGFC silencing elements in both the human and mouse genomes, and suggest that SOX7 can regulate Vegfc transcription through direct binding at these sites. While a handful of factors have been shown to transcriptionally regulate VEGFC expression in the past (Cohen et al, 2020; Gauvrit et al, 2018; Schuermann et al, 2015), this is the first identification of an endothelial-specific and direct molecular mechanism able to regulate Vegfc transcription.…”

Section: Discussionmentioning

confidence: 85%

“…To date, only a handful of factors have been shown to transcriptionally regulate VEGFC expression (Cohen et al, 2020; Gauvrit et al, 2018; Schuermann et al, 2015), with no previous study describing an endothelial-specific and direct molecular mechanism that regulates VEGFC transcription. Our work sheds light into how the BEC-specific SOX7 transcription factor dampens local VEGFC levels to modulate tissue growth in a paracrine manner likely via a combination of mechanisms: 1) indirectly through recruitment and transcriptional control of the repressor protein HEY1 2) directly via binding to silencing elements associated with the Vegfc locus.…”

Section: Discussionmentioning

confidence: 99%

“…Despite a plethora of information on the mode of action, maturation process and signalling mechanisms of VEGFC, there is a lack of understanding of how this growth factor is transcriptionally regulated, especially in the endothelial compartment. While the hematopoietically expressed homeobox (HHEX) genetic pathway has been implicated as an endothelial-specific regulator upstream of VEGFC expression, only the BTB and CNC homology (BACH) family of transcription factors have been shown to directly transactivate the VEGFC promoter and these experiments were performed in human ovarian carcinoma ES2 cells (Cohen et al, 2020; Gauvrit et al, 2018; Schuermann et al, 2015). Thus, there is still a paucity of information on the molecular mechanisms that drive Vegfc transcription in the endothelial cell context, despite the fact that it is well established that endothelial-derived VEGFC is critical for blood vessel angiogenesis and coronary artery formation (Cao et al, 1998; Chen et al, 2014).…”

Section: Introductionmentioning

confidence: 99%

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The blood vasculature instructs lymphatics patterning in a SOX7 dependent manner

Ikn

Jiang

et al. 2021

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Despite a growing catalogue of secreted factors critical for lymphatic network assembly, little is known about the mechanisms that modulate the expression level of these molecular cues in blood vascular endothelial cells (BECs). Here, we show that a BEC-specific transcription factor, SOX7, plays a crucial role in lymphatic vessel patterning by modulating the transcription of lymphangiocrine signals. While SOX7 is not expressed in lymphatic endothelial cells (LECs), loss of SOX7 function in mouse embryos causes a dysmorphic dermal lymphatic phenotype. We identify novel distant regulatory regions in mice and humans that contribute to directly repressing the transcription of a major lymphangiogenic growth factor (Vegfc) in a SOX7-dependent manner. Further, we show that SOX7 directly binds HEY1, a canonical repressor of the Notch pathway, suggesting that transcriptional repression may also be modulated by the recruitment of this protein partner at Vegfc genomic regulatory regions. Our work unveils a role for SOX7 in modulating downstream signalling events crucial for lymphatic patterning, at least in part via the transcriptional repression of VEGFC levels in the blood vascular endothelium.

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“…Despite a plethora of information on the mode of action, maturation process, and signaling mechanisms of VEGFC, there is a lack of understanding of how this growth factor is transcriptionally regulated, especially in the endothelial compartment. While the hematopoietically expressed homeobox (HHEX) genetic pathway has been implicated as an endothelial-specific regulator upstream of VEGFC expression, only the BTB and CNC homology (BACH) family of transcription factors have been shown to directly transactivate the VEGFC promoter and these experiments were performed in human ovarian carcinoma ES2 cells (Schuermann et al, 2015;Gauvrit et al, 2018;Cohen et al, 2020). Thus, there is still a paucity of information on the molecular mechanisms that drive Vegfc transcription in the endothelial cell context, despite the fact that it is well-established that endothelial-derived VEGFC is critical for blood vessel angiogenesis and coronary artery formation (Cao et al, 1998;Chen et al, 2014).…”

Section: Introductionmentioning

confidence: 99%

The blood vasculature instructs lymphatic patterning in a SOX7‐dependent manner

et al. 2023

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Despite a growing catalog of secreted factors critical for lymphatic network assembly, little is known about the mechanisms that modulate the expression level of these molecular cues in blood vascular endothelial cells (BECs). Here, we show that a BEC‐specific transcription factor, SOX7, plays a crucial role in a non‐cell‐autonomous manner by modulating the transcription of angiocrine signals to pattern lymphatic vessels. While SOX7 is not expressed in lymphatic endothelial cells (LECs), the conditional loss of SOX7 function in mouse embryos causes a dysmorphic dermal lymphatic phenotype. We identify novel distant regulatory regions in mice and humans that contribute to directly repressing the transcription of a major lymphangiogenic growth factor (Vegfc) in a SOX7‐dependent manner. Further, we show that SOX7 directly binds HEY1, a canonical repressor of the Notch pathway, suggesting that transcriptional repression may also be modulated by the recruitment of this protein partner at Vegfc genomic regulatory regions. Our work unveils a role for SOX7 in modulating downstream signaling events crucial for lymphatic patterning, at least in part via the transcriptional repression of VEGFC levels in the blood vascular endothelium.

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BACH family members regulate angiogenesis and lymphangiogenesis by modulating VEGFC expression

Cited by 4 publications

References 103 publications

VEGFC/FLT4-induced cell-cycle arrest mediates sprouting and differentiation of venous and lymphatic endothelial cells

VEGFC/FLT4-induced cell-cycle arrest mediates sprouting and differentiation of venous and lymphatic endothelial cells

The blood vasculature instructs lymphatics patterning in a SOX7 dependent manner

The blood vasculature instructs lymphatic patterning in a SOX7‐dependent manner

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