Cooperative ETS transcription factors are required for lymphatic endothelial cell integrity and resilience
Myung Jin Yang, Seok Kang, Seon Pyo Hong, Hokyung Jin, Jin-Hui Yoon, Cheolhwa Jin, Chae Min Yuk, Lydia Getachew Gebeyehu, Junho Jung, Sung-Hwan Yoon, Hyuek Jong Lee, Gou Young Koh
Myung Jin Yang, Seok Kang, Seon Pyo Hong, Hokyung Jin, Jin-Hui Yoon, Cheolhwa Jin, Chae Min Yuk, Lydia Getachew Gebeyehu, Junho Jung, Sung-Hwan Yoon, Hyuek Jong Lee, Gou Young Koh
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Research Article Cell biology Development Vascular biology

Cooperative ETS transcription factors are required for lymphatic endothelial cell integrity and resilience

Abstract

Lymphatics maintain fluid homeostasis, immune surveillance, and tissue integrity. Here, we identified the E26 transformation-specific transcription factors Erg and Fli1 as essential cooperative regulators of lymphatic integrity and function. Using inducible lymphatic endothelial cell–specific deletion in mice, we demonstrated that combined loss of Erg and Fli1 in adults results in fatal lymphatic failure, including chylothorax, chylous ascites, and impaired lymphatic drainage. Single-cell transcriptomic analysis revealed that loss of Erg and Fli1 causes disrupted lymphatic heterogeneity and dysregulation of key lymphatic genes, including valve-specific gene profiles. Erg and Fli1 coordinated lymphatic-immune crosstalk by transcriptionally regulating C-C motif chemokine ligand 21, which mediates DC trafficking. Erg or Fli1 loss also induced proinflammatory and prothrombotic gene expression, further contributing to lymphatic dysfunction. During embryonic development, the codeletion led to lymphatic mispatterning and loss of valve-initiating lymphatic endothelial cell clusters. The impact of loss of Erg and Fli1 function on lymphatic development in mice is consistent with FOXC2 mutations in lymphedema-distichiasis syndrome or ERG gene variants underlying primary lymphedema in humans. Moreover, Erg and Fli1 were required for regenerative lymphangiogenesis and lymphatic repair following injury in adults. Our findings establish Erg and Fli1 as core transcriptional regulators of lymphatic identity, integrity, and function.

Authors

Myung Jin Yang, Seok Kang, Seon Pyo Hong, Hokyung Jin, Jin-Hui Yoon, Cheolhwa Jin, Chae Min Yuk, Lydia Getachew Gebeyehu, Junho Jung, Sung-Hwan Yoon, Hyuek Jong Lee, Gou Young Koh

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Figure 8

Erg and Fli1 are essential for lymphatic plexus patterning during embryonic development.

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Erg and Fli1 are essential for lymphatic plexus patterning during embryo...
(A) Diagram depicting tamoxifen (Tmx) administrations to WT, ErgiΔLEC, Fli1iΔLEC, and Erg/Fli1iΔLEC embryos at E12.5 and E14.5 and analyses at E16.5. (B) Images of WT, ErgiΔLEC, Fli1iΔLEC, and Erg/Fli1iΔLEC embryos at E16.5. White and yellow arrowheads indicate hemorrhage and edema. Scale bars: 2 mm. (CI) Immunofluorescence images of Prox1 and Vegfr3 expression in E16.5 dorsal skin lymphatics and comparison of indicated parameters. Areas within yellow and white dashed boxes are magnified in middle and right panels. Scale bars: 200 μm. Each dot indicates a value from 1 mouse, and n = 4 mice/group from 2 independent experiments. Data are shown as the mean ± SD; P value versus WT by 1-way ANOVA followed by Dunnett’s post hoc test.