Lysophosphatidic acid–induced YAP/TAZ activation promotes developmental angiogenesis by repressing Notch ligand Dll4

Yasuda, Daisuke; Kobayashi, Daiki; Akahoshi, Noriyuki; Ohto-Nakanishi, Takayo; Yoshioka, Kazuaki; Takuwa, Yoh; Mizuno, Seiya; Takahashi, Satoru; Ishii, Satoshi

doi:10.1172/jci121955

Cited by 89 publications

(80 citation statements)

References 77 publications

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“…Tumor microenvironments are very heterogeneous and cancer type-specific, implying that ATX/LPA signaling outcome will critically depend on the composition and LPAR expression repertoire of the immune cell infiltrate. LPAR6 is of special interest here as it provides a crucial link with ATX and G13 during embryonic development (van Meeteren et al, 2006;Yasuda et al, 2019) and is abundantly expressed in immune cells ( Figure 3D). LPAR6 has a rather low affinity for 1-acyl-LPA species (Yung et al, 2014), which may explain the relatively high IC50 value for 1-oleyl-LPA observed in the T-cell migration assays (Fig.…”

Section: Discussionmentioning

confidence: 99%

Autotaxin impedes anti-tumor immunity by suppressing chemotaxis and tumor infiltration of CD8⁺T cells

Matas-Rico

Àvila

Zon

et al. 2020

Preprint

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To improve immunotherapy efficacy, a better understanding of the factors that regulate Tcell migration into tumors is essential. Here we uncover a role for autotaxin (ATX) in this process. ATX (encoded by ENPP2) produces lysophosphatidic acid (LPA) that activates G protein-coupled receptors (LPAR1-6) to regulate multiple (patho)physiological processes, including tumor progression via LPAR1 and lymphocyte homing via LPAR2.Unexpectedly, we find that melanoma cell-secreted ATX is a major chemorepellent for tumor-infiltrating lymphocytes ex vivo through Gα12/13-coupled LPAR6, with ATX functioning as an LPA-producing chaperone. Using an anti-cancer vaccination model, we provide proof-of-concept that secreted ATX opposes tumor infiltration of CD8+ T cells.Additionally, ENPP2 expression in melanoma tumors correlates with reduced CD8+ T-cell infiltration as inferred from single-cell transcriptomics. Hence, by counteracting T-cell infiltration while activating tumor cells via different LPA receptors, the ATX/LPA complex exerts dual actions in the tumor immune microenvironment, which may provide new therapeutic approaches.

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Section: Discussionmentioning

confidence: 99%

Autotaxin impedes anti-tumor immunity by suppressing chemotaxis and tumor infiltration of CD8⁺T cells

Matas-Rico

Àvila

Zon

et al. 2020

Preprint

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“…In our studies, we observed a strong upregulation of YAP/TAZ target genes Cyr61 and Ctgf due to loading; this response was significantly abrogated by YAP/TAZ inhibitor VP only under the delayed loading condition. These results suggest that delayed loading activates YAP signaling (perhaps through Itgb1), which leads to an increased number of active sprout tip cells (53) and thus upregulation of genes associated with active tip cells, to enhance vascularization.…”

Section: Discussionmentioning

confidence: 90%

“…In vasculature, they have recently been implicated in transducing the atherogenic effects of oscillatory shear stress (17) -one of the most well-studied examples of vascular mechanosensitivity (9). Additionally, YAP and TAZ are known to promote sprouting angiogenesis, even in systems that are not directly mechanically stimulated (24), through molecular regulators of sprout tip cell selection (53). In our studies, we observed a strong upregulation of YAP/TAZ target genes Cyr61 and Ctgf due to loading; this response was significantly abrogated by YAP/TAZ inhibitor VP only under the delayed loading condition.…”

Section: Discussionmentioning

confidence: 99%

Mechanical Regulation of Microvascular Angiogenesis

Ruehle

Eastburn

LaBelle

et al. 2020

Preprint

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Statement of Significance:Mechanical cues influence tissue regeneration, and although vasculature is known to be mechanically sensitive, remarkably little is known about the effects of bulk extracellular matrix deformation on the nascent vessel networks found in healing tissues.Here, we demonstrated that load initiation time, magnitude, and mode all regulate microvascular growth, as well as upstream angiogenic and mechanotransduction signaling pathways. Across all tested magnitudes and modes, microvascular network formation and upstream signaling were powerfully regulated by the timing of load initiation. This work provides a new foundational understanding of how extracellular matrix mechanics regulate angiogenesis and has critical implications for clinical translation of new regenerative medicine therapies and physical rehabilitation strategies designed to enhance revascularization during tissue regeneration.

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“…When the promiscuous Gα protein is co-expressed with LPA 6 , LPA activates LPA 6 to increase intracellular Ca 2+ and reduce cAMP and ERK1/2 activation which stimulated by forskolin [9,47]. As already mentioned, the transcriptional regulators YAP and TAZ can be activated by the LPA-LPA 4 /LPA 6 -Gα12/Gα13 signaling pathway, and both YAP and TAZ are involved in tumor progression [35]. Moreover, another article mentions the binding of LPA to the LPA 6 receptor to regulate vascular permeability [49].…”

Section: Lpar6mentioning

confidence: 82%

“…It indicates that LPA4 receptor can promote angiogenesis and vascular development. In addition, the regulatory factor Yes-associated protein (YAP) and the transcriptional coactivator with PDZ-binding motif (TAZ) can also be activated by LPA4/LPA6 via the Gα12/Gα13 signaling pathway [35]. YAP and TAZ can accelerate the progression of cancer by promoting the proliferation and migration of cancer cells, such as accelerating liver cancer, bladder cancer and lung cancer [36][37][38].…”

Section: Lpar4mentioning

confidence: 99%

Lysophosphatidic Acid Receptors: Biochemical and Clinical Implications in Different Diseases

Xiang¹,

Lü²,

Shao³

et al. 2020

J. Cancer

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Lysophosphatidic acid (LPA, 1-acyl-2-hemolytic-sn-glycerol-3-phosphate) extracted from membrane phospholipid is a kind of simple bioactive glycophospholipid, which has many biological functions such as stimulating cell multiplication, cytoskeleton recombination, cell survival, drug-fast, synthesis of DNA and ion transport. Current studies have shown that six G-coupled protein receptors (LPAR1-6) can be activated by LPA. They stimulate a variety of signal transduction pathways through heterotrimeric G-proteins (such as Gα12/13, Gαq/11, Gαi/o and GαS). LPA and its receptors play vital roles in cancers, nervous system diseases, cardiovascular diseases, liver diseases, metabolic diseases, etc. In this article, we discussed the structure of LPA receptors and elucidated their functions in various diseases, in order to better understand them and point out new therapeutic schemes for them.

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Lysophosphatidic acid–induced YAP/TAZ activation promotes developmental angiogenesis by repressing Notch ligand Dll4

Cited by 89 publications

References 77 publications

Autotaxin impedes anti-tumor immunity by suppressing chemotaxis and tumor infiltration of CD8⁺T cells

Autotaxin impedes anti-tumor immunity by suppressing chemotaxis and tumor infiltration of CD8⁺T cells

Mechanical Regulation of Microvascular Angiogenesis

Lysophosphatidic Acid Receptors: Biochemical and Clinical Implications in Different Diseases

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Lysophosphatidic acid–induced YAP/TAZ activation promotes developmental angiogenesis by repressing Notch ligand Dll4

Cited by 89 publications

References 77 publications

Autotaxin impedes anti-tumor immunity by suppressing chemotaxis and tumor infiltration of CD8+T cells

Autotaxin impedes anti-tumor immunity by suppressing chemotaxis and tumor infiltration of CD8+T cells

Mechanical Regulation of Microvascular Angiogenesis

Lysophosphatidic Acid Receptors: Biochemical and Clinical Implications in Different Diseases

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Product

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Autotaxin impedes anti-tumor immunity by suppressing chemotaxis and tumor infiltration of CD8⁺T cells

Autotaxin impedes anti-tumor immunity by suppressing chemotaxis and tumor infiltration of CD8⁺T cells