Inhibition of <scp>VEGF</scp>‐dependent angiogenesis and tumor angiogenesis by an optimized antibody targeting <scp>CLEC</scp>14a

Kim, Taek-Keun; Park, Chang Sik; Jang, Ji-Hye; Kim, Mi Ra; Na, Hee-Jun; Lee, Kangseung; Kim, Hyun Jung; Heo, Kyun; Yoo, Byong Chul; Kim, Young‐Myeong; Lee, Je-Wook; Kim, Su Jin; Kim, Eun Sung; Kim, Dae Young; Cha, Kiweon; Lee, Tae Gyu; Lee, Sukmook

doi:10.1002/1878-0261.12169

Cited by 30 publications

(18 citation statements)

References 43 publications

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“…tested a human colorectal cancer cell line HCT116 as well as a bevacizumab‐resistant version of this line. Both cell lines showed significant reductions in in vivo angiogenesis following treatment with CLEC14A antibodies when these cells were embedded in Matrigel and injected subcutaneously . This suggests a possible use for targeting of CLEC14A in patients that have acquired resistance to VEGF blockade.…”

Section: Considerations and Perspectivesmentioning

confidence: 87%

“…Finally, these antibodies could reduce HUVEC cell migration and tube formation based on in vitro assays. Further studies optimised the solubility and stability of the CLEC14A CTLD‐targeting antibodies and showed that they could block angiogenesis in mouse models utilising Matrigel plugs injected with recombinant VEGF or human tumour cells . Collectively, these results suggest that the CTLD of CLEC14A has functional roles in angiogenesis.…”

Section: Clec14a Roles In Vascular Biology and Cancermentioning

confidence: 96%

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C‐type lectin domain group 14 proteins in vascular biology, cancer and inflammation

et al. 2019

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The C‐type lectin domain (CTLD) group 14 family of transmembrane glycoproteins consist of thrombomodulin, CD93, CLEC14A and CD248 (endosialin or tumour endothelial marker‐1). These cell surface proteins exhibit similar ectodomain architecture and yet mediate a diverse range of cellular functions, including but not restricted to angiogenesis, inflammation and cell adhesion. Thrombomodulin, CD93 and CLEC14A can be expressed by endothelial cells, whereas CD248 is expressed by vasculature associated pericytes, activated fibroblasts and tumour cells among other cell types. In this article, we review the current literature of these family members including their expression profiles, interacting partners, as well as established and speculated functions. We focus primarily on their roles in the vasculature and inflammation as well as their contributions to tumour immunology. The CTLD group 14 family shares several characteristic features including their ability to be proteolytically cleaved and engagement of some shared extracellular matrix ligands. Each family member has strong links to tumour development and in particular CD93, CLEC14A and CD248 have been proposed as attractive candidate targets for cancer therapy.

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Section: Considerations and Perspectivesmentioning

confidence: 87%

Section: Clec14a Roles In Vascular Biology and Cancermentioning

confidence: 96%

C‐type lectin domain group 14 proteins in vascular biology, cancer and inflammation

et al. 2019

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“…The C-type lectin domain has been shown to engage other matrix proteins, such as multimerin 2 (MMRN2) and heat-shock protein 70-1A (61,62). Antibodies blocking these interactions or targeting the C-type lectin domain have been shown to decrease cell migration and tumor angiogenesis in a manner dependent on MMRN2 (42,62) or VEGFA (68). Whether these antibodies block the GAG-binding site is not known.…”

Section: Lphams and The Heparan Sulfate Interactomementioning

confidence: 99%

Proteomics-based screening of the endothelial heparan sulfate interactome reveals that C-type lectin 14a (CLEC14A) is a heparin-binding protein

Sandoval

Toledo

Painter

et al. 2020

Journal of Biological Chemistry

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Animal cells express heparan sulfate proteoglycans that perform many important cellular functions by way of heparan sulfate–protein interactions. The identification of membrane heparan sulfate–binding proteins is challenging because of their low abundance and the need for extensive enrichment. Here, we report a proteomics workflow for the identification and characterization of membrane-anchored and extracellular proteins that bind heparan sulfate. The technique is based on limited proteolysis of live cells in the absence of denaturation and fixation, heparin-affinity chromatography, and high-resolution LC-MS/MS, and we designate it LPHAMS. Application of LPHAMS to U937 monocytic and primary murine and human endothelial cells identified 55 plasma membrane, extracellular matrix, and soluble secreted proteins, including many previously unidentified heparin-binding proteins. The method also facilitated the mapping of the heparin-binding domains, making it possible to predict the location of the heparin-binding site. To validate the discovery feature of LPHAMS, we characterized one of the newly-discovered heparin-binding proteins, C-type lectin 14a (CLEC14A), a member of the C-type lectin family that modulates angiogenesis. We found that the C-type lectin domain of CLEC14A binds one-to-one to heparin with nanomolar affinity, and using molecular modeling and mutagenesis, we mapped its heparin-binding site. CLEC14A physically interacted with other glycosaminoglycans, including endothelial heparan sulfate and chondroitin sulfate E, but not with neutral or sialylated oligosaccharides. The LPHAMS technique should be applicable to other cells and glycans and provides a way to expand the repertoire of glycan-binding proteins for further study.

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“…CLEC14A has also been reported to regulate pro-angiogenic phenotypes such as filopodia formation, cell migration and tube formation in HUVECs (31,32); it localizes to the inter-cellular boundary and regulates cell adhesion through its CTLD (31). Targeted neutralization of CLEC14A using an anti-CTLD antibody was shown to inhibit endothelial cell migration, cell-cell contact and tube formation by blocking CTLD-CTLD interactions, and downregulating CLEC14A expression at the endothelial cell surface (36,37). A Stable Isotope Labelling with Amino Acids in Cell Culture-based proteomics study showed the upregulation of CLEC14A expression during tubule morphogenesis, and the analysis of post-translational modifications of CLEC14A identified a phosphorylation site at Ser483, near the PDZ-binding domain in the cytoplasmic tail (38).…”

Section: Clec14amentioning

confidence: 99%

C‑type lectin family XIV members and angiogenesis: A review

2019

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The growth and metastasis of tumors is dependent on angiogenesis. C-type lectins are carbohydrate-binding proteins with a diverse range of functions. The C-type lectin family XIV members are transmembrane glycoproteins, and all four members of this family have been reported to regulate angiogenesis, although the detailed mechanism of action has yet to be completely elucidated. They interact with extracellular matrix proteins and mediate cell-cell adhesion by their lectin-like domain. The aim of the present study was to summarize the available information on the function and mechanism of C-type lectin family XIV in angiogenesis and discuss their potential as targets for cancer therapy. Contents 1. Introduction 2. C-type lectin family XIV 3. CLEC14A 4. Thrombomodulin 5. CD93 6. Endosialin 7. Conclusions and prospects

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Inhibition of VEGF‐dependent angiogenesis and tumor angiogenesis by an optimized antibody targeting CLEC14a

Cited by 30 publications

References 43 publications

C‐type lectin domain group 14 proteins in vascular biology, cancer and inflammation

C‐type lectin domain group 14 proteins in vascular biology, cancer and inflammation

Proteomics-based screening of the endothelial heparan sulfate interactome reveals that C-type lectin 14a (CLEC14A) is a heparin-binding protein

C‑type lectin family XIV members and angiogenesis: A review

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