Inhibition of angiogenesis by a synthetic fusion protein VTF derived from vasostatin and tumstatin

Gu, Qing; Sun, Cihuang; Luo, Jinxian; Zhang, Tianyuan; Wang, Lijing

doi:10.1097/cad.0000000000000134

Cited by 3 publications

(2 citation statements)

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“…In an additional experiment, gene electrotransfer of naked plasmid DNA containing the tumstatin cDNA has been adopted to investigate the anti-tumor effect of tumstatin in B16F1 melanoma-bearing mice: A marked decrease in tumor growth and an increase in mouse survival was observed, indicating that this strategy appears appealing in terms of gene delivery and tumor suppression ( 140 ). In addition, the pET-15b vector generated to express a synthetic fusion protein, VTF, which is composed of vasostatin and tumstatin with a (Gly-Ser-Gly)2 bridge, demonstrated the suppression of B16 melanoma growth and the potent inhibition of tumor blood vessels formation in vivo , when compared with a single inhibitor, the fusion proteins of different angiogenesis inhibitors targeting different pathways exhibited improved therapeutic effects ( 141 ). Additionally, as T42, which was derived from two active domains of tumstatin, has demonstrated anti-tumor efficacy, a previous study constructed two adenoviral vectors with T42 and 4xT42 peptide genes to evaluate their anti-cancer effects on breast cancer in vitro and in vivo ; the results suggested evidence that this modality may be a potential alternative for the treatment of breast cancer ( 142 ).…”

Section: Anti-angiogenesis Gene Therapy and Angiogenesis Inhibitorsmentioning

confidence: 99%

Tumor angiogenesis and anti‑angiogenic gene therapy for cancer (Review)

et al. 2018

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When Folkman first suggested a theory about the association between angiogenesis and tumor growth in 1971, the hypothesis of targeting angiogenesis to treat cancer was formed. Since then, various studies conducted across the world have additionally confirmed the theory of Folkman, and numerous efforts have been made to explore the possibilities of curing cancer by targeting angiogenesis. Among them, anti-angiogenic gene therapy has received attention due to its apparent advantages. Although specific problems remain prior to cancer being fully curable using anti-angiogenic gene therapy, several methods have been explored, and progress has been made in pre-clinical and clinical settings over previous decades. The present review aimed to provide up-to-date information concerning tumor angiogenesis and gene delivery systems in anti-angiogenic gene therapy, with a focus on recent developments in the study and application of the most commonly studied and newly identified anti-angiogenic candidates for anti-angiogenesis gene therapy, including interleukin-12, angiostatin, endostatin, tumstatin, anti-angiogenic metargidin peptide and endoglin silencing.

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Section: Anti-angiogenesis Gene Therapy and Angiogenesis Inhibitorsmentioning

confidence: 99%

Tumor angiogenesis and anti‑angiogenic gene therapy for cancer (Review)

et al. 2018

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“…The combination of matricryptins with inhibitors of pro-angiogenic pathways, chemotherapy, or radiotherapy enhance their therapeutic efficacy. Tumstatin has been fused to another endogenous inhibitor of angiogenesis, vasostatin (Gu et al, 2014 ) and to tumor necrosis factor α, which has anti-tumoral and anti-angiogenic properties, which results in a more effective fusion protein than tumstatin alone (Luo et al, 2006 ). Endostatin has been fused to the proapoptotic domain (BH3) of the BAX protein (Chura-Chambi et al, 2014 ), to tumor necrosis factor-related apoptosis-inducing ligand (Zheng et al, 2013 ) and one of its anti-angiogenic sequences to an heptapeptide inhibitor of MMPs (Qiu et al, 2013 ).…”

Section: Matricryptins As Potential Drugsmentioning

confidence: 99%

Matricryptins Network with Matricellular Receptors at the Surface of Endothelial and Tumor Cells

Ricard‐Blum

Vallet

2016

Front. Pharmacol.

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The extracellular matrix (ECM) is a source of bioactive fragments called matricryptins or matrikines resulting from the proteolytic cleavage of extracellular proteins (e.g., collagens, elastin, and laminins) and proteoglycans (e.g., perlecan). Matrix metalloproteinases (MMPs), cathepsins, and bone-morphogenetic protein-1 release fragments, which regulate physiopathological processes including tumor growth, metastasis, and angiogenesis, a pre-requisite for tumor growth. A number of matricryptins, and/or synthetic peptides derived from them, are currently investigated as potential anti-cancer drugs both in vitro and in animal models. Modifications aiming at improving their efficiency and their delivery to their target cells are studied. However, their use as drugs is not straightforward. The biological activities of these fragments are mediated by several receptor families. Several matricryptins may bind to the same matricellular receptor, and a single matricryptin may bind to two different receptors belonging or not to the same family such as integrins and growth factor receptors. Furthermore, some matricryptins interact with each other, integrins and growth factor receptors crosstalk and a signaling pathway may be regulated by several matricryptins. This forms an intricate 3D interaction network at the surface of tumor and endothelial cells, which is tightly associated with other cell-surface associated molecules such as heparan sulfate, caveolin, and nucleolin. Deciphering the molecular mechanisms underlying the behavior of this network is required in order to optimize the development of matricryptins as anti-cancer agents.

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