Phenotypic knockout of VEGF-R2 and Tie-2 with an intradiabody reduces tumor growth and angiogenesis<i>in vivo</i>

Jendreyko, Nina; Popkov, Mikhail; Rader, Christoph; Barbas, Carlos F.

doi:10.1073/pnas.0503168102

Cited by 82 publications

(60 citation statements)

References 34 publications

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“…In a melanoma xenograft model, VEGFR-2 and Tie2 intradiabodies have reduced subcutaneous tumor growth. 38 In a prostate tumor model, combined local delivery of endostatin-angiostatin and sTie2 revealed increased treatment effect. 39 Inhibition of Tie2 has been utilized in cancer models including mammary tumors, 32 melanoma 32,40 and glioblastoma multiforme 41 and reduced tumor growth has been achieved.…”

Section: Discussionmentioning

confidence: 99%

Cotargeting of VEGFR-1 and -3 and angiopoietin receptor Tie2 reduces the growth of solid human ovarian cancer in mice

et al. 2010

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Despite optimal surgery and chemotherapy, the prognosis of ovarian cancer patients remains poor and new treatments are urgently needed. Solid tumors require the formation of new vessels for growth and metastasis. In the present study, we have used soluble vascular endothelial growth factor (sVEGF) receptors sVEGFR-1 and -3, soluble receptors Tie1 and Tie2 and their combinations in an ovarian cancer xenograft model. Human ovarian cancer cells were injected intraperitoneally into nude mice (n ¼ 42) and magnetic resonance imaging (MRI) was used for confirming tumors before gene delivery. Treatment with combined AdsVEGFR-1, AdsVEGFR-3 and AdsTie2 significantly decreased the size of the intraperitoneal tumors compared with the controls (AdLacZ; P ¼ 0.038) with significantly less microvessels and vascular area. Unexpectedly, treatment with combined AdsTie1 and AdsTie2 led to a dramatic shortening of the survival which was not observed in the groups receiving either of the soluble receptors alone (P ¼ 0.031). The only difference to other treatments was liver toxicity observed after the combined Tie receptor treatment.In conclusion, combined inhibition of VEGFR-1, VEGFR-3 and Tie2 pathways was safe and provided efficient therapy for ovarian cancer in mice.

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Section: Discussionmentioning

confidence: 99%

Cotargeting of VEGFR-1 and -3 and angiopoietin receptor Tie2 reduces the growth of solid human ovarian cancer in mice

et al. 2010

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“…9 Consequently, impairing two anti-angiogenic pathways at a time is more efficient than monotherapy. 10,11 Given the heterogeneous responses to anti-angiogenesis in animal models and the increasing use of anti-VEGF therapy in humans (Bevacizumab, Avastin TM ), it is important to comprehend how tumor cells react to such therapies on a molecular level. This knowledge most certainly will help to identify new ''druggable'' targets 12 for adjuvant anti-angiogenic intervention.…”

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confidence: 99%

Experimental anti‐angiogenesis causes upregulation of genes associated with poor survival in glioblastoma

Saidi

Javerzat

Bellahcène

et al. 2007

Intl Journal of Cancer

101

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Vascular endothelial growth factor (VEGF) inhibitors are the most promising anti‐angiogenic agents used increasingly in the clinic. However, to be efficient, anti‐VEGF agents need to be associated with classic chemotherapy. Exploring gene regulation in tumor cells during anti‐angiogenesis might help to comprehend the molecular basis of response to treatment. To generate a defined anti‐angiogenic condition in vivo, we transfected human glioma cells with short‐interfering RNAs against VEGF‐A and implanted them on the chick chorio‐allantoic membrane. Gene regulation in avascular tumors was studied using human Affymetrix™ GeneChips. Potentially important genes were further studied in glioma patients. Despite strong VEGF inhibition, we observed recurrent formation of small, avascular tumors. CHI3L2, IL1B, PI3/elafin and CHI3L1, which encodes for YKL‐40, a putative prognosticator for various diseases, including cancer, were strongly up‐regulated in avascular glioma. In glioblastoma patients, these genes showed coregulation and their expression differed significantly from low‐grade glioma. Importantly, high levels of CHI3L1 (p = 0.036) and PI3/elafin mRNA (p = 0.0004) were significantly correlated with poor survival. Cox regression analysis further confirmed that PI3 and CHI3L1 levels are survival markers independent from patient age and sex. Elafin‐positive tumor cells were only found in glioblastoma, where they were clustered around necrotic areas. PI3/elafin is strongly induced by serum deprivation and hypoxia in U87 glioma cells in vitro. Our results indicate that anti‐angiogenesis in experimental glioma drives expression of critical genes which relate to disease aggressiveness in glioblastoma patients. In particular, CHI3L1 and PI3/elafin may be useful as new prognostic markers and new therapeutic targets. © 2007 Wiley‐Liss, Inc.

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“…The most commonly used intrabodies are in the form of scFv as a single polypeptide. Other antibody formats have also been used, including Fab fragments [79] , single domain antibodies [80] , conventional IgG antibodies, and multivalent bispecific fragments (for example, "intradiabody" [81] ). Intrabodies, through the use of N-or C-terminal tags that encode natural intracellular trafficking signals, can direct the antibody-antigen interaction to a specific cellular compartment [82] .…”

Section: Intrabodymentioning

confidence: 99%

Research and development of next generation of antibody-based therapeutics

Zhu

2010

Acta Pharmacol Sin

122

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Monoclonal antibodies (mAb) are emerging as one of the major class of therapeutic agents in the treatment of many human diseases, in particular in cancer and immunological disorders. To date, 28 mAb have been approved by the United States Food and Drug Administration for clinical applications. In addition, several hundreds of mAb are being developed clinically by many biotech and pharmaceutical companies for various disease indications. Many challenges still remain, however, and the full potential of therapeutic antibodies has yet to be realized. With the advancement of antibody engineering technologies and our further understanding of disease biology as well as antibody mechanism of action, many classes of novel antibody formats or antibody derived molecules are emerging as promising new generation therapeutics. These new antibody formats or molecules are carefully designed and engineered to acquire special features, such as improved pharmacokinetics, increased selectivity, and enhanced efficacy. These new agents may have the potential to revolutionize both our thinking and practice in the efforts to research and develop next generation antibody-based therapeutics.

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Phenotypic knockout of VEGF-R2 and Tie-2 with an intradiabody reduces tumor growth and angiogenesisin vivo

Cited by 82 publications

References 34 publications

Cotargeting of VEGFR-1 and -3 and angiopoietin receptor Tie2 reduces the growth of solid human ovarian cancer in mice

Cotargeting of VEGFR-1 and -3 and angiopoietin receptor Tie2 reduces the growth of solid human ovarian cancer in mice

Experimental anti‐angiogenesis causes upregulation of genes associated with poor survival in glioblastoma

Research and development of next generation of antibody-based therapeutics

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