Literature DB >> 22547351

Predicting the effects of anti-angiogenic agents targeting specific VEGF isoforms.

Stacey D Finley1, Aleksander S Popel.   

Abstract

Vascular endothelial growth factor (VEGF) is a key mediator of angiogenesis, whose effect on cancer growth and development is well characterized. Alternative splicing of VEGF leads to several different isoforms, which are differentially expressed in various tumor types and have distinct functions in tumor blood vessel formation. Many cancer therapies aim to inhibit angiogenesis by targeting VEGF and preventing intracellular signaling leading to tumor vascularization; however, the effects of targeting specific VEGF isoforms have received little attention in the clinical setting. In this work, we investigate the effects of selectively targeting a single VEGF isoform, as compared with inhibiting all isoforms. We utilize a molecular-detailed whole-body compartment model of VEGF transport and kinetics in the presence of breast tumor. The model includes two major VEGF isoforms, VEGF(121) and VEGF(165), receptors VEGFR1 and VEGFR2, and co-receptors Neuropilin-1 and Neuropilin-2. We utilize the model to predict the concentrations of free VEGF, the number of VEGF/VEGFR2 complexes (considered to be pro-angiogenic), and the receptor occupancy profiles following inhibition of VEGF using isoform-specific anti-VEGF agents. We predict that targeting VEGF(121) leads to a 54% and 84% reduction in free VEGF in tumors that secrete both VEGF isoforms or tumors that overexpress VEGF(121), respectively. Additionally, 21% of the VEGFR2 molecules in the blood are ligated following inhibition of VEGF(121), compared with 88% when both isoforms are targeted. Targeting VEGF(121) reduces tumor free VEGF and is an effective treatment strategy. Our results provide a basis for clinical investigation of isoform-specific anti-VEGF agents.

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Year:  2012        PMID: 22547351      PMCID: PMC3385824          DOI: 10.1208/s12248-012-9363-4

Source DB:  PubMed          Journal:  AAPS J        ISSN: 1550-7416            Impact factor:   4.009


  47 in total

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4.  Lymphatic metastasis in the absence of functional intratumor lymphatics.

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Authors:  Eugene W M Ng; David T Shima; Perry Calias; Emmett T Cunningham; David R Guyer; Anthony P Adamis
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6.  Tumour control by whole brain irradiation of anti-VEGF-treated mice bearing intracerebral glioma.

Authors:  Joost J C Verhoeff; Lukas J A Stalpers; An Claes; Koos E Hovinga; Gijsbert D Musters; W Peter Vandertop; Dick J Richel; William P J Leenders; Wouter R van Furth
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7.  Vascular endothelial growth factor splice variants and their prognostic value in breast and ovarian cancer.

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8.  Tissue-specific expression pattern of vascular endothelial growth factor isoforms in the malignant transformation of lung and colon.

Authors:  N Cheung; M P Wong; S T Yuen; S Y Leung; L P Chung
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9.  Functional and structural characteristics of tumor angiogenesis in lung cancers overexpressing different VEGF isoforms assessed by DCE- and SSCE-MRI.

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10.  Pharmacokinetics and pharmacodynamics of VEGF-neutralizing antibodies.

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  27 in total

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2.  Dynamics of tumor-associated macrophages in a quantitative systems pharmacology model of immunotherapy in triple-negative breast cancer.

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4.  Effect of tumor microenvironment on tumor VEGF during anti-VEGF treatment: systems biology predictions.

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Review 5.  Computational systems biology approaches to anti-angiogenic cancer therapeutics.

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6.  Compartment model predicts VEGF secretion and investigates the effects of VEGF trap in tumor-bearing mice.

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7.  New models of pulmonary hypertension based on VEGF receptor blockade-induced endothelial cell apoptosis.

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9.  Overexpression of miRNA-497 inhibits tumor angiogenesis by targeting VEGFR2.

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Review 10.  Oncogenic alternative splicing switches: role in cancer progression and prospects for therapy.

Authors:  Serena Bonomi; Stefania Gallo; Morena Catillo; Daniela Pignataro; Giuseppe Biamonti; Claudia Ghigna
Journal:  Int J Cell Biol       Date:  2013-10-27
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