Mouse fibrosarcoma VEGF164 Cell Line
Invented by Prof Gillian Tozer from University Of Sheffield
Invented at Cancer Research UK London Research Institute: Lincoln's Inn Fields
- Datasheet
- References (2)
- Inventor Info
Info
| Catalogue Number | 153240 |
| Antigen/Gene or Protein Targets | VEGF120 |
| Parental Line | MEF |
| Synonyms | VEGF-A, VEGF120, VEGF164, VEGF188 |
| Host | Mouse |
| Tissue | Embryo |
| Disease Keywords | Cancer |
| Model | Immortalised Line |
| Relevance |
Mouse fibrosarcoma cell lines that are capable of expressing all vascular endothelial growth factor (VEGF) isoforms (control) or only single isoforms of VEGF (VEGF120, VEGF164, or VEGF188) were developed under endogenous VEGF promoter control. Using Cre/Lox technology, mice expressing all or only single isoforms of VEGF, known as Vegfa120/120, Vegfa164/164, and Vegfa188/188 mice were developed. Primary fibroblasts were isolated from mouse embryos that were produced by heterozygous breeding pairs of mice expressing single or all isoforms of vascular endothelial growth factor-A (VEGF-A) on Swiss background. Fibroblasts were immortalized and oncogenically transformed by retroviral transduction with SV40 and HRAS (characterised in Tozer et al., 2008. Cancer Res; 68: (7)). The original rationale for the development of these cell lines relates to the fact that tubulin-binding vascular-disrupting agents (VDA) are currently in clinical trials for cancer therapy but the factors that influence tumour susceptibility to these agents are poorly understood. Researchers evaluated the consequences of modifying tumour vascular morphology and function on vascular and therapeutic response to combretastatin-A4 3-O-phosphate (CA-4-P), which was chosen as a model VDA. The cell lines themselves could be potentially valuable for the commercial/pharmaceutical industry. |
| Production Details | Using Cre/Lox technology, mice expressing all or only single isoforms of VEGF, known as Vegfa120/120, Vegfa164/164, and Vegfa188/188 mice were developed. Primary fibroblasts were isolated from mouse embryos that were produced by heterozygous breeding pairs of mice expressing single or all isoforms of vascular endothelial growth factor-A (VEGF-A) on Swiss background. Fibroblasts were immortalized and oncogenically transformed by retroviral transduction with SV40 and HRAS (characterised in Tozer et al., 2008. Cancer Res; 68: (7)). |
| Conditional | No |
| Research Area | Cancer, Cell Signaling & Signal Transduction, Developmental Biology, Drug Discovery & Development, Metabolism |
| Growth/Phenotype Keywords | Adherent |
| Recommended Growing Conditions | High glucose DMEM (Invitrogen) medium, L-glutamine, FCS, G-418 and puromycin. antibiotics G-418 and puromycin |
| Cellosaurus ID | CVCL_HG20 |
References: 2 entries
Tozer et al. 2008. Cancer Res. 68(7):2301-11. PMID: 18381437.
Blood vessel maturation and response to vascular-disrupting therapy in single vascular endothelial growth factor-A isoform-producing tumors.
Europe PMC ID: 18381437
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References: 2 entries
Tozer et al. 2008. Cancer Res. 68(7):2301-11. PMID: 18381437.
Blood vessel maturation and response to vascular-disrupting therapy in single vascular endothelial growth factor-A isoform-producing tumors.
Add a reference
