Vascular Endothelial Growth Factor A

Alternative Names

  • VEGFA
  • VEGF

Associated Diseases

Type 2 Diabetes Mellitus
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OMIM Number

192240

NCBI Gene ID

7422

Uniprot ID

P15692

Length

16,279 bases

No. of Exons

9

No. of isoforms

17

Protein Name

Vascular endothelial growth factor A

Molecular Mass

27042 Da

Amino Acid Count

232

Genomic Location

chr6:43,770,208-43,786,486

Gene Map Locus
6p21.1

Description

This gene is a member of the PDGF/VEGF growth factor family. It encodes a heparin-binding protein, which exists as a disulfide-linked homodimer. This growth factor induces proliferation and migration of vascular endothelial cells, and is essential for both physiological and pathological angiogenesis. Disruption of this gene in mice resulted in abnormal embryonic blood vessel formation. This gene is upregulated in many known tumors and its expression is correlated with tumor stage and progression. Elevated levels of this protein are found in patients with POEMS syndrome, also known as Crow-Fukase syndrome. Allelic variants of this gene have been associated with microvascular complications of diabetes 1 (MVCD1) and atherosclerosis. Alternatively spliced transcript variants encoding different isoforms have been described. There is also evidence for alternative translation initiation from upstream non-AUG (CUG) codons resulting in additional isoforms. A recent study showed that a C-terminally extended isoform is produced by use of an alternative in-frame translation termination codon via a stop codon readthrough mechanism, and that this isoform is antiangiogenic. Expression of some isoforms derived from the AUG start codon is regulated by a small upstream open reading frame, which is located within an internal ribosome entry site. The levels of VEGF are increased during infection with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), thus promoting inflammation by facilitating recruitment of inflammatory cells, and by increasing the level of angiopoietin II (Ang II), one of two products of the SARS-CoV-2 binding target, angiotensin-converting enzyme 2 (ACE2). In turn, Ang II facilitates the elevation of VEGF, thus forming a vicious cycle in the release of inflammatory cytokines. [From RefSeq]

Epidemiology in the Arab World

View Map
Variant NameCountryGenomic LocationClinvar Clinical SignificanceCTGA Clinical Significance Condition(s)HGVS ExpressionsdbSNPClinvar
NG_008732.1:g.4534= United Arab EmiratesNC_000006.12:g.43769749=AssociationType 2 Diabetes MellitusNG_008732.1:g.4534=833061
NM_001025366.2:c.658+398G>AUnited Arab EmiratesNC_000006.12:g.43774790G>AAssociationType 2 Diabetes MellitusNG_008732.1:g.9575G>A; NM_001025366.2:c.658+398G>A; NP_001020537.2:p.?833068
NM_001025366.2:c.659-99G>AUnited Arab EmiratesNC_000006.12:g.43777370G>ABenignAssociationType 2 Diabetes MellitusNG_008732.1:g.12155G>A; NM_001025366.2:c.659-99G>A; NP_001020537.2:p.?30249971233590
NM_001025366.2:c.855+175C>TUnited Arab EmiratesNC_000006.12:g.43777840C>TBenignAssociationType 2 Diabetes MellitusNG_008732.1:g.12625C>T; NM_001025366.2:c.855+175C>T; NP_001020537.2:p.?30249981285895

Other Reports

Oman

Al-Moundhri et al. (2009) investigated the associations between VEGF gene polymorphisms and gastric cancer (GC) risk predisposition and prognostic characteristics in an Omani population, an ethnic group which has not been studied previously. Three VEGF polymorphisms (+405 G/C, -460 T/C, and +936 C/T) were analyzed in 130 GC patients and 130 controls. Results did not reveal any significant associations between the VEGF polymorphisms and GC risk. A significant correlations between the +405 C/C genotype and both poor tumor differentiation (P = 0.007) and lymph node metastasis (P = 0.03) and between the -460 T/T genotype and poor tumor differentiation (P = 0.03) with a statistical trend toward lymph node involvement (P = 0.05), were observed in this study. VEGF gene polymorphisms had been found to have no significant effects on survival, but the VEGF +405 G/G genotype had been found to have a statistical trend toward lower survival rate with a hazard ratio of 1.6 [95% CI, 0.9-2.9] compared with the VEGF +405 CC/GC combined genotype (P = 0.049). By using multivariate analysis, Al-Moundhri et al. (2009) found that disease stage at diagnosis and the +405 G/G genotype were independent variables of adverse prognostic significance. No associations between the six common haplotypes identified and both GC risk predisposition and survival were found. Al-Moundhri et al. (2009) suggested from this study that VEGF polymorphisms have no role in GC risk predisposition, but may have prognostic significance in GC patients.

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