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Last update 08 May 2025

PDGFB x VEGF

Last update 08 May 2025

Basic Info

Related Targets

PDGFBVEGF

Drugs associated with PDGFB x VEGF

ABBV642

Target

PDGFB x VEGF

Mechanism

PDGFB inhibitors [+1]

Active Org.

AbbVie AS

Originator Org.

AbbVie AS

Active Indication

Wet age-related macular degeneration

Inactive Indication-

Drug Highest PhasePreclinical

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

MP0260

Target

PDGFB x VEGF-A

Mechanism

PDGFB inhibitors [+1]

Active Org.-

Originator Org.

Molecular Partners AG

Active Indication-

Inactive Indication

Wet age-related macular degeneration

Drug Highest PhasePending

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

100 Clinical Results associated with PDGFB x VEGF

100 Translational Medicine associated with PDGFB x VEGF

0 Patents (Medical) associated with PDGFB x VEGF

272

Literatures (Medical) associated with PDGFB x VEGF

01 Apr 2025·Alzheimer's & Dementia

Blood biomarkers of vascular dysfunction in small vessel disease progression: Insights from a longitudinal neuroimaging study

Article

Author: Chappell, Francesca M. ; Sleight, Emilie ; Wardlaw, Joanna M. ; Wiseman, Stewart ; Jochems, Angela C. C. ; Thrippleton, Michael J. ; Stringer, Michael S. ; Backhouse, Ellen V. ; Brown, Rosalind ; Clancy, Una ; Valdés‐Hernandez, Maria C. ; Cheng, Yajun ; Doubal, Fergus N. ; Jaime Garcia, Daniela ; Montagne, Axel ; Arteaga, Carmen ; Zhang, Junfang

AbstractINTRODUCTIONThis study explored the relationship between blood biomarkers of cerebrovascular function and small vessel disease (SVD) neuroimaging markers and cognitive outcomes in highly‐phenotyped participants.METHODSWe conducted cross‐sectional and 1‐year longitudinal analyses on 181 patients with mild ischemic stroke, enriched for SVD features. We examined relationships between a panel of 13 blood biomarkers and magnetic resonance imaging (MRI) markers of SVD (structural lesions, diffusion‐weighted imaging [DWI]‐positive lesions, blood‐brain barrier (BBB) permeability, and cerebrovascular reactivity (CVR), and cognition.RESULTSIn linear mixed models, vascular endothelial growth factor was significantly associated with incident DWI‐positive lesions over 1 year. Intercellular adhesion molecule‐1 was linked with lower CVR while platelet‐derived growth factor‐subunit B and Endothelin‐1 were associated with higher CVR. Platelet‐Selectin levels were associated with mild cognitive impairment at 1 year.DISCUSSIONOur results support the role of endothelial and pericyte dysfunction in SVD burden and progression and suggest that specific biomarkers relate to distinct SVD manifestations.Highlights

Small vessel disease (SVD) lacks specific or predictive biomarker signatures.

Vascular endothelial growth factor levels were linked to incident lesions detected over 1 year.

Circulating intercellular adhesion molecule‐1 related to lower cerebrovascular reactivity.

Platelet‐selectin levels were associated with mild cognitive impairment longitudinally.

These findings could help stratify patients at high‐risk of rapid‐progression SVD.

01 Apr 2025·Plastic & Reconstructive Surgery

Comparative Study of Adipose-Derived Stem Cells from Localized Scleroderma Patients and Healthy Donors in Treating Skin Fibrosis

Article

Author: Kang, Lin ; Huang, Jiuzuo ; Long, Xiao ; Wang, Hayson Chenyu ; Yang, Yuemei ; Li, Ziming ; Li, Yunzhu ; Xiao, Yiding ; Li, Zhujun ; Yu, Nanze

Background:Localized scleroderma (LoS) is an autoimmune disease characterized by fibrosis of the skin and atrophy of the subcutaneous fat tissue. Use of adipose-derived mesenchymal stem cells (ASCs) is a promising treatment approach for LoS. However, ASCs from scleroderma patients (LoS ASCs) have been shown to exhibit altered characteristics compared with ASCs from healthy donors (healthy ASCs). This study aimed to compare the abilities of LoS ASCs and healthy ASCs in treating skin fibrosis.Methods:The paracrine ability of ASCs was tested with cytokine array. Bleomycin-challenged mouse models received subcutaneous injection of LoS ASCs and healthy ASCs. Pathologic staining and Western blotting of collagenase type I and α-smooth muscle actin was performed. Fibroblasts derived from LoS lesions (LoS FB) were co-cultured with ASCs, and subjected to RNA sequencing to further explore the similarities and differences in the treatment mechanism.Results:In vivo comparison revealed that healthy ASCs had a stronger proliferation ability and secreted higher levels of growth factors and cytokines, including vascular endothelial growth factor A, platelet-derived growth factor fibroblasts, and interleukin-10. Pathologic staining of the skin in mouse models treated with ASCs demonstrated that healthy ASCs were more effective in reducing dermal thickness and collagen deposition, and increasing microvessel density and the proportion of M2 macrophages. Co-culture with both healthy ASCs and LoS ASCs reduced the proliferation and migration abilities of LoS FB, and the protein expression of α-smooth muscle actin and collagenase type I. RNA sequencing and validation revealed potential difference in the canonical Wnt pathway.Conclusion:Healthy ASCs exhibited stronger proliferation, paracrine, antifibrosis, proangiogenesis, and immunomodulation abilities in treating skin fibrosis in scleroderma mouse models.Clinical Relevance Statement:Allogenic ASCs obtained from healthy donors are more efficient in treating skin fibrosis, and could serve as a potential alternative for patients who are not suitable candidates for liposuction surgery in the future.

01 Jan 2025·Molecular vision

Identification of genetic factors underlying severe retinopathy of prematurity in preterm infants.

Article

Author: Cheng, Ping ; Wang, Zhangsheng ; Sun, Huiqing ; Yu, Zengyuan ; Xing, Shan ; Li, Lifeng ; Xia, Zhiyi ; Li, Mingchao ; Zhang, Hongbo

ObjectiveRetinopathy of prematurity (ROP) is a pathological condition characterized by abnormal proliferation of retinal vessels and it represents the primary cause of visual impairment in preterm infants. There is increasing backing for the involvement of genetic factors in the onset of ROP.MethodsA prospective cohort study assessed the allele frequency and genotype distribution of gene polymorphisms in angiogenesis, inflammation and oxygen-sensing pathways in preterm infants with severe ROP. The role of genetic polymorphism in ROP development was investigated using next-generation sequencing (NGS) combined with candidate genes and data mining methods.ResultsA total of 47 confirmed severe ROP cases and gestational age, birthweight and days of oxygen therapy plus 35 similar control infants were enrolled in this study. In the initial hypothesis-generating survey, we selected a p value of 0.01 to minimize false positives while retaining true positives. Using this criterion, we identified 19 single-nucleotide polymorphisms across 11 genes that were associated with the occurrence of ROP (ZNF717, IHH, SEC22B, IGSF3, HYDIN), GGT1, FRG1, CDC27, LRRC37A3, CTAGE4 and ADAMTS7; all p<0.001). Compared with the control group, 62 single-nucleotide polymorphisms in 19 candidate genes (VEGF, EPO, EPAS-1, HIF1A, RUNX1, ESR1, CFH, PDGFB, JAK, STAT, IGF-1, IGFBP2, GPX4, TLR4, ROS1, CYP, TP53BP1, NOS3, TNF) representing angiogenic, inflammation, oxygen-sensing pathways and proliferative retinopathic diseases were found to be associated with the development of severe ROP (all p<0.01).ConclusionsUsing NGS gene analysis suggests that genetic risk factors may play an important role in susceptibility to the development of ROP.

News (Medical) associated with PDGFB x VEGF

03 Jan 2023

·www.sciencedaily.com

Researchers hypothesized that AMD and COVID-19 share common genetic risk factors and carried out a study that identified a novel association of the two diseases with variants in the PDGFB gene. This gene encodes a platelet derived growth factor (Pdgf) which has a role in the formation of new blood vessels and is involved in the abnormal blood vessel changes that occur in AMD. They also found that more severe COVID-19 outcomes were associated with AMD likely arising from genetic predisposition to dysfunction involving complement proteins, as well as with a higher level of Pdgf in blood serum. Recent evidence has emerged to suggest that age-related macular degeneration (AMD) is a clinical risk factor for increased risk for infection and mortality. AMD has been reported to confer higher risk of severe complications of SARS-CoV-2 infection, including respiratory failure and death (25 percent), a risk which is higher than Type 2 diabetes (21 percent) and obesity (13 percent). Considering these observations, researchers from Boston University Chobanian & Avedisian School of Medicine hypothesized that AMD and COVID-19 share common genetic risk factors and designed and executed a study that identified a novel association of the two diseases with variants in the PDGFB gene. This gene encodes a platelet derived growth factor (PDGF) which has a role in the formation of new blood vessels and is involved in the abnormal blood vessel changes that occur in AMD. They also found that more severe COVID-19 outcomes were associated with AMD likely arising from genetic predisposition to dysfunction involving complement proteins, as well as with a higher level of PDGF in blood serum. "Our findings add to the body of evidence for the increased risk of infection and mortality from COVID-19 among AMD patients. Our analysis lends credence to previously reported clinical studies that found those with AMD have a higher risk for COVID-19 infection and severe disease, and that this increased risk may have a genetic basis," explained co-corresponding author Lindsay A. Farrer, PhD, chief of biomedical genetics. The BU research team conducted a genome-wide search for variants that are jointly associated with AMD and each of three COVID-19 outcomes (infection rate, critical illness and hospitalization) using large genetic datasets that contained tens of thousands of individuals. These datasets were previously assembled and studied separately for genetic factors contributing to the risk of AMD and for each of the COVID-19 disease outcomes. Subsequently, the researchers analyzed publicly available data from patients with AMD or COVID-19 and control groups to assess the association of variants in PDGFB with the gene activity. Finally, they employed an analytical technique that allowed them to investigate causal relationships between PDGFB gene variants, PDGFB concentration in blood, AMD, and COVID-19 outcomes. According to the researchers, these findings suggest that lowering PDGFB gene activity and serum PDGF concentration may reduce the severity of COVID-19, particularly among older people. "Therapeutic strategies combining anti-VEGF therapy (a current treatment for AMD that limits blood vessel growth in the eye that can harm vision) with antagonists (drugs that bind to receptors) for blocking PDGF signaling have been considered even more effective than the single VEGF treatment and are currently under investigation in clinical trials," added co-corresponding author Manju L. Subramanian, MD, associate professor of ophthalmology. The researchers believe this discovery of shared genetic risk factors will require a larger sample size for critical illness and hospitalizations to better understand the shared pathology and risk factors that contribute to worsening clinical outcomes in both disease states. These findings appear online in the Journal of Clinical Medicine. This work was supported by National Institutes of Health grants RF1 AG057519, R01 AG069453, R01 AG048927, U19 AG068753, and U01 AG062602.

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