The Cardiac Syndecan-2 Interactome

Mathiesen, Sabrina Bech; Lunde, Marianne; Stensland, Maria; Martinsen, Marita; Nyman, Tuula A.; Christensen, Geir; Carlson, Cathrine R.

doi:10.3389/fcell.2020.00792

Cited by 6 publications

(6 citation statements)

References 112 publications

(103 reference statements)

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“…Relevant genes identified as some of the top upregulated and downregulated in our dataset include MYL12A, FBXO32, NR2F2, and PTGES, though FBXO32 and PTGES show the most promise as potential targets for screening, prevention, and/or treatment strategies for TOF. MYL12a is a partner of syndecan-2 interactome, which is upregulated during development and suspected to be involved in fibroblast contractility and cardiac fibrosis (Mathiesen et al, 2020). Syndecans are hypothesized to play a role in cardiac remodeling via their alterations of and interaction with the extracellular matrix (Mathiesen et al, 2020).…”

Section: Upregulated and Downregulated Genesmentioning

confidence: 99%

“…MYL12a is a partner of syndecan-2 interactome, which is upregulated during development and suspected to be involved in fibroblast contractility and cardiac fibrosis (Mathiesen et al, 2020). Syndecans are hypothesized to play a role in cardiac remodeling via their alterations of and interaction with the extracellular matrix (Mathiesen et al, 2020). MYL12a specifically has been noted to be involved in focal adhesion, leukocyte transendothelial migration, and regulation of the actin cytoskeleton (Mathiesen et al, 2020).…”

Section: Upregulated and Downregulated Genesmentioning

confidence: 99%

“…Syndecans are hypothesized to play a role in cardiac remodeling via their alterations of and interaction with the extracellular matrix (Mathiesen et al, 2020). MYL12a specifically has been noted to be involved in focal adhesion, leukocyte transendothelial migration, and regulation of the actin cytoskeleton (Mathiesen et al, 2020). MYL12a has been reported to be upregulated in patients with Pompe disease as well, which is characterized by cardiomyocyte hypertrophy (Karada g Gürel & Gürel, 2022).…”

Section: Upregulated and Downregulated Genesmentioning

confidence: 99%

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Meta‐analysis reveals differential gene expression in tetralogy of Fallot versus controls

Voskamp,

Hammonds,

Knapp

et al. 2023

Birth Defects Research

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ObjectivesTetralogy of Fallot (TOF) is the most common cyanotic congenital heart defect in the United States. We aimed to identify genetic variations associated with TOF using meta‐analysis of publicly available digital samples to spotlight targets for prevention, screening, and treatment strategies.MethodsWe used the Search Tag Analyze Resource for Gene Expression Omnibus (STARGEO) platform to identify 39 TOF and 19 non‐TOF right ventricle tissue samples from microarray data and identified upregulated and downregulated genes. Associated gene expression data were analyzed using ingenuity pathway analysis and restricted to genes with a statistically significant (p < .05) difference and an absolute experimental log ratio >0.1 between disease and control samples.ResultsOur analysis identified 220 genes whose expression profiles were significantly altered in TOF vs. non‐TOF samples. The most striking differences identified in gene expression included genes FBXO32, PTGES, MYL12a, and NR2F2. Some top associated canonical pathways included adrenergic signaling, estrogen receptor signaling, and the role of NFAT in cardiac hypertrophy. In general, genes involved in adaptive, defensive, and reparative cardiovascular responses showed altered expression in TOF vs. non‐TOF samples.ConclusionsWe introduced the interpretation of open “big data” using the STARGEO platform to define robust genomic signatures of congenital heart disease pathology of TOF. Overall, our meta‐analysis results indicated increased metabolism, inflammation, and altered gene expression in TOF patients. Estrogen receptor signaling and the role of NFAT in cardiac hypertrophy represent unique pathways upregulated in TOF patients and are potential targets for future pharmacologic treatments.

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Section: Upregulated and Downregulated Genesmentioning

confidence: 99%

Section: Upregulated and Downregulated Genesmentioning

confidence: 99%

Section: Upregulated and Downregulated Genesmentioning

confidence: 99%

See 1 more Smart Citation

Meta‐analysis reveals differential gene expression in tetralogy of Fallot versus controls

Voskamp,

Hammonds,

Knapp

et al. 2023

Birth Defects Research

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“…AP2A2 has a partially non-redundant function with AP2A1 owing to its unique peroxisome proliferator-activated receptor (PPAR) α responding domain, which increases fatty acid oxidization in the adipose tissue [81] by interacting with syndecan-2, a mediator of extracellular matrix (ECM) signaling in cardiac tissue [82]. Listeria monocytogenes bacteria-induced cytotoxicity was reportedly inhibited by the binding of bacterial proteins to AP2A2 in a pathway enabling bacterial growth in host cells [83].…”

Section: Ap2 Complexmentioning

confidence: 99%

“…Both AP2A1 and AP2A2 were reported to confer resistance to erlotinib, an anti-cancer drug, in lung cancer cells [ 78 ]; interact with Shc, an SH2-containing proto-oncogene involved in growth factor signaling in mammalian cancer cells [ 79 ]; and function in hemopoietic stem cell development [ 80 ]. AP2A2 has a partially non-redundant function with AP2A1 owing to its unique peroxisome proliferator-activated receptor (PPAR) α responding domain, which increases fatty acid oxidization in the adipose tissue [ 81 ] by interacting with syndecan-2, a mediator of extracellular matrix (ECM) signaling in cardiac tissue [ 82 ]. Listeria monocytogenes bacteria-induced cytotoxicity was reportedly inhibited by the binding of bacterial proteins to AP2A2 in a pathway that enable bacterial growth in host cells [ 83 ].…”

Section: Ap2 Complexmentioning

confidence: 99%

Role of adaptin protein complexes in intracellular trafficking and their impact on diseases

Shin

Nile

2021

Bioengineered

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Adaptin proteins (APs) play a crucial role in intracellular cell trafficking. The 'classical' role of APs is carried out by AP1-3, which bind to clathrin, cargo, and accessory proteins. Accordingly, AP1-3 are crucial for both vesicle formation and sorting. All APs consist of four subunits that are indispensable for their functions. In fact, based on studies using cells, model organism knockdown/knock-out, and human variants, each subunit plays crucial roles and contributes to the specificity of each AP. These studies also revealed that the sorting and intracellular trafficking function of AP can exert varying effects on pathology by controlling features such as cell development, signal transduction related to the apoptosis and proliferation pathways in cancer cells, organelle integrity, receptor presentation, and viral infection. Although the roles and functions of AP1-3 are relatively well studied, the functions of the less abundant and more recently identified APs, AP4 and AP5, are still to be investigated. Further studies on these APs may enable a better understanding and targeting of specific diseases.

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Syndecan-2 Biology and Its Role in Colorectal Carcinoma

Couchman

2022

The Extracellular Matrix and the Tumor Microenvironment

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The Cardiac Syndecan-2 Interactome

Cited by 6 publications

References 112 publications

Meta‐analysis reveals differential gene expression in tetralogy of Fallot versus controls

Meta‐analysis reveals differential gene expression in tetralogy of Fallot versus controls

Role of adaptin protein complexes in intracellular trafficking and their impact on diseases

Syndecan-2 Biology and Its Role in Colorectal Carcinoma

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