Circulating monocytes and cardiac macrophages in diastolic dysfunction (Mus musculus)
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Description
This pathway is modeled based on fig 10 in Hulsmans et al, and was developed in collaboration with Dr. Matthias Nahrendorf.
Circulating monocytes and myocardial macrophage density are increased in diastolic dysfunction, and the macrophage expansion is partially driven by monocyte recruitment. Mechanistically, cardiac macrophages produce more IL-10 leading to autocrine activation toward a fibrogenic phenotype. A profibrotic macrophage subset secretes more Spp1 (OPN) and fewer proteases and MMPs, contributing to fibroblast activation, collagen deposition, and subsequently increased myocardial stiffness and diastolic dysfunction. (Description based on figure 10 legend).
Quality Tags
Ontology Terms
Saving...Bibliography
- Hulsmans M, Sager HB, Roh JD, Valero-Muñoz M, Houstis NE, Iwamoto Y, Sun Y, Wilson RM, Wojtkiewicz G, Tricot B, Osborne MT, Hung J, Vinegoni C, Naxerova K, Sosnovik DE, Zile MR, Bradshaw AD, Liao R, Tawakol A, Weissleder R, Rosenzweig A, Swirski FK, Sam F, Nahrendorf M; ''Cardiac macrophages promote diastolic dysfunction.''; J Exp Med, 2018 PubMed Europe PMC Scholia
History
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External references
DataNodes
| Name | Type | Database reference | Comment |
|---|---|---|---|
| Ccl2 | GeneProduct | ENSMUSG00000035385 (Ensembl)  | |
| Ccr2 | GeneProduct | ENSMUSG00000049103 (Ensembl) | |
| Il10 | GeneProduct | ENSMUSG00000016529 (Ensembl) | |
| ROS | Metabolite | CHEBI:26523 (ChEBI) | |
| Spp1 | GeneProduct | ENSMUSG00000029304 (Ensembl) |
Annotated Interactions
No annotated interactions
