Unknown

Dataset Information

0

Opticin Ameliorates Hypoxia-Induced Retinal Angiogenesis by Suppression of Integrin α2-I Domain-Collagen Complex Formation and RhoA/ROCK1 Signaling.

ABSTRACT:

Purpose

It was previously demonstrated that opticin (OPTC) inhibits the collagen-induced promotion of bioactivities of human retinal vascular endothelial cells (hRVECs). The present in vivo study aimed to further investigate the regulatory role of opticin in vitreous collagen-mediated retinal neovascularization and to elucidate its regulatory mechanisms with regard to integrin α2-I domain-GXXGER complex formation and RhoA/ROCK1 signal change. The regulatory role of Mg2+ on integrin α2-I domain-GXXGER complex formation in the above process was also investigated.

Methods

The zebrafish model of hypoxia-induced retinopathy was established, and OPTC-overexpressing plasmids were intravitreally injected to assess the antiangiogenesis effect of opticin. The regulatory role of opticin in integrin α2-I domain-GXXGER complex formation in vivo was analyzed by mass spectrometry. The mRNA and protein expression of RhoA/ROCK1 were examined. The concentration of Mg2+ as an activator of the integrin α2-I domain-GXXGER complex was measured. Solid-phase binding assays were performed to investigate the interference of opticin in integrin α2 collagen binding and the regulatory role of Mg2+ in that process.

Results

Opticin and OPTC-overexpressing plasmid injection reduced retinal neovascularization in the zebrafish model of hypoxia-induced retinopathy. Mass spectrometry revealed that opticin could inhibit integrin α2-I domain-GXXGER complex formation. The Mg2+ concentration was also decreased by opticin, which was another indication of the complex activation. Injection of OPTC-overexpressing plasmids inhibited mRNA and the protein expression of RhoA/ROCK1 in the zebrafish model of hypoxia-induced retinopathy. The solid-phase binding assay revealed that opticin could block integrin α2-collagen I binding in the presence of Mg2+.

Conclusions

Opticin exerts its antiangiogenesis effect by interfering in the Mg2+-modulated integrin α2-I domain-collagen complex formation and suppressing the downstream RhoA/ ROCK1 signaling pathway.

SUBMITTER: Liu X 

PROVIDER: S-EPMC8762695 | biostudies-literature |

REPOSITORIES: biostudies-literature

Json Xml

Similar Datasets

Unknown Fibroblast-derived HGF drives acinar lung cancer cell polarization through integrin-dependent RhoA-ROCK1 inhibition.
| S-EPMC6214180 | biostudies-literature
Unknown Hypoxia-inducible factors mediate coordinated RhoA-ROCK1 expression and signaling in breast cancer cells.
| S-EPMC3903228 | biostudies-other
Unknown Site-specific <i>N</i>-glycosylation of integrin α2 mediates collagen-dependent cell survival.
| S-EPMC8501769 | biostudies-literature
Unknown RhoA/ROCK1 signaling regulates stress granule formation and apoptosis.
| S-EPMC2815184 | biostudies-literature
Unknown Matrix-bound PAI-1 supports cell blebbing via RhoA/ROCK1 signaling.
| S-EPMC3283740 | biostudies-literature
Unknown Concurrent suppression of integrin alpha5, radixin, and RhoA phenocopies the effects of miR-31 on metastasis.
| S-EPMC2891350 | biostudies-literature
Unknown THBS4/integrin α2 axis mediates BM-MSCs to promote angiogenesis in gastric cancer associated with chronic <i>Helicobacter pylori</i> infection.
| S-EPMC8386559 | biostudies-literature
Unknown Cell surface transglutaminase promotes RhoA activation via integrin clustering and suppression of the Src-p190RhoGAP signaling pathway.
| S-EPMC1415321 | biostudies-literature
Unknown AMF siRNA treatment of keloid through inhibition signaling pathway of RhoA/ROCK1.
| S-EPMC6545443 | biostudies-literature
Unknown Suppression of hypoxia-induced excessive angiogenesis by metformin via elevating tumor blood perfusion.
| S-EPMC5650310 | biostudies-literature