期刊
DIABETES CARE
卷 43, 期 7, 页码 1520-1529出版社
AMER DIABETES ASSOC
DOI: 10.2337/dc19-2227
关键词
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资金
- Italian Ministry of Health
- Ricerca Corrente
- Foundation Cariplo [2016-0922]
- British Heart Foundation
- Diabetic ONLUS Association, section of Treviso
OBJECTIVE In patients with type 2 diabetes (T2D) and critical limb ischemia (CLI), migration of circulating CD34(+)cells predicted cardiovascular mortality at 18 months after revascularization. This study aimed to provide long-term validation and mechanistic understanding of the biomarker. RESEARCH DESIGN AND METHODS The association between CD34(+)cell migration and cardiovascular mortality was reassessed at 6 years after revascularization. In a new series of T2D-CLI and control subjects, immuno-sorted bone marrow CD34(+)cells were profiled for miRNA expression and assessed for apoptosis and angiogenesis activity. The differentially regulated miRNA-21 and its proapoptotic target, PDCD4, were titrated to verify their contribution in transferring damaging signals from CD34(+)cells to endothelial cells. RESULTS Multivariable regression analysis confirmed that CD34(+)cell migration forecasts long-term cardiovascular mortality. CD34(+)cells from T2D-CLI patients were more apoptotic and less proangiogenic than those from control subjects and featured miRNA-21 downregulation, modulation of several long noncoding RNAs acting as miRNA-21 sponges, and upregulation of the miRNA-21 proapoptotic target PDCD4. Silencing miR-21 in control CD34(+)cells phenocopied the T2D-CLI cell behavior. In coculture, T2D-CLI CD34(+)cells imprinted naive endothelial cells, increasing apoptosis, reducing network formation, and modulating the TUG1 sponge/miRNA-21/PDCD4 axis. Silencing PDCD4 or scavenging reactive oxygen species protected endothelial cells from the negative influence of T2D-CLI CD34(+)cells. CONCLUSIONS Migration of CD34(+)cells predicts long-term cardiovascular mortality in T2D-CLI patients. An altered paracrine signaling conveys antiangiogenic and proapoptotic features from CD34(+)cells to the endothelium. This damaging interaction may increase the risk for life-threatening complications.
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