Department of Pharmaceutical Sciences, College of Health Professions, North Dakota State University, Sudro-16, Albrecht Blvd., Fargo, ND, 58108, USA.
School of Biomedical Sciences, University of North Dakota, Grand Forks, ND, 58202, USA.
Sci Rep. 2023 Feb 13;13(1):2543. doi: 10.1038/s41598-023-29853-w.
Aging is associated with chronic systemic inflammation largely due to increased myelopoiesis, which in turn increases risk for vascular disease. We have previously shown evidence for the therapeutic potential of Angiotensin-(1-7) (Ang-(1-7)) in reversing vasoreparative dysfunction in aging. This study tested the hypothesis that ischemic vascular repair in aging by Ang-(1-7) involves attenuation of myelopoietic potential in the bone marrow and decreased mobilization of inflammatory cells. Young or Old male mice of age 3-4 and 22-24 months, respectively, received Ang-(1-7) (1 µg/kg/min, s.c.) for four weeks. Myelopoiesis was evaluated in the bone marrow (BM) cells by carrying out the colony forming unit (CFU-GM) assay followed by flow cytometry of monocyte-macrophages. Expression of pro-myelopoietic factors and alarmins in the hematopoietic progenitor-enriched BM cells was evaluated. Hindlimb ischemia (HLI) was induced by femoral ligation, and mobilization of monocytes into the blood stream was determined. Blood flow recovery was monitored by Laser Doppler imaging and infiltration of inflammatory cells was evaluated by immunohistochemistry. BM cells from Old mice generated a higher number of monocytes (Ly6GCD11bLy6C) and M1 macrophages (Ly6CF4/80) compared to that of Young, which was reversed by Ang-(1-7). Gene expression of selected myelopoietic factors, alarmins (S100A8, S100A9, S100A14 and HMGb1) and the receptor for alarmins, RAGE, was higher in the Old hematopoietic progenitor-enriched BM cells compared to the Young. Increased expressions of these factors were decreased by Ang-(1-7). Ischemia-induced mobilization of monocytes was higher in Old mice with decreased blood flow recovery and increased infiltration of monocyte-macrophages compared to the Young, all of which were reversed by Ang-(1-7). Enhanced ischemic vascular repair by Ang-(1-7) in aging is largely by decreasing the generation and recruitment of inflammatory monocyte-macrophages to the areas of ischemic injury. This is associated with decreased alarmin signaling in the BM-hematopoietic progenitor cells.
衰老是与慢性系统性炎症相关,主要是由于髓系细胞过度生成,这反过来又增加了血管疾病的风险。我们之前已经证明了血管紧张素-(1-7)(Ang-(1-7))在逆转衰老中血管修复功能障碍方面的治疗潜力。本研究通过检测 Ang-(1-7)对衰老的缺血性血管修复作用是否涉及骨髓中髓系生成潜能的衰减和炎症细胞的动员减少,来验证这一假设。分别给予 3-4 个月和 22-24 个月龄的年轻或年老雄性小鼠 Ang-(1-7)(1µg/kg/min,皮下注射)4 周。通过集落形成单位(CFU-GM)检测和单核-巨噬细胞流式细胞术评估骨髓(BM)细胞中的髓系生成。评估富含造血祖细胞的 BM 细胞中促髓系生成因子和警报素的表达。通过股动脉结扎诱导后肢缺血(HLI),并测定单核细胞向血流中的动员。通过激光多普勒成像监测血流恢复,通过免疫组织化学评估炎症细胞浸润。与年轻小鼠相比,老年小鼠的 BM 细胞产生了更多的单核细胞(Ly6GCD11bLy6C)和 M1 巨噬细胞(Ly6CF4/80),这一现象被 Ang-(1-7)逆转。与年轻小鼠相比,富含造血祖细胞的老年 BM 细胞中选定的髓系生成因子、警报素(S100A8、S100A9、S100A14 和 HMGb1)和警报素受体 RAGE 的基因表达更高。Ang-(1-7)降低了这些因子的表达。与年轻小鼠相比,老年小鼠的单核细胞动员增加,血流恢复减少,单核-巨噬细胞浸润增加,所有这些都被 Ang-(1-7)逆转。Ang-(1-7)在衰老中增强的缺血性血管修复主要是通过减少炎症性单核-巨噬细胞向缺血损伤部位的生成和募集来实现的。这与 BM-造血祖细胞中警报素信号的减少有关。
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