Shen Lei, Zhang Peng, Zhang Shanqiang, Xie Liping, Yao Lijie, Lang Weiya, Lian Jie, Qin Wei, Zhang Meng, Ji Liang
Department of Anatomy, Qiqihar Medical University, Qiqihar, Heilongjiang 161006, P.R. China.
Exp Ther Med. 2017 Jun;13(6):3021-3031. doi: 10.3892/etm.2017.4305. Epub 2017 Apr 5.
C-X-C motif chemokine ligand 8 (CXCL-8) promotes cell homing and angiogenesis. However, under hypoxic conditions, the role of CXCL-8 in the homing of human umbilical vein endothelial cells (HUVECs), and its effect on the healing of skin ulcers caused by ischemia and hypoxia remain unknown. In the current study, assays measuring cell proliferation, angiogenesis and cell migration were performed to evaluate alterations in the proliferation, angiogenic capacity and chemotaxis of HUVECs treated with CXCL-8 protein and/or an Akt inhibitor (AZD5363 group) under hypoxic conditions. Changes in the levels of Akt, signal transducer and activator of transcription 3 (STAT3), vascular endothelial growth factor (VEGF), malondialdehyde (MDA) and total-superoxide dismutase (total-SOD) were also detected by western blotting and ELISA. In addition, experiments were performed using a skin ulcer model in mice. Ischemic and hypoxic skin ulcers were created on the thighs of C57BL/6J mice, and the effects of CXCL-8 and HUVEC transplantation on the healing capacity of skin ulcers was determined by injecting mice with HUVECs and/or CXCL-8 recombinant protein (CXCL-8, HUVEC and HUVEC + CXCL-8 groups). Vascular endothelial cell homing, changes in vascular density and the expression of VEGF, SOD, EGF and MDA within the ulcer tissue were subsequently measured. experiments demonstrated that HUVEC proliferation, migration and tube forming capacity were significantly increased by CXCL-8 under hypoxic conditions. Additionally, levels of VEGF, MDA and SOD were significantly higher in the CXCL-8 group, though were significantly decreased by the Akt and STAT3 inhibitors. experiments demonstrated that the expression of VEGF, total-SOD and EGF proteins were higher in the skin ulcer tissue of mice treated with CXCL-8 + HUVEC, relative to mice treated with HUVECs alone. Furthermore, vascular endothelial cell homing and vascular density were significantly increased in the CXCL-8 + HUVEC group, indicating that combined use of HUVECs and CXCL-8 may promote the healing of ischemic skin ulcers. The present results demonstrate that CXCL-8 may stimulate vascular endothelial cells to secrete VEGF, SOD and other cytokines via the Akt-STAT3 pathway, which in turn serves a key regulatory role in the recruitment of vascular endothelial cells, reduction of hypoxia-related injury and promotion of tissue repair following hypoxic/ischemic injury.
C-X-C基序趋化因子配体8(CXCL-8)可促进细胞归巢和血管生成。然而,在缺氧条件下,CXCL-8在人脐静脉内皮细胞(HUVECs)归巢中的作用及其对缺血缺氧所致皮肤溃疡愈合的影响尚不清楚。在本研究中,进行了测量细胞增殖、血管生成和细胞迁移的实验,以评估在缺氧条件下用CXCL-8蛋白和/或Akt抑制剂(AZD5363组)处理的HUVECs在增殖、血管生成能力和趋化性方面的变化。还通过蛋白质印迹法和酶联免疫吸附测定法检测了Akt、信号转导子和转录激活子3(STAT3)、血管内皮生长因子(VEGF)、丙二醛(MDA)和总超氧化物歧化酶(总SOD)水平的变化。此外,使用小鼠皮肤溃疡模型进行了实验。在C57BL/6J小鼠的大腿上制造缺血缺氧性皮肤溃疡,并通过给小鼠注射HUVECs和/或CXCL-8重组蛋白(CXCL-8组、HUVEC组和HUVEC + CXCL-8组)来确定CXCL-8和HUVEC移植对皮肤溃疡愈合能力的影响。随后测量了溃疡组织内血管内皮细胞归巢、血管密度变化以及VEGF、SOD、表皮生长因子(EGF)和MDA的表达。实验表明,在缺氧条件下,CXCL-8可显著提高HUVEC的增殖、迁移和管形成能力。此外,CXCL-8组中VEGF、MDA和SOD水平显著升高,不过Akt和STAT3抑制剂可使其显著降低。实验表明,与单独用HUVECs处理的小鼠相比,用CXCL-8 + HUVEC处理的小鼠皮肤溃疡组织中VEGF、总SOD和EGF蛋白的表达更高。此外,CXCL-8 + HUVEC组中血管内皮细胞归巢和血管密度显著增加,表明联合使用HUVECs和CXCL-8可能促进缺血性皮肤溃疡的愈合。目前的结果表明,CXCL-8可能通过Akt-STAT3途径刺激血管内皮细胞分泌VEGF、SOD和其他细胞因子,这反过来在缺氧/缺血性损伤后血管内皮细胞的募集、缺氧相关损伤的减轻和组织修复中起关键调节作用。
