Aonuma Tatsuya, Takehara Naofumi, Maruyama Keisuke, Kabara Maki, Matsuki Motoki, Yamauchi Atsushi, Kawabe Jun-Ichi, Hasebe Naoyuki
Department of Internal Medicine, Division of Cardiology, Nephrology, Pulmonology, and Neurology, Asahikawa Medical University, Asahikawa, Japan.
Department of Internal Medicine, Division of Cardiology, Nephrology, Pulmonology, and Neurology, Asahikawa Medical University, Asahikawa, Japan Department of Cardiovascular Regeneration and Innovation, Asahikawa Medical University, Asahikawa, Japan
Stem Cells Transl Med. 2016 Aug;5(8):1067-78. doi: 10.5966/sctm.2015-0281. Epub 2016 Jun 22.
: Overcoming the insufficient survival of cell grafts is an essential objective in cell-based therapy. Apurinic/apyrimidinic endonuclease/redox factor 1 (APE1) promotes cell survival and may enhance the therapeutic effect of engrafted cells. The aim of this study is to determine whether APE1 overexpression in cardiac progenitor cells (CPCs) could ameliorate the efficiency of cell-based therapy. CPCs isolated from 8- to 10-week-old C57BL/6 mouse hearts were infected with retrovirus harboring APE1-DsRed (APE1-CPC) or a DsRed control (control-CPC). Oxidative stress-induced apoptosis was then assessed in APE1-CPCs, control-CPCs, and neonatal rat ventricular myocytes (NRVMs) cocultured with these CPCs. This analysis revealed that APE1 overexpression inhibited CPC apoptosis with activation of transforming growth factor β-activated kinase 1 (TAK1) and nuclear factor (NF)-κB. In the coculture model, NRVM apoptosis was inhibited to a greater extent in the presence of APE1-CPCs compared with control-CPCs. Moreover, the number of surviving DsRed-positive CPC grafts was significantly higher 7 days after the transplant of APE1-CPCs into a mouse myocardial infarction model, and the left ventricular ejection fraction showed greater improvement with attenuation of fibrosis 28 days after the transplant of APE1-CPCs compared with control-CPCs. Additionally, fewer inflammatory macrophages and a higher percentage of cardiac α-sarcomeric actinin-positive CPC-grafts were observed in mice injected with APE1-CPCs compared with control-CPCs after 7 days. In conclusion, antiapoptotic APE1-CPC graft, which increased TAK1-NF-κB pathway activation, survived effectively in the ischemic heart, restored cardiac function, and reduced cardiac inflammation and fibrosis. APE1 overexpression in CPCs may serve as a novel strategy to improve cardiac cell therapy.
Improving the survival of cell grafts is essential to maximize the efficacy of cell therapy. The authors investigated the role of APE1 in CPCs under ischemic conditions and evaluated the therapeutic efficacy of transplanted APE1-overexpressing CPCs in a mouse model of myocardial infarction. APE1 hindered apoptosis in CPC grafts subjected to oxidative stress caused in part by increased TAK1-NF-κB pathway activation. Furthermore, APE1-CPC grafts that effectively survived in the ischemic heart restored cardiac function and attenuated fibrosis through pleiotropic mechanisms that remain to be characterized. These findings suggest that APE1 overexpression in CPCs may be a novel strategy to reinforce cardiac cell therapy.
克服细胞移植后存活率不足是细胞治疗的一个重要目标。脱嘌呤/脱嘧啶内切核酸酶/氧化还原因子1(APE1)可促进细胞存活,并可能增强移植细胞的治疗效果。本研究的目的是确定心脏祖细胞(CPC)中APE1的过表达是否能提高细胞治疗的效率。从8至10周龄C57BL/6小鼠心脏分离出的CPC用携带APE1-DsRed的逆转录病毒(APE1-CPC)或DsRed对照(对照-CPC)进行感染。然后评估与这些CPC共培养的APE1-CPC、对照-CPC和新生大鼠心室肌细胞(NRVM)中氧化应激诱导的细胞凋亡。该分析表明,APE1过表达通过激活转化生长因子β激活激酶1(TAK1)和核因子(NF)-κB抑制CPC凋亡。在共培养模型中,与对照-CPC相比,在存在APE1-CPC的情况下,NRVM凋亡受到更大程度的抑制。此外,将APE1-CPC移植到小鼠心肌梗死模型中7天后,存活的DsRed阳性CPC移植数量显著更高,并且与对照-CPC相比,在移植APE1-CPC 28天后,左心室射血分数改善更大,纤维化减轻。另外,与对照-CPC相比,在注射APE1-CPC的小鼠中,7天后观察到炎症巨噬细胞更少,心脏α-肌动蛋白阳性CPC移植的百分比更高。总之,抗凋亡的APE1-CPC移植通过增加TAK1-NF-κB途径激活,在缺血心脏中有效存活,恢复心脏功能,并减少心脏炎症和纤维化。CPC中APE1过表达可能是改善心脏细胞治疗的一种新策略。
提高细胞移植的存活率对于最大化细胞治疗的疗效至关重要。作者研究了缺血条件下APE1在CPC中的作用,并在小鼠心肌梗死模型中评估了移植的过表达APE1的CPC的治疗效果。APE1通过部分增加TAK1-NF-κB途径激活所引起的氧化应激,阻碍CPC移植中的细胞凋亡。此外,在缺血心脏中有效存活的APE1-CPC移植通过多种尚未明确的机制恢复心脏功能并减轻纤维化。这些发现表明,CPC中APE1过表达可能是加强心脏细胞治疗的一种新策略。
