Department of Pharmacology and Toxicology, University at Buffalo, Buffalo, New York.
The Clinical and Translational Research Center, University at Buffalo, Buffalo, New York.
Am J Physiol Heart Circ Physiol. 2022 Nov 1;323(5):H904-H916. doi: 10.1152/ajpheart.00373.2022. Epub 2022 Sep 9.
Allogeneic cardiosphere-derived cell (CDC) therapy has been demonstrated to improve myocardial function when administered to reperfused myocardial infarcts. We previously pretreated animals with low-dose cyclosporine immunosuppression to limit allogeneic CDC rejection, but whether it is necessary and, if so, can be initiated at the time of reperfusion remains uncertain. Closed-chest swine ( = 29 animals) were subjected to a 90-min left anterior descending (LAD) coronary artery occlusion. Using a three-way blinded design, we randomized two groups to receive global intracoronary infusions of 20 × 10 CDCs 30 min after reperfusion. A third control group was treated with saline. One CDC group received cyclosporine 10 min before reperfusion (2.5 mg/kg iv and 100 mg/day po), whereas the other groups received placebos. After 1 mo, neither chronic infarct size relative to area at risk (saline control, 46.2 ± 4.0%; CDCs, 46.4 ± 2.1%; and CDCs + cyclosporine, 49.2 ± 3.1%; = 0.79) nor ejection fraction (saline control, 51 ± 2%; CDCs, 51 ± 2%; and CDC + cyclosporine, 48 ± 2%; = 0.42) were different among treatment groups. Multiple histological measures of cellular remodeling, myocyte proliferation, and apoptosis were also not different among treatment groups. In contrast to previous studies, we were unable to reproduce the cardioprotective effects demonstrated by allogeneic CDCs without cyclosporine. Furthermore, initiation of intravenous cyclosporine at the time of reperfusion followed by oral therapy was not sufficient to elicit the functional improvement observed in studies where cyclosporine was started 72 h before CDC therapy. This suggests that oral cyclosporine pretreatment may be necessary to effect cardiac repair with allogeneic CDCs. In a three-way blinded, randomized design, we determined whether allogeneic CDCs administered at reperfusion improved myocardial function and whether intravenous cyclosporine enhanced their efficacy. In contrast to prior studies using oral cyclosporine, CDCs with or without intravenous cyclosporine had no effect on function or infarct size. This indicates that CDCs may be most efficacious for treating chronic LV dysfunction where cyclosporine can be initiated at least 72 h before cell therapy.
同种异体心脏球源性细胞(CDC)治疗已被证明可改善再灌注心肌梗死的心肌功能。我们之前使用低剂量环孢素免疫抑制预处理动物,以限制同种异体 CDC 的排斥反应,但这种预处理是否有必要,如果有必要,是否可以在再灌注时开始,目前仍不确定。采用闭胸猪(=29 只动物)进行 90 分钟左前降支(LAD)冠状动脉闭塞。采用三向盲法设计,我们将两组随机分为两组,在再灌注后 30 分钟接受 20×10 个 CDC 的全冠状动脉内输注。第三组对照组给予生理盐水。一组 CDC 组在再灌注前 10 分钟给予环孢素(2.5mg/kg 静脉注射和 100mg/天口服),而其他组给予安慰剂。1 个月后,慢性梗死面积相对于危险区(生理盐水对照组 46.2±4.0%;CDC 组 46.4±2.1%;CDC+环孢素组 49.2±3.1%;=0.79)和射血分数(生理盐水对照组 51±2%;CDC 组 51±2%;和 CDC+环孢素组 48±2%;=0.42)在治疗组之间均无差异。细胞重塑、心肌细胞增殖和细胞凋亡的多种组织学测量也在治疗组之间无差异。与之前的研究相反,我们未能在没有环孢素的情况下复制同种异体 CDC 所显示的心脏保护作用。此外,在再灌注时开始静脉内环孢素,然后进行口服治疗,不足以引起在环孢素开始于 CDC 治疗前 72 小时开始的研究中观察到的功能改善。这表明口服环孢素预处理可能是用同种异体 CDC 进行心脏修复所必需的。在三向盲法、随机设计中,我们确定了再灌注时给予同种异体 CDC 是否改善心肌功能,以及静脉内环孢素是否增强其疗效。与之前使用口服环孢素的研究相反,给予或不给予静脉内环孢素的 CDC 对功能或梗死面积均无影响。这表明,CDC 可能对治疗慢性 LV 功能障碍最有效,其中环孢素至少可以在细胞治疗前 72 小时开始。
