用于治疗慢性肢体缺血的胎儿祖细胞。
Fetal progenitor cells for treatment of chronic limb ischemia.
作者信息
Kukharchuk Oleksandr, Bopardikar Abhijit, Anand Baskaran Padma Priya, Kukharchuk Andrii, Kulkarni Rohit, Ranbhor Ranjit
机构信息
ReeLabs Pvt. Ltd. 1st Floor, KK Chambers, Sir P.T. Rd., Azad Maidan, Fort, Mumbai 400001, India.
ReeLabs Inc. 16192 Coastal Hwy, Lewes, DE 19958, USA.
出版信息
Am J Stem Cells. 2024 Jun 15;13(3):169-190. doi: 10.62347/MZKI8393. eCollection 2024.
OBJECTIVES
This study investigated the therapeutic potential of fetal progenitor cells (FPCs) in the treatment of chronic non-healing wounds and ulcers associated with chronic limb ischemia (CLI). The research aimed to elucidate the mechanism of action of FPCs and evaluate their efficacy and safety in CLI patients.
METHODS
The researchers isolated FPCs from aborted human fetal liver, brain, and skin tissues and thoroughly characterized them. The preclinical phase of the study involved assessing the effects of FPCs in a rat model of CLI. Subsequently, a randomized controlled clinical trial was conducted to compare the efficacy of FPCs with standard treatment and autologous bone marrow mononuclear cells in CLI patients. The clinical trial lasted 12 months, with a follow-up period of 24-36 months. The primary outcomes included wound healing, frequency of major and minor amputations, pain reduction, and the incidence of complications. Secondary outcomes involved changes in local hemodynamics and histological, ultrastructural, and immunohistochemical assessments of angiogenesis.
RESULTS
In the animal model, FPC treatment significantly enhanced angiogenesis and accelerated healing of ischemic wounds compared to controls. The clinical trial in CLI patients demonstrated that the FPC therapy achieved substantially higher rates of complete wound closure, prevention of major amputation, pain reduction, and improvement in ankle-brachial index compared to control groups. Notably, the study reported no serious adverse events.
CONCLUSIONS
FPC therapy exhibited remarkable efficacy in promoting the healing of ischemic wounds, preventing amputation, and improving symptoms and quality of life in patients with CLI. The proangiogenic and provasculogenic effects of FPCs may be attributed to their ability to secrete specific growth factors. These findings provide new insights into the development of cellular therapeutic angiogenesis as a promising approach for the treatment of peripheral arterial diseases.
目的
本研究调查了胎儿祖细胞(FPCs)在治疗与慢性肢体缺血(CLI)相关的慢性不愈合伤口和溃疡方面的治疗潜力。该研究旨在阐明FPCs的作用机制,并评估其在CLI患者中的疗效和安全性。
方法
研究人员从流产的人类胎儿肝脏、大脑和皮肤组织中分离出FPCs,并对其进行了全面表征。该研究的临床前阶段涉及评估FPCs在CLI大鼠模型中的作用。随后,进行了一项随机对照临床试验,以比较FPCs与标准治疗以及自体骨髓单个核细胞在CLI患者中的疗效。该临床试验持续了12个月,随访期为24至36个月。主要结局包括伤口愈合、大截肢和小截肢的频率、疼痛减轻以及并发症的发生率。次要结局涉及局部血流动力学的变化以及血管生成的组织学、超微结构和免疫组织化学评估。
结果
在动物模型中,与对照组相比,FPC治疗显著增强了血管生成并加速了缺血性伤口的愈合。CLI患者的临床试验表明,与对照组相比,FPC治疗在实现完全伤口闭合、预防大截肢、减轻疼痛以及改善踝肱指数方面的比率要高得多。值得注意的是,该研究报告没有严重不良事件。
结论
FPC治疗在促进缺血性伤口愈合、预防截肢以及改善CLI患者的症状和生活质量方面显示出显著疗效。FPCs的促血管生成和血管新生作用可能归因于它们分泌特定生长因子的能力。这些发现为细胞治疗性血管生成的发展提供了新的见解,这是一种治疗外周动脉疾病的有前景的方法。
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