MSC Transplantation in Eight Severe COVID-19 Patients: Can Cytokine Storm Be Reversed?

N. Erçelen, B. Bilgili, B. Monteleone, F. Gül, G. Gulay, Nagihan Alpaydin, Ozan Demir, Murat Şimşek, D. Turan, Omer Karadeniz, Elif Karadeniz, Nagihan Batıgun, I. Cinel
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引用次数: 6

Abstract

The COVID-19 disease is a global pandemic, with the first case diagnosed in December 2019, as reported by World Health Organization (WHO). In 17% of patients, COVID-19 causes severe Acute Respiratory Distress Syndrome (ARDS) due to release of large amounts of pro-inflammatory cytokines and chemokines in the lungs. In a retrospective observational study from Milan, 9% of the people, who tested positive for COVID-19, needed ICU care with respiratory support. The demand for ICU beds and health care personnel brought significant overload to sustain the care of these patients. Search for effective therapies is underway. However, the result of severe infection of COVID-19 still leads to the inevitable fatalities with the current available therapies. Mesenchymal Stem Cells (MSCs) have been isolated about 30 years ago (Supplementary Data 1). There are over 5,000 articles published on MSCs. Moreover, anti-inflammatory and immunemodulatory properties of MSCs have been well studied. Exogenously administered MSCs are medicinal. They generate positive therapeutic outcomes by secreting bioactive factors that exhibit immunomodulatory, and regenerative effects by fabricating, and secreting antibiotic proteins, where they hone in on sites of injury or disease. Hence, Arnold Caplan has proposed recently to change the name of MSCs to Medicinal Signaling Cells. As MSCs arise from pericytes, they can be isolated from a variety of vascularized tissues. Each separate tissue-specific stem cell interacts with its underlying vascular endothelial cells, and adjacent specific pericyte/MSC “Universal Stem Cell Niche” (pMSCs). Each specific pMSCs have both pMSCs common, and unique chemical, and functional features. Meanwhile, the major therapeutic role of pMSCs in vivo at various sites of disease or injury are very similar when comparing these different pMSCs. Over the past decade, the emphasis has shifted toward harnessing the pMSCs’ ability to produce factors and cytokines that stimulate innate tissue repair, modulate inflammation, and immune responses. MSCs express function on Toll-Like Receptors (TLRs). Triggering different TLRs, depending on exposure times promote either pro- or anti-inflammatory function in MSCs. Pre-clinical studies demonstrated that the majority of infused MSCs initially distributed in the lungs. Subsequent studies showed improved pulmonary functions beginning shortly after administration with no evidence of pulmonary safety risk. These studies indicated the local beneficial MSCs-mediated effect on pulmonary airways . A recent pilot study from China explored the therapeutic outcomes of MSC transplantation in seven poor prognoses COVID-19 patients with pneumonia. The results revealed that MSC transplantation was safe and effective treatment option. The peripheral lymphocytes increased after the treatment, and the overactivated cytokine-secreting immune cells disappeared in 3-6 days. A group of regulatory DC cell population dramatically increased. Meanwhile, the level of TNF-α is significantly decreased, while IL-10 increased in the MSC transplantation group compared to the placebo control group. Furthermore, the gene expression profile showed MSCs were ACE2- and TMPRSS2-, which indicated MSCs were free from COVID-19 infection . Here we report our clinical observations of eight cases, before and after MSC transplantation, to assess the clinical therapeutic effects of MSC transplantation on COVID-19 severe/critically severe patients. Though broader studies are needed, we advised a clinical application protocol and algorithm by evaluating the poor prognostic markers significantly related by MSC transplantation to prevent the overload in ICU clinics, as well as, to shorten hospitalization time.
8例重症COVID-19患者的MSC移植:细胞因子风暴可以逆转吗?
据世界卫生组织(世卫组织)报告,2019年12月确诊的第一例COVID-19疾病是一种全球大流行。在17%的患者中,由于肺部释放大量促炎细胞因子和趋化因子,COVID-19会导致严重急性呼吸窘迫综合征(ARDS)。在米兰的一项回顾性观察研究中,9%的COVID-19检测呈阳性的人需要ICU护理和呼吸支持。对ICU床位和医护人员的需求带来了严重的超负荷,以维持对这些患者的护理。目前正在寻找有效的治疗方法。然而,在现有的治疗方法下,COVID-19严重感染的结果仍不可避免地导致死亡。间充质干细胞(Mesenchymal Stem Cells, MSCs)大约在30年前被分离出来(补充数据1)。关于MSCs的文章已经发表了5000多篇。此外,MSCs的抗炎和免疫调节特性也得到了很好的研究。外源性给药的间充质干细胞是药用的。它们通过分泌具有免疫调节和再生作用的生物活性因子产生积极的治疗效果,并通过制造和分泌抗生素蛋白,在损伤或疾病的部位聚集。因此,Arnold Caplan最近提出将MSCs更名为Medicinal Signaling Cells。由于间充质干细胞起源于周细胞,它们可以从多种血管化组织中分离出来。每个单独的组织特异性干细胞与其潜在的血管内皮细胞和邻近的特定周细胞/MSC“通用干细胞生态位”(pMSCs)相互作用。每种特定的pMSCs都具有pMSCs共同的、独特的化学和功能特征。同时,在比较这些不同的pMSCs时,pMSCs在体内疾病或损伤的各个部位的主要治疗作用非常相似。在过去的十年中,重点已经转移到利用pMSCs产生刺激先天组织修复、调节炎症和免疫反应的因子和细胞因子的能力。MSCs表达toll样受体(TLRs)的功能。根据暴露时间触发不同的tlr,可促进MSCs的促炎或抗炎功能。临床前研究表明,大多数注入的MSCs最初分布在肺部。随后的研究表明,在给药后不久,肺功能开始改善,没有肺安全风险的证据。这些研究表明,局部有益的间充质干细胞介导的作用对肺气道。中国最近的一项试点研究探讨了7例预后不良的COVID-19肺炎患者的MSC移植治疗结果。结果表明,骨髓间充质干细胞移植是一种安全有效的治疗方案。治疗后外周血淋巴细胞增多,过度活化的分泌细胞因子的免疫细胞在3 ~ 6 d内消失。一组调节性DC细胞数量显著增加。同时,与安慰剂对照组相比,MSC移植组TNF-α水平明显降低,IL-10水平升高。此外,基因表达谱显示MSCs为ACE2-和TMPRSS2-,表明MSCs不受COVID-19感染。在此,我们报告了8例MSC移植前后的临床观察,以评估MSC移植对COVID-19重型/危重型患者的临床治疗效果。虽然需要更广泛的研究,但我们通过评估与间充质干细胞移植显著相关的不良预后指标,建议临床应用方案和算法,以防止ICU诊所超载,缩短住院时间。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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