Systematic review and meta-analysis of cell therapy for COVID-19: global clinical trial landscape, published safety/efficacy outcomes, cell product manufacturing and clinical delivery

Couto, Pedro Silva; Al-Arawe, Nada; Filgueiras, Igor Salerno; Fonseca, Dennyson Leandro M.; Hinterseher, Irene; Catar, Rusan; Chinnadurai, Raghavan; Bersenev, Alexey; Cabral-Marques, Otávio; Moll, Guido; Verter, Frances

doi:10.3389/fimmu.2023.1200180

Cited by 13 publications

(5 citation statements)

References 140 publications

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“…Therapies focused on preventing secondary damage post injury and suppressing a dysregulated immune response will serve to improve patient outcomes. Although treating coagulopathic patients with pro-coagulant MSCs must be approached with caution ( 16 , 19 , 20 , 103 ), MSCs’ immunomodulation potential suggests that their use in any population such as trauma patients who are susceptible to a hyperactive immune response and coagulopathy ( 110 ) may be beneficial. It is hoped that these short-term assays will aid in developing, screening, and customizing cell therapy for the aid of the patient.…”

Section: Discussionmentioning

confidence: 99%

“…Their potential was also recently realized in several COVID therapies (12)(13)(14)(15). The most comprehensive and up-to-date summary on the use of MSCs for COVID19 was recently published by Couto et al in Frontiers Immunology 2023 (16).…”

Section: Background and Introductionmentioning

confidence: 99%

“…The most comprehensive and up-to-date summary on the use of MSCs for COVID19 was recently published by Couto et al. in Frontiers Immunology 2023 ( 16 ).…”

Section: Background and Introductionmentioning

confidence: 99%

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Short-term assays for mesenchymal stromal cell immunosuppression of T-lymphocytes

Herzig,

Christy,

Montgomery

et al. 2023

Front. Immunol.

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IntroductionTrauma patients are susceptible to coagulopathy and dysfunctional immune responses. Mesenchymal stromal cells (MSCs) are at the forefront of the cellular therapy revolution with profound immunomodulatory, regenerative, and therapeutic potential. Routine assays to assess immunomodulation activity examine MSC effects on proliferation of peripheral blood mononuclear cells (PBMCs) and take 3–7 days. Assays that could be done in a shorter period of time would be beneficial to allow more rapid comparison of different MSC donors. The studies presented here focused on assays for MSC suppression of mitogen-stimulated PBMC activation in time frames of 24 h or less.MethodsThree potential assays were examined—assays of apoptosis focusing on caspase activation, assays of phosphatidyl serine externalization (PS+) on PBMCs, and measurement of tumor necrosis factor alpha (TNFα) levels using rapid ELISA methods. All assays used the same initial experimental conditions: cryopreserved PBMCs from 8 to 10 pooled donors, co-culture with and without MSCs in 96-well plates, and PBMC stimulation with mitogen for 2–72 h.ResultsSuppression of caspase activity in activated PBMCs by incubation with MSCs was not robust and was only significant at times after 24 h. Monitoring PS+ of live CD3+ or live CD4+/CD3+ mitogen-activated PBMCs was dose dependent, reproducible, robust, and evident at the earliest time point taken, 2 h, although no increase in the percentage of PS+ cells was seen with time. The ability of MSC in co-culture to suppress PBMC PS+ externalization compared favorably to two concomitant assays for MSC co-culture suppression of PBMC proliferation, at 72 h by ATP assay, or at 96 h by fluorescently labeled protein signal dilution. TNFα release by mitogen-activated PBMCs was dose dependent, reproducible, robust, and evident at the earliest time point taken, with accumulating signal over time. However, suppression levels with MSC co-culture was reliably seen only after 24 h.DiscussionTakeaways from these studies are as follows: (1) while early measures of PBMC activation is evident at 2–6 h, immunosuppression was only reliably detected at 24 h; (2) PS externalization at 24 h is a surrogate assay for MSC immunomodulation; and (3) rapid ELISA assay detection of TNFα release by PBMCs is a robust and sensitive assay for MSC immunomodulation at 24 h.

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Section: Discussionmentioning

confidence: 99%

Section: Background and Introductionmentioning

confidence: 99%

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Short-term assays for mesenchymal stromal cell immunosuppression of T-lymphocytes

Herzig,

Christy,

Montgomery

et al. 2023

Front. Immunol.

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“…In addition to the clinical trials using UC-MSCs introduced in Tables 1 and 2 , there are accumulating early-phase clinical trials using UC-MSCs [ 17 , 20 , 23 , 33 – 35 ] for engraftment facilitation in HSCT for aplastic anemia [ 36 ], neurogenic injuries, diabetes mellitus (DM), heart and angioplasty, liver damage including liver cirrhosis, inflammatory bowel diseases such as Crohn’s disease and ulcerative colitis, prevention of acute rejection in renal transplantation, and collagen diseases [ 33 ]. The number of relevant clinical trials on the NIH clinical trial website ( https://00m.in/HHVJP ) has increased up to 95 trials, including complete, recruiting, and not-yet-recruiting status, as of the end of May 2023.…”

Section: Cb and Uc For Exploring New Cell Modalitiesmentioning

confidence: 99%

Umbilical cord blood and cord tissue banking as somatic stem cell resources to support medical cell modalities

Nagamura-Inoue,

Nagamura

2023

Inflamm Regener

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Human umbilical cord blood (CB) and umbilical cord tissue (UC) are attractive sources of somatic stem cells for gene and cell therapies. CB and UC can be obtained noninvasively from donors. CB, a known source of hematopoietic stem cells for transplantation, has attracted attention as a new source of immune cells, including universal chimeric antigen receptor-T cell therapy (CAR-T) and, more recently, universal CAR-natural killer cells. UC-derived mesenchymal stromal cells (UC-MSCs) have a higher proliferation potency than those derived from adult tissues and can be used anon-HLA restrictively. UC-MSCs meet the MSC criteria outlined by the International Society of Gene and Cellular Therapy. UC-MSCs are negative for HLA-DR, CD80, and CD86 and have an immunosuppressive ability that mitigates the proliferation of activated lymphocytes through secreting indoleamine 2,3-dioxygenase 1 and prostaglandin E2, and the expression of PD-L2 and PD-L1. We established the off-the-shelf cord blood/cord bank IMSUT CORD to support novel cell therapy modalities, including the CB-derived immune cells, MSCs, MSCs-derived extracellular vesicles, biological carriers loaded with chemotherapy drugs, prodrug, oncolytic viruses, nanoparticles, human artificial chromosome, combinational products with a scaffold, bio3D printing, and so on.

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“…After establishing the functional role of RABs directed against the angiotensin II type 1 receptor (AT1R) and endothelin receptor type A (ETAR) for vascular integrity and graft function/survival in the KTx setting ( 4 , 8 , 9 , 11 – 16 ), subsequent studies have identified several RABs directed against GPCR targets typically associated with the vasculature, such as protease-activated receptors (PARs), neuronal and chemokine receptors, and the levels of these RABs are often modulated with patient age and disease status ( 1 , 17 , 18 ). Vasculature-associated RAB targets can be found on different types of micro-/macro-vascular endothelial cells (ECs), vascular smooth muscle cells (VSCMs), and perivascular multipotent mesenchymal stromal/stem cells (MSCs), but also neuronal cells, which are all often employed as model systems to study respective molecular signaling mechanisms ( 1 , 19 , 20 ).…”

Section: Introductionmentioning

confidence: 99%

Autoantibodies from patients with kidney allograft vasculopathy stimulate a proinflammatory switch in endothelial cells and monocytes mediated via GPCR-directed PAR1-TNF-α signaling

Moll,

Luecht,

Gyamfi

et al. 2023

Front. Immunol.

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Non-HLA-directed regulatory autoantibodies (RABs) are known to target G-protein coupled receptors (GPCRs) and thereby contribute to kidney transplant vasculopathy and failure. However, the detailed underlying signaling mechanisms in human microvascular endothelial cells (HMECs) and immune cells need to be clarified in more detail. In this study, we compared the immune stimulatory effects and concomitant intracellular and extracellular signaling mechanisms of immunoglobulin G (IgG)-fractions from kidney transplant patients with allograft vasculopathy (KTx-IgG), to that from patients without vasculopathy, or matched healthy controls (Con-IgG). We found that KTx-IgG from patients with vasculopathy, but not KTx-IgG from patients without vasculopathy or Con-IgG, elicits HMEC activation and subsequent upregulation and secretion of tumor necrosis factor alpha (TNF-α) from HMECs, which was amplified in the presence of the protease-activated thrombin receptor 1 (PAR1) activator thrombin, but could be omitted by selectively blocking the PAR1 receptor. The amount and activity of the TNF-α secreted by HMECs stimulated with KTx-IgG from patients with vasculopathy was sufficient to induce subsequent THP-1 monocytic cell activation. Furthermore, AP-1/c-FOS, was identified as crucial transcription factor complex controlling the KTx-IgG-induced endothelial TNF-α synthesis, and mircoRNA-let-7f-5p as a regulatory element in modulating the underlying signaling cascade. In conclusion, exposure of HMECs to KTx-IgG from patients with allograft vasculopathy, but not KTx-IgG from patients without vasculopathy or healthy Con-IgG, triggers signaling through the PAR1-AP-1/c-FOS-miRNA-let7-axis, to control TNF-α gene transcription and TNF-α-induced monocyte activation. These observations offer a greater mechanistic understanding of endothelial cells and subsequent immune cell activation in the clinical setting of transplant vasculopathy that can eventually lead to transplant failure, irrespective of alloantigen-directed responses.

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Systematic review and meta-analysis of cell therapy for COVID-19: global clinical trial landscape, published safety/efficacy outcomes, cell product manufacturing and clinical delivery

Cited by 13 publications

References 140 publications

Short-term assays for mesenchymal stromal cell immunosuppression of T-lymphocytes

Short-term assays for mesenchymal stromal cell immunosuppression of T-lymphocytes

Umbilical cord blood and cord tissue banking as somatic stem cell resources to support medical cell modalities

Autoantibodies from patients with kidney allograft vasculopathy stimulate a proinflammatory switch in endothelial cells and monocytes mediated via GPCR-directed PAR1-TNF-α signaling

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