Amniotic Membrane Mesenchymal Cells-Derived Factors Skew T Cell Polarization Toward Treg and Downregulate Th1 and Th17 Cells Subsets

Pianta, Stefano; Signoroni, Patrizia Bonassi; Muradore, Ivan; Rodrigues, Melissa Francis; Rossi, Daniele; Silini, Antonietta; Parolini, Ornella

doi:10.1007/s12015-014-9558-4

Cited by 117 publications

(105 citation statements)

References 68 publications

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“…Also, MSCs induce trimethylation at promoter of Foxp3 resulting to suppress of ROR-C trimethylation through IL-10 production. These evidence lead to decrease T H 17 as well as increase of Treg frequencies [26]. Enhanced immune suppressive effects of IFN-γ treated MSCs are partially associated to induce of IDO and PGE2 production in MSCs by IFN-γ.…”

Section: Discussionmentioning

confidence: 94%

TNF-α modulates the immunosuppressive effects of MSCs on dendritic cells and T cells

Mohammadpour

Pourfathollah

Zarif

et al. 2015

International Immunopharmacology

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Section: Discussionmentioning

confidence: 94%

TNF-α modulates the immunosuppressive effects of MSCs on dendritic cells and T cells

Mohammadpour

Pourfathollah

Zarif

et al. 2015

International Immunopharmacology

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“…Human AECs exert immunomodulatory effects on lymphocytes by fostering the Th2 anti-inflammatory phenotype over Th1, both by acting directing with lymphocytes and through the conditioned medium, which contains secreted factors [36]. Amniotic cells dose-dependently inhibit the proliferation of activated peripheral blood mononuclear cells (PBMCs) [10, 19], but only few studies have focused on the effects of AECs on macrophages [37, 38, 39].…”

Section: Discussionmentioning

confidence: 99%

Conditioned medium derived from rat amniotic epithelial cells confers protection against inflammation, cancer, and senescence

et al. 2016

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Amniotic epithelial cells (AECs) are a class of fetal stem cells that derives from the epiblast and resides in the amnion until birth. AECs are suitable candidates for regenerative medicine because of the ease of collection, their low immunogenicity and inability to form tumors after transplantation. Even though human AECs have been widely investigated, the fact remains that very little is known about AECs isolated from rat, one of the most common animal models in medical testing. In this study, we showed that rat AECs retained stemness properties and plasticity, expressed the pluripotency markers Sox2, Nanog, and Oct4 and were able to differentiate toward the osteogenic lineage. The addition of conditioned medium collected from rat AECs to lipopolysaccharide-activated macrophages elicited anti-inflammatory properties through a decrease of Tnfa expression and slowed tumor cell proliferation in vitro and in vivo. The senescence-associated secretory phenotype was also significantly lower upon incubation of senescent human IMR-90 fibroblast cells with conditioned medium from rat AECs. These results confirm the potential of AECs in the modulation of inflammatory mechanisms and open new therapeutic possibilities for regenerative medicine and anti-aging therapies as well.

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“…Abundant information has been published on the relationship between MSC 2 and resolution of the inflammatory setting, and tissue protection and repair[24-34]. Some of the well-known anti-inflammatory effects mediated by MSC 2 are skewing macrophages to the M2 immunosuppressive alternative phenotype[35-41], promoting T cells to T regulatory (T reg ) cell differentiation[42-48], skewing monocyte-derived dendritic cells to a regulatory phenotype[49-54], inhibiting neutrophil influx and respiratory burst while maintaining or even increasing its phagocytic capacity[55-59], inhibiting mast cell degranulation[60-62], and inhibiting pro-inflammatory activities of T cells[63-72], natural killer (NK) cells[73-79] and B cells[80-84]. Furthermore, throughout the numerous reports describing the regulatory role of MSCs attenuating (at some point) inflammation, several intercellular molecular signals have consistently emerged as relevant.…”

Section: Mscs and Immunomodulationmentioning

confidence: 99%

Immunomodulatory oligonucleotide IMT504: Effects on mesenchymal stem cells as a first-in-class immunoprotective/immunoregenerative therapy

Zorzopulos¹,

Opal²,

Hernando-Insúa³

et al. 2017

WJSC

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The immune responses of humans and animals to insults (i.e., infections, traumas, tumoral transformation and radiation) are based on an intricate network of cells and chemical messengers. Abnormally high inflammation immediately after insult or abnormally prolonged pro-inflammatory stimuli bringing about chronic inflammation can lead to life-threatening or severely debilitating diseases. Mesenchymal stem cell (MSC) transplant has proved to be an effective therapy in preclinical studies which evaluated a vast diversity of inflammatory conditions. MSCs lead to resolution of inflammation, preparation for regeneration and actual regeneration, and then ultimate return to normal baseline or homeostasis. However, in clinical trials of transplanted MSCs, the expectations of great medical benefit have not yet been fulfilled. As a practical alternative to MSC transplant, a synthetic drug with the capacity to boost endogenous MSC expansion and/or activation may also be effective. Regarding this, IMT504, the prototype of a major class of immunomodulatory oligonucleotides, induces in vivo expansion of MSCs, resulting in a marked improvement in preclinical models of neuropathic pain, osteoporosis, diabetes and sepsis. IMT504 is easily manufactured and has an excellent preclinical safety record. In the small number of patients studied thus far, IMT504 has been well-tolerated, even at very high dosage. Further clinical investigation is necessary to demonstrate the utility of IMT504 for resolution of inflammation and regeneration in a broad array of human diseases that would likely benefit from an immunoprotective/immunoregenerative therapy.

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Amniotic Membrane Mesenchymal Cells-Derived Factors Skew T Cell Polarization Toward Treg and Downregulate Th1 and Th17 Cells Subsets

Cited by 117 publications

References 68 publications

TNF-α modulates the immunosuppressive effects of MSCs on dendritic cells and T cells

TNF-α modulates the immunosuppressive effects of MSCs on dendritic cells and T cells

Conditioned medium derived from rat amniotic epithelial cells confers protection against inflammation, cancer, and senescence

Immunomodulatory oligonucleotide IMT504: Effects on mesenchymal stem cells as a first-in-class immunoprotective/immunoregenerative therapy

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