Engineering Strategies for Allogeneic Solid Tissue Acceptance

Sousa, Ana Rita; Mano, J. F.; Oliveira, Mariana B.

doi:10.1016/j.molmed.2021.03.005

Cited by 6 publications

(8 citation statements)

References 107 publications

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“…For GVHD, full hematopoietic chimerism has been suggested amongst different strategies for the recipient's response to allograft acceptance. In contrast, tolerogenic leukocytes, apoptotic donor leukocytes, mesenchymal stem cells, costimulation blockade, and immunization have shown no or minimal risk 66 …”

Section: Some Strategies To Achieve Allograft Acceptancementioning

confidence: 99%

“…However, because mixed chimerism caused tolerance to human kidney allografts but not to pancreatic islet, lung, or heart allografts, the efficacy of chimerism in avoiding allograft rejection appears to be tissue‐type dependent 71 . Despite lowering the risk of GVHD and retaining immunological competence, permanent mixed chimeras appear only to prevent rejection in HLA‐matched allograft recipients, and the efficiency of transitory mixed chimeras in inducing tolerance varies across recipients 66 . Similar to chimerism, tolerogenic leukocyte research focuses on kidney and liver transplants.…”

Section: Some Strategies To Achieve Allograft Acceptancementioning

confidence: 99%

“…In contrast, tolerogenic leukocytes, apoptotic donor leukocytes, mesenchymal stem cells, costimulation blockade, and immunization have shown no or minimal risk. 66 Cell therapy is becoming increasingly popular as an alternative to conventional drug therapy for treating allograft rejection. 67,68 Hematopoietic chimerism is one of the most effective methods for inducing tolerance to donor-derived tissue and organ grafts without using immunosuppressive drugs; here, the host's bone marrow is completely replaced by a donor bone marrow to create a full chimera.…”

Section: Some Strategies To Achieve Allograft Acceptancementioning

confidence: 99%

“…71 Despite lowering the risk of GVHD and retaining immunological competence, permanent mixed chimeras appear only to prevent rejection in HLA-matched allograft recipients, and the efficiency of transitory mixed chimeras in inducing tolerance varies across recipients. 66 Similar to chimerism, tolerogenic leukocyte research focuses on kidney and liver transplants. Although autologous cell sources are favored, their suppressive capacity varies.…”

Section: Some Strategies To Achieve Allograft Acceptancementioning

confidence: 99%

See 3 more Smart Citations

The role of efferocytosis and transplant rejection: Strategies in promoting transplantation tolerance using apoptotic cell therapy and/or synthetic particles

Vafadar,

Vosough,

Jahromi

et al. 2023

Cell Biochemistry & Function

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Recently, efforts have been made to recognize the precise reason(s) for transplant failure and the process of rejection utilizing the molecular signature. Most transplant recipients do not appreciate the unknown length of survival of allogeneic grafts with the existing standard of care. Two noteworthy immunological pathways occur during allogeneic transplant rejection. A nonspecific innate immune response predominates in the early stages of the immune reaction, and allogeneic antigens initiate a donor‐specific adaptive reaction. Though the adaptive response is the major cause of allograft rejection, earlier pro‐inflammatory responses that are part of the innate immune response are also regarded as significant in graft loss. The onset of the innate and adaptive immune response causes chronic and acute transplant rejection. Currently employed immunosuppressive medications have shown little or no influence on chronic rejection and, as a result, on overall long‐term transplant survival. Furthermore, long‐term pharmaceutical immunosuppression is associated with side effects, toxicity, and an increased risk of developing diseases, both infectious and metabolic. As a result, there is a need for the development of innovative donor‐specific immunosuppressive medications to regulate the allorecognition pathways that induce graft loss and to reduce the side effects of immunosuppression. Efferocytosis is an immunomodulatory mechanism with fast and efficient clearance of apoptotic cells (ACs). As such, AC therapy strategies have been suggested to limit transplant‐related sequelae. Efferocytosis‐based medicines/treatments can also decrease the use of immunosuppressive drugs and have no detrimental side effects. Thus, this review aims to investigate the impact of efferocytosis on transplant rejection/tolerance and identify approaches using AC clearance to increase transplant viability.

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Section: Some Strategies To Achieve Allograft Acceptancementioning

confidence: 99%

Section: Some Strategies To Achieve Allograft Acceptancementioning

confidence: 99%

Section: Some Strategies To Achieve Allograft Acceptancementioning

confidence: 99%

Section: Some Strategies To Achieve Allograft Acceptancementioning

confidence: 99%

See 2 more Smart Citations

The role of efferocytosis and transplant rejection: Strategies in promoting transplantation tolerance using apoptotic cell therapy and/or synthetic particles

Vafadar,

Vosough,

Jahromi

et al. 2023

Cell Biochemistry & Function

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show abstract

“…Although survival rates have improved due to optimized surgical methods, advanced organ acquisition, and medical therapy, immune rejection is still the main cause of organ transplantation failure. [1,2] Immunosuppressive drugs currently used clinically are mainly targeted adaptive immunity T cells, including the classic "Calcineurin-NFAT" T cell activation pathway and the mTOR metabolic pathway related to T cell growth and proliferation. [3,4] The long-term use of these drugs, however, can cause serious liver and kidney toxicity and even trigger leukemia.…”

Section: Introductionmentioning

confidence: 99%

Dual‐Targeting Nanovesicles Carrying CSF1/CD47 Identified from Single‐Cell Transcriptomics of Innate Immune Cells in Heart Transplant for Alleviating Acute Rejection

Xu,

Mao,

et al. 2023

Adv Healthcare Materials

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Although immunosuppressive drugs for targeting T cells are the standard of care in acute transplantation rejection, the role of innate immune cells should not be ignored. Here, we performed single‐cell RNA sequencing (scRNA‐seq) and flow cytometry to reveal the dynamic changes of innate immune cells within the acute rejection time and found a significantly‐increased presence of Ly6G−Ly6C+ inflammatory macrophages and decreased presence of neutrophils among all types of immune cells. Next, to further explore potential targets regulating Ly6G−Ly6C+ inflammatory macrophages, scRNA‐seq was used to analyze the reciprocal signaling of both neutrophils and macrophages, along with the surface genes of macrophages. We found that activating CSF1/CSF1R and CD47/SIRPα signaling may serve as a strategy to relieve Ly6G−Ly6C+ inflammatory macrophage‐mediated early graft rejection. To investigate this hypothesis, CSF1/CD47 dual‐targeting nanovesicles (NVs) derived from IFN‐γ‐stimulated iPSC‐MSCs were designed and constructed. We confirmed that CSF1/CD47 NVs synergistically induced the differentiation of Ly6G−Ly6C− M2 inhibitory macrophages by the CSF1/CSF1R pathway, and inhibited the phagocytosis of inflammatory macrophages and inflammatory response by the CD47/SIRPα pathway, ultimately relieving immune rejection. Our study highlights the power of dual‐targeting CSF1/CD47 NVs as an immunosuppressant against early innate immune responses with the potential for broad clinical applications.This article is protected by copyright. All rights reserved

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Encapsulated Mesenchymal Stromal Cells as Cyclic Providers of Immunomodulatory Secretomes: A Living on‐Demand Delivery System

Sousa,

Gonçalves,

Neves

et al. 2024

Adv Healthcare Materials

Self Cite

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The stimulation of mesenchymal stromal cells (MSCs) with inflammatory molecules is often employed to boost their therapeutic effect. Prolonged exposure to inflammatory molecules has been explored to improve their action since MSCs therapies seem to be improved transiently with such stimuli. However, the possibility of cyclically stimulating MSCs to recover their optimized therapeutic potential is still to be elucidated, although the efficacy of cell‐based therapies may be dependent on the ability to readapt to the relapse pathological conditions. Here, we report the response of MSCs, encapsulated in alginate hydrogels and cultured for 22 days, using three different regimes: single, continuous, and intermittent stimulation with IFNγ. Exposure to IFNγ led to a decrease in the secretion of IL‐10, which was cyclically countered by IFNγ weaning. Conditioned media collected at different stages of pulsatile stimulation showed an immunomodulatory potential towards macrophages, which directly correlated with IL‐10 concentration in media. To understand whether the correlation between cyclic stimulation of MSCs and other biological actions could be observed, the effect on endothelial cells was studied, showcasing an overall modest influence on tube formation. Overall, our results describe the response of encapsulated MSCs to unusual pulsatile simulation regimens, exploring encapsulated MSCs as a living on‐demand release systems of tailored secretomes with recoverable immunomodulatory action.This article is protected by copyright. All rights reserved

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Engineering Strategies for Allogeneic Solid Tissue Acceptance

Cited by 6 publications

References 107 publications

The role of efferocytosis and transplant rejection: Strategies in promoting transplantation tolerance using apoptotic cell therapy and/or synthetic particles

The role of efferocytosis and transplant rejection: Strategies in promoting transplantation tolerance using apoptotic cell therapy and/or synthetic particles

Dual‐Targeting Nanovesicles Carrying CSF1/CD47 Identified from Single‐Cell Transcriptomics of Innate Immune Cells in Heart Transplant for Alleviating Acute Rejection

Encapsulated Mesenchymal Stromal Cells as Cyclic Providers of Immunomodulatory Secretomes: A Living on‐Demand Delivery System

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