Liver Ischemia and Reperfusion Induce Periportal Expression of Necroptosis Executor pMLKL Which Is Associated With Early Allograft Dysfunction After Transplantation

Shi, Shaojun; Bonaccorsi‐Riani, Eliano; Schurink, Ivo J.; Bosch, Thierry van den; Doukas, Michael; Lila, Karishma A.; Roest, Henk P.; Xhema, Daela; Gianello, Pierre; Jonge, Jeroen de; Verstegen, Monique M.A.; Laan, Luc J. W. van der

doi:10.3389/fimmu.2022.890353

Cited by 5 publications

(6 citation statements)

References 53 publications

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“…Both apoptosis and necrosis were observed in hepatocytes after IR [ 25 ]. IR induces periportal expression of MLKL in human liver grafts, and is associated with early allograft dysfunction after transplantation [ 26 ]. Ferroptosis is induced by iron overload during liver IR injury [ 27 ].…”

Section: Discussionmentioning

confidence: 99%

Defective efferocytosis by aged macrophages promotes STING signaling mediated inflammatory liver injury

Cheng

et al. 2023

Cell Death Discov.

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Aged livers have shown aggravated liver ischemia and reperfusion (IR) injury. Timely efferocytosis of apoptotic cells is a key mechanism for avoiding excessive inflammation and tissue injury. Here, we investigated the alteration of efferocytosis by aged macrophages and its role in regulating macrophage STING (stimulator of interferon genes) signaling and liver IR injury. Aged and young mice were subjected to liver partial IR model. Liver injury and inflammation were measured. Efferocytosis by aged macrophages and the underlying regulatory mechanism were analyzed as well. Aged macrophages exhibited impaired efferocytosis with decreased MerTK (c-mer proto-oncogene tyrosine kinase) activation, which was reversed by treatment of the MerTK CRISPR activation plasmid. Increased MerTK cleavage by ADAM17 (a disintegrin and metalloproteinase 17) due to enhanced ROS (reactive oxygen species) levels contributed to defective efferocytosis by aged macrophages. MerTK activation by suppressing ADAM17 or ROS improved aged macrophage efferocytosis, leading to reduced inflammatory liver injury. Moreover, increased apoptotic hepatocytes, DNA accumulation, and macrophage STING activation were observed in aged ischemic livers. Improvement in efferocytosis by aged macrophages via MerTK activation suppressed STING activation and inflammatory liver injury. Our study demonstrates that aging suppresses MerTK- mediated macrophage efferocytosis to promote macrophage STING activation and inflammatory liver IR injury, suggesting a new mechanism and potential therapy to promote inflammation resolution and efferocytosis in aged livers.

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Section: Discussionmentioning

confidence: 99%

Defective efferocytosis by aged macrophages promotes STING signaling mediated inflammatory liver injury

Cheng

et al. 2023

Cell Death Discov.

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“…Almost all of these studies are based on cell culture and animal models. There are only two human organ studies, one in the lung [ 40 ] and another in the liver [ 35 ]. More clinical research should be conducted to determine the significance of necroptosis in human organ transplants.…”

Section: Discussionmentioning

confidence: 99%

“…Human liver grafts with a high pMLKL index had significantly elevated serum levels of aminotransferases and lactate dehydrogenase 24 h after transplantation, signifying lytic cell death. Thus, the pMLKL index can serve as a reliable prognostic tool for the progression of EAD [ 35 ].…”

Section: Necroptosis In Solid Organ Transplantationmentioning

confidence: 99%

Necroptosis in Organ Transplantation: Mechanisms and Potential Therapeutic Targets

Zhao,

Main,

Aujla

et al. 2023

Cells

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Organ transplantation remains the only treatment option for patients with end-stage organ dysfunction. However, there are numerous limitations that challenge its clinical application, including the shortage of organ donations, the quality of donated organs, injury during organ preservation and reperfusion, primary and chronic graft dysfunction, acute and chronic rejection, infection, and carcinogenesis in post-transplantation patients. Acute and chronic inflammation and cell death are two major underlying mechanisms for graft injury. Necroptosis is a type of programmed cell death involved in many diseases and has been studied in the setting of all major solid organ transplants, including the kidney, heart, liver, and lung. It is determined by the underlying donor organ conditions (e.g., age, alcohol consumption, fatty liver, hemorrhage shock, donation after circulatory death, etc.), preservation conditions and reperfusion, and allograft rejection. The specific molecular mechanisms of necroptosis have been uncovered in the organ transplantation setting, and potential targeting drugs have been identified. We hope this review article will promote more clinical research to determine the role of necroptosis and other types of programmed cell death in solid organ transplantation to alleviate the clinical burden of ischemia–reperfusion injury and graft rejection.

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“…Overall evidence suggests that necroptosis plays a relevant role as a form of lytic cell death in the IRI model, although some studies do not attribute any effects to necroptosis [ 208 , 209 ]. A recent study revealed the presence of activated MLKL in human liver grafts before and after reperfusion [ 210 ]. Interestingly, patients experiencing early allograft dysfunction show a significant increase in MLKL activation, which correlates with serum liver enzyme levels.…”

Section: Cell Death In Liver Diseasementioning

confidence: 99%

Cell Death in Liver Disease and Liver Surgery

Stoess,

Choi,

Onyuru

et al. 2024

Biomedicines

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Cell death is crucial for maintaining tissue balance and responding to diseases. However, under pathological conditions, the surge in dying cells results in an overwhelming presence of cell debris and the release of danger signals. In the liver, this gives rise to hepatic inflammation and hepatocellular cell death, which are key factors in various liver diseases caused by viruses, toxins, metabolic issues, or autoimmune factors. Both clinical and in vivo studies strongly affirm that hepatocyte death serves as a catalyst in the progression of liver disease. This advancement is characterized by successive stages of inflammation, fibrosis, and cirrhosis, culminating in a higher risk of tumor development. In this review, we explore pivotal forms of cell death, including apoptosis, pyroptosis, and necroptosis, examining their roles in both acute and chronic liver conditions, including liver cancer. Furthermore, we discuss the significance of cell death in liver surgery and ischemia-reperfusion injury. Our objective is to illuminate the molecular mechanisms governing cell death in liver diseases, as this understanding is crucial for identifying therapeutic opportunities aimed at modulating cell death pathways.

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Liver Ischemia and Reperfusion Induce Periportal Expression of Necroptosis Executor pMLKL Which Is Associated With Early Allograft Dysfunction After Transplantation

Cited by 5 publications

References 53 publications

Defective efferocytosis by aged macrophages promotes STING signaling mediated inflammatory liver injury

Defective efferocytosis by aged macrophages promotes STING signaling mediated inflammatory liver injury

Necroptosis in Organ Transplantation: Mechanisms and Potential Therapeutic Targets

Cell Death in Liver Disease and Liver Surgery

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