Iron overload promotes mitochondrial fragmentation in mesenchymal stromal cells from myelodysplastic syndrome patients through activation of the AMPK/MFF/Drp1 pathway

Zheng, Qingqing; Zhao, Yuwu; Guo, Juan; Zhao, Sida; Fei, Chengming; Xiao, Chao; Wu, Dong; Wu, Lingyun; Chang, Chunkang

doi:10.1038/s41419-018-0552-7

Cited by 88 publications

(70 citation statements)

References 52 publications

(57 reference statements)

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“…reported that iron overload damages MSC through AMPK/MFF/Drp1 pathway in MDS. 27 Thus, further research should investigate the effect of iron overload on the BM microenvironment in MDS.…”

Section: Discussionmentioning

confidence: 99%

Iron overload impairs normal hematopoietic stem and progenitor cells through reactive oxygen species and shortens survival in myelodysplastic syndrome mice

Jin

Cao

et al. 2018

Haematologica

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There is increasing clinical evidence to suggest a suppressive effect on hematopoiesis in myelodysplastic syndrome patients with iron overload. However, how iron overload influences hematopoiesis in myelodysplastic syndrome (MDS) remains unknown. Here, the RUNX1S291fs-transduced bone marrow mononuclear cells were yielded and transplanted into lethally irradiated recipient mice together with radioprotective bone marrow cells to generate MDS mice. Eight weeks post transplantation, the recipient mice received an intraperitoneal injection of 0.2 mL iron dextran at a concentration of 25 mg/mL once every other day for a total of 8 times to establish an iron overload model. In the present study, we show that iron overload impairs the frequency and colony-forming capacity of normal hematopoietic stem and progenitor cells, especially in erythroid, in MDS mice, which is due, at least in part, to growth differentiation factor 11-induced reactive oxygen species, shortening survival of MDS mice. Given that we are the first to construct an iron overload model in MDS mice, we hope this model will be helpful for further exploring the influence and mechanism of iron overload on MDS.

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“…reported that iron overload damages MSC through AMPK/MFF/Drp1 pathway in MDS. 27 Thus, further research should investigate the effect of iron overload on the BM microenvironment in MDS.…”

Section: Discussionmentioning

confidence: 99%

Iron overload impairs normal hematopoietic stem and progenitor cells through reactive oxygen species and shortens survival in myelodysplastic syndrome mice

Jin

Cao

et al. 2018

Haematologica

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“…Drp1 is activated and causes the fragmentation of mitochondria in neuronal cells ( 95 ). This is linked to iron overload, AMPK activation, MFF ( 96 ), and ubiquitination of A-kinase anchor protein 121 ( 97 ). Conversely, ROS induced mitophagy is suppressed by depleting Drp1 ( 98 ).…”

Section: Mitochondrial Dynamics Plays a Key Role In Immune Cell Metabmentioning

confidence: 99%

Diverse Roles of Mitochondria in Immune Responses: Novel Insights Into Immuno-Metabolism

et al. 2018

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Lack of immune system cells or impairment in differentiation of immune cells is the basis for many chronic diseases. Metabolic changes could be the root cause for this immune cell impairment. These changes could be a result of altered transcription, cytokine production from surrounding cells, and changes in metabolic pathways. Immunity and mitochondria are interlinked with each other. An important feature of mitochondria is it can regulate activation, differentiation, and survival of immune cells. In addition, it can also release signals such as mitochondrial DNA (mtDNA) and mitochondrial ROS (mtROS) to regulate transcription of immune cells. From current literature, we found that mitochondria can regulate immunity in different ways. First, alterations in metabolic pathways (TCA cycle, oxidative phosphorylation, and FAO) and mitochondria induced transcriptional changes can lead to entirely different outcomes in immune cells. For example, M1 macrophages exhibit a broken TCA cycle and have a pro-inflammatory role. By contrast, M2 macrophages undergo β-oxidation to produce anti-inflammatory responses. In addition, amino acid metabolism, especially arginine, glutamine, serine, glycine, and tryptophan, is critical for T cell differentiation and macrophage polarization. Second, mitochondria can activate the inflammatory response. For instance, mitochondrial antiviral signaling and NLRP3 can be activated by mitochondria. Third, mitochondrial mass and mobility can be influenced by fission and fusion. Fission and fusion can influence immune functions. Finally, mitochondria are placed near the endoplasmic reticulum (ER) in immune cells. Therefore, mitochondria and ER junction signaling can also influence immune cell metabolism. Mitochondrial machinery such as metabolic pathways, amino acid metabolism, antioxidant systems, mitochondrial dynamics, mtDNA, mitophagy, and mtROS are crucial for immune functions. Here, we have demonstrated how mitochondria coordinate to alter immune responses and how changes in mitochondrial machinery contribute to alterations in immune responses. A better understanding of the molecular components of mitochondria is necessary. This can help in the development of safe and effective immune therapy or prevention of chronic diseases. In this review, we have presented an updated prospective of the mitochondrial machinery that drives various immune responses.

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“…Repeated blood transfusion could accelerate iron absorption, which results in iron overload in some patients. Iron overload can increase the production of mitochondrial reactive oxygen species (ROS), induce the dysfunction of mesenchymal stem cells [8], promote erythroid apoptosis through regulating HIF-1a/ROS signalling pathway in MDS patients [9], injure the function of MDS-derived mesenchymal stromal cells (MSCs) and promote mitochondrial fragmentation in MSCs from MDS patients [10,11]. In light of this, we could speculate that the deterioration of anaemia in iron overloaded MDS patients may be related to the injury of hematopoietic cell and the abnormality of apoptosis.…”

Section: Introductionmentioning

confidence: 99%

Effect of iron chelation therapy on EPO-STAT5 signalling pathway and EPO resistance in iron-overloaded low-risk myelodysplastic syndrome patients

Yao

2019

Hematology

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Objectives: Background/aims: We aim to explore low-risk MDS patients' ESA response and the difference between iron-overloaded (IO) group and the control group in the expression of SOCS1, STAT5 and BCL2L1 which play a key role to EPO-STAT5 signal pathway. Methods: 56 low-risk MDS patients were divided into experimental group, IO patients; control group, non-IO patients. Among experimental group, 28 IO patients were treated with iron chelation therapy (ICT). SOCS1, phosphorylated STAT5 (p-STAT5) and BCL2L1 protein concentration in bone marrow supernatant have been analyzed by ELISA, STAT5a+b protein concentration in bone marrow mononuclear cells (BMMC) have been analyzed by Western blot, and mRNA expression of them have been detected in BMMC by RQ-PCR. The percentage of CD71 + cells in BMMC, apoptotic rate of CD71 + cells and ROS expression in CD71 + cells were detected by Flow cytometry. Results: Compared with the control group, the sEPO concentration, the efficacy of ESA and the expression of SOCS1, apoptotic rates of CD71 + cells and ROS expression in CD71 + cells in IO group were increased, the expression of STAT5 and BCL2L1 was reduced. Interestingly, after receiving ICT, some patients with EPO resistance have responded again to ESA treatment, with the decrease of the expression of SOCS1, apoptotic rates of CD71 + cells, ROS expression in CD71 + cells and the increase of the expression of STAT5 and BCL2L1. Conclusion: Iron overload can increase EPO resistance and the expression of SOCS1, inhibit the expression of STAT5 and BCL2L1. ICT could allivation of EPO resistance.

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Iron overload promotes mitochondrial fragmentation in mesenchymal stromal cells from myelodysplastic syndrome patients through activation of the AMPK/MFF/Drp1 pathway

Cited by 88 publications

References 52 publications

Iron overload impairs normal hematopoietic stem and progenitor cells through reactive oxygen species and shortens survival in myelodysplastic syndrome mice

Iron overload impairs normal hematopoietic stem and progenitor cells through reactive oxygen species and shortens survival in myelodysplastic syndrome mice

Diverse Roles of Mitochondria in Immune Responses: Novel Insights Into Immuno-Metabolism

Effect of iron chelation therapy on EPO-STAT5 signalling pathway and EPO resistance in iron-overloaded low-risk myelodysplastic syndrome patients

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