<i>miR-144/451</i>
            represses the LKB1/AMPK/mTOR pathway to promote red cell precursor survival during recovery from acute anemia

Xiao, Fang; Shen, Feiyang; Lechauve, Christophe; Peng, Xu; Zhao, Guowei; Itkow, Jacobi; Wu, Fan; Hou, Yaying; Wu, Xiaohui; Yu, Lingling; Xiu, Huiqing; Wang, Mengli; Zhang, Ruiling; Wang, Fangfang; Zhang, Yanqing; Wang, Daxin; Weiss, Mitchell J.; Yu, Duonan

doi:10.3324/haematol.2017.177394

Cited by 36 publications

(52 citation statements)

References 49 publications

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“…Thus, in GBM cells, metabolic stress triggers a Cab39/AMPK-mediated positive feedback response between miR-451 and OCT1, which allows tumor cells to quickly adapt to variations of glucose concentrations in the tumor microenvironment. These findings in GBM cells uncover miR-451 as a major player in AMPK signaling, which is consistent with a recent finding in erythroid cells that miR-451 is an important effector that represses Cab39/AMPK activity [46]. The inconsistency is that deficiency of miR-451 in nucleated erythroid cells results in apoptosis, rather than adaptation for survival, in numerous stress conditions, including deprivation of glucose in culture medium ( [46]; unpublished data).…”

Section: Regulation Of Mir-144/451 Expression At Transcriptional Levelssupporting

confidence: 88%

“…These findings in GBM cells uncover miR-451 as a major player in AMPK signaling, which is consistent with a recent finding in erythroid cells that miR-451 is an important effector that represses Cab39/AMPK activity [46]. The inconsistency is that deficiency of miR-451 in nucleated erythroid cells results in apoptosis, rather than adaptation for survival, in numerous stress conditions, including deprivation of glucose in culture medium ( [46]; unpublished data). Farnesoid X Receptor (FXR) is a nuclear receptor and controls many aspects of lipid metabolism.…”

Section: Regulation Of Mir-144/451 Expression At Transcriptional Levelssupporting

confidence: 88%

“…Over expression of miR-144 or miR-451 enhances maturation of murine erythroleukemic cells, whereas depletion of miR-451 has the opposite effect [29,55]. Surprisingly, in vivo deletion of such abundantly expressed miR-144/451 genes only leads to mild hemolytic anemia [18][19][20]46], partially due to the erythrocytes' impaired capacity to remove reactive oxygen species (ROS) [19]. In animals, deletion of genomic miR-144/451 sequences elevates the level of miR-451 target gene (Ywhaz) product 14-3-3zeta, which sequesters the nuclear factor FoxO3 in the cytoplasm, thereby blocking transcription of anti-oxidant enzymes catalase (Cat) and glutathione peroxidase 1 (Gpx1) by FoxO3 [19].…”

Section: Mir-144/451 In Erythrocyte Development and Red Cell Diseasesmentioning

confidence: 99%

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miR-144/451 in hematopoiesis and beyond

Wang

2019

ExRNA

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MicroRNAs (miRNAs), a class of 18-25 nucleotide (nt) non-coding RNAs, usually inhibit the expression of their target genes. They are transcribed from endogenous genes and are processed for maturation by multiple pathways. miR-144/451, a bicistronic gene locus, encodes miR-144 and miR-451, both of which are highly conserved in evolution. These two miRNAs are on the same primary RNA molecule whose transcription is controlled by multiple nuclear proteins, including GATA1, GATA4, Myc, Oct1, Pax4, FXR, AP1, SMAD3 and SMAD4 depending on tissue types. They are abundant and almost exclusively exist in red blood cells, but low expression of both miR-144 and miR-451 are also detected in non-erythroid lineages. Interestingly, deletion of both miR-144 and miR-451 DNA sequences coding pre-miR-144/451 hairpins in mice leads only mild microcytic anemia but worsen upon a number of stresses including developmental stress, acute blood loss, phenohydrazine-induced hemolysis and precursor depletion by chemotherapeutic drug 5-FU. Such knockout animals older than 15 months also spontaneously develop malignant tumors including B-lymphoma and acute myeloid leukemia, indicating that miR-144/451 is a bona fide tumor-suppressing gene in non-erythroid cells, though its levels are much lower compared to that in red blood cells. Consistent with the findings in animals, disruption of miR-144/451 expression and their abnormal functions are observed in human hematopoietic and non-hematopoietic organs. Moreover, miR-451 is the only miRNA discovered so far whose maturation does not depend on Dicer, an enzyme required by all other miRNAs for maturation. This review focuses on the biogenesis, transcriptional regulation and biological roles of miR-144/451 in erythropoiesis, tumor initiation and other pathological conditions.

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Section: Regulation Of Mir-144/451 Expression At Transcriptional Levelssupporting

confidence: 88%

Section: Regulation Of Mir-144/451 Expression At Transcriptional Levelssupporting

confidence: 88%

Section: Mir-144/451 In Erythrocyte Development and Red Cell Diseasesmentioning

confidence: 99%

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miR-144/451 in hematopoiesis and beyond

Wang

2019

ExRNA

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“…Results miR-144 suppressed the proliferation of glioma cells. The miRNAs array analysis from several groups indicated that miR-144 and miR-451a, as anti-tumor miRNAs located in the same cluster, were decreased in different tumor tissues and modulated tumor development [20][21][22] . However, the detail mechanism still remains unclear.…”

Section: Ros Generation Detectionmentioning

confidence: 99%

“…Therefore identification glioma-related miRNAs and elucidation their effects and regulatory mechanisms have important roles in gliomas therapy. miR-144 located within the miR-144/miR-451a cluster and plays significant roles in tumor progression [20][21][22] . Several reports indicated that miR-144 could suppress tumor cell proliferation and block the cell cycle [23][24][25] .…”

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confidence: 99%

MicroRNA-144 represses gliomas progression and elevates susceptibility to Temozolomide by targeting CAV2 and FGF7

Liu

Ren

Zhao

et al. 2020

Sci Rep

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Malignant gliomas are the most common tumor in central nervous system with poor prognosis. Due to the limitation of histological classification in earlier diagnosis and individualized medicine, it is necessary to combine the molecular signatures and the pathological characteristics of gliomas. Lots of microRNAs presented abnormal expression in gliomas and modulated gliomas development.Exploration the miRNAs profile is helpful for the diagnosis, therapy and prognosis of gliomas. It has been demonstrated that miR-144 plays important roles in solid tumors. However, the detail mechanisms remained unrevealed. In this study, we have demonstrated the level of miR-144 decreased in glioma tissues from patients, especially in gliomas with higher grades. MiR-144 was also validated have lower expression in glioma cell lines compared with cortical neuron cell by using qRT-PCR. The in vitro functional experiment indicated miR-144 improved gliomas progression through repressing proliferation, sensitizing to chemotherapeutics and inhibiting metastasis. We further identified fibroblast growth factor 7 (FGF7) and Caveolin 2 (CAV2) were target genes of miR-144 by luciferase reporter assay and western blotting. The mechanisms study suggested forced FGF7 expression elevated Akt activation and decreased reactive oxygen species (ROS) generation. The MTT and cell cycle assay indicated miR-144 suppressed glioma cells proliferation through modulating FGF mediated Akt signaling pathway. Meanwhile, miR-144 promoted Temozolomide (TMZ) induced apoptosis in glioma cells via increasing ROS production by using FACS. On the other hand, CAV2, as another target of miR-144, accelerated glioma cells migration and invasion via promoting glioma cells EMT progress. Retrieved expression of FGF7 or CAV2 rescued the proliferation and migration function mediated by miR-144. Furthermore, the in vivo experiments in PDX models displayed the anti-tumor function of miR-144, which could be retrieved by overexpression of FGF7 and CAV2. Taken together, these findings indicated miR-144 acted as a potential target against gliomas progression and uncovered a novel regulatory mechanism, which may provide a new therapeutic strategy and prognostic indicator for gliomas.

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A comprehensive review on miR‐451: A promising cancer biomarker with therapeutic potential

Khordadmehr

Jigari-Asl

Ezzati

et al. 2019

Journal Cellular Physiology

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MicroRNAs (miRNAs) are proposed as a family of short noncoding molecules able to manage and control the expression of the gene targets at the posttranscriptional level. They contribute in several fundamental physiological mechanisms as well as a verity of human and animal diseases such as cancer progression. Among these tiny RNAs, miR-451 placed on chromosome 17 at 17q11.2 presents an essential role in many biological processes in health condition and also in pathogenesis of different diseases. Besides, it has been recently considered as a valuable biomarker for cancer detection, prognosis and treatment. Therefore, this review will provide the critical functions of miR-451 on biological mechanisms including cell cycle and proliferation, cell survival and apoptosis, differentiation and development as well as disease initiation and progression such as tumor formation, migration, invasion, and metastasis.

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miR-144/451 represses the LKB1/AMPK/mTOR pathway to promote red cell precursor survival during recovery from acute anemia

Cited by 36 publications

References 49 publications

miR-144/451 in hematopoiesis and beyond

miR-144/451 in hematopoiesis and beyond

MicroRNA-144 represses gliomas progression and elevates susceptibility to Temozolomide by targeting CAV2 and FGF7

A comprehensive review on miR‐451: A promising cancer biomarker with therapeutic potential

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