HCSGD entry for ELAVL1

1. General information

Official gene symbolELAVL1
Entrez ID1994
Gene full nameELAV (embryonic lethal, abnormal vision, Drosophila)-like 1 (Hu antigen R)
Other gene symbolsELAV1 HUR Hua MelG
Links to Entrez GeneLinks to Entrez Gene

2. Neighbors in the network

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This gene isn't in Literature mining network.

3. Gene ontology annotation

GO ID

GO term

Evidence

Category

GO:0000166Nucleotide bindingIEAmolecular_function
GO:0003723RNA bindingIDA IEAmolecular_function
GO:0003725Double-stranded RNA bindingIDAmolecular_function
GO:0003729MRNA bindingTASmolecular_function
GO:0005515Protein bindingIPImolecular_function
GO:0005634NucleusIDAcellular_component
GO:0005654NucleoplasmTAScellular_component
GO:0005737CytoplasmIDAcellular_component
GO:0005829CytosolTAScellular_component
GO:0006417Regulation of translationIMPbiological_process
GO:0007275Multicellular organismal developmentTASbiological_process
GO:0010467Gene expressionTASbiological_process
GO:0016070RNA metabolic processTASbiological_process
GO:0016071MRNA metabolic processTASbiological_process
GO:0017091AU-rich element bindingIDAmolecular_function
GO:0019901Protein kinase bindingIPImolecular_function
GO:0035925MRNA 3'-UTR AU-rich region bindingIDAmolecular_function
GO:0045727Positive regulation of translationIDAbiological_process
GO:0048255MRNA stabilizationIDA IMPbiological_process
GO:00709353'-UTR-mediated mRNA stabilizationIDA IMPbiological_process
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4. Expression levels in datasets

  • Meta-analysis result

p-value upp-value downFDR upFDR down
0.94758951030.07316494810.99999024730.5099509929

  • Individual experiment result
    ( "-" represent NA in the specific microarray platform )

Data sourceUp or downLog fold change
GSE11954Down-0.0548875786
GSE13712_SHEARDown-0.0178643075
GSE13712_STATICDown-0.2254652944
GSE19018Down-0.3022635497
GSE19899_A1Down-0.2399801925
GSE19899_A2Up0.3680050611
PubMed_21979375_A1Down-0.5189395275
PubMed_21979375_A2Down-0.5820323588
GSE35957Down-0.1569838009
GSE36640Down-0.6121973984
GSE54402Up0.2319032987
GSE9593Down-0.3138992063
GSE43922Down-0.0982122673
GSE24585Down-0.1836880141
GSE37065Down-0.1329836617
GSE28863_A1Up0.3335822172
GSE28863_A2Up0.3349943351
GSE28863_A3Down-0.1462931916
GSE28863_A4Up0.1658927774
GSE48662Down-0.6038537512

5. Regulation relationships with compounds/drugs/microRNAs

  • Compounds

Not regulated by compounds

  • Drugs

Not regulated by drugs

  • MicroRNAs

  • mirTarBase

MiRNA_name

mirBase ID

miRTarBase ID

Experiment

Support type

References (Pubmed ID)

hsa-miR-519b-3pMIMAT0002837MIRT003731qRT-PCR//Western blotFunctional MTI19088191
hsa-miR-519c-3pMIMAT0002832MIRT003732qRT-PCR//Western blotFunctional MTI19088191
hsa-miR-519a-3pMIMAT0002869MIRT003733qRT-PCR//Western blotFunctional MTI19088191
hsa-miR-125a-5pMIMAT0000443MIRT005421Luciferase reporter assay//Western blotFunctional MTI19875930
hsa-miR-340-5pMIMAT0004692MIRT019606SequencingFunctional MTI (Weak)20371350
hsa-miR-93-5pMIMAT0000093MIRT048754CLASHFunctional MTI (Weak)23622248
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  • mirRecord

MicroRNA name

mirBase ID

Target site number

MiRNA mature ID

Test method inter

MiRNA regulation site

Reporter target site

Pubmed ID

hsa-miR-125a-5pMIMAT00004431hsa-miR-125a-5p{Western blot}{overexpression by miRNA precursor transfection}19875930
hsa-miR-125b-5pMIMAT00004231hsa-miR-125b{Western blot}{overexpression by miRNA precursor transfection}19875930
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6. Text-mining results about the gene

Gene occurances in abstracts of cellular senescence-associated articles: 6 abstracts the gene occurs.


PubMed ID of the article

Sentenece the gene occurs

25104461HuR and post-transcriptional regulation in vascular aging
25104461HuR (ELAV11 (embryonic lethal, abnormal vision)-like 1), a ubiquitously expressed member of the ELAV-like RNA-binding protein family, has been shown to regulate the stability and translation of mRNAs that encode factors regulating cellular senescence, thereby impacting on aging
25018007Loss of HuR leads to senescence-like cytokine induction in rodent fibroblasts by activating NF-kappaB
25018007BACKGROUND: HuR (human antigen R) is a ubiquitously expressed member of the Hu/ELAV family of proteins that is involved in diverse biological processes
25018007HuR has also been shown to play an important role in cell cycle arrest during replicative senescence in both human and mouse cells
25018007METHODS: Senescence-associated phenotypes were analyzed in MEFs and other cell line in which HuR expression is inhibited by sh-RNA-mediated knockdown
25018007RESULTS: RNAi-mediated HuR inhibition resulted in an increase in SASP-related cytokines
25018007In the absence of HuR, cells were defective in the DNA-damage response, and single strand DNA breaks accumulated, which may have caused the activation of NF-kappaB and subsequent cytokine induction
25018007CONCLUSIONS: In the absence of HuR, cells exhibit multiple senescence-associated phenotypes
25018007Our findings suggest that HuR regulates not only the replicative lifespan, but also the expression of SASP-related cytokines in mouse fibroblasts
22510478This inhibition in large part resulted from the downregulation of SIRT1, which in turn was because of decrease in the expression of the translation regulator HuR
18585896Signalling pathways regulating nucleo-cytoplasmic shuttling of the mRNA-binding protein HuR
18585896Accordingly, a large number of reports have documented that the Human antigen R (HuR), a ubiquitously expressed member of the ELAV protein family, is one of the major actors in this scenario
18585896Consequently, HuR is implicated in a large variety of pathologies in which deregulated stabilisation of many short-lived key mRNAs is causally linked with the onset and course of disease
18585896Since HuR is most abundantly localised within the cell nucleus, export of HuR to the cytoplasm seems a major prerequisite for its stabilising effects on its cognate target adenylate- and uridylate-rich elements (AREs) containing cargo mRNAs
18585896Although, the list of reports demonstrating a critical involvement of different signalling cascades in HuR-triggered mRNA functions is steadily growing, the mechanisms underlying HuR trafficking are not well understood
18585896For this reason, the review will cover the most recent advances of knowledge of signalling cascades involved in the stimulus-dependent nucleo-cytoplasmic HuR shuttling and a special emphasis will be put on the possible regulatory role of posttranslational HuR modification
12730239Increased AMP:ATP ratio and AMP-activated protein kinase activity during cellular senescence linked to reduced HuR function
12730239HuR function was previously shown to be implicated in the maintenance of a "young cell" phenotype in models of replicative cellular senescence
11486028Loss of HuR is linked to reduced expression of proliferative genes during replicative senescence
11486028Here, using two models of replicative senescence, we describe the influence of the RNA-binding protein HuR in regulating the expression of several genes whose expression decreases during senescence
11486028We demonstrate that HuR levels, HuR binding to target mRNAs encoding proliferative genes, and the half-lives of such mRNAs are lower in senescent cells
11486028Importantly, overexpression of HuR in senescent cells restored a "younger" phenotype, while a reduction in HuR expression accentuated the senescent phenotype
11486028Our studies highlight a critical role for HuR during the process of replicative senescence
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