Difference between revisions of "MIR17HG"

From LncRNAWiki
Jump to: navigation, search
 
(10 intermediate revisions by the same user not shown)
Line 1: Line 1:
 
==Annotated Information==
 
==Annotated Information==
===Approved Symbol===
+
===Name===
MIR17HG
+
Approved Symbol:MIR17HG
===Approved Name===
+
 
miR-17-92a-1 cluster host gene
+
Approved Name:miR-17-92a-1 cluster host gene
===Previous Symbols===
+
 
C13orf25, MIRHG1
+
Previous Symbols:C13orf25, MIRHG1
===Synonyms===
+
 
FLJ14178, MIRH1, MIHG1, NCRNA00048, miR-17-92, LINC00048
+
Synonyms: FLJ14178, MIRH1, MIHG1, NCRNA00048, miR-17-92, LINC00048
 +
 
 +
RefSeq ID:NR_027349
 +
 
 +
Ensembl ID:ENSG00000215417
 +
 
 +
LncBook ID: [https://bigd.big.ac.cn/lncbook/transcript?transid=HSALNT0205332 HSALNT0205332]
 
===Chromosome===
 
===Chromosome===
 
13q31.3
 
13q31.3
===RefSeq ID===
+
 
NR_027349
 
 
===OMIM ID===
 
===OMIM ID===
 
609415
 
609415
===Ensembl ID===
+
===Disease===
ENSG00000215417
+
lymphoma, syndromic developmental defect
===pubmed IDs===
 
15126345, 15944707, 16266980, 17210683, 23551855
 
  
 
===Characteristics===
 
===Characteristics===
Line 48: Line 51:
  
 
==Labs working on this lncRNA==
 
==Labs working on this lncRNA==
* Division of Cardiovascular Medicine, Cardiovascular Institute, Stanford University School of Medicine, Stanford, CA 94305 <ref name="ref1" />.
+
Krannert Institute of Cardiology and Division of Cardiology, Department of Medicine, Indiana University School of Medicine, Indianapolis, Indiana 46202, USA .<ref name="ref1"/>
* Cold Spring Harbor Laboratory, Watson School of Biological Sciences, 1 Bungtown Road, Cold Spring Harbor, New York 11724, USA <ref name="ref1" />.
+
 
 +
Computational Medicine Center, Thomas Jefferson University, Philadelphia, PA 19107, USA. <ref name="ref2"/>.
 +
 
 +
Division of Cellular and Developmental Biology, MCB Department, University of California at Berkeley, Berkeley, CA 94705, USA. <ref name="ref3"/>.
 +
 
 +
Cold Spring Harbor Laboratory, Watson School of Biological Sciences, 1 Bungtown Road, Cold Spring Harbor, New York 11724, USA. <ref name="ref4"/>.
 +
 
 +
Division of Molecular Oncology, Aichi Cancer Center Research Institute, Japan.<ref name="ref5"/>.
  
 
==References==
 
==References==
 
<references>
 
<references>
<ref name="ref1"> Han P, Li W, Lin CH, Yang J, Shang C, Nurnberg ST, Jin KK, Xu W, Lin CY, Lin CJ, Xiong Y, Chien HC, Zhou B, Ashley E, Bernstein D, Chen PS, Chen HS, Quertermous T, Chang CP.(2014) A long non-coding RNA protects the heart from pathologicalhypertrophy. Nature 514(7520):102-6 .</ref>(1)
+
<ref name="ref1">Han P, Li W, Lin CH, Yang J, Shang C, Nurnberg ST, Jin KK, Xu W, Lin CY, Lin CJ, Xiong Y, Chien HC, Zhou B, Ashley E, Bernstein D, Chen PS, Chen HS, Quertermous T, Chang CP.(2014) A long non-coding RNA protects the heart from pathologicalhypertrophy. Nature 514(7520):102-6 .</ref>(1)
<ref name="ref2"> Mogilyansky E, Rigoutsos I. (2013)The miR-17/92 cluster: a comprehensive update on its genomics, genetics, functions and increasingly important and numerous roles in health and disease. Cell Death Differ. 20(12):1603–1614 .</ref>(2)
+
 
<ref name="ref3"> Olive V, Li Q, He L. Mir-17-92: a polycistronic oncomir with pleiotropic functions. Immunol Rev. 2013;253(1):158–166.</ref>(3)
+
<ref name="ref2">Mogilyansky E, Rigoutsos I. (2013)The miR-17/92 cluster: a comprehensive update on its genomics, genetics, functions and increasingly important and numerous roles in health and disease. Cell Death Differ. 20(12):1603–1614 .</ref>(2)
<ref name="ref4"> Lin He1, J. Michael Thomson, Michael T. Hemann1, Eva Hernando-Monge4, David Mu1,Summer Goodson2, Scott Powers1, Carlos Cordon-Cardo4, Scott W. Lowe1, Gregory J. Hannon1, and Scott M. Hammond.(2005)A microRNA polycistron as a potential human oncogene.Nature 435(7043): 828–833.</ref>(4)
+
 
<ref name="ref5"> Yoji Hayashita, Hirotaka Osada, Yoshio Tatematsu, Hideki Yamada, Kiyoshi Yanagisawa, Shuta Tomida, Yasushi Yatabe, Katsunobu Kawahara, Yoshitaka Sekido, Takashi Takahashi (2005) A Polycistronic MicroRNA Cluster, miR-17-92, Is Overexpressed in Human Lung Cancers and Enhances Cell Proliferation.Cancer Research CAN-05-2352.</ref>(5)
+
<ref name="ref3">Olive V, Li Q, He L. Mir-17-92: a polycistronic oncomir with pleiotropic functions. Immunol Rev. 2013;253(1):158–166.</ref>(3)
 +
 
 +
<ref name="ref4">Lin He1, J. Michael Thomson, Michael T. Hemann1, Eva Hernando-Monge4, David Mu1,Summer Goodson2, Scott Powers1, Carlos Cordon-Cardo4, Scott W. Lowe1, Gregory J. Hannon1, and Scott M. Hammond.(2005)A microRNA polycistron as a potential human oncogene.Nature 435(7043): 828–833.</ref>(4)
 +
 
 +
<ref name="ref5">Yoji Hayashita, Hirotaka Osada, Yoshio Tatematsu, Hideki Yamada, Kiyoshi Yanagisawa, Shuta Tomida, Yasushi Yatabe, Katsunobu Kawahara, Yoshitaka Sekido, Takashi Takahashi (2005) A Polycistronic MicroRNA Cluster, miR-17-92, Is Overexpressed in Human Lung Cancers and Enhances Cell Proliferation.Cancer Research CAN-05-2352.</ref>(5)
 
</references>
 
</references>

Latest revision as of 12:10, 11 August 2019

Annotated Information

Name

Approved Symbol:MIR17HG

Approved Name:miR-17-92a-1 cluster host gene

Previous Symbols:C13orf25, MIRHG1

Synonyms: FLJ14178, MIRH1, MIHG1, NCRNA00048, miR-17-92, LINC00048

RefSeq ID:NR_027349

Ensembl ID:ENSG00000215417

LncBook ID: HSALNT0205332

Chromosome

13q31.3

OMIM ID

609415

Disease

lymphoma, syndromic developmental defect

Characteristics

miR-17-92 cluster, which comprises seven miRNAs and resides in intron 3 of the C13orf25 gene at 13q31.3 [1].

Cellular Localization

The mir-17–92 polycistron,is located in a region of DNA that is amplified in human B-cell lymphomas.

Function

Gene (MIR17HG), which is involved in the development, progression, and aggressiveness of colorectal cancer [2].

This polycistronic gene, called MIR17HG or Oncomir-1 because of its mainly oncogenic functions (ie, activities that enhance cell proliferation, inhibit apoptosis, and modulate angiogenesis), is related to the homologous MIR106a–363 cluster on chromosome X and the MIR106b–25 cluster on chromosome 7.8,9.[3] [4].

Regulation

Finding of preferential overexpression of the miR-17-92 cluster in lung cancers with small-cell lung cancer histology, a subtype of lung cancer with prominent neuroendocrine feature, warrants study on its regulation and potential involvement from the cell differentiation point of view [1].

Diseases

  • colorectal cancer
  • lung cancer

Expression

Expression levels of the six MIR17HG cluster members (miR-17, miR-18a, miR-19a, miR-19b-1, miR-20a,and miR-92a-1) were also quantified by RT-qPCR in 34 cases for which RNA was available. In particular, the expression of all six miRs was detected in 23 of 34 cases. miR-19b-1 and miR-92a-1 showed the highest expression level, while miR-18a showed the lowest [2].

Tumours resulting from combined c-myc and mir-17–19b expression consistently invaded visceral organs outside the lymphoid compartment, including liver, lung and occasionally kidney [5].

Sequence

>gi|224994258|ref|NR_027349.1| Homo sapiens miR-17-92a-1 cluster host gene (MIR17HG), transcript variant 2, long non-coding RNA

000001 GAAGCTCTCC TCGCGGGGCG GGCCGGCCGG CCGCACCCCC GGCCTGGGGC CTCCGGTCGT AGTAAAGCGC AGGCGGGCGG 000080
000081 GGAGGCGGGA GCAGGAGCCC GCGGCCGGCC AGCCGAAGAT GGTGGCGGCT ACTCCTCCTG TCATACACGT GGACCTAACT 000160
000161 GCACCAGTAG CTTTTCTGAG AATACTTGCT GAAAAGGAAG TTTTCTGGAA TGGTATTTGC TAAGTGGAAG CCAGAAGAGG 000240
000241 AGGAAAATGT TTTGCCACGT GGATGTGAAG ATTTCCTCTA AAAGGCAGAC CTGTCTAACT ACAAGCCAGA CTTGGGTTTT 000320
000321 CTCCTGTAGT TTGAAGACAC ACTGACTCCT GACAAAATGC AGCCTGCAAC TTCCTGGAGA ACAACTCAGT GTCACATTAA 000400
000401 AGTTTATTAT GTATTTAATG ATACACTGTT TAATTGACAG TTTTGCATAG TTTGTCTAAC TTTAGAGAAT TAAGAGCCTC 000480
000481 TCAACTGAGC AGTAAAGGTA AGGAGAGCTC AATCTGCACA GAGCCAGTTT TTAGTGTTTG ATGGAAATAA GATCATCATG 000560
000561 CCCACTTGAG ACTTCAGATT ATTCTTTAGC TTAGTGGTTG TATGAGTTAC ATCTTATTAA AGTCGAAATT AATGTAGTTT 000640
000641 TCTGCCTTGA TAACATTTCA TATGTGGTAT TAGTTTTAAA GGGTCATTAG GAAAATGCAC ATATTCCATG AATTTTAAGA 000720
000721 CCCATAGAAA AGTTGAAGAA TGCTTAATTT TCTTATCCAG TAATGTAAAC ACAGAGACAG AACATTGAGA TGTGCCTAGT 000800
000801 TCTGTATTTA CAGTTTGGTC TGGCTGTTTG AGTTCTAGCG CATTTAATGT TAATAAATAA AATACTGCAT TTTAAAGCTG 000880
000881 TTAAGAAATT GTCCAGAACG AGAATATTGA AATAAAAACT TCAAGGT

Labs working on this lncRNA

Krannert Institute of Cardiology and Division of Cardiology, Department of Medicine, Indiana University School of Medicine, Indianapolis, Indiana 46202, USA .[2]

Computational Medicine Center, Thomas Jefferson University, Philadelphia, PA 19107, USA. [3].

Division of Cellular and Developmental Biology, MCB Department, University of California at Berkeley, Berkeley, CA 94705, USA. [4].

Cold Spring Harbor Laboratory, Watson School of Biological Sciences, 1 Bungtown Road, Cold Spring Harbor, New York 11724, USA. [5].

Division of Molecular Oncology, Aichi Cancer Center Research Institute, Japan.[1].

References

  1. 1.0 1.1 1.2 Yoji Hayashita, Hirotaka Osada, Yoshio Tatematsu, Hideki Yamada, Kiyoshi Yanagisawa, Shuta Tomida, Yasushi Yatabe, Katsunobu Kawahara, Yoshitaka Sekido, Takashi Takahashi (2005) A Polycistronic MicroRNA Cluster, miR-17-92, Is Overexpressed in Human Lung Cancers and Enhances Cell Proliferation.Cancer Research CAN-05-2352.
  2. 2.0 2.1 2.2 Han P, Li W, Lin CH, Yang J, Shang C, Nurnberg ST, Jin KK, Xu W, Lin CY, Lin CJ, Xiong Y, Chien HC, Zhou B, Ashley E, Bernstein D, Chen PS, Chen HS, Quertermous T, Chang CP.(2014) A long non-coding RNA protects the heart from pathologicalhypertrophy. Nature 514(7520):102-6 .
  3. 3.0 3.1 Mogilyansky E, Rigoutsos I. (2013)The miR-17/92 cluster: a comprehensive update on its genomics, genetics, functions and increasingly important and numerous roles in health and disease. Cell Death Differ. 20(12):1603–1614 .
  4. 4.0 4.1 Olive V, Li Q, He L. Mir-17-92: a polycistronic oncomir with pleiotropic functions. Immunol Rev. 2013;253(1):158–166.
  5. 5.0 5.1 Lin He1, J. Michael Thomson, Michael T. Hemann1, Eva Hernando-Monge4, David Mu1,Summer Goodson2, Scott Powers1, Carlos Cordon-Cardo4, Scott W. Lowe1, Gregory J. Hannon1, and Scott M. Hammond.(2005)A microRNA polycistron as a potential human oncogene.Nature 435(7043): 828–833.