Ube3a-ATS

SNHG14
Identifiers
Aliases	SNHG14, 115HG, LNCAT, NCRNA00214, UBE3A-AS, UBE3A-AS1, UBE3AATS, small nucleolar RNA host gene 14, IC-SNURF-SNRPN, U-UBE3A-ATS, UBE3A-ATS, Ube3a-ATS
External IDs	OMIM: 616259; GeneCards: SNHG14; OMA:SNHG14 - orthologs
Orthologs
	104472715
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	ENSG00000224078
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	n; a
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	Wikidata
View/Edit Human

UBE3A-ATS/Ube3a-ATS (human/mouse), otherwise known as ubiquitin ligase E3A-ATS, is the name for the antisense DNA strand that is transcribed as part of a larger transcript called LNCAT (large non-coding antisense transcript) at the Ube3a locus. The Ube3a locus is imprinted and in the central nervous system expressed only from the maternal allele. Silencing of Ube3a on the paternal allele is thought to occur through the Ube3a-ATS part of LNCAT,^[2] since non-coding antisense transcripts are often found at imprinted loci.^[3] The deletion and/or mutation of Ube3a on the maternal chromosome causes Angelman syndrome (AS) and Ube3a-ATS may prove to be an important aspect in finding a therapy for this disease. While in patients with AS the maternal Ube3a allele is inactive, the paternal allele is intact but epigenetically silenced. If unsilenced, the paternal allele could be a source of active Ube3a protein in AS patients. Therefore, understanding the mechanisms of how Ube3a-ATS might be involved in silencing the paternal Ube3a may lead to new therapies for AS. This possibility has been demonstrated by a recent study where the drug topotecan, administered to mice suffering from AS, activated expression of the paternal Ube3a gene by lowering the transcription of Ube3a-ATS.^[4]

^ "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
^ Runte M, Hüttenhofer A, Gross S, Kiefmann M, Horsthemke B, Buiting K (November 2001). "The IC-SNURF-SNRPN transcript serves as a host for multiple small nucleolar RNA species and as an antisense RNA for UBE3A". Human Molecular Genetics. 10 (23): 2687–2700. doi:10.1093/hmg/10.23.2687. PMID 11726556.
^ Royo H, Cavaillé J (March 2008). "Non-coding RNAs in imprinted gene clusters". Biology of the Cell. 100 (3): 149–166. doi:10.1042/BC20070126. PMID 18271756. S2CID 8145761.
^ Huang HS, Allen JA, Mabb AM, King IF, Miriyala J, Taylor-Blake B, et al. (December 2011). "Topoisomerase inhibitors unsilence the dormant allele of Ube3a in neurons". Nature. 481 (7380): 185–189. doi:10.1038/nature10726. PMC 3257422. PMID 22190039.

[1] "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.

[Runte2001-2] Runte M, Hüttenhofer A, Gross S, Kiefmann M, Horsthemke B, Buiting K (November 2001). "The IC-SNURF-SNRPN transcript serves as a host for multiple small nucleolar RNA species and as an antisense RNA for UBE3A". Human Molecular Genetics. 10 (23): 2687–2700. doi:10.1093/hmg/10.23.2687. PMID 11726556.

[Royo2008-3] Royo H, Cavaillé J (March 2008). "Non-coding RNAs in imprinted gene clusters". Biology of the Cell. 100 (3): 149–166. doi:10.1042/BC20070126. PMID 18271756. S2CID 8145761.

[Huang2012-4] Huang HS, Allen JA, Mabb AM, King IF, Miriyala J, Taylor-Blake B, et al. (December 2011). "Topoisomerase inhibitors unsilence the dormant allele of Ube3a in neurons". Nature. 481 (7380): 185–189. doi:10.1038/nature10726. PMC 3257422. PMID 22190039.

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