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High Positive Correlations between ANRIL and p16-CDKN2A/p15-CDKN2B/p14-ARF Gene Cluster Overexpression in Multi-Tumor Types Suggest Deregulated Activation of an ANRIL-ARF Bidirectional Promoter.


ABSTRACT: The CDKN2B-AS1 gene, also called ANRIL, is located at the human CDKN2A/B locus at 9p21.3 and transcribed by RNA polymerase II into a long non-coding RNA of 3834 bp. The CDKN2B-AS1 gene overlaps a critical region of 125 kb covering the CDKN2B gene. The CDKN2A/B locus encompasses three major tumor suppressors juxtaposed and joined into a p16-CDKN2A/p15-CDKN2B/p14-ARF gene cluster. CDKN2A encodes splice variants p16-CDKN2A and p14-ARF, and CDKN2B encodes p15-CDKN2B. ANRIL shares a bidirectional promoter with the p14-ARF gene and is transcribed from the opposite strand to the cluster. We performed an analysis of the expression level of ANRIL and tumor suppressor p16-CDKN2A, p15-CDKN2B, and p14-ARF genes using quantitative RT-PCR in a multitumor panel. We observed the overexpression of the four genes ANRIL, p16-CDKN2A, p15-CDKN2B, and p14-ARF in the great majority of the 17 different cancer types. ANRIL was upregulated in 13/17 tumors compared to normal tissues, ranging from 5% (prostate cancer) to 91% (cervix cancer), with variable expression of p16-CDKN2A, p15-CDKN2B, and p14-ARF genes. A high positive correlation was identified between levels of expression of ANRIL and the three tumor suppressors. The strongest positive association was observed with p14-ARF (p < 0.001) in all but one (lung squamous cell carcinoma) of the examined tumor types. This correlation suggests coordinated deregulated mechanisms in all cancer types through aberrant activation of a bidirectional p14-ARF/ANRIL promoter. Furthermore, significant positive correlation was unexpectedly established in prostatic carcinomas, in contradiction with previous data.

SUBMITTER: Drak Alsibai K 

PROVIDER: S-EPMC6789474 | biostudies-literature | 2019 Aug

REPOSITORIES: biostudies-literature

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High Positive Correlations between <i>ANRIL</i> and <i>p16</i>-<i>CDKN2A</i>/<i>p15</i>-<i>CDKN2B</i>/<i>p14</i>-<i>ARF</i> Gene Cluster Overexpression in Multi-Tumor Types Suggest Deregulated Activation of an <i>ANRIL-ARF</i> Bidirectional Promoter.

Drak Alsibai Kinan K   Vacher Sophie S   Meseure Didier D   Nicolas Andre A   Lae Marick M   Schnitzler Anne A   Chemlali Walid W   Cros Jerome J   Longchampt Elisabeth E   Cacheux Wulfran W   Pignot Geraldine G   Callens Celine C   Pasmant Eric E   Allory Yves Y   Bieche Ivan I  

Non-coding RNA 20190821 3


The <i>CDKN2B-AS1</i> gene, also called <i>ANRIL</i>, is located at the human <i>CDKN2A/B</i> locus at 9p21.3 and transcribed by RNA polymerase II into a long non-coding RNA of 3834 bp. The <i>CDKN2B-AS1</i> gene overlaps a critical region of 125 kb covering the <i>CDKN2B</i> gene. The <i>CDKN2A/B</i> locus encompasses three major tumor suppressors juxtaposed and joined into a <i>p16-CDKN2A/p15-CDKN2B/p14-ARF</i> gene cluster. <i>CDKN2A</i> encodes splice variants p16-CDKN2A and p14-ARF, and <i>  ...[more]

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