<p>Recent studies have demonstrated that a subset of long “noncoding” RNAs (lncRNAs) produce functional polypeptides and proteins. In this study, we discovered a 132 amino acid protein in human breast cancer cells named XCP (<Emphasis Type="Underline">X</Emphasis>-linked <Emphasis Type="Underline">C</Emphasis>ancer-associated <Emphasis Type="Underline">P</Emphasis>olypeptide), which is encoded by <i>lncRNA1456</i> (a.k.a. <i>RHOXF1P3</i>), a transcript previously thought to be noncoding. <i>lncRNA1456</i> is a pancreas- and testis-specific RNA whose gene is located on chromosome X. We found that the expression of <i>lncRNA1456</i> and XCP is highly upregulated in the luminal A, luminal B, and HER2 molecular subtypes of breast cancer. XCP modulates both estrogen-dependent and estrogen-independent growth of breast cancer cells by regulating cancer pathways, as shown in cell and xenograft models. XCP shares some homology with homeodomain-containing proteins and interacts with the histone demethylase plant homeodomain finger protein 8 (PHF8), which is also encoded by an X-linked gene. Mechanistically, XCP is required for the binding of PHF8 to chromatin. Moreover, XCP stimulates the histone demethylase activity of PHF8 to regulate gene expression in breast cancer cells. These findings identify XCP as a coregulator of PHF8 in the chromatin-dependent regulation of gene expression and emphasize the need to interrogate the potential functional roles of open reading frames originating from noncoding RNAs.</p>

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X-linked cancer-associated polypeptide (XCP) from lncRNA1456 modulates PHF8 histone demethylase activity to regulate the epigenome, gene expression, and cellular pathways in breast cancer

  • Shrikanth S. Gadad,
  • Cristel V. Camacho,
  • Xuan Gong,
  • Micah Thornton,
  • Venkat S. Malladi,
  • Anusha Nagari,
  • Aishwarya Sundaresan,
  • Tulip Nandu,
  • Sneh Koul,
  • Yan Peng,
  • W. Lee Kraus

摘要

Recent studies have demonstrated that a subset of long “noncoding” RNAs (lncRNAs) produce functional polypeptides and proteins. In this study, we discovered a 132 amino acid protein in human breast cancer cells named XCP (X-linked Cancer-associated Polypeptide), which is encoded by lncRNA1456 (a.k.a. RHOXF1P3), a transcript previously thought to be noncoding. lncRNA1456 is a pancreas- and testis-specific RNA whose gene is located on chromosome X. We found that the expression of lncRNA1456 and XCP is highly upregulated in the luminal A, luminal B, and HER2 molecular subtypes of breast cancer. XCP modulates both estrogen-dependent and estrogen-independent growth of breast cancer cells by regulating cancer pathways, as shown in cell and xenograft models. XCP shares some homology with homeodomain-containing proteins and interacts with the histone demethylase plant homeodomain finger protein 8 (PHF8), which is also encoded by an X-linked gene. Mechanistically, XCP is required for the binding of PHF8 to chromatin. Moreover, XCP stimulates the histone demethylase activity of PHF8 to regulate gene expression in breast cancer cells. These findings identify XCP as a coregulator of PHF8 in the chromatin-dependent regulation of gene expression and emphasize the need to interrogate the potential functional roles of open reading frames originating from noncoding RNAs.