Expression of L1 retrotransposon open reading frame protein 1 in gynecologic cancers

Expression of L1 retrotransposon open reading frame protein 1 in gynecologic cancers

LINE-1 (L1) retrotransposons are mobile genetic elements capable of “copy-and-pasting” their own sequences into random genomic loci, and one of the proteins it uses to achieve mobility is LINE-1 open reading frame 1 protein (L1ORF1p). L1ORF1p expression is found across many epithelial cancers, inclu...

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Veröffentlicht in:Human pathology 2019-10, Vol.92, p.39-47
Hauptverfasser: Xia, Zhouchunyang, Cochrane, Dawn R., Tessier-Cloutier, Basile, Leung, Samuel, Karnezis, Anthony N., Cheng, Angela S., Farnell, David A., Magrill, Jamie, Schmidt, Dietmar, Kommoss, Stefan, Kommoss, Felix K.F., Kommoss, Friederich, McAlpine, Jessica N., Gilks, C. Blake, Koebel, Martin, Rabban, Joseph T., Huntsman, David G.
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Biomarkers
Endometrial cancer
Genomes
Gynecological cancer
Gynecological cancers
Gynecology
L1ORF1p
LINE-1 retrotransposon
Mutation
Ovarian cancer
p53
Serous tubal intraepithelial carcinomas (STICs)
Stains & staining
Tumors
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container_end_page 47
container_issue
container_start_page 39
container_title Human pathology
container_volume 92
creator Xia, Zhouchunyang
Cochrane, Dawn R.
Tessier-Cloutier, Basile
Leung, Samuel
Karnezis, Anthony N.
Cheng, Angela S.
Farnell, David A.
Magrill, Jamie
Schmidt, Dietmar
Kommoss, Stefan
Kommoss, Felix K.F.
Kommoss, Friederich
McAlpine, Jessica N.
Gilks, C. Blake
Koebel, Martin
Rabban, Joseph T.
Huntsman, David G.
description LINE-1 (L1) retrotransposons are mobile genetic elements capable of “copy-and-pasting” their own sequences into random genomic loci, and one of the proteins it uses to achieve mobility is LINE-1 open reading frame 1 protein (L1ORF1p). L1ORF1p expression is found across many epithelial cancers, including small cohorts of ovarian and endometrial cancers, and is highly expressed in cancers with mutant p53 expressions. Here we aimed to gain insights into L1ORF1p expression levels within specific histotypes of ovarian cancers: high-grade serous (n = 585), low-grade serous (n = 26), clear cell (n = 132), endometrioid (n = 148), and mucinous (n = 32) ovarian cancers, as well as endometrial cancers (n = 607) using tissue microarray (TMA's). We demonstrated that L1ORF1p expression is associated with advanced stage and serous histotype in gynecological cancers. Like previous studies, we found a higher proportion of L1ORF1p expression in cases with aberrant p53 expression. We evaluated the expression of L1ORF1p in serous tubal intraepithelial carcinomas (STICs) (n = 6) and p53 signature lesions (n = 2) in fallopian tubes. Three STIC cases displayed aberrant p53 overexpression with corresponding L1ORF1p expression in the same tissues, but such correlation was not seen in the two p53 signature lesions, suggesting that L1 protein may be expressed after dysplastic transformation. The remaining three STIC cases have TP53 nonsense mutations with absent p53 expression but a strong and clear L1ORF1p expression within the STIC lesions. While L1ORF1p may not be prognostic in gynecological cancers, it may be useful clinically as a diagnostic IHC marker for p53 null STIC lesions and this warrants further investigation. •LINE-1 retrotransposon open reading frame 1 (L1ORF1p) is expressed in many cancers.•L1ORF1p associates with advanced stage and serous histotype in gynecological cancers.•L1ORF1p is expressed in STIC lesions, including in p53 null lesions.
doi_str_mv 10.1016/j.humpath.2019.06.001
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Here we aimed to gain insights into L1ORF1p expression levels within specific histotypes of ovarian cancers: high-grade serous (n = 585), low-grade serous (n = 26), clear cell (n = 132), endometrioid (n = 148), and mucinous (n = 32) ovarian cancers, as well as endometrial cancers (n = 607) using tissue microarray (TMA's). We demonstrated that L1ORF1p expression is associated with advanced stage and serous histotype in gynecological cancers. Like previous studies, we found a higher proportion of L1ORF1p expression in cases with aberrant p53 expression. We evaluated the expression of L1ORF1p in serous tubal intraepithelial carcinomas (STICs) (n = 6) and p53 signature lesions (n = 2) in fallopian tubes. Three STIC cases displayed aberrant p53 overexpression with corresponding L1ORF1p expression in the same tissues, but such correlation was not seen in the two p53 signature lesions, suggesting that L1 protein may be expressed after dysplastic transformation. The remaining three STIC cases have TP53 nonsense mutations with absent p53 expression but a strong and clear L1ORF1p expression within the STIC lesions. 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The remaining three STIC cases have TP53 nonsense mutations with absent p53 expression but a strong and clear L1ORF1p expression within the STIC lesions. 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Here we aimed to gain insights into L1ORF1p expression levels within specific histotypes of ovarian cancers: high-grade serous (n = 585), low-grade serous (n = 26), clear cell (n = 132), endometrioid (n = 148), and mucinous (n = 32) ovarian cancers, as well as endometrial cancers (n = 607) using tissue microarray (TMA's). We demonstrated that L1ORF1p expression is associated with advanced stage and serous histotype in gynecological cancers. Like previous studies, we found a higher proportion of L1ORF1p expression in cases with aberrant p53 expression. We evaluated the expression of L1ORF1p in serous tubal intraepithelial carcinomas (STICs) (n = 6) and p53 signature lesions (n = 2) in fallopian tubes. Three STIC cases displayed aberrant p53 overexpression with corresponding L1ORF1p expression in the same tissues, but such correlation was not seen in the two p53 signature lesions, suggesting that L1 protein may be expressed after dysplastic transformation. The remaining three STIC cases have TP53 nonsense mutations with absent p53 expression but a strong and clear L1ORF1p expression within the STIC lesions. While L1ORF1p may not be prognostic in gynecological cancers, it may be useful clinically as a diagnostic IHC marker for p53 null STIC lesions and this warrants further investigation. •LINE-1 retrotransposon open reading frame 1 (L1ORF1p) is expressed in many cancers.•L1ORF1p associates with advanced stage and serous histotype in gynecological cancers.•L1ORF1p is expressed in STIC lesions, including in p53 null lesions.</abstract><cop>United States</cop><pub>Elsevier Inc</pub><pmid>31220479</pmid><doi>10.1016/j.humpath.2019.06.001</doi><tpages>9</tpages></addata></record>
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source Elsevier ScienceDirect Journals Complete
subjects Biomarkers
Endometrial cancer
Genomes
Gynecological cancer
Gynecological cancers
Gynecology
L1ORF1p
LINE-1 retrotransposon
Mutation
Ovarian cancer
p53
Serous tubal intraepithelial carcinomas (STICs)
Stains & staining
Tumors
title Expression of L1 retrotransposon open reading frame protein 1 in gynecologic cancers
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