Whole-Exome Sequencing of Rare Site Endometriosis-Associated Cancer

Malignant transformation of extraovarian endometriosis is rare, with the carcinogenesis mechanism unclear. To clarify the actionable variants of rare-site endometriosis-associated cancer (RSEAC), we performed whole-exome sequencing for the tumor, in two patients. The intestine was affected in both c...

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Published in	Diseases Vol. 9; no. 1; p. 14
Main Authors	Kurose, Sonomi, Nakayama, Kentaro, Razia, Sultana, Ishikawa, Masako, Ishibashi, Tomoka, Yamashita, Hitomi, Sato, Seiya, Sakiyama, Asuka, Yoshioka, Shinya, Kobayashi, Misa, Nakayama, Satoru, Otuski, Yoshiro, Ishikawa, Noriyoshi, Kyo, Satoru
Format	Journal Article
Language	English
Published	Switzerland MDPI AG 04.02.2021 MDPI
Subjects	actionable variants Astrocytoma Breast cancer Cancer Carcinogenesis CD8 antigen Chemotherapy Deoxyribonucleic acid DNA Endocrine therapy Endometriosis Epigenetics exome sequencing Frameshift mutation Genotype & phenotype Homologous recombination Hormones immune checkpoint inhibitor Immune checkpoint inhibitors Immunohistochemistry Intestine Medical research Menopause Mutation Ovaries p53 Protein Pancreas Pancreatic cancer Patients PD-1 protein Phenotypes PTEN protein rare site endometriosis-associated cancer Tumor suppressor genes Tumors Womens health United States > US Japan exome sequencing immune checkpoint inhibitor actionable variants rare site endometriosis-associated cancer
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ISSN	2079-9721 2079-9721
DOI	10.3390/diseases9010014

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Abstract	Malignant transformation of extraovarian endometriosis is rare, with the carcinogenesis mechanism unclear. To clarify the actionable variants of rare-site endometriosis-associated cancer (RSEAC), we performed whole-exome sequencing for the tumor, in two patients. The intestine was affected in both cases, although the histology was that of clear cell carcinoma and undifferentiated carcinoma, respectively. Therefore, the cases were referred to as endometriosis-associated intestinal tumors (EIATs). Actionable variants (all frameshift mutations) were identified in tumor suppressor genes ARID1A, PTEN, and p53; however, no oncogenic variants were identified. Both cases were microsatellite stable. The patient with undifferentiated carcinoma exhibited hypermutator and homologous recombination deficiency phenotypes. The dominant mutation signatures were signature 30 (small subset of breast cancers) and 19 (pilocytic astrocytoma) in patient 1, and signature 5 (small subset of breast cancers) and 3 (breast, ovarian, and pancreatic cancers) in patient 2. Immunohistochemistry revealed positive CD8 and PD-1 expression in both patients; patient 1 also showed positive PDL-1 expression. Our results suggest that RSEAC is associated with variants of tumor suppressor genes as epigenetic alterations. Mutation signature-based whole-exome sequencing could be useful to select an adjuvant chemotherapy regimen. High CD8 and PD-1 expression in RSEAC suggests that immune checkpoint inhibitors are useful for treatment.
AbstractList	Malignant transformation of extraovarian endometriosis is rare, with the carcinogenesis mechanism unclear. To clarify the actionable variants of rare-site endometriosis-associated cancer (RSEAC), we performed whole-exome sequencing for the tumor, in two patients. The intestine was affected in both cases, although the histology was that of clear cell carcinoma and undifferentiated carcinoma, respectively. Therefore, the cases were referred to as endometriosis-associated intestinal tumors (EIATs). Actionable variants (all frameshift mutations) were identified in tumor suppressor genes ARID1A, PTEN, and p53; however, no oncogenic variants were identified. Both cases were microsatellite stable. The patient with undifferentiated carcinoma exhibited hypermutator and homologous recombination deficiency phenotypes. The dominant mutation signatures were signature 30 (small subset of breast cancers) and 19 (pilocytic astrocytoma) in patient 1, and signature 5 (small subset of breast cancers) and 3 (breast, ovarian, and pancreatic cancers) in patient 2. Immunohistochemistry revealed positive CD8 and PD-1 expression in both patients; patient 1 also showed positive PDL-1 expression. Our results suggest that RSEAC is associated with variants of tumor suppressor genes as epigenetic alterations. Mutation signature-based whole-exome sequencing could be useful to select an adjuvant chemotherapy regimen. High CD8 and PD-1 expression in RSEAC suggests that immune checkpoint inhibitors are useful for treatment. Malignant transformation of extraovarian endometriosis is rare, with the carcinogenesis mechanism unclear. To clarify the actionable variants of rare-site endometriosis-associated cancer (RSEAC), we performed whole-exome sequencing for the tumor, in two patients. The intestine was affected in both cases, although the histology was that of clear cell carcinoma and undifferentiated carcinoma, respectively. Therefore, the cases were referred to as endometriosis-associated intestinal tumors (EIATs). Actionable variants (all frameshift mutations) were identified in tumor suppressor genes ARID1A, PTEN, and p53; however, no oncogenic variants were identified. Both cases were microsatellite stable. The patient with undifferentiated carcinoma exhibited hypermutator and homologous recombination deficiency phenotypes. The dominant mutation signatures were signature 30 (small subset of breast cancers) and 19 (pilocytic astrocytoma) in patient 1, and signature 5 (small subset of breast cancers) and 3 (breast, ovarian, and pancreatic cancers) in patient 2. Immunohistochemistry revealed positive CD8 and PD-1 expression in both patients; patient 1 also showed positive PDL-1 expression. Our results suggest that RSEAC is associated with variants of tumor suppressor genes as epigenetic alterations. Mutation signature-based whole-exome sequencing could be useful to select an adjuvant chemotherapy regimen. High CD8 and PD-1 expression in RSEAC suggests that immune checkpoint inhibitors are useful for treatment.Malignant transformation of extraovarian endometriosis is rare, with the carcinogenesis mechanism unclear. To clarify the actionable variants of rare-site endometriosis-associated cancer (RSEAC), we performed whole-exome sequencing for the tumor, in two patients. The intestine was affected in both cases, although the histology was that of clear cell carcinoma and undifferentiated carcinoma, respectively. Therefore, the cases were referred to as endometriosis-associated intestinal tumors (EIATs). Actionable variants (all frameshift mutations) were identified in tumor suppressor genes ARID1A, PTEN, and p53; however, no oncogenic variants were identified. Both cases were microsatellite stable. The patient with undifferentiated carcinoma exhibited hypermutator and homologous recombination deficiency phenotypes. The dominant mutation signatures were signature 30 (small subset of breast cancers) and 19 (pilocytic astrocytoma) in patient 1, and signature 5 (small subset of breast cancers) and 3 (breast, ovarian, and pancreatic cancers) in patient 2. Immunohistochemistry revealed positive CD8 and PD-1 expression in both patients; patient 1 also showed positive PDL-1 expression. Our results suggest that RSEAC is associated with variants of tumor suppressor genes as epigenetic alterations. Mutation signature-based whole-exome sequencing could be useful to select an adjuvant chemotherapy regimen. High CD8 and PD-1 expression in RSEAC suggests that immune checkpoint inhibitors are useful for treatment. Malignant transformation of extraovarian endometriosis is rare, with the carcinogenesis mechanism unclear. To clarify the actionable variants of rare-site endometriosis-associated cancer (RSEAC), we performed whole-exome sequencing for the tumor, in two patients. The intestine was affected in both cases, although the histology was that of clear cell carcinoma and undifferentiated carcinoma, respectively. Therefore, the cases were referred to as endometriosis-associated intestinal tumors (EIATs). Actionable variants (all frameshift mutations) were identified in tumor suppressor genes , , and ; however, no oncogenic variants were identified. Both cases were microsatellite stable. The patient with undifferentiated carcinoma exhibited hypermutator and homologous recombination deficiency phenotypes. The dominant mutation signatures were signature 30 (small subset of breast cancers) and 19 (pilocytic astrocytoma) in patient 1, and signature 5 (small subset of breast cancers) and 3 (breast, ovarian, and pancreatic cancers) in patient 2. Immunohistochemistry revealed positive CD8 and PD-1 expression in both patients; patient 1 also showed positive PDL-1 expression. Our results suggest that RSEAC is associated with variants of tumor suppressor genes as epigenetic alterations. Mutation signature-based whole-exome sequencing could be useful to select an adjuvant chemotherapy regimen. High CD8 and PD-1 expression in RSEAC suggests that immune checkpoint inhibitors are useful for treatment. Malignant transformation of extraovarian endometriosis is rare, with the carcinogenesis mechanism unclear. To clarify the actionable variants of rare-site endometriosis-associated cancer (RSEAC), we performed whole-exome sequencing for the tumor, in two patients. The intestine was affected in both cases, although the histology was that of clear cell carcinoma and undifferentiated carcinoma, respectively. Therefore, the cases were referred to as endometriosis-associated intestinal tumors (EIATs). Actionable variants (all frameshift mutations) were identified in tumor suppressor genes ARID1A , PTEN , and p53 ; however, no oncogenic variants were identified. Both cases were microsatellite stable. The patient with undifferentiated carcinoma exhibited hypermutator and homologous recombination deficiency phenotypes. The dominant mutation signatures were signature 30 (small subset of breast cancers) and 19 (pilocytic astrocytoma) in patient 1, and signature 5 (small subset of breast cancers) and 3 (breast, ovarian, and pancreatic cancers) in patient 2. Immunohistochemistry revealed positive CD8 and PD-1 expression in both patients; patient 1 also showed positive PDL-1 expression. Our results suggest that RSEAC is associated with variants of tumor suppressor genes as epigenetic alterations. Mutation signature-based whole-exome sequencing could be useful to select an adjuvant chemotherapy regimen. High CD8 and PD-1 expression in RSEAC suggests that immune checkpoint inhibitors are useful for treatment.
Author	Ishikawa, Masako Razia, Sultana Kurose, Sonomi Kyo, Satoru Sato, Seiya Nakayama, Satoru Ishikawa, Noriyoshi Nakayama, Kentaro Yamashita, Hitomi Yoshioka, Shinya Sakiyama, Asuka Otuski, Yoshiro Kobayashi, Misa Ishibashi, Tomoka
AuthorAffiliation	1 Department of Obstetrics and Gynecology, Shimane University School of Medicine, Izumo 693-8501, Japan; dokinchan.lj.1108@gmail.com (S.K.); raeedahmed@yahoo.com (S.R.); m-ishi@med.shimane-u.ac.jp (M.I.); tomoka@med.shimane-u.ac.jp (T.I.); memedasudasu1103@gmail.com (H.Y.); sato_seiya9534@yahoo.co.jp (S.S.); satoruky@med.shimane-u.ac.jp (S.K.) 4 Department of Organ Pathology, Seirei Hamamatsu Hospital, Hamamatsu 430-8558, Japan; kanatomo@med.shimane-u.ac.jp 2 Department of Obstetrics and Gynecology, Kobe City Medical Center Hospital, Kobe 650-0047, Japan; wishkitty.happy.914@gmail.com (A.S.); s.yoshioka@kcho.jp (S.Y.) 5 Department of Organ Pathology, Shimane University School of Medicine, Izumo 693-8501, Japan; otsuki@sis.seirei.or.jp 3 Department of Obstetrics and Gynecology, Seirei Hamamatsu Hospital, Hamamatsu 430-8558, Japan; misan_bobo@yahoo.co.jp (M.K.); satoru@sis.seirei.or.jp (S.N.)
AuthorAffiliation_xml	– name: 1 Department of Obstetrics and Gynecology, Shimane University School of Medicine, Izumo 693-8501, Japan; dokinchan.lj.1108@gmail.com (S.K.); raeedahmed@yahoo.com (S.R.); m-ishi@med.shimane-u.ac.jp (M.I.); tomoka@med.shimane-u.ac.jp (T.I.); memedasudasu1103@gmail.com (H.Y.); sato_seiya9534@yahoo.co.jp (S.S.); satoruky@med.shimane-u.ac.jp (S.K.) – name: 4 Department of Organ Pathology, Seirei Hamamatsu Hospital, Hamamatsu 430-8558, Japan; kanatomo@med.shimane-u.ac.jp – name: 5 Department of Organ Pathology, Shimane University School of Medicine, Izumo 693-8501, Japan; otsuki@sis.seirei.or.jp – name: 3 Department of Obstetrics and Gynecology, Seirei Hamamatsu Hospital, Hamamatsu 430-8558, Japan; misan_bobo@yahoo.co.jp (M.K.); satoru@sis.seirei.or.jp (S.N.) – name: 2 Department of Obstetrics and Gynecology, Kobe City Medical Center Hospital, Kobe 650-0047, Japan; wishkitty.happy.914@gmail.com (A.S.); s.yoshioka@kcho.jp (S.Y.)
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CitedBy_id	crossref_primary_10_1016_j_cellsig_2021_110139 crossref_primary_10_3390_biomedicines11072036 crossref_primary_10_3389_fbioe_2022_918368 crossref_primary_10_3390_cimb46090555
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Keywords	exome sequencing immune checkpoint inhibitor actionable variants rare site endometriosis-associated cancer
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Snippet	Malignant transformation of extraovarian endometriosis is rare, with the carcinogenesis mechanism unclear. To clarify the actionable variants of rare-site...
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SubjectTerms	actionable variants Astrocytoma Breast cancer Cancer Carcinogenesis CD8 antigen Chemotherapy Deoxyribonucleic acid DNA Endocrine therapy Endometriosis Epigenetics exome sequencing Frameshift mutation Genotype & phenotype Homologous recombination Hormones immune checkpoint inhibitor Immune checkpoint inhibitors Immunohistochemistry Intestine Medical research Menopause Mutation Ovaries p53 Protein Pancreas Pancreatic cancer Patients PD-1 protein Phenotypes PTEN protein rare site endometriosis-associated cancer Tumor suppressor genes Tumors Womens health
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Title	Whole-Exome Sequencing of Rare Site Endometriosis-Associated Cancer
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