Whole exome sequence analysis of serous borderline tumors of the ovary

Serous borderline tumor (SBT) is a unique histopathologic entity of the ovary, believed to be intermediate between benign cystadenoma and invasive low-grade serous carcinoma. While somatic mutations in the KRAS or BRAF, and rarely ERBB2, genes have been well characterized in SBTs, other genetic alte...

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Published in	Gynecologic oncology Vol. 130; no. 3; pp. 560 - 564
Main Authors	Boyd, Jeff, Luo, Biao, Peri, Suraj, Wirchansky, Beth, Hughes, Lucinda, Forsythe, Caitlin, Wu, Hong
Format	Journal Article
Language	English
Published	United States Elsevier Inc 01.09.2013
Subjects	Cell Adhesion Molecules - genetics Cell Cycle Proteins - genetics Cell Transformation, Neoplastic - genetics Cystadenoma, Serous - genetics Exome Exome - genetics F-Box Proteins - genetics F-Box-WD Repeat-Containing Protein 7 Female Gene Hematology, Oncology, and Palliative Medicine High-Throughput Nucleotide Sequencing Humans Middle Aged Mutation Mutation, Missense Obstetrics and Gynecology Ovarian Ovarian Neoplasms - genetics Proto-Oncogene Proteins B-raf - genetics Sequence Analysis, DNA Sequence Deletion Serous borderline tumor Ubiquitin-Protein Ligases - genetics Exome Ovarian Mutation Serous borderline tumor Gene
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ISSN	0090-8258 1095-6859 1095-6859
DOI	10.1016/j.ygyno.2013.06.007

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Abstract	Serous borderline tumor (SBT) is a unique histopathologic entity of the ovary, believed to be intermediate between benign cystadenoma and invasive low-grade serous carcinoma. While somatic mutations in the KRAS or BRAF, and rarely ERBB2, genes have been well characterized in SBTs, other genetic alterations have not been described. Toward a more comprehensive understanding of the molecular genetic architecture of SBTs, we undertook whole exome sequencing of this tumor type. Following pathologic review and laser capture microdissection to enrich for tumor cells, whole exomes were prepared from DNA of two independent SBTs and subjected to massively parallel DNA sequencing. Both tumors contained an activating mutation of the BRAF gene. A total of 15 additional somatic mutations were identified, nine in one tumor and six in the other. Eleven were missense mutations and four were nonsense or deletion mutations. Fourteen of the 16 genes found to be mutated in this study have been reported to be mutated in other cancers. Furthermore, 12 of these genes are mutated in ovarian cancers. The FBXW7 and KIAA1462 genes are noteworthy candidates for a pathogenic role in serous borderline tumorigenesis. These findings suggest that a very small number of somatic genetic mutations are characteristic of SBTs of the ovary, thus supporting their classification as a relatively genetically stable tumor type. The mutant genes described herein represent novel candidates for the pathogenesis of ovarian SBT. •This study examined the entire exome of serous borderline tumors (SBTs) of the ovary for somatic genetic mutations.•A very small number of mutations are characteristic of SBTs of the ovary.•Novel candidate genes for the pathogenesis of ovarian SBT were identified.
AbstractList	Serous borderline tumor (SBT) is a unique histopathologic entity of the ovary, believed to be intermediate between benign cystadenoma and invasive low-grade serous carcinoma. While somatic mutations in the KRAS or BRAF, and rarely ERBB2, genes have been well characterized in SBTs, other genetic alterations have not been described. Toward a more comprehensive understanding of the molecular genetic architecture of SBTs, we undertook whole exome sequencing of this tumor type. Following pathologic review and laser capture microdissection to enrich for tumor cells, whole exomes were prepared from DNA of two independent SBTs and subjected to massively parallel DNA sequencing. Both tumors contained an activating mutation of the BRAF gene. A total of 15 additional somatic mutations were identified, nine in one tumor and six in the other. Eleven were missense mutations and four were nonsense or deletion mutations. Fourteen of the 16 genes found to be mutated in this study have been reported to be mutated in other cancers. Furthermore, 12 of these genes are mutated in ovarian cancers. The FBXW7 and KIAA1462 genes are noteworthy candidates for a pathogenic role in serous borderline tumorigenesis. These findings suggest that a very small number of somatic genetic mutations are characteristic of SBTs of the ovary, thus supporting their classification as a relatively genetically stable tumor type. The mutant genes described herein represent novel candidates for the pathogenesis of ovarian SBT. •This study examined the entire exome of serous borderline tumors (SBTs) of the ovary for somatic genetic mutations.•A very small number of mutations are characteristic of SBTs of the ovary.•Novel candidate genes for the pathogenesis of ovarian SBT were identified. Serous borderline tumor (SBT) is a unique histopathologic entity of the ovary, believed to be intermediate between benign cystadenoma and invasive low-grade serous carcinoma. While somatic mutations in the KRAS or BRAF, and rarely ERBB2, genes have been well characterized in SBTs, other genetic alterations have not been described. Toward a more comprehensive understanding of the molecular genetic architecture of SBTs, we undertook whole exome sequencing of this tumor type.OBJECTIVESerous borderline tumor (SBT) is a unique histopathologic entity of the ovary, believed to be intermediate between benign cystadenoma and invasive low-grade serous carcinoma. While somatic mutations in the KRAS or BRAF, and rarely ERBB2, genes have been well characterized in SBTs, other genetic alterations have not been described. Toward a more comprehensive understanding of the molecular genetic architecture of SBTs, we undertook whole exome sequencing of this tumor type.Following pathologic review and laser capture microdissection to enrich for tumor cells, whole exomes were prepared from DNA of two independent SBTs and subjected to massively parallel DNA sequencing.METHODSFollowing pathologic review and laser capture microdissection to enrich for tumor cells, whole exomes were prepared from DNA of two independent SBTs and subjected to massively parallel DNA sequencing.Both tumors contained an activating mutation of the BRAF gene. A total of 15 additional somatic mutations were identified, nine in one tumor and six in the other. Eleven were missense mutations and four were nonsense or deletion mutations. Fourteen of the 16 genes found to be mutated in this study have been reported to be mutated in other cancers. Furthermore, 12 of these genes are mutated in ovarian cancers. The FBXW7 and KIAA1462 genes are noteworthy candidates for a pathogenic role in serous borderline tumorigenesis.RESULTSBoth tumors contained an activating mutation of the BRAF gene. A total of 15 additional somatic mutations were identified, nine in one tumor and six in the other. Eleven were missense mutations and four were nonsense or deletion mutations. Fourteen of the 16 genes found to be mutated in this study have been reported to be mutated in other cancers. Furthermore, 12 of these genes are mutated in ovarian cancers. The FBXW7 and KIAA1462 genes are noteworthy candidates for a pathogenic role in serous borderline tumorigenesis.These findings suggest that a very small number of somatic genetic mutations are characteristic of SBTs of the ovary, thus supporting their classification as a relatively genetically stable tumor type. The mutant genes described herein represent novel candidates for the pathogenesis of ovarian SBT.CONCLUSIONSThese findings suggest that a very small number of somatic genetic mutations are characteristic of SBTs of the ovary, thus supporting their classification as a relatively genetically stable tumor type. The mutant genes described herein represent novel candidates for the pathogenesis of ovarian SBT. AbstractObjectiveSerous borderline tumor (SBT) is a unique histopathologic entity of the ovary, believed to be intermediate between benign cystadenoma and invasive low-grade serous carcinoma. While somatic mutations in the KRAS or BRAF, and rarely ERBB2, genes have been well characterized in SBTs, other genetic alterations have not been described. Toward a more comprehensive understanding of the molecular genetic architecture of SBTs, we undertook whole exome sequencing of this tumor type. MethodsFollowing pathologic review and laser capture microdissection to enrich for tumor cells, whole exomes were prepared from DNA of two independent SBTs and subjected to massively parallel DNA sequencing. ResultsBoth tumors contained an activating mutation of the BRAF gene. A total of 15 additional somatic mutations were identified, nine in one tumor and six in the other. Eleven were missense mutations and four were nonsense or deletion mutations. Fourteen of the 16 genes found to be mutated in this study have been reported to be mutated in other cancers. Furthermore, 12 of these genes are mutated in ovarian cancers. The FBXW7 and KIAA1462 genes are noteworthy candidates for a pathogenic role in serous borderline tumorigenesis. ConclusionsThese findings suggest that a very small number of somatic genetic mutations are characteristic of SBTs of the ovary, thus supporting their classification as a relatively genetically stable tumor type. The mutant genes described herein represent novel candidates for the pathogenesis of ovarian SBT. Serous borderline tumor (SBT) is a unique histopathologic entity of the ovary, believed to be intermediate between benign cystadenoma and invasive low-grade serous carcinoma. While somatic mutations in the KRAS or BRAF, and rarely ERBB2, genes have been well characterized in SBTs, other genetic alterations have not been described. Toward a more comprehensive understanding of the molecular genetic architecture of SBTs, we undertook whole exome sequencing of this tumor type. Following pathologic review and laser capture microdissection to enrich for tumor cells, whole exomes were prepared from DNA of two independent SBTs and subjected to massively parallel DNA sequencing. Both tumors contained an activating mutation of the BRAF gene. A total of 15 additional somatic mutations were identified, nine in one tumor and six in the other. Eleven were missense mutations and four were nonsense or deletion mutations. Fourteen of the 16 genes found to be mutated in this study have been reported to be mutated in other cancers. Furthermore, 12 of these genes are mutated in ovarian cancers. The FBXW7 and KIAA1462 genes are noteworthy candidates for a pathogenic role in serous borderline tumorigenesis. These findings suggest that a very small number of somatic genetic mutations are characteristic of SBTs of the ovary, thus supporting their classification as a relatively genetically stable tumor type. The mutant genes described herein represent novel candidates for the pathogenesis of ovarian SBT.
Author	Boyd, Jeff Forsythe, Caitlin Peri, Suraj Hughes, Lucinda Luo, Biao Wu, Hong Wirchansky, Beth
AuthorAffiliation	a Cancer Genome Institute, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111, USA d Biostatistics and Bioinformatics Core Facility, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111 USA c Department of Pathology, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111, USA b Cancer Biology Program, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111, USA
AuthorAffiliation_xml	– name: d Biostatistics and Bioinformatics Core Facility, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111 USA – name: c Department of Pathology, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111, USA – name: a Cancer Genome Institute, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111, USA – name: b Cancer Biology Program, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111, USA
Author_xml	– sequence: 1 givenname: Jeff surname: Boyd fullname: Boyd, Jeff email: jeff.boyd@fccc.edu organization: Cancer Genome Institute, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111, USA – sequence: 2 givenname: Biao surname: Luo fullname: Luo, Biao organization: Cancer Genome Institute, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111, USA – sequence: 3 givenname: Suraj surname: Peri fullname: Peri, Suraj organization: Biostatistics and Bioinformatics Core Facility, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111 USA – sequence: 4 givenname: Beth surname: Wirchansky fullname: Wirchansky, Beth organization: Cancer Genome Institute, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111, USA – sequence: 5 givenname: Lucinda surname: Hughes fullname: Hughes, Lucinda organization: Cancer Genome Institute, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111, USA – sequence: 6 givenname: Caitlin surname: Forsythe fullname: Forsythe, Caitlin organization: Cancer Genome Institute, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111, USA – sequence: 7 givenname: Hong surname: Wu fullname: Wu, Hong organization: Department of Pathology, Fox Chase Cancer Center, 333 Cottman Ave., Philadelphia, PA 19111, USA
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Snippet	Serous borderline tumor (SBT) is a unique histopathologic entity of the ovary, believed to be intermediate between benign cystadenoma and invasive low-grade... AbstractObjectiveSerous borderline tumor (SBT) is a unique histopathologic entity of the ovary, believed to be intermediate between benign cystadenoma and...
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SubjectTerms	Cell Adhesion Molecules - genetics Cell Cycle Proteins - genetics Cell Transformation, Neoplastic - genetics Cystadenoma, Serous - genetics Exome Exome - genetics F-Box Proteins - genetics F-Box-WD Repeat-Containing Protein 7 Female Gene Hematology, Oncology, and Palliative Medicine High-Throughput Nucleotide Sequencing Humans Middle Aged Mutation Mutation, Missense Obstetrics and Gynecology Ovarian Ovarian Neoplasms - genetics Proto-Oncogene Proteins B-raf - genetics Sequence Analysis, DNA Sequence Deletion Serous borderline tumor Ubiquitin-Protein Ligases - genetics
Title	Whole exome sequence analysis of serous borderline tumors of the ovary
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