28 results on '"Lee, Cheng Han"'
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2. Targeted RNA Sequencing Highlights a Diverse Genomic and Morphologic Landscape in Low-grade Endometrial Stromal Sarcoma, Including Novel Fusion Genes
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Kolin, David L., Nucci, Marisa R., Turashvili, Gulisa, Song, Sharon J., Corbett-Burns, Sophie, Cesari, Matthew, Chang, Martin C., Clarke, Blaise, Demicco, Elizabeth, Dube, Valerie, Lee, Cheng-Han, Rouzbahman, Marjan, Shaw, Patricia, Cin, Paola Dal, Swanson, David, and Dickson, Brendan C.
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- 2023
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3. Ectomesenchymal Chondromyxoid Tumor
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Dickson, Brendan C, Antonescu, Cristina R, Argyris, Prokopios P, Bilodeau, Elizabeth A, Bullock, Martin J, Freedman, Paul D, Gnepp, Douglas R, Jordan, Richard C, Koutlas, Ioannis G, Lee, Cheng-Han, Leong, Iona, Merzianu, Mihai, Purgina, Bibianna M, Thompson, Lester DR, Wehrli, Bret, Wright, John M, Swanson, David, Zhang, Lei, and Bishop, Justin A
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Biomedical and Clinical Sciences ,Clinical Sciences ,Clinical Research ,Genetics ,Human Genome ,Cancer ,Aetiology ,2.1 Biological and endogenous factors ,Actins ,Adolescent ,Adult ,Biomarkers ,Tumor ,DNA-Binding Proteins ,Desmin ,Female ,Gene Fusion ,Genetic Predisposition to Disease ,Glial Fibrillary Acidic Protein ,Humans ,Immunohistochemistry ,In Situ Hybridization ,Fluorescence ,Keratins ,Male ,Middle Aged ,Neoplasms ,Connective and Soft Tissue ,Phenotype ,Retrospective Studies ,S100 Proteins ,Sequence Analysis ,RNA ,Tongue Neoplasms ,Transcription Factors ,Young Adult ,ectomesenchymal chondromyxoid tumor ,tongue ,gene rearrangement ,RREB1 ,MKL2 ,EWSR1 ,CREM ,Pathology ,Clinical sciences - Abstract
Ectomesenchymal chondromyxoid tumor is a rare and benign neoplasm with a predilection for the anterior dorsal tongue. Despite morphologic heterogeneity, most cases are characterized by a proliferation of bland spindle cells with a distinctive reticular growth pattern and myxoid stroma. The immunophenotype of these neoplasms is likewise variable; most cases express glial fibrillary acid protein and S100 protein, with inconsistent reports of keratin and myoid marker expression. The molecular pathogenesis is poorly understood; however, a subset of cases has been reported to harbor EWSR1 gene rearrangement. Following identification of an RREB1-MKL2 fusion gene by RNA Sequencing in an index patient, a retrospective review of additional cases of ectomesenchymal chondromyxoid tumors was performed to better characterize the clinical, immunohistochemical, and molecular attributes of this neoplasm. A total of 21 cases were included in this series. A marked predisposition for the dorsal tongue was confirmed. Most cases conformed to prior morphologic descriptions; however, hypercellularity, hyalinized stroma, and necrosis were rare attributes not previously emphasized. The neoplastic cells frequently coexpressed glial fibrillary acid protein, S100 protein, keratin, smooth muscle actin, and/or desmin; a single case was found to contain significant myogenin expression. An RREB1-MKL2 fusion product was identified in 19 tumors (90%), a single tumor (5%) had an EWSR1-CREM fusion product, and the remaining case lacked any known fusion gene by RNA Sequencing. The latter 2 cases subtly differed morphologically from many in the cohort. This series illustrates that recurrent RREB1-MKL2 fusions occur in most, perhaps all, cases of ectomesenchymal chondromyxoid tumor.
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- 2018
4. Pleural Malignant Mesotheliomas Do Not Demonstrate SWItch/Sucrose Nonfermentable (SWI/SNF) Complex Deficiency
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Ren, He Zhen, Tessier-Cloutier, Basile, Naso, Julia R., Koebel, Martin, Lee, Cheng-Han, and Churg, Andrew
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- 2021
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5. Novel PLAG1 Gene Rearrangement Distinguishes a Subset of Uterine Myxoid Leiomyosarcoma From Other Uterine Myxoid Mesenchymal Tumors
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Arias-Stella, Javier A., III, Benayed, Ryma, Oliva, Esther, Young, Robert H., Hoang, Lien N., Lee, Cheng-Han, Jungbluth, Achim A., Frosina, Denise, Soslow, Robert A., Antonescu, Cristina R., Ladanyi, Marc, and Chiang, Sarah
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- 2019
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6. ALK Is a Specific Diagnostic Marker for Inflammatory Myofibroblastic Tumor of the Uterus
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Mohammad, Nissreen, Haimes, Josh D., Mishkin, Skyler, Kudlow, Brian A., Leong, May Ying, Chew, Sung Hock, Koay, Eleanor, Whitehouse, Ann, Cope, Nichola, Ali, Rola H., Köbel, Martin, Stewart, Colin J.R., McCluggage, W. Glenn, and Lee, Cheng-Han
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- 2018
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7. Ectomesenchymal Chondromyxoid Tumor: A Neoplasm Characterized by Recurrent RREB1-MKL2 Fusions
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Dickson, Brendan C., Antonescu, Cristina R., Argyris, Prokopios P., Bilodeau, Elizabeth A., Bullock, Martin J., Freedman, Paul D., Gnepp, Douglas R., Jordan, Richard C., Koutlas, Ioannis G., Lee, Cheng-Han, Leong, Iona, Merzianu, Mihai, Purgina, Bibianna M., Thompson, Lester D.R., Wehrli, Bret, Wright, John M., Swanson, David, Zhang, Lei, and Bishop, Justin A.
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- 2018
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8. Molecular Profiling of Hyalinizing Clear Cell Carcinomas Revealed a Subset of Tumors Harboring a Novel EWSR1-CREM Fusion: Report of 3 Cases
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Chapman, Erin, Skalova, Alena, Ptakova, Nikola, Martinek, Petr, Goytain, Angela, Tucker, Tracy, Xiong, Wei, Leader, Mary, Kudlow, Brian A., Haimes, Josh D., Hayes, Malcolm M., Bohus, Peter, Miesbauerova, Marketa, Lee, Cheng-Han, and Ng, Tony L.
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- 2018
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9. BCOR Internal Tandem Duplication in High-grade Uterine Sarcomas
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Mariño-Enriquez, Adrián, Lauria, Alexandra, Przybyl, Joanna, Ng, Tony L., Kowalewska, Magdalena, Debiec-Rychter, Maria, Ganesan, Raji, Sumathi, Vaiyapuri, George, Suzanne, McCluggage, W. Glenn, Nucci, Marisa R., Lee, Cheng-Han, and Fletcher, Jonathan A.
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- 2018
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10. Undifferentiated Endometrial Carcinomas Show Frequent Loss of Core Switch/Sucrose Nonfermentable Complex Proteins
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Köbel, Martin, Hoang, Lien N., Tessier-Cloutier, Basile, Meng, Bo, Soslow, Robert A., Stewart, Colin J.R., and Lee, Cheng-Han
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- 2018
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11. Interobserver Agreement in Endometrial Carcinoma Histotype Diagnosis Varies Depending on The Cancer Genome Atlas (TCGA)-based Molecular Subgroup
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Hoang, Lien N., Kinloch, Mary A., Leo, Joyce M., Grondin, Katherine, Lee, Cheng-Han, Ewanowich, Carol, Köbel, Martin, Cheng, Angela, Talhouk, Aline, McConechy, Melissa, Huntsman, David G., McAlpine, Jessica N., Soslow, Robert A., and Gilks, C. Blake
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- 2017
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12. Recurrent KAT6B/A::KANSL1Fusions Characterize a Potentially Aggressive Uterine Sarcoma Morphologically Overlapping With Low-grade Endometrial Stromal Sarcoma
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Agaimy, Abbas, Clarke, Blaise A., Kolin, David L., Lee, Cheng-Han, Lee, Jen-Chieh, McCluggage, W. Glenn, Pöschke, Patrik, Stoehr, Robert, Swanson, David, Turashvili, Gulisa, Beckmann, Matthias W., Hartmann, Arndt, Antonescu, Cristina R., and Dickson, Brendan C.
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With the widespread application of next-generation sequencing, the genetic landscape of uterine mesenchymal neoplasms has been evolving rapidly to include several recently identified fusion genes. Although chromosomal rearrangements involving the 10q22 and 17q21.31 loci have been reported in occasional uterine leiomyomas decades ago, the corresponding KAT6B::KANSL1fusion has been only recently identified in 2 uterine tumors diagnosed as leiomyoma and leiomyosarcoma. We herein describe 13 uterine stromal neoplasms carrying a KAT6B::KANSL1(n=11) and KAT6A::KANSL1(n=2) fusion. Patient ages ranged from 33 to 81 years (median, 49 y). Tumor size was 2.6 to 23.5 cm (median, 8.2 cm). Nine tumors were myometrium-centered, and 3 had an intracavitary component. Original diagnoses were mostly low-grade endometrial stromal sarcoma (LG-ESS; 10 cases) with atypical features (limited CD10 expression, sex cord-like features, pericytic vasculature, and frequent myxoid changes). Treatment was hysterectomy±bilateral salpingo-oophorectomy (10), myomectomy (1), and curettage (2). Five patients were disease-free at 6 to 34 months, 3 (27%) died of disease at 2 to 47 months, and 3 were alive with disease at 2, 17, and 17 years. Histologically, most tumors showed variable overlap with LG-ESS, but they were generally well-circumscribed lacking the extensive permeative and angioinvasive growth typical of LG-ESS. They were composed of monotonous medium-sized oval and spindle cells arranged into diffuse sheets with prominent spiral-type arterioles and frequent pericytoma-like vascular pattern. Variable myxoid stromal changes were frequent. Mitotic activity ranged from 1 to >20 in 10 HPFs. Immunohistochemistry showed variable expression of CD10 (12/13), estrogen receptor (8/11), progesterone receptor (8/11), smooth muscle actin (9/11), desmin (4/12), h-caldesmon (2/10), calretinin (3/8), inhibin (1/7), WT1 (4/7), cyclin D1 (5/11; diffuse in only 1 case), and pankeratin (5/10). This series characterizes a KAT6B/A::KANSL1fusion-positive uterine stromal neoplasm within the morphologic spectrum of LG-ESS but with atypical features. The relationship of these neoplasms to genuine LG-ESS remains unclear. This molecular subtype of uterine endometrial stromal sarcoma has the potential for an unfavorable clinical course despite the absence of widely invasive growth; nevertheless, analysis of more cases is necessary to delineate the phenotypic spectrum and biological potential of this tumor.
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- 2022
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13. Endometrial Stromal Sarcomas With BCORInternal Tandem Duplication and Variant BCOR/BCORL1Rearrangements Resemble High-grade Endometrial Stromal Sarcomas With Recurrent CDK4Pathway Alterations and MDM2Amplifications
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Kommoss, Felix K.F., Chiang, Sarah, Köbel, Martin, Koelsche, Christian, Chang, Kenneth Tou-En, Irving, Julie A., Dickson, Brendan, Thiryayi, Sakinah, Rouzbahman, Marjan, Rasty, Golnar, von Deimling, Andreas, Lee, Cheng-Han, and Turashvili, Gulisa
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The distinction between low-grade and high-grade endometrial stromal sarcomas (LGESS, HGESS) is increasingly defined by genetics. Recently, variant genomic alterations involving BCORor BCORL1have been reported in endometrial stromal sarcoma (ESS), although it remains unclear whether these justify a diagnosis of LGESS or HGESS. In this study, we describe clinicopathologic and molecular features of ESS with such alterations to help clarify their classification in the spectrum of ESS. We collected a cohort of 13 ESS harboring variant alteration involving BCOR(6 with internal tandem duplication, 1 with EP300::BCORfusion, 1 with BCOR::LPPfusion) and BCORL1 (4 with JAZF1::BCORL1fusion, 1 with EPC1::BCORL1fusion). The median patient age at primary diagnosis was 51 years (range: 18 to 70 y). Median tumor size at primary diagnosis was 9.3 cm (range: 4.5 to 21 cm), and extrauterine disease spread (stage IIIB-C) was present in 27%. The tumors were composed of round to spindled cells with cellularity and cytologic atypia ranging from mild to marked and a median mitotic count of 18/10 HPFs (range: 2 to 85/10 HPFs). At least focally myopermeative growth was noted in 8/8 assessable cases. Of 12 patients with follow-up data (median: 25 mo), 4 patients died of disease and 3 were alive with recurrent disease. Unsupervised hierarchical clustering of DNA methylation data together with a large cohort of uterine mesenchymal tumors that included YWHAE::NUTM2and ZC3H7B::BCORHGESS and molecularly confirmed LGESS revealed a common methylation signature for all ESS with variant BCORand BCORL1alterations and HGESS with YWHAE::NUTM2and ZC3H7B::BCORgene fusion. Copy number analysis revealed amplifications of CDK4and MDM2, as well as homozygous deletions of CDKN2A/Band NF1in a subset of tumors. Our results indicate that ESS with BCORinternal tandem duplication and variant BCORand BCORL1rearrangements clinically and molecularly resemble conventional HGESS.
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- 2022
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14. Accurate Distinction of Ovarian Clear Cell From Endometrioid Carcinoma Requires Integration of Phenotype, Immunohistochemical Predictions, and Genotype
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Rodriguez, Monica, Kang, Eun Young, Farrington, Kyo, Cook, Linda S., Le, Nhu D., Karnezis, Anthony N., Lee, Cheng-Han, Nelson, Gregg S., Terzic, Tatjana, Lee, Sandra, and Köbel, Martin
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Supplemental Digital Content is available in the text.Ovarian clear cell carcinoma (OCCC) and ovarian endometrioid carcinoma (OEC) are both associated with endometriosis but differ in histologic phenotype, biomarker profile, and survival. Our objectives were to refine immunohistochemical (IHC) panels that help distinguish the histotypes and reassess the prevalence of mismatch repair deficiency (MMRd) in immunohistochemically confirmed OCCC. We selected 8 candidate IHC markers to develop first-line and second-line panels in a training set of 344 OCCC/OEC cases. Interobserver reproducibility of histotype diagnosis was assessed in an independent testing cohort of 100 OCC/OEC initially without and subsequently with IHC. The prevalence of MMRd was evaluated using the testing cohort and an expansion set of 844 ovarian carcinomas. The 2 prototypical combinations (OCCC: Napsin A+/HNF1B diffusely+/PR−; OEC: Napsin A−/HNF1B nondiffuse/PR+) occurred in 75% of cases and were 100% specific. A second-line panel (ELAPOR1, AMACR, CDX2) predicted the remaining cases with 83% accuracy. Integration of IHC improved interobserver reproducibility (κ=0.778 vs. 0.882, P<0.0001). The prevalence of MMRd was highest in OEC (11.5%, 44/383), lower in OCCC (1.7%, 5/297), and high-grade serous carcinomas (0.7%, 5/699), and absent in mucinous (0/126) and low-grade serous carcinomas (0/50). All 5 MMRd OCCC were probable Lynch syndrome cases with prototypical IHC profile but ambiguous morphologic features: 3/5 with microcystic architecture and 2/5 with intratumoral stromal inflammation. Integration of first-line and second-line IHC panels increases diagnostic precision and enhances prognostication and triaging for predisposing/predictive molecular biomarker testing. Our data support universal Lynch syndrome screening in all patients with OEC when the diagnosis of other histotypes has been vigorously excluded.
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- 2021
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15. Clinicopathologic Characterization of GREB1-rearranged Uterine Sarcomas With Variable Sex-Cord Differentiation
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Lee, Cheng-Han, Kao, Yu-Chien, Lee, Wan-Ru, Hsiao, Yi-Wen, Lu, Tzu-Pin, Chu, Chia-Ying, Lin, Yi-Jia, Huang, Hsuan-Ying, Hsieh, Tsung-Han, Liu, Yun-Ru, Liang, Cher-Wei, Chen, Tom Wei-Wu, Yip, Stephen, Lum, Amy, Kuo, Kuan-Ting, Jeng, Yung-Ming, Yu, Shih-Chen, Chung, Yung-Chuan, and Lee, Jen-Chieh
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Supplemental Digital Content is available in the text.Uterine mesenchymal tumors are genetically heterogenous; those with uniform cytomorphology, best exemplified by endometrial stromal tumors, often contain various fusion genes. Novel fusions involving ESR1and GREB1, key factors in sex hormone pathways, have been implicated in rare uterine mesenchymal tumors. Particularly, the fusions between 5′-ESR1/GREB1and 3′-NCOA2/NCOA3were recently identified in 4 uterine tumors resembling ovarian sex-cord tumor (UTROSCT). By RNA sequencing, pathology review, and FISH screening, we identified 4 uterine sarcomas harboring rearranged GREB1, including GREB1-NCOA2and the novel GREB1-NR4A3, GREB1-SS18, and GREB1-NCOA1, validated by RT-PCR and/or FISH. They occurred in the myometrium of postmenopausal women and were pathologically similar despite minor differences. Tumor cells were generally uniform and epithelioid, with vesicular nuclei and distinct to prominent nucleoli. Growth patterns included solid sheets, trabeculae/cords, nests, and fascicles. Only 1 tumor showed small foci of definitive sex-cord components featuring well-formed tubules, retiform structures, Leydig-like cells, and lipid-laden cells and exhibiting convincing immunoreactivity to sex-cord markers (calretinin, α-inhibin, and Melan-A). In contrast, all the 4 classic UTROSCT we collected occurred in premenopausal patients, consisted predominantly of unequivocal sex-cord elements, prominently expressed multiple sex-cord markers, and harbored ESR1-NCOA3fusion. Combined with previously reported cases, GREB1-rearranged tumors involved significantly older women (P=0.001), tended to be larger and more mitotically active, showed more variable and often inconspicuous sex-cord differentiation, and appeared to behave more aggressively than ESR1-rearranged UTROSCT. Therefore, these 2 groups of tumors might deserve separate consideration, despite some overlapping features and the possibility of belonging to the same disease spectrum.
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- 2019
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16. Novel PLAG1Gene Rearrangement Distinguishes a Subset of Uterine Myxoid Leiomyosarcoma From Other Uterine Myxoid Mesenchymal Tumors
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Arias-Stella, Javier A., Benayed, Ryma, Oliva, Esther, Young, Robert H., Hoang, Lien N., Lee, Cheng-Han, Jungbluth, Achim A., Frosina, Denise, Soslow, Robert A., Antonescu, Cristina R., Ladanyi, Marc, and Chiang, Sarah
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Genetic alterations in uterine myxoid leiomyosarcoma are unknown. We investigate the clinicopathologic features of 19 uterine tumors previously diagnosed as myxoid leiomyosarcomas in which tumoral RNA was subjected to targeted RNA sequencing. PLAG1, BCOR, BCORL1, HMGA2, and ALKbreak-apart fluorescence in situ hybridization (FISH) and BCOR, PLAG1, and ALK immunohistochemistry were performed in cases which failed or lacked fusions by sequencing. The diagnosis of myxoid leiomyosarcoma was confirmed in 15 cases after exclusion of 4 tumors with BCORand ALKrearrangements. These 15 patients presented at a median age of 50 years with stage I (3), II (2), III (2), and IV (1) tumors, respectively; stage was unknown in 7 cases. Tumor size ranged from 10 to 24 cm. Matrix was myxoid in all tumors and also eosinophilic in 2. Cells were spindled, epithelioid, and both in 10, 2, and 3 tumors and showed mild, moderate, and severe nuclear atypia in 3, 8, and 4 tumors, respectively. Mitotic index ranged from <1 to 14/10 HPF, while tumor necrosis was present in 6 (40%). Novel TRPS1-PLAG1or RAD51B-PLAG1fusions were detected by sequencing in 4 tumors, 3 of which were also confirmed by FISH. Diffuse PLAG1 expression was seen in 7 tumors, including 4 with PLAG1rearrangement. No morphologic differences were seen among PLAG1fusion-positive and fusion-negative tumors. No PLAG1, HMGA2, ALK, BCOR, or BCORL1rearrangements were detected by FISH in 11 tumors. On the basis of sequencing and FISH results, PLAG1rearrangements resulting in PLAG1 expression underpin ~25% of myxoid leiomyosarcomas and may serve as a useful diagnostic biomarker. Immunohistochemistry, targeted RNA sequencing, and/or FISH may distinguish myxoid leiomyosarcoma from its morphologic mimics.
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- 2019
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17. BCORInternal Tandem Duplication in High-grade Uterine Sarcomas
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Mariño-Enriquez, Adrián, Lauria, Alexandra, Przybyl, Joanna, Ng, Tony L., Kowalewska, Magdalena, Debiec-Rychter, Maria, Ganesan, Raji, Sumathi, Vaiyapuri, George, Suzanne, McCluggage, W. Glenn, Nucci, Marisa R., Lee, Cheng-Han, and Fletcher, Jonathan A.
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Endometrial stromal sarcomas (ESSs) are mesenchymal uterine tumors characterized by recurrent genetic events, most commonly chromosomal rearrangements, that create oncogenic gene fusions. High-grade endometrial stromal sarcomas (HG-ESSs), as defined in the 2014 World Health Organization Classification, typically contain oncogenic YWHAE-NUTM2fusions; however, although not well characterized, there are tumors morphologically overlapping with HG-ESS that do not contain the YWHAE-NUTM2fusions. These fusions are also found in certain pediatric primitive sarcomas, including clear cell sarcoma of the kidney and soft tissue undifferentiated round cell sarcoma of infancy. A subset of these same pediatric sarcomas lack YWHAE-NUTM2fusions and instead have internal tandem duplications (ITDs) involving exon 15 of BCOR(BCORITD). We investigated the presence of BCORITD by targeted sequencing in a series of 31 uterine sarcomas, comprising 5 low-grade ESS, 13 uterine sarcomas diagnosed as HG-ESS, and 13 undifferentiated uterine sarcomas. BCORITD were present in 1 uterine sarcoma diagnosed as HG-ESS and 2 undifferentiated sarcomas with uniform nuclear features, all of which lacked any of the recurrent chromosome translocations known to occur in ESS. These 3 high-grade sarcomas with BCORITD affected young patients (average age, 24) and morphologically were composed of nonpleomorphic spindle cells admixed with epithelioid and round cell areas. Focal myxoid stroma was present in 2 cases. Mitotic activity was brisk, necrosis was present, and there was lymphovascular involvement in all cases. The 3 uterine sarcomas with BCORITD exhibited diffuse cyclin D1 immunohistochemical expression and there was diffuse BCOR expression in the 2 cases tested. Long-term follow-up in 2 patients revealed 1 to be tumor-free after 22 years and the other to die of disease after 8 years. In conclusion, BCORITD is an oncogenic alternative to YWHAE-NUTM2fusion in high-grade uterine sarcomas with uniform nuclear features. We propose that neoplasms with the morphology described and BCORITD be regarded as a unique subtype of high-grade uterine sarcoma, possibly within the family of endometrial stromal neoplasia.
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- 2018
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18. Undifferentiated and Dedifferentiated Endometrial Carcinomas With POLEExonuclease Domain Mutations Have a Favorable Prognosis
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Espinosa, Iñigo, Lee, Cheng-Han, D’Angelo, Emanuela, Palacios, José, and Prat, Jaime
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POLEexonuclease domain mutations have recently been described in undifferentiated endometrial carcinoma but, because of the rarity of this aggressive type of endometrial cancer, their prognostic significance is unknown. We have analyzed the immunophenotype (ARID1A, MLH1, PMS2, MSH2, MSH6, p53, β-catenin, and SMARCB1) and mutational status (POLE, PIK3CA, and PTEN) of 21 undifferentiated carcinomas (8 undifferentiated and 13 dedifferentiated carcinomas). Loss of ARID1A expression was observed in 9 of 19 cases (47%), loss of expression of at least 1 DNA mismatch repair protein in 7 (7/21; 33%), and p53 immunoreaction was aberrant (mutated/inactivated) in 11 cases (11/21; 52%). All tumors were negative for β-catenin. Normal nuclear SMARCB1 (INI1) staining was found in all but 1 dedifferentiated case. Two undifferentiated and 7 dedifferentiated carcinomas showed POLEexonuclease domain mutations (9/21; 42%). PIK3CAmutations occurred in six tumors (6/21; 28%) (2 undifferentiated and 4 dedifferentiated carcinomas). PTENmutations were found in 7 of 15 cases (47%) (4 undifferentiated and 3 dedifferentiated carcinomas). POLE-mutated undifferentiated and dedifferentiated endometrial carcinomas were more frequently stage I tumors than similar carcinomas lacking exonuclease domain mutations (7/9; 78% vs. 3/12; 25%; P=0.023) and patients had significantly better outcome (disease-specific survival) than those without POLEexonuclease domain mutations (P=0.02). Determination of the POLEmutation status is important for the management of these patients.
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- 2017
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19. Uterine Inflammatory Myofibroblastic Tumors Frequently Harbor ALKFusions With IGFBP5and THBS1
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Haimes, Josh D., Stewart, Colin J.R., Kudlow, Brian A., Culver, Brady P., Meng, Bo, Koay, Eleanor, Whitehouse, Ann, Cope, Nichola, Lee, Jen-Chieh, Ng, Tony, McCluggage, W. Glenn, and Lee, Cheng-Han
- Abstract
Supplemental Digital Content is available in the text.Inflammatory myofibroblastic tumor (IMT) can occur in a number of anatomic sites, including the uterus. Like its soft tissue counterpart, uterine IMT frequently expresses ALK and harbors ALKgenetic rearrangements. The aim of this study is to fully characterize the genetic fusions that occur in uterine IMT. We studied 11 uterine IMTs with typical histology and 8 uterine myxoid smooth muscle tumors (5 leiomyomas, 1 smooth muscle tumor of uncertain malignant potential, and 2 leiomyosarcomas) in which the differential of IMT was considered, using a RNA-sequencing–based fusion assay to detect genetic fusions involving ALK, ROS1, RET, NTRK1/3, and other genes. ALK was expressed in 10 of 11 IMTs and 1 tumor initially categorized as a myxoid leiomyoma (granular cytoplasmic staining with paranuclear accentuation). Fusion transcripts involving ALKwere identified in 9 of 10 ALK immunopositive IMTs, with 3 harboring IGFBP5-ALK, 3 harboring THBS1-ALK, 2 harboring FN1-ALK, and 1 harboring TIMP3-ALK. Among the smooth muscle tumors, IGFBP5-ALKfusion transcript was identified in only 1 ALK immunopositive case. Further review revealed that although a diagnosis of IMT was considered for the ALK immunopositive myxoid leiomyoma, this diagnosis was not initially rendered only because fluorescence in situ hybridization analysis was interpreted as negative for ALKgenetic rearrangement; this case is best reclassified as an IMT. Notably, all the ALKfusions identified in our study included the transmembrane domain-encoding exon 19 of ALK. Our findings confirm the high frequency of ALKfusions in uterine IMT, with an enrichment of novel 5′ ALKfusion partners (IGFBP5, THBS1, and TIMP3) and exon 19-containing ALKfusion. Given that IGFBP5and FN1are both situated on the same chromosome as ALK, fluorescence in situ hybridization analysis for ALKrearrangement may not be reliable and a negative result should not exclude a diagnosis of uterine IMT if the histologic features and ALK immunostaining findings are supportive.
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- 2017
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20. ETV6-NTRK3 Is Expressed in a Subset of ALK-Negative Inflammatory Myofibroblastic Tumors
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Alassiri, Ali H., Ali, Rola H., Shen, Yaoqing, Lum, Amy, Strahlendorf, Caron, Deyell, Rebecca, Rassekh, Rod, Sorensen, Poul H., Laskin, Janessa, Marra, Marco, Yip, Stephen, Lee, Cheng-Han, and Ng, Tony L.
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Supplemental Digital Content is available in the text.Inflammatory myofibroblastic tumor (IMT) is a genetically heterogenous tumor of the viscera and soft tissues, with multiple molecular features having been demonstrated in this tumor type. About 50% of cases harbor an anaplastic lymphoma kinase (ALK) gene rearrangement, and recent studies have described novel fusions involving the ROS1and PDGFRβgenes in a subset of ALK-negative cases. However, the molecular features of the remaining subset of cases are not yet defined. We report a case of a large, highly aggressive IMT of the lung in a 17-year-old girl. This case was molecularly characterized through whole-genome and transcriptome sequencing. Subsequently, we investigated a cohort of 15 ALK-negative IMTs of various anatomic sites. All cases were screened using fluorescence in situ hybridization (FISH) for rearrangement of the ETV6locus and with reverse transcription polymerase chain reaction (RT-PCR) for the ETV6-NTRK3 fusion transcript. Whole-genome and transcriptome sequencing revealed an ETV6-NTRK3 fusion transcript in our index case. This was confirmed by FISH studies for ETV6gene rearrangement, as well as by RT-PCR. In addition, 2 additional cases in our cohort demonstrated ETV6rearrangement by FISH. The presence of ETV6-NTRK3 fusion transcript was demonstrated by RT-PCR in one of these additional cases. In summary, we demonstrate the expression of the ETV6-NTRK3 fusion oncogene in a small subset of IMTs, lending further support to the role of oncogenic tyrosine kinases in the pathophysiology of this tumor type. Our data also further expand the growing spectrum of tumor types expressing the ETV6-NTRK3 fusion.
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- 2016
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21. Primary Pseudomyogenic Hemangioendothelioma of Bone
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Inyang, Alero, Mertens, Fredrik, Puls, Florian, Sumathi, Vaiyapuri, Inwards, Carrie, Folpe, Andrew, Lee, Cheng-Han, Zhang, Yaxia, Symmans, Pennie, Rubin, Brian, Nielsen, Gunnlaugur P., Nguyen, Van-Hung, and Rosenberg, Andrew E.
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Pseudomyogenic hemangioendothelioma (PMH) is a well-recognized neoplasm that usually arises in the soft tissue; concurrent bone involvement occurs in 24% of cases. PMH of bone without soft tissue involvement is rare. We describe the clinicopathologic findings of 10 such cases, the largest series reported to date. The study included 9 male and 1 female patient; their ages ranged from 12 to 74 years (mean 36.7 y). All patients had multiple tumors with a distinct regional distribution: 45% restricted to the lower extremity; 25% to the spine and pelvis; and 15% to the upper extremity. On imaging studies the tumors were well circumscribed and lytic. The neoplasms were composed of spindled cells arranged in intersecting fascicles with scattered epithelioid cells; epithelioid cells predominated in 3 cases. The neoplastic cells contained abundant densely eosinophilic cytoplasm and vesicular nuclei. There was limited cytologic atypia and necrosis, few mitoses (0 to 2/10 high-power fields), and inconspicuous stroma. Unique findings included abundant intratumoral reactive woven bone and hemorrhage with numerous osteoclast-like giant cells. Immunohistochemically, most tumors were positive for keratin, ERG, and CD31; CD34 was negative. The balanced t(7:19)(q22;13) translocation was documented in 3 cases. Follow-up is limited, but no patient developed documented visceral dissemination, and all have stable or progressive osseous disease. PMH exclusively involving bone is rare. It is multicentric, often involves the lower extremity, and has unusual morphology. The differential diagnosis includes epithelioid vascular neoplasms, giant cell tumor, bone forming neoplasms, and metastatic carcinoma. Because of its rarity, unusual presentation, and morphology, accurate diagnosis can be challenging.
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- 2016
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22. Molecular Analysis of Mixed Endometrial Carcinomas Shows Clonality in Most Cases
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Köbel, Martin, Meng, Bo, Hoang, Lien N., Almadani, Noorah, Li, Xiaodong, Soslow, Robert A., Gilks, C. Blake, and Lee, Cheng-Han
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Mixed endometrial carcinoma refers to a tumor that comprises 2 or more distinct histotypes. We studied 18 mixed-type endometrial carcinomas—11 mixed serous and low-grade endometrioid carcinomas (SC/EC), 5 mixed clear cell and low-grade ECs (CCC/EC), and 2 mixed CCC and SCs (CCC/SC), using targeted next-generation sequencing and immunohistochemistry to compare the molecular profiles of the different histotypes present in each case. In 16 of 18 cases there was molecular evidence that both components shared a clonal origin. Eight cases (6 EC/SC, 1 EC/CCC, and 1 SC/CCC) showed an SC molecular profile that was the same in both components. Five cases (3 CCC/EC and 2 SC/EC) showed a shared endometrioid molecular profile and identical mismatch-repair protein deficiency in both components. A single SC/EC case harbored the same POLEexonuclease domain mutation in both components. One SC/CCC and 1 EC/CCC case showed both shared and unique molecular features in the 2 histotype components, suggesting early molecular divergence from a common clonal origin. In 2 cases, there were no shared molecular features, and these appear to be biologically unrelated synchronous tumors. Overall, these results show that the different histologic components in mixed endometrial carcinomas typically share the same molecular aberrations. Mixed endometrial carcinomas most commonly occur through morphologic mimicry, whereby tumors with serous-type molecular profile show morphologic features of EC or CCC, or through underlying deficiency in DNA nucleotide repair, with resulting rapid accrual of mutations and intratumoral phenotypic heterogeneity. Less commonly, mixed endometrial carcinomas are the result of early molecular divergence from a common progenitor clone or are synchronous biologically unrelated tumors (collision tumors).
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- 2016
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23. Microcystic Stromal Tumor
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Irving, Julie A., Lee, Cheng-Han, Yip, Stephen, Oliva, Esther, McCluggage, W. Glenn, and Young, Robert H.
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Since our first description of the microcystic stromal tumor (MST) of the ovary, a rare and distinctive neoplasm with a definitional, usually striking microcystic pattern and a CD10+/vimentin+/inhibin−/calretinin−immunophenotype, 3 examples with β-catenin nuclear localization, and CTNNB1mutation have been reported. We undertook a detailed immunohistochemical study and molecular analysis of CTNNB1and FOXL2of 15 cases of MST to further characterize this neoplasm and establish its histogenesis. Diffuse nuclear staining for FOXL2, WT-1, cyclin D1, and β-catenin was present in all tumors tested, and 12/15 were positive for steroidogenic factor-1 (SF-1). Heterozygous missense point mutations in exon 3 of CTNNB1were detected in 8 of 14 cases, resulting in amino acid changes at codons 32, 34, 35, and 37. There was no correlation between CTNNB1exon 3 mutation status and tumor immunophenotype. All 14 cases tested showed wild-type FOXL2. Our study establishes that MST of the ovary exhibits a characteristic FOXL2/SF-1/WT-1/cyclin D1/nuclear β-catenin–positive immunohistochemical profile, which may be useful in diagnosis and in the exclusion of histologic mimics. The presence of diffuse nuclear FOXL2 and WT-1 immunostaining in all cases and SF-1 in most supports the classification of MST within the sex cord-stromal category. Aberrant nuclear β-catenin expression, detected in all MSTs, appears to be the result of stabilizing CTNNB1mutations in 57% of cases, providing further evidence that dysregulation of the Wnt/B-catenin pathway is involved in the tumorigenesis of MST and may involve activation of β-catenin with upregulation of cyclin D1.
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- 2015
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24. Histotype-Genotype Correlation in 36 High-grade Endometrial Carcinomas
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Hoang, Lien N., McConechy, Melissa K., Köbel, Martin, Han, Guangming, Rouzbahman, Marjan, Davidson, Ben, Irving, Julie, Ali, Rola H., Leung, Sam, McAlpine, Jessica N., Oliva, Esther, Nucci, Marisa R., Soslow, Robert A., Huntsman, David G., Gilks, C. Blake, and Lee, Cheng-Han
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Endometrioid, serous, and clear cell carcinomas are the major types of endometrial carcinoma. Histologic distinction between these different tumor types can be difficult in high-grade cases, in which significant interobserver diagnostic disagreement exists. Endometrioid and clear cell carcinomas frequently harbor ARID1Aandor PTENmutations. Serous carcinoma acquires TP53mutationsinactivation at onset, with a significant subset harboring an additional mutation in PPP2R1A. This study examines the correlation between tumor histotype and genotype in 36 previously genotyped high-grade endometrial carcinomas. This included 23 endometrioidclear cell genotype and 13 serous genotype tumors. Eight subspecialty pathologists reviewed representative online slides and rendered diagnoses before and after receiving p53, p16, and estrogen receptor immunostaining results. statistics for histotype-genotype concordance were calculated. The average values for histotype-genotype concordance was 0.55 (range, 0.30 to 0.67) on the basis of morphologic evaluation alone and it improved to 0.68 (range, 0.54 to 0.81) after immunophenotype consideration (P<0.001). Genotype-incompatible diagnoses were rendered by at least 2 pathologists in 12 of 36 cases (33) (3 cases by 28 pathologists, 2 by 38, 2 by 48, 3 by 68, 1 by 78, and 1 case by 88 pathologists). Six of the 12 were endometrioidclear cell genotype tumors, and the other 6 were serous genotype tumors. The histopathologic features associated with histotype-genotype–discordant cases were reviewed, and specific diagnostic recommendations were made to improve concordance. This study found that although the majority of morphologic diagnoses are genotype concordant, genotype-incompatible diagnoses are made in a significant subset of cases. Judicious use and interpretation of p53 immunohistochemistry in selected scenarios can improve histotype-genotype concordance.
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- 2013
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25. Endometrial Stromal Sarcomas With Sex Cord Differentiation Are Associated With PHF1Rearrangement
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D’Angelo, Emanuela, Ali, Rola H., Espinosa, Inigo, Lee, Cheng-Han, Huntsman, David G., Gilks, Blake, and Prat, Jaime
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Endometrial stromal tumors may pose diagnostic challenges particularly when they exhibit variant histologic appearances, involve extrauterine sites, or present as metastatic disease. In such cases, use of immunohistochemical markers and identification of specific nonrandom chromosomal rearrangements may be helpful. Over the last decade, fluorescence in situ hybridization (FISH) has been progressively incorporated as a diagnostic tool for the evaluation of endometrial stromal tumors. The purpose of this study was to review a series of these tumors and compare the results of FISH analysis with the clinicopathologic characteristics. Three endometrial stromal nodules (ESNs), 13 endometrial stromal sarcomas (ESSs), and 7 undifferentiated endometrial sarcomas (UESs) were reviewed. Three metastases from 1 of the ESS cases were also analyzed. Nine of these tumors (1 ESN, 8 ESSs, and 1 UES) exhibited unusual histologic features, including smooth muscle (3), sex cord (7), epithelioid (1), fibromyxoid (1), and skeletal muscle (2) differentiation. A tissue microarray was prepared, and FISH analysis was performed using break-apart and fusion probes for JAZF1, SUZ12, EPC1, and PHF1genes. FISH was successful in 22 cases, and rearrangements involving JAZF1, SUZ12, EPC1, and PHF1genes were detected in 10 of the 22 (45) uterine tumors, including 2 of the 3 ESNs and 8 of 12 ESSs. Genetic rearrangements were found neither in the 3 metastases of the ESS nor in any of the UESs. It is noteworthy that a correlation between sex cord differentiation and PHF1rearrangement was encountered in ESSs (P=0.008). In our series, all ESSs showing sex cords had PHF1genetic rearrangement, suggesting that such rearrangements may induce sex cord differentiation.
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- 2013
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26. Cyclin D1 as a Diagnostic Immunomarker for Endometrial Stromal Sarcoma With YWHAE-FAM22Rearrangement
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Lee, Cheng-Han, Ali, Rola H., Rouzbahman, Marjan, Marino-Enriquez, Adrian, Zhu, Meijun, Guo, Xiangqian, Brunner, Alayne L., Chiang, Sarah, Leung, Samuel, Nelnyk, Nataliya, Huntsman, David G., Blake Gilks, C., Nielsen, Torsten O., Cin, Paola Dal, van de Rijn, Matt, Oliva, Esther, Fletcher, Jonathan A., and Nucci, Marisa R.
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Endometrial stromal sarcoma (ESS) characterized by YWHAE-FAM22genetic fusion is histologically higher grade and clinically more aggressive than ESS with JAZF1-SUZ12or equivalent genetic rearrangements, hence it is clinically important to recognize this subset of ESS. To identify diagnostic immunomarkers for this biologically defined ESS subset, we compared gene expression profiles between YWHAE-FAM22ESSand JAZF1-rearranged ESS. These studies showed consistent upregulation of cyclin D1 in YWHAE-FAM22ESS compared with JAZF1-SUZ12ESS. Immunohistochemically, the high-grade round cell component of all 12 YWHAE-FAM22ESS demonstrated diffuse (≥70) moderate to strong nuclear cyclin D1 staining, and this diffuse positivity was not seen in 34 ESSs with JAZF1and equivalent genetic rearrangements or in 21 low-grade ESS with no demonstrable genetic rearrangements. In a series of 243 non-ESS pure uterine mesenchymal and mixed epithelial-mesenchymal tumors, only 2 of 8 undifferentiated endometrial sarcomas with nuclear uniformity and 1 of 80 uterine leiomyosarcomas demonstrate diffuse cyclin D1 immunoreactivity. Both cyclin D1-positive undifferentiated endometrial sarcomas showed diffuse strong CD10 staining, which is consistently absent in the high-grade round cell component of YWHAE-FAM22ESS. The low-grade spindle cell component of YWHAE-FAM22ESS showed a spatially heterogenous cyclin D1 staining pattern that was weaker and less diffuse overall. Our findings indicate that cyclin D1 is a sensitive and specific diagnostic immunomarker for YWHAE-FAM22ESS. When evaluating high-grade uterine sarcomas, cyclin D1 can be included in the immunohistochemical panel as an indicator of YWHAE-FAM22ESS.
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- 2012
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27. The Clinicopathologic Features of YWHAE-FAM22Endometrial Stromal Sarcomas
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Lee, Cheng-Han, Mariño-Enriquez, Adrian, Ou, Wenbin, Zhu, Meijun, Ali, Rola H., Chiang, Sarah, Amant, Frédéric, Gilks, C. Blake, van de Rijn, Matt, Oliva, Esther, Debiec-Rychter, Maria, Dal Cin, Paola, Fletcher, Jonathan A., and Nucci, Marisa R.
- Abstract
Endometrial stromal sarcoma (ESS) is a genetically heterogenous group of uterine sarcomas, of which almost half are associated with JAZF1rearrangement. We recently identified a novel genetic fusion between YWHAEand FAM22ABin ESS harboring t(10;17)(q22;p13) and herein describe the clinicopathologic features of 13 YWHAE-FAM22ESS cases (11 primary and 3 metastatic) and compare them with 20 ESS cases with JAZF1rearrangement. Ten of 11 primary uterine tumors contained morphologically high-grade areas composed of round cells arranged in nests with a delicate stromal capillary network. The tumor cells showed large nuclei with irregular nuclear contours and significant mitotic activity (>10 mitoses10 HPF) in addition to focal tumor necrosis, in contrast to JAZF1ESS, which lacked a nested growth pattern, were composed of cells with small roundoval nuclei, and typically had <5 MF10 HPF. In 7 of the 11 uterine tumors, there was an additional cytologically bland and mitotically weakly active spindle cell component with a fibrousfibromyxoid stroma (ESS, fibromyxoid variant). Two metastatic tumors (pulmonary) also contained round cell and spindle cell components, whereas 1 metastasis (vaginal) was composed solely of the spindle cell component. In both primary and metastatic tumors, the spindle cells were diffusely positive for estrogen and progesterone receptors and CD10, in contrast to the round cell areas, which were negative. Clinically, 10 of 12 patients with YWHAE-FAM22ESS presented with FIGO stages II to III disease, in contrast to only 4 of 16 patients with JAZF1ESS presenting with stages II to III disease (P<0.05). Tumors with YWHAE-FAM22rearrangements constitute a distinct group of ESS, which is associated with high-grade morphology and aggressive clinical behavior compared to JAZF1ESS. Thus, their distinction from typical JAZF1ESS is important for prognostic and therapeutic purposes.
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- 2012
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28. Expression of Subtype-Specific Group 1 Leiomyosarcoma Markers in a Wide Variety of Sarcomas by Gene Expression Analysis and Immunohistochemistry
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Mills, Anne M., Beck, Andrew H., Montgomery, Kelli D., Zhu, Shirley X., Espinosa, Inigo, Lee, Cheng-Han, Subramanian, Subbaya, Fletcher, Christopher D., van de Rijn, Matt, and West, Robert B.
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Leiomyosarcomas (LMSs) constitute approximately one quarter of all sarcomas and are usually defined by morphologic criteria andor immunoreactivity for actin or desmin. Among high-grade lesions, the distinction from undifferentiated pleomorphic sarcoma (UPS) can be problematic, and previous studies have shown that a significant number of LMS cases may be hiding under the diagnosis of UPS. We recently described 3 novel molecular LMS subtypes that are distributed similarly over LMSs of gyneocologic and non-gyneocologic origins. The group 1 subtype shows an improved disease-specific survival compared with the other 2 groups that is independent of histologic grade. Group 1 comprises approximately 25 of all LMSs, and is defined by a shared pattern of gene expression, a distinct pattern of genomic changes, and reactivity for at least 3 of 5 immunohistochemistry (IHC) markers (smooth muscle gamma actin, calsequestrin 2, human muscle cofilin2, myosin light chain kinase, and sarcolemmal membrane associated protein), as tested on 271 cases of LMS in tissue microarrays. These IHC markers have not been well characterized in non-LMS sarcomas. Here we provide a characterization of these 5 markers across normal tissues, an additional 59 cases of LMS, and a wide range of 565 non-LMS soft tissue tumors from 44 diagnostic categories, with a focus on UPS. When analyzed individually, the 5 markers were found to be expressed in many sarcomas other than LMSs. However, when analyzed by the same criteria used for the recognition of group 1 LMSs, in which a case is scored positive when at least 3 of 5 markers reacted, coordinate expression was seen in significant numbers of cases from only 3 diagnostic groups that included 22 of leiomyomas (n=22), 16 of gastrointestinal stromal tumors (n=43), and 18 of endometrial stromal sarcomas (n=11). In addition, 5 (n=57) of UPSs showed a staining pattern similar to that seen in group 1 LMSs. To further examine the possibility that group 1 LMS constitutes a small part of cases diagnosed as UPS, we examined the expression of the top 500 genes from the group 1 LMS expression signature in 29 UPSs by complementary DNA microarray. Unsupervised hierarchical clustering of 29 UPS expression showed that 2 (7) had coordinated high levels of expression of genes from the group 1 LMS signature, a rate similar to that seen by IHC analysis. These findings show that group 1 LMS IHC markers smooth muscle gamma actin, calsequestrin 2, human muscle cofilin2, myosin light chain kinase, and sarcolemmal membrane associated protein when coordinately expressed have specificity for a subset of LMS when compared with other sarcomas, and may be useful for the recognition of group 1 LMS cases within cases diagnosed as UPS.
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- 2011
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