Your search keyword '"Sarah Chiang"' showing total 103 results

1. Expanding the molecular spectrum of gene fusions in endometrial stromal sarcoma: Novel subunits of the chromatin remodeling complexes <scp>PRC2</scp> and <scp>NuA4</scp> / <scp>TIP60</scp> as alternative fusion partners

Author

Josephine K. Dermawan, Nooshin Dashti, Sarah Chiang, Gulisa Turashvili, Brendan C. Dickson, Lora H. Ellenson, Martina Kirchner, Albrecht Stenzinger, Gunhild Mechtersheimer, Abbas Agaimy, and Cristina R. Antonescu

Subjects

Cancer Research, Genetics

Published

2022

2. Mullerian adenosarcoma: clinicopathologic and molecular characterization highlighting recurrent BAP1 loss and distinctive features of high-grade tumors

Author

Amir Momeni Boroujeni, Elizabeth Kertowidjojo, Xinyu Wu, Robert Soslow, Sarah Chiang, Edaise da Silva, Britta Weigelt, and M. Herman Chui

Subjects

Ribonuclease III, DEAD-box RNA Helicases, Phosphatidylinositol 3-Kinases, Adenosarcoma, Tumor Suppressor Proteins, Homozygote, Uterine Neoplasms, Humans, Female, Ubiquitin Thiolesterase, Sequence Deletion, Pathology and Forensic Medicine

Abstract

Mullerian adenosarcoma is an uncommon mesenchymal tumor of the gynecologic tract, usually of uterine origin. Tumors are generally low-grade and associated with good prognosis, whereas high-grade adenosarcomas are rare and less well studied. Herein, we sought to characterize the molecular features of 27 adenosarcomas (primary uterine, n = 19, cervical, n = 3, ovarian, n = 4, peritoneal, n = 1), enriched for high-grade tumors (n = 17) subjected to targeted panel sequencing. Recurrent genetic alterations in adenosarcomas included TP53 mutations (n = 4, 15%), restricted to high-grade cases, BAP1 homozygous deletions (n = 4, 15%), DICER1 mutations (n = 4, 15%), ARID1A mutations (n = 3), TERT promoter mutations (n = 2) and amplification (n = 1), ATRX frameshift mutation/homozygous deletions (n = 3), MDM2 (n = 2), CDK4 (n = 2) and CCNE1 (n = 2) amplifications, as well as alterations involving members of the PI3K (PTEN, n = 3; PIK3CA, n = 4; AKT1, n = 2) and MAPK (KRAS, n = 4, BRAF, n = 2) signaling pathways. One tumor harbored an ESR1-NCOA3 fusion and another had an MLH1 homozygous deletion, associated with loss of MLH1 and PMS2 protein expression. The fraction of genome altered was significantly higher in high-grade compared to low-grade adenosarcomas (P = 0.001). Somatic ATRX frameshift mutations were found in two patients with low-grade adenosarcoma with high-grade recurrences and one case of high-grade adenosarcoma with an adjacent low-grade component. Immunohistochemical analysis for BAP1 revealed loss of nuclear expression in 6/24 (25%) cases, including all 4 tumors with BAP1 deletions. Notably, out of 196 mesenchymal neoplasms of gynecologic origin, BAP1 homozygous deletion was only found in adenosarcomas (4/27,15% adenosarcomas vs 0/169, 0% other mesenchymal neoplasms, P = 0.0003). This study demonstrates that high-grade adenosarcomas are heterogeneous at the molecular level and are characterized by genomic instability and TP53 mutations; ATRX loss may be involved in high-grade transformation of low-grade adenosarcoma; and BAP1 inactivation appears to be a specific pathogenic driver in a subset of adenosarcomas.

Published

2022

3. Primary characteristics and outcomes of newly diagnosed low-grade endometrial stromal sarcoma

Author

Evan S Smith, Corinne Jansen, Kathryn M Miller, Sarah Chiang, Kaled M Alektiar, Martee L Hensley, Jennifer J Mueller, Nadeem R Abu-Rustum, and Mario M Leitao

Subjects

Adult, Aged, 80 and over, Sarcoma, Endometrial Stromal, Lymphadenopathy, Obstetrics and Gynecology, Middle Aged, Hysterectomy, Article, Endometrial Neoplasms, Young Adult, Oncology, Lymphatic Metastasis, Humans, Lymph Node Excision, Female, Neoplasm Recurrence, Local, Aged, Neoplasm Staging, Retrospective Studies

Abstract

ObjectiveTo assess potential predictive variables for nodal metastasis and survival outcomes in patients with newly diagnosed, low-grade endometrial stromal sarcoma.MethodsWe performed a single-institution, retrospective analysis of consecutive patients with newly diagnosed, low-grade endometrial stromal sarcoma who presented between January 1, 1980 and December 31, 2019 and underwent hysterectomy at our institution or presented within 3 months of primary surgery elsewhere before recurrence. Patients who presented to our institution only at recurrence were excluded. Patients with ResultsWe identified 127 consecutive patients for analysis. Median age at diagnosis was 48 years (range 19–88 years); 91 (74.6%) of 127 were pre-menopausal; and 74 (58.3%) of 127 had uterine-confined, stage I tumors. Of 56 patients (44.1%) who underwent lymph node sampling, 10 (17.9%) had nodal metastasis. Of the 10 with nodal metastasis, 1 (10%) did not have lymphadenopathy or extra-uterine disease, 4 (40%) had lymphadenopathy only, 1 (10%) had extra-uterine disease only, and 4 (40%) had both. Among the 29 patients without apparent extra-uterine disease or gross lymphadenopathy, there was one occult lymph node metastasis (3.4%). Gross lymphadenopathy at time of surgery was predictive for lymph node metastasis (pConclusionsLymph node dissection in patients with low-grade endometrial stromal sarcoma should be reserved for those with clinically suspicious lymphadenopathy. Disease stage correlated with progression-free survival but not disease-specific survival. Post-operative therapy did not improve progression-free survival or disease-specific survival.

Published

2022

4. Endometrial Stromal Sarcomas With BCOR Internal Tandem Duplication and Variant BCOR/BCORL1 Rearrangements Resemble High-grade Endometrial Stromal Sarcomas With Recurrent CDK4 Pathway Alterations and MDM2 Amplifications

Author

Felix K.F. Kommoss, Sarah Chiang, Martin Köbel, Christian Koelsche, Kenneth Tou-En Chang, Julie A. Irving, Brendan Dickson, Sakinah Thiryayi, Marjan Rouzbahman, Golnar Rasty, Andreas von Deimling, Cheng-Han Lee, and Gulisa Turashvili

Subjects

Sarcoma, Endometrial Stromal, Cyclin-Dependent Kinase 4, Proto-Oncogene Proteins c-mdm2, Sarcoma, Soft Tissue Neoplasms, Endometrial Neoplasms, Pathology and Forensic Medicine, Repressor Proteins, Proto-Oncogene Proteins, Uterine Neoplasms, Humans, Female, Surgery, Gene Fusion, Anatomy

Abstract

The distinction between low-grade and high-grade endometrial stromal sarcomas (LGESS, HGESS) is increasingly defined by genetics. Recently, variant genomic alterations involving BCOR or BCORL1 have 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::BCOR fusion, 1 with BCOR::LPP fusion) and BCORL1 ( 4 with JAZF1::BCORL1 fusion, 1 with EPC1::BCORL1 fusion). 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::NUTM2 and Z C3H7B::BCOR HGESS and molecularly confirmed LGESS revealed a common methylation signature for all ESS with variant BCOR and BCORL1 alterations and HGESS with YWHAE::NUTM2 and ZC3H7B::BCOR gene fusion. Copy number analysis revealed amplifications of CDK4 and MDM2 , as well as homozygous deletions of CDKN2A/B and NF1 in a subset of tumors. Our results indicate that ESS with BCOR internal tandem duplication and variant BCOR and BCORL1 rearrangements clinically and molecularly resemble conventional HGESS.

Published

2022

5. Figure S1 from Clinical Utility of Prospective Molecular Characterization in Advanced Endometrial Cancer

Author

David M. Hyman, Barry S. Taylor, David B. Solit, Deborah F. DeLair, Carol Aghajanian, Nadeem R. Abu-Rustum, Michael F. Berger, Ahmet Zehir, Britta Weigelt, Jennifer Mueller, Bob T. Li, Marc Ladanyi, Robert A. Soslow, Kay J. Park, Sarah Chiang, Rajmohan Murali, Sumit Middha, Sarah J. Schweber, Mila Gorsky, Claire Friedman, Alexandra Snyder Charen, Tiffany A. Troso-Sandoval, David R. Spriggs, Paul Sabbatini, Vicky Makker, Martee L. Hensley, Jason A. Konner, William P. Tew, Roisin E. O'Cearbhaill, Rachel N. Grisham, Karen A. Cadoo, Dmitriy Zamarin, Matthew T. Chang, Preethi Srinivasan, Chaitanya Bandlamudi, Mark T.A. Donoghue, and Tara E. Soumerai

Abstract

Progression-free survival and hazard ratios by histology

Published

2023

6. Supplementary Data from Genomic Landscape of Uterine Sarcomas Defined Through Prospective Clinical Sequencing

Author

David M. Hyman, Mark T.A. Donoghue, Barry S. Taylor, Evan Rosenbaum, William D. Tap, Preethi Srinivasan, Chaitanya Bandlamudi, Achim A. Jungbluth, Sarah Chiang, Robert Soslow, Rajmohan Murali, David B. Solit, Shweta S. Chavan, and Martee L. Hensley

Abstract

Supplementary Table 1

Published

2023

7. Data from IDH2 Mutations Define a Unique Subtype of Breast Cancer with Altered Nuclear Polarity

Author

Stuart J. Schnitt, Jorge S. Reis-Filho, A. John Iafrate, Matija Snuderl, Edi Brogi, Tarek Hammour, Xiaolong Liu, Song Lu, Kalliopi P. Siziopikou, Raymond S. Lim, Jonathan Serrano, Benjamin L. McCalip, Hwei-Choo Soh, Jonathan D. Marotti, Julie M. Batten, Andreas von Deimling, Kimberly S. Cole, Gabrielle M. Baker, Stefan Pusch, Jörg Balss, Achim A. Jungbluth, Charlotte K.Y. Ng, Salvatore Piscuoglio, Felipe C. Geyer, Anqi Li, Thais Basili, Kathleen A. Burke, Luciano G. Martelotto, Ashwini Raghavendra, Fresia Pareja, Huei-Chi Wen, Britta Weigelt, and Sarah Chiang

Abstract

Solid papillary carcinoma with reverse polarity (SPCRP) is a rare breast cancer subtype with an obscure etiology. In this study, we sought to describe its unique histopathologic features and to identify the genetic alterations that underpin SPCRP using massively parallel whole-exome and targeted sequencing. The morphologic and immunohistochemical features of SPCRP support the invasive nature of this subtype. Ten of 13 (77%) SPCRPs harbored hotspot mutations at R172 of the isocitrate dehydrogenase IDH2, of which 8 of 10 displayed concurrent pathogenic mutations affecting PIK3CA or PIK3R1. One of the IDH2 wild-type SPCRPs harbored a TET2 Q548* truncating mutation coupled with a PIK3CA H1047R hotspot mutation. Functional studies demonstrated that IDH2 and PIK3CA hotspot mutations are likely drivers of SPCRP, resulting in its reversed nuclear polarization phenotype. Our results offer a molecular definition of SPCRP as a distinct breast cancer subtype. Concurrent IDH2 and PIK3CA mutations may help diagnose SPCRP and possibly direct effective treatment. Cancer Res; 76(24); 7118–29. ©2016 AACR.

Published

2023

8. Data from Clinical Utility of Prospective Molecular Characterization in Advanced Endometrial Cancer

Author

David M. Hyman, Barry S. Taylor, David B. Solit, Deborah F. DeLair, Carol Aghajanian, Nadeem R. Abu-Rustum, Michael F. Berger, Ahmet Zehir, Britta Weigelt, Jennifer Mueller, Bob T. Li, Marc Ladanyi, Robert A. Soslow, Kay J. Park, Sarah Chiang, Rajmohan Murali, Sumit Middha, Sarah J. Schweber, Mila Gorsky, Claire Friedman, Alexandra Snyder Charen, Tiffany A. Troso-Sandoval, David R. Spriggs, Paul Sabbatini, Vicky Makker, Martee L. Hensley, Jason A. Konner, William P. Tew, Roisin E. O'Cearbhaill, Rachel N. Grisham, Karen A. Cadoo, Dmitriy Zamarin, Matthew T. Chang, Preethi Srinivasan, Chaitanya Bandlamudi, Mark T.A. Donoghue, and Tara E. Soumerai

Abstract

Purpose:Advanced-stage endometrial cancers have limited treatment options and poor prognosis, highlighting the need to understand genetic drivers of therapeutic vulnerabilities and/or prognostic predictors. We examined whether prospective molecular characterization of recurrent and metastatic disease can reveal grade and histology-specific differences, facilitating enrollment onto clinical trials.Experimental Design:We integrated prospective clinical sequencing and IHC data with detailed clinical and treatment histories for 197 tumors, profiled by MSK-IMPACT from 189 patients treated at Memorial Sloan Kettering Cancer Center.Results:Patients had advanced disease and high-grade histologies, with poor progression-free survival on first-line therapy (PFS1). When matched for histology and grade, the genomic landscape was similar to that of primary untreated disease profiled by TCGA. Using multiple complementary genomic and mutational signature-based methods, we identified patients with microsatellite instability (MSI), even when standard MMR protein IHC staining failed. Tumor and matched normal DNA sequencing identified rare pathogenic germline mutations in BRCA2 and MLH1. Clustering the pattern of DNA copy-number alterations revealed a novel subset characterized by heterozygous losses across the genome and significantly worse outcomes compared with other clusters (median PFS1 9.6 months vs. 17.0 and 17.4 months; P = 0.006). Of the 68% of patients harboring potentially actionable mutations, 27% were enrolled to matched clinical trials, of which 47% of these achieved clinical benefit.Conclusions:Prospective clinical sequencing of advanced endometrial cancer can help refine prognosis and aid treatment decision making by simultaneously detecting microsatellite status, germline predisposition syndromes, and potentially actionable mutations. A small overall proportion of all patients tested received investigational, genomically matched therapy as part of clinical trials.

Published

2023

9. Supplementary Data from Integrated Analysis of Ovarian Juvenile Granulosa Cell Tumors Reveals Distinct Epigenetic Signatures and Recurrent TERT Rearrangements

Author

George Jour, Matija Snuderl, Deborah F. DeLair, Paolo Cotzia, Esther Oliva, Anais Malpica, Pratibha S. Shukla, Lauren E. Schwartz, Kristen M. Thomas, Julieta E. Barroeta, Sarah Chiang, Xiaojun Feng, Rebecca L. Linn, Guomiao Shen, Jonathan Serrano, Varshini Vasudevaraja, Kelsey Zhu, and Theodore Vougiouklakis

Abstract

Supplementary Data from Integrated Analysis of Ovarian Juvenile Granulosa Cell Tumors Reveals Distinct Epigenetic Signatures and Recurrent TERT Rearrangements

Published

2023

10. Table S1 from Clinical Utility of Prospective Molecular Characterization in Advanced Endometrial Cancer

Author

David M. Hyman, Barry S. Taylor, David B. Solit, Deborah F. DeLair, Carol Aghajanian, Nadeem R. Abu-Rustum, Michael F. Berger, Ahmet Zehir, Britta Weigelt, Jennifer Mueller, Bob T. Li, Marc Ladanyi, Robert A. Soslow, Kay J. Park, Sarah Chiang, Rajmohan Murali, Sumit Middha, Sarah J. Schweber, Mila Gorsky, Claire Friedman, Alexandra Snyder Charen, Tiffany A. Troso-Sandoval, David R. Spriggs, Paul Sabbatini, Vicky Makker, Martee L. Hensley, Jason A. Konner, William P. Tew, Roisin E. O'Cearbhaill, Rachel N. Grisham, Karen A. Cadoo, Dmitriy Zamarin, Matthew T. Chang, Preethi Srinivasan, Chaitanya Bandlamudi, Mark T.A. Donoghue, and Tara E. Soumerai

Abstract

Additional clinical information for patients in MSKCC cohort

Published

2023

11. Supplementary Materials and Methods from IDH2 Mutations Define a Unique Subtype of Breast Cancer with Altered Nuclear Polarity

Author

Stuart J. Schnitt, Jorge S. Reis-Filho, A. John Iafrate, Matija Snuderl, Edi Brogi, Tarek Hammour, Xiaolong Liu, Song Lu, Kalliopi P. Siziopikou, Raymond S. Lim, Jonathan Serrano, Benjamin L. McCalip, Hwei-Choo Soh, Jonathan D. Marotti, Julie M. Batten, Andreas von Deimling, Kimberly S. Cole, Gabrielle M. Baker, Stefan Pusch, Jörg Balss, Achim A. Jungbluth, Charlotte K.Y. Ng, Salvatore Piscuoglio, Felipe C. Geyer, Anqi Li, Thais Basili, Kathleen A. Burke, Luciano G. Martelotto, Ashwini Raghavendra, Fresia Pareja, Huei-Chi Wen, Britta Weigelt, and Sarah Chiang

Abstract

Document containing methods on whole exome and targeted massively parallel sequencing analysis, 2-hydroxyglutarate (2HG) assay of cell lines, methylation profiling, and supplementary references.

Published

2023

12. Figure S4 from Clinical Utility of Prospective Molecular Characterization in Advanced Endometrial Cancer

Author

David M. Hyman, Barry S. Taylor, David B. Solit, Deborah F. DeLair, Carol Aghajanian, Nadeem R. Abu-Rustum, Michael F. Berger, Ahmet Zehir, Britta Weigelt, Jennifer Mueller, Bob T. Li, Marc Ladanyi, Robert A. Soslow, Kay J. Park, Sarah Chiang, Rajmohan Murali, Sumit Middha, Sarah J. Schweber, Mila Gorsky, Claire Friedman, Alexandra Snyder Charen, Tiffany A. Troso-Sandoval, David R. Spriggs, Paul Sabbatini, Vicky Makker, Martee L. Hensley, Jason A. Konner, William P. Tew, Roisin E. O'Cearbhaill, Rachel N. Grisham, Karen A. Cadoo, Dmitriy Zamarin, Matthew T. Chang, Preethi Srinivasan, Chaitanya Bandlamudi, Mark T.A. Donoghue, and Tara E. Soumerai

Abstract

Reanalysis of TCGA high copy number burden cluster four. A. Ploidy and purity corrected clustering of SCNAs. B. Comparison of PFS between the two clusters identified in S4A.

Published

2023

13. Supplementary Figures and Tables from IDH2 Mutations Define a Unique Subtype of Breast Cancer with Altered Nuclear Polarity

Author

Stuart J. Schnitt, Jorge S. Reis-Filho, A. John Iafrate, Matija Snuderl, Edi Brogi, Tarek Hammour, Xiaolong Liu, Song Lu, Kalliopi P. Siziopikou, Raymond S. Lim, Jonathan Serrano, Benjamin L. McCalip, Hwei-Choo Soh, Jonathan D. Marotti, Julie M. Batten, Andreas von Deimling, Kimberly S. Cole, Gabrielle M. Baker, Stefan Pusch, Jörg Balss, Achim A. Jungbluth, Charlotte K.Y. Ng, Salvatore Piscuoglio, Felipe C. Geyer, Anqi Li, Thais Basili, Kathleen A. Burke, Luciano G. Martelotto, Ashwini Raghavendra, Fresia Pareja, Huei-Chi Wen, Britta Weigelt, and Sarah Chiang

Abstract

Document containing figures illustrating results of Sanger sequencing, DNA methylation profiling of SPCRPs, the analysis of IDH2 expression in non-malignant breast epithelial cells and its downstream effects, and tables describing the antibodies used for immunohistochemical analysis, the alterations surveyed by the SNaPshot genotyping assay, Sanger sequencing primers, and statistics and results of the massively parallel sequencing analyses.

Published

2023

14. Supplementary Figure from Integrated Analysis of Ovarian Juvenile Granulosa Cell Tumors Reveals Distinct Epigenetic Signatures and Recurrent TERT Rearrangements

Author

George Jour, Matija Snuderl, Deborah F. DeLair, Paolo Cotzia, Esther Oliva, Anais Malpica, Pratibha S. Shukla, Lauren E. Schwartz, Kristen M. Thomas, Julieta E. Barroeta, Sarah Chiang, Xiaojun Feng, Rebecca L. Linn, Guomiao Shen, Jonathan Serrano, Varshini Vasudevaraja, Kelsey Zhu, and Theodore Vougiouklakis

Abstract

Supplementary Figure from Integrated Analysis of Ovarian Juvenile Granulosa Cell Tumors Reveals Distinct Epigenetic Signatures and Recurrent TERT Rearrangements

Published

2023

15. Figure S2 from Clinical Utility of Prospective Molecular Characterization in Advanced Endometrial Cancer

Author

David M. Hyman, Barry S. Taylor, David B. Solit, Deborah F. DeLair, Carol Aghajanian, Nadeem R. Abu-Rustum, Michael F. Berger, Ahmet Zehir, Britta Weigelt, Jennifer Mueller, Bob T. Li, Marc Ladanyi, Robert A. Soslow, Kay J. Park, Sarah Chiang, Rajmohan Murali, Sumit Middha, Sarah J. Schweber, Mila Gorsky, Claire Friedman, Alexandra Snyder Charen, Tiffany A. Troso-Sandoval, David R. Spriggs, Paul Sabbatini, Vicky Makker, Martee L. Hensley, Jason A. Konner, William P. Tew, Roisin E. O'Cearbhaill, Rachel N. Grisham, Karen A. Cadoo, Dmitriy Zamarin, Matthew T. Chang, Preethi Srinivasan, Chaitanya Bandlamudi, Mark T.A. Donoghue, and Tara E. Soumerai

Abstract

Comparison of most recurrently mutated genes in MSKCC vs. TCGA cohort

Published

2023

16. Data from Genomic Landscape of Uterine Sarcomas Defined Through Prospective Clinical Sequencing

Author

David M. Hyman, Mark T.A. Donoghue, Barry S. Taylor, Evan Rosenbaum, William D. Tap, Preethi Srinivasan, Chaitanya Bandlamudi, Achim A. Jungbluth, Sarah Chiang, Robert Soslow, Rajmohan Murali, David B. Solit, Shweta S. Chavan, and Martee L. Hensley

Abstract

Purpose:We examined whether prospective molecular characterization of advanced metastatic disease can reveal grade and/or histology-specific differences to inform diagnosis and facilitate enrollment onto clinical trials.Experimental Design:Patients with uterine sarcoma consented to a prospective study of next-generation sequencing (NGS). Clinical annotations were extracted from their medical record. Tumor and matched normal DNA were subjected to NGS, and the genomic landscape was explored for survival correlations and therapeutic targetability.Results:Tumors from 107 women were sequenced and included leiomyosarcoma (n = 80), high-grade non-leiomyosarcoma (n = 22), low-grade endometrial stromal sarcoma (LG-ESS, n = 4), and smooth muscle tumor of uncertain malignant potential (STUMP, n = 2). Genomic profiling influenced histologic diagnosis in three cases. Common uterine leiomyosarcoma alterations were loss-of-function mutations in TP53 (56%), RB1 (51%), and ATRX (31%). Homozygous deletions of BRCA2 were present in 5% of these patients. PTEN alteration frequency was higher in the metastases samples as compared with the primary samples. Genomes of low-grade tumors were largely silent, while 50.5% of high-grade tumors had whole-genome duplication. Two metastatic uterine leiomyosarcoma cases were hypermutated. Both had prolonged disease-free survival. Potentially actionable mutations were identified in 48 patients (45%), 8 (17%) of whom received matched therapy with 2 achieving clinical responses. Among patients with uterine leiomyosarcoma with somatic BRCA2 alterations, sustained partial responses were observed with PARP inhibitor–containing therapy.Discussion:Prospective genomic profiling can contribute to diagnostic precision and inform treatment selection in patients with uterine sarcomas. There was evidence of clinical benefit in patients with uterine leiomyosarcoma with somatic BRCA2 alterations treated with PARP inhibitors.

Published

2023

17. Figure S3 from Clinical Utility of Prospective Molecular Characterization in Advanced Endometrial Cancer

Author

David M. Hyman, Barry S. Taylor, David B. Solit, Deborah F. DeLair, Carol Aghajanian, Nadeem R. Abu-Rustum, Michael F. Berger, Ahmet Zehir, Britta Weigelt, Jennifer Mueller, Bob T. Li, Marc Ladanyi, Robert A. Soslow, Kay J. Park, Sarah Chiang, Rajmohan Murali, Sumit Middha, Sarah J. Schweber, Mila Gorsky, Claire Friedman, Alexandra Snyder Charen, Tiffany A. Troso-Sandoval, David R. Spriggs, Paul Sabbatini, Vicky Makker, Martee L. Hensley, Jason A. Konner, William P. Tew, Roisin E. O'Cearbhaill, Rachel N. Grisham, Karen A. Cadoo, Dmitriy Zamarin, Matthew T. Chang, Preethi Srinivasan, Chaitanya Bandlamudi, Mark T.A. Donoghue, and Tara E. Soumerai

Abstract

Mutation cancer cell fraction (CCF) comparisons between matched pairs of primary tumor and metastasis

Published

2023

18. Data from Clinicopathologic and Genomic Analysis of TP53-Mutated Endometrial Carcinomas

Author

Robert A. Soslow, Britta Weigelt, Lora H. Ellenson, Marc Ladanyi, Nadeem R. Abu-Rustum, Carol Aghajanian, Kaled M. Alektiar, Eric V. Rios-Doria, Rajmohan Murali, Sarah Chiang, Chad M. Vanderbilt, Wissam Dahoud, and Amir Momeni-Boroujeni

Abstract

Purpose:Copy number–high endometrial carcinomas were described by The Cancer Genome Atlas as high-grade endometrioid and serous cancers showing frequent copy-number alterations (CNA), low mutational burden (i.e., non-hypermutant), near-universal TP53 mutation, and unfavorable clinical outcomes. We sought to investigate and compare the clinicopathologic and molecular characteristics of non-hypermutant TP53-altered endometrial carcinomas of four histologic types.Experimental Design:TP53-mutated endometrial carcinomas, defined as TP53-mutant tumors lacking microsatellite instability or pathogenic POLE mutations, were identified (n = 238) in a cohort of 1,239 endometrial carcinomas subjected to clinical massively parallel sequencing of 410–468 cancer-related genes. Somatic mutations and CNAs (n = 238), and clinicopathologic features were determined (n = 185, initial treatment planning at our institution).Results:TP53-mutated endometrial carcinomas encompassed uterine serous (n = 102, 55.1%), high-grade endometrial carcinoma with ambiguous features/not otherwise specified (EC-NOS; n = 44, 23.8%), endometrioid carcinomas of all tumor grades (n = 28, 15.1%), and clear cell carcinomas (n = 11, 5.9%). PTEN mutations were significantly more frequent in endometrioid carcinomas, SPOP mutations in clear cell carcinomas, and CCNE1 amplification in serous carcinomas/EC-NOS; however, none of these genomic alterations were exclusive to any given histologic type. ERBB2 amplification was present at similar frequencies across TP53-mutated histologic types (7.7%–18.6%). Although overall survival was similar across histologic types, serous carcinomas presented more frequently at stage IV, had more persistent and/or recurrent disease, and reduced disease-free survival.Conclusions:TP53-mutated endometrial carcinomas display clinical and molecular similarities across histologic subtypes. Our data provide evidence to suggest performance of ERBB2 assessment in all TP53-mutated endometrial carcinomas. Given the distinct clinical features of serous carcinomas, histologic classification continues to be relevant.

Published

2023

19. Supplementary Data from Clinicopathologic and Genomic Analysis of TP53-Mutated Endometrial Carcinomas

Author

Robert A. Soslow, Britta Weigelt, Lora H. Ellenson, Marc Ladanyi, Nadeem R. Abu-Rustum, Carol Aghajanian, Kaled M. Alektiar, Eric V. Rios-Doria, Rajmohan Murali, Sarah Chiang, Chad M. Vanderbilt, Wissam Dahoud, and Amir Momeni-Boroujeni

Abstract

Supplementary Methods Supplementary Figures S1-S5 Supplementary Tables S1, S2

Published

2023

20. Supplementary Figure Legends from IDH2 Mutations Define a Unique Subtype of Breast Cancer with Altered Nuclear Polarity

Author

Stuart J. Schnitt, Jorge S. Reis-Filho, A. John Iafrate, Matija Snuderl, Edi Brogi, Tarek Hammour, Xiaolong Liu, Song Lu, Kalliopi P. Siziopikou, Raymond S. Lim, Jonathan Serrano, Benjamin L. McCalip, Hwei-Choo Soh, Jonathan D. Marotti, Julie M. Batten, Andreas von Deimling, Kimberly S. Cole, Gabrielle M. Baker, Stefan Pusch, Jörg Balss, Achim A. Jungbluth, Charlotte K.Y. Ng, Salvatore Piscuoglio, Felipe C. Geyer, Anqi Li, Thais Basili, Kathleen A. Burke, Luciano G. Martelotto, Ashwini Raghavendra, Fresia Pareja, Huei-Chi Wen, Britta Weigelt, and Sarah Chiang

Abstract

Legends for Supplementary Figures S1-S5

Published

2023

21. Supplementary Table and Figure Legends from Clinical Utility of Prospective Molecular Characterization in Advanced Endometrial Cancer

Author

David M. Hyman, Barry S. Taylor, David B. Solit, Deborah F. DeLair, Carol Aghajanian, Nadeem R. Abu-Rustum, Michael F. Berger, Ahmet Zehir, Britta Weigelt, Jennifer Mueller, Bob T. Li, Marc Ladanyi, Robert A. Soslow, Kay J. Park, Sarah Chiang, Rajmohan Murali, Sumit Middha, Sarah J. Schweber, Mila Gorsky, Claire Friedman, Alexandra Snyder Charen, Tiffany A. Troso-Sandoval, David R. Spriggs, Paul Sabbatini, Vicky Makker, Martee L. Hensley, Jason A. Konner, William P. Tew, Roisin E. O'Cearbhaill, Rachel N. Grisham, Karen A. Cadoo, Dmitriy Zamarin, Matthew T. Chang, Preethi Srinivasan, Chaitanya Bandlamudi, Mark T.A. Donoghue, and Tara E. Soumerai

Abstract

Supplementary Table and Figure Legends

Published

2023

22. Supplementary Figures from Genomic Landscape of Uterine Sarcomas Defined Through Prospective Clinical Sequencing

Author

David M. Hyman, Mark T.A. Donoghue, Barry S. Taylor, Evan Rosenbaum, William D. Tap, Preethi Srinivasan, Chaitanya Bandlamudi, Achim A. Jungbluth, Sarah Chiang, Robert Soslow, Rajmohan Murali, David B. Solit, Shweta S. Chavan, and Martee L. Hensley

Abstract

Supplementary Figures

Published

2023

23. Table S2 from Clinical Utility of Prospective Molecular Characterization in Advanced Endometrial Cancer

Author

David M. Hyman, Barry S. Taylor, David B. Solit, Deborah F. DeLair, Carol Aghajanian, Nadeem R. Abu-Rustum, Michael F. Berger, Ahmet Zehir, Britta Weigelt, Jennifer Mueller, Bob T. Li, Marc Ladanyi, Robert A. Soslow, Kay J. Park, Sarah Chiang, Rajmohan Murali, Sumit Middha, Sarah J. Schweber, Mila Gorsky, Claire Friedman, Alexandra Snyder Charen, Tiffany A. Troso-Sandoval, David R. Spriggs, Paul Sabbatini, Vicky Makker, Martee L. Hensley, Jason A. Konner, William P. Tew, Roisin E. O'Cearbhaill, Rachel N. Grisham, Karen A. Cadoo, Dmitriy Zamarin, Matthew T. Chang, Preethi Srinivasan, Chaitanya Bandlamudi, Mark T.A. Donoghue, and Tara E. Soumerai

Abstract

Recurrent cases in MSKCC vs. TCGA cohort

Published

2023

24. Data from Integrated Analysis of Ovarian Juvenile Granulosa Cell Tumors Reveals Distinct Epigenetic Signatures and Recurrent TERT Rearrangements

Author

George Jour, Matija Snuderl, Deborah F. DeLair, Paolo Cotzia, Esther Oliva, Anais Malpica, Pratibha S. Shukla, Lauren E. Schwartz, Kristen M. Thomas, Julieta E. Barroeta, Sarah Chiang, Xiaojun Feng, Rebecca L. Linn, Guomiao Shen, Jonathan Serrano, Varshini Vasudevaraja, Kelsey Zhu, and Theodore Vougiouklakis

Abstract

Purpose:Adult granulosa cell tumor (AGCT) is characterized by the somatic FOXL2 p.C134W mutation, and recurrences have been associated with TERT promoter and KMT2D-truncating mutations. Conversely, the molecular underpinnings of the rare juvenile granulosa cell tumor (JGCT) have not been well elucidated. To this end, we applied a tumor-only integrated approach to investigate the genomic, transcriptomic, and epigenomic landscape of 31 JGCTs to identify putative oncogenic drivers.Experimental Design:Multipronged analyses of 31 JGCTs were performed utilizing a clinically validated next-generation sequencing (NGS) panel targeting 580 cancer-related genes for genomic interrogation, in addition to targeted RNA NGS for transcriptomic exploration. Genome-wide DNA methylation profiling was conducted using an Infinium Methylation EPIC array targeting 866,562 CpG methylation sites.Results:We identified frequent KMT2C-truncating mutations along with other mutated genes implicated in the switch/sucrose nonfermentable (SWI/SNF) chromatin remodeling complex, in addition to previously reported hotspot AKT1 and DICER1 mutations. Targeted transcriptome sequencing revealed recurrent TERT rearrangements (13%) involving partners CLPTM1L or DROSHA, and differential gene expression analysis showed FGFR1 upregulation in the TERT non-rearranged JGCTs under direct promoter control. Genome-wide DNA methylation rendered a clear delineation between AGCTs and JGCTs at the epigenomic level, further supporting its diagnostic utility in distinguishing among these tumors.Conclusions:This is the largest comprehensive molecular study of JGCTs, where we further expand our current understanding of JGCT pathogenesis and demonstrate putative oncogenic drivers and TERT rearrangements in a subset of tumors. Our findings further offer insights into possible targeted therapies in a rare entity.

Published

2023

25. TSC2-mutant uterine sarcomas with JAZF1-SUZ12 fusions demonstrate hybrid features of endometrial stromal sarcoma and PEComa and are responsive to mTOR inhibition

Author

Rajmohan Murali, Amir Momeni-Boroujeni, Seth M. Cohen, Kay J. Park, Lora H. Ellenson, Matija Snuderl, Edaise M da Silva, Cheng-Han Lee, Ryma Benayed, Nadeem R. Abu-Rustum, Jason A. Konner, Varshini Vasudevaraja, Marc Ladanyi, Sarah Chiang, Achim A. Jungbluth, Jonathan Serrano, Mark A. Dickson, Britta Weigelt, Carol Aghajanian, Robert A. Soslow, Martee L. Hensley, Arnaud Da Cruz Paula, Esther Oliva, and Colin J.R. Stewart

Subjects

Pathology, medicine.medical_specialty, Somatic cell, Biology, Article, Perivascular Epithelioid Cell, Pathology and Forensic Medicine, Cohort Studies, Diagnosis, Differential, medicine, Humans, Epigenetics, In Situ Hybridization, Fluorescence, PI3K/AKT/mTOR pathway, Aged, Endometrial stromal sarcoma, Sarcoma, Methylation, DNA Methylation, Middle Aged, medicine.disease, Immunohistochemistry, Mutation, Uterine Neoplasms, Female, Epithelioid cell

Abstract

Uterine perivascular epithelioid cell tumor (PEComa) is a rare mesenchymal neoplasm that occasionally shares morphologic and immunohistochemical overlap with low- and high-grade endometrial stromal sarcoma (LGESS and HGESS). In this study, we sought to characterize the clinical, morphologic, genetic, and epigenetic features of five uterine sarcomas that display histologic features of LGESS, HGESS, and PEComa. All tumors demonstrated epithelioid cells often associated with a low-grade spindled component resembling LGESS, with both regions expressing CD10, ER, PR, variable HMB45, and Melan-A immunoreactivity, and strong cathepsin K and pS6 expression. Targeted massively parallel sequencing analysis revealed the presence of somatic TSC2 mutations in all five cases, of which four harbored concurrent or consecutive JAZF1-SUZ12 gene fusions. Unsupervised hierarchical clustering analysis of methylation profiles of TSC2-mutant uterine sarcomas (n = 4), LGESS (n = 10), and HGESS (n = 12) demonstrated two clusters consisting of (1) all LGESS and TSC2-mutant uterine sarcomas and (2) all HGESS. KEGG pathway analysis detected methylation differences in genes involved in PI3K/AKT, calcium, and Rap1 signaling. TSC2-mutant uterine sarcomas were responsive to hormone suppression, and mTOR inhibition demonstrated clinical benefit in four patients with these neoplasms. Our results suggest that these tumors represent histologically distinctive LGESS with TSC2 mutations. TSC2 mutations and JAZF1-SUZ12 fusion may help diagnose these tumors and possibly direct effective treatment.

Published

2022

26. Fat Grafting for Volume Augmentation in Prepectoral Breast Reconstruction

Author

William R. Moritz, Halley Darrach, Hayden Schott, Michael Finnan, Sarah Chiang, Annahita Fotouhi, Franca Kraenzlin, Nima Khavanin, Karan Chopra, and Justin M. Sacks

Published

2023

27. Expanding the molecular spectrum of gene fusions in endometrial stromal sarcoma: Novel subunits of the chromatin remodeling complexes PRC2 and NuA4/TIP60 as alternative fusion partners

Author

Josephine K, Dermawan, Nooshin, Dashti, Sarah, Chiang, Gulisa, Turashvili, Brendan C, Dickson, Lora H, Ellenson, Martina, Kirchner, Albrecht, Stenzinger, Gunhild, Mechtersheimer, Abbas, Agaimy, and Cristina R, Antonescu

Abstract

Endometrial stromal sarcomas (ESS) are morphologically and molecularly heterogeneous. We report novel gene fusions (EPC1::EED, EPC1::EZH2, ING3::PHF1) identified by targeted RNA sequencing in five cases. The ING3::PHF1-fusion positive ESS presented in a 58-year-old female as extrauterine mesocolonic, ovarian masses, and displayed large, monomorphic ovoid-to-epithelioid cells arranged in solid sheets. The patient remained alive with disease 13 months after surgery. The three ESS with EPC1::EED occurred in the uterine corpus in patients with a median age of 58 years (range 27-62 years). One tumor showed a uniform epithelioid nested morphology, while the other two were composed of monomorphic spindle cells in fascicles with elevated mitotic figures, focal tumor cell necrosis, and lymphovascular invasion. At a median follow-up of 20 months, two patients developed local recurrence, including one with concomitant distant metastasis, while one patient remained free of disease. All three patients were alive at the last follow-up. The EPC1::EZH2-fusion positive ESS presented in a 52-year-old female in the uterus, and displayed uniform spindled cells arranged in short fascicles, with focally elevated mitotic activity but without necrosis. The patient remained free of disease 3 months after surgery. All cases were diffusely positive for CD10; four diffusely express estrogen and progesterone receptors. Our study expands the molecular spectrum of EPC1 and PHF1-related gene fusions in ESS to include additional novel subunits of the PRC2 and/or NuA4/TIP60 complexes. These cases displayed a monomorphic epithelioid or spindled phenotype, spanning low-grade and high-grade cytomorphology, all expressing CD10 and commonly ER and PR, and are prone to local and/or distant spread.

Published

2022

28. Integrated digital pathology at scale: A solution for clinical diagnostics and cancer research at a large academic medical center

Author

Yukako Yagi, Evangelos Stamelos, D Vijay K Yarlagadda, Christine England, Melissa Murray, Allyne Manzo, Thomas J. Fuchs, Chad M. Vanderbilt, Luke Geneslaw, Michael H.A. Roehrl, Victor E. Reuter, Jennifer Samboy, S. Joseph Sirintrapun, Dilip Giri, Jianjiong Gao, Marc-Henri Jean, Juan C Perin, David S. Klimstra, Lorraine Corsale, Meera Hameed, Peter J. Schüffler, Carlie S. Sigel, Matthew G. Hanna, John Philip, John Ziegler, Lee K. Tan, Neeraj H G Paramasivam, U. Bhanot, Orly Ardon, Young Suk Kim, Christina Virgo, and Sarah Chiang

Subjects

Male, 0301 basic medicine, AcademicSubjects/SCI01060, Computer science, Health Informatics, Research and Applications, 03 medical and health sciences, Computational pathology, 0302 clinical medicine, Blueprint, Neoplasms, Humans, Use case, Pandemics, AcademicSubjects/MED00580, Academic Medical Centers, Pathology, Clinical, business.industry, COVID-19, Digital pathology, honest broker, pathology, artificial intelligence, ddc, whole slide imaging, 030104 developmental biology, Workflow, 030220 oncology & carcinogenesis, Scale (social sciences), Cancer research, Honest Broker, AcademicSubjects/SCI01530, digital pathology, business, Quality assurance, Medical Informatics, computational pathology

Abstract

Objective Broad adoption of digital pathology (DP) is still lacking, and examples for DP connecting diagnostic, research, and educational use cases are missing. We blueprint a holistic DP solution at a large academic medical center ubiquitously integrated into clinical workflows; researchapplications including molecular, genetic, and tissue databases; and educational processes. Materials and Methods We built a vendor-agnostic, integrated viewer for reviewing, annotating, sharing, and quality assurance of digital slides in a clinical or research context. It is the first homegrown viewer cleared by New York State provisional approval in 2020 for primary diagnosis and remote sign-out during the COVID-19 (coronavirus disease 2019) pandemic. We further introduce an interconnected Honest Broker for BioInformatics Technology (HoBBIT) to systematically compile and share large-scale DP research datasets including anonymized images, redacted pathology reports, and clinical data of patients with consent. Results The solution has been operationally used over 3 years by 926 pathologists and researchers evaluating 288 903 digital slides. A total of 51% of these were reviewed within 1 month after scanning. Seamless integration of the viewer into 4 hospital systems clearly increases the adoption of DP. HoBBIT directly impacts the translation of knowledge in pathology into effective new health measures, including artificial intelligence–driven detection models for prostate cancer, basal cell carcinoma, and breast cancer metastases, developed and validated on thousands of cases. Conclusions We highlight major challenges and lessons learned when going digital to provide orientation for other pathologists. Building interconnected solutions will not only increase adoption of DP, but also facilitate next-generation computational pathology at scale for enhanced cancer research.

Published

2021

29. Uterine carcinosarcomas: From pathology to practice

Author

Matthew A. Powell, Erin K. Crane, Sean C. Dowdy, Alexander Shushkevich, Douglas A. Levine, Brian M. Slomovitz, Michael D. Toboni, Jubilee Brown, Sarah Chiang, Premal H. Thaker, and Ann H. Klopp

Subjects

0301 basic medicine, medicine.medical_specialty, MEDLINE, Disease, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Carcinosarcoma, Uterine cancer, Adjuvant therapy, Humans, Medicine, Uterine carcinosarcoma, Intensive care medicine, business.industry, Endometrial cancer, Obstetrics and Gynecology, medicine.disease, Combined Modality Therapy, Carboplatin, Clinical trial, 030104 developmental biology, Oncology, chemistry, 030220 oncology & carcinogenesis, Uterine Neoplasms, Female, business

Abstract

Objective Uterine carcinosarcoma (UCS) is a rare but aggressive cancer. In early-stage disease data guiding treatment is sparse. The purpose of this review is to summarize the findings from the 2019 NRG oncology group summer symposium meeting as well as a review of the current literature, with a particular focus on molecular targets, ongoing clinical trials, and treatment of early and advanced/recurrent disease. Methods A combination of expert presentations and an extensive literature search was undertaken to summarize the literature in this review. MEDLINE was queried for peer-reviewed publications on UCS. This search was not limited by year or study design, but was limited to English language publications. ClinicalTrials.gov was queried for ongoing trials in UCS. Results UCS is a rare cancer that is biphasic, with the carcinomatous component driving its aggressive nature. Level 3 evidence regarding early stage disease is lacking, but retrospective data suggests adjuvant therapy is warranted. The recent results of GOG 261 have contributed valuable information towards treatment strategy, including use of paclitaxel and carboplatin for UCS. Clinical trials are ongoing to investigate new targeted agents in UCS. Conclusion Ongoing endometrial cancer clinical trials now include UCS patients. In combination with advances in molecular profiling, this will provide patients with UCS improved therapeutic options. Until that time, surgical resection and traditional cytotoxic chemotherapy remains standard of care.

Published

2021

30. Medical <scp>student‐led</scp> social phone calls with elder mistreatment victims: Changes in loneliness, depression, and perspectives of aging

Author

Gabrielle Hoyumpa, Analisa Narro, Matthew Law, Bronson Ciavarra, Vanessa Phung, Sarah Chiang, Tyson Oyler, Hayden Lydick, Renee Flores, Jessica Lee, and Jason Burnett

Subjects

Aging, Students, Medical, Depression, Loneliness, Humans, Geriatrics and Gerontology, Elder Abuse, Aged

Published

2022

31. Targeted RNA expression profiling identifies high-grade endometrial stromal sarcoma as a clinically relevant molecular subtype of uterine sarcoma

Author

Amir Momeni-Boroujeni, Marc Ladanyi, Sarah Chiang, Cristina R. Antonescu, Ryma Benayed, Robert Wolber, Stephen Yip, Nissreen Mohammad, Cheng-Han Lee, Martin Köbel, Brendan C. Dickson, Martee L. Hensley, and Mario M. Leitao

Subjects

Adult, Leiomyosarcoma, 0301 basic medicine, Pathology, medicine.medical_specialty, Stromal cell, Sarcoma, Endometrial Stromal, Pathology and Forensic Medicine, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, GLI1, Biomarkers, Tumor, medicine, Humans, In Situ Hybridization, Fluorescence, Endometrial stromal sarcoma, biology, Uterine sarcoma, medicine.diagnostic_test, Gene Expression Profiling, Estrogen Receptor alpha, RNA, Middle Aged, medicine.disease, Immunohistochemistry, Endometrial Neoplasms, Gene Expression Regulation, Neoplastic, body regions, 030104 developmental biology, 030220 oncology & carcinogenesis, Uterine Neoplasms, biology.protein, Female, Fluorescence in situ hybridization

Abstract

High-grade endometrial stromal sarcoma (HGESS) may harbor YWHAE-NUTM2A/B fusion, ZC3H7B-BCOR fusion, and BCOR internal tandem duplication (ITD). NTRK3 upregulation and pan-Trk expression were reported in soft tissue lesions that share similar morphology and genetic abnormalities. To confirm these findings in HGESS, differential expression analysis was performed at gene level comparing 11 HGESS with 48 other uterine sarcomas, including 9 low-grade endometrial stromal sarcomas, 23 undifferentiated uterine sarcomas, and 16 leiomyosarcomas, using targeted RNA sequencing data. Pan-Trk immunohistochemistry was performed on 35 HGESS, including 10 tumors with RNA expression data, with genotypes previously confirmed by targeted RNA sequencing, fluorescence in situ hybridization, and/or genomic PCR. Unsupervised hierarchical clustering of the top 25% of differentially expressed probes identified three molecular groups: (1) high NTRK3, FGFR3, RET, BCOR, GLI1, and PTCH1 and low ESR1 expression; (2) low NTRK3, FGFR3, RET, BCOR, GLI1, and PTCH1 and high ESR1 expression; and (3) low NTRK3, FGFR3, RET, BCOR, GLI1, PTCH1, and ESR1 expression. Among HGESS, 64% of tumors clustered in group 1, while 27% clustered in group 2. Cytoplasmic and/or nuclear pan-Trk staining of variable extent and intensity was seen in 91% of HGESS regardless of cyclin D1 and/or BCOR positivity. ER and PR expression was seen in 44% of HGESS despite ESR1 downregulation. Two patients with ER and PR positive but ESR1 downregulated stage I HGESS were treated with endocrine therapy, and both recurred at 12 and 36 months after primary resection. By RNA expression, HGESS appear homogenous and distinct from other uterine sarcomas by activation of kinases, including NTRK3, and sonic hedgehog pathway genes along with downregulation of ESR1. Most HGESS demonstrate pan-Trk staining which may serve as a diagnostic biomarker. ESR1 downregulation is seen in some HGESS that express ER and PR which raises implications in the utility of endocrine therapy in these patients.

Published

2021

32. Clinical sequencing of soft tissue and bone sarcomas delineates diverse genomic landscapes and potential therapeutic targets

Author

Benjamin A. Nacev, Francisco Sanchez-Vega, Shaleigh A. Smith, Cristina R. Antonescu, Evan Rosenbaum, Hongyu Shi, Cerise Tang, Nicholas D. Socci, Satshil Rana, Rodrigo Gularte-Mérida, Ahmet Zehir, Mrinal M. Gounder, Timothy G. Bowler, Anisha Luthra, Bhumika Jadeja, Azusa Okada, Jonathan A. Strong, Jake Stoller, Jason E. Chan, Ping Chi, Sandra P. D’Angelo, Mark A. Dickson, Ciara M. Kelly, Mary Louise Keohan, Sujana Movva, Katherine Thornton, Paul A. Meyers, Leonard H. Wexler, Emily K. Slotkin, Julia L. Glade Bender, Neerav N. Shukla, Martee L. Hensley, John H. Healey, Michael P. La Quaglia, Kaled M. Alektiar, Aimee M. Crago, Sam S. Yoon, Brian R. Untch, Sarah Chiang, Narasimhan P. Agaram, Meera R. Hameed, Michael F. Berger, David B. Solit, Nikolaus Schultz, Marc Ladanyi, Samuel Singer, and William D. Tap

Subjects

Osteosarcoma, Multidisciplinary, Humans, General Physics and Astronomy, Bone Neoplasms, Sarcoma, Soft Tissue Neoplasms, Genomics, General Chemistry, General Biochemistry, Genetics and Molecular Biology

Abstract

The genetic, biologic, and clinical heterogeneity of sarcomas poses a challenge for the identification of therapeutic targets, clinical research, and advancing patient care. Because there are > 100 sarcoma subtypes, in-depth genetic studies have focused on one or a few subtypes. Herein, we report a comparative genetic analysis of 2,138 sarcomas representing 45 pathological entities. This cohort is prospectively analyzed using targeted sequencing to characterize subtype-specific somatic alterations in targetable pathways, rates of whole genome doubling, mutational signatures, and subtype-agnostic genomic clusters. The most common alterations are in cell cycle control and TP53, receptor tyrosine kinases/PI3K/RAS, and epigenetic regulators. Subtype-specific associations include TERT amplification in intimal sarcoma and SWI/SNF alterations in uterine adenosarcoma. Tumor mutational burden, while low compared to other cancers, varies between and within subtypes. This resource will improve sarcoma models, motivate studies of subtype-specific alterations, and inform investigations of genetic factors and their correlations with treatment response.

Published

2022

33. Clinicopathologic and Genomic Analysis of TP53-Mutated Endometrial Carcinomas

Author

Lora H. Ellenson, Carol Aghajanian, Robert A. Soslow, Marc Ladanyi, Eric Rios-Doria, Nadeem R. Abu-Rustum, Kaled M. Alektiar, Chad M. Vanderbilt, Sarah Chiang, Britta Weigelt, Rajmohan Murali, Amir Momeni-Boroujeni, and Wissam Dahoud

Subjects

0301 basic medicine, Cancer Research, Pathology, medicine.medical_specialty, Massive parallel sequencing, endocrine system diseases, biology, business.industry, Not Otherwise Specified, Microsatellite instability, SPOP, medicine.disease, 03 medical and health sciences, Serous fluid, 030104 developmental biology, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, Carcinoma, medicine, biology.protein, PTEN, business, Clear cell

Abstract

Purpose: Copy number–high endometrial carcinomas were described by The Cancer Genome Atlas as high-grade endometrioid and serous cancers showing frequent copy-number alterations (CNA), low mutational burden (i.e., non-hypermutant), near-universal TP53 mutation, and unfavorable clinical outcomes. We sought to investigate and compare the clinicopathologic and molecular characteristics of non-hypermutant TP53-altered endometrial carcinomas of four histologic types. Experimental Design: TP53-mutated endometrial carcinomas, defined as TP53-mutant tumors lacking microsatellite instability or pathogenic POLE mutations, were identified (n = 238) in a cohort of 1,239 endometrial carcinomas subjected to clinical massively parallel sequencing of 410–468 cancer-related genes. Somatic mutations and CNAs (n = 238), and clinicopathologic features were determined (n = 185, initial treatment planning at our institution). Results: TP53-mutated endometrial carcinomas encompassed uterine serous (n = 102, 55.1%), high-grade endometrial carcinoma with ambiguous features/not otherwise specified (EC-NOS; n = 44, 23.8%), endometrioid carcinomas of all tumor grades (n = 28, 15.1%), and clear cell carcinomas (n = 11, 5.9%). PTEN mutations were significantly more frequent in endometrioid carcinomas, SPOP mutations in clear cell carcinomas, and CCNE1 amplification in serous carcinomas/EC-NOS; however, none of these genomic alterations were exclusive to any given histologic type. ERBB2 amplification was present at similar frequencies across TP53-mutated histologic types (7.7%–18.6%). Although overall survival was similar across histologic types, serous carcinomas presented more frequently at stage IV, had more persistent and/or recurrent disease, and reduced disease-free survival. Conclusions: TP53-mutated endometrial carcinomas display clinical and molecular similarities across histologic subtypes. Our data provide evidence to suggest performance of ERBB2 assessment in all TP53-mutated endometrial carcinomas. Given the distinct clinical features of serous carcinomas, histologic classification continues to be relevant.

Published

2021

34. Genomic Profiling Aids Classification of Diagnostically Challenging Uterine Mesenchymal Tumors With Myomelanocytic Differentiation

Author

Mamta Rao, Marc Ladanyi, Robert A. Soslow, Regina G. H. Beets-Tan, Rajmohan Murali, Ryma Benayed, Yanming Zhang, Achim A. Jungbluth, Carlene Gonzalez, Britta Weigelt, Niamh Conlon, Denise Frosina, Sarah Chiang, David M. Hyman, Martee L. Hensley, Pier Selenica, David B. Solit, RS: GROW - R3 - Innovative Cancer Diagnostics & Therapy, School Office GROW, and Faculteit FHML Centraal

Subjects

0301 basic medicine, Pathology, CELL NEOPLASM PECOMA, ENDOMETRIAL STROMAL SARCOMAS, medicine.disease_cause, melanocytic differentiation, 0302 clinical medicine, CDKN2A, SMOOTH-MUSCLE TUMORS, genetics, PRACTICAL ISSUES, Mutation, myomelanocytic differentiation, Sarcoma, Middle Aged, 030220 oncology & carcinogenesis, Uterine Neoplasms, Immunohistochemistry, Female, Anatomy, perivascular epithelioid cell tumor, Adult, Leiomyosarcoma, EXPRESSION, medicine.medical_specialty, allelic loss, Perivascular Epithelioid Cell Neoplasms, pecoma, Biology, Article, Pathology and Forensic Medicine, MED12, 03 medical and health sciences, leiomyoma, Biomarkers, Tumor, medicine, Humans, ATRX, Aged, TSC2 GENE, Endometrial stromal sarcoma, uterus, MUTATIONS, Gene Expression Profiling, leiomyosarcoma, medicine.disease, 030104 developmental biology, somatic mutations, Surgery, pathology

Abstract

Although diagnosis of high-grade uterine mesenchymal tumors (high-grade UMTs) exhibiting classic morphologic features is straightforward, diagnosis is more challenging in tumors in which prototypical features are poorly developed, focal and/or co-exist with features seen in other neoplasms. Here, we sought to define the repertoire of somatic genetic alterations in diagnostically challenging UMTs with myomelanocytic differentiation, including some reported as perivascular epithelioid cell tumors (PEComas). In 17 samples from 15 women, the tumors were histologically heterogeneous. Immunohistochemical expression of at least one melanocytic marker (HMB45, Melan-A or MiTF) was identified in all tumors, and of myogenic markers (desmin or SMA) in most tumors. Targeted massively parallel sequencing revealed several genetic alterations, most commonly in TP53 (41% mutation, 12% deletion), TSC2 (29% mutation, 6% deletion), RB1 (18% deletion), ATRX (24% mutation), MED12 (12% mutation), BRCA2 (12% deletion), CDKN2A (6% deletion) as well as FGFR3, NTRK1 and ERBB3 amplification (each 6%). Gene rearrangements (JAZF1-SUZ12; DNAJB6-PLAG1 and SFPQ-TFE3) were identified in three tumors. Integrating histopathologic, immunohistochemical and genetic findings, tumors from 4 patients were consistent with malignant PEComa (one TFE3-rearranged); 6 were classified as leiomyosarcomas; 3 showed overlapping features of PEComa and other sarcoma types (leiomyosarcoma or low-grade endometrial stromal sarcoma); and 2 were classified as sarcoma, not otherwise specified. Our findings suggest that diagnostically challenging UMTs with myomelanocytic differentiation represent a heterogeneous group of neoplasms which harbor a diverse repertoire of somatic genetic alterations; these genetic alterations can aid classification.

Published

2021

35. The impact of tumor fragmentation in patients with stage I uterine leiomyosarcoma on patterns of recurrence and oncologic outcome

Author

Nadeem R. Abu-Rustum, Jennifer J. Mueller, Alexia Iasonos, Sarah Chiang, Martee L. Hensley, Mario M. Leitao, Oliver Zivanovic, Silvana Pedra Nobre, Qin C. Zhou, Melody So, and Jennifer Ducie

Subjects

Adult, Leiomyosarcoma, 0301 basic medicine, medicine.medical_specialty, Mitotic index, Lymphovascular invasion, medicine.medical_treatment, Morcellation, Hysterectomy, Article, 03 medical and health sciences, Peritoneal cavity, Neoplasm Seeding, 0302 clinical medicine, Peritoneum, Humans, Medicine, Aged, Neoplasm Staging, Retrospective Studies, business.industry, Obstetrics and Gynecology, Middle Aged, Prognosis, Progression-Free Survival, Surgery, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Uterine Neoplasms, Cohort, Vagina, Female, Morcellator, Neoplasm Recurrence, Local, business

Abstract

Objective To evaluate the impact of tumor fragmentation on oncologic outcomes in patients with stage I uterine leiomyosarcoma (uLMS). Methods We identified all patients diagnosed with stage I uLMS presenting to our institution within three months of primary surgery, 1/2000–1/2019. Patients with recurrent disease were excluded. The non-morcellated group had total hysterectomy without documented specimen fragmentation; the morcellated group, total hysterectomy with documented specimen fragmentation. We defined fragmentation as manual fragmentation or morcellation (via power morcellator or otherwise) of the specimen in peritoneal cavity or vagina. Appropriate statistical analyses were performed. Results 152 patients met inclusion criteria. 107 (70%) underwent total hysterectomy (non-morcellated); 45 (30%) underwent morcellation. Median age at diagnosis for the entire cohort was 55 years (range 30–91). Median follow-up was 42.1 months (range 1.1–197.8). 40 (26.3%) patients had primary surgery at our institution, 112 (73.7%) at an outside hospital. In total 110 (72.3%) recurred: 72/107 (67.2%) non-morcellated; 38/44 (86.3%) morcellated. Median progression-free survival (PFS) for non-morcellated versus morcellated was 13.8 (95%CI 9.2–20.2) versus 7.3 months (95%CI 3–13.1), HR 1.5 (95%CI 1.02–2.24); P = 0.04. Median overall survival (OS) for non-morcellated versus morcellated was 82.1 (95%CI 52.4–122) versus 47.8 months (95%CI 28.5–129.6), HR 1.1 (95%CI 0.67–1.82); P = 0.7. Among patients with recurrence, 69.4% of non-morcellated recurred at hematogenous sites only, 18.1% recurred in peritoneum only; 28.9% of morcellated recurred at hematogenous sites, 63.2% in peritoneum. Race, lymphovascular invasion, postoperative chemotherapy, were independently associated with PFS. Mitotic index was independently associated with OS. Conclusions Tumor fragmentation/morcellation was associated with significantly higher risk of recurrence and a nearly 4-fold increase in peritoneal recurrence. Prognostic biomarkers remain important in predicting oncologic outcomes, independent of fragmentation or treatment.

Published

2021

36. Recent advances in smooth muscle tumors withPGRandPLAG1gene fusions and myofibroblastic uterine neoplasms

Author

Sarah Chiang

Subjects

Adult, Cancer Research, Pathology, medicine.medical_specialty, Uterus, Biology, Neoplasms, Muscle Tissue, 03 medical and health sciences, 0302 clinical medicine, Biomarkers, Tumor, Genetics, medicine, Humans, Epithelioid leiomyosarcoma, Uterine Neoplasm, Smooth Muscle Tumor, Gene Rearrangement, Mesenchymal stem cell, High-Throughput Nucleotide Sequencing, Middle Aged, DNA-Binding Proteins, body regions, medicine.anatomical_structure, PLAG1 gene, 030220 oncology & carcinogenesis, Uterine Neoplasms, Immunohistochemistry, Female, Gene Fusion, Receptors, Progesterone, Myxoid Leiomyosarcoma, Transcription Factors

Abstract

Uterine epithelioid and myxoid leiomyosarcomas and inflammatory myofibroblastic tumors are rare mesenchymal neoplasms. Next-generation sequencing recently detected novel PGR fusions in uterine epithelioid leiomyosarcomas that demonstrate characteristic rhabdoid and spindled morphology. PLAG1 gene fusions have also been identified in a subset of myxoid leiomyosarcomas and are associated with PLAG1 overexpression. ALK rearrangements underpin the vast majority of uterine inflammatory myofibroblastic tumors, which demonstrate morphologic, and immunohistochemical features similar to those of inflammatory myofibroblastic tumors elsewhere. This review summarizes the morphologic, immunophenotypic, and molecular genetic features of PGR fusion-positive epithelioid leiomyosarcoma, PLAG1 fusion-positive myxoid leiomyosarcoma, and inflammatory myofibroblastic tumors of the uterus.

Published

2020

37. State of the science: Uterine sarcomas: From pathology to practice

Author

Kevin Holcomb, Ramey D. Littell, Alexander Shushkevich, Martee L. Hensley, Michael D. Toboni, Mario M. Leitao, Naishadh A. Shah, Katherine Anne Thornton, Premal H. Thaker, Douglas A. Levine, Sarah Chiang, Brian M. Slomovitz, Jubilee Brown, Matthew A. Powell, Ann H. Klopp, and Sean C. Dowdy

Subjects

Leiomyosarcoma, 0301 basic medicine, medicine.medical_specialty, Antineoplastic Agents, Hormonal, Biopsy, Sarcoma, Endometrial Stromal, MEDLINE, Disease, Hysterectomy, Medical Oncology, Disease-Free Survival, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Carcinosarcoma, Uterine cancer, Biomarkers, Tumor, medicine, Adjuvant therapy, Humans, Uterine carcinosarcoma, Intensive care medicine, Endometrial Ablation Techniques, Adenosarcoma, business.industry, Endometrial cancer, Uterus, Obstetrics and Gynecology, Prognosis, medicine.disease, Carboplatin, Clinical trial, 030104 developmental biology, Oncology, chemistry, Chemotherapy, Adjuvant, 030220 oncology & carcinogenesis, Practice Guidelines as Topic, Uterine Neoplasms, Female, Radiotherapy, Adjuvant, Neoplasm Grading, Neoplasm Recurrence, Local, business

Abstract

Objective Uterine carcinosarcoma (UCS) is a rare but aggressive cancer. In early-stage disease data guiding treatment is sparse. The purpose of this review is to summarize the findings from the 2019 NRG oncology group summer symposium meeting as well as a review of the current literature, with a particular focus on molecular targets, ongoing clinical trials, and treatment of early and advanced/recurrent disease. Methods A combination of expert presentations and an extensive literature search was undertaken to summarize the literature in this review. MEDLINE was queried for peer-reviewed publications on UCS. This search was not limited by year or study design, but was limited to English language publications. ClinicalTrials.gov was queried for ongoing trials in UCS. Results UCS is a rare cancer that is biphasic, with the carcinomatous component driving its aggressive nature. Level 3 evidence regarding early stage disease is lacking, but retrospective data suggests adjuvant therapy is warranted. The recent results of GOG 261 have contributed valuable information towards treatment strategy, including use of paclitaxel and carboplatin for UCS. Clinical trials are ongoing to investigate new targeted agents in UCS. Conclusion Ongoing endometrial cancer clinical trials now include UCS patients. In combination with advances in molecular profiling, this will provide patients with UCS improved therapeutic options. Until that time, surgical resection and traditional cytotoxic chemotherapy remains standard of care.

Published

2020

38. High-Grade Sarcomas with Myogenic Differentiation Harboring Hotspot PDGFRB Mutations

Author

Josephine K. Dermawan, Sarah Chiang, Martee L. Hensley, William D. Tap, and Cristina R. Antonescu

Subjects

Pathology and Forensic Medicine

Published

2023

39. Molecular-Based Immunohistochemical Algorithm for Uterine Leiomyosarcoma Diagnosis

Author

Amir Momeni-Boroujeni, Elham Yousefi, Ridin Balakrishnan, Stephanie Riviere, Elizabeth Kertowidjojo, Martee L. Hensley, Marc Ladanyi, Lora H. Ellenson, and Sarah Chiang

Subjects

Pathology and Forensic Medicine

Published

2023

40. High-Grade Endometrial Stromal Sarcomas With YWHAE::NUTM2 Gene Fusion Exhibit Recurrent CDKN2A Alterations and Absence of p16 Staining is a Poor Prognostic Marker

Author

Felix K.F. Kommoss, Lisa-Marie Mar, Brooke E. Howitt, Krisztina Hanley, Gulisa Turashvilli, Rolf Buslei, Julie A. Irving, Brendan C. Dickson, Christian Koelsche, Hans-Peter Sinn, Peter Schirmacher, Andreas von Deimling, Sarah Chiang, W. Glenn McCluggage, Sabrina Croce, Colin J.R. Stewart, and Cheng-Han Lee

Subjects

Pathology and Forensic Medicine

Published

2023

41. Mesenchymal Tumors, Pathology of the Uterine Corpus

Author

Sarah Chiang

Published

2022

42. Inhibition of CXCR4 Enhances the Efficacy of Radiotherapy in Metastatic Prostate Cancer Models

Author

Nisha Gupta, Hiroki Ochiai, Yoshinori Hoshino, Sebastian Klein, Jozef Zustin, Rakesh R. Ramjiawan, Shuji Kitahara, Nir Maimon, Despina Bazou, Sarah Chiang, Sen Li, Daniel H. Schanne, Rakesh. K. Jain, Lance L. Munn, Peigen Huang, Sergey V. Kozin, and Dan G. Duda

Subjects

primary lesions, Cancer Research, bone metastases, Oncology, orthotopic mouse models, prostate cancer, radiotherapy, SDF1α/CXCR4 signaling, vascular normalization

Abstract

Radiotherapy (RT) is a standard treatment for patients with advanced prostate cancer (PCa). Previous preclinical studies showed that SDF1α/CXCR4 axis could mediate PCa metastasis (most often to the bones) and cancer resistance to RT. We found high levels of expression for both SDF1α and its receptor CXCR4 in primary and metastatic PCa tissue samples. In vitro analyses using PCa cells revealed an important role of CXCR4 in cell invasion but not radiotolerance. Pharmacologic inhibition of CXCR4 using AMD3100 showed no efficacy in orthotopic primary and bone metastatic PCa models. However, when combined with RT, AMD3100 potentiated the effect of local single-dose RT (12 Gy) in both models. Moreover, CXCR4 inhibition also reduced lymph node metastasis from primary PCa. Notably, CXCR4 inhibition promoted the normalization of bone metastatic PCa vasculature and reduced tissue hypoxia. In conclusion, the SDF1α/CXCR4 axis is a potential therapeutic target in metastatic PCa patients treated with RT.

Published

2023

43. Clinical sequencing of soft tissue and bone sarcomas delineates diverse genomic landscapes and potential therapeutic targets

Author

Cerise Tang, Hongyu Shi, Timothy G. Bowler, Jake Stoller, Meera Hameed, Neerav Shukla, John H. Healey, Sandra P. D'Angelo, Aimee M. Crago, Ciara Marie Kelly, Mary Louise Keohan, Emily K. Slotkin, Nicholas D. Socci, Cristina R. Antonescu, Ping Chi, Leonard H. Wexler, Samuel Singer, Azusa Okada, Michael P. La Quaglia, Ahmet Zehir, Julia Glade Bender, Satshil Rana, Evan Rosenbaum, Brian R. Untch, Nikolaus Schultz, Jason E. Chan, Jonathan A. Strong, Sujana Movva, Benjamin A. Nacev, Mrinal M. Gounder, David B. Solit, Kaled M. Alektiar, Paul A. Meyers, Shaleigh A. Smith, Rodrigo Gularte-Mérida, Bhumika Jadeja, Martee L. Hensley, Sarah Chiang, Francisco Sanchez-Vega, Sam S. Yoon, Narasimhan P. Agaram, Mark A. Dickson, Katherine Thornton, Michael F. Berger, William D. Tap, Anisha Luthra, and Marc Ladanyi

Subjects

Clinical research, Somatic cell, biology.protein, medicine, Cancer research, Sarcoma, Epigenetics, Biology, Bone Sarcoma, medicine.disease, Genome, Receptor tyrosine kinase, PI3K/AKT/mTOR pathway

Abstract

The genetic, biologic, and clinical heterogeneity of sarcomas poses a challenge for the identification of therapeutic targets, clinical research, and advancing patient care. Because there are > 100 sarcoma subtypes, in-depth genetic studies have focused on one or a few subtypes. Herein, we report a comparative genetic analyses analysis of 2,138 sarcomas representing 45 pathological entities. This cohort was prospectively analyzed using targeted sequencing to characterize subtype-specific somatic alterations in targetable pathways, rates of whole genome doubling, mutational signatures, and subtype-agnostic genomic clusters. The most common alterations were in cell cycle control andTP53, receptor tyrosine kinases/PI3K/RAS, and epigenetic regulators. Subtype-specific associations includedTERTamplification in intimal sarcoma and SWI/SNF alterations in uterine adenosarcoma. Tumor mutational burden, while low compared to other cancers, varied between and within subtypes. This resource will improve sarcoma models, motivate studies of subtype-specific alterations, and inform investigations of genetic factors and their correlations with treatment response.

Published

2021

44. ESR1 hotspot mutations in endometrial stromal sarcoma with high-grade transformation and endocrine treatment

Author

Kimberly Dessources, Kathryn M. Miller, Elizabeth Kertowidjojo, Arnaud Da Cruz Paula, Youran Zou, Pier Selenica, Edaise M. da Silva, Ryma Benayed, Charles W. Ashley, Nadeem R. Abu-Rustum, Snjezana Dogan, Robert A. Soslow, Martee L. Hensley, Britta Weigelt, and Sarah Chiang

Subjects

Recurrence, Sarcoma, Endometrial Stromal, Mutation, Estrogen Receptor alpha, Humans, RNA, Female, Pathology and Forensic Medicine, Endometrial Neoplasms

Abstract

High-grade endometrial stromal sarcomas (HGESSs) are more aggressive and have higher rates of resistance to endocrine therapy than low-grade endometrial stromal sarcomas (LGESSs). The pathogenesis of hormonal resistance in these lesions has yet to be defined. Here we sought to histologically and genetically characterize 3 LGESSs and their recurrences that underwent histologic high-grade transformation following endocrine therapy. For this, DNA from primary tumors and select subsequent recurrences were subject to massively parallel sequencing targeting 468 cancer-related genes. Somatic mutation analyses were performed using validated bioinformatics methods. In addition, RNA from each case was evaluated for the presence of gene fusions using targeted RNA-sequencing. All patients initially presented with LGESS, developed HGESS recurrences, and received at least 2 lines of hormonal suppressive therapy. Gene fusions classically described as associated with LGESS were identified in all 3 cases, including JAZF1-PHF1, EPC1-PHF1 and JAZF1-SUZ12 fusions for Cases 1, 2 and 3, respectively. Targeted sequencing analysis revealed that none of the primary LGESS, however the HGESS recurrences of Cases 1 and 3, and the LGESS and HGESS recurrences of Case 2 post endocrine treatment harbored ESR1 p.Y537S hotspot mutations. These ESR1 ligand-binding domain mutations have been found as a mechanism of acquired endocrine resistance in breast cancer. Also, a reduction in estrogen receptor (ER) expression was observed in recurrences. Our findings suggest that the ESR1 p.Y537S hotspot mutation in LGESS with histologic high-grade transformation may be associated with endocrine resistance in these lesions. Furthermore, our data suggest that genetic analyses may be performed in recurrent LGESS following hormonal therapy, development of high-grade morphology, and/or altered/diminished ER expression.

Published

2021

45. Integrated Analysis of Ovarian Juvenile Granulosa Cell Tumors Reveals Distinct Epigenetic Signatures and Recurrent TERT Rearrangements

Author

Theodore Vougiouklakis, Kelsey Zhu, Varshini Vasudevaraja, Jonathan Serrano, Guomiao Shen, Rebecca L. Linn, Xiaojun Feng, Sarah Chiang, Julieta E. Barroeta, Kristen M. Thomas, Lauren E. Schwartz, Pratibha S. Shukla, Anais Malpica, Esther Oliva, Paolo Cotzia, Deborah F. DeLair, Matija Snuderl, and George Jour

Subjects

Adult, DEAD-box RNA Helicases, Epigenomics, Ovarian Neoplasms, Ribonuclease III, Cancer Research, Oncology, Mutation, Humans, Female, Telomerase, Epigenesis, Genetic, Granulosa Cell Tumor

Abstract

Purpose: Adult granulosa cell tumor (AGCT) is characterized by the somatic FOXL2 p.C134W mutation, and recurrences have been associated with TERT promoter and KMT2D-truncating mutations. Conversely, the molecular underpinnings of the rare juvenile granulosa cell tumor (JGCT) have not been well elucidated. To this end, we applied a tumor-only integrated approach to investigate the genomic, transcriptomic, and epigenomic landscape of 31 JGCTs to identify putative oncogenic drivers. Experimental Design: Multipronged analyses of 31 JGCTs were performed utilizing a clinically validated next-generation sequencing (NGS) panel targeting 580 cancer-related genes for genomic interrogation, in addition to targeted RNA NGS for transcriptomic exploration. Genome-wide DNA methylation profiling was conducted using an Infinium Methylation EPIC array targeting 866,562 CpG methylation sites. Results: We identified frequent KMT2C-truncating mutations along with other mutated genes implicated in the switch/sucrose nonfermentable (SWI/SNF) chromatin remodeling complex, in addition to previously reported hotspot AKT1 and DICER1 mutations. Targeted transcriptome sequencing revealed recurrent TERT rearrangements (13%) involving partners CLPTM1L or DROSHA, and differential gene expression analysis showed FGFR1 upregulation in the TERT non-rearranged JGCTs under direct promoter control. Genome-wide DNA methylation rendered a clear delineation between AGCTs and JGCTs at the epigenomic level, further supporting its diagnostic utility in distinguishing among these tumors. Conclusions: This is the largest comprehensive molecular study of JGCTs, where we further expand our current understanding of JGCT pathogenesis and demonstrate putative oncogenic drivers and TERT rearrangements in a subset of tumors. Our findings further offer insights into possible targeted therapies in a rare entity.

Published

2021

46. Uterine Cervical Sarcoma With a Novel RET-SPECC1L Fusion in an Adult

Author

Morgan Altinok, David M. Kushner, Elizabeth L Dickson Michelson, Paul Weisman, Sarah Chiang, Marc Ladanyi, Erica Carballo, Jessica J.F. Kram, and Darya Buehler

Subjects

Fusion gene, business.industry, Treatment outcome, medicine, Cancer research, Surgery, Gene rearrangement, Sarcoma, Anatomy, medicine.disease, business, Homology (biology), Pathology and Forensic Medicine

Published

2019

47. Extramammary Paget disease shows differential expression of B7 family members B7-H3, B7-H4, PD-L1, PD-L2 and cancer/testis antigens NY-ESO-1 and MAGE-A

Author

Travis J. Hollmann, Maryam Pourmaleki, Jonathan H. Young, Marcia Edelweiss, Dennis S. Chi, Sarah Chiang, Lev Roshal, Ingo K. Mellinghoff, Klaus J. Busam, Yanyun Li, Nicholas D. Socci, and Mianlei Zhang

Subjects

0301 basic medicine, Surgical margin, medicine.medical_treatment, 03 medical and health sciences, 0302 clinical medicine, Antigen, PD-L1, cancer/testis antigens, medicine, B7 family, biology, business.industry, Cancer, Immunotherapy, medicine.disease, 3. Good health, extramammary paget disease, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Cancer/testis antigens, Adenocarcinoma, immunotherapy, NY-ESO-1, business, Research Paper, targetable molecules

Abstract

Extramammary Paget disease (EMPD) is a rare cutaneous adenocarcinoma of the anogenital region most commonly treated with surgical excision. Surgical margin clearance is often problematic and recurrence rates remain high indicating the need for additional therapeutic options. Topical immunomodulators have been used with reported success suggesting EMPD may respond to other immunotherapies. This study investigates EMPD protein expression of targetable B7 family members and cancer/testis antigens (CTAs) B7-H3, B7-H4, PD-L1, PD-L2, MAGE-A, and NY-ESO-1 and components of antigen presenting machinery B2M and MHC-I. Fifty-seven specimens from 48 patients (31 female and 17 male), representing in situ, invasive, and metastatic disease of primary and secondary origin were stained and scored (627 total slides). The percentage of cases expressing each immune regulatory molecule in the in situ followed by invasive tumor components was: B7-H3 (94, 90), B7-H4 (82, 78), PD-L1 (6, 10), MAGE-A (39, 50), NY-ESO-1 (16, 20), B2M (100, 89), and MHC-I (78, 79). PD-L2 was negative in all cases. There was high correlation between marker expression within the in situ and invasive tumor components of the same case. B7-H4 was preferentially expressed in primary cutaneous EMPD. Co-expression of B7 family members B7-H3 and B7-H4 was found within the in situ and invasive tumor components of 74% and 48% of cases, respectively. These findings provide an initial characterization of EMPD tumor cell expression of B7-H3, B7-H4, PD-L1, PD-L2, MAGE-A, and NY-ESO-1 and indicate the potential for new immunotherapeutic options for patients with EMPD.

Published

2019

48. DNA methylation-based classification of sinonasal undifferentiated carcinoma

Author

Marc Cohen, Amir Momeni Boroujeni, Marc Ladanyi, Ryan Ptashkin, Michael F. Berger, Matija Snuderl, Deborah J. Chute, Snjezana Dogan, Ian Ganly, Hun Jae Jung, Sarah Chiang, Varshini Vasudevaraja, Bin Xu, Achim A. Jungbluth, Ronald Ghossein, and Jonathan Serrano

Subjects

Adult, Male, 0301 basic medicine, Pathology, medicine.medical_specialty, ARID1A, Maxillary Sinus Neoplasms, Biology, Article, Pathology and Forensic Medicine, Young Adult, 03 medical and health sciences, Sinonasal undifferentiated carcinoma, 0302 clinical medicine, Carcinoma, medicine, Humans, Carcinoma, Small Cell, Aged, Aged, 80 and over, Olfactory Neuroblastoma, Large cell, SMARCB1 Protein, Methylation, DNA Methylation, Middle Aged, medicine.disease, Immunohistochemistry, Isocitrate Dehydrogenase, Carcinoma, Neuroendocrine, 030104 developmental biology, CpG site, 030220 oncology & carcinogenesis, Mutation, DNA methylation, Female

Abstract

Sinonasal undifferentiated carcinoma (SNUC) is an aggressive malignancy harboring IDH2 R172 mutations in >80% cases. We explored the potential of genome-wide DNA methylation profiling to elucidate tumor biology and improve the diagnosis of sinonasal undifferentiated carcinoma and its histologic mimics. Forty-two cases, including sinonasal undifferentiated, large cell neuroendocrine, small cell neuroendocrine, and SMARCB1-deficient carcinomas and olfactory neuroblastoma, were profiled by Illumina Infinium Methylation EPIC array interrogating >850,000 CpG sites. The data were analyzed using a custom bioinformatics pipeline. IDH2 mutation status was determined by the targeted exome sequencing (MSK- IMPACTTM) in most cases. H3K27 methylation level was assessed by the immunohistochemistry-based H-score. DNA methylation-based semi-supervised hierarchical clustering analysis segregated IDH2 mutants, mostly sinonasal undifferentiated (n = 10) and large cell neuroendocrine carcinomas (n = 4), from other sinonasal tumors, and formed a single cluster irrespective of the histologic type. t-distributed stochastic neighbor embedding dimensionality reduction analysis showed no overlap between IDH2 mutants, SMARCB1-deficient carcinoma and olfactory neuroblastoma. IDH2 mutants demonstrated a global methylation phenotype and an increase in repressive trimethylation of H3K27 in comparison to IDH2 wild-type tumors (p < 0.001). Kyoto Encyclopedia of Genes and Genomes (KEGG) pathway analysis showed no difference in pathway activation between IDH2-mutated sinonasal undifferentiated and large cell neuroendocrine carcinomas. In comparison to SMARCB1-deficient, IDH2-mutated carcinomas were associated with better disease-free survival (p = 0.034) and lower propensity for lung metastasis (p = 0.002). ARID1A mutations were common in small cell neuroendocrine carcinoma but not among IDH2 mutants (3/3 versus 0/18 and p < 0.001). IDH2 mutations in sinonasal carcinomas induce a hypermethylator phenotype and define a molecular subgroup of tumors arising in this location. IDH2- mutated sinonasal undifferentiated carcinoma and large cell neuroendocrine carcinoma likely represent a phenotypic spectrum of the same entity, which is distinct from small cell neuroendocrine and SMARCB1-deficient sinonasal carcinomas. DNA methylation-based analysis of the sinonasal tumors has potential to improve the diagnostic accuracy and classification of tumors arising in this location.

Published

2019

49. Novel PLAG1 Gene Rearrangement Distinguishes a Subset of Uterine Myxoid Leiomyosarcoma From Other Uterine Myxoid Mesenchymal Tumors

Author

Marc Ladanyi, Javier A. Arias-Stella, Robert H. Young, Esther Oliva, Robert A. Soslow, Denise Frosina, Cheng-Han Lee, Sarah Chiang, Achim A. Jungbluth, Cristina R. Antonescu, Lien N. Hoang, and Ryma Benayed

Subjects

Adult, Leiomyosarcoma, 0301 basic medicine, Pathology, medicine.medical_specialty, Biology, Article, Pathology and Forensic Medicine, Diagnosis, Differential, 03 medical and health sciences, 0302 clinical medicine, HMGA2, Biomarkers, Tumor, medicine, Humans, Aged, Gene Rearrangement, Mesenchymal stem cell, RNA, Gene rearrangement, Middle Aged, DNA-Binding Proteins, body regions, 030104 developmental biology, PLAG1 gene, 030220 oncology & carcinogenesis, Uterine Neoplasms, biology.protein, Female, Surgery, Anatomy, Myxoid Leiomyosarcoma

Abstract

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 ALK break-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 BCOR and ALK rearrangements. These 15 patients presented at a median age of 50 years with stage I (3), II (2), III (2), and IV (1), 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

Published

2019

50. Evaluating The Use Of Glass, Wifi And Mac Scores As Predictors Of Limb Salvage Success In Patients Receiving Free Tissue Transfer For Chronic Lower Extremity Wounds

Author

Hayden Schott, Sarah Chiang, Rachel Skladman, Gayan De Silva, Patrick Geraghty, and John Felder

Subjects

Surgery, Cardiology and Cardiovascular Medicine

Published

2022