Your search keyword '"Rossitza Christova"' showing total 35 results

1. Systematic study of tissue factor expression in solid tumors

Author

Johann S. deBono, Jeffrey R. Harris, Saskia M. Burm, Adriaan Vanderstichele, Mischa A. Houtkamp, Saida Aarass, Ruth Riisnaes, Ines Figueiredo, Daniel Nava Rodrigues, Rossitza Christova, Siel Olbrecht, Hans W. M. Niessen, Sigrid R. Ruuls, Danita H. Schuurhuis, Jeroen J. Lammerts van Bueren, Esther C. W. Breij, and Ignace Vergote

Subjects

biopsies expression, immunohistochemistry, solid tumor, targeted therapy, tissue factor, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Elevated tissue factor (TF) expression, although restricted in normal tissue, has been reported in multiple solid cancers, and expression has been associated with poor prognosis. This manuscript compares TF expression across various solid tumor types via immunohistochemistry in a single study, which has not been performed previously. Aims To increase insight in the prevalence and cellular localization of TF expression across solid cancer types, we performed a detailed and systematic analysis of TF expression in tumor tissue obtained from patients with ovarian, esophageal, bladder, cervical, endometrial, pancreatic, prostate, colon, breast, non‐small cell lung cancer (NSCLC), head and neck squamous cell carcinoma (HNSCC), and glioblastoma. The spatial and temporal variation of TF expression was analyzed over time and upon disease progression in patient‐matched biopsies taken at different timepoints. In addition, TF expression in patient‐matched primary tumor and metastatic lesions was also analyzed. Methods and Results TF expression was detected via immunohistochemistry (IHC) using a validated TF‐specific antibody. TF was expressed in all cancer types tested, with highest prevalence in pancreatic cancer, cervical cancer, colon cancer, glioblastoma, HNSCC, and NSCLC, and lowest in breast cancer. Staining was predominantly membranous in pancreatic, cervical, and HNSCC, and cytoplasmic in glioblastoma and bladder cancer. In general, expression was consistent between biopsies obtained from the same patient over time, although variability was observed for individual patients. NSCLC biopsies of primary tumor and matched lymph node metastases showed no clear difference in TF expression overall, although individual patient changes were observed. Conclusion This study shows that TF is expressed across a broad range of solid cancer types, and expression is present upon tumor dissemination and over the course of treatment.

Published

2023

2. Figure S1 from HER3 Is an Actionable Target in Advanced Prostate Cancer

Author

Johann de Bono, Wei Yuan, Jonathan Welti, Antje Neeb, Andrea Alimonti, Michael M. Shen, Andrea Califano, Amanda Swain, Paul Workman, Suzanne Carreira, Jian Ning, Lorenzo Buroni, Claudia Bertan, Alec Paschalis, Christina Guo, Nina Tunariu, Caterina Aversa, Pasquale Rescigno, Diletta Bianchini, Semini Sumanasuriya, Gunther Boysen, Gemma Fowler, Penny Flohr, Rita Pereira, Matthew Clarke, Abdullah Alajati, Jan Rekowski, David Dolling, Maryou Lambros, Ines Figueiredo, George Seed, Rossitza Christova, Beshara Sheehan, Adam Sharp, Martina Troiani, Daniela Brina, Ana Ferreira, Mateus Crespo, Alessandro Vasciaveo, Mariantonietta D’Ambrosio, Bora Gurel, Ruth Riisnaes, Susana Miranda, and Veronica Gil

Abstract

Supplementary Figure S1

Published

2023

3. Supplementary Data from HER3 Is an Actionable Target in Advanced Prostate Cancer

Author

Johann de Bono, Wei Yuan, Jonathan Welti, Antje Neeb, Andrea Alimonti, Michael M. Shen, Andrea Califano, Amanda Swain, Paul Workman, Suzanne Carreira, Jian Ning, Lorenzo Buroni, Claudia Bertan, Alec Paschalis, Christina Guo, Nina Tunariu, Caterina Aversa, Pasquale Rescigno, Diletta Bianchini, Semini Sumanasuriya, Gunther Boysen, Gemma Fowler, Penny Flohr, Rita Pereira, Matthew Clarke, Abdullah Alajati, Jan Rekowski, David Dolling, Maryou Lambros, Ines Figueiredo, George Seed, Rossitza Christova, Beshara Sheehan, Adam Sharp, Martina Troiani, Daniela Brina, Ana Ferreira, Mateus Crespo, Alessandro Vasciaveo, Mariantonietta D’Ambrosio, Bora Gurel, Ruth Riisnaes, Susana Miranda, and Veronica Gil

Abstract

Supplementary methods and Supplementary figure legends - Tracked Changes

Published

2023

4. Data from HER3 Is an Actionable Target in Advanced Prostate Cancer

Author

Johann de Bono, Wei Yuan, Jonathan Welti, Antje Neeb, Andrea Alimonti, Michael M. Shen, Andrea Califano, Amanda Swain, Paul Workman, Suzanne Carreira, Jian Ning, Lorenzo Buroni, Claudia Bertan, Alec Paschalis, Christina Guo, Nina Tunariu, Caterina Aversa, Pasquale Rescigno, Diletta Bianchini, Semini Sumanasuriya, Gunther Boysen, Gemma Fowler, Penny Flohr, Rita Pereira, Matthew Clarke, Abdullah Alajati, Jan Rekowski, David Dolling, Maryou Lambros, Ines Figueiredo, George Seed, Rossitza Christova, Beshara Sheehan, Adam Sharp, Martina Troiani, Daniela Brina, Ana Ferreira, Mateus Crespo, Alessandro Vasciaveo, Mariantonietta D’Ambrosio, Bora Gurel, Ruth Riisnaes, Susana Miranda, and Veronica Gil

Abstract

It has been recognized for decades that ERBB signaling is important in prostate cancer, but targeting ERBB receptors as a therapeutic strategy for prostate cancer has been ineffective clinically. However, we show here that membranous HER3 protein is commonly highly expressed in lethal prostate cancer, associating with reduced time to castration resistance (CR) and survival. Multiplex immunofluorescence indicated that the HER3 ligand NRG1 is detectable primarily in tumor-infiltrating myelomonocytic cells in human prostate cancer; this observation was confirmed using single-cell RNA sequencing of human prostate cancer biopsies and murine transgenic prostate cancer models. In castration-resistant prostate cancer (CRPC) patient-derived xenograft organoids with high HER3 expression as well as mouse prostate cancer organoids, recombinant NRG1 enhanced proliferation and survival. Supernatant from murine bone marrow–derived macrophages and myeloid-derived suppressor cells promoted murine prostate cancer organoid growth in vitro, which could be reversed by a neutralizing anti-NRG1 antibody and ERBB inhibition. Targeting HER3, especially with the HER3-directed antibody–drug conjugate U3-1402, exhibited antitumor activity against HER3-expressing prostate cancer. Overall, these data indicate that HER3 is commonly overexpressed in lethal prostate cancer and can be activated by NRG1 secreted by myelomonocytic cells in the tumor microenvironment, supporting HER3-targeted therapeutic strategies for treating HER3-expressing advanced CRPC.Significance:HER3 is an actionable target in prostate cancer, especially with anti-HER3 immunoconjugates, and targeting HER3 warrants clinical evaluation in prospective trials.

Published

2023

5. Supplementary Table S1 and Fig S1 and S2 from Selective Inhibition of SIN3 Corepressor with Avermectins as a Novel Therapeutic Strategy in Triple-Negative Breast Cancer

Author

Samuel Waxman, Ming-Ming Zhou, Eduardo Farias, Arthur Zelent, Christopher J. Lord, Alan Ashworth, Yordan Sbirkov, Rachel Brough, Jessica Frankum, Edgardo V. Ariztia, Rajal Sharma, Shuai Yang, Nidhi Bansal, Rossitza Christova, Veronica Gil, Louise Howell, Mihaly Mezei, Lei Zeng, Boris A. Leibovitch, Kevin Petrie, and Yeon-Jin Kwon

Abstract

Supplementary Table S1 and Fig S1 and S2. Supplementary Table 1: qPCR primers used in this study; Supplementary Figure S1: Structures of compounds screened in Figure 1A and 1B; Supplementary Figure S2: Proximity ligation assay (PLA) analyzing SIN3A-MAD interactions

Published

2023

6. Supplementary Table S2 from Selective Inhibition of SIN3 Corepressor with Avermectins as a Novel Therapeutic Strategy in Triple-Negative Breast Cancer

Author

Samuel Waxman, Ming-Ming Zhou, Eduardo Farias, Arthur Zelent, Christopher J. Lord, Alan Ashworth, Yordan Sbirkov, Rachel Brough, Jessica Frankum, Edgardo V. Ariztia, Rajal Sharma, Shuai Yang, Nidhi Bansal, Rossitza Christova, Veronica Gil, Louise Howell, Mihaly Mezei, Lei Zeng, Boris A. Leibovitch, Kevin Petrie, and Yeon-Jin Kwon

Abstract

Supplementary Table S2. List of genes with expression regulated by selamectin treatment

Published

2023

7. Data from Selective Inhibition of SIN3 Corepressor with Avermectins as a Novel Therapeutic Strategy in Triple-Negative Breast Cancer

Author

Samuel Waxman, Ming-Ming Zhou, Eduardo Farias, Arthur Zelent, Christopher J. Lord, Alan Ashworth, Yordan Sbirkov, Rachel Brough, Jessica Frankum, Edgardo V. Ariztia, Rajal Sharma, Shuai Yang, Nidhi Bansal, Rossitza Christova, Veronica Gil, Louise Howell, Mihaly Mezei, Lei Zeng, Boris A. Leibovitch, Kevin Petrie, and Yeon-Jin Kwon

Abstract

Triple-negative breast cancers (TNBC) lacking estrogen, progesterone, and HER2 receptors account for 10% to 20% of breast cancer and are indicative of poor prognosis. The development of effective treatment strategies therefore represents a pressing unmet clinical need. We previously identified a molecularly targeted approach to target aberrant epigenetics of TNBC using a peptide corresponding to the SIN3 interaction domain (SID) of MAD. SID peptide selectively blocked binding of SID-containing proteins to the paired α-helix (PAH2) domain of SIN3, resulting in epigenetic and transcriptional modulation of genes associated with epithelial–mesenchymal transition (EMT). To find small molecule inhibitor (SMI) mimetics of SID peptide, we performed an in silico screen for PAH2 domain–binding compounds. This led to the identification of the avermectin macrocyclic lactone derivatives selamectin and ivermectin (Mectizan) as candidate compounds. Both selamectin and ivermectin phenocopied the effects of SID peptide to block SIN3–PAH2 interaction with MAD, induce expression of CDH1 and ESR1, and restore tamoxifen sensitivity in MDA-MB-231 human and MMTV-Myc mouse TNBC cells in vitro. Treatment with selamectin or ivermectin led to transcriptional modulation of genes associated with EMT and maintenance of a cancer stem cell phenotype in TNBC cells. This resulted in impairment of clonogenic self-renewal in vitro and inhibition of tumor growth and metastasis in vivo. Underlining the potential of avermectins in TNBC, pathway analysis revealed that selamectin also modulated the expression of therapeutically targetable genes. Consistent with this, an unbiased drug screen in TNBC cells identified selamectin-induced sensitization to a number of drugs, including those targeting modulated genes. Mol Cancer Ther; 14(8); 1824–36. ©2015 AACR.

Published

2023

8. Legends supplementary figures/ tables from SPOP-Mutated/CHD1-Deleted Lethal Prostate Cancer and Abiraterone Sensitivity

Author

Johann S. de Bono, Joaquin Mateo, Suzanne Carreira, Christopher E. Barbieri, Wei Yuan, Mark A. Rubin, Theresa MacDonald, Adam Sharp, Jane Goodall, Matthew Clarke, Mark Atkin, Flavia M. de Oliveira, Claudia Bertan, Sara Aziz, Veronica Gil, Rossitza Christova, Ana Ferreira, Inês Figueiredo, Susana Miranda, Nina Tunariu, Raquel Perez-Lopez, Deirdre Moloney, Joanne Hunt, Diletta Bianchini, Semini Sumanasuriya, Zafeiris Zafeiriou, Mateus Crespo, Ruth Riisnaes, David Dolling, George Seed, Pasquale Rescigno, Daniel N. Rodrigues, and Gunther Boysen

Abstract

Supplementary figure and table legends

Published

2023

9. Supplementary Figure from JMJD6 Is a Druggable Oxygenase That Regulates AR-V7 Expression in Prostate Cancer

Author

Johann S. de Bono, Adam Sharp, Stephen R. Plymate, Christopher J. Schofield, Bissan Al-Lazikani, Andrea Alimonti, Nina Tunariu, Suzanne Carreira, Maryou B. Lambros, Susana Miranda, Mateus Crespo, Lorenzo Buroni, Veronica S. Gil, Rossitza Christova, Bora Gurel, Akane Kawamura, Martine Abboud, Marc A. Moesser, Md. Saiful Islam, Anthony Tumber, Patrizio Di Micco, Takuma Uo, Soojin Kim, Juan M. Jiménez-Vacas, Daniel Nava Rodrigues, Ruth Riisnaes, Ana Ferreira, Rita Pereira, Ines Figueiredo, Wei Yuan, Antje J. Neeb, Jonathan Welti, and Alec Paschalis

Abstract

Supplementary Figure from JMJD6 Is a Druggable Oxygenase That Regulates AR-V7 Expression in Prostate Cancer

Published

2023

10. Supplementary Table from JMJD6 Is a Druggable Oxygenase That Regulates AR-V7 Expression in Prostate Cancer

Author

Johann S. de Bono, Adam Sharp, Stephen R. Plymate, Christopher J. Schofield, Bissan Al-Lazikani, Andrea Alimonti, Nina Tunariu, Suzanne Carreira, Maryou B. Lambros, Susana Miranda, Mateus Crespo, Lorenzo Buroni, Veronica S. Gil, Rossitza Christova, Bora Gurel, Akane Kawamura, Martine Abboud, Marc A. Moesser, Md. Saiful Islam, Anthony Tumber, Patrizio Di Micco, Takuma Uo, Soojin Kim, Juan M. Jiménez-Vacas, Daniel Nava Rodrigues, Ruth Riisnaes, Ana Ferreira, Rita Pereira, Ines Figueiredo, Wei Yuan, Antje J. Neeb, Jonathan Welti, and Alec Paschalis

Abstract

Supplementary Table from JMJD6 Is a Druggable Oxygenase That Regulates AR-V7 Expression in Prostate Cancer

Published

2023

11. Supplementary Figure 2 from SPOP-Mutated/CHD1-Deleted Lethal Prostate Cancer and Abiraterone Sensitivity

Author

Johann S. de Bono, Joaquin Mateo, Suzanne Carreira, Christopher E. Barbieri, Wei Yuan, Mark A. Rubin, Theresa MacDonald, Adam Sharp, Jane Goodall, Matthew Clarke, Mark Atkin, Flavia M. de Oliveira, Claudia Bertan, Sara Aziz, Veronica Gil, Rossitza Christova, Ana Ferreira, Inês Figueiredo, Susana Miranda, Nina Tunariu, Raquel Perez-Lopez, Deirdre Moloney, Joanne Hunt, Diletta Bianchini, Semini Sumanasuriya, Zafeiris Zafeiriou, Mateus Crespo, Ruth Riisnaes, David Dolling, George Seed, Pasquale Rescigno, Daniel N. Rodrigues, and Gunther Boysen

Abstract

Additional Information on molecular analyses determining CHD1 and SPOP status

Published

2023

12. Supplementary Figure 1 from SPOP-Mutated/CHD1-Deleted Lethal Prostate Cancer and Abiraterone Sensitivity

Author

Johann S. de Bono, Joaquin Mateo, Suzanne Carreira, Christopher E. Barbieri, Wei Yuan, Mark A. Rubin, Theresa MacDonald, Adam Sharp, Jane Goodall, Matthew Clarke, Mark Atkin, Flavia M. de Oliveira, Claudia Bertan, Sara Aziz, Veronica Gil, Rossitza Christova, Ana Ferreira, Inês Figueiredo, Susana Miranda, Nina Tunariu, Raquel Perez-Lopez, Deirdre Moloney, Joanne Hunt, Diletta Bianchini, Semini Sumanasuriya, Zafeiris Zafeiriou, Mateus Crespo, Ruth Riisnaes, David Dolling, George Seed, Pasquale Rescigno, Daniel N. Rodrigues, and Gunther Boysen

Abstract

Sample overview

Published

2023

13. Supplementary Table 1 from SPOP-Mutated/CHD1-Deleted Lethal Prostate Cancer and Abiraterone Sensitivity

Author

Johann S. de Bono, Joaquin Mateo, Suzanne Carreira, Christopher E. Barbieri, Wei Yuan, Mark A. Rubin, Theresa MacDonald, Adam Sharp, Jane Goodall, Matthew Clarke, Mark Atkin, Flavia M. de Oliveira, Claudia Bertan, Sara Aziz, Veronica Gil, Rossitza Christova, Ana Ferreira, Inês Figueiredo, Susana Miranda, Nina Tunariu, Raquel Perez-Lopez, Deirdre Moloney, Joanne Hunt, Diletta Bianchini, Semini Sumanasuriya, Zafeiris Zafeiriou, Mateus Crespo, Ruth Riisnaes, David Dolling, George Seed, Pasquale Rescigno, Daniel N. Rodrigues, and Gunther Boysen

Abstract

SPOP mutation identified in this cohort.

Published

2023

14. Data from SPOP-Mutated/CHD1-Deleted Lethal Prostate Cancer and Abiraterone Sensitivity

Author

Johann S. de Bono, Joaquin Mateo, Suzanne Carreira, Christopher E. Barbieri, Wei Yuan, Mark A. Rubin, Theresa MacDonald, Adam Sharp, Jane Goodall, Matthew Clarke, Mark Atkin, Flavia M. de Oliveira, Claudia Bertan, Sara Aziz, Veronica Gil, Rossitza Christova, Ana Ferreira, Inês Figueiredo, Susana Miranda, Nina Tunariu, Raquel Perez-Lopez, Deirdre Moloney, Joanne Hunt, Diletta Bianchini, Semini Sumanasuriya, Zafeiris Zafeiriou, Mateus Crespo, Ruth Riisnaes, David Dolling, George Seed, Pasquale Rescigno, Daniel N. Rodrigues, and Gunther Boysen

Abstract

Purpose: CHD1 deletions and SPOP mutations frequently cooccur in prostate cancer with lower frequencies reported in castration-resistant prostate cancer (CRPC). We monitored CHD1 expression during disease progression and assessed the molecular and clinical characteristics of CHD1-deleted/SPOP-mutated metastatic CRPC (mCRPC).Experimental Design: We identified 89 patients with mCRPC who had hormone-naive and castration-resistant tumor samples available: These were analyzed for CHD1, PTEN, and ERG expression by IHC. SPOP status was determined by targeted next-generation sequencing (NGS). We studied the correlations between these biomarkers and (i) overall survival from diagnosis; (ii) overall survival from CRPC; (iii) duration of abiraterone treatment; and (iv) response to abiraterone. Relationship with outcome was analyzed using Cox regression and log-rank analyses.Results: CHD1 protein loss was detected in 11 (15%) and 13 (17%) of hormone-sensitive prostate cancer (HSPC) and CRPC biopsies, respectively. Comparison of CHD1 expression was feasible in 56 matched, same patient HSPC and CRPC biopsies. CHD1 protein status in HSPC and CRPC correlated in 55 of 56 cases (98%). We identified 22 patients with somatic SPOP mutations, with six of these mutations not reported previously in prostate cancer. SPOP mutations and/or CHD1 loss was associated with a higher response rate to abiraterone (SPOP: OR, 14.50 P = 0.001; CHD1: OR, 7.30, P = 0.08) and a longer time on abiraterone (SPOP: HR, 0.37, P = 0.002, CHD1: HR, 0.50, P = 0.06).Conclusions: SPOP-mutated mCRPCs are strongly enriched for CHD1 loss. These tumors appear highly sensitive to abiraterone treatment. Clin Cancer Res; 24(22); 5585–93. ©2018 AACR.

Published

2023

15. Data from JMJD6 Is a Druggable Oxygenase That Regulates AR-V7 Expression in Prostate Cancer

Author

Johann S. de Bono, Adam Sharp, Stephen R. Plymate, Christopher J. Schofield, Bissan Al-Lazikani, Andrea Alimonti, Nina Tunariu, Suzanne Carreira, Maryou B. Lambros, Susana Miranda, Mateus Crespo, Lorenzo Buroni, Veronica S. Gil, Rossitza Christova, Bora Gurel, Akane Kawamura, Martine Abboud, Marc A. Moesser, Md. Saiful Islam, Anthony Tumber, Patrizio Di Micco, Takuma Uo, Soojin Kim, Juan M. Jiménez-Vacas, Daniel Nava Rodrigues, Ruth Riisnaes, Ana Ferreira, Rita Pereira, Ines Figueiredo, Wei Yuan, Antje J. Neeb, Jonathan Welti, and Alec Paschalis

Abstract

Endocrine resistance (EnR) in advanced prostate cancer is fatal. EnR can be mediated by androgen receptor (AR) splice variants, with AR splice variant 7 (AR-V7) arguably the most clinically important variant. In this study, we determined proteins key to generating AR-V7, validated our findings using clinical samples, and studied splicing regulatory mechanisms in prostate cancer models. Triangulation studies identified JMJD6 as a key regulator of AR-V7, as evidenced by its upregulation with in vitro EnR, its downregulation alongside AR-V7 by bromodomain inhibition, and its identification as a top hit of a targeted siRNA screen of spliceosome-related genes. JMJD6 protein levels increased (P < 0.001) with castration resistance and were associated with higher AR-V7 levels and shorter survival (P = 0.048). JMJD6 knockdown reduced prostate cancer cell growth, AR-V7 levels, and recruitment of U2AF65 to AR pre-mRNA. Mutagenesis studies suggested that JMJD6 activity is key to the generation of AR-V7, with the catalytic machinery residing within a druggable pocket. Taken together, these data highlight the relationship between JMJD6 and AR-V7 in advanced prostate cancer and support further evaluation of JMJD6 as a therapeutic target in this disease.Significance:This study identifies JMJD6 as being critical for the generation of AR-V7 in prostate cancer, where it may serve as a tractable target for therapeutic intervention.

Published

2023

16. Supplementary Figure 3 from SPOP-Mutated/CHD1-Deleted Lethal Prostate Cancer and Abiraterone Sensitivity

Author

Johann S. de Bono, Joaquin Mateo, Suzanne Carreira, Christopher E. Barbieri, Wei Yuan, Mark A. Rubin, Theresa MacDonald, Adam Sharp, Jane Goodall, Matthew Clarke, Mark Atkin, Flavia M. de Oliveira, Claudia Bertan, Sara Aziz, Veronica Gil, Rossitza Christova, Ana Ferreira, Inês Figueiredo, Susana Miranda, Nina Tunariu, Raquel Perez-Lopez, Deirdre Moloney, Joanne Hunt, Diletta Bianchini, Semini Sumanasuriya, Zafeiris Zafeiriou, Mateus Crespo, Ruth Riisnaes, David Dolling, George Seed, Pasquale Rescigno, Daniel N. Rodrigues, and Gunther Boysen

Abstract

Combined SPOP/ CHD1 status and time/ response to abiraterone.

Published

2023

17. Systematic study of tissue factor expression in solid tumors

Author

Johann S. de Bono, Jeffrey R. Harris, Saskia M. Burm, Adriaan Vanderstichele, Mischa A. Houtkamp, Saida Aarass, Ruth Riisnaes, Ines Figueiredo, Daniel Nava Rodrigues, Rossitza Christova, Siel Olbrecht, Hans W. M. Niessen, Sigrid R. Ruuls, Danita H. Schuurhuis, Jeroen J. Lammerts van Bueren, Esther C. W. Breij, Ignace Vergote, Pathology, and ACS - Heart failure & arrhythmias

Subjects

Cancer Research, Science & Technology, biopsies expression, PROGRESSION, targeted therapy, tissue factor, CANCER, Oncology, immunohistochemistry, SURVIVAL, GROWTH, solid tumor, HEMOSTASIS, Life Sciences & Biomedicine, TF

Abstract

BACKGROUND: Elevated tissue factor (TF) expression, although restricted in normal tissue, has been reported in multiple solid cancers, and expression has been associated with poor prognosis. This manuscript compares TF expression across various solid tumor types via immunohistochemistry in a single study, which has not been performed previously. AIMS: To increase insight in the prevalence and cellular localization of TF expression across solid cancer types, we performed a detailed and systematic analysis of TF expression in tumor tissue obtained from patients with ovarian, esophageal, bladder, cervical, endometrial, pancreatic, prostate, colon, breast, non-small cell lung cancer (NSCLC), head and neck squamous cell carcinoma (HNSCC), and glioblastoma. The spatial and temporal variation of TF expression was analyzed over time and upon disease progression in patient-matched biopsies taken at different timepoints. In addition, TF expression in patient-matched primary tumor and metastatic lesions was also analyzed. METHODS AND RESULTS: TF expression was detected via immunohistochemistry (IHC) using a validated TF-specific antibody. TF was expressed in all cancer types tested, with highest prevalence in pancreatic cancer, cervical cancer, colon cancer, glioblastoma, HNSCC, and NSCLC, and lowest in breast cancer. Staining was predominantly membranous in pancreatic, cervical, and HNSCC, and cytoplasmic in glioblastoma and bladder cancer. In general, expression was consistent between biopsies obtained from the same patient over time, although variability was observed for individual patients. NSCLC biopsies of primary tumor and matched lymph node metastases showed no clear difference in TF expression overall, although individual patient changes were observed. CONCLUSION: This study shows that TF is expressed across a broad range of solid cancer types, and expression is present upon tumor dissemination and over the course of treatment. ispartof: CANCER REPORTS vol:6 issue:2 ispartof: location:United States status: published

Published

2022

18. HER3 is an Actionable Target in Advanced Prostate Cancer

Author

Johann S. de Bono, Pasquale Rescigno, Suzanne Carreira, Gemma Fowler, Penelope Flohr, Christina Guo, Mateus Crespo, Andrea Alimonti, Alessandro Vasciaveo, Jian Ning, Bora Gurel, Beshara Sheehan, Jonathan Welti, Semini Sumanasuriya, Alec Paschalis, Lorenzo Buroni, Abdullah Alajati, Ana Ferreira, Susana Miranda, Claudia Bertan, George Seed, Rita de Cássia Pereira, Paul Workman, Rossitza Christova, Diletta Bianchini, Wei Yuan, Matthew Clarke, Andrea Califano, Gunther Boysen, Antje Neeb, Maryou B K Lambros, Adam Sharp, David Dolling, Nina Tunariu, Michael M. Shen, Daniela Brina, Ines Figueiredo, Amanda Swain, Ruth Riisnaes, Jan Rekowski, Caterina Aversa, Martina Troiani, Mariantonietta D'Ambrosio, and Veronica Gil

Subjects

Male, Cancer Research, Receptor, ErbB-3, Cell, Apoptosis, Mice, SCID, ErbB Receptors, Prostate cancer, Mice, Antineoplastic Agents, Immunological, Mice, Inbred NOD, ErbB-3, Monoclonal, Tumor Cells, Cultured, Tumor Microenvironment, Prospective Studies, skin and connective tissue diseases, Humanized, Tumor, Cultured, medicine.diagnostic_test, biology, Chemistry, Prognosis, Tumor Cells, Organoids, Survival Rate, medicine.anatomical_structure, Immunological, Oncology, Antibody, Receptor, Neuregulin-1, Antineoplastic Agents, Animals, Antibodies, Monoclonal, Humanized, Biomarkers, Tumor, Camptothecin, Cell Proliferation, Follow-Up Studies, Humans, Prostatic Neoplasms, Xenograft Model Antitumor Assays, Immunofluorescence, SCID, Antibodies, Article, ErbB, medicine, Organoid, Tumor microenvironment, medicine.disease, body regions, Cancer research, biology.protein, Inbred NOD, Biomarkers

Abstract

It has been recognized for decades that ERBB signaling is important in prostate cancer, but targeting ERBB receptors as a therapeutic strategy for prostate cancer has been ineffective clinically. However, we show here that membranous HER3 protein is commonly highly expressed in lethal prostate cancer, associating with reduced time to castration resistance (CR) and survival. Multiplex immunofluorescence indicated that the HER3 ligand NRG1 is detectable primarily in tumor-infiltrating myelomonocytic cells in human prostate cancer; this observation was confirmed using single-cell RNA sequencing of human prostate cancer biopsies and murine transgenic prostate cancer models. In castration-resistant prostate cancer (CRPC) patient-derived xenograft organoids with high HER3 expression as well as mouse prostate cancer organoids, recombinant NRG1 enhanced proliferation and survival. Supernatant from murine bone marrow–derived macrophages and myeloid-derived suppressor cells promoted murine prostate cancer organoid growth in vitro, which could be reversed by a neutralizing anti-NRG1 antibody and ERBB inhibition. Targeting HER3, especially with the HER3-directed antibody–drug conjugate U3-1402, exhibited antitumor activity against HER3-expressing prostate cancer. Overall, these data indicate that HER3 is commonly overexpressed in lethal prostate cancer and can be activated by NRG1 secreted by myelomonocytic cells in the tumor microenvironment, supporting HER3-targeted therapeutic strategies for treating HER3-expressing advanced CRPC. Significance: HER3 is an actionable target in prostate cancer, especially with anti-HER3 immunoconjugates, and targeting HER3 warrants clinical evaluation in prospective trials.

Published

2021

19. Elucidating Prostate Cancer Behaviour During Treatment via Low-pass Whole-genome Sequencing of Circulating Tumour DNA

Author

Stephen J. Pettitt, Antje Neeb, Lorna Pope, Jane Goodall, Suzanne Carreira, Joe Baxter, Pasquale Rescigno, Harry Parr, Diletta Bianchini, Claudia Bertan, Stéphane Oudard, Christine Geffriaud-Ricouard, Christopher J. Lord, Sandrine Macé, Oliver Sartor, Ayse Ozatilgan, Rossitza Christova, Gemma Fowler, Maryou B. Lambros, Wei Yuan, Ines Figueiredo, Niven Mehra, Joaquin Mateo, Jan Rekowski, Penelope Flohr, George Seed, Mario A. Eisenberger, Semini Sumanasuriya, Adam Sharp, Mustapha Chadjaa, Johann S. de Bono, Institut Català de la Salut, [Sumanasuriya S] The Institute of Cancer Research, University of London, London, UK. The Royal Marsden Hospital, London, UK. [Seed G, Parr H, Christova R, Pope L, Bertan C] The Institute of Cancer Research, University of London, London, UK. [Mateo J] Vall d’Hebron Institute of Oncology (VHIO), Barcelona, Spain, and Vall d'Hebron Barcelona Hospital Campus

Subjects

Oncology, Male, 030232 urology & nephrology, Docetaxel, Tumour fraction, Other subheadings::Other subheadings::/drug therapy [Other subheadings], Circulating Tumor DNA, Prostate cancer, chemistry.chemical_compound, Cell-free DNA, 0302 clinical medicine, Prospective Studies, cfDNA, Elements genètics mòbils, Cabazitaxel, Otros calificadores::Otros calificadores::/genética [Otros calificadores], Prostate Cancer, Hazard ratio, DNA, Neoplasm, mCRPC, Prostatic Neoplasms, Castration-Resistant, Cell-free fetal DNA, Pharmaceutical Preparations, 030220 oncology & carcinogenesis, Urological cancers Radboud Institute for Health Sciences [Radboudumc 15], Pròstata - Càncer - Aspectes genètics, medicine.drug, medicine.medical_specialty, lpWGS, Urology, Otros calificadores::Otros calificadores::/farmacoterapia [Otros calificadores], Context (language use), nucleótidos y nucleósidos de ácidos nucleicos::ácidos nucleicos::ácidos nucleicos libres de células::ADN tumoral circulante [COMPUESTOS QUÍMICOS Y DROGAS], 03 medical and health sciences, Taxanes, Internal medicine, medicine, Other subheadings::Other subheadings::/genetics [Other subheadings], Enzalutamide, Humans, Taxane, Nucleic Acids, Nucleotides, and Nucleosides::Nucleic Acids::Cell-Free Nucleic Acids::Circulating Tumor DNA [CHEMICALS AND DRUGS], business.industry, ctDNA, medicine.disease, Pròstata - Càncer - Tractament, Neoplasms::Neoplasms by Site::Urogenital Neoplasms::Genital Neoplasms, Male::Prostatic Neoplasms::Prostatic Neoplasms, Castration-Resistant [DISEASES], Metastatic castration-resistant prostate cancer, chemistry, neoplasias::neoplasias por localización::neoplasias urogenitales::neoplasias de los genitales masculinos::neoplasias de la próstata::neoplasias prostáticas resistentes a la castración [ENFERMEDADES], Low-pass whole-genome sequencing, business

Abstract

Background Better blood tests to elucidate the behaviour of metastatic castration-resistant prostate cancer (mCRPC) are urgently needed to drive therapeutic decisions. Plasma cell-free DNA (cfDNA) comprises normal and circulating tumour DNA (ctDNA). Low-pass whole-genome sequencing (lpWGS) of ctDNA can provide information on mCRPC behaviour. Objective To validate and clinically qualify plasma lpWGS for mCRPC. Design, setting, and participants Plasma lpWGS data were obtained for mCRPC patients consenting to optional substudies of two prospective phase 3 trials (FIRSTANA and PROSELICA). In FIRSTANA, chemotherapy-naïve patients were randomised to treatment with docetaxel (75 mg/m2) or cabazitaxel (20 or 25 mg/m2). In PROSELICA, patients previously treated with docetaxel were randomised to 20 or 25 mg/m2 cabazitaxel. lpWGS data were generated from 540 samples from 188 mCRPC patients acquired at four different time points (screening, cycle 1, cycle 4, and end of study). Outcome measurements and statistical analysis lpWGS data for ctDNA were evaluated for prognostic, response, and tumour genomic measures. Associations with response and survival data were determined for tumour fraction. Genomic biomarkers including large-scale transition (LST) scores were explored in the context of prior treatments. Results and limitations Plasma tumour fraction was prognostic for overall survival in univariable and stratified multivariable analyses (hazard ratio 1.75, 95% confidence interval 1.08–2.85; p = 0.024) and offered added value compared to existing biomarkers (C index 0.722 vs 0.709; p = 0.021). Longitudinal changes were associated with drug response. PROSELICA samples were enriched for LSTs (p = 0.029) indicating genomic instability, and this enrichment was associated with prior abiraterone and enzalutamide treatment but not taxane or radiation therapy. Higher LSTs were correlated with losses of RB1/RNASEH2B, independent of BRCA2 loss. Conclusions Plasma lpWGS of ctDNA describes CRPC behaviour, providing prognostic and response data of clinical relevance. The added prognostic value of the ctDNA fraction over established biomarkers should be studied further. Patient summary We studied tumour DNA in blood samples from patients with prostate cancer. We found that levels of tumour DNA in blood were indicative of disease prognosis, and that changes after treatment could be detected. We also observed a “genetic scar” in the results that was associated with certain previous treatments. This test allows an assessment of tumour activity that can complement existing tests, offer insights into drug response, and detect clinically relevant genetic changes., Take Home Message Tumour fraction, independent from cell-free DNA concentration and other clinical variables, is prognostic, with low-pass whole-genome sequencing profiles detecting abiraterone/enzalutamide-induced emerging genomic instability that is likely to be acquired as a result of tumour development.

Published

2021

20. JMJD6 Is a Druggable Oxygenase That Regulates AR-V7 Expression in Prostate Cancer

Author

Takuma Uo, Maryou B. Lambros, Suzanne Carreira, Ruth Riisnaes, Veronica Gil, Juan M. Jiménez-Vacas, Ana Ferreira, Susana Miranda, Andrea Alimonti, Jonathan Welti, Lorenzo Buroni, Mateus Crespo, Anthony Tumber, Daniel Nava Rodrigues, Marc A. Moesser, Alec Paschalis, Antje Neeb, Martine I. Abboud, Nina Tunariu, Patrizio Di Micco, Md. Saiful Islam, Akane Kawamura, Rossitza Christova, Wei Yuan, Bissan Al-Lazikani, Ines Figueiredo, Rita Pereira, Christopher J. Schofield, Stephen R. Plymate, Johann S. de Bono, Bora Gurel, Adam Sharp, and Soojin Kim

Subjects

0301 basic medicine, Male, Cancer Research, Jumonji Domain-Containing Histone Demethylases, Druggability, Antineoplastic Agents, Article, Cohort Studies, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Castration Resistance, Downregulation and upregulation, Cell Line, Tumor, Medicine, Humans, Protein Isoforms, Molecular Targeted Therapy, Enzyme Inhibitors, Retrospective Studies, Gene knockdown, business.industry, Alternative splicing, medicine.disease, Prognosis, 3. Good health, Bromodomain, Androgen receptor, Gene Expression Regulation, Neoplastic, Alternative Splicing, Prostatic Neoplasms, Castration-Resistant, 030104 developmental biology, Oncology, Receptors, Androgen, 030220 oncology & carcinogenesis, Cancer research, Oxygenases, business

Abstract

Endocrine resistance (EnR) in advanced prostate cancer is fatal. EnR can be mediated by androgen receptor (AR) splice variants, with AR splice variant 7 (AR-V7) arguably the most clinically important variant. In this study, we determined proteins key to generating AR-V7, validated our findings using clinical samples, and studied splicing regulatory mechanisms in prostate cancer models. Triangulation studies identified JMJD6 as a key regulator of AR-V7, as evidenced by its upregulation with in vitro EnR, its downregulation alongside AR-V7 by bromodomain inhibition, and its identification as a top hit of a targeted siRNA screen of spliceosome-related genes. JMJD6 protein levels increased (P < 0.001) with castration resistance and were associated with higher AR-V7 levels and shorter survival (P = 0.048). JMJD6 knockdown reduced prostate cancer cell growth, AR-V7 levels, and recruitment of U2AF65 to AR pre-mRNA. Mutagenesis studies suggested that JMJD6 activity is key to the generation of AR-V7, with the catalytic machinery residing within a druggable pocket. Taken together, these data highlight the relationship between JMJD6 and AR-V7 in advanced prostate cancer and support further evaluation of JMJD6 as a therapeutic target in this disease. Significance: This study identifies JMJD6 as being critical for the generation of AR-V7 in prostate cancer, where it may serve as a tractable target for therapeutic intervention.

Published

2021

21. Abstract LB-270: Discovery of genomic correlates and tumor purity as an independent clinical factor of poor outcome in advanced prostate cancer lpWGS CNA data

Author

Gemma Fowler, Maryou B. Lambros, Pasquale Rescigno, Sandrine Macé, Rossitza Christova, Penelope Flohr, Wei Yuan, Claudia Bertan, Jane Goodall, Lorna Pope, George Seed, Suzanne Carreira, Johann S. de Bono, Semini Sumanasuriya, Harry Parr, and Mustapha Chadjaa

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Taxane, business.industry, Cancer, medicine.disease, Clinical trial, 03 medical and health sciences, chemistry.chemical_compound, Prostate cancer, 030104 developmental biology, 0302 clinical medicine, chemistry, 030220 oncology & carcinogenesis, Internal medicine, Cohort, medicine, Enzalutamide, business, Mace, Survival analysis

Abstract

Background: We, and others, have shown that responses to therapies in metastatic castration-resistant prostate cancer (mCRPC) can be monitored using plasma cell-free DNA (cfDNA), and that this can be both quantitative and qualitative. In this study, we explored the utility of low pass whole genome sequencing (lpWGS) of cfDNA in mCRPC patients treated on two large prospectively collected Phase III trials of taxane chemotherapy, FIRSTANA (NCT01308567) and PROSELICA (NCT01308580). Methods: Plasma samples collated from the FIRSTANA and PROSELICA trials were evaluated. cfDNA was isolated and analysed with lpWGS using the Illumina NovaSeq 6000. Reads were aligned using BWA-MEM and quality controlled using Picard and FASTQC. Whole-genome copy number aberration (CNA) profiles were generated using ichorCNA, which also estimated tumor purity and ploidy. Log-rank tests were used for univariable survival comparisons, and Cox proportional hazard models were used for multivariable survival analysis. Results: Overall, lp-WGS data was generated from 528 samples acquired at three different timepoints (Baseline [SCR and C1], C4 and EOS), representing 188 unique patients. We observed CNA profiles in line with emergent mCRPC subtypes including highly aberrant, large-scale events which have been linked to homologous-repair deficient tumors. We found that CNAs in this cohort matched other published studies with frequent amplifications of AR (~30%), copy-gains of PI3KCA (~45%) and copy-loss of NKX3-1 (~75%), RB1 (~70%) and PTEN (~50%). We did not observe changes in baseline tumor purity or ploidy between the FIRSTANA and PROSELICA cohorts. Following calculation of a large-scale transition (LST) score (measuring CNA breakpoints), we observed that this was significantly elevated (Wilcox test, p=0.0073) in cases that had prior exposure to second line androgen deprivation (abiraterone or enzalutamide). Baseline tumor purity values were associated with several mCRPC clinical variables including ECOG performance status. High lpWGS tumor purity values were univariably associated with poorer overall survival in both FIRSTANA and PROSELICA cohorts (log-rank test p=0.0021 and 0.0009), and were also associated with significantly poorer RPFS and PSAPFS. Tumor purity was also associated (HR 1.66, p=0.036) with survival when assessed using multivariable models alongside other mCRPC clinical variables, including cell-free DNA concentration. Further, longitudinal changes in tumor purity on treatment can be illustrative of drug responses. Conclusions: In our analysis of this prospectively collected clinical trial data, we show mCRPC CNA profiles in cfDNA, and that these CNAs may be induced by prior aggressive treatments. We also found that tumor purity estimation can serve as a robust, competitive indicator of both overall survival and, assessed longitudinally, shows clear association with drug response. We envision that these techniques will enable improved strategies for monitoring mCRPC patients. Citation Format: George Seed, Semini Sumanasuriya, Claudia Bertan, Harry Parr, Gemma Fowler, Rossitza Christova, Lorna Pope, Jane Goodall, Maryou Lambros, Pasquale Rescigno, Penelope Flohr, Suzanne Carreira, Wei Yuan, Mustapha Chadjaa, Sandrine Mace, Johann De Bono. Discovery of genomic correlates and tumor purity as an independent clinical factor of poor outcome in advanced prostate cancer lpWGS CNA data [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr LB-270.

Published

2020

22. SPOP-Mutated/CHD1-Deleted Lethal Prostate Cancer and Abiraterone Sensitivity

Author

Gunther Boysen, Theresa Y. MacDonald, Pasquale Rescigno, Christopher E. Barbieri, Ruth Riisnaes, David Dolling, Joanne Hunt, Joaquin Mateo, Flavia M. de Oliveira, Jane Goodall, Suzanne Carreira, Sara Aziz, Johann S. de Bono, Deirdre Moloney, Zafeiris Zafeiriou, Veronica Gil, Ana Ferreira, Claudia Bertan, Ines Figueiredo, Daniel Nava Rodrigues, Adam Sharp, Mark A. Rubin, Susana Miranda, Mateus Crespo, Mark Atkin, Rossitza Christova, George Seed, Raquel Perez-Lopez, Diletta Bianchini, Nina Tunariu, Wei Yuan, Matthew Clarke, and Semini Sumanasuriya

Subjects

0301 basic medicine, Oncology, Male, Cancer Research, medicine.medical_specialty, Gene Expression, SPOP, Article, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Internal medicine, Cell Line, Tumor, medicine, PTEN, Humans, RNA, Small Interfering, 610 Medicine & health, Aged, Neoplasm Staging, biology, Proportional hazards model, business.industry, DNA Helicases, Cancer, Nuclear Proteins, Prostatic Neoplasms, Middle Aged, medicine.disease, DNA-Binding Proteins, Repressor Proteins, 030104 developmental biology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Mutation, biology.protein, Disease Progression, Immunohistochemistry, Cancer biomarkers, Androstenes, Neoplasm Grading, business, Synthetic Lethal Mutations, Gene Deletion

Abstract

Purpose: CHD1 deletions and SPOP mutations frequently cooccur in prostate cancer with lower frequencies reported in castration-resistant prostate cancer (CRPC). We monitored CHD1 expression during disease progression and assessed the molecular and clinical characteristics of CHD1-deleted/SPOP-mutated metastatic CRPC (mCRPC). Experimental Design: We identified 89 patients with mCRPC who had hormone-naive and castration-resistant tumor samples available: These were analyzed for CHD1, PTEN, and ERG expression by IHC. SPOP status was determined by targeted next-generation sequencing (NGS). We studied the correlations between these biomarkers and (i) overall survival from diagnosis; (ii) overall survival from CRPC; (iii) duration of abiraterone treatment; and (iv) response to abiraterone. Relationship with outcome was analyzed using Cox regression and log-rank analyses. Results: CHD1 protein loss was detected in 11 (15%) and 13 (17%) of hormone-sensitive prostate cancer (HSPC) and CRPC biopsies, respectively. Comparison of CHD1 expression was feasible in 56 matched, same patient HSPC and CRPC biopsies. CHD1 protein status in HSPC and CRPC correlated in 55 of 56 cases (98%). We identified 22 patients with somatic SPOP mutations, with six of these mutations not reported previously in prostate cancer. SPOP mutations and/or CHD1 loss was associated with a higher response rate to abiraterone (SPOP: OR, 14.50 P = 0.001; CHD1: OR, 7.30, P = 0.08) and a longer time on abiraterone (SPOP: HR, 0.37, P = 0.002, CHD1: HR, 0.50, P = 0.06). Conclusions: SPOP-mutated mCRPCs are strongly enriched for CHD1 loss. These tumors appear highly sensitive to abiraterone treatment. Clin Cancer Res; 24(22); 5585–93. ©2018 AACR.

Published

2018

23. CHD1 loss sensitizes prostate cancer to DNA damaging therapy by promoting error-prone double-strand break repair

Author

Miguel Ramalho-Santos, Rossitza Christova, Mateus Crespo, Hong Wu, Penny Flohr, T.R. Shenoy, F.M. Koh, J.S. de Bono, Zafeiris Zafeiriou, Amanda Swain, M.Y. Wang, Ruth Riisnaes, Weilong Guo, D.Y. Xu, Pasquale Rescigno, Gunther Boysen, Wei Yuan, Q.Z. Xu, C. Wang, Daniel Nava Rodrigues, Y. Wang, L.Z. Zhang, Sarah Aziz, Nina Tunariu, Eleanor Knight, and Veronica Gil

Subjects

0301 basic medicine, Genome instability, Male, DNA End-Joining Repair, Time Factors, DNA damage, Down-Regulation, SPOP, Biology, Poly(ADP-ribose) Polymerase Inhibitors, medicine.disease_cause, Radiation Tolerance, Cdh1 Proteins, 03 medical and health sciences, Cell Line, Tumor, medicine, Tumor Cells, Cultured, Animals, Humans, DNA Breaks, Double-Stranded, Genetic Predisposition to Disease, Mice, Knockout, Mutation, Dose-Response Relationship, Drug, Protein Stability, Prostatic Neoplasms, Recombinational DNA Repair, Hematology, Double Strand Break Repair, Non-homologous end joining, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Cross-Linking Reagents, Phenotype, Oncology, Cancer research, Homologous recombination, Tumor Suppressor p53-Binding Protein 1, Gene Deletion

Abstract

Background Deletion of the chromatin remodeler chromodomain helicase DNA-binding protein 1 (CHD1) is a common genomic alteration found in human prostate cancers (PCas). CHD1 loss represents a distinct PCa subtype characterized by SPOP mutation and higher genomic instability. However, the role of CHD1 in PCa development in vivo and its clinical utility remain unclear. Patients and methods To study the role of CHD1 in PCa development and its loss in clinical management, we generated a genetically engineered mouse model with prostate-specific deletion of murine Chd1 as well as isogenic CHD1 wild-type and homozygous deleted human benign and PCa lines. We also developed patient-derived organoid cultures and screened patients with metastatic PCa for CHD1 loss. Results We demonstrate that CHD1 loss sensitizes cells to DNA damage and causes a synthetic lethal response to DNA damaging therapy in vitro, in vivo, ex vivo, in patient-derived organoid cultures and in a patient with metastatic PCa. Mechanistically, CHD1 regulates 53BP1 stability and CHD1 loss leads to decreased error-free homologous recombination (HR) repair, which is compensated by increased error-prone non-homologous end joining (NHEJ) repair for DNA double-strand break (DSB) repair. Conclusions Our study provides the first in vivo and in patient evidence supporting the role of CHD1 in DSB repair and in response to DNA damaging therapy. We uncover mechanistic insights that CHD1 modulates the choice between HR and NHEJ DSB repair and suggest that CHD1 loss may contribute to the genomic instability seen in this subset of PCas.

Published

2017

24. Cell-free DNA as a biomarker for taxane treatment in advanced prostate cancer

Author

Jane Goodall, Diletta Bianchini, Semini Sumanasuriya, Rossitza Christova, Wei Yuan, Johann S. de Bono, Niven Mehra, Lorna Pope, Penelope Flohr, Pasquale Rescigno, George Seed, Suzanne Carreira, Mustapha Chadjaa, Sandrine Macé, and Gemma Fowler

Subjects

Cancer Research, Taxane, business.industry, medicine.disease, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Oncology, Docetaxel, Cell-free fetal DNA, Cabazitaxel, 030220 oncology & carcinogenesis, medicine, Cancer research, Biomarker (medicine), Chemotherapeutic drugs, business, 030215 immunology, medicine.drug

Abstract

5070 Background: Antitumor efficacy of chemotherapeutic drugs docetaxel and cabazitaxel against hormone-sensitive and castration-resistant prostate cancer (CRPC) is well recognized. The identification and validation of minimally invasive biomarkers of taxane response remain of paramount importance. Methods: Serial pre-, during and post-treatment plasma samples were collected prospectively from two large Phase III clinical trials, FIRSTANA (NCT01308567) and PROSELICA (NCT01308580). Chemotherapy-naïve patients (pts) were treated with docetaxel (75 mg/m2) or cabazitaxel (20 or 25 mg/m2) in FIRSTANA, and pts previously treated with docetaxel received cabazitaxel (20 or 25 mg/m2) as second-line chemotherapy in PROSELICA. Plasma cell-free DNA (cfDNA) was extracted, low-pass whole genome sequencing (lp-WGS) libraries were prepared using the QIAGEN QiaSeq FX DNA library kit, and samples sequenced on the Illumina NovaSeq 6000. Targeted next-generation sequencing (NGS) on a custom-made AmpliSeq panel of 30 genes, pre-selected for putative roles in taxane resistance, was also performed. lp-WGS copy number (CN) profiles were generated using ichorCNA (v0.1.0) and targeted NGS variant calls derived using IonReporter software. Results: Overall, lp-WGS data was generated from 265 samples (99 pts; 51 treated on the FIRSTANA study, 48 treated on the PROSELICA study), acquired at three time-points (pre-, during and at progression). Average cfDNA input was 10 ng and mean coverage achieved was ~2X (SD 1.2X). We observed changes in lp-WGS tumor purity over time as a result of therapy; samples from non-responding pts exhibited significantly higher tumor purity values post-treatment compared with samples from responding pts (p = 0.02). Targeted NGS results were available from 294 pts (153 from FIRSTANA, 141 from PROSELICA), and changes in tumor purity were also associated with treatment response (p = 0.04). CN frequency of key CRPC genes was similar to previously reported datasets; several aberrant loci associated with response to taxane therapy. Conclusions: cfDNA lp-WGS may have clinical utility in the management of lethal prostate cancer. Funding: Sanofi. Clinical trial information: NCT01308580, NCT01308567.

Published

2019

25. CTCF binds to sites in the major histocompatibility complex that are rapidly reconfigured in response to interferon-gamma

Author

Babatunji W Ogunkolade, Shihong Mao, Christopher A. Pieri, Johan Aarum, Jaroslaw Szary, Stephen A. Krawetz, Tania A. Jones, Diego Ottaviani, Muhammad A. Mumin, Elliott Lever, Denise Sheer, and Rossitza Christova

Subjects

Genetics, CCCTC-Binding Factor, Binding Sites, CD74, biology, chemical and pharmacologic phenomena, Gene Regulation, Chromatin and Epigenetics, Matrix Attachment Regions, Major histocompatibility complex, Acquired immune system, Chromatin, MHC Class II Gene, Major Histocompatibility Complex, Repressor Proteins, Interferon-gamma, CTCF, MHC class I, biology.protein, CIITA, Humans, Cells, Cultured, Transcription Factors

Abstract

Activation of the major histocompatibility complex (MHC) by interferon-gamma (IFN-γ) is a fundamental step in the adaptive immune response to pathogens. Here, we show that reorganization of chromatin loop domains in the MHC is evident within the first 30 min of IFN-γ treatment of fibroblasts, and that further dynamic alterations occur up to 6 h. These very rapid changes occur at genomic sites which are occupied by CTCF and are close to IFN-γ-inducible MHC genes. Early responses to IFN-γ are thus initiated independently of CIITA, the master regulator of MHC class II genes and prepare the MHC for subsequent induction of transcription.

Published

2012

26. Targeting the SIN3A-PF1 interaction inhibits epithelial to mesenchymal transition and maintenance of a stem cell phenotype in triple negative breast cancer

Author

Boris A. Leibovitch, Yordan Sbirkov, Emily Bernstein, Eun Jee Lee, Edgardo V. Ariztia, Ming-Ming Zhou, Joanna Wexler, Louise Howell, Nidhi Bansal, Arthur Zelent, Rajal Sharma, Eduardo F. Farias, Kevin Petrie, Jun Zhu, Chi-Yeh Chung, Rossitza Christova, Samuel Waxman, and Veronica Gil

Subjects

Oncology, cancer stem cells, medicine.medical_specialty, Epithelial-Mesenchymal Transition, Triple Negative Breast Neoplasms, Biology, 03 medical and health sciences, Mice, 0302 clinical medicine, Cancer stem cell, Internal medicine, Spheroids, Cellular, medicine, Tumor Cells, Cultured, Animals, Humans, Epithelial–mesenchymal transition, Epigenetics, Triple-negative breast cancer, 030304 developmental biology, Adaptor Proteins, Signal Transducing, sub_healthsciences, Homeodomain Proteins, 0303 health sciences, epigenetics, Cancer, medicine.disease, Primary tumor, 3. Good health, Protein Structure, Tertiary, Repressor Proteins, Sin3 Histone Deacetylase and Corepressor Complex, 030220 oncology & carcinogenesis, triple negative breast cancer, Immunology, PF1, Neoplastic Stem Cells, Female, Stem cell, SIN3, sub_biomedicalsciences, Priority Research Paper, Transcription Factors

Abstract

// Nidhi Bansal 1 , Kevin Petrie 2 , Rossitza Christova 2,* , Chi-Yeh Chung 3,* , Boris A. Leibovitch 1 , Louise Howell 2 , Veronica Gil 2 , Yordan Sbirkov 2 , EunJee Lee 4 , Joanna Wexler 1 , Edgardo V. Ariztia 1 , Rajal Sharma 1 , Jun Zhu 4 , Emily Bernstein 5 , Ming-Ming Zhou 1 , Arthur Zelent 6 , Eduardo Farias 1 and Samuel Waxman 1 1 Division of Hematology and Oncology, The Tisch Cancer Institute, Icahn School of Medicine at Mount Sinai, New York, USA 2 Division of Clinical Studies, Institute of Cancer Research, Sutton, United Kingdom 3 Department of Oncological Sciences, Department of Genetics and Genomic Sciences, Graduate School of Biomedical Sciences, Icahn School of Medicine at Mount Sinai, New York, USA 4 Genetics and Genomic Science, Icahn School of Medicine at Mount Sinai, New York, USA 5 Department of Oncological Sciences, Graduate School of Biomedical Sciences, Icahn School of Medicine at Mount Sinai, New York, USA 6 Division of Hemato-Oncology, Department of Medicine, Sylvester Comprehensive Cancer Center, Miller School of Medicine, University of Miami, Florida, USA * These authors have contributed equally to this work Correspondence to: Samuel Waxman, email: // Keywords : epigenetics, SIN3, PF1, triple negative breast cancer, cancer stem cells Received : July 17, 2015 Accepted : September 24, 2015 Published : October 09, 2015 Abstract Triple negative breast cancer (TNBC) is characterized by a poorly differentiated phenotype and limited treatment options. Aberrant epigenetics in this subtype represent a potential therapeutic opportunity, but a better understanding of the mechanisms contributing to the TNBC pathogenesis is required. The SIN3 molecular scaffold performs a critical role in multiple cellular processes, including epigenetic regulation, and has been identified as a potential therapeutic target. Using a competitive peptide corresponding to the SIN3 interaction domain of MAD (Tat-SID), we investigated the functional consequences of selectively blocking the paired amphipathic α-helix (PAH2) domain of SIN3. Here, we report the identification of the SID-containing adaptor PF1 as a factor required for maintenance of the TNBC stem cell phenotype and epithelial-to-mesenchymal transition (EMT). Tat-SID peptide blocked the interaction between SIN3A and PF1, leading to epigenetic modulation and transcriptional downregulation of TNBC stem cell and EMT markers. Importantly, Tat-SID treatment also led to a reduction in primary tumor growth and disseminated metastatic disease in vivo . In support of these findings, knockdown of PF1 expression phenocopied treatment with Tat-SID both in vitro and in vivo . These results demonstrate a critical role for a complex containing SIN3A and PF1 in TNBC and provide a rational for its therapeutic targeting.

Published

2015

27. Selective Inhibition of SIN3 Corepressor with Avermectins as a Novel Therapeutic Strategy in Triple-Negative Breast Cancer

Author

Boris A. Leibovitch, Rajal Sharma, Shuai Yang, Mihaly Mezei, Alan Ashworth, Eduardo F. Farias, Lei Zeng, Edgardo V. Ariztia, Louise Howell, Rossitza Christova, Nidhi Bansal, Ming-Ming Zhou, Rachel Brough, Kevin Petrie, Yordan Sbirkov, Veronica Gil, Yeon-Jin Kwon, Samuel Waxman, Christopher J. Lord, Arthur Zelent, and Jessica Frankum

Subjects

Models, Molecular, Cancer Research, Drug Resistance, Molecular Conformation, Triple Negative Breast Neoplasms, Pharmacology, chemistry.chemical_compound, Mice, Models, 2.1 Biological and endogenous factors, Aetiology, Triple-negative breast cancer, Avermectin, Cancer, Tumor, Antiparasitic Agents, Pharmacology and Pharmaceutical Sciences, Cadherins, CD, Tumor Burden, Gene Expression Regulation, Neoplastic, Oncology, 5.1 Pharmaceuticals, Stem Cell Research - Nonembryonic - Non-Human, Female, Development of treatments and therapeutic interventions, Biotechnology, medicine.drug, Oncology and Carcinogenesis, Biology, Article, Cell Line, Cancer stem cell, Antigens, CD, Cell Line, Tumor, Breast Cancer, parasitic diseases, Genetics, medicine, Animals, Humans, Protein Interaction Domains and Motifs, Oncology & Carcinogenesis, Epigenetics, Antigens, Clonogenic assay, Cell Proliferation, Neoplastic, Ivermectin, Animal, Estrogen Receptor alpha, Molecular, Stem Cell Research, Xenograft Model Antitumor Assays, Repressor Proteins, Disease Models, Animal, Gene Expression Regulation, chemistry, Drug Resistance, Neoplasm, Disease Models, Neoplasm, Corepressor, Estrogen receptor alpha, Tamoxifen

Abstract

Triple-negative breast cancers (TNBC) lacking estrogen, progesterone, and HER2 receptors account for 10% to 20% of breast cancer and are indicative of poor prognosis. The development of effective treatment strategies therefore represents a pressing unmet clinical need. We previously identified a molecularly targeted approach to target aberrant epigenetics of TNBC using a peptide corresponding to the SIN3 interaction domain (SID) of MAD. SID peptide selectively blocked binding of SID-containing proteins to the paired α-helix (PAH2) domain of SIN3, resulting in epigenetic and transcriptional modulation of genes associated with epithelial–mesenchymal transition (EMT). To find small molecule inhibitor (SMI) mimetics of SID peptide, we performed an in silico screen for PAH2 domain–binding compounds. This led to the identification of the avermectin macrocyclic lactone derivatives selamectin and ivermectin (Mectizan) as candidate compounds. Both selamectin and ivermectin phenocopied the effects of SID peptide to block SIN3–PAH2 interaction with MAD, induce expression of CDH1 and ESR1, and restore tamoxifen sensitivity in MDA-MB-231 human and MMTV-Myc mouse TNBC cells in vitro. Treatment with selamectin or ivermectin led to transcriptional modulation of genes associated with EMT and maintenance of a cancer stem cell phenotype in TNBC cells. This resulted in impairment of clonogenic self-renewal in vitro and inhibition of tumor growth and metastasis in vivo. Underlining the potential of avermectins in TNBC, pathway analysis revealed that selamectin also modulated the expression of therapeutically targetable genes. Consistent with this, an unbiased drug screen in TNBC cells identified selamectin-induced sensitization to a number of drugs, including those targeting modulated genes. Mol Cancer Ther; 14(8); 1824–36. ©2015 AACR.

Published

2014

28. Detecting DNA–Protein Interactions in Living Cells—ChIP Approach

Author

Rossitza Christova

Subjects

Genetics, Immunoprecipitation, Epigenetics, Computational biology, ChIP-on-chip, Biology, Chromatin immunoprecipitation, Gene, ChIA-PET, Chromatin, ChIP-sequencing

Abstract

DNA-binding proteins play a critical role in many major cellular processes. The immunoprecipitation of protein complexes with associated DNA fragments, termed chromatin immunoprecipitation or ChIP, allows for the analysis of the binding of protein factors in their natural environment. It evolved from a confirmation assay to a discovery tool that really changed our understanding of the biology of living cells. With the widespread use of next-generation high-throughput sequencing technologies, factor binding can not only be assessed in an unbiased and genome-wide manner but can also be predicted and linked to gene expression and chromatin structure. This review summarizes the current advances of the ChIP-based approaches to decipher gene regulatory and epigenetic network in the cells. The limitations of the method are discussed and the future ChIP-based developments are explored.

Published

2013

29. Abstract 4976: Monitoring CHD1 during prostate cancer progression

Author

Juan M. Mosquera, Daniel Nava Rodrigues, Adam Sharp, Mark A. Rubin, Sara Aziz, Niven Mehra, Joaquin Mateo, Theresa Y. MacDonald, Veronica Gil, Christopher E. Barbieri, Ruth Riisnaes, Rossitza Christova, Mateus Crespo, Susana Miranda, Gunther Boysen, Ines Figueiredo, Pasquale Rescigno, and Johann S. de Bono

Subjects

Oncology, Cancer Research, medicine.medical_specialty, biology, medicine.diagnostic_test, business.industry, Cancer, medicine.disease, Androgen receptor, Prostate cancer, medicine.anatomical_structure, Docetaxel, Prostate, Internal medicine, biology.protein, Medicine, PTEN, Immunohistochemistry, business, medicine.drug, Fluorescence in situ hybridization

Abstract

Adenocarcinomas of the prostate consist of a collection of malignancies with distinct molecular underpinnings. Linking molecular background to clinical behaviour, i.e. tumour progression and response to therapy has not yet been fully established. This is in large measure due to a paucity of well-annotated patient cohorts, which cover the evolution from localized, hormone naïve to metastatic castration resistant prostate cancer. Deletions in the gene Chromodomain Helicase DNA Binding Protein 1 (CHD1) are among the most frequent genomic alterations in prostate cancer. CHD1 is a ATPase-dependent helicase mediating a variety of biological processes by modifying chromatin structure. In hormone sensitive prostate cancer, loss of CHD1 has been associated with increased genomic instability and aggressiveness. Here we monitor CHD1 status during the progression from hormone sensitive (HSPC) to castration resistant prostate cancer (CRPC). To molecularly stratify this patient subgroup we correlate CHD1 status with markers of prostate cancer including AR, ERG, PTEN and Ki67. Finally, we analyze the impact of alterations in CHD1 on outcome and response to therapy of CRPC patients. We retrospectively identified 52 patients of whom HSPC and CRPC tissue was available for immunohistochemical analysis of CHD1, ERG, PTEN, AR and Ki67 as well as for CHD1 fluorescence in situ hybridization. Relationship with outcome was analyzed using univariate Cox regression and log-rank analyses. By using Fluorescence In Situ Hybridization (FISH) and immunohistochemistry (IHC) in a cohort of 52 men who developed CRPC, we show that the frequency of loss of CHD1 does not change during disease progression (7.7% in HSPC vs 9.6% in CRPC). Homozygously deleted tumors demonstrate a tendency towards poorer prognosis but this observation lacks statistical power in our cohort. Interestingly, in patients that show CHD1 protein expression in their hormone naïve sample, a decrease of expression in the matched CRPC sample correlates with poorer overall survival (OS) (p = 0.03). Although preclinical data suggest a role for CHD1 in androgen receptor (AR) activity, CHD1 expression did not correlate with AR protein level. Additionally, Ki67 expression did not show correlation with CHD1 levels of expression. Further molecular stratification confirms a known mutual exclusive relationship with the expression of the ERG transcription factor (p = 0.048). Clinically, although decreased CHD1 protein expression during disease progression correlated with worse outcome (overall survival (p = 0.03) and survival from diagnosis of CRPC (p = 0.02)), no significant impact on survival after docetaxel or abiraterone treatment was measured.Here we monitor CHD1 deletion during prostate cancer progression. Our results show that this genomic marker defines a distinct molecular subgroup of prostate cancer. In addition, loss of CHD1 protein expression during disease progression is associated with poorer clinical outcome. Citation Format: Gunther Boysen, Daniel Nava Rodrigues, Joaquin Mateo, Rossitza Christova, Ruth Riisnaes, Mateus Crespo, Theresa MacDonald, Susana Miranda, Ines Figueiredo, Veronica Gil, Sara Aziz, Adam Sharp, Niven Mehra, Pasquale Rescigno, Juan M. Mosquera, Christopher E. Barbieri, Mark A. Rubin, Johann S. de Bono. Monitoring CHD1 during prostate cancer progression. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 4976.

Published

2016

30. Association of plasma cell-free DNA concentration [cfDNA] with outcome from taxane therapy (TT) for castration resistant prostate cancer (CRPC)

Author

Stéphane Oudard, David Lorente, Gunther Boysen, Rossitza Christova, Mustapha Chadjaa, Niven Mehra, Lorna Pope, Sandrine Macé, Karim Fizazi, Oliver Sartor, Jane Goodall, Nuria Porta, Emma Hall, Johann S. de Bono, Penelope Flohr, Suzanne Carreira, Mario A. Eisenberger, and Diletta Bianchini

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Taxane, business.industry, 030232 urology & nephrology, Plasma cell, Castration resistant, urologic and male genital diseases, medicine.disease, Free dna, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Internal medicine, Medicine, business

Abstract

5014Background: Biomarkers are needed to guide CRPC treatment; we evaluated [cfDNA] pre- and post-TT, associating this with outcome. Methods: cfDNA was isolated and quantified from 1 mL of plasma, ...

Published

2016

31. Reconfiguration of genomic anchors upon transcriptional activation of the human major histocompatibility complex

Author

Badmavady Segarane, Stephan Beck, Tim Forshew, Eleni M. Tomazou, Stephen A. Krawetz, Richard Mitter, Tania A. Jones, Rossitza Christova, Adrian E. Platts, Elliott Lever, Vardhman K. Rakyan, Diego Ottaviani, and Denise Sheer

Subjects

Transcriptional Activation, Letter, Genes, MHC Class II, Human leukocyte antigen, Computational biology, Biology, Major histocompatibility complex, Genome, Cell Line, Major Histocompatibility Complex, Interferon-gamma, HLA Antigens, Genetics, Transcriptional regulation, Humans, Scaffold/matrix attachment region, Gene, Genetics (clinical), B-Lymphocytes, Models, Genetic, Genome, Human, Fibroblasts, Matrix Attachment Regions, Chromatin, Recombinant Proteins, biology.protein, Chromatin Loop

Abstract

The folding of chromatin into topologically constrained loop domains is essential for genomic function. We have identified genomic anchors that define the organization of chromatin loop domains across the human major histocompatibility complex (MHC). This locus contains critical genes for immunity and is associated with more diseases than any other region of the genome. Classical MHC genes are expressed in a cell type-specific pattern and can be induced by cytokines such as interferon-gamma (IFNG). Transcriptional activation of the MHC was associated with a reconfiguration of chromatin architecture resulting from the formation of additional genomic anchors. These findings suggest that the dynamic arrangement of genomic anchors and loops plays a role in transcriptional regulation.

Published

2008

32. P-STAT1 mediates higher-order chromatin remodelling of the human MHC in response to IFNgamma

Author

Diane Watling, Ana P. Costa-Pereira, Tania A. Jones, Denise Sheer, Rossitza Christova, Andreas Bolzer, Pei-Jun Wu, and Ian M. Kerr

Subjects

Transcription, Genetic, Quantitative Trait Loci, Major histocompatibility complex, Antiviral Agents, Chromatin remodeling, stat, Histones, Major Histocompatibility Complex, Interferon-gamma, Cell Line, Tumor, Humans, STAT1, Phosphorylation, ChIA-PET, Immunity, Cellular, biology, DNA Helicases, Nuclear Proteins, Acetylation, Cell Biology, Chromatin Assembly and Disassembly, Molecular biology, Chromatin, Histone, STAT1 Transcription Factor, biology.protein, Protein Processing, Post-Translational, Signal Transduction, Transcription Factors

Abstract

Transcriptional activation of the major histocompatibility complex (MHC) by IFNγ is a key step in cell-mediated immunity. At an early stage of IFNγ induction, chromatin carrying the entire MHC locus loops out from the chromosome 6 territory. We show here that JAK/STAT signalling triggers this higher-order chromatin remodelling and the entire MHC locus becomes decondensed prior to transcriptional activation of the classical HLA class II genes. A single point mutation of STAT1 that prevents phosphorylation is sufficient to abolish chromatin remodelling, thus establishing a direct link between the JAK/STAT signalling pathway and human chromatin architecture. The onset of chromatin remodelling corresponds with the binding of activated STAT1 and the chromatin remodelling enzyme BRG1 at specific sites within the MHC, and is followed by RNA-polymerase recruitment and histone hyperacetylation. We propose that the higher-order chromatin remodelling of the MHC locus is an essential step to generate a transcriptionally permissive chromatin environment for subsequent activation of classical HLA genes.

Published

2007

33. Abstract 807: Selamectin and ivermectin are small molecule inhibitors that interfere with Sin3A-PAH2 function and exert anti-tumor activity in triple-negative breast cancer

Author

Nidhi Bansal, Edgardo Aritzia, Eduardo F. Farias, Shuai Yang, Authur Zelent, Boris A. Leibovitch, Samuel Waxman, Rajal Sharma, Ming-Ming Zhou, Rossitza Christova, Yeon-Jin Kwon, Mihaly Mezei, and Lei Zeng

Subjects

Cancer Research, Biology, Pharmacology, Cell cycle, In vitro, chemistry.chemical_compound, Selamectin, Oncology, Paclitaxel, chemistry, In vivo, parasitic diseases, medicine, Transcription factor, Tamoxifen, Triple-negative breast cancer, medicine.drug

Abstract

INTRODUCTION: Sin3 is a complex scaffolding protein that participates in epigenetic regulation involved in a variety of biological processes, including chromatin remodeling, development, differentiation, cell cycle and survival. Paired Amphipathic domain 2 (PAH2) domain of Sin3 was shown to interact with Sin3 interacting domain (SID)-containing transcription factors, such as Mxd1, KLF10/11, and REST. Previously, we reported that SID transcripts and decoy peptides disrupt the interactions between Sin3-PAH2 domain and SID-containing transcription factors and induce epigenetic reprogramming in TNBC. RESULTS AND CONCLUSION: Here we show that fourteen SMIs mimicking SID decoys were identified by in silico computation from a chemical library composed of 115,000 compounds. We confirmed that selamectin and ivermectin are SID decoys using duo-link assays. Our NMR 15N-HSQC spectroscopy binding results further demonstrated ivermectin, which shares the same binding site as selamectin, directly interacted with PAH2. Moreover, selamectin inhibited Sin3 repression activity as measured by mammalian two-hybrid and in vitro GST pull-down assays. Notably, ivermectin was approved by Food and Drug Administration (FDA) to treat small animals and human. However, the anti-tumorigenic roles for these SMIs had not been investigated in TNBC in vitro and in vivo. Remarkably, these SMIs did not affect growth in 2-dimensional (2D) clonogenecity assay, but significantly suppressed growth in 3D matrigel and tumorsphere cultures. Moreover, selamectin significantly suppressed Myc mammary tumor growth in vivo more than 50 percent without any cytotoxicity. Selamectin and ivermectin induced re-expression of CDH1 and ESR1, restoring tamoxifen sensitivity. Treatment with these compounds inhibited in vitro invasion as measured by Boyden chamber in MCF7/ADR and MDA-MB-231 cells. Selamectin and ivermectin were shown to alleviate multidrug resistance and enhance doxorubicin and paclitaxel cytotoxicity in MCF7/ADR cells, which is unrelated to disruption of Sin3-PAH2. Based on further studies of the Sin3A complexes using selamectin and ivermectin, we seek to identify novel SMIs with better efficiency for targeting Sin3 complex and treating TNBCs in the future. Citation Format: Yeon-Jin Kwon, Boris A. Leibovitch, Lei Zeng, Mihaly Mezei, Rossitza Christova, Shuai Yang, Rajal Sharma, Edgardo Aritzia, nidhi bansal, Ming-Ming Zhou, Authur Zelent, Eduardo Farias, Samuel Waxman. Selamectin and ivermectin are small molecule inhibitors that interfere with Sin3A-PAH2 function and exert anti-tumor activity in triple-negative breast cancer. [abstract]. In: Proceedings of the 105th Annual Meeting of the American Association for Cancer Research; 2014 Apr 5-9; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2014;74(19 Suppl):Abstract nr 807. doi:10.1158/1538-7445.AM2014-807

Published

2014

34. Abstract 411: Targeted PF1, JARID1B inhibition induces epigenetic reprogramming in triple negative breast cancer

Author

Arthur Zelent, Boris A. Leibovitch, Samuel Waxman, Kevin Petrie, Eduardo F. Farias, Edgardo V. Ariztia, Veronica Gil, Rossitza Christova, Nidhi Bansal, Louise Howell, and Ming-Ming Zhou

Subjects

Cancer Research, Oncology, Cancer cell, Cancer research, Estrogen receptor, H3K4me3, Epigenetics, Biology, Bioinformatics, Reprogramming, Transcription factor, Epigenetic therapy, Triple-negative breast cancer

Abstract

Triple Negative Breast cancer (TNBC) is an aggressive subtype of breast cancer associated with early recurrence and poor prognosis. The treatment options are limited due to lack of expression of common drug targets: estrogen receptor (ER), Progesterone receptor (PR) and Epidermal growth factor receptor 2 (Her2). Epigenetic programs can generate aberrant transcription contributing to TNBC progression; however the dynamic and reversible nature of epigenetic changes offers the possibility to reprogram cancer cells to re-express targets that can render TNBC sensitive to targeted therapies like tamoxifen. Envisioning such ‘epidrugs’, we previously published that targeting PAH2 domain of the master transcriptional scaffold Sin3 by stable expression of 13-mer peptide corresponding to a specific motif called SID (mSin3A interaction domain) disrupts its interaction with a small group of SID-containing transcription factors. This interference reverts the expression of important breast cancer-associated genes and impairs tumor growth in vivo. We have now extended our study towards the evaluation of a cell penetrating SID peptide (pSID) in in vitro and in vivo models to establish parameters for the design of targeted epigenetic therapy for TNBC. pSID co-localizes with Sin3A and interference with PAH2-mediated Sin3A functions by pSID is shown by disruption of Sin3A-MAD1 interactions in Co-IP and Duo-Link assays. pSID treatment in MDA-MB 231 cells results in functional re-expression of CDH1 and ER along with increased H3K4 and decreased H3K27 methylation on their promoters. We also show reduction in the tumorsphere formation by pSID-pretreated MDA-MB-231 cells indicating possible epigenetic reprogramming of tumor initiating stem cells towards a differentiated phenotype. Support to this hypothesis is added by the 50% reduction in tumor growth and re-expression of CDH1 observed in FVB mice injected with pSID-pretreated MMTV-myc cells. Moreover, microarray expression analysis indicates pSID-induced EMT reversal, increased cell adhesion and reduced cell migration. Intriguingly, upon further dissection of the mechanism of epigenetic regulation by pSID we show dissociation of two important chromatin readers/modifiers from the Sin3 complex: histone H3K4Me3/2 demethylase JARID1B and H3K4Me0 binding PHD-like domain containing protein PF1; both with significantly correlated overexpression in invasive breast carcinoma. We also observe loss of recruitment of JARID1B but not Sin3A from the CDH1 promoter. Currently studies are underway to understand the cooperative role between JARID1B and PF1 in potentiating the aberrant transcription regulation by Sin3 at important breast cancer-associated promoters that can be selectively reprogrammed by SID decoys. We believe this selectivity can limit the otherwise adverse affects that may be observed by the use of generic HDAC inhibitors and demethylating agents. Citation Format: Rossitza Christova, Kevin Petrie, Nidhi Bansal, Boris Leibovitch, Louise Howell, Veronica Gil, Ming-Ming Zhou, Edgardo Ariztia, Eduardo Farias, Arthur Zelent, Samuel Waxman. Targeted PF1, JARID1B inhibition induces epigenetic reprogramming in triple negative breast cancer. [abstract]. In: Proceedings of the 105th Annual Meeting of the American Association for Cancer Research; 2014 Apr 5-9; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2014;74(19 Suppl):Abstract nr 411. doi:10.1158/1538-7445.AM2014-411

Published

2014

35. Association of human TFIID-promoter complexes with silenced mitotic chromatin in vivo

Author

Thomas Oelgeschläger and Rossitza Christova

Subjects

Mitosis, RNA polymerase II, Promoter, Cell Biology, Biology, Phosphoproteins, Molecular biology, Chromatin, Cell biology, Transcription Factors, TFII, Transcription Factor TFIID, biology.protein, Transcription Factor TFIIB, Humans, Gene Silencing, RNA Polymerase II, Transcription factor II D, Promoter Regions, Genetic, Transcription factor II B, RNA polymerase II holoenzyme, HeLa Cells, Transcription Factors

Abstract

When eukaryotic cells enter mitosis, transcription is abruptly silenced. Earlier studies indicated that most transcription factors and RNA polymerase II (RNAP II) are displaced when chromatin is condensed into mitotic chromosomes. A more recent study suggested that hitherto unidentified factors might 'bookmark' previously active genes for rapid reactivation after cell division. Here we used chromatin immunoprecipitation (ChIP) assays to examine the association of TFIID, TFIIB, NC2 and RNAP II with various gene promoters in asynchronous and mitotic human cell populations. We show that TFIID and TFIIB can remain associated with active gene promoters during mitosis whereas RNA polymerase II is displaced, and also that NC2, originally identified as ubiquitous repressor of transcription, is associated with active gene promoters in asynchronous cell populations and is displaced from some, but not all, genes in mitotic cells. Consistent with the remarkable stability of TFIID-promoter complexes observed in vitro, our data suggest that these complexes can withstand condensation of chromatin into transcriptionally silent chromosomes. Stable TFIID-promoter complexes are therefore implicated in the propagation of cell-type-specific gene expression patterns through cell division.

Published

2001