Your search keyword '"Megan Washington"' showing total 14 results

1. Baseline mutational patterns and sustained MRD negativity in patients with high-risk smoldering myeloma

Author

Sham Mailankody, Dickran Kazandjian, Neha Korde, Mark Roschewski, Elisabet Manasanch, Manisha Bhutani, Nishant Tageja, Mary Kwok, Yong Zhang, Adriana Zingone, Laurence Lamy, Rene Costello, Candis Morrison, Malin Hultcrantz, Austin Christofferson, Megan Washington, Martin Boateng, Seth M. Steinberg, Maryalice Stetler-Stevenson, William D. Figg, Elli Papaemmanuil, Wyndham H. Wilson, Jonathan J. Keats, and Ola Landgren

Subjects

Specialties of internal medicine, RC581-951

Abstract

Abstract: Early results of a prospective phase 2 clinical trial of carfilzomib, lenalidomide, and dexamethasone followed by lenalidomide maintenance in high-risk smoldering myeloma showed promising results that were previously published. Here, we provide novel insights into the genetic landscape of high-risk smoldering myeloma and information on sustained minimal residual disease (MRD) negativity with an expanded cohort of patients. Eighteen patients with high-risk smoldering myeloma were enrolled between 29 May 2012, and 14 January 2014. We included patients with newly diagnosed multiple myeloma enrolled in a parallel trial who received the same therapy (reference group). The overall response rate was 100%. With median potential follow-up of 43.3 months, 10 (63%) remain in MRD negativity, and the estimated 4-year progression-free and overall survival rates are 71% and 100%, respectively. Importantly, we report differences in mutational patterns in patients with high-risk smoldering myeloma and newly diagnosed multiple myeloma, reflected in a lower frequency of mutations in significant myeloma genes (6.6% vs 45%) and NFKB pathway genes (6.6% vs 25%). Treatment with carfilzomib, lenalidomide, and dexamethasone followed by lenalidomide maintenance was associated with a 100% response rate and 63% MRD negativity with a safety profile consistent with previous reports for this regimen. This study had a small numbers of participants, but there seemed to be important differences in the genetic landscape of patients with high-risk smoldering myeloma and those with newly diagnosed multiple myeloma, suggestive of a more treatment-responsive biology in early disease.

Published

2017

2. Somatic inactivating PTPRJ mutations and dysregulated pathways identified in canine malignant melanoma by integrated comparative genomic analysis.

Author

William P D Hendricks, Victoria Zismann, Karthigayini Sivaprakasam, Christophe Legendre, Kelsey Poorman, Waibhav Tembe, Nieves Perdigones, Jeffrey Kiefer, Winnie Liang, Valerie DeLuca, Mitchell Stark, Alison Ruhe, Roe Froman, Nicholas S Duesbery, Megan Washington, Jessica Aldrich, Mark W Neff, Matthew J Huentelman, Nicholas Hayward, Kevin Brown, Douglas Thamm, Gerald Post, Chand Khanna, Barbara Davis, Matthew Breen, Alexander Sekulic, and Jeffrey M Trent

Subjects

Genetics, QH426-470

Abstract

Canine malignant melanoma, a significant cause of mortality in domestic dogs, is a powerful comparative model for human melanoma, but little is known about its genetic etiology. We mapped the genomic landscape of canine melanoma through multi-platform analysis of 37 tumors (31 mucosal, 3 acral, 2 cutaneous, and 1 uveal) and 17 matching constitutional samples including long- and short-insert whole genome sequencing, RNA sequencing, array comparative genomic hybridization, single nucleotide polymorphism array, and targeted Sanger sequencing analyses. We identified novel predominantly truncating mutations in the putative tumor suppressor gene PTPRJ in 19% of cases. No BRAF mutations were detected, but activating RAS mutations (24% of cases) occurred in conserved hotspots in all cutaneous and acral and 13% of mucosal subtypes. MDM2 amplifications (24%) and TP53 mutations (19%) were mutually exclusive. Additional low-frequency recurrent alterations were observed amidst low point mutation rates, an absence of ultraviolet light mutational signatures, and an abundance of copy number and structural alterations. Mutations that modulate cell proliferation and cell cycle control were common and highlight therapeutic axes such as MEK and MDM2 inhibition. This mutational landscape resembles that seen in BRAF wild-type and sun-shielded human melanoma subtypes. Overall, these data inform biological comparisons between canine and human melanoma while suggesting actionable targets in both species.

Published

2018

3. Comprehensive molecular profiling of 718 Multiple Myelomas reveals significant differences in mutation frequencies between African and European descent cases.

Author

Zarko Manojlovic, Austin Christofferson, Winnie S Liang, Jessica Aldrich, Megan Washington, Shukmei Wong, Daniel Rohrer, Scott Jewell, Rick A Kittles, Mary Derome, Daniel Auclair, David Wesley Craig, Jonathan Keats, and John D Carpten

Subjects

Genetics, QH426-470

Abstract

Multiple Myeloma (MM) is a plasma cell malignancy with significantly greater incidence and mortality rates among African Americans (AA) compared to Caucasians (CA). The overall goal of this study is to elucidate differences in molecular alterations in MM as a function of self-reported race and genetic ancestry. Our study utilized somatic whole exome, RNA-sequencing, and correlated clinical data from 718 MM patients from the Multiple Myeloma Research Foundation CoMMpass study Interim Analysis 9. Somatic mutational analyses based upon self-reported race corrected for ancestry revealed significant differences in mutation frequency between groups. Of interest, BCL7A, BRWD3, and AUTS2 demonstrate significantly higher mutation frequencies among AA cases. These genes are all involved in translocations in B-cell malignancies. Moreover, we detected a significant difference in mutation frequency of TP53 and IRF4 with frequencies higher among CA cases. Our study provides rationale for interrogating diverse tumor cohorts to best understand tumor genomics across populations.

Published

2017

4. Table S5-6 from Ponatinib Shows Potent Antitumor Activity in Small Cell Carcinoma of the Ovary Hypercalcemic Type (SCCOHT) through Multikinase Inhibition

Author

Jeffrey M. Trent, David G. Huntsman, Bernard E. Weissman, Praveen Nair, Barbara C. Vanderhyden, Ralf Hass, Aleksandar Sekulic, Anthony N. Karnezis, Yemin Wang, Michael B. Major, Emily M. Cousins, Victoria L. Zismann, Salvatore J. Facista, Megan Washington, Winnie S. Liang, Nanyun Tang, Chris Sereduk, Elizabeth A. Raupach, Patrick Pirrotte, Ritin Sharma, Pilar Ramos, Jeffrey Kiefer, Hongwei Yin, Krystal A. Orlando, William P.D. Hendricks, and Jessica D. Lang

Abstract

Supplemental Table 5. SCCOHT-1 ABPP data; Supplemental Table 6. BIN67 ABPP data.

Published

2023

5. Table S3 from Ponatinib Shows Potent Antitumor Activity in Small Cell Carcinoma of the Ovary Hypercalcemic Type (SCCOHT) through Multikinase Inhibition

Author

Jeffrey M. Trent, David G. Huntsman, Bernard E. Weissman, Praveen Nair, Barbara C. Vanderhyden, Ralf Hass, Aleksandar Sekulic, Anthony N. Karnezis, Yemin Wang, Michael B. Major, Emily M. Cousins, Victoria L. Zismann, Salvatore J. Facista, Megan Washington, Winnie S. Liang, Nanyun Tang, Chris Sereduk, Elizabeth A. Raupach, Patrick Pirrotte, Ritin Sharma, Pilar Ramos, Jeffrey Kiefer, Hongwei Yin, Krystal A. Orlando, William P.D. Hendricks, and Jessica D. Lang

Abstract

IC50 summary of validated drug hits in SCCOHT cell lines.

Published

2023

6. Data from Ponatinib Shows Potent Antitumor Activity in Small Cell Carcinoma of the Ovary Hypercalcemic Type (SCCOHT) through Multikinase Inhibition

Author

Jeffrey M. Trent, David G. Huntsman, Bernard E. Weissman, Praveen Nair, Barbara C. Vanderhyden, Ralf Hass, Aleksandar Sekulic, Anthony N. Karnezis, Yemin Wang, Michael B. Major, Emily M. Cousins, Victoria L. Zismann, Salvatore J. Facista, Megan Washington, Winnie S. Liang, Nanyun Tang, Chris Sereduk, Elizabeth A. Raupach, Patrick Pirrotte, Ritin Sharma, Pilar Ramos, Jeffrey Kiefer, Hongwei Yin, Krystal A. Orlando, William P.D. Hendricks, and Jessica D. Lang

Abstract

Purpose: Small cell carcinoma of the ovary, hypercalcemic type (SCCOHT) is a rare, aggressive ovarian cancer in young women that is universally driven by loss of the SWI/SNF ATPase subunits SMARCA4 and SMARCA2. A great need exists for effective targeted therapies for SCCOHT.Experimental Design: To identify underlying therapeutic vulnerabilities in SCCOHT, we conducted high-throughput siRNA and drug screens. Complementary proteomics approaches profiled kinases inhibited by ponatinib. Ponatinib was tested for efficacy in two patient-derived xenograft (PDX) models and one cell-line xenograft model of SCCOHT.Results: The receptor tyrosine kinase (RTK) family was enriched in siRNA screen hits, with FGFRs and PDGFRs being overlapping hits between drug and siRNA screens. Of multiple potent drug classes in SCCOHT cell lines, RTK inhibitors were only one of two classes with selectivity in SCCOHT relative to three SWI/SNF wild-type ovarian cancer cell lines. We further identified ponatinib as the most effective clinically approved RTK inhibitor. Reexpression of SMARCA4 was shown to confer a 1.7-fold increase in resistance to ponatinib. Subsequent proteomic assessment of ponatinib target modulation in SCCOHT cell models confirmed inhibition of nine known ponatinib target kinases alongside 77 noncanonical ponatinib targets in SCCOHT. Finally, ponatinib delayed tumor doubling time 4-fold in SCCOHT-1 xenografts while reducing final tumor volumes in SCCOHT PDX models by 58.6% and 42.5%.Conclusions: Ponatinib is an effective agent for SMARCA4-mutant SCCOHT in both in vitro and in vivo preclinical models through its inhibition of multiple kinases. Clinical investigation of this FDA-approved oncology drug in SCCOHT is warranted. Clin Cancer Res; 24(8); 1932–43. ©2018 AACR.

Published

2023

7. Figures S1-3 from Ponatinib Shows Potent Antitumor Activity in Small Cell Carcinoma of the Ovary Hypercalcemic Type (SCCOHT) through Multikinase Inhibition

Author

Jeffrey M. Trent, David G. Huntsman, Bernard E. Weissman, Praveen Nair, Barbara C. Vanderhyden, Ralf Hass, Aleksandar Sekulic, Anthony N. Karnezis, Yemin Wang, Michael B. Major, Emily M. Cousins, Victoria L. Zismann, Salvatore J. Facista, Megan Washington, Winnie S. Liang, Nanyun Tang, Chris Sereduk, Elizabeth A. Raupach, Patrick Pirrotte, Ritin Sharma, Pilar Ramos, Jeffrey Kiefer, Hongwei Yin, Krystal A. Orlando, William P.D. Hendricks, and Jessica D. Lang

Abstract

Supplemental Figure 1. COV434-pIND20-Brg1 SMARCA4 induction optimization; Supplemental Figure 2. Kinase hits from siRNA screen mapped to kinome dendrogram; Supplemental Figure 3. ClueGo analysis of validated siRNA screen hits.

Published

2023

8. Supplemental Methods from Ponatinib Shows Potent Antitumor Activity in Small Cell Carcinoma of the Ovary Hypercalcemic Type (SCCOHT) through Multikinase Inhibition

Author

Jeffrey M. Trent, David G. Huntsman, Bernard E. Weissman, Praveen Nair, Barbara C. Vanderhyden, Ralf Hass, Aleksandar Sekulic, Anthony N. Karnezis, Yemin Wang, Michael B. Major, Emily M. Cousins, Victoria L. Zismann, Salvatore J. Facista, Megan Washington, Winnie S. Liang, Nanyun Tang, Chris Sereduk, Elizabeth A. Raupach, Patrick Pirrotte, Ritin Sharma, Pilar Ramos, Jeffrey Kiefer, Hongwei Yin, Krystal A. Orlando, William P.D. Hendricks, and Jessica D. Lang

Abstract

Supplemental Materials and Methods

Published

2023

9. Feeding Habits of Vector Mosquitoes in Harris County, TX, 2018

Author

Taylor Guynup, Megan Washington, Chris Fredregill, Elizabeth M Dewey, Christopher Tarrand, R. Jason Pitts, Dagne Duguma, and James G Mann

Subjects

030231 tropical medicine, Population, Zoology, Human pathogen, Mosquito Vectors, Aedes aegypti, DNA barcoding, 03 medical and health sciences, 0302 clinical medicine, Aedes, Animals, education, 030304 developmental biology, 0303 health sciences, education.field_of_study, General Veterinary, biology, Host (biology), Transmission (medicine), Feeding Behavior, Blood feeding, biology.organism_classification, Texas, Culex, Culicidae, Infectious Diseases, Insect Science, Vector (epidemiology), Female, Parasitology

Abstract

Mosquito-borne pathogens contribute significantly to the global burden of infectious diseases and are a continuing public health concern in the United States. Blood feeding by vector mosquitoes is a critical step in the transmission of human pathogens. Continuous surveillance of mosquito feeding patterns, especially in major population centers, is necessary for sustainable, effective control strategies. To better understand female feeding habits in Harris County, TX, we trapped mosquitoes from various locations, distributed among urban and semi-urban environments. Bloodmeal hosts were determined using a cytochrome C oxidase I DNA barcoding strategy. We identified a diverse array of vertebrate hosts with a high degree of avian host utilization, most surprisingly from anthropophilic species like Aedes aegypti (L.). We also detected sequences from two different vertebrate hosts in about half of specimens examined, suggesting that multiple bloodmeals had been acquired in the same feeding cycle by a sizable fraction of females in both urban and semi-urban locations. The high proportion of feeding on domestic chickens may indicate that a significant number of homeowners are rearing chickens within close proximity to study trap sites. As non-amplifying hosts, chickens may have a diluting effect on West Nile virus, as well as a zooprophylactic effect in their immediate vicinities. Ultimately, spatial and temporal host utilization patterns add insight into potential disease transmission dynamics, thereby informing vector control strategies in Harris County and other metropolitan areas.

Published

2020

10. Genomic Basis of Multiple Myeloma Subtypes from the MMRF CoMMpass Study

Author

Hearn Jay Cho, Jennifer Stumph, Sara Nasser, Kyle McBride, Saad Z. Usmani, David Craig, Andrea Donnelly, Norma C. Gutiérrez, John D. Carpten, Christophe Legendre, Sagar Lonial, Megan Washington, Kimberly Collison, Austin Christofferson, Mattia D'Agostino, Shari Kyman, David S. Siegel, Darla K. Liles, Jeffrey L. Wolf, Jesus G. Berdeja, Barbara Zaugg, Jessica Aldrich, Ahmet Kurdoglu, Scott D. Jewell, Jonathan J Keats, Ruben Niesvizky, Adrienne Helland, Rebecca Reiman, Mary Derome, Brooks Benard, Andrzej Jakubowiak, Brianne Docter, Meghan Kirchhoff, Moshe Yair Levy, Kristi Stephenson, Bryce Turner, Ajai Chari, Jackie McDonald, Pam Kidd, Daniel Penaherrera, Ravi Vij, Martin Boateng, Winnie S. Liang, Daniel Auclair, Sheri Skerget, Maureen Toone, Jennifer Yesil, Venkata Yellapantula, Lori Cuyugan, Alex Blanski, Gregory Orloff, Sundar Jagannath, Erica Tassone, Manuela Gamella, Jonathan Adkins, Chase Miller, Daniel C. Rohrer, and Kenneth C. Anderson

Subjects

Oncology, medicine.medical_specialty, Transition (genetics), business.industry, medicine.medical_treatment, Immunotherapy, medicine.disease, Precision medicine, Genome, Internal medicine, Cohort, medicine, business, Exome, Gene, Multiple myeloma

Abstract

Multiple myeloma is a treatable, but currently incurable, hematological malignancy of plasma cells characterized by diverse and complex tumor genetics for which precision medicine approaches to treatment are lacking. The MMRF CoMMpass study is a longitudinal, observational clinical study of newly diagnosed multiple myeloma patients where tumor samples are characterized using whole genome, exome, and RNA sequencing at diagnosis and progression, and clinical data is collected every three months. Analyses of the baseline cohort identified genes that are the target of recurrent gain- and loss-of-function events. Consensus clustering identified 8 and 12 unique copy number and expression subtypes of myeloma, respectively, identifying high- risk genetic subtypes and elucidating many of the molecular underpinnings of these unique biological groups. Analysis of serial samples showed 25.5% of patients transition to a high-risk expression subtype at progression. We observed robust expression of immunotherapy targets in this subtype, suggesting a potential therapeutic option.

Published

2021

11. Somatic inactivating PTPRJ mutations and dysregulated pathways identified in canine melanoma by integrated comparative genomic analysis

Author

Jessica Aldrich, Jeffrey M. Trent, Megan Washington, William P.D. Hendricks, Alison L. Ruhe, Karthigayini Sivaprakasam, Victoria Zismann, Mark W. Neff, Matthew Breen, Gerry Post, Matthew J. Huentelman, Nicholas S. Duesbery, Winnie S. Liang, Barbara Davis, Jeff Kiefer, Chand Khanna, Nicholas K. Hayward, Waibhav Tembe, Christophe Legendre, Kevin N. Brown, Roe Froman, Valerie DeLuca, Douglas H. Thamm, Aleksandar Sekulic, Mitchell S. Stark, and Kelsey Poorman

Subjects

Whole genome sequencing, Sanger sequencing, Genetics, 0303 health sciences, Tumor suppressor gene, Melanoma, Point mutation, Biology, medicine.disease, 3. Good health, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, 030220 oncology & carcinogenesis, medicine, symbols, Ultraviolet light, Canine Melanoma, neoplasms, 030304 developmental biology, Comparative genomic hybridization

Abstract

Canine malignant melanoma, a significant cause of mortality in domestic dogs, is a powerful comparative model for human melanoma, but little is known about its genetic etiology. We mapped the genomic landscape of canine melanoma through multi-platform analysis of 37 tumors (31 mucosal, 3 acral, 2 cutaneous, and 1 uveal) and 17 matching constitutional samples including long- and short-insert whole genome sequencing, RNA sequencing, array comparative genomic hybridization, single nucleotide polymorphism array, and targeted Sanger sequencing analyses. We identified novel predominantly truncating mutations in the putative tumor suppressor genePTPRJin 19% of cases. NoBRAFmutations were detected, but activatingRASmutations (24% of cases) occurred in conserved hotspots in all cutaneous and acral and 13% of mucosal subtypes.MDM2amplifications (24%) andTP53mutations (19%) were mutually exclusive. Additional low-frequency recurrent alterations were observed amidst low point mutation rates, an absence of ultraviolet light mutational signatures, and an abundance of copy number and structural alterations. Mutations that modulate cell proliferation and cell cycle control were common and highlight therapeutic axes such as MEK and MDM2 inhibition. This mutational landscape resembles that seen inBRAFwild-type and sun-shielded human melanoma subtypes. Overall, these data inform biological comparisons between canine and human melanoma while suggesting actionable targets in both species.AUTHOR SUMMARYMelanoma, an aggressive cancer arising from transformed melanocytes, commonly occurs in pet dogs. Unlike human melanoma, which most often occurs in sun-exposed cutaneous skin, canine melanoma typically arises in sun-shielded oral mucosa. Clinical features of canine melanoma resemble those of human melanoma, particularly the less common sun-shielded human subtypes. However, whereas the genomic basis of diverse human melanoma subtypes is well understood, canine melanoma genomics remain poorly defined. Similarly, although diverse new treatments for human melanoma based on a biologic disease understanding have recently shown dramatic improvements in outcomes for these patients, treatments for canine melanoma are limited and outcomes remain universally poor. Detailing the genomic basis of canine melanoma thus provides untapped potential for improving the lives of pet dogs while also helping to establish canine melanoma as a comparative model system for informing human melanoma biology and treatment. In order to better define the genomic landscape of canine melanoma, we performed multi-platform characterization of 37 tumors. Our integrated analysis confirms that these tumors commonly contain mutations in canine orthologs of human cancer genes such asRAS,MDM2, andTP53as well mutational patterns that share important similarities with human melanoma subtypes. We have also found a new putative cancer gene,PTPRJ, frequently mutated in canine melanoma. These data will guide additional biologic and therapeutic studies in canine melanoma while framing the utility of comparative studies of canine and human cancers more broadly.

Published

2017

12. Ponatinib Shows Potent Antitumor Activity in Small Cell Carcinoma of the Ovary Hypercalcemic Type (SCCOHT) through Multikinase Inhibition

Author

Patrick Pirrotte, Anthony N. Karnezis, Jeff Kiefer, Jeffrey M. Trent, Krystal A. Orlando, Michael B. Major, Bernard E. Weissman, David G. Huntsman, Megan Washington, Yemin Wang, Nanyun Tang, Ritin Sharma, Elizabeth A. Raupach, Emily M. Cousins, Victoria Zismann, Barbara C. Vanderhyden, Pilar Ramos, Winnie S. Liang, Hongwei Yin, Praveen Nair, William P.D. Hendricks, Chris Sereduk, Salvatore Facista, Aleksandar Sekulic, Ralf Hass, and Jessica D. Lang

Subjects

0301 basic medicine, Cancer Research, Cell, Pharmacology, Receptor tyrosine kinase, law.invention, chemistry.chemical_compound, Mice, 0302 clinical medicine, law, Protein Interaction Mapping, Protein Interaction Maps, Carcinoma, Small Cell, RNA, Small Interfering, Cancer, Ovarian Neoplasms, 0303 health sciences, Tumor, biology, Kinase, Ponatinib, Imidazoles, Ovarian Cancer, 3. Good health, Pyridazines, medicine.anatomical_structure, Oncology, 5.1 Pharmaceuticals, 030220 oncology & carcinogenesis, SMARCA4, Female, Development of treatments and therapeutic interventions, Biotechnology, Oncology and Carcinogenesis, Antineoplastic Agents, Small Interfering, Small-cell carcinoma, Article, Cell Line, 03 medical and health sciences, Rare Diseases, In vivo, Cell Line, Tumor, medicine, Animals, Humans, Oncology & Carcinogenesis, Protein Kinase Inhibitors, 030304 developmental biology, Animal, business.industry, Carcinoma, Computational Biology, Receptor Protein-Tyrosine Kinases, Small Cell, medicine.disease, Xenograft Model Antitumor Assays, Disease Models, Animal, Orphan Drug, Good Health and Well Being, 030104 developmental biology, chemistry, Disease Models, Cancer research, biology.protein, RNA, Suppressor, business, Ovarian cancer

Abstract

Structured AbstractPurpose: Subunits of the SWI/SNF chromatin-remodeling complex are tumor suppressors inactivated in ∼20% of all cancers. Yet, few targeted treatments for SWI/SNF-mutant cancers exist. Small cell carcinoma of the ovary, hypercalcemic type (SCCOHT) is a rare, aggressive ovarian cancer in young women that is universally driven by loss of the SWI/SNF ATPase subunits, SMARCA4 and SMARCA2. Given poor two-year survival rates for these women, a great need exists for effective targeted therapies.Experimental Design: To identify underlying therapeutic vulnerabilities in SCCOHT, we conducted high-throughput siRNA and drug screens. Complementary proteomics approaches comprehensively profiled kinases inhibited by ponatinib. Ponatinib was tested for efficacy in two PDX models and one cell line xenograft model of SCCOHT.Results: FGFRs and PDGFRs were overlapping hits between screens and the receptor tyrosine kinase (RTK) family was enriched in the siRNA screen hits. Evaluation of eleven RTK inhibitors in three SCCOHT cell lines identified ponatinib, an inhibitor of multiple RTKs, as the most effective clinically approved agent. Proteomics approaches confirmed inhibition of known targets of ponatinib and more than 20 non-canonical ponatinib targets. Ponatinib also delayed tumor doubling time 4-fold in SCCOHT-1 xenografts and reducing final tumor volumes in two SCCOHT patient-derived xenograft (PDX) models by 58.6% and 42.5%.Conclusion: Ponatinib is an effective agent for SCCOHT in both in vitro and in vivo preclinical models through its inhibition of multiple kinases. Clinical investigation of this FDA-approved oncology drug in SCCOHT is warranted.Additional InformationThis work was supported by research funds from the Canadian Cancer Society Research Institute 34 (#703458, D.G.H.), the National Institutes of Health (R01 CA195670-01, B.E.W., D.G.H., and 35 J.M.T., and T32 HL007106-39 to E.M.C), the Terry Fox Research Institute Initiative New Frontiers Program in Cancer (#1021, D.G.H.), the British Columbia Cancer Foundation (D.G.H.), the VGH & UBC Foundation (D.G.H.), the Anne Rita Monahan Foundation (P.R.), the Marsha Rivkin Center for Ovarian Cancer Research (J.M.T.), the Ovarian Cancer Alliance of Arizona (J.M.T.), the Small Cell Ovarian Cancer Foundation (P.R., J.D.L., B.V., and J.M.T.), and philanthropic support to the TGen Foundation (J.M.T.).COI disclosure statement: The authors declare no potential conflicts of interest.

Published

2017

13. Baseline mutational patterns and sustained MRD negativity in patients with high-risk smoldering myeloma

Author

Elli Papaemmanuil, Sham Mailankody, Megan Washington, Elisabet E. Manasanch, Manisha Bhutani, Mark Roschewski, Nishant Tageja, Austin Christofferson, Ola Landgren, Jonathan J Keats, Mary Kwok, Rene Costello, Wyndham H. Wilson, William D. Figg, Maryalice Stetler-Stevenson, Neha Korde, Laurence Lamy, Dickran Kazandjian, Martin Boateng, Seth M. Steinberg, Malin Hultcrantz, Candis Morrison, Yong Zhang, and Adriana Zingone

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, Clinical Trials and Observations, Phases of clinical research, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, immune system diseases, Internal medicine, hemic and lymphatic diseases, medicine, Multiple myeloma, Dexamethasone, Lenalidomide, business.industry, Hematology, medicine.disease, Carfilzomib, Minimal residual disease, Regimen, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, Cohort, business, medicine.drug

Abstract

Early results of a prospective phase 2 clinical trial of carfilzomib, lenalidomide, and dexamethasone followed by lenalidomide maintenance in high-risk smoldering myeloma showed promising results that were previously published. Here, we provide novel insights into the genetic landscape of high-risk smoldering myeloma and information on sustained minimal residual disease (MRD) negativity with an expanded cohort of patients. Eighteen patients with high-risk smoldering myeloma were enrolled between 29 May 2012, and 14 January 2014. We included patients with newly diagnosed multiple myeloma enrolled in a parallel trial who received the same therapy (reference group). The overall response rate was 100%. With median potential follow-up of 43.3 months, 10 (63%) remain in MRD negativity, and the estimated 4-year progression-free and overall survival rates are 71% and 100%, respectively. Importantly, we report differences in mutational patterns in patients with high-risk smoldering myeloma and newly diagnosed multiple myeloma, reflected in a lower frequency of mutations in significant myeloma genes (6.6% vs 45%) and NFKB pathway genes (6.6% vs 25%). Treatment with carfilzomib, lenalidomide, and dexamethasone followed by lenalidomide maintenance was associated with a 100% response rate and 63% MRD negativity with a safety profile consistent with previous reports for this regimen. This study had a small numbers of participants, but there seemed to be important differences in the genetic landscape of patients with high-risk smoldering myeloma and those with newly diagnosed multiple myeloma, suggestive of a more treatment-responsive biology in early disease.

Published

2017

14. COPB2 loss of function causes a coatopathy with osteoporosis and developmental delay

Author

Shan Chen, Yi-Chien Lee, Bernardo Blanco-Sánchez, Nitesh R. Mehta, Xiaohui Li, Brendan Lee, Catherine DeVile, Jill A. Rosenfeld, Daryl A. Scott, Ming-Ming Jiang, V. Reid Sutton, I-Wen Song, Kyu Sang Joeng, Rossella Venditti, Yuqing Chen, Richard A. Gibbs, John Hicks, Alistair Calder, Ghayda Mirzaa, David R. Murdock, Jeremy Wegner, Gladys Zapata, Tashunka Taylor-Miller, David R. Eyre, Aurélie Clément, Brian Dawson, Joseph M. Sliepka, Jason D. Heaney, Marwan Shinawi, Shalini N. Jhangiani, Donna M. Muzny, Dominyka Batkovskyte, Lisa Emrick, John R. Seavitt, Ronit Marom, Brenna A. Tremp, Maria Antonietta De Matteis, Zixue Jin, Lindsay C. Burrage, Denise G. Lanza, Monte Westerfield, Jeremy Allgrove, Rolf W. Stottmann, Jennifer B. Phillips, Rowenna Roberts, Abbey A. Scott, Neil A. Hanchard, Mahim Jain, Megan Washington, Alyssa A. Tran, Mary E. Dickinson, Ingo Grafe, MaryAnn Weis, Marom, R., Burrage, L. C., Venditti, R., Clement, A., Blanco-Sanchez, B., Jain, M., Scott, D. A., Rosenfeld, J. A., Sutton, V. R., Shinawi, M., Mirzaa, G., Devile, C., Roberts, R., Calder, A. D., Allgrove, J., Grafe, I., Lanza, D. G., Li, X., Joeng, K. S., Lee, Y. -C., Song, I. -W., Sliepka, J. M., Batkovskyte, D., Washington, M., Dawson, B. C., Jin, Z., Jiang, M. -M., Chen, S., Chen, Y., Tran, A. A., Emrick, L. T., Murdock, D. R., Hanchard, N. A., Zapata, G. E., Mehta, N. R., Weis, M. A., Scott, A. A., Tremp, B. A., Phillips, J. B., Wegner, J., Taylor-Miller, T., Gibbs, R. A., Muzny, D. M., Jhangiani, S. N., Hicks, J., Stottmann, R. W., Dickinson, M. E., Seavitt, J. R., Heaney, J. D., Eyre, D. R., Westerfield, M., De Matteis, M. A., and Lee, B.

Subjects

Male, Embryo, Nonmammalian, Developmental Disabilities, Golgi Apparatus, Ascorbic Acid, Haploinsufficiency, Endoplasmic Reticulum, Coatomer Protein, Severity of Illness Index, Bone and Bones, Collagen Type I, Article, Coat Protein Complex I, Mice, symbols.namesake, Intellectual Disability, Genetics, Animals, Humans, COPI complex, RNA, Small Interfering, Child, Zebrafish, Genetics (clinical), Chemistry, Endoplasmic reticulum, collagen trafficking, Brain, Gene Expression Regulation, Developmental, COPB2, juvenile osteoporosis, COPI, Fibroblasts, Golgi apparatus, Ascorbic acid, Cell biology, Coatomer, Child, Preschool, Unfolded protein response, symbols, Osteoporosis, coatopathy, Female, Type I collagen

Abstract

Summary Coatomer complexes function in the sorting and trafficking of proteins between subcellular organelles. Pathogenic variants in coatomer subunits or associated factors have been reported in multi-systemic disorders, i.e., coatopathies, that can affect the skeletal and central nervous systems. We have identified loss-of-function variants in COPB2, a component of the coatomer complex I (COPI), in individuals presenting with osteoporosis, fractures, and developmental delay of variable severity. Electron microscopy of COPB2-deficient subjects’ fibroblasts showed dilated endoplasmic reticulum (ER) with granular material, prominent rough ER, and vacuoles, consistent with an intracellular trafficking defect. We studied the effect of COPB2 deficiency on collagen trafficking because of the critical role of collagen secretion in bone biology. COPB2 siRNA-treated fibroblasts showed delayed collagen secretion with retention of type I collagen in the ER and Golgi and altered distribution of Golgi markers. copb2-null zebrafish embryos showed retention of type II collagen, disorganization of the ER and Golgi, and early larval lethality. Copb2+/− mice exhibited low bone mass, and consistent with the findings in human cells and zebrafish, studies in Copb2+/− mouse fibroblasts suggest ER stress and a Golgi defect. Interestingly, ascorbic acid treatment partially rescued the zebrafish developmental phenotype and the cellular phenotype in Copb2+/− mouse fibroblasts. This work identifies a form of coatopathy due to COPB2 haploinsufficiency, explores a potential therapeutic approach for this disorder, and highlights the role of the COPI complex as a regulator of skeletal homeostasis.