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1. Combined PD-1, BRAF and MEK inhibition in BRAFV600E colorectal cancer: a phase 2 trial

Author

Jun Tian, Jonathan H. Chen, Sherry X. Chao, Karin Pelka, Marios Giannakis, Julian Hess, Kelly Burke, Vjola Jorgji, Princy Sindurakar, Jonathan Braverman, Arnav Mehta, Tomonori Oka, Mei Huang, David Lieb, Maxwell Spurrell, Jill N. Allen, Thomas A. Abrams, Jeffrey W. Clark, Andrea C. Enzinger, Peter C. Enzinger, Samuel J. Klempner, Nadine J. McCleary, Jeffrey A. Meyerhardt, David P. Ryan, Matthew B. Yurgelun, Katie Kanter, Emily E. Van Seventer, Islam Baiev, Gary Chi, Joy Jarnagin, William B. Bradford, Edmond Wong, Alexa G. Michel, Isobel J. Fetter, Giulia Siravegna, Angelo J. Gemma, Arlene Sharpe, Shadmehr Demehri, Rebecca Leary, Catarina D. Campbell, Omer Yilmaz, Gad A. Getz, Aparna R. Parikh, Nir Hacohen, and Ryan B. Corcoran

Subjects
General Medicine, General Biochemistry, Genetics and Molecular Biology
Abstract

While BRAF inhibitor combinations with EGFR and/or MEK inhibitors have improved clinical efficacy in BRAFV600E colorectal cancer (CRC), response rates remain low and lack durability. Preclinical data suggest that BRAF/MAPK pathway inhibition may augment the tumor immune response. We performed a proof-of-concept single-arm phase 2 clinical trial of combined PD-1, BRAF and MEK inhibition with sparatlizumab (PDR001), dabrafenib and trametinib in 37 patients with BRAFV600E CRC. The primary end point was overall response rate, and the secondary end points were progression-free survival, disease control rate, duration of response and overall survival. The study met its primary end point with a confirmed response rate (24.3% in all patients; 25% in microsatellite stable patients) and durability that were favorable relative to historical controls of BRAF-targeted combinations alone. Single-cell RNA sequencing of 23 paired pretreatment and day 15 on-treatment tumor biopsies revealed greater induction of tumor cell-intrinsic immune programs and more complete MAPK inhibition in patients with better clinical outcome. Immune program induction in matched patient-derived organoids correlated with the degree of MAPK inhibition. These data suggest a potential tumor cell-intrinsic mechanism of cooperativity between MAPK inhibition and immune response, warranting further clinical evaluation of optimized targeted and immune combinations in CRC. ClinicalTrials.gov registration: NCT03668431.

Published
2023

2. Data from Reverse Transcriptase Inhibition Disrupts Repeat Element Life Cycle in Colorectal Cancer

Author

David T. Ting, Benjamin D. Greenbaum, Peter J. Park, Kathleen H. Burns, David R. Walt, Shelley L. Berger, Theodore S. Hong, Martin J. Aryee, Miguel N. Rivera, Vikram Deshpande, Ryan B. Corcoran, David P. Ryan, Jennifer Y. Wo, Lipika Goyal, Jeffrey W. Clark, Lawrence S. Blaszkowsky, Jill N. Allen, Hui Zheng, Yasmeen Senussi, Padric M. Garden, Limor Cohen, Vishal Thapar, Matteo Ligorio, Kshitij S. Arora, Niyati Desai, Linda T. Nieman, Michael J. Raabe, Jasmin Joseph-Chazan, Chenyue Lu, Eric C. Tai, Kevin D. Vo, Emily E. Van Seventer, Richard Y. Ebright, Nova Xu, Antuan V. Tran, Stefanie Gerstberger, Annamaria Szabolcs, Charly R. Good, Katherine A. Alexander, Connie Wu, Martin S. Taylor, Christopher Jaicks, Katherine H. Xu, Chong Chu, Anupriya S. Kulkarni, Eunae You, Alexander Solovyov, Aparna R. Parikh, and Mihir Rajurkar

Abstract

Altered RNA expression of repetitive sequences and retrotransposition are frequently seen in colorectal cancer, implicating a functional importance of repeat activity in cancer progression. We show the nucleoside reverse transcriptase inhibitor 3TC targets activities of these repeat elements in colorectal cancer preclinical models with a preferential effect in p53-mutant cell lines linked with direct binding of p53 to repeat elements. We translate these findings to a human phase II trial of single-agent 3TC treatment in metastatic colorectal cancer with demonstration of clinical benefit in 9 of 32 patients. Analysis of 3TC effects on colorectal cancer tumorspheres demonstrates accumulation of immunogenic RNA:DNA hybrids linked with induction of interferon response genes and DNA damage response. Epigenetic and DNA-damaging agents induce repeat RNAs and have enhanced cytotoxicity with 3TC. These findings identify a vulnerability in colorectal cancer by targeting the viral mimicry of repeat elements.Significance:Colorectal cancers express abundant repeat elements that have a viral-like life cycle that can be therapeutically targeted with nucleoside reverse transcriptase inhibitors (NRTI) commonly used for viral diseases. NRTIs induce DNA damage and interferon response that provide a new anticancer therapeutic strategy.This article is highlighted in the In This Issue feature, p. 1397

Published
2023

3. Supplementary Figure from Reverse Transcriptase Inhibition Disrupts Repeat Element Life Cycle in Colorectal Cancer

Author

David T. Ting, Benjamin D. Greenbaum, Peter J. Park, Kathleen H. Burns, David R. Walt, Shelley L. Berger, Theodore S. Hong, Martin J. Aryee, Miguel N. Rivera, Vikram Deshpande, Ryan B. Corcoran, David P. Ryan, Jennifer Y. Wo, Lipika Goyal, Jeffrey W. Clark, Lawrence S. Blaszkowsky, Jill N. Allen, Hui Zheng, Yasmeen Senussi, Padric M. Garden, Limor Cohen, Vishal Thapar, Matteo Ligorio, Kshitij S. Arora, Niyati Desai, Linda T. Nieman, Michael J. Raabe, Jasmin Joseph-Chazan, Chenyue Lu, Eric C. Tai, Kevin D. Vo, Emily E. Van Seventer, Richard Y. Ebright, Nova Xu, Antuan V. Tran, Stefanie Gerstberger, Annamaria Szabolcs, Charly R. Good, Katherine A. Alexander, Connie Wu, Martin S. Taylor, Christopher Jaicks, Katherine H. Xu, Chong Chu, Anupriya S. Kulkarni, Eunae You, Alexander Solovyov, Aparna R. Parikh, and Mihir Rajurkar

Abstract

Supplementary Figure from Reverse Transcriptase Inhibition Disrupts Repeat Element Life Cycle in Colorectal Cancer

Published
2023

4. Supplementary Data from Reverse Transcriptase Inhibition Disrupts Repeat Element Life Cycle in Colorectal Cancer

Author

David T. Ting, Benjamin D. Greenbaum, Peter J. Park, Kathleen H. Burns, David R. Walt, Shelley L. Berger, Theodore S. Hong, Martin J. Aryee, Miguel N. Rivera, Vikram Deshpande, Ryan B. Corcoran, David P. Ryan, Jennifer Y. Wo, Lipika Goyal, Jeffrey W. Clark, Lawrence S. Blaszkowsky, Jill N. Allen, Hui Zheng, Yasmeen Senussi, Padric M. Garden, Limor Cohen, Vishal Thapar, Matteo Ligorio, Kshitij S. Arora, Niyati Desai, Linda T. Nieman, Michael J. Raabe, Jasmin Joseph-Chazan, Chenyue Lu, Eric C. Tai, Kevin D. Vo, Emily E. Van Seventer, Richard Y. Ebright, Nova Xu, Antuan V. Tran, Stefanie Gerstberger, Annamaria Szabolcs, Charly R. Good, Katherine A. Alexander, Connie Wu, Martin S. Taylor, Christopher Jaicks, Katherine H. Xu, Chong Chu, Anupriya S. Kulkarni, Eunae You, Alexander Solovyov, Aparna R. Parikh, and Mihir Rajurkar

Abstract

Supplementary Data from Reverse Transcriptase Inhibition Disrupts Repeat Element Life Cycle in Colorectal Cancer

Published
2023

5. MAF file for CNVs from Real-time Genomic Characterization of Advanced Pancreatic Cancer to Enable Precision Medicine

Author

Brian M. Wolpin, Scott L. Carter, Ryan B. Corcoran, William C. Hahn, Jen Jen Yeh, Nikhil Wagle, David A. Tuveson, Paul B. Shyn, Jeffrey W. Miller, Robert J. Mayer, Matthew H. Kulke, Bruce E. Johnson, Jason L. Hornick, Gad Getz, Levi A. Garraway, Charles S. Fuchs, Matthew B. Yurgelun, Dean J. Welsch, Deborah Knoerzer, Richard B. Lanman, Rebecca J. Nagy, Stuart G. Silverman, Ewa Sicinska, Geoffrey I. Shapiro, Marvin Ryou, Douglas A. Rubinson, Michael H. Rosenthal, Kimberly Perez, Anuj K. Patel, Kimmie Ng, Janet E. Murphy, Jeffrey A. Meyerhardt, Nadine J. McCleary, Kunal Jajoo, Leona A. Doyle, James M. Cleary, Thomas Clancy, Kelly P. Burke, Joseph P. St. Pierre, Heather A. Shahzade, Emily E. Van Seventer, Brandon Nadres, Annacarolina Da Silva, Ana Babic, Nelly Oliver, Karla Helvie, Kristin Anderka, Lori Marini, Devin McCabe, Emma Reilly, Marisa W. Welch, Dorisanne Ragon, Lauren K. Brais, Jaegil Kim, Srivatsan Raghavan, Mehlika Hazar-Rethinam, Arezou A. Ghazani, Richard A. Moffitt, Nicholas D. Camarda, Jonathan A. Nowak, and Andrew J. Aguirre

Abstract

MAF file for copy number variations identified in the cohort

Published
2023

6. Supplementary Table 1 from Polyclonal Secondary FGFR2 Mutations Drive Acquired Resistance to FGFR Inhibition in Patients with FGFR2 Fusion–Positive Cholangiocarcinoma

Author

Andrew X. Zhu, Nabeel Bardeesy, Ryan B. Corcoran, Dejan Juric, Alberto Bardelli, Ralph Tiedt, Diana Graus Porta, Gad Getz, A. John Iafrate, James R. Stone, David P. Ryan, Pascal Furet, Christelle Stamm, Louise Barys, Barbara Schacher-Engstler, Sabrina Baltschukat, Joseph M. Gurski, Emily E. Van Seventer, Jiaoyuan Elisabeth Sun, Laura Henderson, Stephanie Reyes, Benedetta Mussolin, Avinash Kambadakone, Vikram Deshpande, Phuong Vu, Jochen K. Lennerz, Leanne G. Ahronian, Ignaty Leshchiner, Giulia Siravegna, Leah Y. Liu, Supriya K. Saha, and Lipika Goyal

Abstract

Complete Data for Genetic Analysis of ctDNA and Tumor Tissue for All Samples.

Published
2023

7. Supplementary Table S4 from Real-time Genomic Characterization of Advanced Pancreatic Cancer to Enable Precision Medicine

Author

Brian M. Wolpin, Scott L. Carter, Ryan B. Corcoran, William C. Hahn, Jen Jen Yeh, Nikhil Wagle, David A. Tuveson, Paul B. Shyn, Jeffrey W. Miller, Robert J. Mayer, Matthew H. Kulke, Bruce E. Johnson, Jason L. Hornick, Gad Getz, Levi A. Garraway, Charles S. Fuchs, Matthew B. Yurgelun, Dean J. Welsch, Deborah Knoerzer, Richard B. Lanman, Rebecca J. Nagy, Stuart G. Silverman, Ewa Sicinska, Geoffrey I. Shapiro, Marvin Ryou, Douglas A. Rubinson, Michael H. Rosenthal, Kimberly Perez, Anuj K. Patel, Kimmie Ng, Janet E. Murphy, Jeffrey A. Meyerhardt, Nadine J. McCleary, Kunal Jajoo, Leona A. Doyle, James M. Cleary, Thomas Clancy, Kelly P. Burke, Joseph P. St. Pierre, Heather A. Shahzade, Emily E. Van Seventer, Brandon Nadres, Annacarolina Da Silva, Ana Babic, Nelly Oliver, Karla Helvie, Kristin Anderka, Lori Marini, Devin McCabe, Emma Reilly, Marisa W. Welch, Dorisanne Ragon, Lauren K. Brais, Jaegil Kim, Srivatsan Raghavan, Mehlika Hazar-Rethinam, Arezou A. Ghazani, Richard A. Moffitt, Nicholas D. Camarda, Jonathan A. Nowak, and Andrew J. Aguirre

Abstract

Treatment history for patients enrolled on the PancSeq protocol.

Published
2023

8. Supplementary Table S3 from Real-time Genomic Characterization of Advanced Pancreatic Cancer to Enable Precision Medicine

Author

Brian M. Wolpin, Scott L. Carter, Ryan B. Corcoran, William C. Hahn, Jen Jen Yeh, Nikhil Wagle, David A. Tuveson, Paul B. Shyn, Jeffrey W. Miller, Robert J. Mayer, Matthew H. Kulke, Bruce E. Johnson, Jason L. Hornick, Gad Getz, Levi A. Garraway, Charles S. Fuchs, Matthew B. Yurgelun, Dean J. Welsch, Deborah Knoerzer, Richard B. Lanman, Rebecca J. Nagy, Stuart G. Silverman, Ewa Sicinska, Geoffrey I. Shapiro, Marvin Ryou, Douglas A. Rubinson, Michael H. Rosenthal, Kimberly Perez, Anuj K. Patel, Kimmie Ng, Janet E. Murphy, Jeffrey A. Meyerhardt, Nadine J. McCleary, Kunal Jajoo, Leona A. Doyle, James M. Cleary, Thomas Clancy, Kelly P. Burke, Joseph P. St. Pierre, Heather A. Shahzade, Emily E. Van Seventer, Brandon Nadres, Annacarolina Da Silva, Ana Babic, Nelly Oliver, Karla Helvie, Kristin Anderka, Lori Marini, Devin McCabe, Emma Reilly, Marisa W. Welch, Dorisanne Ragon, Lauren K. Brais, Jaegil Kim, Srivatsan Raghavan, Mehlika Hazar-Rethinam, Arezou A. Ghazani, Richard A. Moffitt, Nicholas D. Camarda, Jonathan A. Nowak, and Andrew J. Aguirre

Abstract

PancSeq protocol gene list for CLIA-certified somatic and germline analysis from whole exome sequencing data.

Published
2023

9. Supplementary Figures from Real-time Genomic Characterization of Advanced Pancreatic Cancer to Enable Precision Medicine

Author

Brian M. Wolpin, Scott L. Carter, Ryan B. Corcoran, William C. Hahn, Jen Jen Yeh, Nikhil Wagle, David A. Tuveson, Paul B. Shyn, Jeffrey W. Miller, Robert J. Mayer, Matthew H. Kulke, Bruce E. Johnson, Jason L. Hornick, Gad Getz, Levi A. Garraway, Charles S. Fuchs, Matthew B. Yurgelun, Dean J. Welsch, Deborah Knoerzer, Richard B. Lanman, Rebecca J. Nagy, Stuart G. Silverman, Ewa Sicinska, Geoffrey I. Shapiro, Marvin Ryou, Douglas A. Rubinson, Michael H. Rosenthal, Kimberly Perez, Anuj K. Patel, Kimmie Ng, Janet E. Murphy, Jeffrey A. Meyerhardt, Nadine J. McCleary, Kunal Jajoo, Leona A. Doyle, James M. Cleary, Thomas Clancy, Kelly P. Burke, Joseph P. St. Pierre, Heather A. Shahzade, Emily E. Van Seventer, Brandon Nadres, Annacarolina Da Silva, Ana Babic, Nelly Oliver, Karla Helvie, Kristin Anderka, Lori Marini, Devin McCabe, Emma Reilly, Marisa W. Welch, Dorisanne Ragon, Lauren K. Brais, Jaegil Kim, Srivatsan Raghavan, Mehlika Hazar-Rethinam, Arezou A. Ghazani, Richard A. Moffitt, Nicholas D. Camarda, Jonathan A. Nowak, and Andrew J. Aguirre

Abstract

Supplementary Figure S1: Overview of workflow and data generation. Supplementary Figure S2: Analysis of neoplastic cellularity. Supplementary Figure S3: Recurrent copy number alterations. Supplementary Figure S4: Mutational signature analysis. Supplementary Figure S5: Analysis of PDAC gene expression signatures. Supplementary Figure S6: Clinically relevant alterations in the cohort.

Published
2023

10. Table S1 from TAS-120 Overcomes Resistance to ATP-Competitive FGFR Inhibitors in Patients with FGFR2 Fusion–Positive Intrahepatic Cholangiocarcinoma

Author

Nabeel Bardeesy, Ryan B. Corcoran, Andrew X. Zhu, Dejan Juric, Gad Getz, Hiroshi Hirai, David T. Ting, Cyril H. Benes, William C. Hahn, A. John Iafrate, Alberto Bardelli, Robin K. Kelley, Rona Yaeger, James J. Harding, Vikram Deshpande, Kenneth K. Tanabe, Cristina R. Ferrone, Janet E. Murphy, Emily E. Van Seventer, Islam Baiev, Isobel J. Fetter, Ipsita Dey-Guha, Heather A. Shahzade, Brandon Nadres, Sachie Otsuki, Takeshi Sagara, Stephanie Reyes, Ron Arellano, Raul N. Uppot, Supriya K. Saha, Krushna C. Patra, Phuong Vu, Raymond W.S. Ng, Giulia Siravegna, Liudmila Elagina, Ignaty Leschiner, Srivatsan Raghavan, Jochen K. Lennerz, Ferran Fece de la Cruz, Leah Y. Liu, Lei Shi, and Lipika Goyal

Abstract

Primer sequences

Published
2023

11. Supplementary Figures 1 - 6 from Polyclonal Secondary FGFR2 Mutations Drive Acquired Resistance to FGFR Inhibition in Patients with FGFR2 Fusion–Positive Cholangiocarcinoma

Author

Andrew X. Zhu, Nabeel Bardeesy, Ryan B. Corcoran, Dejan Juric, Alberto Bardelli, Ralph Tiedt, Diana Graus Porta, Gad Getz, A. John Iafrate, James R. Stone, David P. Ryan, Pascal Furet, Christelle Stamm, Louise Barys, Barbara Schacher-Engstler, Sabrina Baltschukat, Joseph M. Gurski, Emily E. Van Seventer, Jiaoyuan Elisabeth Sun, Laura Henderson, Stephanie Reyes, Benedetta Mussolin, Avinash Kambadakone, Vikram Deshpande, Phuong Vu, Jochen K. Lennerz, Leanne G. Ahronian, Ignaty Leshchiner, Giulia Siravegna, Leah Y. Liu, Supriya K. Saha, and Lipika Goyal

Abstract

Supplementary Figure S1. Confirmation of secondary point mutation in FGFR2-ZMYM4 allele. Supplementary Figure S2. Homology between FGFR2 and FGFR3 proteins. Supplementary Figure S3. FGFR2-OPTN fusion detected in all autopsy lesions. Supplementary Figure S4. FoundationOne analysis of autopsy lesions. Supplementary Figure S5. PTEN loss of heterozygosity (LOH) identified in Patient #2. Supplementary Figure S6. Mutational analysis of original resection specimen from Patient #2.

Published
2023

12. Supplementary Experimental Methods from Real-time Genomic Characterization of Advanced Pancreatic Cancer to Enable Precision Medicine

Author

Brian M. Wolpin, Scott L. Carter, Ryan B. Corcoran, William C. Hahn, Jen Jen Yeh, Nikhil Wagle, David A. Tuveson, Paul B. Shyn, Jeffrey W. Miller, Robert J. Mayer, Matthew H. Kulke, Bruce E. Johnson, Jason L. Hornick, Gad Getz, Levi A. Garraway, Charles S. Fuchs, Matthew B. Yurgelun, Dean J. Welsch, Deborah Knoerzer, Richard B. Lanman, Rebecca J. Nagy, Stuart G. Silverman, Ewa Sicinska, Geoffrey I. Shapiro, Marvin Ryou, Douglas A. Rubinson, Michael H. Rosenthal, Kimberly Perez, Anuj K. Patel, Kimmie Ng, Janet E. Murphy, Jeffrey A. Meyerhardt, Nadine J. McCleary, Kunal Jajoo, Leona A. Doyle, James M. Cleary, Thomas Clancy, Kelly P. Burke, Joseph P. St. Pierre, Heather A. Shahzade, Emily E. Van Seventer, Brandon Nadres, Annacarolina Da Silva, Ana Babic, Nelly Oliver, Karla Helvie, Kristin Anderka, Lori Marini, Devin McCabe, Emma Reilly, Marisa W. Welch, Dorisanne Ragon, Lauren K. Brais, Jaegil Kim, Srivatsan Raghavan, Mehlika Hazar-Rethinam, Arezou A. Ghazani, Richard A. Moffitt, Nicholas D. Camarda, Jonathan A. Nowak, and Andrew J. Aguirre

Abstract

Supplementary Experimental Methods

Published
2023

13. MAF file for mutations from Real-time Genomic Characterization of Advanced Pancreatic Cancer to Enable Precision Medicine

Author

Brian M. Wolpin, Scott L. Carter, Ryan B. Corcoran, William C. Hahn, Jen Jen Yeh, Nikhil Wagle, David A. Tuveson, Paul B. Shyn, Jeffrey W. Miller, Robert J. Mayer, Matthew H. Kulke, Bruce E. Johnson, Jason L. Hornick, Gad Getz, Levi A. Garraway, Charles S. Fuchs, Matthew B. Yurgelun, Dean J. Welsch, Deborah Knoerzer, Richard B. Lanman, Rebecca J. Nagy, Stuart G. Silverman, Ewa Sicinska, Geoffrey I. Shapiro, Marvin Ryou, Douglas A. Rubinson, Michael H. Rosenthal, Kimberly Perez, Anuj K. Patel, Kimmie Ng, Janet E. Murphy, Jeffrey A. Meyerhardt, Nadine J. McCleary, Kunal Jajoo, Leona A. Doyle, James M. Cleary, Thomas Clancy, Kelly P. Burke, Joseph P. St. Pierre, Heather A. Shahzade, Emily E. Van Seventer, Brandon Nadres, Annacarolina Da Silva, Ana Babic, Nelly Oliver, Karla Helvie, Kristin Anderka, Lori Marini, Devin McCabe, Emma Reilly, Marisa W. Welch, Dorisanne Ragon, Lauren K. Brais, Jaegil Kim, Srivatsan Raghavan, Mehlika Hazar-Rethinam, Arezou A. Ghazani, Richard A. Moffitt, Nicholas D. Camarda, Jonathan A. Nowak, and Andrew J. Aguirre

Abstract

MAF file for mutations identified in the cohort

Published
2023

14. Figure S1 and S2 from TAS-120 Overcomes Resistance to ATP-Competitive FGFR Inhibitors in Patients with FGFR2 Fusion–Positive Intrahepatic Cholangiocarcinoma

Author

Nabeel Bardeesy, Ryan B. Corcoran, Andrew X. Zhu, Dejan Juric, Gad Getz, Hiroshi Hirai, David T. Ting, Cyril H. Benes, William C. Hahn, A. John Iafrate, Alberto Bardelli, Robin K. Kelley, Rona Yaeger, James J. Harding, Vikram Deshpande, Kenneth K. Tanabe, Cristina R. Ferrone, Janet E. Murphy, Emily E. Van Seventer, Islam Baiev, Isobel J. Fetter, Ipsita Dey-Guha, Heather A. Shahzade, Brandon Nadres, Sachie Otsuki, Takeshi Sagara, Stephanie Reyes, Ron Arellano, Raul N. Uppot, Supriya K. Saha, Krushna C. Patra, Phuong Vu, Raymond W.S. Ng, Giulia Siravegna, Liudmila Elagina, Ignaty Leschiner, Srivatsan Raghavan, Jochen K. Lennerz, Ferran Fece de la Cruz, Leah Y. Liu, Lei Shi, and Lipika Goyal

Abstract

Supplementary Figures and Legends

Published
2023

15. Data from TAS-120 Overcomes Resistance to ATP-Competitive FGFR Inhibitors in Patients with FGFR2 Fusion–Positive Intrahepatic Cholangiocarcinoma

Author

Nabeel Bardeesy, Ryan B. Corcoran, Andrew X. Zhu, Dejan Juric, Gad Getz, Hiroshi Hirai, David T. Ting, Cyril H. Benes, William C. Hahn, A. John Iafrate, Alberto Bardelli, Robin K. Kelley, Rona Yaeger, James J. Harding, Vikram Deshpande, Kenneth K. Tanabe, Cristina R. Ferrone, Janet E. Murphy, Emily E. Van Seventer, Islam Baiev, Isobel J. Fetter, Ipsita Dey-Guha, Heather A. Shahzade, Brandon Nadres, Sachie Otsuki, Takeshi Sagara, Stephanie Reyes, Ron Arellano, Raul N. Uppot, Supriya K. Saha, Krushna C. Patra, Phuong Vu, Raymond W.S. Ng, Giulia Siravegna, Liudmila Elagina, Ignaty Leschiner, Srivatsan Raghavan, Jochen K. Lennerz, Ferran Fece de la Cruz, Leah Y. Liu, Lei Shi, and Lipika Goyal

Abstract

ATP-competitive fibroblast growth factor receptor (FGFR) kinase inhibitors, including BGJ398 and Debio 1347, show antitumor activity in patients with intrahepatic cholangiocarcinoma (ICC) harboring activating FGFR2 gene fusions. Unfortunately, acquired resistance develops and is often associated with the emergence of secondary FGFR2 kinase domain mutations. Here, we report that the irreversible pan-FGFR inhibitor TAS-120 demonstrated efficacy in 4 patients with FGFR2 fusion–positive ICC who developed resistance to BGJ398 or Debio 1347. Examination of serial biopsies, circulating tumor DNA (ctDNA), and patient-derived ICC cells revealed that TAS-120 was active against multiple FGFR2 mutations conferring resistance to BGJ398 or Debio 1347. Functional assessment and modeling the clonal outgrowth of individual resistance mutations from polyclonal cell pools mirrored the resistance profiles observed clinically for each inhibitor. Our findings suggest that strategic sequencing of FGFR inhibitors, guided by serial biopsy and ctDNA analysis, may prolong the duration of benefit from FGFR inhibition in patients with FGFR2 fusion–positive ICC.Significance:ATP-competitive FGFR inhibitors (BGJ398, Debio 1347) show efficacy in FGFR2-altered ICC; however, acquired FGFR2 kinase domain mutations cause drug resistance and tumor progression. We demonstrate that the irreversible FGFR inhibitor TAS-120 provides clinical benefit in patients with resistance to BGJ398 or Debio 1347 and overcomes several FGFR2 mutations in ICC models.This article is highlighted in the In This Issue feature, p. 983

Published
2023

16. Supplementary Material from Convergent Therapeutic Strategies to Overcome the Heterogeneity of Acquired Resistance in BRAFV600E Colorectal Cancer

Author

Ryan B. Corcoran, Eliezer M. Van Allen, A. John Iafrate, Dora Dias-Santagata, Nicholas A. Jessop, Joseph M. Gurski, Catriona B. Hong, Brandon Nadres, Emily E. Van Seventer, Theodore S. Hong, Janet E. Murphy, Jason E. Faris, Eunice L. Kwak, Jeffrey W. Clark, Jill N. Allen, Aparna R. Parikh, Lifeng Chen, Heather A. Shahzade, Leanne G. Ahronian, David Liu, G. Celine Han, Marianna Kleyman, and Mehlika Hazar-Rethinam

Abstract

Supplementary Figures, Tables, Methods

Published
2023

17. Supplementary Table S2 from Real-time Genomic Characterization of Advanced Pancreatic Cancer to Enable Precision Medicine

Author

Brian M. Wolpin, Scott L. Carter, Ryan B. Corcoran, William C. Hahn, Jen Jen Yeh, Nikhil Wagle, David A. Tuveson, Paul B. Shyn, Jeffrey W. Miller, Robert J. Mayer, Matthew H. Kulke, Bruce E. Johnson, Jason L. Hornick, Gad Getz, Levi A. Garraway, Charles S. Fuchs, Matthew B. Yurgelun, Dean J. Welsch, Deborah Knoerzer, Richard B. Lanman, Rebecca J. Nagy, Stuart G. Silverman, Ewa Sicinska, Geoffrey I. Shapiro, Marvin Ryou, Douglas A. Rubinson, Michael H. Rosenthal, Kimberly Perez, Anuj K. Patel, Kimmie Ng, Janet E. Murphy, Jeffrey A. Meyerhardt, Nadine J. McCleary, Kunal Jajoo, Leona A. Doyle, James M. Cleary, Thomas Clancy, Kelly P. Burke, Joseph P. St. Pierre, Heather A. Shahzade, Emily E. Van Seventer, Brandon Nadres, Annacarolina Da Silva, Ana Babic, Nelly Oliver, Karla Helvie, Kristin Anderka, Lori Marini, Devin McCabe, Emma Reilly, Marisa W. Welch, Dorisanne Ragon, Lauren K. Brais, Jaegil Kim, Srivatsan Raghavan, Mehlika Hazar-Rethinam, Arezou A. Ghazani, Richard A. Moffitt, Nicholas D. Camarda, Jonathan A. Nowak, and Andrew J. Aguirre

Abstract

Characteristics of biopsies obtained on PancSeq protocol.

Published
2023

18. Supplementary Figures from Minimal Residual Disease Detection using a Plasma-only Circulating Tumor DNA Assay in Patients with Colorectal Cancer

Author

Ryan B. Corcoran, Genevieve M. Boland, AmirAli Talasaz, Victoria M. Raymond, James C. Cusack, Rocco Ricciardi, David Berger, Hiroko Kunitake, Motaz Qadan, Cristina R. Ferrone, Liliana Bordeianou, Theodore S. Hong, Jennifer Y. Wo, Colin D. Weekes, David P. Ryan, Eric J. Roeland, Ryan D. Nipp, Samuel J. Klempner, Lipika Goyal, Bruce J. Giantonio, Joseph W. Franses, Jon S. Dubois, Jeffrey W. Clark, Lawrence S. Blaszkowsky, Jill N. Allen, Heather A. Shahzade, Isobel J. Fetter, Yojan S. Shah, Islam Baiev, Joy Jarnagin, Nihaarika Sharma, John H. Carmichael, Susannah Phillips, Benchun Miao, Kathryn D. Fosbenner, Madeleine G. Fish, Katie Kanter, Yupeng He, Ariel Jaimovich, Anna V. Hartwig, Giulia Siravegna, Emily E. Van Seventer, and Aparna R. Parikh

Abstract

Supplementary Figures

Published
2023

19. Data from Serial ctDNA Monitoring to Predict Response to Systemic Therapy in Metastatic Gastrointestinal Cancers

Author

Ryan B. Corcoran, Jeffrey W. Clark, Nora Horick, Giulia Siravegna, Theodore S. Hong, Jochen K. Lennerz, A. John Iafrate, Dora Dias-Santagata, Andrew X. Zhu, Jennifer Y. Wo, Colin D. Weekes, Eric Roeland, Ryan D. Nipp, Lipika Goyal, Bruce Giantonio, David P. Ryan, Lawrence S. Blaszkowsky, Jill N. Allen, Heather A. Shahzade, Brandon Nadres, Kathryn Fosbenner, Bezaye Teshome, Madeleine G. Fish, Ashraf Thabet, Isobel J. Fetter, Emily E. Van Seventer, Katie Kanter, Jaime L. Schneider, Amikasra Mojtahed, and Aparna R. Parikh

Abstract

Purpose:ctDNA offers a promising, noninvasive approach to monitor therapeutic efficacy in real-time. We explored whether the quantitative percent change in ctDNA early after therapy initiation can predict treatment response and progression-free survival (PFS) in patients with metastatic gastrointestinal cancer.Experimental Design:A total of 138 patients with metastatic gastrointestinal cancers and tumor profiling by next-generation sequencing had serial blood draws pretreatment and at scheduled intervals during therapy. ctDNA was assessed using individualized droplet digital PCR measuring the mutant allele fraction in plasma of mutations identified in tumor biopsies. ctDNA changes were correlated with tumor markers and radiographic response.Results:A total of 138 patients enrolled. A total of 101 patients were evaluable for ctDNA and 68 for tumor markers at 4 weeks. Percent change of ctDNA by 4 weeks predicted partial response (PR, P < 0.0001) and clinical benefit [CB: PR and stable disease (SD), P < 0.0001]. ctDNA decreased by 98% (median) and >30% for all PR patients. ctDNA change at 8 weeks, but not 2 weeks, also predicted CB (P < 0.0001). Four-week change in tumor markers also predicted response (P = 0.0026) and CB (P = 0.022). However, at a clinically relevant specificity threshold of 90%, 4-week ctDNA change more effectively predicted CB versus tumor markers, with a sensitivity of 60% versus 24%, respectively (P = 0.0109). Patients whose 4-week ctDNA decreased beyond this threshold (≥30% decrease) had a median PFS of 175 days versus 59.5 days (HR, 3.29; 95% CI, 1.55–7.00; P < 0.0001).Conclusions:Serial ctDNA monitoring may provide early indication of response to systemic therapy in patients with metastatic gastrointestinal cancer prior to radiographic assessments and may outperform standard tumor markers, warranting further evaluation.

Published
2023

20. Supplementary Data from Serial ctDNA Monitoring to Predict Response to Systemic Therapy in Metastatic Gastrointestinal Cancers

Author

Ryan B. Corcoran, Jeffrey W. Clark, Nora Horick, Giulia Siravegna, Theodore S. Hong, Jochen K. Lennerz, A. John Iafrate, Dora Dias-Santagata, Andrew X. Zhu, Jennifer Y. Wo, Colin D. Weekes, Eric Roeland, Ryan D. Nipp, Lipika Goyal, Bruce Giantonio, David P. Ryan, Lawrence S. Blaszkowsky, Jill N. Allen, Heather A. Shahzade, Brandon Nadres, Kathryn Fosbenner, Bezaye Teshome, Madeleine G. Fish, Ashraf Thabet, Isobel J. Fetter, Emily E. Van Seventer, Katie Kanter, Jaime L. Schneider, Amikasra Mojtahed, and Aparna R. Parikh

Abstract

Supplementary Figures

Published
2023

22. Data from Minimal Residual Disease Detection using a Plasma-only Circulating Tumor DNA Assay in Patients with Colorectal Cancer

Author

Ryan B. Corcoran, Genevieve M. Boland, AmirAli Talasaz, Victoria M. Raymond, James C. Cusack, Rocco Ricciardi, David Berger, Hiroko Kunitake, Motaz Qadan, Cristina R. Ferrone, Liliana Bordeianou, Theodore S. Hong, Jennifer Y. Wo, Colin D. Weekes, David P. Ryan, Eric J. Roeland, Ryan D. Nipp, Samuel J. Klempner, Lipika Goyal, Bruce J. Giantonio, Joseph W. Franses, Jon S. Dubois, Jeffrey W. Clark, Lawrence S. Blaszkowsky, Jill N. Allen, Heather A. Shahzade, Isobel J. Fetter, Yojan S. Shah, Islam Baiev, Joy Jarnagin, Nihaarika Sharma, John H. Carmichael, Susannah Phillips, Benchun Miao, Kathryn D. Fosbenner, Madeleine G. Fish, Katie Kanter, Yupeng He, Ariel Jaimovich, Anna V. Hartwig, Giulia Siravegna, Emily E. Van Seventer, and Aparna R. Parikh

Abstract

Purpose:Detection of persistent circulating tumor DNA (ctDNA) after curative-intent surgery can identify patients with minimal residual disease (MRD) who will ultimately recur. Most ctDNA MRD assays require tumor sequencing to identify tumor-derived mutations to facilitate ctDNA detection, requiring tumor and blood. We evaluated a plasma-only ctDNA assay integrating genomic and epigenomic cancer signatures to enable tumor-uninformed MRD detection.Experimental Design:A total of 252 prospective serial plasma specimens from 103 patients with colorectal cancer undergoing curative-intent surgery were analyzed and correlated with recurrence.Results:Of 103 patients, 84 [stage I (9.5%), II (23.8%), III (47.6%), IV (19%)] had evaluable plasma drawn after completion of definitive therapy, defined as surgery only (n = 39) or completion of adjuvant therapy (n = 45). In “landmark” plasma drawn 1-month (median, 31.5 days) after definitive therapy and >1 year follow-up, 15 patients had detectable ctDNA, and all 15 recurred [positive predictive value (PPV), 100%; HR, 11.28 (P < 0.0001)]. Of 49 patients without detectable ctDNA at the landmark timepoint, 12 (24.5%) recurred. Landmark recurrence sensitivity and specificity were 55.6% and 100%. Incorporating serial longitudinal and surveillance (drawn within 4 months of recurrence) samples, sensitivity improved to 69% and 91%. Integrating epigenomic signatures increased sensitivity by 25%–36% versus genomic alterations alone. Notably, standard serum carcinoembryonic antigen levels did not predict recurrence [HR, 1.84 (P = 0.18); PPV = 53.9%].Conclusions:Plasma-only MRD detection demonstrated favorable sensitivity and specificity for recurrence, comparable with tumor-informed approaches. Integrating analysis of epigenomic and genomic alterations enhanced sensitivity. These findings support the potential clinical utility of plasma-only ctDNA MRD detection.See related commentary by Bent and Kopetz, p. 5449

Published
2023

23. Supplementary Table S2 from Serial ctDNA Monitoring to Predict Response to Systemic Therapy in Metastatic Gastrointestinal Cancers

Author

Ryan B. Corcoran, Jeffrey W. Clark, Nora Horick, Giulia Siravegna, Theodore S. Hong, Jochen K. Lennerz, A. John Iafrate, Dora Dias-Santagata, Andrew X. Zhu, Jennifer Y. Wo, Colin D. Weekes, Eric Roeland, Ryan D. Nipp, Lipika Goyal, Bruce Giantonio, David P. Ryan, Lawrence S. Blaszkowsky, Jill N. Allen, Heather A. Shahzade, Brandon Nadres, Kathryn Fosbenner, Bezaye Teshome, Madeleine G. Fish, Ashraf Thabet, Isobel J. Fetter, Emily E. Van Seventer, Katie Kanter, Jaime L. Schneider, Amikasra Mojtahed, and Aparna R. Parikh

Abstract

Supplementary Table S2

Published
2023

25. Supplementary Table S4 from Serial ctDNA Monitoring to Predict Response to Systemic Therapy in Metastatic Gastrointestinal Cancers

Author

Ryan B. Corcoran, Jeffrey W. Clark, Nora Horick, Giulia Siravegna, Theodore S. Hong, Jochen K. Lennerz, A. John Iafrate, Dora Dias-Santagata, Andrew X. Zhu, Jennifer Y. Wo, Colin D. Weekes, Eric Roeland, Ryan D. Nipp, Lipika Goyal, Bruce Giantonio, David P. Ryan, Lawrence S. Blaszkowsky, Jill N. Allen, Heather A. Shahzade, Brandon Nadres, Kathryn Fosbenner, Bezaye Teshome, Madeleine G. Fish, Ashraf Thabet, Isobel J. Fetter, Emily E. Van Seventer, Katie Kanter, Jaime L. Schneider, Amikasra Mojtahed, and Aparna R. Parikh

Abstract

Supplementary Table S4

Published
2023

26. Supplementary Methods from Serial ctDNA Monitoring to Predict Response to Systemic Therapy in Metastatic Gastrointestinal Cancers

Author

Ryan B. Corcoran, Jeffrey W. Clark, Nora Horick, Giulia Siravegna, Theodore S. Hong, Jochen K. Lennerz, A. John Iafrate, Dora Dias-Santagata, Andrew X. Zhu, Jennifer Y. Wo, Colin D. Weekes, Eric Roeland, Ryan D. Nipp, Lipika Goyal, Bruce Giantonio, David P. Ryan, Lawrence S. Blaszkowsky, Jill N. Allen, Heather A. Shahzade, Brandon Nadres, Kathryn Fosbenner, Bezaye Teshome, Madeleine G. Fish, Ashraf Thabet, Isobel J. Fetter, Emily E. Van Seventer, Katie Kanter, Jaime L. Schneider, Amikasra Mojtahed, and Aparna R. Parikh

Abstract

Supplementary Methods

Published
2023

28. Supplementary Table S1 from Serial ctDNA Monitoring to Predict Response to Systemic Therapy in Metastatic Gastrointestinal Cancers

Author

Ryan B. Corcoran, Jeffrey W. Clark, Nora Horick, Giulia Siravegna, Theodore S. Hong, Jochen K. Lennerz, A. John Iafrate, Dora Dias-Santagata, Andrew X. Zhu, Jennifer Y. Wo, Colin D. Weekes, Eric Roeland, Ryan D. Nipp, Lipika Goyal, Bruce Giantonio, David P. Ryan, Lawrence S. Blaszkowsky, Jill N. Allen, Heather A. Shahzade, Brandon Nadres, Kathryn Fosbenner, Bezaye Teshome, Madeleine G. Fish, Ashraf Thabet, Isobel J. Fetter, Emily E. Van Seventer, Katie Kanter, Jaime L. Schneider, Amikasra Mojtahed, and Aparna R. Parikh

Abstract

Supplementary Table S1

Published
2023

29. Supplementary Tables from Minimal Residual Disease Detection using a Plasma-only Circulating Tumor DNA Assay in Patients with Colorectal Cancer

Author

Ryan B. Corcoran, Genevieve M. Boland, AmirAli Talasaz, Victoria M. Raymond, James C. Cusack, Rocco Ricciardi, David Berger, Hiroko Kunitake, Motaz Qadan, Cristina R. Ferrone, Liliana Bordeianou, Theodore S. Hong, Jennifer Y. Wo, Colin D. Weekes, David P. Ryan, Eric J. Roeland, Ryan D. Nipp, Samuel J. Klempner, Lipika Goyal, Bruce J. Giantonio, Joseph W. Franses, Jon S. Dubois, Jeffrey W. Clark, Lawrence S. Blaszkowsky, Jill N. Allen, Heather A. Shahzade, Isobel J. Fetter, Yojan S. Shah, Islam Baiev, Joy Jarnagin, Nihaarika Sharma, John H. Carmichael, Susannah Phillips, Benchun Miao, Kathryn D. Fosbenner, Madeleine G. Fish, Katie Kanter, Yupeng He, Ariel Jaimovich, Anna V. Hartwig, Giulia Siravegna, Emily E. Van Seventer, and Aparna R. Parikh

Abstract

Supplementary Tables

Published
2023

30. Data from Integrative Molecular Characterization of Resistance to Neoadjuvant Chemoradiation in Rectal Cancer

Author

Eliezer M. Van Allen, Theodore S. Hong, Ryan B. Corcoran, Henning Willers, Scott L. Carter, Jennifer Y. Wo, Adam Tracy, Emily E. Van Seventer, Stephanie A. Wankowicz, Brendan Reardon, David Liu, Claire A. Margolis, Jochen K. Lennerz, and Sophia C. Kamran

Abstract

Purpose:Molecular properties associated with complete response or acquired resistance to concurrent chemotherapy and radiotherapy (CRT) are incompletely characterized.Experimental Design: We performed integrated whole-exome/transcriptome sequencing and immune infiltrate analysis on rectal adenocarcinoma tumors prior to neoadjuvant CRT (pre-CRT) and at time of resection (post-CRT) in 17 patients [8 complete/partial responders, 9 nonresponders (NR)].Results:CRT was not associated with increased tumor mutational burden or neoantigen load and did not alter the distribution of established somatic tumor mutations in rectal cancer. Concurrent KRAS/TP53 mutations (KP) associated with NR tumors and were enriched for an epithelial–mesenchymal transition transcriptional program. Furthermore, NR was associated with reduced CD4/CD8 T-cell infiltrates and a post-CRT M2 macrophage phenotype. Absence of any local tumor recurrences, KP/NR status predicted worse progression-free survival, suggesting that local immune escape during or after CRT with specific genomic features contributes to distant progression.Conclusions:Overall, while CRT did not impact genomic profiles, CRT impacted the tumor immune microenvironment, particularly in resistant cases.

Published
2023

31. Reverse Transcriptase Inhibition Disrupts Repeat Element Life Cycle in Colorectal Cancer

Author

Mihir Rajurkar, Aparna R. Parikh, Alexander Solovyov, Eunae You, Anupriya S. Kulkarni, Chong Chu, Katherine H. Xu, Christopher Jaicks, Martin S. Taylor, Connie Wu, Katherine A. Alexander, Charly R. Good, Annamaria Szabolcs, Stefanie Gerstberger, Antuan V. Tran, Nova Xu, Richard Y. Ebright, Emily E. Van Seventer, Kevin D. Vo, Eric C. Tai, Chenyue Lu, Jasmin Joseph-Chazan, Michael J. Raabe, Linda T. Nieman, Niyati Desai, Kshitij S. Arora, Matteo Ligorio, Vishal Thapar, Limor Cohen, Padric M. Garden, Yasmeen Senussi, Hui Zheng, Jill N. Allen, Lawrence S. Blaszkowsky, Jeffrey W. Clark, Lipika Goyal, Jennifer Y. Wo, David P. Ryan, Ryan B. Corcoran, Vikram Deshpande, Miguel N. Rivera, Martin J. Aryee, Theodore S. Hong, Shelley L. Berger, David R. Walt, Kathleen H. Burns, Peter J. Park, Benjamin D. Greenbaum, and David T. Ting

Subjects
Life Cycle Stages, Oncology, Lamivudine, Animals, Humans, RNA, RNA-Directed DNA Polymerase, DNA, Interferons, Tumor Suppressor Protein p53, Colorectal Neoplasms, Antiviral Agents, Article
Abstract

Altered RNA expression of repetitive sequences and retrotransposition are frequently seen in colorectal cancer, implicating a functional importance of repeat activity in cancer progression. We show the nucleoside reverse transcriptase inhibitor 3TC targets activities of these repeat elements in colorectal cancer preclinical models with a preferential effect in p53-mutant cell lines linked with direct binding of p53 to repeat elements. We translate these findings to a human phase II trial of single-agent 3TC treatment in metastatic colorectal cancer with demonstration of clinical benefit in 9 of 32 patients. Analysis of 3TC effects on colorectal cancer tumorspheres demonstrates accumulation of immunogenic RNA:DNA hybrids linked with induction of interferon response genes and DNA damage response. Epigenetic and DNA-damaging agents induce repeat RNAs and have enhanced cytotoxicity with 3TC. These findings identify a vulnerability in colorectal cancer by targeting the viral mimicry of repeat elements.Significance:Colorectal cancers express abundant repeat elements that have a viral-like life cycle that can be therapeutically targeted with nucleoside reverse transcriptase inhibitors (NRTI) commonly used for viral diseases. NRTIs induce DNA damage and interferon response that provide a new anticancer therapeutic strategy.This article is highlighted in the In This Issue feature, p. 1397

Published
2022

32. Methylated Septin9 (mSEPT9): A Promising Blood-Based Biomarker for the Detection and Screening of Early-Onset Colorectal Cancer

Author

Holli A. Loomans-Kropp, Yurong Song, Manish Gala, Aparna R. Parikh, Emily E. Van Seventer, Rocio Alvarez, Megan P. Hitchins, Robert H. Shoemaker, and Asad Umar

Subjects
Article
Abstract

Early-onset colorectal cancer (EOCRC), defined as a diagnosis under age 50, is an emerging public health burden. As many of these individuals fall outside of screening guidelines, the development of a minimally invasive, accurate screening modality for this population is warranted. We evaluated the FDA-approved blood-based biomarker methylated Septin9 (mSEPT9) test as screening tool for EOCRC. EOCRC plasma, healthy plasma, and serum-free conditioned media from cancer cell lines were collected. Cell-free DNA (cfDNA) was isolated and bisulfite converted for use in the assay. mSEPT9 and ACTB measured using Epi proColon V2.0. EOCRC plasma was collected at Massachusetts General Hospital (2005–2019) and controls were collected at the NIH and by ZenBio Inc. (prior to 2019). Twenty-seven EOCRC cases, 48 healthy controls Significance: mSEPT9 may be a novel biomarker for the detection of early-onset colorectal cancer, as it demonstrated high sensitivity and specificity in our study.

Published
2022

33. Care Patterns and Overall Survival in Patients With Early-Onset Metastatic Colorectal Cancer

Author

Janet E. Murphy, David P. Ryan, Samuel J. Klempner, Joseph W. Franses, Madeleine Fish, Aparna Raj Parikh, Jon Dubois, Emily E. Van Seventer, Jill N. Allen, Theodore S. Hong, Katie Kanter, Lawrence S. Blaszkowsky, Eric Roeland, Jennifer Y. Wo, Jeffrey W. Clark, Bruce J. Giantonio, Colin D. Weekes, Ryan B. Corcoran, Ryan D. Nipp, Lipika Goyal, Nora Horick, and Gianluca Mauri

Subjects
Adult, Oncology, medicine.medical_specialty, Colorectal cancer, MEDLINE, 03 medical and health sciences, 0302 clinical medicine, Text mining, Internal medicine, medicine, Overall survival, Humans, In patient, Biological Specimen Banks, 030304 developmental biology, Early onset, 0303 health sciences, Rectal Neoplasms, Oncology (nursing), business.industry, Incidence, Health Policy, Incidence (epidemiology), Middle Aged, Prognosis, medicine.disease, 030220 oncology & carcinogenesis, Colorectal Neoplasms, business
Abstract

PURPOSE: Colorectal cancer (CRC) incidence in patients younger than 50 years of age, commonly defined as early-onset (EO-CRC), is rising. EO-CRC often presents with distinct clinicopathologic features. However, data on prognosis are conflicting and outcomes with modern treatment approaches for metastatic disease are still limited. MATERIALS AND METHODS: We prospectively enrolled patients with metastatic CRC (mCRC) to a biobanking and clinical data collection protocol from 2014 to 2018. We grouped the cohort based on age at initial diagnosis: < 40 years, 40-49 years, and ≥ 50 years. We used regression models to examine associations among age at initial diagnosis, treatments, clinicopathologic features, and survival. RESULTS: We identified 466 patients with mCRC (45 [10%] age < 40 years, 109 [23%] age 40-49 years, and 312 [67%] age ≥ 50 years). Patients < 40 years of age were more likely to have received multiple metastatic resections (odds ratio [OR], 3.533; P = .0066) than their older counterparts. Patients with EO-CRC were more likely to receive triplet therapy than patients > 50 years of age (age < 40 years: OR, 6.738; P = .0002; age 40-49 years: OR, 2.949; P = .0166). Patients 40-49 years of age were more likely to have received anti-EGFR therapy (OR, 2.633; P = .0016). Despite differences in care patterns, age did not predict overall survival. CONCLUSION: Despite patients with EO-CRC receiving more intensive treatments, survival was similar to the older counterpart. However, EO-CRC had clinical and molecular features associated with worse prognoses. Improved biologic understanding is needed to optimize clinical management of EO-CRC. The cost-benefit ratio of exposing patients with EO-CRC to more intensive treatments has to be carefully evaluated.

Published
2021

34. Results and Molecular Correlates from a Pilot Study of Neoadjuvant Induction FOLFIRINOX Followed by Chemoradiation and Surgery for Gastroesophageal Adenocarcinomas

Author

Emily E. Van Seventer, Jill N. Allen, David P. Ryan, Michael Lanuti, Florence K. Keane, Jeffrey W. Clark, Theodore S. Hong, Ryan B. Corcoran, Mari Mino-Kenudson, Aparna Raj Parikh, Christopher R. Morse, Lorraine C. Drapek, Eric Roeland, Jennifer Y. Wo, Christian V. Baglini, Beow Y. Yeap, Benjamin Christopher, Christine A. Ulysse, Isobel J Fetter, Melin J. Khandekar, Rebecca S. Heist, Heather A. Shahzade, Samuel J. Klempner, Christine E. Eyler, and John T. Mullen

Subjects
Cancer Research, Treatment response, medicine.medical_specialty, Intention-to-treat analysis, business.industry, FOLFIRINOX, Locally advanced, Carboplatin, Surgery, chemistry.chemical_compound, Oncology, Paclitaxel, chemistry, Cohort, Medicine, business, Prospective cohort study
Abstract

Purpose: We performed a NCI-sponsored, prospective study of neoadjuvant FOLFIRINOX followed by chemoradiation with carboplatin/paclitaxel followed by surgery in patients with locally advanced gastric or gastroesophageal cancer. Patients and Methods: The primary objective was to determine completion rate of neoadjuvant FOLFIRINOX × 8 followed by chemoradiation. Secondary endpoints were toxicity and pathologic complete response (pCR) rate. Exploratory analysis was performed of circulating tumor DNA (ctDNA) to treatment response. Results: From October 2017 to June 2018, 25 patients were enrolled. All patients started FOLFIRINOX, 92% completed all eight planned cycles, and 88% completed chemoradiation. Twenty (80%) patients underwent surgical resection, and 7 had a pCR (35% in resected cohort, 28% intention to treat). Tumor-specific mutations were identified in 21 (84%) patients, of whom 4 and 17 patients had undetectable and detectable ctDNA at baseline, respectively. Presence of detectable post-chemoradiation ctDNA (P = 0.004) and/or postoperative ctDNA (P = 0.045) were associated with disease recurrence. Conclusions: Here we show neoadjuvant FOLFIRINOX followed by chemoradiation for locally advanced gastroesophageal cancer is feasible and yields a high rate of pCR. ctDNA appears to be a promising predictor of postoperative recurrence. See related commentary by Catenacci, p. 6281

Published
2021

35. Radiation therapy enhances immunotherapy response in microsatellite stable colorectal and pancreatic adenocarcinoma in a phase II trial

Author

Jeffrey W. Clark, Lauren Matlack, Sanya Arshad, Ryan B. Corcoran, Aparna Raj Parikh, Benjamin D. Greenbaum, Colin D. Weekes, Michael J. Raabe, Lorraine C. Drapek, Jon Dubois, Theodore S. Hong, David P. Ryan, David T. Ting, Lipika Goyal, Bronwen Foreman, Bruce J. Giantonio, Leilana Ly, Hannah Thel, Arnav Mehta, Lawrence S. Blaszkowsky, Nir Hacohen, Andrew X. Zhu, Jennifer Y. Wo, David Hoyos, Ryan D. Nipp, Emily E. Van Seventer, Jill N. Allen, Annamaria Szabolcs, Jessica A. Meurer, David J. Lieb, and Beow Y. Yeap

Subjects
Oncology, Cancer Research, medicine.medical_specialty, Performance status, business.industry, Colorectal cancer, medicine.medical_treatment, Ipilimumab, medicine.disease, digestive system diseases, Immune checkpoint, Radiation therapy, Internal medicine, Pancreatic cancer, medicine, Adenocarcinoma, Nivolumab, business, medicine.drug
Abstract

Overcoming intrinsic resistance to immune checkpoint blockade for microsatellite stable (MSS) colorectal cancer (CRC) and pancreatic ductal adenocarcinoma (PDAC) remains challenging. We conducted a single-arm, non-randomized, phase II trial (NCT03104439) combining radiation, ipilimumab and nivolumab to treat patients with metastatic MSS CRC (n = 40) and PDAC (n = 25) with an Eastern Cooperative Oncology Group (ECOG) performance status of 0 or 1. The primary endpoint was disease control rate (DCR) by intention to treat. DCRs were 25% for CRC (ten of 40; 95% confidence interval (CI), 13–41%) and 20% for PDAC (five of 25; 95% CI, 7–41%). In the per-protocol analysis, defined as receipt of radiation, DCR was 37% (ten of 27; 95% CI, 19–58%) in CRC and 29% (five of 17; 95% CI, 10–56%) in PDAC. Pretreatment biopsies revealed low tumor mutational burden for all samples but higher numbers of natural killer (NK) cells and expression of the HERVK repeat RNA in patients with disease control. This study provides proof of concept of combining radiation with immune checkpoint blockade in immunotherapy-resistant cancers. Ting and colleagues report the safety and efficacy of combined radiation and immunotherapy in a phase II trial on patients with MSS colorectal or pancreatic cancer and observe that disease control correlates with higher repetitive RNA transcription.

Published
2021

36. Percentile‐based averaging and skeletal muscle gauge improve body composition analysis: validation at multiple vertebral levels

Author

Florian J. Fintelmann, Emily E. Van Seventer, J. Peter Marquardt, Nora Horick, Till D. Best, Eric Roeland, and Ryan D. Nipp

Subjects
Male, Sarcopenia, medicine.medical_specialty, Percentile, Coefficient of determination, Survival, Concordance, Skeletal muscle, Diseases of the musculoskeletal system, Body Mass Index, Correlation, Lumbar, Physiology (medical), Internal medicine, Humans, Medicine, Orthopedics and Sports Medicine, Muscle, Skeletal, Aged, business.industry, QM1-695, Patient‐reported outcomes, Middle Aged, medicine.disease, Body composition analysis, medicine.anatomical_structure, RC925-935, Human anatomy, Body Composition, Cardiology, Female, Tomography, X-Ray Computed, business, Body mass index
Abstract

Background Skeletal muscle metrics on computed tomography (CT) correlate with clinical and patient‐reported outcomes. We hypothesize that aggregating skeletal muscle measurements from multiple vertebral levels and skeletal muscle gauge (SMG) better predict outcomes than skeletal muscle radioattenuation (SMRA) or ‐index (SMI) at a single vertebral level. Methods We performed a secondary analysis of prospectively collected clinical (overall survival, hospital readmission, time to unplanned hospital readmission or death, and readmission or death within 90 days) and patient‐reported outcomes (physical and psychological symptom burden captured as Edmonton Symptom Assessment Scale and Patient Health Questionnaire) of patients with advanced cancer who experienced an unplanned admission to Massachusetts General Hospital from 2014 to 2016. First, we assessed the correlation of skeletal muscle cross‐sectional area, SMRA, SMI, and SMG at one or more of the following thoracic (T) or lumbar (L) vertebral levels: T5, T8, T10, and L3 on CT scans obtained ≤50 days before index assessment. Second, we aggregated measurements across all available vertebral levels using percentile‐based averaging (PBA) to create the average percentile. Third, we constructed one regression model adjusted for age, sex, sociodemographic factors, cancer type, body mass index, and intravenous contrast for each combination of (i) vertebral level and average percentile, (ii) muscle metrics (SMRA, SMI, & SMG), and (iii) clinical and patient‐reported outcomes. Fourth, we compared the performance of vertebral levels and muscle metrics by ranking otherwise identical models by concordance statistic, number of included patients, coefficient of determination, and significance of muscle metric. Results We included 846 patients (mean age: 63.5 ± 12.9 years, 50.5% males) with advanced cancer [predominantly gastrointestinal (32.9%) or lung (18.9%)]. The correlation of muscle measurements between vertebral levels ranged from 0.71 to 0.84 for SMRA and 0.67 to 0.81 for SMI. The correlation of individual levels with the average percentile was 0.90–0.93 for SMRA and 0.86–0.92 for SMI. The intrapatient correlation of SMRA with SMI was 0.21–0.40. PBA allowed for inclusion of 8–47% more patients than any single‐level analysis. PBA outperformed single‐level analyses across all comparisons with average ranks 2.6, 2.9, and 1.6 for concordance statistic, coefficient of determination, and significance (range 1–5, μ = 3), respectively. On average, SMG outperformed SMRA and SMI across outcomes and vertebral levels: the average rank of SMG was 1.4, 1.4, and 1.4 for concordance statistic, coefficient of determination, and significance (range 1–3, μ = 2), respectively. Conclusions Multivertebral level skeletal muscle analyses using PBA and SMG independently and additively outperform analyses using individual levels and SMRA or SMI.

Published
2021

37. Circulating Tumor DNA Predicts Pathologic and Clinical Outcomes Following Neoadjuvant Chemoradiation and Surgery for Patients With Locally Advanced Rectal Cancer

Author

Colin D. Weekes, James C. Cusack, Christine E. Eyler, Lipika Goyal, Jochen K. Lennerz, Emily E. Van Seventer, Jill N. Allen, Jennifer Y. Wo, Peter J. Ulintz, Andrew X. Zhu, Hui Zheng, Susan G.R. McDuff, Theodore S. Hong, Daniel Kim, David P. Ryan, Mehlika Hazar-Rethinam, Jeffrey W. Clark, Ryan B. Corcoran, Isobel J Fetter, Brandon Nadres, Lawrence S. Blaszkowsky, Aparna Raj Parikh, and Karin M. Hardiman

Subjects
Male, 0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Colorectal cancer, Locally advanced, Circulating Tumor DNA, 03 medical and health sciences, 0302 clinical medicine, Predictive Value of Tests, Internal medicine, medicine, Humans, Aged, Neoplasm Staging, Retrospective Studies, Rectal Neoplasms, business.industry, ORIGINAL REPORTS, Perioperative, Middle Aged, medicine.disease, Neoadjuvant Therapy, Treatment Outcome, 030104 developmental biology, Circulating tumor DNA, 030220 oncology & carcinogenesis, Female, business
Abstract

PURPOSE This study was designed to assess the ability of perioperative circulating tumor DNA (ctDNA) to predict surgical outcome and recurrence following neoadjuvant chemoradiation for locally advanced rectal cancer (LARC). MATERIALS AND METHODS Twenty-nine patients with newly diagnosed LARC treated between January 2014 and February 2018 were enrolled. Patients received long-course neoadjuvant chemoradiation prior to surgery. Plasma ctDNA was collected at baseline, preoperatively, and postoperatively. Next-generation sequencing was used to identify mutations in the primary tumor, and mutation-specific droplet digital polymerase chain reaction was used to assess mutation fraction in ctDNA. RESULTS The median age was 54 years. The overall margin-negative, node-negative resection rate was 73% and was significantly higher among patients with undetectable preoperative ctDNA (n = 17, 88%) versus patients with detectable preoperative ctDNA (n = 9, 44%; P = .028). Undetectable ctDNA was also associated with more favorable neoadjuvant rectal scores (univariate linear regression, P = .029). Recurrence-free survival (RFS) was calculated for the subset (n = 19) who both underwent surgery and had postoperative ctDNA available. At a median follow-up of 20 months, patients with detectable postoperative ctDNA experienced poorer RFS (hazard ratio, 11.56; P = .007). All patients (4 of 4) with detectable postoperative ctDNA recurred (positive predictive value = 100%), whereas only 2 of 15 patients with undetectable ctDNA recurred (negative predictive value = 87%). CONCLUSION Among patients treated with neoadjuvant chemoradiation for LARC, patients with undetectable preoperative ctDNA were more likely to have a favorable surgical outcome as measured by the rate of margin-negative, node-negative resections and neoadjuvant rectal score. Furthermore, we have confirmed prior reports indicating that detectable postoperative ctDNA is associated with worse RFS. Future prospective study is needed to assess the potential for ctDNA to assist with personalizing treatment for LARC.

Published
2021

38. Minimal Residual Disease Detection using a Plasma-only Circulating Tumor DNA Assay in Patients with Colorectal Cancer

Author

Jennifer Y. Wo, Ryan D. Nipp, David P. Ryan, Emily E. Van Seventer, Lawrence S. Blaszkowsky, Jill N. Allen, Heather A. Shahzade, James C. Cusack, Yupeng He, Hiroko Kunitake, Liliana Bordeianou, Lipika Goyal, Motaz Qadan, Samuel J. Klempner, Jon Dubois, Kathryn Fosbenner, AmirAli Talasaz, Benchun Miao, Cristina R. Ferrone, Bruce J. Giantonio, John H. Carmichael, Jeffrey W. Clark, Victoria M. Raymond, Susannah T. Phillips, Yojan S. Shah, Islam Baiev, Aparna Raj Parikh, Colin D. Weekes, Ariel Jaimovich, Genevieve M. Boland, Ryan B. Corcoran, David H. Berger, Joy X. Jarnagin, Katie Kanter, Nihaarika Sharma, Giulia Siravegna, Isobel J Fetter, Madeleine Fish, Theodore S. Hong, Eric Roeland, Joseph W. Franses, Rocco Ricciardi, and Anna Hartwig

Subjects
0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, biology, Colorectal cancer, business.industry, Cancer, medicine.disease, Minimal residual disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Text mining, Carcinoembryonic antigen, Circulating tumor DNA, 030220 oncology & carcinogenesis, Internal medicine, medicine, Adjuvant therapy, biology.protein, In patient, business
Abstract

Purpose: Detection of persistent circulating tumor DNA (ctDNA) after curative-intent surgery can identify patients with minimal residual disease (MRD) who will ultimately recur. Most ctDNA MRD assays require tumor sequencing to identify tumor-derived mutations to facilitate ctDNA detection, requiring tumor and blood. We evaluated a plasma-only ctDNA assay integrating genomic and epigenomic cancer signatures to enable tumor-uninformed MRD detection. Experimental Design: A total of 252 prospective serial plasma specimens from 103 patients with colorectal cancer undergoing curative-intent surgery were analyzed and correlated with recurrence. Results: Of 103 patients, 84 [stage I (9.5%), II (23.8%), III (47.6%), IV (19%)] had evaluable plasma drawn after completion of definitive therapy, defined as surgery only (n = 39) or completion of adjuvant therapy (n = 45). In “landmark” plasma drawn 1-month (median, 31.5 days) after definitive therapy and >1 year follow-up, 15 patients had detectable ctDNA, and all 15 recurred [positive predictive value (PPV), 100%; HR, 11.28 (P < 0.0001)]. Of 49 patients without detectable ctDNA at the landmark timepoint, 12 (24.5%) recurred. Landmark recurrence sensitivity and specificity were 55.6% and 100%. Incorporating serial longitudinal and surveillance (drawn within 4 months of recurrence) samples, sensitivity improved to 69% and 91%. Integrating epigenomic signatures increased sensitivity by 25%–36% versus genomic alterations alone. Notably, standard serum carcinoembryonic antigen levels did not predict recurrence [HR, 1.84 (P = 0.18); PPV = 53.9%]. Conclusions: Plasma-only MRD detection demonstrated favorable sensitivity and specificity for recurrence, comparable with tumor-informed approaches. Integrating analysis of epigenomic and genomic alterations enhanced sensitivity. These findings support the potential clinical utility of plasma-only ctDNA MRD detection. See related commentary by Bent and Kopetz, p. 5449

Published
2021

39. Associations of Skeletal Muscle With Symptom Burden and Clinical Outcomes in Hospitalized Patients With Advanced Cancer

Author

Florian J. Fintelmann, Christopher P. Bridge, Jennifer S. Temel, Areej El-Jawahri, J. Peter Marquardt, Eric Roeland, Till D. Best, Michael H. Rosenthal, Chinenye C. Azoba, Nora Horick, Emily E. Van Seventer, Amelie S. Troschel, Joseph A. Greer, Ryan D. Nipp, and Richard Newcomb

Subjects
Male, Sarcopenia, medicine.medical_specialty, Hospitalized patients, Radiodensity, 03 medical and health sciences, Low muscle mass, 0302 clinical medicine, Neoplasms, Internal medicine, medicine, Humans, 030212 general & internal medicine, Muscle, Skeletal, Aged, business.industry, Hazard ratio, Symptom burden, Skeletal muscle, Odds ratio, Middle Aged, Advanced cancer, Hospitalization, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Female, business
Abstract

Background: Low muscle mass (quantity) is common in patients with advanced cancer, but little is known about muscle radiodensity (quality). We sought to describe the associations of muscle mass and radiodensity with symptom burden, healthcare use, and survival in hospitalized patients with advanced cancer. Methods: We prospectively enrolled hospitalized patients with advanced cancer from September 2014 through May 2016. Upon admission, patients reported their physical (Edmonton Symptom Assessment System [ESAS]) and psychological (Patient Health Questionnaire-4 [PHQ-4]) symptoms. We used CT scans performed per routine care within 45 days before enrollment to evaluate muscle mass and radiodensity. We used regression models to examine associations of muscle mass and radiodensity with patients’ symptom burden, healthcare use (hospital length of stay and readmissions), and survival. Results: Of 1,121 patients enrolled, 677 had evaluable muscle data on CT (mean age, 62.86 ± 12.95 years; 51.1% female). Older age and female sex were associated with lower muscle mass (age: B, –0.16; PPPP=.014), and higher BMI was associated with higher muscle mass (B, 0.58; PPPP=.016), ESAS-Total (B, –0.29; P=.002), PHQ-4-Depression (B, –0.03; P=.006), and PHQ-4-Anxiety (B, –0.03; P=.008) symptoms, as well as decreased hospital length of stay (B, –0.07; P=.005), risk of readmission or death in 90 days (odds ratio, 0.97; PPConclusions: Although muscle mass (quantity) only correlated with survival, we found that muscle radiodensity (quality) was associated with patients’ symptoms, healthcare use, and survival. These findings underscore the added importance of assessing muscle quality when seeking to address adverse muscle changes in oncology.

Published
2021

40. Associations of baseline patient‐reported outcomes with treatment outcomes in advanced gastrointestinal cancer

Author

Jon Dubois, Kathryn Fosbenner, Amirkasra Mojtahed, Bruce J. Giantonio, Aparna Raj Parikh, Nora Horick, Colin D. Weekes, Eric Roeland, Lipika Goyal, Areej El-Jawahri, Samuel J. Klempner, Ryan D. Nipp, Emily E. Van Seventer, Therese M. Mulvey, Joseph W. Franses, Jill N. Allen, David P. Ryan, Katie Kanter, Jeffrey W. Clark, Lawrence S. Blaszkowsky, Ryan B. Corcoran, and Madeleine Fish

Subjects
Adult, Male, Cancer Research, medicine.medical_specialty, Treatment response, Treatment outcome, 03 medical and health sciences, 0302 clinical medicine, Quality of life, Surveys and Questionnaires, Internal medicine, medicine, Humans, Patient Reported Outcome Measures, 030212 general & internal medicine, Gastrointestinal cancer, Aged, Gastrointestinal Neoplasms, Aged, 80 and over, business.industry, Hazard ratio, Cancer, Odds ratio, Middle Aged, medicine.disease, Progression-Free Survival, humanities, Treatment Outcome, Oncology, 030220 oncology & carcinogenesis, Quality of Life, Female, business, Progressive disease
Abstract

BACKGROUND Patient-reported outcomes (PROs) assessing quality of life (QOL) and symptom burden correlate with clinical outcomes in patients with cancer. However, to the authors' knowledge, data regarding associations between PROs and treatment response are lacking. METHODS The authors prospectively approached consecutive patients with advanced gastrointestinal cancer who were initiating a new treatment. Prior to treatment, patients reported their QOL (Functional Assessment of Cancer Therapy-General [FACT-G], 4 subscales: Functional, Physical, Emotional, Social; higher scores indicate better QOL) and symptom burden (Edmonton Symptom Assessment System [ESAS], Patient Health Questionnaire-4 [PHQ-4]; higher scores represent greater symptoms). Regression models were used to examine associations of baseline PROs with treatment response (clinical benefit or progressive disease [PD] at time of first scan), healthcare utilization, and survival. RESULTS From May 2019 to April 2020, a total of 112 patients with advanced gastrointestinal cancer were enrolled. For treatment response, 64.3% had CB and 35.7% had PD. Higher baseline ESAS-Physical (odds ratio, 1.04; P = .027) and lower FACT-G Functional (odds ratio, 0.92; P = .038) scores were associated with PD. Higher ESAS-Physical (hazard ratio [HR], 1.03; P = .044) and lower FACT-G Total (HR, 0.96; P = .005), FACT-G Physical (HR, 0.89; P < .001), and FACT-G Functional (HR, 0.87; P < .001) scores were associated with a greater hospitalization risk. Lower FACT-G Total (HR, 0.96; P = .009) and FACT-G Emotional (HR, 0.86; P = .012) scores as well as higher ESAS-Total (HR, 1.03; P = .014) and ESAS-Physical (HR, 1.04; P = .032) scores were associated with worse survival. CONCLUSIONS Baseline PROs are associated with treatment response in patients with advanced gastrointestinal cancer, namely physical symptoms and functional QOL, in addition to health care use and survival. The findings of the current study support the association between PROs and important clinical outcomes, including the novel finding of treatment response.

Published
2020

41. Response to Anti-EGFR Therapy in Patients with BRAF non-V600–Mutant Metastatic Colorectal Cancer

Author

Hideaki Bando, Emily E. Van Seventer, Takayuki Yoshino, Ryan B. Corcoran, Aparna Raj Parikh, Hiroya Taniguchi, Neal Rosen, Elisa de Stanchina, Sebastian Mondaca, Hiromichi Ebi, Daisuke Kotani, Huiyong Zhao, Rona Yaeger, Zhan Yao, and Claire N. Thant

Subjects
Male, Proto-Oncogene Proteins B-raf, 0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, endocrine system diseases, Colorectal cancer, Mutant, Cetuximab, Mice, SCID, medicine.disease_cause, Article, EGFR Antibody, 03 medical and health sciences, 0302 clinical medicine, Mice, Inbred NOD, Internal medicine, Tumor Cells, Cultured, medicine, Animals, Humans, Molecular Targeted Therapy, Prospective Studies, Kinase activity, Prospective cohort study, Protein Kinase Inhibitors, neoplasms, Survival rate, Mutation, biology, Rectal Neoplasms, business.industry, Prognosis, medicine.disease, Xenograft Model Antitumor Assays, digestive system diseases, ErbB Receptors, Survival Rate, 030104 developmental biology, 030220 oncology & carcinogenesis, Colonic Neoplasms, biology.protein, Female, Antibody, Colorectal Neoplasms, business
Abstract

Purpose: While mutations in BRAF in metastatic colorectal cancer (mCRC) most commonly occur at the V600 amino acid, with the advent of next-generation sequencing, non-V600 BRAF mutations are increasingly identified in clinical practice. It is unclear whether these mutants, like BRAF V600E, confer resistance to anti-EGFR therapy. Experimental Design: We conducted a multicenter pooled analysis of consecutive patients with non-V600 BRAF-mutated mCRCs identified between 2010 and 2017. Non-V600 BRAF mutations were divided into functional classes based on signaling mechanism and kinase activity: activating and RAS-independent (class 2) or kinase-impaired and RAS-dependent (class 3). Results: Forty patients with oncogenic non-V600 BRAF–mutant mCRC received anti-EGFR antibody treatment [n = 12 (30%) class 2 and n = 28 (70%) class 3]. No significant differences in clinical characteristics were observed by mutation class. In contrast, while only 1 of 12 patients with class 2 BRAF mCRC responded, 14 of 28 patients with class 3 BRAF responded to anti-EGFR therapy (response rate, 8% and 50%, respectively, P = 0.02). Specifically, in first- or second-line, 1 of 6 (17%) patients with class 2 and 7 of 9 (78%) patients with class 3 BRAF mutants responded (P = 0.04). In third- or later-line, none of 6 patients with class 2 and 7 of 19 (37%) patients with class 3 BRAF mutants responded (P = 0.14). Conclusions: Response to EGFR antibody treatment in mCRCs with class 2 BRAF mutants is rare, while a large portion of CRCs with class 3 BRAF mutants respond. Patients with colorectal cancer with class 3 BRAF mutations should be considered for anti-EGFR antibody treatment. See related commentary by Fontana and Valeri, p. 6896

Published
2019

42. Muscle Loss Is Associated with Overall Survival in Patients with Metastatic Colorectal Cancer Independent of Tumor Mutational Status and Weight Loss

Author

Patrick Connor Johnson, Eric Roeland, Areej El-Jawahri, Jennifer S. Temel, Emily E. Van Seventer, Christopher P. Bridge, Madeleine Fish, Florian J. Fintelmann, Nora Horick, Katie Kanter, Ryan D. Nipp, Amelie S. Troschel, Ryan B. Corcoran, J. Peter Marquardt, and Till D. Best

Subjects
Male, Proto-Oncogene Proteins B-raf, Oncology, Sarcopenia, Cancer Research, medicine.medical_specialty, Survival, Colorectal cancer, medicine.medical_treatment, Skeletal muscle, Outcomes, Disease, Body composition, 030218 nuclear medicine & medical imaging, 03 medical and health sciences, 0302 clinical medicine, Weight loss, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, Weight Loss, Gastrointestinal Cancer, Humans, Medicine, Muscle, Skeletal, Aged, Retrospective Studies, Chemotherapy, business.industry, Hazard ratio, Middle Aged, medicine.disease, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Mutation, Female, medicine.symptom, Colorectal Neoplasms, business, 600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit::610 Medizin und Gesundheit, Cohort study
Abstract

Background Survival in patients with metastatic colorectal cancer (mCRC) has been associated with tumor mutational status, muscle loss, and weight loss. We sought to explore the combined effects of these variables on overall survival. Materials and Methods We performed an observational cohort study, prospectively enrolling patients receiving chemotherapy for mCRC. We retrospectively assessed changes in muscle (using computed tomography) and weight, each dichotomized as >5% or ≤5% loss, at 3, 6, and 12 months after diagnosis of mCRC. We used regression models to assess relationships between tumor mutational status, muscle loss, weight loss, and overall survival. Additionally, we evaluated associations between muscle loss, weight loss, and tumor mutational status. Results We included 226 patients (mean age 59 ± 13 years, 53% male). Tumor mutational status included 44% wild type, 42% RAS‐mutant, and 14% BRAF‐mutant. Patients with >5% muscle loss at 3 and 12 months experienced worse survival controlling for mutational status and weight (3 months hazard ratio, 2.66; p < .001; 12 months hazard ratio, 2.10; p = .031). We found an association of >5% muscle loss with BRAF‐mutational status at 6 and 12 months. Weight loss was not associated with survival nor mutational status. Conclusion Increased muscle loss at 3 and 12 months may identify patients with mCRC at risk for decreased overall survival, independent of tumor mutational status. Specifically, >5% muscle loss identifies patients within each category of tumor mutational status with decreased overall survival in our sample. Our findings suggest that quantifying muscle loss on serial computed tomography scans may refine survival estimates in patients with mCRC. Implications for Practice In this study of 226 patients with metastatic colorectal cancer, it was found that losing >5% skeletal muscle at 3 and 12 months after the diagnosis of metastatic disease was associated with worse overall survival, independent of tumor mutational status and weight loss. Interestingly, results did not show a significant association between weight loss and overall survival. These findings suggest that muscle quantification on serial computed tomography may refine survival estimates in patients with metastatic colorectal cancer beyond mutational status., Cancer cachexia has traditionally been defined using weight loss; however, loss of skeletal muscle may be a more objective measure. This article reports the results of a retrospective study that assessed whether skeletal muscle loss is associated with overall survival in patients with metastatic colorectal cancer, independent of tumor mutational status and weight loss.

Published
2021

43. Radiation Induced Checkpoint Immunotherapy Response in Refractory Colorectal and Pancreatic Adenocarcinoma

Author

Beow Y. Yeap, Bronwen Foreman, David Hoyos, Nir Hacohen, Sanya Arshad, Jennifer Y. Wo, Lauren Matlack, Jon Dubois, Benjamin Greenbaum, Colin D. Weekes, David P. Ryan, David J. Lieb, Lawrence S. Blaszkowsky, Ryan D. Nipp, Arnav Mehta, Leilana Ly, Emily E. Van Seventer, Annamaria Szabolcs, Jill N. Allen, Jessica A. Meurer, Lorraine C. Drapek, Jeffrey W. Clark, Andrew X. Zhu, Ryan B. Corcoran, Lipika Goyal, Bruce J. Giantonio, Hannah Thel, Theodore S. Hong, David T. Ting, and Aparna Raj Parikh

Subjects
Refractory, business.industry, medicine.medical_treatment, medicine, Cancer research, Adenocarcinoma, Radiation induced, Immunotherapy, medicine.disease, business, digestive system diseases
Abstract

Immune checkpoint blockade has limited efficacy in microsatellite stable (MSS) colorectal (CRC) and pancreatic (PDAC) cancer. Preclinical models have demonstrated the use of radiation to activate the innate immune response and stimulate responsiveness to immune checkpoint blockade. Here, we describe a Phase 2 trial of radiation therapy combined with combined anti-CTLA4 (ipilimumab) and anti-PD1 (nivolumab) antibodies in MSS CRC and PDAC. In the per protocol analysis disease control rate was 37% (10/27) in CRC and 29% (5/17) in PDAC with an overall response rate of 15% (4/27) and 18% (3/17), respectively. Whole exome and RNA sequencing of biopsies from 17 patients revealed low tumor mutational burden in all tumors, but a notable upregulation of interferon stimulated genes with concordant high expression of multiple repeat RNA transcripts in responders. Altogether, this study provides foundational human proof of concept of radiation with combination immune checkpoint blockade therapy in otherwise immunotherapy resistant cancers.

Published
2020

44. Radiation therapy enhances immunotherapy response in microsatellite stable colorectal and pancreatic adenocarcinoma in a phase II trial

Author

Aparna R, Parikh, Annamaria, Szabolcs, Jill N, Allen, Jeffrey W, Clark, Jennifer Y, Wo, Michael, Raabe, Hannah, Thel, David, Hoyos, Arnav, Mehta, Sanya, Arshad, David J, Lieb, Lorraine C, Drapek, Lawrence S, Blaszkowsky, Bruce J, Giantonio, Colin D, Weekes, Andrew X, Zhu, Lipika, Goyal, Ryan D, Nipp, Jon S, Dubois, Emily E, Van Seventer, Bronwen E, Foreman, Lauren E, Matlack, Leilana, Ly, Jessica A, Meurer, Nir, Hacohen, David P, Ryan, Beow Y, Yeap, Ryan B, Corcoran, Benjamin D, Greenbaum, David T, Ting, and Theodore S, Hong

Subjects
Pancreatic Neoplasms, Treatment Outcome, Radiotherapy, Humans, Immunologic Factors, Immunotherapy, Adenocarcinoma, Colorectal Neoplasms, Immune Checkpoint Inhibitors, Carcinoma, Pancreatic Ductal, Microsatellite Repeats
Abstract

Overcoming intrinsic resistance to immune checkpoint blockade for microsatellite stable (MSS) colorectal cancer (CRC) and pancreatic ductal adenocarcinoma (PDAC) remains challenging. We conducted a single-arm, non-randomized, phase II trial (NCT03104439) combining radiation, ipilimumab and nivolumab to treat patients with metastatic MSS CRC (n = 40) and PDAC (n = 25) with an Eastern Cooperative Oncology Group (ECOG) performance status of 0 or 1. The primary endpoint was disease control rate (DCR) by intention to treat. DCRs were 25% for CRC (ten of 40; 95% confidence interval (CI), 13-41%) and 20% for PDAC (five of 25; 95% CI, 7-41%). In the per-protocol analysis, defined as receipt of radiation, DCR was 37% (ten of 27; 95% CI, 19-58%) in CRC and 29% (five of 17; 95% CI, 10-56%) in PDAC. Pretreatment biopsies revealed low tumor mutational burden for all samples but higher numbers of natural killer (NK) cells and expression of the HERVK repeat RNA in patients with disease control. This study provides proof of concept of combining radiation with immune checkpoint blockade in immunotherapy-resistant cancers.

Published
2020

45. Leveraging the Potential Synergy Between Patient‐Reported Outcomes and Body Composition Analysis in Patients with Cancer

Author

Florian J. Fintelmann, Eric Roeland, Emily E. Van Seventer, and Ryan D. Nipp

Subjects
Oncology, Cancer Research, medicine.medical_specialty, business.industry, Editorials, Cancer, Composition analysis, medicine.disease, Text mining, Internal medicine, Neoplasms, medicine, Body Composition, Humans, In patient, Patient Reported Outcome Measures, business
Abstract

In the oncology setting, data on the relationship between body composition, patient-reported outcomes, and patient outcomes are limited. This editorial outlines the available data and discusses the potential for using such information as a strategy to predict and enhance patient outcomes.

Published
2020

46. Serial ctDNA monitoring to predict response to systemic therapy in metastatic gastrointestinal cancers

Author

Nora Horick, Andrew X. Zhu, Bruce J. Giantonio, Eric Roeland, Jaime L. Schneider, Jochen K. Lennerz, Brandon Nadres, Lipika Goyal, Ashraf Thabet, David P. Ryan, Emily E. Van Seventer, Madeleine Fish, Theodore S. Hong, Jill N. Allen, Dora Dias-Santagata, Kathryn Fosbenner, Jeffrey W. Clark, Aparna Raj Parikh, Ryan B. Corcoran, A. John Iafrate, Amirkasra Mojtahed, Heather A. Shahzade, Colin D. Weekes, Katie Kanter, Bezaye Teshome, Lawrence S. Blaszkowsky, Jennifer Y. Wo, Ryan D. Nipp, Giulia Siravegna, and Isobel J Fetter

Subjects
0301 basic medicine, Oncology, Adult, Male, Cancer Research, medicine.medical_specialty, Treatment response, Mutant allele, Antineoplastic Agents, Systemic therapy, Article, Circulating Tumor DNA, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Internal medicine, Partial response, medicine, Biomarkers, Tumor, Humans, In patient, Digital polymerase chain reaction, Gastrointestinal cancer, Longitudinal Studies, Prospective Studies, Neoplasm Metastasis, Aged, Gastrointestinal Neoplasms, Aged, 80 and over, business.industry, High-Throughput Nucleotide Sequencing, Middle Aged, medicine.disease, Survival Rate, 030104 developmental biology, Treatment Outcome, 030220 oncology & carcinogenesis, Mutation, Disease Progression, Female, business, Blood drawing
Abstract

Purpose: ctDNA offers a promising, noninvasive approach to monitor therapeutic efficacy in real-time. We explored whether the quantitative percent change in ctDNA early after therapy initiation can predict treatment response and progression-free survival (PFS) in patients with metastatic gastrointestinal cancer. Experimental Design: A total of 138 patients with metastatic gastrointestinal cancers and tumor profiling by next-generation sequencing had serial blood draws pretreatment and at scheduled intervals during therapy. ctDNA was assessed using individualized droplet digital PCR measuring the mutant allele fraction in plasma of mutations identified in tumor biopsies. ctDNA changes were correlated with tumor markers and radiographic response. Results: A total of 138 patients enrolled. A total of 101 patients were evaluable for ctDNA and 68 for tumor markers at 4 weeks. Percent change of ctDNA by 4 weeks predicted partial response (PR, P < 0.0001) and clinical benefit [CB: PR and stable disease (SD), P < 0.0001]. ctDNA decreased by 98% (median) and >30% for all PR patients. ctDNA change at 8 weeks, but not 2 weeks, also predicted CB (P < 0.0001). Four-week change in tumor markers also predicted response (P = 0.0026) and CB (P = 0.022). However, at a clinically relevant specificity threshold of 90%, 4-week ctDNA change more effectively predicted CB versus tumor markers, with a sensitivity of 60% versus 24%, respectively (P = 0.0109). Patients whose 4-week ctDNA decreased beyond this threshold (≥30% decrease) had a median PFS of 175 days versus 59.5 days (HR, 3.29; 95% CI, 1.55–7.00; P < 0.0001). Conclusions: Serial ctDNA monitoring may provide early indication of response to systemic therapy in patients with metastatic gastrointestinal cancer prior to radiographic assessments and may outperform standard tumor markers, warranting further evaluation.

Published
2020

47. Associations of sarcopenia with hematologic toxicity, treatment intensity, and healthcare utilization in patients with metastatic colorectal cancer

Author

Matthew Lei, Ryan David Nipp, Erica Tavares, Uvette Lou, Erica Grasso, Stephanie Y Mui, Jan Peter Marquardt, Till D. Best, Emily E. Van Seventer, Anurag Saraf, Ismail Tahir, Nora K. Horick, Florian J. Fintelmann, and Eric Roeland

Subjects
Cancer Research, Oncology
Abstract

84 Background: We evaluated the impact of baseline sarcopenia on hematologic toxicity, treatment intensity, and healthcare utilization in patients with mCRC receiving FOLFOX or FOLFIRI. Methods: We retrospectively analyzed patients with mCRC who received care at our institution from 1/2011-11/2018 and were part of a biobanking protocol. Included adults received either first-line palliative FOLFOX- or FOLFIRI-based regimens and were followed for 6 months. We categorized sarcopenia based on skeletal muscle index measured at diagnosis of metastatic disease and pre-defined sex-specific cutoff values (F < 39 cm2/m2, M < 55cm2/m2). Our primary aim was to evaluate the association of sarcopenia and hematologic toxicity, defined as the incidence of grade ≥3 (G≥3) neutropenia, thrombocytopenia, or anemia (NCI CTCAE v5.0). Secondary endpoints included treatment intensity (dose reductions, treatment delays, relative-dose intensity [RDI]), and healthcare utilization (ED visits and/or hospitalizations). Bivariate analyses were used to evaluate associations between baseline sarcopenia and outcomes. Results: 126 of 177 screened patients met inclusion criteria (70 (56%) males, median age 61 yrs (range, 29-85)). 59 (46.8%) patients were sarcopenic. More patients received FOLFOX than FOLFIRI (92 [73.0%] vs. 34 [27.0%]). At baseline, patients had a median weight 76.9kg (IQR, 70.0-90.4 kg), BMI 26.6 kg/m2 (IQR, 24.1-30.5 kg/m2), and BSA 1.90 m2 (IQR, 1.72-2.01 m2). The incidence of G≥3 hematologic toxicity was 39.0% vs. 23.9% in sarcopenic and non-sarcopenic patients, respectively (p = 0.06). Patients with sarcopenia experienced higher incidence of G≥3 neutropenia (30.5% vs. 14.9%, p = 0.03), while G≥3 thrombocytopenia was similar (3.4% vs. 1.5%). The incidence of dose reductions and treatment delays did not differ significantly (86.4% vs. 89.5%, 72.9% vs. 71.6%, respectively). RDI was decreased for the 5FU bolus (52.5% vs. 65.0%, p = 0.02). Rates of ED visits (32.2% vs. 19.4%, p = 0.10) and hospitalizations (32.2% vs. 26.9%, p = 0.51) did not differ compared between patients with and without sarcopenia. Conclusions: Patients with mCRC and baseline sarcopenia receiving FOLFOX- or FOLFIRI experienced a higher incidence of G≥3 neutropenia and lower 5FU bolus treatment intensity. Studies are needed to understand how best to adjust treatment according to patients’ muscle mass.

Published
2022

48. Real-time Genomic Characterization of Advanced Pancreatic Cancer to Enable Precision Medicine

Author

Emily E. Van Seventer, Ana Babic, Jeffrey W. Miller, Deborah Knoerzer, Marvin Ryou, Heather A. Shahzade, Nadine Jackson McCleary, Jaegil Kim, Douglas A. Rubinson, Mehlika Hazar-Rethinam, Rebecca J. Nagy, Kristin Anderka, David A. Tuveson, Robert J. Mayer, Scott L. Carter, Leona A. Doyle, Nelly Oliver, Nicholas D. Camarda, Kimmie Ng, Matthew B. Yurgelun, Lauren K. Brais, Levi A. Garraway, Jeffrey A. Meyerhardt, Arezou A. Ghazani, Richard A. Moffitt, Stuart G. Silverman, Thomas E. Clancy, Srivatsan Raghavan, Annacarolina da Silva, Brandon Nadres, James M. Cleary, Andrew J. Aguirre, Kunal Jajoo, Kelly P. Burke, Michael H. Rosenthal, Emma Reilly, Kimberly Perez, Jonathan A. Nowak, Charles S. Fuchs, Dean Welsch, Jen Jen Yeh, Matthew H. Kulke, Marisa W. Welch, William C. Hahn, Anuj K. Patel, Ryan B. Corcoran, Karla Helvie, Paul B. Shyn, Gad Getz, Nikhil Wagle, Dorisanne Y. Ragon, Lori Marini, Geoffrey I. Shapiro, Janet E. Murphy, Brian M. Wolpin, Richard B. Lanman, Devin McCabe, Jason L. Hornick, Bruce E. Johnson, Ewa Sicinska, and Joseph P. St. Pierre

Subjects
Adult, Male, 0301 basic medicine, DNA Repair, MAP Kinase Signaling System, DNA repair, Germline, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Pancreatic cancer, Exome Sequencing, Carcinoma, medicine, Humans, Gene Regulatory Networks, Clinical significance, Precision Medicine, Homologous Recombination, Germ-Line Mutation, Exome sequencing, Aged, Aged, 80 and over, Sequence Analysis, RNA, business.industry, Gene Expression Profiling, Genetic Variation, Genomics, Middle Aged, medicine.disease, Precision medicine, Gene Expression Regulation, Neoplastic, Pancreatic Neoplasms, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, Female, business, Carcinoma, Pancreatic Ductal
Abstract

Clinically relevant subtypes exist for pancreatic ductal adenocarcinoma (PDAC), but molecular characterization is not yet standard in clinical care. We implemented a biopsy protocol to perform time-sensitive whole-exome sequencing and RNA sequencing for patients with advanced PDAC. Therapeutically relevant genomic alterations were identified in 48% (34/71) and pathogenic/likely pathogenic germline alterations in 18% (13/71) of patients. Overall, 30% (21/71) of enrolled patients experienced a change in clinical management as a result of genomic data. Twenty-six patients had germline and/or somatic alterations in DNA-damage repair genes, and 5 additional patients had mutational signatures of homologous recombination deficiency but no identified causal genomic alteration. Two patients had oncogenic in-frame BRAF deletions, and we report the first clinical evidence that this alteration confers sensitivity to MAPK pathway inhibition. Moreover, we identified tumor/stroma gene expression signatures with clinical relevance. Collectively, these data demonstrate the feasibility and value of real-time genomic characterization of advanced PDAC. Significance: Molecular analyses of metastatic PDAC tumors are challenging due to the heterogeneous cellular composition of biopsy specimens and rapid progression of the disease. Using an integrated multidisciplinary biopsy program, we demonstrate that real-time genomic characterization of advanced PDAC can identify clinically relevant alterations that inform management of this difficult disease. Cancer Discov; 8(9); 1096–111. ©2018 AACR. See related commentary by Collisson, p. 1062. This article is highlighted in the In This Issue feature, p. 1047

Published
2018

49. Convergent Therapeutic Strategies to Overcome the Heterogeneity of Acquired Resistance in BRAFV600E Colorectal Cancer

Author

G. Celine Han, Heather A. Shahzade, Mehlika Hazar-Rethinam, Eunice L. Kwak, Leanne G. Ahronian, David Liu, Jeffrey W. Clark, Aparna Raj Parikh, Theodore S. Hong, Ryan B. Corcoran, Eliezer M. Van Allen, Jason E. Faris, Emily E. Van Seventer, Jill N. Allen, Catriona B. Hong, Nicholas A. Jessop, Joseph M. Gurski, Marianna Kleyman, Janet E. Murphy, Lifeng Chen, A. John Iafrate, Brandon Nadres, and Dora Dias-Santagata

Subjects
0301 basic medicine, MAPK/ERK pathway, Colorectal cancer, MEK inhibitor, Clone (cell biology), Cancer, Drug resistance, Biology, medicine.disease, 03 medical and health sciences, 030104 developmental biology, Oncology, medicine, Cancer research, Neoplasm, Exome sequencing
Abstract

Clonal heterogeneity associated with acquired resistance presents a critical therapeutic challenge. Whole-exome sequencing of paired tumor biopsies and targeted sequencing of cell-free DNA (cfDNA) from patients with BRAFV600E colorectal cancer receiving BRAF inhibitor combinations identified 14 distinct alterations in MAPK pathway components driving acquired resistance, with as many as eight alterations in a single patient. We developed a pooled clone system to study clonal outgrowth during acquired resistance, in vitro and in vivo. In vitro, the dynamics of individual resistant clones could be monitored in real time in cfDNA isolated from culture media during therapy. Outgrowth of multiple resistant clones was observed during therapy with BRAF, EGFR, and MEK inhibitor combinations. However, ERK inhibition, particularly in combination with BRAF and EGFR inhibition, markedly abrogated clonal outgrowth in vitro and in vivo. Thus, convergent, up-front therapy may suppress outgrowth of heterogeneous clones harboring clinically observed resistance alterations, which may improve clinical outcome. Significance: We observed heterogeneous, recurrent alterations in the MAPK pathway as key drivers of acquired resistance in BRAFV600E colorectal cancer, with multiple concurrent resistance alterations detectable in individual patients. Using a novel pooled clone system, we identify convergent up-front therapeutic strategies capable of intercepting multiple resistance mechanisms as potential approaches to suppress emergence of acquired resistance. Cancer Discov; 8(4); 417–27. ©2018 AACR. See related commentary by Janku, p. 389. See related article by Corcoran et al., p. 428. This article is highlighted in the In This Issue feature, p. 371

Published
2018

50. Patient-reported care satisfaction and symptom burden in hospitalized patients with cancer

Author

Joseph A. Greer, Emily E. Van Seventer, Ryan D. Nipp, Carolyn L. Qian, Vicki A. Jackson, Eva Gaufberg, Irene Wang, Areej El-Jawahri, Emilia Kaslow-Zieve, Richard Newcomb, Charu Vyas, Chinenye C. Azoba, David P. Ryan, and Jennifer S. Temel

Subjects
medicine.medical_specialty, Cancer Research, Healthcare utilization, Oncology, Hospitalized patients, business.industry, medicine, Symptom burden, Cancer, Intensive care medicine, medicine.disease, business
Abstract

2013 Background: Hospitalized patients with cancer often experience high symptom burden, which may impact their care satisfaction and use of health care services. Yet, studies describing these patients’ care satisfaction, symptom burden, and health care utilization are lacking. Methods: We prospectively enrolled patients with cancer and unplanned hospitalizations from 9/2014-4/2017. Upon admission, patients self-reported their care satisfaction (FAMCARE items asking about satisfaction regarding speed with which symptoms are treated and coordination of care) and physical (Edmonton Symptom Assessment System [ESAS]) and psychological (Patient Health Questionnaire 4 [PHQ4]) symptom burden. We used regression models to identify patient factors associated with care satisfaction. We also explored associations between patients’ care satisfaction, symptom burden, and hospital length of stay (LOS) in models adjusted for age, sex, marital status, comorbidity score, cancer type, cancer documented as curable/incurable, time since cancer diagnosis, and admission to a dedicated oncology service. Results: We enrolled 1,576 of 1,749 (90.1%) consecutive patients (mean age = 63.19±13.39 years, 46.3% female). Most reported being very satisfied/satisfied with the speed with which symptoms are treated (89.0%) and coordination of care (90.1%). Older age (B = 0.01, P < .02 for both) and admission to a dedicated oncology service (B = 0.20, P < .01 for both) were each independently associated with higher satisfaction with the speed with which symptoms are treated and coordination of care. Higher satisfaction with the speed with which symptoms are treated was associated with lower PHQ4 depression (B = -0.14, P = .01), PHQ4 anxiety (B = -0.11, P < .01), ESAS physical (B = -1.30, P < .01), and ESAS total (B = -2.44, P < .01) symptoms. Higher satisfaction with coordination of care was associated with lower PHQ4 depression (B = -0.14, P = .02), PHQ4 anxiety (B = -0.16, P < .01), ESAS physical (B = -1.30, P < .01), and ESAS total (B = -2.75, P < .01) symptoms. Satisfaction with the speed with which symptoms are treated (B = -0.47, P = .03) and coordination of care (B = -0.50, P = .03) were both associated with shorter hospital LOS. Conclusions: Most hospitalized patients with cancer reported high care satisfaction, which was associated with older age and admission to a dedicated oncology service. We found relationships among higher care satisfaction, lower symptom burden, and shorter hospital LOS, underscoring the importance of efforts to enhance symptom management and care coordination in this population.

Published
2021

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