Your search keyword '"Small Cell Lung Carcinoma"' showing total 83 results

1. Atezolizumab plus stereotactic ablative radiotherapy for medically inoperable patients with early-stage non-small cell lung cancer: a multi-institutional phase I trial.

Author

Mirhadi, Amin, Mirhadi, Amin, Shiao, Stephen, Beckett, Laurel, Merleev, Alexander, Marusina, Alina, Eastham, David, Vick, Logan, McGee, Heather, Lara, Frances, Garcia, Leslie, Morris, Leigh, Kelly, Karen, Riess, Jonathan, Schalper, Kurt, Borowsky, Alexander, Monjazeb, Arta, Murphy, William, Maverakis, Emanual, Canter, Robert, Li, Tianhong, Daly, Megan, Chen, Shuai, Luxardi, Guillaume, Mirhadi, Amin, Mirhadi, Amin, Shiao, Stephen, Beckett, Laurel, Merleev, Alexander, Marusina, Alina, Eastham, David, Vick, Logan, McGee, Heather, Lara, Frances, Garcia, Leslie, Morris, Leigh, Kelly, Karen, Riess, Jonathan, Schalper, Kurt, Borowsky, Alexander, Monjazeb, Arta, Murphy, William, Maverakis, Emanual, Canter, Robert, Li, Tianhong, Daly, Megan, Chen, Shuai, and Luxardi, Guillaume

Abstract

Stereotactic ablative radiotherapy (SABR) is a standard-of-care for medically-inoperable-early-stage non-small cell lung cancer (NSCLC). One third of patients progress and chemotherapy is rarely used in this population. We questioned if addition of the immune-checkpoint-inhibitor (ICI) atezolizumab to standard-of-care SABR can improve outcomes. We initiated a multi-institutional single-arm phase I study (NCT02599454) enrolling twenty patients with the primary endpoint of maximum tolerated dose (MTD); secondary endpoints of safety and efficacy; and exploratory mechanistic correlatives. Treatment is well tolerated and full dose atezolizumab (1200 mg) is the MTD. Efficacy signals include early responses (after 2 cycles of ICI, before initiation of SABR) in 17% of patients. Biomarkers of functional adaptive immunity, including T cell activation in the tumor and response to ex-vivo stimulation by circulating T cells, are highly predictive of benefit. These results require validation and are being tested in a phase III randomized trial.

Published

2023

2. Targeting PEA3 transcription factors to mitigate small cell lung cancer progression.

Author

Shia, David W, Shia, David W, Choi, WooSuk, Vijayaraj, Preethi, Vuong, Valarie, Sandlin, Jenna M, Lu, Michelle M, Aziz, Adam, Marin, Caliope, Aros, Cody J, Sen, Chandani, Durra, Abdo, Lund, Andrew J, Purkayastha, Arunima, Rickabaugh, Tammy M, Graeber, Thomas G, Gomperts, Brigitte N, Shia, David W, Shia, David W, Choi, WooSuk, Vijayaraj, Preethi, Vuong, Valarie, Sandlin, Jenna M, Lu, Michelle M, Aziz, Adam, Marin, Caliope, Aros, Cody J, Sen, Chandani, Durra, Abdo, Lund, Andrew J, Purkayastha, Arunima, Rickabaugh, Tammy M, Graeber, Thomas G, and Gomperts, Brigitte N

Abstract

Small cell lung cancer (SCLC) remains a lethal disease with a dismal overall survival rate of 6% despite promising responses to upfront combination chemotherapy. The key drivers of such rapid mortality include early metastatic dissemination in the natural course of the disease and the near guaranteed emergence of chemoresistant disease. Here, we found that we could model the regression and relapse seen in clinical SCLC in vitro. We utilized time-course resolved RNA-sequencing to globally profile transcriptome changes as SCLC cells responded to a combination of cisplatin and etoposide-the standard-of-care in SCLC. Comparisons across time points demonstrated a distinct transient transcriptional state resembling embryonic diapause. Differential gene expression analysis revealed that expression of the PEA3 transcription factors ETV4 and ETV5 were transiently upregulated in the surviving fraction of cells which we determined to be necessary for efficient clonogenic expansion following chemotherapy. The FGFR-PEA3 signaling axis guided the identification of a pan-FGFR inhibitor demonstrating in vitro and in vivo efficacy in delaying progression following combination chemotherapy, observed inhibition of phosphorylation of the FGFR adaptor FRS2 and corresponding downstream MAPK and PI3K-Akt signaling pathways. Taken together, these data nominate PEA3 transcription factors as key mediators of relapse progression in SCLC and identify a clinically actionable small molecule candidate for delaying relapse of SCLC.

Published

2023

3. YAP silencing by RB1 mutation is essential for small-cell lung cancer metastasis.

Author

Wu, Zhengming, Wu, Zhengming, Su, Junhui, Li, Fu-Long, Chen, Tao, Mayner, Jaimie, Engler, Adam, Ma, Shenghong, Li, Qingquan, Guan, Kun-Liang, Wu, Zhengming, Wu, Zhengming, Su, Junhui, Li, Fu-Long, Chen, Tao, Mayner, Jaimie, Engler, Adam, Ma, Shenghong, Li, Qingquan, and Guan, Kun-Liang

Abstract

Small cell lung cancer (SCLC) is highly lethal due to its prevalent metastasis. Most SCLCs have inactivating mutations in TP53 and RB1. We find that loss of YAP expression is key for SCLC cells to acquire rapid ameboid migration and high metastatic potential. YAP functions through its target genes CCN1/CCN2 to inhibit SCLC ameboid migration. RB1 mutation contributes to YAP transcriptional silencing via E2F7, which recruits the RCOR co-repressor complex to YAP promoter. We discover that benzamide family HDAC inhibitors stimulate YAP expression by inhibiting the RCOR-HDAC complex, thereby suppressing SCLC metastasis and improving survival in a mouse model. Our study unveils the molecular and cellular basis underlying SCLCs high metastatic potential, the previously unrecognized role of YAP in suppressing ameboid migration and tumor metastasis, and the mechanism of YAP transcription regulation involving E2F7, RCOR, and Sin3 HDAC. This study reveals a therapeutic potential of benzamides for SCLC treatment.

Published

2023

4. Addition of Immune Checkpoint Inhibitors to Chemotherapy vs Chemotherapy Alone as First-Line Treatment in Extensive-Stage Small-Cell Lung Carcinoma: A Systematic Review and Meta-Analysis

Author

Universidad de Sevilla. Departamento de Medicina, Arriola, Edurne, González Cao, María, Domine, Manuel, De Castro, Javier, Cobo, Manuel, Bernabé-Caro, Reyes, Isla, Dolores, Universidad de Sevilla. Departamento de Medicina, Arriola, Edurne, González Cao, María, Domine, Manuel, De Castro, Javier, Cobo, Manuel, Bernabé-Caro, Reyes, and Isla, Dolores

Abstract

Introduction The addition of immune checkpoint inhibitors (ICIs) to conventional chemotherapy (CT) as first-line treatment improves survival in extensive-stage small-cell lung cancer (ES-SCLC). The aim of this meta-analysis was to determine the relative efficacy of first-line ICIs compared with CT in patients with ES-SCLC. Methods Two independent reviewers extracted relevant data according to PRISMA guidelines and assessed the risk of bias using the Cochrane Collaboration's risk-of-bias tool. Meta-analysis was conducted using random-effects models to calculate an average effect size for overall survival (OS), progression-free survival (PFS), and safety outcomes in the overall populations and clinically relevant subgroups. Results A literature search of PubMed and Embase was performed. Six randomized controlled clinical trials (IMpower133, CHECKMATE-451, CASPIAN, KEYNOTE-604, and phase II and III ipilimumab plus CT trials) with a total of 3757 patients were included. Compared with CT alone, ICIs plus CT showed a favourable effect on OS (hazard ratio [HR] 0.85; 95% confidence intervals [CI] 0.79–0.96) and PFS (HR 0.78; 95% CI 0.72–0.83) but a non-significant increase in the risk of experiencing any adverse event (relative risk, 1.05; 95% CI 0.99–1.11). The estimated HR for OS favoured ICI combinations in all planned subgroups according to age (< 65 years/≥ 65 years), sex (men/women), and ECOG performance status (0/1). Analysis by specific ICI revealed significant improvements in OS only for atezolizumab + CT (HR 1.36; 95% CI 1.09–1.69) and durvalumab + CT (HR 1.35; 95% CI 1.12–1.62) compared with CT alone. Conclusion Combining anti-programmed cell death ligand 1 antibodies with platinum/etoposide is a superior therapeutic approach compared to CT alone for the first-line treatment of patients with ES-SCLC.

Published

2022

5. Addition of Immune Checkpoint Inhibitors to Chemotherapy vs Chemotherapy Alone as First-Line Treatment in Extensive-Stage Small-Cell Lung Carcinoma: A Systematic Review and Meta-Analysis

Author

Universidad de Sevilla. Departamento de Medicina, Arriola, Edurne, González Cao, María, Domine, Manuel, De Castro, Javier, Cobo, Manuel, Bernabé-Caro, Reyes, Isla, Dolores, Universidad de Sevilla. Departamento de Medicina, Arriola, Edurne, González Cao, María, Domine, Manuel, De Castro, Javier, Cobo, Manuel, Bernabé-Caro, Reyes, and Isla, Dolores

Abstract

Introduction The addition of immune checkpoint inhibitors (ICIs) to conventional chemotherapy (CT) as first-line treatment improves survival in extensive-stage small-cell lung cancer (ES-SCLC). The aim of this meta-analysis was to determine the relative efficacy of first-line ICIs compared with CT in patients with ES-SCLC. Methods Two independent reviewers extracted relevant data according to PRISMA guidelines and assessed the risk of bias using the Cochrane Collaboration's risk-of-bias tool. Meta-analysis was conducted using random-effects models to calculate an average effect size for overall survival (OS), progression-free survival (PFS), and safety outcomes in the overall populations and clinically relevant subgroups. Results A literature search of PubMed and Embase was performed. Six randomized controlled clinical trials (IMpower133, CHECKMATE-451, CASPIAN, KEYNOTE-604, and phase II and III ipilimumab plus CT trials) with a total of 3757 patients were included. Compared with CT alone, ICIs plus CT showed a favourable effect on OS (hazard ratio [HR] 0.85; 95% confidence intervals [CI] 0.79–0.96) and PFS (HR 0.78; 95% CI 0.72–0.83) but a non-significant increase in the risk of experiencing any adverse event (relative risk, 1.05; 95% CI 0.99–1.11). The estimated HR for OS favoured ICI combinations in all planned subgroups according to age (< 65 years/≥ 65 years), sex (men/women), and ECOG performance status (0/1). Analysis by specific ICI revealed significant improvements in OS only for atezolizumab + CT (HR 1.36; 95% CI 1.09–1.69) and durvalumab + CT (HR 1.35; 95% CI 1.12–1.62) compared with CT alone. Conclusion Combining anti-programmed cell death ligand 1 antibodies with platinum/etoposide is a superior therapeutic approach compared to CT alone for the first-line treatment of patients with ES-SCLC.

Published

2022

6. Surgical Outcomes for Early Stage Non-small Cell Lung Cancer at Facilities With Stereotactic Body Radiation Therapy Programs.

Author

Syed, Yusef A, Syed, Yusef A, Stokes, William, Rupji, Manali, Liu, Yuan, Khullar, Onkar, Sebastian, Nikhil, Higgins, Kristin, Bradley, Jeffrey D, Curran, Walter J, Ramalingam, Suresh, Taylor, James, Sancheti, Manu, Fernandez, Felix, Moghanaki, Drew, Syed, Yusef A, Syed, Yusef A, Stokes, William, Rupji, Manali, Liu, Yuan, Khullar, Onkar, Sebastian, Nikhil, Higgins, Kristin, Bradley, Jeffrey D, Curran, Walter J, Ramalingam, Suresh, Taylor, James, Sancheti, Manu, Fernandez, Felix, and Moghanaki, Drew

Abstract

BackgroundPatients undergoing surgery for early stage non-small cell lung cancer (NSCLC) may be at high risk for postoperative mortality. Access to stereotactic body radiation therapy (SBRT) may facilitate more appropriate patient selection for surgery.Research questionIs postoperative mortality associated with early stage NSCLC lower at facilities with higher use of SBRT?Study design and methodsPatients with early stage NSCLC reported to the National Cancer Database between 2004 and 2015 were included. Use of SBRT was defined by each facility's SBRT experience (in years) and SBRT to surgery volume ratios. Multivariate logistic regression was used to test for the associations between SBRT use and postoperative mortality.ResultsThe study cohort consisted of 202,542 patients who underwent surgical resection of cT1-T2N0M0 NSCLC tumors. The 90-day postoperative mortality rate declined during the study period from 4.6% to 2.6% (P < .001), the proportion of facilities that used SBRT increased from 4.6% to 77.5% (P < .001), and the proportion of patients treated with SBRT increased from 0.7% to 15.4% (P < .001). On multivariate analysis, lower 90-day postoperative mortality rates were observed at facilities with > 6 years of SBRT experience (OR, 0.84; 95% CI, 0.76-0.94; P = .003) and SBRT to surgery volume ratios of more than 17% (OR, 0.85; 95% CI, 0.79-0.92; P < .001). Ninety-day mortality also was associated with surgical volume, region, year, age, sex, and race, among other covariates. Interaction testing between these covariates showed negative results.InterpretationPatients who underwent resection for early stage NSCLC at facilities with higher SBRT use showed lower rates of postoperative mortality. These findings suggest that the availability and use of SBRT may improve the selection of patients for surgery who are predicted to be at high risk of postoperative mortality.

Published

2022

7. Graded Prognostic Assessment (GPA) for Patients With Lung Cancer and Brain Metastases: Initial Report of the Small Cell Lung Cancer GPA and Update of the Non-Small Cell Lung Cancer GPA Including the Effect of Programmed Death Ligand 1 and Other Prognostic Factors.

Author

Sperduto, Paul, Sperduto, Paul, De, Brian, Li, Jing, Carpenter, David, Kirkpatrick, John, Milligan, Michael, Shih, Helen, Kutuk, Tugce, Kotecha, Rupesh, Higaki, Hajime, Otsuka, Manami, Aoyama, Hidefumi, Bourgoin, Malie, Roberge, David, Dajani, Salah, Sachdev, Sean, Gainey, Jordan, Buatti, John, Breen, William, Brown, Paul, Gallitto, Matthew, Wang, Tony, Shanley, Ryan, Lou, Emil, Shiao, Jay, Gaspar, Laurie, Tanabe, Satoshi, Nakano, Toshimichi, An, Yi, Chiang, Veronica, Zeng, Liang, Soliman, Hany, Elhalawani, Hesham, Cagney, Daniel, Thomas, Evan, Boggs, Drexell, Ahluwalia, Manmeet, Mehta, Minesh, Braunstein, Steve, Ni, Lisa, Sperduto, Paul, Sperduto, Paul, De, Brian, Li, Jing, Carpenter, David, Kirkpatrick, John, Milligan, Michael, Shih, Helen, Kutuk, Tugce, Kotecha, Rupesh, Higaki, Hajime, Otsuka, Manami, Aoyama, Hidefumi, Bourgoin, Malie, Roberge, David, Dajani, Salah, Sachdev, Sean, Gainey, Jordan, Buatti, John, Breen, William, Brown, Paul, Gallitto, Matthew, Wang, Tony, Shanley, Ryan, Lou, Emil, Shiao, Jay, Gaspar, Laurie, Tanabe, Satoshi, Nakano, Toshimichi, An, Yi, Chiang, Veronica, Zeng, Liang, Soliman, Hany, Elhalawani, Hesham, Cagney, Daniel, Thomas, Evan, Boggs, Drexell, Ahluwalia, Manmeet, Mehta, Minesh, Braunstein, Steve, and Ni, Lisa

Abstract

PURPOSE: Patients with lung cancer and brain metastases represent a markedly heterogeneous population. Accurate prognosis is essential to optimally individualize care. In prior publications, we described the graded prognostic assessment (GPA), but a GPA for patients with small cell lung cancer (SCLC) has never been reported, and in non-small cell lung cancer (NSCLC), the effect of programmed death ligand 1 (PD-L1) was unknown. The 3-fold purpose of this work is to provide the initial report of an SCLC GPA, to evaluate the effect of PD-L1 on survival in patients with NSCLC, and to update the Lung GPA accordingly. METHODS AND MATERIALS: A multivariable analysis of prognostic factors and treatments associated with survival was performed on 4183 patients with lung cancer (3002 adenocarcinoma, 611 nonadenocarcinoma, 570 SCLC) with newly diagnosed brain metastases between January 1, 2015, and December 31, 2020, using a multi-institutional retrospective database. Significant variables were used to update the Lung GPA. RESULTS: Overall median survival for lung adenocarcinoma, SCLC, and nonadenocarcinoma was 17, 10, and 8 months, respectively, but varied widely by GPA from 2 to 52 months. In SCLC, the significant prognostic factors were age, performance status, extracranial metastases, and number of brain metastases. In NSCLC, the distribution of molecular markers among patients with lung adenocarcinoma and known primary tumor molecular status revealed alterations/expression in PD-L1 50% to 100%, PD-L1 1% to 49%, epidermal growth factor receptor, and anaplastic lymphoma kinase in 32%, 31%, 30%, and 7%, respectively. Median survival of patients with lung adenocarcinoma and brain metastases with 0, 1% to 49%, and ≥50% PD-L1 expression was 17, 19, and 24 months, respectively (P < .01), confirming PD-L1 is a prognostic factor. Previously identified prognostic factors for NSCLC (epidermal growth factor receptor and anaplastic lymphoma kinase status, performance status, age, nu

Published

2022

8. Association of Operability With Post-Treatment Mortality in Early-Stage Non-Small Cell Lung Cancer.

Author

Stokes, William, Stokes, William, Xiong, Niya, Liu, Yuan, Higgins, Kristin, Tian, Sibo, Bradley, Jeffrey, Moghanaki, Drew, Rusthoven, Chad, Stokes, William, Stokes, William, Xiong, Niya, Liu, Yuan, Higgins, Kristin, Tian, Sibo, Bradley, Jeffrey, Moghanaki, Drew, and Rusthoven, Chad

Abstract

BACKGROUND: Operability is both a crucial determinant in treatment selection and a potential confounder in analyses comparing surgery with non-surgical approaches such as stereotactic body radiotherapy (SBRT). We aimed to assess the association between operability status and intervention with post-treatment mortality in early-stage non-small cell lung cancer (NSCLC). PATIENTS AND METHODS: We defined four groups of patients with cT1-T2N0M0 NSCLC diagnosed 2010 to 2014 from the National Cancer Database: SBRT patients deemed operable vs. inoperable and surgery patients receiving open vs. minimally-invasive approaches. Mortality rates at 30, 60, and 90 days post-treatment were calculated and compared. RESULTS: We abstracted 80,108 patients, 0.8% undergoing SBRT and operable, 13.2% undergoing SBRT and inoperable, 52.4% undergoing open surgery, and 33.7% undergoing minimally-invasive surgery. Mortality rates were highest among open surgery patients and lowest among operable SBRT patients (2.0% vs. 0.2% at 30 days and 3.7% vs. 0.7% at 90 days), with intermediate results in the other two groups. These findings persisted on multivariate Cox regression: compared to patients undergoing minimally-invasive surgery, mortality risk was highest among open surgery patients (30 days HR 1.32, 95%CI 1.16-1.51; 90 days HR 1.36, 95%CI 1.24-1.50; both P < .001) and lowest among operable SBRT patients (30 days HR 0.09, 95%CI 0.01-0.64; 90 days HR 0.15, 95%CI 0.05-0.46; both P ≤ .016). These associations were maintained in a propensity score-matched subset. CONCLUSION: Operable patients undergoing SBRT experience minimal post-treatment mortality compared to their inoperable counterparts. These findings illustrate the potential for confounding by operability to bias results in cohort studies that compare surgical vs. non-surgical approaches in early-stage NSCLC.

Published

2022

9. Addition of Immune Checkpoint Inhibitors to Chemotherapy vs Chemotherapy Alone as First-Line Treatment in Extensive-Stage Small-Cell Lung Carcinoma: A Systematic Review and Meta-Analysis

Author

Universidad de Sevilla. Departamento de Medicina, Arriola, Edurne, González Cao, María, Domine, Manuel, De Castro, Javier, Cobo, Manuel, Bernabé-Caro, Reyes, Isla, Dolores, Universidad de Sevilla. Departamento de Medicina, Arriola, Edurne, González Cao, María, Domine, Manuel, De Castro, Javier, Cobo, Manuel, Bernabé-Caro, Reyes, and Isla, Dolores

Abstract

Introduction The addition of immune checkpoint inhibitors (ICIs) to conventional chemotherapy (CT) as first-line treatment improves survival in extensive-stage small-cell lung cancer (ES-SCLC). The aim of this meta-analysis was to determine the relative efficacy of first-line ICIs compared with CT in patients with ES-SCLC. Methods Two independent reviewers extracted relevant data according to PRISMA guidelines and assessed the risk of bias using the Cochrane Collaboration's risk-of-bias tool. Meta-analysis was conducted using random-effects models to calculate an average effect size for overall survival (OS), progression-free survival (PFS), and safety outcomes in the overall populations and clinically relevant subgroups. Results A literature search of PubMed and Embase was performed. Six randomized controlled clinical trials (IMpower133, CHECKMATE-451, CASPIAN, KEYNOTE-604, and phase II and III ipilimumab plus CT trials) with a total of 3757 patients were included. Compared with CT alone, ICIs plus CT showed a favourable effect on OS (hazard ratio [HR] 0.85; 95% confidence intervals [CI] 0.79–0.96) and PFS (HR 0.78; 95% CI 0.72–0.83) but a non-significant increase in the risk of experiencing any adverse event (relative risk, 1.05; 95% CI 0.99–1.11). The estimated HR for OS favoured ICI combinations in all planned subgroups according to age (< 65 years/≥ 65 years), sex (men/women), and ECOG performance status (0/1). Analysis by specific ICI revealed significant improvements in OS only for atezolizumab + CT (HR 1.36; 95% CI 1.09–1.69) and durvalumab + CT (HR 1.35; 95% CI 1.12–1.62) compared with CT alone. Conclusion Combining anti-programmed cell death ligand 1 antibodies with platinum/etoposide is a superior therapeutic approach compared to CT alone for the first-line treatment of patients with ES-SCLC.

Published

2022

10. Tri-modal management of primary small cell carcinoma of the pancreas (SCCP): a rare neuroendocrine carcinoma (NEC).

Author

Elzein, Safa, Elzein, Safa, Bao, Fei, Lin, Ray, Schnickel, Gabriel, Lowy, Andrew M, Botta, Gregory P, Elzein, Safa, Elzein, Safa, Bao, Fei, Lin, Ray, Schnickel, Gabriel, Lowy, Andrew M, and Botta, Gregory P

Abstract

BackgroundPrimary small cell carcinoma of the pancreas (SCCP) is a rare malignant neuroendocrine carcinoma (NEC). Typically, it presents with lymphovascular invasion as well as metastasis at the time of diagnosis which portends a dismal prognosis. Treatment is typically based on therapy used for other aggressive NECs such as small cell lung cancer. Although multimodal surgery, radiation and chemotherapy may improve prognosis, the outcome generally remains poor.Case presentationHere we present a primary SCCP managed with neoadjuvant multi-agent chemotherapy combined with radiotherapy and surgery CONCLUSIONS: Multi-disciplinary therapy resulted in an ongoing 28 + month radiographic complete response and overall survival.

Published

2021

11. Small Cell Lung Cancer, Version 2.2022, NCCN Clinical Practice Guidelines in Oncology.

Author

Ganti, Apar Kishor P, Ganti, Apar Kishor P, Loo, Billy W, Bassetti, Michael, Blakely, Collin, Chiang, Anne, D'Amico, Thomas A, D'Avella, Christopher, Dowlati, Afshin, Downey, Robert J, Edelman, Martin, Florsheim, Charles, Gold, Kathryn A, Goldman, Jonathan W, Grecula, John C, Hann, Christine, Iams, Wade, Iyengar, Puneeth, Kelly, Karen, Khalil, Maya, Koczywas, Marianna, Merritt, Robert E, Mohindra, Nisha, Molina, Julian, Moran, Cesar, Pokharel, Saraswati, Puri, Sonam, Qin, Angel, Rusthoven, Chad, Sands, Jacob, Santana-Davila, Rafael, Shafique, Michael, Waqar, Saiama N, Gregory, Kristina M, Hughes, Miranda, Ganti, Apar Kishor P, Ganti, Apar Kishor P, Loo, Billy W, Bassetti, Michael, Blakely, Collin, Chiang, Anne, D'Amico, Thomas A, D'Avella, Christopher, Dowlati, Afshin, Downey, Robert J, Edelman, Martin, Florsheim, Charles, Gold, Kathryn A, Goldman, Jonathan W, Grecula, John C, Hann, Christine, Iams, Wade, Iyengar, Puneeth, Kelly, Karen, Khalil, Maya, Koczywas, Marianna, Merritt, Robert E, Mohindra, Nisha, Molina, Julian, Moran, Cesar, Pokharel, Saraswati, Puri, Sonam, Qin, Angel, Rusthoven, Chad, Sands, Jacob, Santana-Davila, Rafael, Shafique, Michael, Waqar, Saiama N, Gregory, Kristina M, and Hughes, Miranda

Abstract

The NCCN Clinical Practice Guidelines in Oncology (NCCN Guidelines) for Small Cell Lung Cancer (SCLC) provide recommended management for patients with SCLC, including diagnosis, primary treatment, surveillance for relapse, and subsequent treatment. This selection for the journal focuses on metastatic (known as extensive-stage) SCLC, which is more common than limited-stage SCLC. Systemic therapy alone can palliate symptoms and prolong survival in most patients with extensive-stage disease. Smoking cessation counseling and intervention should be strongly promoted in patients with SCLC and other high-grade neuroendocrine carcinomas. The "Summary of the Guidelines Updates" section in the SCLC algorithm outlines the most recent revisions for the 2022 update, which are described in greater detail in this revised Discussion text.

Published

2021

12. ESTRO ACROP guidelines for target volume definition in the thoracic radiation treatment of small cell lung cancer.

Author

UCL - SSS/IREC/MIRO - Pôle d'imagerie moléculaire, radiothérapie et oncologie, UCL - (SLuc) Service de radiothérapie oncologique, Le Pechoux, Cecile, Faivre-Finn, Corinne, Ramella, Sara, McDonald, Fiona, Manapov, Farkhad, Putora, Paul Martin, Slotman, Ben, De Ruysscher, Dirk, Ricardi, Umberto, Geets, Xavier, Belderbos, José, Pöttgen, Christoph, Dziadiuszko, Rafal, Peeters, Stephanie, Lievens, Yolande, Hurkmans, Coen, Van Houtte, Paul, Nestle, Ursula, UCL - SSS/IREC/MIRO - Pôle d'imagerie moléculaire, radiothérapie et oncologie, UCL - (SLuc) Service de radiothérapie oncologique, Le Pechoux, Cecile, Faivre-Finn, Corinne, Ramella, Sara, McDonald, Fiona, Manapov, Farkhad, Putora, Paul Martin, Slotman, Ben, De Ruysscher, Dirk, Ricardi, Umberto, Geets, Xavier, Belderbos, José, Pöttgen, Christoph, Dziadiuszko, Rafal, Peeters, Stephanie, Lievens, Yolande, Hurkmans, Coen, Van Houtte, Paul, and Nestle, Ursula

Abstract

Radiotherapy (RT) plays a major role in the treatment of small cell lung cancer (SCLC). Therefore, the ACROP committee was asked by ESTRO to provide recommendations on target volume delineation for standard clinical scenarios in definitive (chemo)-radiotherapy (CRT), adjuvant RT for stages I-III SCLC and consolidation thoracic RT for stage IV disease. The aim of these guidelines is to standardise and optimise the process of RT treatment planning for clinical practice and prospective studies. The process for the development of the guidelines included the evaluation of a structured questionnaire followed by a consensus discussion, voting and writing process within the committee. Firstly, we provide recommendations for both the imaging to be performed as part of the diagnostic work-up and for the RT planning process. Secondly, recommendations are made for target volume delineation including delineation of the primary gross tumour volume (GTV) and lymph node GTV and clinical tumour volume (CTV) expansion in the context of definitive and adjuvant RT. With regard to internal target volume (ITV) and planning target volume (PTV) definitions, we make recommendations about the management of geometric uncertainties and target motion. Finally, we provide our opinions on organ at risk (OAR) delineation and organisational issues to be considered.

Published

2020

13. A Timeline of Immune Checkpoint Inhibitor Approvals in Small Cell Lung Cancer.

Author

Gill, Jennifer, Gill, Jennifer, Cetnar, Jeremy Paul, Prasad, Vinay, Gill, Jennifer, Gill, Jennifer, Cetnar, Jeremy Paul, and Prasad, Vinay

Abstract

In this commentary, we review the timeline of clinical trials and regulatory actions of approved immune checkpoint inhibitors for small cell lung cancer, discuss challenges faced by regulatory agencies, and highlight paradoxical lessons that emerge. Accelerated approvals may fail to expedite drugs to market in this setting and further research on overall survival benefit is needed to prove drug efficacy.

Published

2020

14. Dietary glycemic index, glycemic load, and lung cancer risk: A case-control study in Los Angeles County.

Author

Chang, Chun-Pin, Chang, Chun-Pin, Meyers, Travis J, Fu, Alan, Zhang, Ming-Yan, Tashkin, Donald P, Rao, Jian-Yu, Cozen, Wendy, Mack, Thomas M, Hashibe, Mia, Morgenstern, Hal, Zhang, Zuo-Feng, Chang, Chun-Pin, Chang, Chun-Pin, Meyers, Travis J, Fu, Alan, Zhang, Ming-Yan, Tashkin, Donald P, Rao, Jian-Yu, Cozen, Wendy, Mack, Thomas M, Hashibe, Mia, Morgenstern, Hal, and Zhang, Zuo-Feng

Abstract

BackgroundAlthough there is some evidence of positive associations between both the glycemic index (GI) and glycemic load (GL) with cancer risk, the relationships with lung cancer risk remain largely unexplored. We evaluated the associations between GI and GL with lung cancer.MethodsThe analyses were performed using data from a population-based case-control study recruited between 1999 and 2004 in Los Angeles County. Dietary factors were collected from 593 incident lung cancer cases and 1026 controls using a modified food frequency questionnaire. GI and GL were estimated using a food composition table. Adjusted odds ratios (ORs) and 95 % confidence intervals (CI) were estimated using unconditional logistic regression adjusting for potential confounders.ResultsDietary GI was positively associated with lung cancer (OR for upper vs. lower tertile = 1.62; 95 % CI: 1.17, 2.25). For histologic subtypes, positive associations were observed between GI and adenocarcinoma (OR for upper vs. lower tertile = 1.82; 95 % CI: 1.22, 2.70) and small cell carcinoma (OR for upper vs. lower tertile = 2.68; 95 % CI: 1.25, 5.74). No clear association between GL and lung cancer was observed.ConclusionThese findings suggest that high dietary GI was associated with increased lung cancer risk, and the positive associations were observed for both lung adenocarcinoma and small cell lung carcinoma. Replication in an independent dataset is merited for a broader interpretation of our results.

Published

2020

15. Axon-like protrusions promote small cell lung cancer migration and metastasis.

Author

Yang, Dian, Yang, Dian, Qu, Fangfei, Cai, Hongchen, Chuang, Chen-Hua, Lim, Jing Shan, Jahchan, Nadine, Grüner, Barbara M, S Kuo, Christin, Kong, Christina, Oudin, Madeleine J, Winslow, Monte M, Sage, Julien, Yang, Dian, Yang, Dian, Qu, Fangfei, Cai, Hongchen, Chuang, Chen-Hua, Lim, Jing Shan, Jahchan, Nadine, Grüner, Barbara M, S Kuo, Christin, Kong, Christina, Oudin, Madeleine J, Winslow, Monte M, and Sage, Julien

Abstract

Metastasis is the main cause of death in cancer patients but remains a poorly understood process. Small cell lung cancer (SCLC) is one of the most lethal and most metastatic cancer types. SCLC cells normally express neuroendocrine and neuronal gene programs but accumulating evidence indicates that these cancer cells become relatively more neuronal and less neuroendocrine as they gain the ability to metastasize. Here we show that mouse and human SCLC cells in culture and in vivo can grow cellular protrusions that resemble axons. The formation of these protrusions is controlled by multiple neuronal factors implicated in axonogenesis, axon guidance, and neuroblast migration. Disruption of these axon-like protrusions impairs cell migration in culture and inhibits metastatic ability in vivo. The co-option of developmental neuronal programs is a novel molecular and cellular mechanism that contributes to the high metastatic ability of SCLC.

Published

2019

16. Phase II Study of Roniciclib in Combination with Cisplatin/Etoposide or Carboplatin/Etoposide as First-Line Therapy in Patients with Extensive-Disease Small Cell Lung Cancer

Author

Reck, M, Horn, L, Novello, S, Barlesi, F, Albert, I, Juhasz, E, Kowalski, D, Robinet, G, Cadranel, J, Bidoli, P, Chung, J, Fritsch, A, Drews, U, Wagner, A, Govindan, R, Reck M., Horn L., Novello S., Barlesi F., Albert I., Juhasz E., Kowalski D., Robinet G., Cadranel J., Bidoli P., Chung J., Fritsch A., Drews U., Wagner A., Govindan R., Reck, M, Horn, L, Novello, S, Barlesi, F, Albert, I, Juhasz, E, Kowalski, D, Robinet, G, Cadranel, J, Bidoli, P, Chung, J, Fritsch, A, Drews, U, Wagner, A, Govindan, R, Reck M., Horn L., Novello S., Barlesi F., Albert I., Juhasz E., Kowalski D., Robinet G., Cadranel J., Bidoli P., Chung J., Fritsch A., Drews U., Wagner A., and Govindan R.

Abstract

Introduction: This phase II study evaluated the efficacy and safety of the pan-cyclin–dependent kinase inhibitor roniciclib with platinum-based chemotherapy in patients with extensive-disease SCLC. Methods: In this randomized, double-blind study, unselected patients with previously untreated extensive-disease SCLC received roniciclib, 5 mg, or placebo twice daily according to a 3 days–on, 4 days–off schedule in 21-day cycles, with concomitant cisplatin or carboplatin on day 1 and etoposide on days 1 to 3. The primary end point was progression-free survival. Other end points included overall survival, objective response rate, and safety. Results: A total of 140 patients received treatment: 70 with roniciclib plus chemotherapy and 70 with placebo plus chemotherapy. Median progression-free survival times was 4.9 months (95% confidence interval [CI]: 4.2–5.5) with roniciclib plus chemotherapy and 5.5 months (95% CI: 4.6–5.6) with placebo plus chemotherapy (hazard ratio [HR] = 1.242, 95% CI: 0.820–1.881, p = 0.8653). Median overall survival times was 9.7 months (95% CI: 7.9–11.1) with roniciclib plus chemotherapy and 10.3 months (95% CI: 8.7–11.9) with placebo plus chemotherapy (HR = 1.281, 95% CI: 0.776–1.912, p = 0.7858). The objective response rates were 60.6% with roniciclib plus chemotherapy and 74.6% with placebo plus chemotherapy. Common treatment-emergent adverse events in both groups included nausea, vomiting, and fatigue. Serious treatment-emergent adverse events were more common with roniciclib plus chemotherapy (57.1%) than with placebo plus chemotherapy (38.6%). Conclusions: Roniciclib combined with chemotherapy demonstrated an unfavorable risk-benefit profile in patients with extensive-disease SCLC, and the study was prematurely terminated.

Published

2019

17. Axon-like protrusions promote small cell lung cancer migration and metastasis.

Author

Yang, Dian, Yang, Dian, Qu, Fangfei, Cai, Hongchen, Chuang, Chen-Hua, Lim, Jing Shan, Jahchan, Nadine, Grüner, Barbara M, S Kuo, Christin, Kong, Christina, Oudin, Madeleine J, Winslow, Monte M, Sage, Julien, Yang, Dian, Yang, Dian, Qu, Fangfei, Cai, Hongchen, Chuang, Chen-Hua, Lim, Jing Shan, Jahchan, Nadine, Grüner, Barbara M, S Kuo, Christin, Kong, Christina, Oudin, Madeleine J, Winslow, Monte M, and Sage, Julien

Abstract

Metastasis is the main cause of death in cancer patients but remains a poorly understood process. Small cell lung cancer (SCLC) is one of the most lethal and most metastatic cancer types. SCLC cells normally express neuroendocrine and neuronal gene programs but accumulating evidence indicates that these cancer cells become relatively more neuronal and less neuroendocrine as they gain the ability to metastasize. Here we show that mouse and human SCLC cells in culture and in vivo can grow cellular protrusions that resemble axons. The formation of these protrusions is controlled by multiple neuronal factors implicated in axonogenesis, axon guidance, and neuroblast migration. Disruption of these axon-like protrusions impairs cell migration in culture and inhibits metastatic ability in vivo. The co-option of developmental neuronal programs is a novel molecular and cellular mechanism that contributes to the high metastatic ability of SCLC.

Published

2019

18. Circulating Tumor DNA Profiling in Small-Cell Lung Cancer Identifies Potentially Targetable Alterations.

Author

Devarakonda, Siddhartha, Devarakonda, Siddhartha, Sankararaman, Sumithra, Herzog, Brett H, Gold, Kathryn A, Waqar, Saiama N, Ward, Jeffrey P, Raymond, Victoria M, Lanman, Richard B, Chaudhuri, Aadel A, Owonikoko, Taofeek K, Li, Bob T, Poirier, John T, Rudin, Charles M, Govindan, Ramaswamy, Morgensztern, Daniel, Devarakonda, Siddhartha, Devarakonda, Siddhartha, Sankararaman, Sumithra, Herzog, Brett H, Gold, Kathryn A, Waqar, Saiama N, Ward, Jeffrey P, Raymond, Victoria M, Lanman, Richard B, Chaudhuri, Aadel A, Owonikoko, Taofeek K, Li, Bob T, Poirier, John T, Rudin, Charles M, Govindan, Ramaswamy, and Morgensztern, Daniel

Abstract

PurposePatients with SCLC rarely undergo biopsies at relapse. When pursued, tissue obtained can be inadequate for molecular testing, posing a challenge in identifying potentially targetable alterations in a clinically meaningful time frame. We examined the feasibility of circulating tumor DNA (ctDNA) testing in identifying potentially targetable alterations in SCLC.Experimental designctDNA test results were prospectively collected from patients with SCLC between 2014 and 2017 and analyzed. ctDNA profiles of SCLC at diagnosis and relapse were also compared.ResultsA total of 609 samples collected from 564 patients between 2014 and 2017 were analyzed. The median turnaround time for test results was 14 days. Among patients with data on treatment status, there were 61 samples from 59 patients and 219 samples from 206 patients collected at diagnosis and relapse, respectively. The number of mutations or amplifications detected per sample did not differ by treatment status. Potentially targetable alterations in DNA repair, MAPK and PI3K pathways, and genes such as MYC and ARID1A were identifiable through ctDNA testing. Furthermore, our results support that it may be possible to reconstruct the clonal relationship between detected variants through ctDNA testing.ConclusionsPatients with relapsed SCLC rarely undergo biopsies for molecular testing and often require prompt treatment initiation. ctDNA testing is less invasive and capable of identifying alterations in relapsed disease in a clinically meaningful timeframe. ctDNA testing on an expanded gene panel has the potential to advance our knowledge of the mechanisms underlying treatment resistance in SCLC and aid in the development of novel treatment strategies.

Published

2019

19. Body Mass Index (BMI), BMI Change, and Overall Survival in Patients With SCLC and NSCLC: A Pooled Analysis of the International Lung Cancer Consortium.

Author

Shepshelovich, Daniel, Shepshelovich, Daniel, Xu, Wei, Lu, Lin, Fares, Aline, Yang, Ping, Christiani, David, Zhang, Jie, Shiraishi, Kouya, Ryan, Brid M, Chen, Chu, Schwartz, Ann G, Tardon, Adonina, Wu, Xifeng, Schabath, Matthew B, Teare, M Dawn, Le Marchand, Loic, Zhang, Zuo-Feng, Field, John K, Brenner, Hermann, Diao, Nancy, Xie, Juntao, Kohno, Takashi, Harris, Curtis C, Wenzlaff, Angela S, Fernandez-Tardon, Guillermo, Ye, Yuanqing, Taylor, Fiona, Wilkens, Lynne R, Davies, Michael, Liu, Yi, Barnett, Matt J, Goodman, Gary E, Morgenstern, Hal, Holleczek, Bernd, Brown, M Catherine, Liu, Geoffrey, Hung, Rayjean J, Shepshelovich, Daniel, Shepshelovich, Daniel, Xu, Wei, Lu, Lin, Fares, Aline, Yang, Ping, Christiani, David, Zhang, Jie, Shiraishi, Kouya, Ryan, Brid M, Chen, Chu, Schwartz, Ann G, Tardon, Adonina, Wu, Xifeng, Schabath, Matthew B, Teare, M Dawn, Le Marchand, Loic, Zhang, Zuo-Feng, Field, John K, Brenner, Hermann, Diao, Nancy, Xie, Juntao, Kohno, Takashi, Harris, Curtis C, Wenzlaff, Angela S, Fernandez-Tardon, Guillermo, Ye, Yuanqing, Taylor, Fiona, Wilkens, Lynne R, Davies, Michael, Liu, Yi, Barnett, Matt J, Goodman, Gary E, Morgenstern, Hal, Holleczek, Bernd, Brown, M Catherine, Liu, Geoffrey, and Hung, Rayjean J

Abstract

IntroductionThe relationships between morbid obesity, changes in body mass index (BMI) before cancer diagnosis, and lung cancer outcomes by histology (SCLC and NSCLC) have not been well studied.MethodsIndividual level data analysis was performed on 25,430 patients with NSCLC and 2787 patients with SCLC from 16 studies of the International Lung Cancer Consortium evaluating the association between various BMI variables and lung cancer overall survival, reported as adjusted hazard ratios (aHRs) from Cox proportional hazards models and adjusted penalized smoothing spline plots.ResultsOverall survival of NSCLC had putative U-shaped hazard ratio relationships with BMI based on spline plots: being underweight (BMI < 18.5 kg/m2; aHR = 1.56; 95% confidence interval [CI]:1.43-1.70) or morbidly overweight (BMI > 40 kg/m2; aHR = 1.09; 95% CI: 0.95-1.26) at the time of diagnosis was associated with worse stage-specific prognosis, whereas being overweight (25 kg/m2 ≤ BMI < 30 kg/m2; aHR = 0.89; 95% CI: 0.85-0.95) or obese (30 kg/m2 ≤ BMI ≤ 40 kg/m2; aHR = 0.86; 95% CI: 0.82-0.91) was associated with improved survival. Although not significant, a similar pattern was seen with SCLC. Compared with an increased or stable BMI from the period between young adulthood until date of diagnosis, a decreased BMI was associated with worse outcomes in NSCLC (aHR = 1.24; 95% CI: 1.2-1.3) and SCLC patients (aHR=1.26 (95% CI: 1.0-1.6). Decreased BMI was consistently associated with worse outcome, across clinicodemographic subsets.ConclusionsBoth being underweight or morbidly obese at time of diagnosis is associated with lower stage-specific survival in independent assessments of NSCLC and SCLC patients. In addition, a decrease in BMI at lung cancer diagnosis relative to early adulthood is a consistent marker of poor survival.

Published

2019

20. Phase II Study of Roniciclib in Combination with Cisplatin/Etoposide or Carboplatin/Etoposide as First-Line Therapy in Patients with Extensive-Disease Small Cell Lung Cancer

Author

Reck, M, Horn, L, Novello, S, Barlesi, F, Albert, I, Juhasz, E, Kowalski, D, Robinet, G, Cadranel, J, Bidoli, P, Chung, J, Fritsch, A, Drews, U, Wagner, A, Govindan, R, Reck M., Horn L., Novello S., Barlesi F., Albert I., Juhasz E., Kowalski D., Robinet G., Cadranel J., Bidoli P., Chung J., Fritsch A., Drews U., Wagner A., Govindan R., Reck, M, Horn, L, Novello, S, Barlesi, F, Albert, I, Juhasz, E, Kowalski, D, Robinet, G, Cadranel, J, Bidoli, P, Chung, J, Fritsch, A, Drews, U, Wagner, A, Govindan, R, Reck M., Horn L., Novello S., Barlesi F., Albert I., Juhasz E., Kowalski D., Robinet G., Cadranel J., Bidoli P., Chung J., Fritsch A., Drews U., Wagner A., and Govindan R.

Abstract

Introduction: This phase II study evaluated the efficacy and safety of the pan-cyclin–dependent kinase inhibitor roniciclib with platinum-based chemotherapy in patients with extensive-disease SCLC. Methods: In this randomized, double-blind study, unselected patients with previously untreated extensive-disease SCLC received roniciclib, 5 mg, or placebo twice daily according to a 3 days–on, 4 days–off schedule in 21-day cycles, with concomitant cisplatin or carboplatin on day 1 and etoposide on days 1 to 3. The primary end point was progression-free survival. Other end points included overall survival, objective response rate, and safety. Results: A total of 140 patients received treatment: 70 with roniciclib plus chemotherapy and 70 with placebo plus chemotherapy. Median progression-free survival times was 4.9 months (95% confidence interval [CI]: 4.2–5.5) with roniciclib plus chemotherapy and 5.5 months (95% CI: 4.6–5.6) with placebo plus chemotherapy (hazard ratio [HR] = 1.242, 95% CI: 0.820–1.881, p = 0.8653). Median overall survival times was 9.7 months (95% CI: 7.9–11.1) with roniciclib plus chemotherapy and 10.3 months (95% CI: 8.7–11.9) with placebo plus chemotherapy (HR = 1.281, 95% CI: 0.776–1.912, p = 0.7858). The objective response rates were 60.6% with roniciclib plus chemotherapy and 74.6% with placebo plus chemotherapy. Common treatment-emergent adverse events in both groups included nausea, vomiting, and fatigue. Serious treatment-emergent adverse events were more common with roniciclib plus chemotherapy (57.1%) than with placebo plus chemotherapy (38.6%). Conclusions: Roniciclib combined with chemotherapy demonstrated an unfavorable risk-benefit profile in patients with extensive-disease SCLC, and the study was prematurely terminated.

Published

2019

21. Reprogramming normal human epithelial tissues to a common, lethal neuroendocrine cancer lineage.

Author

Park, Jung Wook, Park, Jung Wook, Lee, John K, Sheu, Katherine M, Wang, Liang, Balanis, Nikolas G, Nguyen, Kim, Smith, Bryan A, Cheng, Chen, Tsai, Brandon L, Cheng, Donghui, Huang, Jiaoti, Kurdistani, Siavash K, Graeber, Thomas G, Witte, Owen N, Park, Jung Wook, Park, Jung Wook, Lee, John K, Sheu, Katherine M, Wang, Liang, Balanis, Nikolas G, Nguyen, Kim, Smith, Bryan A, Cheng, Chen, Tsai, Brandon L, Cheng, Donghui, Huang, Jiaoti, Kurdistani, Siavash K, Graeber, Thomas G, and Witte, Owen N

Abstract

The use of potent therapies inhibiting critical oncogenic pathways active in epithelial cancers has led to multiple resistance mechanisms, including the development of highly aggressive, small cell neuroendocrine carcinoma (SCNC). SCNC patients have a dismal prognosis due in part to a limited understanding of the molecular mechanisms driving this malignancy and the lack of effective treatments. Here, we demonstrate that a common set of defined oncogenic drivers reproducibly reprograms normal human prostate and lung epithelial cells to small cell prostate cancer (SCPC) and small cell lung cancer (SCLC), respectively. We identify shared active transcription factor binding regions in the reprogrammed prostate and lung SCNCs by integrative analyses of epigenetic and transcriptional landscapes. These results suggest that neuroendocrine cancers arising from distinct epithelial tissues may share common vulnerabilities that could be exploited for the development of drugs targeting SCNCs.

Published

2018

22. Integrative genomic profiling of large-cell neuroendocrine carcinomas reveals distinct subtypes of high-grade neuroendocrine lung tumors.

Author

George, Julie, George, Julie, Walter, Vonn, Peifer, Martin, Alexandrov, Ludmil B, Seidel, Danila, Leenders, Frauke, Maas, Lukas, Müller, Christian, Dahmen, Ilona, Delhomme, Tiffany M, Ardin, Maude, Leblay, Noemie, Byrnes, Graham, Sun, Ruping, De Reynies, Aurélien, McLeer-Florin, Anne, Bosco, Graziella, Malchers, Florian, Menon, Roopika, Altmüller, Janine, Becker, Christian, Nürnberg, Peter, Achter, Viktor, Lang, Ulrich, Schneider, Peter M, Bogus, Magdalena, Soloway, Matthew G, Wilkerson, Matthew D, Cun, Yupeng, McKay, James D, Moro-Sibilot, Denis, Brambilla, Christian G, Lantuejoul, Sylvie, Lemaitre, Nicolas, Soltermann, Alex, Weder, Walter, Tischler, Verena, Brustugun, Odd Terje, Lund-Iversen, Marius, Helland, Åslaug, Solberg, Steinar, Ansén, Sascha, Wright, Gavin, Solomon, Benjamin, Roz, Luca, Pastorino, Ugo, Petersen, Iver, Clement, Joachim H, Sänger, Jörg, Wolf, Jürgen, Vingron, Martin, Zander, Thomas, Perner, Sven, Travis, William D, Haas, Stefan A, Olivier, Magali, Foll, Matthieu, Büttner, Reinhard, Hayes, David Neil, Brambilla, Elisabeth, Fernandez-Cuesta, Lynnette, Thomas, Roman K, George, Julie, George, Julie, Walter, Vonn, Peifer, Martin, Alexandrov, Ludmil B, Seidel, Danila, Leenders, Frauke, Maas, Lukas, Müller, Christian, Dahmen, Ilona, Delhomme, Tiffany M, Ardin, Maude, Leblay, Noemie, Byrnes, Graham, Sun, Ruping, De Reynies, Aurélien, McLeer-Florin, Anne, Bosco, Graziella, Malchers, Florian, Menon, Roopika, Altmüller, Janine, Becker, Christian, Nürnberg, Peter, Achter, Viktor, Lang, Ulrich, Schneider, Peter M, Bogus, Magdalena, Soloway, Matthew G, Wilkerson, Matthew D, Cun, Yupeng, McKay, James D, Moro-Sibilot, Denis, Brambilla, Christian G, Lantuejoul, Sylvie, Lemaitre, Nicolas, Soltermann, Alex, Weder, Walter, Tischler, Verena, Brustugun, Odd Terje, Lund-Iversen, Marius, Helland, Åslaug, Solberg, Steinar, Ansén, Sascha, Wright, Gavin, Solomon, Benjamin, Roz, Luca, Pastorino, Ugo, Petersen, Iver, Clement, Joachim H, Sänger, Jörg, Wolf, Jürgen, Vingron, Martin, Zander, Thomas, Perner, Sven, Travis, William D, Haas, Stefan A, Olivier, Magali, Foll, Matthieu, Büttner, Reinhard, Hayes, David Neil, Brambilla, Elisabeth, Fernandez-Cuesta, Lynnette, and Thomas, Roman K

Abstract

Pulmonary large-cell neuroendocrine carcinomas (LCNECs) have similarities with other lung cancers, but their precise relationship has remained unclear. Here we perform a comprehensive genomic (n = 60) and transcriptomic (n = 69) analysis of 75 LCNECs and identify two molecular subgroups: "type I LCNECs" with bi-allelic TP53 and STK11/KEAP1 alterations (37%), and "type II LCNECs" enriched for bi-allelic inactivation of TP53 and RB1 (42%). Despite sharing genomic alterations with adenocarcinomas and squamous cell carcinomas, no transcriptional relationship was found; instead LCNECs form distinct transcriptional subgroups with closest similarity to SCLC. While type I LCNECs and SCLCs exhibit a neuroendocrine profile with ASCL1high/DLL3high/NOTCHlow, type II LCNECs bear TP53 and RB1 alterations and differ from most SCLC tumors with reduced neuroendocrine markers, a pattern of ASCL1low/DLL3low/NOTCHhigh, and an upregulation of immune-related pathways. In conclusion, LCNECs comprise two molecularly defined subgroups, and distinguishing them from SCLC may allow stratified targeted treatment of high-grade neuroendocrine lung tumors.

Published

2018

23. Reprogramming normal human epithelial tissues to a common, lethal neuroendocrine cancer lineage.

Author

Park, Jung Wook, Park, Jung Wook, Lee, John K, Sheu, Katherine M, Wang, Liang, Balanis, Nikolas G, Nguyen, Kim, Smith, Bryan A, Cheng, Chen, Tsai, Brandon L, Cheng, Donghui, Huang, Jiaoti, Kurdistani, Siavash K, Graeber, Thomas G, Witte, Owen N, Park, Jung Wook, Park, Jung Wook, Lee, John K, Sheu, Katherine M, Wang, Liang, Balanis, Nikolas G, Nguyen, Kim, Smith, Bryan A, Cheng, Chen, Tsai, Brandon L, Cheng, Donghui, Huang, Jiaoti, Kurdistani, Siavash K, Graeber, Thomas G, and Witte, Owen N

Abstract

The use of potent therapies inhibiting critical oncogenic pathways active in epithelial cancers has led to multiple resistance mechanisms, including the development of highly aggressive, small cell neuroendocrine carcinoma (SCNC). SCNC patients have a dismal prognosis due in part to a limited understanding of the molecular mechanisms driving this malignancy and the lack of effective treatments. Here, we demonstrate that a common set of defined oncogenic drivers reproducibly reprograms normal human prostate and lung epithelial cells to small cell prostate cancer (SCPC) and small cell lung cancer (SCLC), respectively. We identify shared active transcription factor binding regions in the reprogrammed prostate and lung SCNCs by integrative analyses of epigenetic and transcriptional landscapes. These results suggest that neuroendocrine cancers arising from distinct epithelial tissues may share common vulnerabilities that could be exploited for the development of drugs targeting SCNCs.

Published

2018

24. Reprogramming normal human epithelial tissues to a common, lethal neuroendocrine cancer lineage.

Author

Park, Jung Wook, Park, Jung Wook, Lee, John K, Sheu, Katherine M, Wang, Liang, Balanis, Nikolas G, Nguyen, Kim, Smith, Bryan A, Cheng, Chen, Tsai, Brandon L, Cheng, Donghui, Huang, Jiaoti, Kurdistani, Siavash K, Graeber, Thomas G, Witte, Owen N, Park, Jung Wook, Park, Jung Wook, Lee, John K, Sheu, Katherine M, Wang, Liang, Balanis, Nikolas G, Nguyen, Kim, Smith, Bryan A, Cheng, Chen, Tsai, Brandon L, Cheng, Donghui, Huang, Jiaoti, Kurdistani, Siavash K, Graeber, Thomas G, and Witte, Owen N

Abstract

The use of potent therapies inhibiting critical oncogenic pathways active in epithelial cancers has led to multiple resistance mechanisms, including the development of highly aggressive, small cell neuroendocrine carcinoma (SCNC). SCNC patients have a dismal prognosis due in part to a limited understanding of the molecular mechanisms driving this malignancy and the lack of effective treatments. Here, we demonstrate that a common set of defined oncogenic drivers reproducibly reprograms normal human prostate and lung epithelial cells to small cell prostate cancer (SCPC) and small cell lung cancer (SCLC), respectively. We identify shared active transcription factor binding regions in the reprogrammed prostate and lung SCNCs by integrative analyses of epigenetic and transcriptional landscapes. These results suggest that neuroendocrine cancers arising from distinct epithelial tissues may share common vulnerabilities that could be exploited for the development of drugs targeting SCNCs.

Published

2018

25. Integrative genomic profiling of large-cell neuroendocrine carcinomas reveals distinct subtypes of high-grade neuroendocrine lung tumors.

Author

George, Julie, George, Julie, Walter, Vonn, Peifer, Martin, Alexandrov, Ludmil B, Seidel, Danila, Leenders, Frauke, Maas, Lukas, Müller, Christian, Dahmen, Ilona, Delhomme, Tiffany M, Ardin, Maude, Leblay, Noemie, Byrnes, Graham, Sun, Ruping, De Reynies, Aurélien, McLeer-Florin, Anne, Bosco, Graziella, Malchers, Florian, Menon, Roopika, Altmüller, Janine, Becker, Christian, Nürnberg, Peter, Achter, Viktor, Lang, Ulrich, Schneider, Peter M, Bogus, Magdalena, Soloway, Matthew G, Wilkerson, Matthew D, Cun, Yupeng, McKay, James D, Moro-Sibilot, Denis, Brambilla, Christian G, Lantuejoul, Sylvie, Lemaitre, Nicolas, Soltermann, Alex, Weder, Walter, Tischler, Verena, Brustugun, Odd Terje, Lund-Iversen, Marius, Helland, Åslaug, Solberg, Steinar, Ansén, Sascha, Wright, Gavin, Solomon, Benjamin, Roz, Luca, Pastorino, Ugo, Petersen, Iver, Clement, Joachim H, Sänger, Jörg, Wolf, Jürgen, Vingron, Martin, Zander, Thomas, Perner, Sven, Travis, William D, Haas, Stefan A, Olivier, Magali, Foll, Matthieu, Büttner, Reinhard, Hayes, David Neil, Brambilla, Elisabeth, Fernandez-Cuesta, Lynnette, Thomas, Roman K, George, Julie, George, Julie, Walter, Vonn, Peifer, Martin, Alexandrov, Ludmil B, Seidel, Danila, Leenders, Frauke, Maas, Lukas, Müller, Christian, Dahmen, Ilona, Delhomme, Tiffany M, Ardin, Maude, Leblay, Noemie, Byrnes, Graham, Sun, Ruping, De Reynies, Aurélien, McLeer-Florin, Anne, Bosco, Graziella, Malchers, Florian, Menon, Roopika, Altmüller, Janine, Becker, Christian, Nürnberg, Peter, Achter, Viktor, Lang, Ulrich, Schneider, Peter M, Bogus, Magdalena, Soloway, Matthew G, Wilkerson, Matthew D, Cun, Yupeng, McKay, James D, Moro-Sibilot, Denis, Brambilla, Christian G, Lantuejoul, Sylvie, Lemaitre, Nicolas, Soltermann, Alex, Weder, Walter, Tischler, Verena, Brustugun, Odd Terje, Lund-Iversen, Marius, Helland, Åslaug, Solberg, Steinar, Ansén, Sascha, Wright, Gavin, Solomon, Benjamin, Roz, Luca, Pastorino, Ugo, Petersen, Iver, Clement, Joachim H, Sänger, Jörg, Wolf, Jürgen, Vingron, Martin, Zander, Thomas, Perner, Sven, Travis, William D, Haas, Stefan A, Olivier, Magali, Foll, Matthieu, Büttner, Reinhard, Hayes, David Neil, Brambilla, Elisabeth, Fernandez-Cuesta, Lynnette, and Thomas, Roman K

Abstract

Pulmonary large-cell neuroendocrine carcinomas (LCNECs) have similarities with other lung cancers, but their precise relationship has remained unclear. Here we perform a comprehensive genomic (n = 60) and transcriptomic (n = 69) analysis of 75 LCNECs and identify two molecular subgroups: "type I LCNECs" with bi-allelic TP53 and STK11/KEAP1 alterations (37%), and "type II LCNECs" enriched for bi-allelic inactivation of TP53 and RB1 (42%). Despite sharing genomic alterations with adenocarcinomas and squamous cell carcinomas, no transcriptional relationship was found; instead LCNECs form distinct transcriptional subgroups with closest similarity to SCLC. While type I LCNECs and SCLCs exhibit a neuroendocrine profile with ASCL1high/DLL3high/NOTCHlow, type II LCNECs bear TP53 and RB1 alterations and differ from most SCLC tumors with reduced neuroendocrine markers, a pattern of ASCL1low/DLL3low/NOTCHhigh, and an upregulation of immune-related pathways. In conclusion, LCNECs comprise two molecularly defined subgroups, and distinguishing them from SCLC may allow stratified targeted treatment of high-grade neuroendocrine lung tumors.

Published

2018

26. Clinical predictors of survival in young patients with small cell lung cancer: Results from the California Cancer Registry.

Author

Lara, Joshua D, Lara, Joshua D, Brunson, Ann, Riess, Jonathan W, Kelly, Karen, Lara, Primo N, Gandara, David R, Lara, Joshua D, Lara, Joshua D, Brunson, Ann, Riess, Jonathan W, Kelly, Karen, Lara, Primo N, and Gandara, David R

Abstract

BACKGROUND:Small cell lung cancer (SCLC) is an often lethal disease that commonly occurs in older individuals with a history of heavy tobacco use. Limited epidemiologic and outcomes data are available on young SCLC patients aged less than 50 years of age. We assessed clinical variables related to cause specific survival (CSS) of young patients with SCLC. METHODS:SCLC patients in the California Cancer Registry diagnosed between 1998 and 2012 were included. Primary outcome measure was CSS. Hazard ratios (HR) for CSS were calculated using Cox Proportional Hazards (pH) models for all ages & for patients <50 years, adjusted for baseline variables: age, gender, stage, race, year of diagnosis, initial treatment, socioeconomic status (SES), and location (urban vs. rural). RESULTS:We identified 22,863 SCLC patients, of which 975 were less than 50 years of age (4.2%). Most patients <50years of age were male (51%), white race (71%), and had stage IV disease (60%). A lower proportion of patients aged 50 years or younger was diagnosed in later years: from 40% in 1998-2002 to 24% in 2008-2012. For all SCLC patients, age less than 50 years was an independent predictor of improved CSS (HR=0.82, p<0.0001). Multivariate Cox pH models showed that in younger patients, female sex (HR=0.81, p=0.0045), Asian race (HR=0.57, p=0.0075), and rural residence (HR=0.75, p=0.042) were associated with better CSS, among other variables. CONCLUSIONS:In patients with SCLC, age less than 50 years was an independent predictor of improved CSS. Baseline clinical variables associated with better CSS were identified. These results have potential clinical applications.

Published

2017

27. Prognostic and predictive value of circulating tumor cells and CXCR4 expression as biomarkers for a CXCR4 peptide antagonist in combination with carboplatin-etoposide in small cell lung cancer: exploratory analysis of a phase II study.

Author

Salgia, Ravi, Salgia, Ravi, Weaver, R Waide, McCleod, Michael, Stille, John R, Yan, S Betty, Roberson, Stephanie, Polzer, John, Flynt, Amy, Raddad, Eyas, Peek, Victoria L, Wijayawardana, Sameera R, Um, Suzane L, Gross, Steve, Connelly, Mark C, Morano, Carrie, Repollet, Madeline, Sanders, Renouard, Baeten, Kurt, D'Haese, David, Spigel, David R, Salgia, Ravi, Salgia, Ravi, Weaver, R Waide, McCleod, Michael, Stille, John R, Yan, S Betty, Roberson, Stephanie, Polzer, John, Flynt, Amy, Raddad, Eyas, Peek, Victoria L, Wijayawardana, Sameera R, Um, Suzane L, Gross, Steve, Connelly, Mark C, Morano, Carrie, Repollet, Madeline, Sanders, Renouard, Baeten, Kurt, D'Haese, David, and Spigel, David R

Abstract

Background Circulating tumor cells (CTCs) and chemokine (C-X-C motif) receptor 4 (CXCR4) expression in CTCs and tumor tissue were evaluated as prognostic or predictive markers of CXCR4 peptide antagonist LY2510924 plus carboplatin-etoposide (CE) versus CE in extensive-stage disease small cell lung cancer (ED-SCLC). Methods This exploratory analysis of a phase II study evaluated CXCR4 expression in baseline tumor tissue and peripheral blood CTCs and in post-treatment CTCs. Optimum cutoff values were determined for CTC counts and CXCR4 expression in tumors and CTCs as predictors of survival outcome. Kaplan-Meier estimates and hazard ratios were used to determine biomarker prognostic and predictive values. Results There was weak positive correlation at baseline between CXCR4 expression in tumor tissue and CTCs. Optimum cutoff values were H-score ≥ 210 for CXCR4+ tumor, ≥7% CTCs with CXCR4 expression (CXCR4+ CTCs), and ≥6 CTCs/7.5 mL blood. Baseline H-score for CXCR4+ tumor was not prognostic of progression-free survival (PFS) or overall survival (OS). Baseline CXCR4+ CTCs ≥7% was prognostic of shorter PFS. CTCs ≥6 at baseline and cycle 2, day 1 were prognostic of shorter PFS and OS. None of the biomarkers at their respective optimum cutoffs was predictive of treatment response of LY2510924 plus CE versus CE. Conclusions In patients with ED-SCLC, baseline CXCR4 expression in tumor tissue was not prognostic of survival or predictive of LY2510924 treatment response. Baseline CXCR4+ CTCs ≥7% was prognostic of shorter PFS. CTC count ≥6 at baseline and after 1 cycle of treatment were prognostic of shorter PFS and OS.

Published

2017

28. Prognostic and predictive value of circulating tumor cells and CXCR4 expression as biomarkers for a CXCR4 peptide antagonist in combination with carboplatin-etoposide in small cell lung cancer: exploratory analysis of a phase II study.

Author

Salgia, Ravi, Salgia, Ravi, Weaver, R Waide, McCleod, Michael, Stille, John R, Yan, S Betty, Roberson, Stephanie, Polzer, John, Flynt, Amy, Raddad, Eyas, Peek, Victoria L, Wijayawardana, Sameera R, Um, Suzane L, Gross, Steve, Connelly, Mark C, Morano, Carrie, Repollet, Madeline, Sanders, Renouard, Baeten, Kurt, D'Haese, David, Spigel, David R, Salgia, Ravi, Salgia, Ravi, Weaver, R Waide, McCleod, Michael, Stille, John R, Yan, S Betty, Roberson, Stephanie, Polzer, John, Flynt, Amy, Raddad, Eyas, Peek, Victoria L, Wijayawardana, Sameera R, Um, Suzane L, Gross, Steve, Connelly, Mark C, Morano, Carrie, Repollet, Madeline, Sanders, Renouard, Baeten, Kurt, D'Haese, David, and Spigel, David R

Abstract

Background Circulating tumor cells (CTCs) and chemokine (C-X-C motif) receptor 4 (CXCR4) expression in CTCs and tumor tissue were evaluated as prognostic or predictive markers of CXCR4 peptide antagonist LY2510924 plus carboplatin-etoposide (CE) versus CE in extensive-stage disease small cell lung cancer (ED-SCLC). Methods This exploratory analysis of a phase II study evaluated CXCR4 expression in baseline tumor tissue and peripheral blood CTCs and in post-treatment CTCs. Optimum cutoff values were determined for CTC counts and CXCR4 expression in tumors and CTCs as predictors of survival outcome. Kaplan-Meier estimates and hazard ratios were used to determine biomarker prognostic and predictive values. Results There was weak positive correlation at baseline between CXCR4 expression in tumor tissue and CTCs. Optimum cutoff values were H-score ≥ 210 for CXCR4+ tumor, ≥7% CTCs with CXCR4 expression (CXCR4+ CTCs), and ≥6 CTCs/7.5 mL blood. Baseline H-score for CXCR4+ tumor was not prognostic of progression-free survival (PFS) or overall survival (OS). Baseline CXCR4+ CTCs ≥7% was prognostic of shorter PFS. CTCs ≥6 at baseline and cycle 2, day 1 were prognostic of shorter PFS and OS. None of the biomarkers at their respective optimum cutoffs was predictive of treatment response of LY2510924 plus CE versus CE. Conclusions In patients with ED-SCLC, baseline CXCR4 expression in tumor tissue was not prognostic of survival or predictive of LY2510924 treatment response. Baseline CXCR4+ CTCs ≥7% was prognostic of shorter PFS. CTC count ≥6 at baseline and after 1 cycle of treatment were prognostic of shorter PFS and OS.

Published

2017

29. Clinical predictors of survival in young patients with small cell lung cancer: Results from the California Cancer Registry.

Author

Lara, Joshua D, Lara, Joshua D, Brunson, Ann, Riess, Jonathan W, Kelly, Karen, Lara, Primo N, Gandara, David R, Lara, Joshua D, Lara, Joshua D, Brunson, Ann, Riess, Jonathan W, Kelly, Karen, Lara, Primo N, and Gandara, David R

Abstract

BACKGROUND:Small cell lung cancer (SCLC) is an often lethal disease that commonly occurs in older individuals with a history of heavy tobacco use. Limited epidemiologic and outcomes data are available on young SCLC patients aged less than 50 years of age. We assessed clinical variables related to cause specific survival (CSS) of young patients with SCLC. METHODS:SCLC patients in the California Cancer Registry diagnosed between 1998 and 2012 were included. Primary outcome measure was CSS. Hazard ratios (HR) for CSS were calculated using Cox Proportional Hazards (pH) models for all ages & for patients <50 years, adjusted for baseline variables: age, gender, stage, race, year of diagnosis, initial treatment, socioeconomic status (SES), and location (urban vs. rural). RESULTS:We identified 22,863 SCLC patients, of which 975 were less than 50 years of age (4.2%). Most patients <50years of age were male (51%), white race (71%), and had stage IV disease (60%). A lower proportion of patients aged 50 years or younger was diagnosed in later years: from 40% in 1998-2002 to 24% in 2008-2012. For all SCLC patients, age less than 50 years was an independent predictor of improved CSS (HR=0.82, p<0.0001). Multivariate Cox pH models showed that in younger patients, female sex (HR=0.81, p=0.0045), Asian race (HR=0.57, p=0.0075), and rural residence (HR=0.75, p=0.042) were associated with better CSS, among other variables. CONCLUSIONS:In patients with SCLC, age less than 50 years was an independent predictor of improved CSS. Baseline clinical variables associated with better CSS were identified. These results have potential clinical applications.

Published

2017

30. Randomized Phase II Study Comparing Prophylactic Cranial Irradiation Alone to Prophylactic Cranial Irradiation and Consolidative Extracranial Irradiation for Extensive-Disease Small Cell Lung Cancer (ED SCLC): NRG Oncology RTOG 0937.

Author

Gore, Elizabeth M, Gore, Elizabeth M, Hu, Chen, Sun, Alexander Y, Grimm, Daniel F, Ramalingam, Suresh S, Dunlap, Neal E, Higgins, Kristin A, Werner-Wasik, Maria, Allen, Aaron M, Iyengar, Puneeth, Videtic, Gregory MM, Hales, Russell K, McGarry, Ronald C, Urbanic, James J, Pu, Anthony T, Johnstone, Candice A, Stieber, Volker W, Paulus, Rebecca, Bradley, Jeffrey D, Gore, Elizabeth M, Gore, Elizabeth M, Hu, Chen, Sun, Alexander Y, Grimm, Daniel F, Ramalingam, Suresh S, Dunlap, Neal E, Higgins, Kristin A, Werner-Wasik, Maria, Allen, Aaron M, Iyengar, Puneeth, Videtic, Gregory MM, Hales, Russell K, McGarry, Ronald C, Urbanic, James J, Pu, Anthony T, Johnstone, Candice A, Stieber, Volker W, Paulus, Rebecca, and Bradley, Jeffrey D

Abstract

IntroductionNRG Oncology RTOG 0937 is a randomized phase II trial evaluating 1-year overall survival (OS) with prophylactic cranial irradiation (PCI) or PCI plus consolidative radiation therapy (PCI+cRT) to intrathoracic disease and extracranial metastases for extensive-disease SCLC.MethodsPatients with one to four extracranial metastases were eligible after a complete response or partial response to chemotherapy. Randomization was to PCI or PCI+cRT to the thorax and metastases. Original stratification included partial response versus complete response after chemotherapy and one versus two to four metastases; age younger than 65 years versus 65 years or older was added after an observed imbalance. PCI consisted of 25 Gy in 10 fractions. cRT consisted of 45 Gy in 15 fractions. To detect an improvement in OS from 30% to 45% with a 34% hazard reduction (hazard ratio = 0.66) under a 0.1 type 1 error (one sided) and 80% power, 154 patients were required.ResultsA total of 97 patients were randomized between March 2010 and February 2015. Eleven patients were ineligible (nine in the PCI group and two in the PCI+cRT group), leaving 42 randomized to receive PCI and 44 to receive PCI+cRT. At planned interim analysis, the study crossed the futility boundary for OS and was closed before meeting the accrual target. Median follow-up was 9 months. The 1-year OS was not different between the groups: 60.1% (95% confidence interval [CI]: 41.2-74.7) for PCI and 50.8% (95% CI: 34.0-65.3) for PCI+cRT (p = 0.21). The 3- and 12-month rates of progression were 53.3% and 79.6% for PCI and 14.5% and 75% for PCI+cRT, respectively. Time to progression favored PCI+cRT (hazard ratio = 0.53, 95% CI: 0.32-0.87, p = 0.01). One patient in each arm had grade 4 therapy-related toxicity and one had grade 5 therapy-related pneumonitis with PCI+cRT.ConclusionsOS exceeded predictions for both arms. cRT delayed progression but did not improve 1-year OS.

Published

2017

31. Lung neuroendocrine tumours: deep sequencing of the four World Health Organization histotypes reveals chromatin-remodelling genes as major players and a prognostic role for TERT, RB1, MEN1 and KMT2D

Author

Simbolo, M., Mafficini, A., Sikora, K. O., Fassan, M., Barbi, S., Corbo, V., Mastracci, L., Rusev, B., Grillo, F., Vicentini, C., Ferrara, R., Pilotto, S., Davini, F., Pelosi, Gabriele, Lawlor, R. T., Chilosi, M., Tortora, Giampaolo, Bria, Emilio, Fontanini, G., Volante, M., Scarpa, A., Pelosi G., Tortora G. (ORCID:0000-0002-1378-4962), Bria E. (ORCID:0000-0002-2333-704X), Simbolo, M., Mafficini, A., Sikora, K. O., Fassan, M., Barbi, S., Corbo, V., Mastracci, L., Rusev, B., Grillo, F., Vicentini, C., Ferrara, R., Pilotto, S., Davini, F., Pelosi, Gabriele, Lawlor, R. T., Chilosi, M., Tortora, Giampaolo, Bria, Emilio, Fontanini, G., Volante, M., Scarpa, A., Pelosi G., Tortora G. (ORCID:0000-0002-1378-4962), and Bria E. (ORCID:0000-0002-2333-704X)

Abstract

Next-generation sequencing (NGS) was applied to 148 lung neuroendocrine tumours (LNETs) comprising the four World Health Organization classification categories: 53 typical carcinoid (TCs), 35 atypical carcinoid (ACs), 27 large-cell neuroendocrine carcinomas, and 33 small-cell lung carcinomas. A discovery screen was conducted on 46 samples by the use of whole-exome sequencing and high-coverage targeted sequencing of 418 genes. Eighty-eight recurrently mutated genes from both the discovery screen and current literature were verified in the 46 cases of the discovery screen, and validated on additional 102 LNETs by targeted NGS; their prevalence was then evaluated on the whole series. Thirteen of these 88 genes were also evaluated for copy number alterations (CNAs). Carcinoids and carcinomas shared most of the altered genes but with different prevalence rates. When mutations and copy number changes were combined, MEN1 alterations were almost exclusive to carcinoids, whereas alterations of TP53 and RB1 cell cycle regulation genes and PI3K/AKT/mTOR pathway genes were significantly enriched in carcinomas. Conversely, mutations in chromatin-remodelling genes, including those encoding histone modifiers and members of SWI–SNF complexes, were found at similar rates in carcinoids (45.5%) and carcinomas (55.0%), suggesting a major role in LNET pathogenesis. One AC and one TC showed a hypermutated profile associated with a POLQ damaging mutation. There were fewer CNAs in carcinoids than in carcinomas; however ACs showed a hybrid pattern, whereby gains of TERT, SDHA, RICTOR, PIK3CA, MYCL and SRC were found at rates similar to those in carcinomas, whereas the MEN1 loss rate mirrored that of TCs. Multivariate survival analysis revealed RB1 mutation (p = 0.0005) and TERT copy gain (p = 0.016) as independent predictors of poorer prognosis. MEN1 mutation was associated with poor prognosis in AC (p = 0.0045), whereas KMT2D mutation correlated with longer survival in SCLC (p = 0.0022). I

Published

2017

32. Isoaspartylation appears to trigger small cell lung cancer-associated autoimmunity against neuronal protein ELAVL4.

Author

Pulido, Mario A, Pulido, Mario A, DerHartunian, Meleeneh Kazarian, Qin, Zhenxia, Chung, Eric M, Kang, Diane S, Woodham, Andrew W, Tsou, Jeffrey A, Klooster, Rinse, Akbari, Omid, Wang, Lina, Kast, W Martin, Liu, Stephen V, Verschuuren, Jan JGM, Aswad, Dana W, Laird-Offringa, Ite A, Pulido, Mario A, Pulido, Mario A, DerHartunian, Meleeneh Kazarian, Qin, Zhenxia, Chung, Eric M, Kang, Diane S, Woodham, Andrew W, Tsou, Jeffrey A, Klooster, Rinse, Akbari, Omid, Wang, Lina, Kast, W Martin, Liu, Stephen V, Verschuuren, Jan JGM, Aswad, Dana W, and Laird-Offringa, Ite A

Abstract

Autoantibodies against SCLC-associated neuronal antigen ELAVL4 (HuD) have been linked to smaller tumors and improved survival, but the antigenic epitope and mechanism of autoimmunity have never been solved. We report that recombinant human ELAVL4 protein incubated under physiological conditions acquires isoaspartylation, a type of immunogenic protein damage. Specifically, the N-terminal region of ELAVL4, previously implicated in SCLC-associated autoimmunity, undergoes isoaspartylation in vitro, is recognized by sera from anti-ELAVL4 positive SCLC patients and is highly immunogenic in subcutaneously injected mice and in vitro stimulated human lymphocytes. Our data suggest that isoaspartylated ELAVL4 is the trigger for the SCLC-associated anti-ELAVL4 autoimmune response.

Published

2016

33. Theory Meets Practice for Immune Checkpoint Blockade in Small-Cell Lung Cancer.

Author

Riess, Jonathan W, Riess, Jonathan W, Lara, Primo N, Gandara, David R, Riess, Jonathan W, Riess, Jonathan W, Lara, Primo N, and Gandara, David R

Published

2016

34. Differences in Active and Passive Smoking Exposures and Lung Cancer Incidence Between Veterans and Non-Veterans in the Women's Health Initiative.

Author

Bastian, Lori A, Bastian, Lori A, Gray, Kristen E, DeRycke, Eric, Mirza, Shireen, Gierisch, Jennifer M, Haskell, Sally G, Magruder, Kathryn M, Wakelee, Heather A, Wang, Ange, Ho, Gloria YF, LaCroix, Andrea Z, Bastian, Lori A, Bastian, Lori A, Gray, Kristen E, DeRycke, Eric, Mirza, Shireen, Gierisch, Jennifer M, Haskell, Sally G, Magruder, Kathryn M, Wakelee, Heather A, Wang, Ange, Ho, Gloria YF, and LaCroix, Andrea Z

Abstract

IntroductionWomen Veterans may have higher rates of both active and passive tobacco exposure than their civilian counterparts, thereby increasing their risk for lung cancer.Purpose of the studyTo compare differences in active and passive smoking exposure and lung cancer incidence among women Veterans and non-Veterans using prospective data from the Women's Health Initiative (WHI).Design and methodsWe used data from the WHI, which collected longitudinal demographic, clinical, and laboratory data on 161,808 postmenopausal women. We employed linear and multinomial regression and generalized linear models to compare active and passive smoking exposure between Veterans and non-Veterans and Cox proportional hazards models to estimate differences in lung cancer incidence rates.ResultsAfter adjustment, Veterans had 2.54 additional pack years of smoking compared with non-Veterans (95% confidence interval [CI] 1.68, 3.40). Veterans also had a 1% increase in risk of any passive smoking exposure (95% CI 1.00, 1.02) and a 9% increase in risk of any workplace exposure (95% CI 1.07, 1.11) compared with non-Veterans. After adjustment for age and smoking exposures, Veterans did not have a higher risk of lung cancer compared with non-Veterans (relative risk = 1.06 95% CI 0.86, 1.30).ImplicationsWomen Veterans had higher rates of tobacco use and exposure to passive smoking, which were associated with a higher risk for lung cancer compared with non-Veterans. Clinicians who care for Veterans need to be aware that older women Veterans have more exposures to risk factors for lung cancer.

Published

2016

35. Theory Meets Practice for Immune Checkpoint Blockade in Small-Cell Lung Cancer.

Author

Riess, Jonathan W, Riess, Jonathan W, Lara, Primo N, Gandara, David R, Riess, Jonathan W, Riess, Jonathan W, Lara, Primo N, and Gandara, David R

Published

2016

36. Isoaspartylation appears to trigger small cell lung cancer-associated autoimmunity against neuronal protein ELAVL4.

Author

Pulido, Mario A, Pulido, Mario A, DerHartunian, Meleeneh Kazarian, Qin, Zhenxia, Chung, Eric M, Kang, Diane S, Woodham, Andrew W, Tsou, Jeffrey A, Klooster, Rinse, Akbari, Omid, Wang, Lina, Kast, W Martin, Liu, Stephen V, Verschuuren, Jan JGM, Aswad, Dana W, Laird-Offringa, Ite A, Pulido, Mario A, Pulido, Mario A, DerHartunian, Meleeneh Kazarian, Qin, Zhenxia, Chung, Eric M, Kang, Diane S, Woodham, Andrew W, Tsou, Jeffrey A, Klooster, Rinse, Akbari, Omid, Wang, Lina, Kast, W Martin, Liu, Stephen V, Verschuuren, Jan JGM, Aswad, Dana W, and Laird-Offringa, Ite A

Abstract

Autoantibodies against SCLC-associated neuronal antigen ELAVL4 (HuD) have been linked to smaller tumors and improved survival, but the antigenic epitope and mechanism of autoimmunity have never been solved. We report that recombinant human ELAVL4 protein incubated under physiological conditions acquires isoaspartylation, a type of immunogenic protein damage. Specifically, the N-terminal region of ELAVL4, previously implicated in SCLC-associated autoimmunity, undergoes isoaspartylation in vitro, is recognized by sera from anti-ELAVL4 positive SCLC patients and is highly immunogenic in subcutaneously injected mice and in vitro stimulated human lymphocytes. Our data suggest that isoaspartylated ELAVL4 is the trigger for the SCLC-associated anti-ELAVL4 autoimmune response.

Published

2016

37. New and emerging developments in extensive-stage small cell lung cancer therapeutics.

Author

Parikh, Mamta, Parikh, Mamta, Riess, Jonathan, Lara, Primo N, Parikh, Mamta, Parikh, Mamta, Riess, Jonathan, and Lara, Primo N

Abstract

Purpose of reviewExtensive-stage small cell lung cancer (ES-SCLC) remains a disease with a dismal prognosis, with median survival of approximately 8-10 months. Despite many attempts to develop effective systemic therapies, very little progress has been made in the last several decades. Platinum-based combination chemotherapy remains the standard of care in the first-line setting and is associated with high response rates albeit short-lived. However, there have been recent advances in the use of radiation therapy, as well as new insights into the biology of SCLC.Recent findingsSome of the most appreciable advances in the last decade have involved the use of local radiation therapy. With the use of new laboratory techniques such as genomic sequencing, there remains promise of rationally targeted drug development. Circulating tumor cell research may also provide insights to SCLC biology and further refine treatment.SummarySystemic therapy for SCLC has changed little over the past 30 years with the most significant advances in ES-SCLC relating to radiotherapy rather than systemic therapy. The effectiveness of prophylactic cranial irradiation and thoracic radiotherapy has renewed interest in therapeutics focused on the modulation of DNA damage or repair. Recent developments in genomic sequencing and immunotherapy may translate to new treatment paradigms for SCLC.

Published

2016

38. Differences in Active and Passive Smoking Exposures and Lung Cancer Incidence Between Veterans and Non-Veterans in the Women's Health Initiative.

Author

Bastian, Lori A, Bastian, Lori A, Gray, Kristen E, DeRycke, Eric, Mirza, Shireen, Gierisch, Jennifer M, Haskell, Sally G, Magruder, Kathryn M, Wakelee, Heather A, Wang, Ange, Ho, Gloria YF, LaCroix, Andrea Z, Bastian, Lori A, Bastian, Lori A, Gray, Kristen E, DeRycke, Eric, Mirza, Shireen, Gierisch, Jennifer M, Haskell, Sally G, Magruder, Kathryn M, Wakelee, Heather A, Wang, Ange, Ho, Gloria YF, and LaCroix, Andrea Z

Abstract

IntroductionWomen Veterans may have higher rates of both active and passive tobacco exposure than their civilian counterparts, thereby increasing their risk for lung cancer.Purpose of the studyTo compare differences in active and passive smoking exposure and lung cancer incidence among women Veterans and non-Veterans using prospective data from the Women's Health Initiative (WHI).Design and methodsWe used data from the WHI, which collected longitudinal demographic, clinical, and laboratory data on 161,808 postmenopausal women. We employed linear and multinomial regression and generalized linear models to compare active and passive smoking exposure between Veterans and non-Veterans and Cox proportional hazards models to estimate differences in lung cancer incidence rates.ResultsAfter adjustment, Veterans had 2.54 additional pack years of smoking compared with non-Veterans (95% confidence interval [CI] 1.68, 3.40). Veterans also had a 1% increase in risk of any passive smoking exposure (95% CI 1.00, 1.02) and a 9% increase in risk of any workplace exposure (95% CI 1.07, 1.11) compared with non-Veterans. After adjustment for age and smoking exposures, Veterans did not have a higher risk of lung cancer compared with non-Veterans (relative risk = 1.06 95% CI 0.86, 1.30).ImplicationsWomen Veterans had higher rates of tobacco use and exposure to passive smoking, which were associated with a higher risk for lung cancer compared with non-Veterans. Clinicians who care for Veterans need to be aware that older women Veterans have more exposures to risk factors for lung cancer.

Published

2016

39. Nfib Promotes Metastasis through a Widespread Increase in Chromatin Accessibility.

Author

Denny, Sarah K, Denny, Sarah K, Yang, Dian, Chuang, Chen-Hua, Brady, Jennifer J, Lim, Jing Shan, Grüner, Barbara M, Chiou, Shin-Heng, Schep, Alicia N, Baral, Jessika, Hamard, Cécile, Antoine, Martine, Wislez, Marie, Kong, Christina S, Connolly, Andrew J, Park, Kwon-Sik, Sage, Julien, Greenleaf, William J, Winslow, Monte M, Denny, Sarah K, Denny, Sarah K, Yang, Dian, Chuang, Chen-Hua, Brady, Jennifer J, Lim, Jing Shan, Grüner, Barbara M, Chiou, Shin-Heng, Schep, Alicia N, Baral, Jessika, Hamard, Cécile, Antoine, Martine, Wislez, Marie, Kong, Christina S, Connolly, Andrew J, Park, Kwon-Sik, Sage, Julien, Greenleaf, William J, and Winslow, Monte M

Abstract

Metastases are the main cause of cancer deaths, but the mechanisms underlying metastatic progression remain poorly understood. We isolated pure populations of cancer cells from primary tumors and metastases from a genetically engineered mouse model of human small cell lung cancer (SCLC) to investigate the mechanisms that drive the metastatic spread of this lethal cancer. Genome-wide characterization of chromatin accessibility revealed the opening of large numbers of distal regulatory elements across the genome during metastatic progression. These changes correlate with copy number amplification of the Nfib locus, and differentially accessible sites were highly enriched for Nfib transcription factor binding sites. Nfib is necessary and sufficient to increase chromatin accessibility at a large subset of the intergenic regions. Nfib promotes pro-metastatic neuronal gene expression programs and drives the metastatic ability of SCLC cells. The identification of widespread chromatin changes during SCLC progression reveals an unexpected global reprogramming during metastatic progression.

Published

2016

40. Kwaliteitsindicatoren voor de aanpak van longkanker : Synthese

Author

Verleye, Leen, De Gendt, Cindy, Schillemans, Viki, Robays, Jo, Camberlin, Cécile, Dubois, Cécile, Stordeur, Sabine, Jegou, David, Silversmit, Geert, Van Eycken, E., Wauters, Isabelle, Van Meerbeeck, Jan, Vrijens, France, Verleye, Leen, De Gendt, Cindy, Schillemans, Viki, Robays, Jo, Camberlin, Cécile, Dubois, Cécile, Stordeur, Sabine, Jegou, David, Silversmit, Geert, Van Eycken, E., Wauters, Isabelle, Van Meerbeeck, Jan, and Vrijens, France

Abstract

32 p., ill., Longkanker komt vaak voor en wordt meestal veroorzaakt door roken. De kanker heeft geen goede prognose, vooral als hij pas in een gevorderd stadium wordt ontdekt. In België vormt longkanker de eerste oorzaak van kankersterfte bij mannen, en de tweede bij vrouwen. Ondanks deze sombere resultaten is er toch nog vooruitgang mogelijk, door de zorgkwaliteit te verbeteren. Binnen het kader van een programma voor de verbetering van kankerzorg publiceerde het Federaal Kenniscentrum voor de Gezondheidszorg (KCE) een reeks van 23 kwaliteitsindicatoren voor de diagnose en de behandeling van longkanker. De zorgkwaliteit is in de Belgische ziekenhuizen over het algemeen goed. Toch stelde het KCE opnieuw vast dat de sterfte na de operatie van een longkanker hoger ligt in ziekenhuizen waar jaarlijks minder dan 10 van dergelijke ingrepen worden uitgevoerd. De helft van de ziekenhuizen in ons land blijkt deze drempel niet te halen. Het KCE beveelt daarom ook hier aan om deze ingrepen te centraliseren in ziekenhuizen met de nodige expertise. Daarnaast pleit het KCE ervoor dat er meer rekening wordt gehouden met de wensen en voorkeuren van de patiënt bij de beslissing om een behandeling al dan niet verder te zetten., VOORWOORD 1 -- KERN BOODSCHAPPEN 2 -- SYNTHESE. 4 -- 1. CONTEXT EN DOELSTELLINGEN 8 -- 1.1. LONGKANKER: EEN VEEL VOORKOMENDE EN DODELIJKE ZIEKTE. 8 -- 1.2. DOELSTELLINGEN VAN DIT RAPPORT 9 -- 1.2.1. De drie doelstellingen van dit rapport 9 -- 1.2.2. Doelgroep: in longkanker gespecialiseerde clinici en multidisciplinaire teams 9 -- 2. GEGEVENS EN METHODEN 10 -- 2.1. DE GEGEVENS: KOPPELING TUSSEN DE GEGEVENS VAN HET KANKERREGISTER EN DE ADMINISTRATIEVE DATABANKEN 10 -- 2.2. DE PATIËNTEN: DIAGNOSE GESTELD IN 2010-2011, PATIËNTEN MET ANDERE INVASIEVE TUMOREN WERDEN UITGESLOTEN 10 -- 2.3. ELKE PATIËNT TOEWIJZEN AAN ÉÉN CENTRUM? NIET ZO EENVOUDIG 11 -- 2.4. HOE COMORBIDITEITEN VASTSTELLEN OP BASIS VAN DE GEGEVENS VAN GENEESMIDDELENFACTUREN? 11 -- 2.5. RELATIE TUSSEN ZIEKENHUISVOLUME EN RESULTAAT12 -- 3. WAT VERTELLEN DE INDICATOREN ONS OVER DE KWALITEIT VAN DE ZORG? .13 -- 3.1. EEN STUDIE MET BIJNA 13 000 PATIËNTEN. 13 -- 3.2. DRIEËNTWINTIG GEMETEN KWALITEITSINDICATOREN: VAN DIAGNOSE TOT ZORG BIJ HET LEVENSEINDE 13 -- 3.2.1. Eenjaarsoverleving na de diagnose 17 -- 3.2.2. Kwaliteit van de rapportage aan het Kankerregister (BCR) 17 -- 3.2.3. Diagnose en stadiëring 17 -- 3.2.4. Behandeling 18 -- 3.3. DRIE COMORBIDITEITEN VASTGESTELD AAN DE HAND VAN DE GEGEVENS VAN GENEESMIDDELENFACTUREN 23 -- 3.4. WELKE IMPACT HEEFT HET ZIEKENHUISVOLUME OP DE RESULTATEN? .23 -- 3.4.1. Chirurgisch volume 23 -- 3.4.2. Chirurgisch volume en resultaten 24 -- 3.4.3. Radiotherapievolume 25 -- 3.4.4. Diagnosevolume 25 -- 4. STERKE PUNTEN EN BEPERKINGEN .26 -- 5. CONCLUSIES EN VOORUITZICHTEN 28 -- AANBEVELINGEN 29 -- REFERENTIES 30

Published

2016

41. Quality Indicators for the management of lung cancer : Synthesis

Author

Verleye, Leen, De Gendt, Cindy, Schillemans, Viki, Robays, Jo, Camberlin, Cécile, Dubois, Cécile, Stordeur, Sabine, Jegou, David, Silversmit, Geert, Van Eycken, E., Wauters, Isabelle, Van Meerbeeck, Jan, Vrijens, France, Verleye, Leen, De Gendt, Cindy, Schillemans, Viki, Robays, Jo, Camberlin, Cécile, Dubois, Cécile, Stordeur, Sabine, Jegou, David, Silversmit, Geert, Van Eycken, E., Wauters, Isabelle, Van Meerbeeck, Jan, and Vrijens, France

Abstract

30 p., ill., FOREWORD 1 -- KEY MESSAGES 2 -- SYNTHESIS 4 -- 1 BACKGROUND AND OBJECTIVES 7 -- 1.1 LUNG CANCER, A FREQUENT AND LETHAL DISEASE 7 -- 1.2 IMPROVE QUALITY OF CARE THROUGH FEEDBACK 8 -- 1.2.1 Three objectives 8 -- 1.2.2 Target audience: clinicians specialized in lung cancer and multidisciplinary teams 8 -- 2 DATA AND METHODS 9 -- 2.1 THE DATA: A LINKAGE BETWEEN THE BELGIAN CANCER REGISTRY DATA AND ADMINISTRATIVE DATABASES 9 -- 2.2 THE PATIENTS: DIAGNOSED IN 2010-2011 WITH EXCLUSION OF PATIENTS WITH OTHER INVASIVE TUMOURS 9 -- 2.3 ASSIGNING EACH PATIENT TO A SINGLE CENTRE? NOT STRAIGHTFORWARD… 10 -- 2.4 HOW TO IDENTIFY COMORBIDITY BASED ON DATA OF PHARMACEUTICAL BILLING DATA? 10 -- 2.5 THE ASSOCIATION BETWEEN VOLUME AND OUTCOMES 11 -- 3 WHAT DO THE INDICATORS TELL ABOUT THE QUALITY OF CARE?.12 -- 3.1 A STUDY INCLUDING ALMOST 13 000 PATIENTS 12 -- 3.2 TWENTY-THREE QUALITY INDICATORS MEASURED: FROM DIAGNOSIS TO END-OF-LIFE CARE 12 -- 3.2.1 Survival one year after diagnosis 16 -- 3.2.2 Quality of data reporting to Belgian Cancer Registry (BCR) 16 -- 3.2.3 Diagnosis and staging 16 -- 3.2.4 Treatment 17 -- 3.3 THREE COMORBIDITIES IDENTIFIED USING PATIENT PHARMACEUTICAL BILLING DATA 21 -- 3.4 WHAT’S THE IMPACT OF HOSPITAL VOLUME ON THE OUTCOME? .21 -- 3.4.1 Surgical volume 21 -- 3.4.2 Radiotherapy volume .23 -- 3.4.3 Diagnostic volume 23 -- 4 STRENGTHS AND LIMITATIONS 24 -- 5 CONCLUSIONS AND FUTURE PROSPECTS 25 -- RECOMMENDATIONS 27 -- REFERENCES 28

Published

2016

42. Indicateurs de qualité pour la prise en charge du cancer du poumon : Synthèse

Author

Verleye, Leen, De Gendt, Cindy, Schillemans, Viki, Robays, Jo, Camberlin, Cécile, Dubois, Cécile, Stordeur, Sabine, Jegou, David, Silversmit, Geert, Van Eycken, E., Wauters, Isabelle, Van Meerbeeck, Jan, Vrijens, France, Verleye, Leen, De Gendt, Cindy, Schillemans, Viki, Robays, Jo, Camberlin, Cécile, Dubois, Cécile, Stordeur, Sabine, Jegou, David, Silversmit, Geert, Van Eycken, E., Wauters, Isabelle, Van Meerbeeck, Jan, and Vrijens, France

Abstract

32 p., ill., Le cancer du poumon est un cancer fréquent, généralement lié au tabagisme. Son pronostic est sombre, en particulier quand il est découvert à un stade avancé. En Belgique, il est la première cause de décès par cancer chez l’homme et la seconde chez la femme. En agissant sur la qualité de sa prise en charge, on peut améliorer notablement son pronostic. Dans le cadre d’un programme d’amélioration globale des soins cancérologiques, le Centre Fédéral d’Expertise des Soins de Santé (KCE) publie une série de 23 indicateurs de qualité pour le diagnostic et le traitement de ce cancer. Même si la qualité des soins est globalement bonne dans les hôpitaux belges, le KCE constate une nouvelle fois que la mortalité après une opération chirurgicale pour cancer du poumon est plus élevée dans les hôpitaux où l’on effectue moins de 10 interventions sur le poumon par an, ce qui est le cas de la moitié des hôpitaux belges. Le KCE recommande donc que ces interventions soient centralisées dans les hôpitaux disposant de l’expertise suffisante. Le KCE plaide aussi pour qu’une grande attention soit portée aux souhaits et préférences du patient dans les décisions de poursuivre un traitement., PRÉFACE 1 -- MESSAGES CLÉS 2 -- SYNTHÈSE. 4 -- 1. CONTEXTE ET OBJECTIFS 7 -- 1.1. LE CANCER DU POUMON : UNE MALADIE FRÉQUENTE ET MORTELLE 7 -- 1.2. OBJECTIFS DE CE RAPPORT 8 -- 1.2.1. Trois objectifs 8 -- 1.2.2. Public cible : cliniciens spécialisés dans le cancer du poumon et équipes multidisciplinaires 8 -- 2. DONNÉES ET MÉTHODES 9 -- 2.1. LES DONNÉES : COUPLAGE ENTRE LES DONNÉES DU REGISTRE DU CANCER ET LES BASES DE DONNÉES ADMINISTRATIVES. 9 -- 2.2. LES PATIENTS : DIAGNOSTIC POSÉ EN 2010-2011, LES PATIENTS PORTEURS D’AUTRES TUMEURS INVASIVES ÉTANT EXCLUS 9 -- 2.3. AFFECTER CHAQUE PATIENT À UN SEUL CENTRE ? PAS SI SIMPLE… 10 -- 2.4. COMMENT IDENTIFIER LES COMORBIDITÉS À PARTIR DES DONNÉES DE FACTURATION DE MÉDICAMENTS ? 10 -- 2.5. ASSOCIATION ENTRE VOLUME ET RÉSULTATS 11 -- 3. QUE RÉVÈLENT LES INDICATEURS SUR LA QUALITÉ DES SOINS ?.12 -- 3.1. UNE ÉTUDE INCLUANT PRÈS DE 13 000 PATIENTS 12 -- 3.2. VINGT-TROIS INDICATEURS DE QUALITÉ MESURÉS : DU DIAGNOSTIC AUX SOINS EN FIN DE VIE. 12 -- 3.2.1. Survie un an après le diagnostic. 16 -- 3.2.2. Qualité de la notification des données au Registre du Cancer (BCR).16 -- 3.2.3. Diagnostic et stadification 16 -- 3.2.4. Traitement 17 -- 3.3. TROIS COMORBIDITÉS IDENTIFIÉES AU MOYEN DES DONNÉES DE FACTURATION DE -- MÉDICAMENTS. 22 -- 3.4. QUEL EST L’IMPACT DU VOLUME HOSPITALIER SUR LES RÉSULTATS ? 22 -- 3.4.1. Volume chirurgical 22 -- 3.4.2. Volume chirurgical et résultats. 23 -- 3.4.3. Volume de radiothérapies 24 -- 3.4.4. Volume de diagnostics 24 -- 4. POINTS FORTS ET LIMITES 25 -- 5. CONCLUSIONS ET PERSPECTIVES .27 -- RECOMMANDATIONS28 -- RÉFÉRENCES. 30

Published

2016

43. Relevance of platinum-sensitivity status in relapsed/refractory extensive-stage small-cell lung cancer in the modern era: a patient-level analysis of southwest oncology group trials.

Author

Lara, Primo N, Lara, Primo N, Moon, James, Redman, Mary W, Semrad, Thomas J, Kelly, Karen, Allen, Jeffrey W, Gitlitz, Barbara J, Mack, Philip C, Gandara, David R, Lara, Primo N, Lara, Primo N, Moon, James, Redman, Mary W, Semrad, Thomas J, Kelly, Karen, Allen, Jeffrey W, Gitlitz, Barbara J, Mack, Philip C, and Gandara, David R

Abstract

BackgroundExtensive-stage small-cell lung cancer (SCLC) patients who progress after platinum-based chemotherapy are traditionally categorized as platinum sensitive (progression ≥ 90 days from last platinum dose) or refractory (progression < 90 days), a practice arising from seminal observations of worse survival in refractory patients. Subsequent trials accounted for platinum sensitivity, resulting in higher sample sizes and increased resource use.MethodsTo assess whether platinum-sensitivity status remains associated with outcomes, patient-level data from recent Southwest Oncology Group trials in second- and/or third-line extensive-stage SCLC were pooled. Hazard ratios (HRs) for progression-free survival (PFS) and overall survival (OS) accounting for platinum sensitivity were calculated using unadjusted and adjusted Cox Proportional Hazard models. Recursive partitioning was performed to define prognostic risk groups.ResultsOf 329 patients, 151 were platinum sensitive and 178 refractory. HRs from unadjusted Cox PFS and OS models for refractory versus sensitive disease were 1.0 (95% confidence interval, 0.81-1.25; p = 0.98) and 1.24 (0.99-1.57; p = 0.06), respectively. Adjusted Cox models showed that only elevated serum lactate dehydrogenase (HR, 2.04; p < 0.001), males (HR, 1.36; p = 0.04), performance status of 1 (HR, 1.25; p = 0.02), and weight loss greater than or equal to 5% (1.53, p = 0.01) were independently associated with OS. Platinum-sensitivity status was not associated with PFS (HR, 1.11; p = 0.49) or OS (HR, 1.25; p = 0.14), except in a model that excluded 36 patients who received more than one prior chemotherapy regimen (HR, 1.34; p = 0.049). Prognostic groups with differential OS outcomes (high, intermediate, and poor risk) were identified.ConclusionsPlatinum-sensitivity status may no longer be strongly associated with PFS or OS in at least one multivariate model. Validation of prognostic risk groups identified here is warranted. These data have

Published

2015

44. Association of Actual and Preferred Decision Roles With Patient-Reported Quality of Care: Shared Decision Making in Cancer Care.

Author

Kehl, Kenneth L, Kehl, Kenneth L, Landrum, Mary Beth, Arora, Neeraj K, Ganz, Patricia A, van Ryn, Michelle, Mack, Jennifer W, Keating, Nancy L, Kehl, Kenneth L, Kehl, Kenneth L, Landrum, Mary Beth, Arora, Neeraj K, Ganz, Patricia A, van Ryn, Michelle, Mack, Jennifer W, and Keating, Nancy L

Abstract

ImportanceShared decision making is associated with improved patient-reported outcomes of cancer treatment, but not all patients prefer to participate in medical decisions. Results from studies of the effect of matching between actual and preferred medical decision roles on patients' perceptions of care quality have been conflicting.ObjectivesTo determine whether shared decision making was associated with patient ratings of care quality and physician communication and whether patients' preferred decision roles modified those associations.Design, setting, and participantsWe performed a population- and health system-based survey of participants in the Cancer Care Outcomes Research and Surveillance Consortium (CanCORS) study diagnosed with lung and/or colorectal cancer between 2003 and 2005 (56% with colorectal cancer, 40% with non-small-cell lung cancer, and 5% with small-cell lung cancer). The CanCORS study included 9737 patients (cooperation rate among patients contacted, 59.9%) treated in integrated care delivery systems, academic institutions, private offices, and Veterans Affairs hospitals. The medical records were abstracted between October 11, 2005, and April 30, 2009; all analyses were conducted between 2013 and 2014.InterventionsWe surveyed patients specifically about their preferred roles in cancer treatment decisions and their actual roles in decisions about surgery, chemotherapy, and radiation therapy. We analyzed the responses of 5315 patients who completed baseline surveys and reported decision roles for a total of 10 817 treatment decisions and assessed associations of patients' decision roles with patient-reported quality of care and physician communication.Main outcomes and measuresThe outcomes (identified before data collection) included patient-reported excellent quality of care and top ratings (highest score) on a physician communication scale.ResultsAfter adjustment, patients describing physician-controlled (vs shared) decisions were less likely t

Published

2015

45. Relevance of platinum-sensitivity status in relapsed/refractory extensive-stage small-cell lung cancer in the modern era: a patient-level analysis of southwest oncology group trials.

Author

Lara, Primo N, Lara, Primo N, Moon, James, Redman, Mary W, Semrad, Thomas J, Kelly, Karen, Allen, Jeffrey W, Gitlitz, Barbara J, Mack, Philip C, Gandara, David R, Lara, Primo N, Lara, Primo N, Moon, James, Redman, Mary W, Semrad, Thomas J, Kelly, Karen, Allen, Jeffrey W, Gitlitz, Barbara J, Mack, Philip C, and Gandara, David R

Abstract

BackgroundExtensive-stage small-cell lung cancer (SCLC) patients who progress after platinum-based chemotherapy are traditionally categorized as platinum sensitive (progression ≥ 90 days from last platinum dose) or refractory (progression < 90 days), a practice arising from seminal observations of worse survival in refractory patients. Subsequent trials accounted for platinum sensitivity, resulting in higher sample sizes and increased resource use.MethodsTo assess whether platinum-sensitivity status remains associated with outcomes, patient-level data from recent Southwest Oncology Group trials in second- and/or third-line extensive-stage SCLC were pooled. Hazard ratios (HRs) for progression-free survival (PFS) and overall survival (OS) accounting for platinum sensitivity were calculated using unadjusted and adjusted Cox Proportional Hazard models. Recursive partitioning was performed to define prognostic risk groups.ResultsOf 329 patients, 151 were platinum sensitive and 178 refractory. HRs from unadjusted Cox PFS and OS models for refractory versus sensitive disease were 1.0 (95% confidence interval, 0.81-1.25; p = 0.98) and 1.24 (0.99-1.57; p = 0.06), respectively. Adjusted Cox models showed that only elevated serum lactate dehydrogenase (HR, 2.04; p < 0.001), males (HR, 1.36; p = 0.04), performance status of 1 (HR, 1.25; p = 0.02), and weight loss greater than or equal to 5% (1.53, p = 0.01) were independently associated with OS. Platinum-sensitivity status was not associated with PFS (HR, 1.11; p = 0.49) or OS (HR, 1.25; p = 0.14), except in a model that excluded 36 patients who received more than one prior chemotherapy regimen (HR, 1.34; p = 0.049). Prognostic groups with differential OS outcomes (high, intermediate, and poor risk) were identified.ConclusionsPlatinum-sensitivity status may no longer be strongly associated with PFS or OS in at least one multivariate model. Validation of prognostic risk groups identified here is warranted. These data have

Published

2015

46. Roles of microRNA-Mediated Drug Resistance in Tumor Stem Cells of Small Cell Lung Carcinoma

Author

MISSISSIPPI UNIV MEDICAL CENTER JACKSON, Watabe, Kounosuke, MISSISSIPPI UNIV MEDICAL CENTER JACKSON, and Watabe, Kounosuke

Abstract

Lung cancer is the leading cause of cancer deaths in the world, and according to the statistics of National Cancer Institute s SEER, 219,000 men and women will be diagnosed and 159,000 patients will die from this disease in 2014. Small cell lung carcinoma (SCLC) is the cause of approximately 20% of lung cancer. Chemo-therapy is the first choice of treatment for this carcinoma because SCLC is often highly malignant and metastasizes to the distant organs even at an early stage. Although SCLC is chemotherapy-sensitive at the initial stage, it becomes ultimately chemo-resistant with worse prognosis. Recent stem cell theory suggests that there is a distinct population of tumor cells that has stem-cell like characteristics as well as ability of resistance to chemo-therapy. Moreover, several lines of evidence indicated that the self renewal ability of cancer stem cells is regulated by microRNAs. Therefore, we hypothesize that drug resistance of SCLC is mediated by microRNA in tumor stem cell. In this project, we planned to identify the specific microRNA in the stem cells from SCLC. We have established a method to isolate cancer stem cells from human SCLC cell line, and our results indicate that miR16 and 21 are strongly expressed in these CSCs. We also identified five microRNAs (including miR16 and 21) that are involved in Cisplatin resistance by microRNA library screening. Our results strongly suggest that miR16 and miR21 play critical roles in chemo-resistance of cancer stem cell derived from SCLC. Therefore, these oncomirs may serve as potential biomarkers and therapeutic targets for chemoresistant SCLC., The original document contains color images.

Published

2014

47. Southwest Oncology Group S0802: a randomized, phase II trial of weekly topotecan with and without ziv-aflibercept in patients with platinum-treated small-cell lung cancer.

Author

Allen, Jeffrey W, Allen, Jeffrey W, Moon, James, Redman, Mary, Gadgeel, Shirish M, Kelly, Karen, Mack, Philip C, Saba, Hanna M, Mohamed, Mohamed K, Jahanzeb, Mohammad, Gandara, David R, Allen, Jeffrey W, Allen, Jeffrey W, Moon, James, Redman, Mary, Gadgeel, Shirish M, Kelly, Karen, Mack, Philip C, Saba, Hanna M, Mohamed, Mohamed K, Jahanzeb, Mohammad, and Gandara, David R

Abstract

PurposeDevelopment of new therapies for previously treated small-cell lung cancer (SCLC) is a major unmet need. Here, we describe a randomized, phase II trial of weekly topotecan with or without ziv-aflibercept (VEGF-trap) in this clinical setting.Patients and methodsPatients with previously treated SCLC (one line of platinum-based chemotherapy), performance status of 0 to 1, adequate organ function, treated brain metastases, and no recent vascular events or bleeding diatheses were eligible. Eligible patients were stratified as platinum-sensitive or platinum-refractory and randomly assigned to receive weekly topotecan 4 mg/m(2) intravenously (IV) with or without ziv-aflibercept 6 mg/kg IV every 21 days. Progression-free survival (PFS) at 3 months was the primary end point.ResultsIn 189 randomly assigned patients, treatment arms were well balanced with regard to clinical characteristics. The 3-month PFS was significantly improved with the addition of ziv-aflibercept in patients who had platinum-refractory disease (27% v 10%; P = .02) but not in patients with platinum-sensitive disease (24% v 15%; P = .22). Although response rate was low, disease control rate was higher with combination therapy than with topotecan alone in patients who had platinum-sensitive disease (37% v 18%; P = .05) and in those who had platinum-refractory disease (25% v 15%; P = .14). Overall survival (OS) was not significantly improved in either strata. Grades 3 to 5 toxicities were more common with the addition of ziv-aflibercept.ConclusionZiv-aflibercept improved the 3-month PFS in patients who had platinum-refractory SCLC, but its addition increased toxicity. OS was similar with combined ziv-aflibercept and topotecan compared with topotecan in both strata.

Published

2014

48. Southwest Oncology Group S0802: a randomized, phase II trial of weekly topotecan with and without ziv-aflibercept in patients with platinum-treated small-cell lung cancer.

Author

Allen, Jeffrey W, Allen, Jeffrey W, Moon, James, Redman, Mary, Gadgeel, Shirish M, Kelly, Karen, Mack, Philip C, Saba, Hanna M, Mohamed, Mohamed K, Jahanzeb, Mohammad, Gandara, David R, Allen, Jeffrey W, Allen, Jeffrey W, Moon, James, Redman, Mary, Gadgeel, Shirish M, Kelly, Karen, Mack, Philip C, Saba, Hanna M, Mohamed, Mohamed K, Jahanzeb, Mohammad, and Gandara, David R

Abstract

PurposeDevelopment of new therapies for previously treated small-cell lung cancer (SCLC) is a major unmet need. Here, we describe a randomized, phase II trial of weekly topotecan with or without ziv-aflibercept (VEGF-trap) in this clinical setting.Patients and methodsPatients with previously treated SCLC (one line of platinum-based chemotherapy), performance status of 0 to 1, adequate organ function, treated brain metastases, and no recent vascular events or bleeding diatheses were eligible. Eligible patients were stratified as platinum-sensitive or platinum-refractory and randomly assigned to receive weekly topotecan 4 mg/m(2) intravenously (IV) with or without ziv-aflibercept 6 mg/kg IV every 21 days. Progression-free survival (PFS) at 3 months was the primary end point.ResultsIn 189 randomly assigned patients, treatment arms were well balanced with regard to clinical characteristics. The 3-month PFS was significantly improved with the addition of ziv-aflibercept in patients who had platinum-refractory disease (27% v 10%; P = .02) but not in patients with platinum-sensitive disease (24% v 15%; P = .22). Although response rate was low, disease control rate was higher with combination therapy than with topotecan alone in patients who had platinum-sensitive disease (37% v 18%; P = .05) and in those who had platinum-refractory disease (25% v 15%; P = .14). Overall survival (OS) was not significantly improved in either strata. Grades 3 to 5 toxicities were more common with the addition of ziv-aflibercept.ConclusionZiv-aflibercept improved the 3-month PFS in patients who had platinum-refractory SCLC, but its addition increased toxicity. OS was similar with combined ziv-aflibercept and topotecan compared with topotecan in both strata.

Published

2014

49. PTEN is a potent suppressor of small cell lung cancer.

Author

Cui, Min, Cui, Min, Augert, Arnaud, Rongione, Michael, Conkrite, Karina, Parazzoli, Susan, Nikitin, Alexander Yu, Ingolia, Nicholas, MacPherson, David, Cui, Min, Cui, Min, Augert, Arnaud, Rongione, Michael, Conkrite, Karina, Parazzoli, Susan, Nikitin, Alexander Yu, Ingolia, Nicholas, and MacPherson, David

Abstract

UnlabelledSmall cell lung carcinoma (SCLC) is a highly metastatic tumor type with neuroendocrine features and a dismal prognosis. PTEN mutations and PIK3CA activating mutations have been reported in SCLC but the functional relevance of this pathway is unknown. The PTEN/PIK3CA pathway was interrogated using an AdenoCre-driven mouse model of SCLC harboring inactivated Rb and p53. Inactivation of one allele of PTEN in Rb/p53-deleted mice led to accelerated SCLC with frequent metastasis to the liver. In contrast with the high mutation burden reported in human SCLC, exome analyses revealed a low number of protein-altering mutations in mouse SCLC. Inactivation of both alleles of PTEN in the Rb/p53-deleted system led to nonmetastatic adenocarcinoma with neuroendocrine differentiation. This study reveals a critical role for the PTEN/PI3K pathway in both SCLC and lung adenocarcinoma and provides an ideal system to test the phosphoinositide 3-kinase (PI3K) pathway inhibitors as targeted therapy for subsets of patients with SCLC.ImplicationsThe ability of PTEN inactivation to accelerate SCLC in a genetic mouse model suggests that targeting the PTEN pathway is a therapeutic option for a subset of human patients with SCLC. VISUAL OVERVIEW: http://mcr.aacrjournals.org/content/early/2014/04/28/1541-7786.MCR-13-0554/F1.large.jpg.

Published

2014

50. Left behind? Drug discovery in extensive-stage small-cell lung cancer.

Author

Riess, Jonathan, Riess, Jonathan, Lara, Primo, Riess, Jonathan, Riess, Jonathan, and Lara, Primo

Abstract

Systemic therapy and subsequent survival for patients with extensive-stage small-cell lung cancer (SCLC) are poor and have remained unchanged in the past quarter century. To improve outcomes in these patients, a new drug development paradigm must be adopted that moves away from empiricism and instead focuses on tumor biology and heterogeneity as a means to increase target and drug class diversity. By incorporating tools that have led to new diagnostic and treatment options in non-small-cell lung cancer, there could be hope yet for the future of SCLC therapeutics.

Published

2014