Your search keyword '"Plodkowski A"' showing total 699 results

1. Body mass index and adiposity influence responses to immune checkpoint inhibition in endometrial cancer

Author

Gomez-Banoy, Nicolas, Ortiz, Eduardo J., Jiang, Caroline S., Dagher, Christian, Sevilla, Carlo, Girshman, Jeffrey, Pagano, Andrew M., Plodkowski, Andrew J., Zammarrelli, William A., Mueller, Jennifer J., Aghajanian, Carol, Weigelt, Britta, Makker, Vicky, Cohen, Paul, and Osorio, Juan C.

Subjects

Drug therapy, Physiological aspects, Dosage and administration, Health aspects, Endometrial cancer -- Physiological aspects -- Drug therapy, Body mass index -- Health aspects, Medical research, Adipose tissue -- Health aspects, Immune checkpoint inhibitors -- Physiological aspects -- Dosage and administration, Medicine, Experimental, Adipose tissues -- Health aspects

Abstract

Introduction Endometrial cancer (EC) constitutes the leading cause of gynecologic cancer-related death in the United States and one of the few cancer types with increasing incidence and disease-associated mortality (1). [...], BACKGROUND. Obesity is the foremost risk factor in the development of endometrial cancer (EC). However, the impact of obesity on the response to immune checkpoint inhibitors (ICI) in EC remains poorly understood. This retrospective study investigates the association among BMI, body fat distribution, and clinical and molecular characteristics of EC patients treated with ICI. METHODS. We analyzed progression-free survival (PFS) and overall survival (OS) in EC patients treated with ICI, categorized by BMI, fat-mass distribution, and molecular subtypes. Incidence of immune-related adverse events (irAEs) after ICI was also assessed based on BMI status. RESULTS. 524 EC patients were included in the study. Overweight and obese patients exhibited a significantly prolonged PFS and OS compared with normal BMI patients after treatment with ICI. Multivariable Cox's regression analysis confirmed the independent association of overweight and obesity with improved PFS and OS. Elevated visceral adipose tissue (VAT) was identified as a strong independent predictor for improved PFS to ICI. Associations between obesity and OS/PFS were particularly significant in the copy number-high/TP53abnormal (CN-H/TP53abn) EC molecular subtype. Finally, obese patients demonstrated a higher irAE rate compared with normal BMI individuals. CONCLUSION. Obesity is associated with improved outcomes to ICI in EC patients and a higher rate of irAEs. This association is more pronounced in the CN-H/TP53abn EC molecular subtype. FUNDING. NIH/NCI Cancer Center; MSK Gerstner Physician Scholars Program; National Center for Advancing Translational Sciences (NCATS); Cycle for Survival; Breast Cancer Research Foundation.

Published

2024

2. Profiling of Skeletal Muscle and Adipose Tissue Depots in Men with Advanced Prostate Cancer Receiving Different Forms of Androgen Deprivation Therapy

Author

Tahj A. Blow, Anirudh Murthy, Rahul Grover, Emily Schwitzer, David M. Nanus, Darragh Halpenny, Andrew J. Plodkowski, Lee W. Jones, and Marcus D. Goncalves

Subjects

Prostate cancer, Androgen deprivation therapy, Body composition, Skeletal muscle mass, Subcutaneous adipose tissue, Sarcopenia, Diseases of the genitourinary system. Urology, RC870-923, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Background: Androgen deprivation therapy (ADT) is a common treatment modality for men with prostate cancer. Increases in adipose tissue mass and decreases in skeletal muscle mass are known on-target adverse effects of standard ADT. The effects of newer agents such as abiraterone acetate (ABI) and enzalutamide (ENZA) on body composition and how these compare with standard luteinizing hormone-releasing hormone agonists (aLHRHs) are unclear. Objective: To assess the effects of different forms of androgen deprivation therapy on body composition in men with prostate cancer. Design, setting, and participants: Using a retrospective design, 229 patients receiving aLHRHs alone (n = 120) or in combination with ABI (n = 53) or ENZA (n = 56) were studied. Outcome measurements and statistical analysis: Muscle, visceral adipose tissue (VAT), and subcutaneous adipose tissue (SAT) were assessed at baseline, 6 mo, and 18 mo after initiating therapy using a cross-sectional densitometry analysis performed on standard of care computed tomography images. Response trajectories for all treatment groups were calculated via a two-way analysis of variance post hoc test, for both within-group and between-group differences. Results and limitations: Treatment with aLHRHs, ABI, and ENZA was associated with a median muscle volume loss of –1.4%, –4.8%, and –5.5% at 6 mo, and –7.1%, –8.1%, and –8.3% at 18 mo, respectively. Therapy with aLHRHs was associated with minimal changes in VAT (0.3% at 6 mo and –0.1% at 18 mo). ABI therapy was associated with significant increases in VAT at 6 mo (4.9%) but not at 18 mo (0.5%), and ENZA therapy was associated with significant decreases in VAT (–4.6% at 6 mo and –5.4% at 18 mo). With respect to SAT, treatment with aLHRHs was associated with increases over time (8.6% at 6 mo and 4.7% at 18 mo), ABI was associated with decreases over time (–3.6% at 6 mo and –6.8% at 18 mo), and ENZA had no clear effects (1.7% at 6 mo and 3.3% at 18 mo). Conclusions: ADT regimens cause significant short-term losses in muscle mass, with the most rapid effects occurring with ABI and ENZA. The three regimens have disparate effects on SAT and VAT, suggesting distinct roles of androgens in these tissues. Patient summary: Androgen deprivation therapy alters body composition in men with prostate cancer. Abiraterone and enzalutamide are associated with losses in muscle mass compared with luteinizing hormone-releasing hormone agonists. These treatments impact subcutaneous and visceral fat mass, suggesting distinct roles of androgens in these tissues.

Published

2023

3. Immunotherapy-Mediated Thyroid Dysfunction: Genetic Risk and Impact on Outcomes with PD-1 Blockade in Non–Small Cell Lung Cancer

Author

Luo, Jia, Martucci, Victoria L, Quandt, Zoe, Groha, Stefan, Murray, Megan H, Lovly, Christine M, Rizvi, Hira, Egger, Jacklynn V, Plodkowski, Andrew J, Abu-Akeel, Mohsen, Schulze, Isabell, Merghoub, Taha, Cardenas, Eduardo, Huntsman, Scott, Li, Min, Hu, Donglei, Gubens, Matthew A, Gusev, Alexander, Aldrich, Melinda C, Hellmann, Matthew D, and Ziv, Elad

Subjects

Prevention, Cancer, Genetics, Clinical Research, Lung, Human Genome, Good Health and Well Being, Aged, Carcinoma, Non-Small-Cell Lung, Female, Humans, Immune Checkpoint Inhibitors, Immunotherapy, Lung Neoplasms, Male, Middle Aged, Retrospective Studies, Risk Assessment, Thyroid Diseases, Treatment Outcome, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

PurposeGenetic differences in immunity may contribute to toxicity and outcomes with immune checkpoint inhibitor (CPI) therapy, but these relationships are poorly understood. We examined the genetics of thyroid immune-related adverse events (irAE).Experimental designIn patients with non-small cell lung cancer (NSCLC) treated with CPIs at Memorial Sloan Kettering (MSK) and Vanderbilt University Medical Center (VUMC), we evaluated thyroid irAEs. We typed germline DNA using genome-wide single-nucleotide polymorphism (SNP) arrays and imputed genotypes. Germline SNP imputation was also performed in an independent Dana-Farber Cancer Institute (DFCI) cohort. We developed and validated polygenic risk scores (PRS) for hypothyroidism in noncancer patients using the UK and VUMC BioVU biobanks. These PRSs were applied to thyroid irAEs and CPI response in patients with NSCLC at MSK, VUMC, and DFCI.ResultsAmong 744 patients at MSK and VUMC, thyroid irAEs occurred in 13% and were associated with improved outcomes [progression-free survival adjusted HR (PFS aHR) = 0.68; 95% confidence interval (CI), 0.52-0.88]. The PRS for hypothyroidism developed from UK Biobank predicted hypothyroidism in the BioVU dataset in noncancer patients [OR per standard deviation (SD) = 1.33, 95% CI, 1.29-1.37; AUROC = 0.6]. The same PRS also predicted development of thyroid irAEs in both independent cohorts of patients treated with CPIs (HR per SD = 1.34; 95% CI, 1.08-1.66; AUROC = 0.6). The results were similar in the DFCI cohort. However, PRS for hypothyroidism did not predict CPI benefit.ConclusionsThyroid irAEs were associated with response to anti-PD-1 therapy. Genetic risk for hypothyroidism was associated with risk of developing thyroid irAEs. Additional studies are needed to determine whether other irAEs also have shared genetic risk with known autoimmune disorders and the association with treatment response.

Published

2021

4. Clinical and molecular features of acquired resistance to immunotherapy in non-small cell lung cancer

Author

Memon, Danish, Schoenfeld, Adam J., Ye, Darwin, Fromm, George, Rizvi, Hira, Zhang, Xiang, Keddar, Mohamed Reda, Mathew, Divij, Yoo, Kyung Jin, Qiu, Jingya, Lihm, Jayon, Miriyala, Jayalaksmi, Sauter, Jennifer L., Luo, Jia, Chow, Andrew, Bhanot, Umesh K., McCarthy, Caroline, Vanderbilt, Chad M., Liu, Cailian, Abu-Akeel, Mohsen, Plodkowski, Andrew J., McGranahan, Nicholas, Łuksza, Marta, Greenbaum, Benjamin D., Merghoub, Taha, Achour, Ikbel, Barrett, J. Carl, Stewart, Ross, Beltrao, Pedro, Schreiber, Taylor H., Minn, Andy J., Miller, Martin L., and Hellmann, Matthew D.

Published

2024

5. Profiling of Skeletal Muscle and Adipose Tissue Depots in Men with Advanced Prostate Cancer Receiving Different Forms of Androgen Deprivation Therapy

Author

Blow, Tahj A., Murthy, Anirudh, Grover, Rahul, Schwitzer, Emily, Nanus, David M., Halpenny, Darragh, Plodkowski, Andrew J., Jones, Lee W., and Goncalves, Marcus D.

Published

2023

6. Lineage tracing reveals clonal progenitors and long-term persistence of tumor-specific T cells during immune checkpoint blockade

Author

Pai, Joy A., Hellmann, Matthew D., Sauter, Jennifer L., Mattar, Marissa, Rizvi, Hira, Woo, Hyung Jun, Shah, Nisargbhai, Nguyen, Evelyn M., Uddin, Fathema Z., Quintanal-Villalonga, Alvaro, Chan, Joseph M., Manoj, Parvathy, Allaj, Viola, Baine, Marina K., Bhanot, Umesh K., Jain, Mala, Linkov, Irina, Meng, Fanli, Brown, David, Chaft, Jamie E., Plodkowski, Andrew J., Gigoux, Mathieu, Won, Helen H., Sen, Triparna, Wells, Daniel K., Donoghue, Mark T.A., de Stanchina, Elisa, Wolchok, Jedd D., Loomis, Brian, Merghoub, Taha, Rudin, Charles M., Chow, Andrew, and Satpathy, Ansuman T.

Published

2023

7. Association of cardiac calcium burden with overall survival after radiotherapy for non-small cell lung cancer

Author

Haseltine, Justin M., Apte, Aditya, Jackson, Andrew, Yorke, Ellen, Yu, Anthony F., Plodkowski, Andrew, Wu, Abraham, Peleg, Ariel, Al-Sadawi, Mohammed, Iocolano, Michelle, Gelblum, Daphna, Shaverdian, Narek, Simone, Charles B., II, Rimner, Andreas, Gomez, Daniel R., Shepherd, Annemarie F., and Thor, Maria

Published

2023

8. Body mass index and adiposity influence responses to immune checkpoint inhibition in endometrial cancer

Author

Gomez-Banoy, Nicolas, primary, Ortiz, Eduardo J, additional, Jiang, Caroline S., additional, Dagher, Christian, additional, Sevilla, Carlo, additional, Girshman, Jeffrey, additional, Pagano, Andrew, additional, Plodkowski, Andrew J, additional, Zammarrelli, William, additional, Mueller, Jennifer J., additional, Aghajanian, Carol, additional, Weigelt, Britta, additional, Makker, Vicky, additional, Cohen, Paul, additional, and Osorio, Juan C, additional

Published

2024

9. Deciphering radiological stable disease to immune checkpoint inhibitors

Author

Luo, J., Wu, S., Rizvi, H., Zhang, Q., Egger, J.V., Osorio, J.C., Schoenfeld, A.J., Plodkowski, A.J., Ginsberg, M.S., Callahan, M.K., Maher, C., Shoushtari, A.N., Postow, M.A., Voss, M.H., Kotecha, R.R., Gupta, A., Raja, R., Kris, M.G., and Hellmann, M.D.

Published

2022

10. Immune biomarkers and response to checkpoint inhibition of BRAFV600 and BRAF non-V600 altered lung cancers

Author

Murciano-Goroff, Yonina R., Pak, Terry, Mondaca, Sebastian, Flynn, Jessica R., Montecalvo, Joseph, Rekhtman, Natasha, Halpenny, Darragh, Plodkowski, Andrew J., Wu, Stephanie L., Kris, Mark G., Paik, Paul K., Riely, Gregory J., Yu, Helena A., Rudin, Charles M., Hellmann, Matthew D., Land, Josiah D., Buie, Larry W., Heller, Glenn, Lito, Piro, Yaeger, Rona, Drilon, Alexander, Liu, Dazhi, Li, Bob T., and Offin, Michael

Published

2022

11. COVID-19 in patients with cancer: can baseline radiologic severity and early evolution predict clinical outcomes?

Author

Perez-Johnston, Rocio, Araujo-Filho, Jose, Mckenney, Anna S., Gangai, Natalie, Plodkowski, Andrew J., Liu, Corinne C., Sawan, Peter, Taur, Ying, Morjaria, Sejal M., and Ginsberg, Michelle S.

Published

2022

12. Diminished Efficacy of Programmed Death-(Ligand)1 Inhibition in STK11- and KEAP1-Mutant Lung Adenocarcinoma Is Affected by KRAS Mutation Status

Author

Ricciuti, Biagio, Arbour, Kathryn C., Lin, Jessica J., Vajdi, Amir, Vokes, Natalie, Hong, Lingzhi, Zhang, Jianjun, Tolstorukov, Michael Y., Li, Yvonne Y., Spurr, Liam F., Cherniack, Andrew D., Recondo, Gonzalo, Lamberti, Giuseppe, Wang, Xinan, Venkatraman, Deepti, Alessi, Joao V., Vaz, Victor R., Rizvi, Hira, Egger, Jacklynn, Plodkowski, Andrew J., Khosrowjerdi, Sara, Digumarthy, Subba, Park, Hyesun, Vaz, Nuno, Nishino, Mizuki, Sholl, Lynette M., Barbie, David, Altan, Mehmet, Heymach, John V., Skoulidis, Ferdinandos, Gainor, Justin F., Hellmann, Matthew D., and Awad, Mark M.

Published

2022

13. Association of cardiac calcium burden with overall survival after radiotherapy for non-small cell lung cancer

Author

Justin M. Haseltine, Aditya Apte, Andrew Jackson, Ellen Yorke, Anthony F. Yu, Andrew Plodkowski, Abraham Wu, Ariel Peleg, Mohammed Al-Sadawi, Michelle Iocolano, Daphna Gelblum, Narek Shaverdian, Charles B. Simone, II, Andreas Rimner, Daniel R. Gomez, Annemarie F. Shepherd, and Maria Thor

Subjects

Non-small cell lung cancer, Radiotherapy, Coronary calcifications, Medical physics. Medical radiology. Nuclear medicine, R895-920, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Background and purpose: Coronary calcifications are associated with coronary artery disease in patients undergoing radiotherapy (RT) for non-small cell lung cancer (NSCLC). We quantified calcifications in the coronary arteries and aorta and investigated their relationship with overall survival (OS) in patients treated with definitive RT (Def-RT) or post-operative RT (PORT). Materials and methods: We analyzed 263 NSCLC patients treated from 2004 to 2017. Calcium burden was ascertained with a Hounsfield unit (HU) cutoff of > 130 in addition to a deep learning (DL) plaque estimator. The HU cutoff volumes were defined for coronary arteries (PlaqueCoro) and coronary arteries and aorta combined (PlaqueCoro+Ao), while the DL estimator ranged from 0 (no plaque) to 3 (high plaque). Patient and treatment characteristics were explored for association with OS. Results: The median PlaqueCoro and PlaqueCoro+Ao was 0.75 cm3 and 0.87 cm3 in the Def-RT group and 0.03 cm3 and 0.52 cm3 in the PORT group. The median DL estimator was 2 in both cohorts. In Def-RT, large PlaqueCoro (HR:1.11 (95%CI:1.04–1.19); p = 0.008), and PlaqueCoro+Ao (HR:1.06 (95%CI:1.02–1.11); p = 0.03), and poor Karnofsky Performance Status (HR: 0.97 (95%CI: 0.94–0.99); p = 0.03) were associated with worse OS. No relationship was identified between the plaque volumes and OS in PORT, or between the DL plaque estimator and OS in either Def-RT or PORT. Conclusions: Coronary artery calcification assessed from RT planning CT scans was significantly associated with OS in patients who underwent Def-RT for NSCLC. This HU thresholding method can be straightforwardly implemented such that the role of calcifications can be further explored.

Published

2023

14. STK11/LKB1 Mutations and PD-1 Inhibitor Resistance in KRAS-Mutant Lung Adenocarcinoma.

Author

Skoulidis, Ferdinandos, Goldberg, Michael, Greenawalt, Danielle, Hellmann, Matthew, Awad, Mark, Gainor, Justin, Schrock, Alexa, Hartmaier, Ryan, Trabucco, Sally, Gay, Laurie, Ali, Siraj, Elvin, Julia, Singal, Gaurav, Ross, Jeffrey, Fabrizio, David, Szabo, Peter, Chang, Han, Sasson, Ariella, Srinivasan, Sujaya, Kirov, Stefan, Szustakowski, Joseph, Vitazka, Patrik, Edwards, Robin, Bufill, Jose, Sharma, Neelesh, Ou, Sai-Hong, Peled, Nir, Spigel, David, Rizvi, Hira, Aguilar, Elizabeth, Carter, Brett, Erasmus, Jeremy, Halpenny, Darragh, Plodkowski, Andrew, Long, Niamh, Nishino, Mizuki, Denning, Warren, Galan-Cobo, Ana, Hamdi, Haifa, Hirz, Taghreed, Tong, Pan, Wang, Jing, Rodriguez-Canales, Jaime, Villalobos, Pamela, Parra, Edwin, Kalhor, Neda, Sholl, Lynette, Sauter, Jennifer, Jungbluth, Achim, Mino-Kenudson, Mari, Azimi, Roxana, Elamin, Yasir, Zhang, Jianjun, Leonardi, Giulia, Wong, Kwok-Kin, Lee, J, Papadimitrakopoulou, Vassiliki, Wistuba, Ignacio, Miller, Vincent, Frampton, Garrett, Wolchok, Jedd, Shaw, Alice, Jänne, Pasi, Stephens, Philip, Rudin, Charles, Geese, William, Albacker, Lee, Heymach, John, and Jiang, Fei

Subjects

AMP-Activated Protein Kinase Kinases, Adenocarcinoma of Lung, Adult, Aged, Aged, 80 and over, Animals, Antineoplastic Agents, Immunological, Disease Models, Animal, Drug Resistance, Neoplasm, Humans, Immunotherapy, Lung Neoplasms, Male, Mice, Middle Aged, Mutation, Nivolumab, Prognosis, Programmed Cell Death 1 Receptor, Progression-Free Survival, Protein Serine-Threonine Kinases, Proto-Oncogene Proteins p21(ras)

Abstract

KRAS is the most common oncogenic driver in lung adenocarcinoma (LUAC). We previously reported that STK11/LKB1 (KL) or TP53 (KP) comutations define distinct subgroups of KRAS-mutant LUAC. Here, we examine the efficacy of PD-1 inhibitors in these subgroups. Objective response rates to PD-1 blockade differed significantly among KL (7.4%), KP (35.7%), and K-only (28.6%) subgroups (P < 0.001) in the Stand Up To Cancer (SU2C) cohort (174 patients) with KRAS-mutant LUAC and in patients treated with nivolumab in the CheckMate-057 phase III trial (0% vs. 57.1% vs. 18.2%; P = 0.047). In the SU2C cohort, KL LUAC exhibited shorter progression-free (P < 0.001) and overall (P = 0.0015) survival compared with KRASMUT;STK11/LKB1WT LUAC. Among 924 LUACs, STK11/LKB1 alterations were the only marker significantly associated with PD-L1 negativity in TMBIntermediate/High LUAC. The impact of STK11/LKB1 alterations on clinical outcomes with PD-1/PD-L1 inhibitors extended to PD-L1-positive non-small cell lung cancer. In Kras-mutant murine LUAC models, Stk11/Lkb1 loss promoted PD-1/PD-L1 inhibitor resistance, suggesting a causal role. Our results identify STK11/LKB1 alterations as a major driver of primary resistance to PD-1 blockade in KRAS-mutant LUAC.Significance: This work identifies STK11/LKB1 alterations as the most prevalent genomic driver of primary resistance to PD-1 axis inhibitors in KRAS-mutant lung adenocarcinoma. Genomic profiling may enhance the predictive utility of PD-L1 expression and tumor mutation burden and facilitate establishment of personalized combination immunotherapy approaches for genomically defined LUAC subsets. Cancer Discov; 8(7); 822-35. ©2018 AACR.See related commentary by Etxeberria et al., p. 794This article is highlighted in the In This Issue feature, p. 781.

Published

2018

15. Intra- and inter-reader agreement of iRECIST and RECIST 1.1 criteria for the assessment of tumor response in patients receiving checkpoint inhibitor immunotherapy for lung cancer

Author

Huicochea Castellanos, Sandra, Pagano, Andrew, Plodkowski, Andrew J., Girshman, Jeffrey, Hellmann, Matthew D., Rizvi, Hira, Flynn, Jessica, Zheng, Junting, Capanu, Marinela, Halpenny, Darragh F, and Ginsberg, Michelle S

Published

2021

16. Waxing and waning pattern of mTOR inhibitor-associated pneumonitis in renal cell carcinoma patients: A retrospective observational study

Author

Gluskin, Jill, Plodkowski, Andrew, Girshman, Jeffrey, Sarasohn, Debra, Viteri-Jusué, Ainhoa, Hayan, Sumar, and Torrisi, Jean

Published

2021

17. Percutaneous computed tomography guided biopsy of sub-solid pulmonary nodules: differentiating solid from ground glass components at the time of biopsy

Author

Halpenny, Darragh, Das, Krishna, Ziv, Etay, Plodkowski, Andrew, Zheng, Junting, Capanu, Marinela, Rekhtman, Natasha, Montecalvo, Joseph, Solomon, Stephen B., and Ginsberg, Michelle S.

Published

2021

18. Pre-treatment CT imaging in stage IIIA lung cancer: Can we predict local recurrence after definitive chemoradiotherapy?

Author

Plodkowski, Andrew J., Araujo-Filho, Jose Arimateia Batista, Simmers, Cameron D.A., Girshman, Jeffrey, Raj, Micheal, Zheng, Junting, Rimner, Andreas, and Ginsberg, Michelle S.

Published

2021

19. Risk stratification of cardiac metastases using late gadolinium enhancement cardiovascular magnetic resonance: prognostic impact of hypo-enhancement evidenced tumor avascularity

Author

Angel T. Chan, William Dinsfriend, Jiwon Kim, Brian Yum, Razia Sultana, Christopher A. Klebanoff, Andrew Plodkowski, Rocio Perez Johnston, Michelle S. Ginsberg, Jennifer Liu, Raymond J. Kim, Richard Steingart, and Jonathan W. Weinsaft

Subjects

Cardiovascular magnetic resonance, Cardio-oncology, Cardiac neoplasm, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Abstract Background Late gadolinium enhancement (LGE) cardiovascular magnetic resonance (CMR) is widely used to identify cardiac neoplasms, for which diagnosis is predicated on enhancement stemming from lesion vascularity: Impact of contrast-enhancement pattern on clinical outcomes is unknown. The objective of this study was to determine whether cardiac metastasis (CMET) enhancement pattern on LGE-CMR impacts prognosis, with focus on heterogeneous lesion enhancement as a marker of tumor avascularity. Methods Advanced (stage IV) systemic cancer patients with and without CMET matched (1:1) by cancer etiology underwent a standardized CMR protocol. CMET was identified via established LGE-CMR criteria based on lesion enhancement; enhancement pattern was further classified as heterogeneous (enhancing and non-enhancing components) or diffuse and assessed via quantitative (contrast-to-noise ratio (CNR); signal-to-noise ratio (SNR)) analyses. Embolic events and mortality were tested in relation to lesion location and contrast-enhancement pattern. Results 224 patients were studied, including 112 patients with CMET and unaffected (CMET -) controls matched for systemic cancer etiology/stage. CMET enhancement pattern varied (53% heterogeneous, 47% diffuse). Quantitative analyses were consistent with lesion classification; CNR was higher and SNR lower in heterogeneously enhancing CMET (p

Published

2021

20. Perfusion defects on dual-energy CTA in patients with suspected pulmonary embolism correlate with right heart strain and lower survival

Author

Perez-Johnston, Rocio, Plodkowski, Andrew J., Halpenny, Darragh F., Hayes, Sara A., Capanu, Marinela, Araujo-Filho, J. A. B., Weinsaft, Jonathan W., and Ginsberg, Michelle S.

Published

2021

21. Evaluation and Treatment of Hypertension

Author

Nguyen, Quang T., Plodkowski, Raymond A., Gonzalez-Campoy, J. Michael, editor, Hurley, Daniel L., editor, and Garvey, W. Timothy, editor

Published

2019

22. Diagnostic utility and clinical implication of late gadolinium enhancement cardiac magnetic resonance for detection of catheter associated right atrial thrombus

Author

Plodkowski, Andrew J., Chan, Angel, Gupta, Dipti, Lakhman, Yulia, Kukar, Nina, Kim, Jiwon, Perez-Johnston, Rocio, Ginsberg, Michelle S., Steingart, Richard M., and Weinsaft, Jonathan W.

Published

2020

23. Clinical and molecular correlates of PD-L1 expression in patients with lung adenocarcinomas

Author

Schoenfeld, A.J., Rizvi, H., Bandlamudi, C., Sauter, J.L., Travis, W.D., Rekhtman, N., Plodkowski, A.J., Perez-Johnston, R., Sawan, P., Beras, A., Egger, J.V., Ladanyi, M., Arbour, K.C., Rudin, C.M., Riely, G.J., Taylor, B.S., Donoghue, M.T.A., and Hellmann, M.D.

Published

2020

24. SMARCA4-Deficient Thoracic Sarcomatoid Tumors Represent Primarily Smoking-Related Undifferentiated Carcinomas Rather Than Primary Thoracic Sarcomas

Author

Rekhtman, Natasha, Montecalvo, Joseph, Chang, Jason C., Alex, Deepu, Ptashkin, Ryan N., Ai, Ni, Sauter, Jennifer L., Kezlarian, Brie, Jungbluth, Achim, Desmeules, Patrice, Beras, Amanda, Bishop, Justin A., Plodkowski, Andrew J., Gounder, Mrinal M., Schoenfeld, Adam J., Namakydoust, Azadeh, Li, Bob T., Rudin, Charles M., Riely, Gregory J., Jones, David R., Ladanyi, Marc, and Travis, William D.

Published

2020

25. Efficacy of Platinum/Pemetrexed Combination Chemotherapy in ALK-Positive NSCLC Refractory to Second-Generation ALK Inhibitors

Author

Lin, Jessica J., Schoenfeld, Adam J., Zhu, Viola W., Yeap, Beow Y., Chin, Emily, Rooney, Marguerite, Plodkowski, Andrew J., Digumarthy, Subba R., Dagogo-Jack, Ibiayi, Gainor, Justin F., Ou, Sai-Hong Ignatius, Riely, Gregory J., and Shaw, Alice T.

Published

2020

26. Risk stratification of cardiac metastases using late gadolinium enhancement cardiovascular magnetic resonance: prognostic impact of hypo-enhancement evidenced tumor avascularity

Author

Chan, Angel T., Dinsfriend, William, Kim, Jiwon, Yum, Brian, Sultana, Razia, Klebanoff, Christopher A., Plodkowski, Andrew, Perez Johnston, Rocio, Ginsberg, Michelle S., Liu, Jennifer, Kim, Raymond J., Steingart, Richard, and Weinsaft, Jonathan W.

Published

2021

27. EGFR mutation subtypes and response to immune checkpoint blockade treatment in non-small-cell lung cancer

Author

Hastings, K., Yu, H.A., Wei, W., Sanchez-Vega, F., DeVeaux, M., Choi, J., Rizvi, H., Lisberg, A., Truini, A., Lydon, C.A., Liu, Z., Henick, B.S., Wurtz, A., Cai, G., Plodkowski, A.J., Long, N.M., Halpenny, D.F., Killam, J., Oliva, I., Schultz, N., Riely, G.J., Arcila, M.E., Ladanyi, M., Zelterman, D., Herbst, R.S., Goldberg, S.B., Awad, M.M., Garon, E.B., Gettinger, S., Hellmann, M.D., and Politi, K.

Published

2019

28. Acquired BRAF Rearrangements Induce Secondary Resistance to EGFR therapy in EGFR-Mutated Lung Cancers

Author

Vojnic, Morana, Kubota, Daisuke, Kurzatkowski, Christopher, Offin, Michael, Suzawa, Ken, Benayed, Ryma, Schoenfeld, Adam J., Plodkowski, Andrew J., Poirier, John T., Rudin, Charles M., Kris, Mark G., Rosen, Neal X., Yu, Helena A., Riely, Gregory J., Arcila, Maria E., Somwar, Romel, and Ladanyi, Marc

Published

2019

29. Response to Immune Checkpoint Inhibition as Monotherapy or in Combination With Chemotherapy in Metastatic ROS1-Rearranged Lung Cancers

Author

Noura J. Choudhury, MD, Jaime L. Schneider, MD, PhD, Tejas Patil, MD, Viola W. Zhu, MD, PhD, Debra A. Goldman, MS, Soo-Ryum Yang, MD, Christina J. Falcon, MPH, Andrew Do, BS, Yunan Nie, MD, Andrew J. Plodkowski, MD, Jamie E. Chaft, MD, Subba R. Digumarthy, MD, Natasha Rekhtman, MD, PhD, Maria E. Arcila, MD, Alexia Iasonos, PhD, Sai-Hong I. Ou, MD, PhD, Jessica J. Lin, MD, and Alexander Drilon, MD

Subjects

Non–small cell lung cancer, ROS1 fusion, Immune checkpoint inhibitors, Tumor mutational burden, PD-L1, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Introduction: ROS1 fusions are oncogenic drivers in 1% to 3% of NSCLCs. The activity of immune checkpoint inhibitor (ICI) monotherapy or in combination with chemotherapy (chemotherapy with ICI [chemo-ICI]) in these tumors and their immunophenotype have not been systematically described. Methods: In this multi-institutional retrospective study, tumor programmed death-ligand 1 (PD-L1) expression and tumor mutational burden (TMB) were evaluated in patients with ROS1-rearranged NSCLC. Time-to-treatment discontinuation (TTD) and objective response rate (ORR) (Response Evaluation Criteria in Solid Tumors [RECIST] version 1.1) were calculated for patients treated with ICI or chemo-ICI in the metastatic setting. Results: A total of 184 patients were identified. Among 146 assessable cases, PD-L1 expression was less than 1% in 60 (41%), 1% to 49% in 35 (24%), and greater than or equal to 50% in 51 tumors (35%). Of 100 (92%) TMB-assessable tumors, 92 had less than 10 mutations per megabase. TMB was significantly lower for ROS1-rearranged tumors (n = 97) compared with tumors with EGFR (n = 1250) or KRAS alterations (n = 1653) and all other NSCLC tumors (n = 2753) evaluated with Memorial Sloan Kettering-Integrated Mutation Profiling of Actionable Cancer Targets (median TMB = 2.6 versus 3.5, 7.0, and 6.1 mutations per megabase, p < 0.001). Among patients treated with ICI, median TTD was 2.1 months (95% confidence interval [CI]: 1.0–4.2 mo; n = 28) and ORR 13% (2 of 16 RECIST-assessable; 95% CI: 2%–38%). Among patients treated with chemo-ICI, median TTD was 10 months (95% CI: 4.7–14.1 mo; n = 11) and ORR 83% (5 of 6 RECIST-assessable; 95% CI: 36%–100%). There was no difference in PD-L1 expression (p = 0.91) or TMB (p = 0.83) between responders and nonresponders. Conclusions: Most ROS1-rearranged NSCLCs have low PD-L1 expression and TMB. The activity of ICI in these tumors is modest. In contrast, chemo-ICI can achieve meaningful activity.

Published

2021

30. Supplementary Figure S6 from Clinical and Molecular Features of Long-term Response to Immune Checkpoint Inhibitors in Patients with Advanced Non–Small Cell Lung Cancer

Author

Thummalapalli, Rohit, primary, Ricciuti, Biagio, primary, Bandlamudi, Chaitanya, primary, Muldoon, Daniel, primary, Rizvi, Hira, primary, Elkrief, Arielle, primary, Luo, Jia, primary, Alessi, Joao V., primary, Pecci, Federica, primary, Lamberti, Giuseppe, primary, Di Federico, Alessandro, primary, Hong, Lingzhi, primary, Zhang, Jianjun, primary, Heymach, John V., primary, Gibbons, Don L., primary, Plodkowski, Andrew J., primary, Ravichandran, Vignesh, primary, Donoghue, Mark T.A., primary, Vanderbilt, Chad, primary, Ladanyi, Marc, primary, Rudin, Charles M., primary, Kris, Mark G., primary, Riely, Gregory J., primary, Chaft, Jamie E., primary, Hellmann, Matthew D., primary, Vokes, Natalie I., primary, Awad, Mark M., primary, and Schoenfeld, Adam J., primary

Published

2023

31. Supplementary Table S1 from Clinical and Molecular Features of Long-term Response to Immune Checkpoint Inhibitors in Patients with Advanced Non–Small Cell Lung Cancer

Author

Thummalapalli, Rohit, primary, Ricciuti, Biagio, primary, Bandlamudi, Chaitanya, primary, Muldoon, Daniel, primary, Rizvi, Hira, primary, Elkrief, Arielle, primary, Luo, Jia, primary, Alessi, Joao V., primary, Pecci, Federica, primary, Lamberti, Giuseppe, primary, Di Federico, Alessandro, primary, Hong, Lingzhi, primary, Zhang, Jianjun, primary, Heymach, John V., primary, Gibbons, Don L., primary, Plodkowski, Andrew J., primary, Ravichandran, Vignesh, primary, Donoghue, Mark T.A., primary, Vanderbilt, Chad, primary, Ladanyi, Marc, primary, Rudin, Charles M., primary, Kris, Mark G., primary, Riely, Gregory J., primary, Chaft, Jamie E., primary, Hellmann, Matthew D., primary, Vokes, Natalie I., primary, Awad, Mark M., primary, and Schoenfeld, Adam J., primary

Published

2023

32. Data from Clinical and Molecular Features of Long-term Response to Immune Checkpoint Inhibitors in Patients with Advanced Non–Small Cell Lung Cancer

Author

Thummalapalli, Rohit, primary, Ricciuti, Biagio, primary, Bandlamudi, Chaitanya, primary, Muldoon, Daniel, primary, Rizvi, Hira, primary, Elkrief, Arielle, primary, Luo, Jia, primary, Alessi, Joao V., primary, Pecci, Federica, primary, Lamberti, Giuseppe, primary, Di Federico, Alessandro, primary, Hong, Lingzhi, primary, Zhang, Jianjun, primary, Heymach, John V., primary, Gibbons, Don L., primary, Plodkowski, Andrew J., primary, Ravichandran, Vignesh, primary, Donoghue, Mark T.A., primary, Vanderbilt, Chad, primary, Ladanyi, Marc, primary, Rudin, Charles M., primary, Kris, Mark G., primary, Riely, Gregory J., primary, Chaft, Jamie E., primary, Hellmann, Matthew D., primary, Vokes, Natalie I., primary, Awad, Mark M., primary, and Schoenfeld, Adam J., primary

Published

2023

33. Supplemental Fig. 3 from The GENIE BPC NSCLC Cohort: A Real-World Repository Integrating Standardized Clinical and Genomic Data for 1,846 Patients with Non–Small Cell Lung Cancer

Author

Choudhury, Noura J., primary, Lavery, Jessica A., primary, Brown, Samantha, primary, de Bruijn, Ino, primary, Jee, Justin, primary, Tran, Thinh Ngoc, primary, Rizvi, Hira, primary, Arbour, Kathryn C., primary, Whiting, Karissa, primary, Shen, Ronglai, primary, Hellmann, Matthew, primary, Bedard, Philippe L., primary, Yu, Celeste, primary, Leighl, Natasha, primary, LeNoue-Newton, Michele, primary, Micheel, Christine, primary, Warner, Jeremy L., primary, Ginsberg, Michelle S., primary, Plodkowski, Andrew, primary, Girshman, Jeffrey, primary, Sawan, Peter, primary, Pillai, Shirin, primary, Sweeney, Shawn M., primary, Kehl, Kenneth L., primary, Panageas, Katherine S., primary, Schultz, Nikolaus, primary, Schrag, Deborah, primary, and Riely, Gregory J., primary

Published

2023

34. Data from The GENIE BPC NSCLC Cohort: A Real-World Repository Integrating Standardized Clinical and Genomic Data for 1,846 Patients with Non–Small Cell Lung Cancer

Author

Choudhury, Noura J., primary, Lavery, Jessica A., primary, Brown, Samantha, primary, de Bruijn, Ino, primary, Jee, Justin, primary, Tran, Thinh Ngoc, primary, Rizvi, Hira, primary, Arbour, Kathryn C., primary, Whiting, Karissa, primary, Shen, Ronglai, primary, Hellmann, Matthew, primary, Bedard, Philippe L., primary, Yu, Celeste, primary, Leighl, Natasha, primary, LeNoue-Newton, Michele, primary, Micheel, Christine, primary, Warner, Jeremy L., primary, Ginsberg, Michelle S., primary, Plodkowski, Andrew, primary, Girshman, Jeffrey, primary, Sawan, Peter, primary, Pillai, Shirin, primary, Sweeney, Shawn M., primary, Kehl, Kenneth L., primary, Panageas, Katherine S., primary, Schultz, Nikolaus, primary, Schrag, Deborah, primary, and Riely, Gregory J., primary

Published

2023

35. Supplemental Table 1 from The GENIE BPC NSCLC Cohort: A Real-World Repository Integrating Standardized Clinical and Genomic Data for 1,846 Patients with Non–Small Cell Lung Cancer

Author

Choudhury, Noura J., primary, Lavery, Jessica A., primary, Brown, Samantha, primary, de Bruijn, Ino, primary, Jee, Justin, primary, Tran, Thinh Ngoc, primary, Rizvi, Hira, primary, Arbour, Kathryn C., primary, Whiting, Karissa, primary, Shen, Ronglai, primary, Hellmann, Matthew, primary, Bedard, Philippe L., primary, Yu, Celeste, primary, Leighl, Natasha, primary, LeNoue-Newton, Michele, primary, Micheel, Christine, primary, Warner, Jeremy L., primary, Ginsberg, Michelle S., primary, Plodkowski, Andrew, primary, Girshman, Jeffrey, primary, Sawan, Peter, primary, Pillai, Shirin, primary, Sweeney, Shawn M., primary, Kehl, Kenneth L., primary, Panageas, Katherine S., primary, Schultz, Nikolaus, primary, Schrag, Deborah, primary, and Riely, Gregory J., primary

Published

2023

36. Supplemental Fig. 2 from The GENIE BPC NSCLC Cohort: A Real-World Repository Integrating Standardized Clinical and Genomic Data for 1,846 Patients with Non–Small Cell Lung Cancer

Author

Choudhury, Noura J., primary, Lavery, Jessica A., primary, Brown, Samantha, primary, de Bruijn, Ino, primary, Jee, Justin, primary, Tran, Thinh Ngoc, primary, Rizvi, Hira, primary, Arbour, Kathryn C., primary, Whiting, Karissa, primary, Shen, Ronglai, primary, Hellmann, Matthew, primary, Bedard, Philippe L., primary, Yu, Celeste, primary, Leighl, Natasha, primary, LeNoue-Newton, Michele, primary, Micheel, Christine, primary, Warner, Jeremy L., primary, Ginsberg, Michelle S., primary, Plodkowski, Andrew, primary, Girshman, Jeffrey, primary, Sawan, Peter, primary, Pillai, Shirin, primary, Sweeney, Shawn M., primary, Kehl, Kenneth L., primary, Panageas, Katherine S., primary, Schultz, Nikolaus, primary, Schrag, Deborah, primary, and Riely, Gregory J., primary

Published

2023

37. Supplemental Table 2 from The GENIE BPC NSCLC Cohort: A Real-World Repository Integrating Standardized Clinical and Genomic Data for 1,846 Patients with Non–Small Cell Lung Cancer

Author

Choudhury, Noura J., primary, Lavery, Jessica A., primary, Brown, Samantha, primary, de Bruijn, Ino, primary, Jee, Justin, primary, Tran, Thinh Ngoc, primary, Rizvi, Hira, primary, Arbour, Kathryn C., primary, Whiting, Karissa, primary, Shen, Ronglai, primary, Hellmann, Matthew, primary, Bedard, Philippe L., primary, Yu, Celeste, primary, Leighl, Natasha, primary, LeNoue-Newton, Michele, primary, Micheel, Christine, primary, Warner, Jeremy L., primary, Ginsberg, Michelle S., primary, Plodkowski, Andrew, primary, Girshman, Jeffrey, primary, Sawan, Peter, primary, Pillai, Shirin, primary, Sweeney, Shawn M., primary, Kehl, Kenneth L., primary, Panageas, Katherine S., primary, Schultz, Nikolaus, primary, Schrag, Deborah, primary, and Riely, Gregory J., primary

Published

2023

38. Supplemental Table 4 from The GENIE BPC NSCLC Cohort: A Real-World Repository Integrating Standardized Clinical and Genomic Data for 1,846 Patients with Non–Small Cell Lung Cancer

Author

Choudhury, Noura J., primary, Lavery, Jessica A., primary, Brown, Samantha, primary, de Bruijn, Ino, primary, Jee, Justin, primary, Tran, Thinh Ngoc, primary, Rizvi, Hira, primary, Arbour, Kathryn C., primary, Whiting, Karissa, primary, Shen, Ronglai, primary, Hellmann, Matthew, primary, Bedard, Philippe L., primary, Yu, Celeste, primary, Leighl, Natasha, primary, LeNoue-Newton, Michele, primary, Micheel, Christine, primary, Warner, Jeremy L., primary, Ginsberg, Michelle S., primary, Plodkowski, Andrew, primary, Girshman, Jeffrey, primary, Sawan, Peter, primary, Pillai, Shirin, primary, Sweeney, Shawn M., primary, Kehl, Kenneth L., primary, Panageas, Katherine S., primary, Schultz, Nikolaus, primary, Schrag, Deborah, primary, and Riely, Gregory J., primary

Published

2023

39. Supplemental Fig. 1 from The GENIE BPC NSCLC Cohort: A Real-World Repository Integrating Standardized Clinical and Genomic Data for 1,846 Patients with Non–Small Cell Lung Cancer

Author

Choudhury, Noura J., primary, Lavery, Jessica A., primary, Brown, Samantha, primary, de Bruijn, Ino, primary, Jee, Justin, primary, Tran, Thinh Ngoc, primary, Rizvi, Hira, primary, Arbour, Kathryn C., primary, Whiting, Karissa, primary, Shen, Ronglai, primary, Hellmann, Matthew, primary, Bedard, Philippe L., primary, Yu, Celeste, primary, Leighl, Natasha, primary, LeNoue-Newton, Michele, primary, Micheel, Christine, primary, Warner, Jeremy L., primary, Ginsberg, Michelle S., primary, Plodkowski, Andrew, primary, Girshman, Jeffrey, primary, Sawan, Peter, primary, Pillai, Shirin, primary, Sweeney, Shawn M., primary, Kehl, Kenneth L., primary, Panageas, Katherine S., primary, Schultz, Nikolaus, primary, Schrag, Deborah, primary, and Riely, Gregory J., primary

Published

2023

40. Supplemental Table 3 from The GENIE BPC NSCLC Cohort: A Real-World Repository Integrating Standardized Clinical and Genomic Data for 1,846 Patients with Non–Small Cell Lung Cancer

Author

Choudhury, Noura J., primary, Lavery, Jessica A., primary, Brown, Samantha, primary, de Bruijn, Ino, primary, Jee, Justin, primary, Tran, Thinh Ngoc, primary, Rizvi, Hira, primary, Arbour, Kathryn C., primary, Whiting, Karissa, primary, Shen, Ronglai, primary, Hellmann, Matthew, primary, Bedard, Philippe L., primary, Yu, Celeste, primary, Leighl, Natasha, primary, LeNoue-Newton, Michele, primary, Micheel, Christine, primary, Warner, Jeremy L., primary, Ginsberg, Michelle S., primary, Plodkowski, Andrew, primary, Girshman, Jeffrey, primary, Sawan, Peter, primary, Pillai, Shirin, primary, Sweeney, Shawn M., primary, Kehl, Kenneth L., primary, Panageas, Katherine S., primary, Schultz, Nikolaus, primary, Schrag, Deborah, primary, and Riely, Gregory J., primary

Published

2023

41. PD-L1 expression, tumor mutational burden, and response to immunotherapy in patients with MET exon 14 altered lung cancers

Author

Sabari, J.K., Leonardi, G.C., Shu, C.A., Umeton, R., Montecalvo, J., Ni, A., Chen, R., Dienstag, J., Mrad, C., Bergagnini, I., Lai, W.V., Offin, M., Arbour, K.C., Plodkowski, A.J., Halpenny, D.F., Paik, P.K., Li, B.T., Riely, G.J., Kris, M.G., Rudin, C.M., Sholl, L.M., Nishino, M., Hellmann, M.D., Rekhtman, N., Awad, M.M., and Drilon, A.

Published

2018

42. CT features of HER2-mutant lung adenocarcinomas

Author

Sawan, Peter, Plodkowski, Andrew J., Li, Angela E., Li, Bob T., Drilon, Alexander, Capanu, Marinela, and Ginsberg, Michelle S.

Published

2018

43. Negative association of antibiotics on clinical activity of immune checkpoint inhibitors in patients with advanced renal cell and non-small-cell lung cancer

Author

Derosa, L., Hellmann, M.D., Spaziano, M., Halpenny, D., Fidelle, M., Rizvi, H., Long, N., Plodkowski, A.J., Arbour, K.C., Chaft, J.E., Rouche, J.A., Zitvogel, L., Zalcman, G., Albiges, L., Escudier, B., and Routy, B.

Published

2018

44. Brief Report: Combination of Osimertinib and Dacomitinib to Mitigate Primary and Acquired Resistance in EGFR-Mutant Lung Adenocarcinomas

Author

Arielle Elkrief, Alex Makhnin, Khadeja A. Moses, Linda S. Ahn, Isabel R. Preeshagul, Afsheen N. Iqbal, Sara A. Hayes, Andrew J. Plodkowski, Paul K. Paik, Marc Ladanyi, Mark G. Kris, Gregory J. Riely, Franziska Michor, and Helena A. Yu

Subjects

Cancer Research, Oncology

Abstract

Purpose: Primary and acquired resistance to osimertinib remain significant challenges for patients with EGFR-mutant lung cancers. Acquired EGFR alterations such as EGFR T790M or C797S mediate resistance to EGFR tyrosine kinase inhibitors (TKI) and combination therapy with dual EGFR TKIs may prevent or reverse on-target resistance. Patients and Methods: We conducted two prospective, phase I/II trials assessing combination osimertinib and dacomitinib to address on-target resistance in the primary and acquired resistance settings. In the initial therapy study, patients received dacomitinib and osimertinib in combination as initial therapy. In the acquired resistance trial, dacomitinib with or without osimertinib was administered to patients with EGFR-mutant lung cancers with disease progression on osimertinib alone and evidence of an acquired EGFR second-site mutation. Results: Cutaneous toxicities occurred in 93% (any grade) of patients and diarrhea in 72% (any grade) with the combination. As initial therapy, the overall response to the combination was 73% [95% confidence interval (CI), 50%–88%]. No acquired secondary alterations in EGFR were observed in any patients at progression. In the acquired resistance setting, the overall response was 14% (95% CI, 1%–58%). Conclusions: We observed no acquired secondary EGFR alterations with dual inhibition of EGFR as up-front treatment, but this regimen was associated with greater toxicity. The combination was not effective in reversing acquired resistance after development of a second-site acquired EGFR alteration. Our study highlights the need to develop better strategies to address on-target resistance in patients with EGFR-mutant lung cancers.

Published

2023

45. Outcomes to first-line pembrolizumab in patients with PD-L1-high (≥50%) non–small cell lung cancer and a poor performance status

Author

Mark Awad, Mizuki Nishino, Mehmet Altan, Biagio Ricciuti, Fangxin Hong, Matthew Hellmann, John V Heymach, Joao V Alessi, Elizabeth Jiménez-Aguilar, Zihan Wei, Andrew J Plodkowski, Peter Sawan, Jia Luo, Hira Rizvi, and Brett W Carter

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Background Patients with non–small cell lung cancer (NSCLC) and a poor Eastern Cooperative Oncology Group Performance Status (ECOG PS) have been excluded from phase III immunotherapy clinical trials. We sought to evaluate clinical outcomes to first-line pembrolizumab in patients with advanced NSCLC, a PD-L1 Tumor Proportion Score (TPS) of ≥50%, and an ECOG PS of 2.Methods We performed a multicenter retrospective analysis of patients with metastatic NSCLC and a PD-L1 TPS of ≥50% (negative for genomic alterations in EGFR and ALK) who received treatment with first-line pembrolizumab. Clinical outcomes were compared in patients based on ECOG PS.Results Among the 234 patients, 83.3% (n=195) had an ECOG PS of 0 or 1, and 16.7% (n=39) had an ECOG PS of 2. The baseline clinicopathological characteristics were balanced between the ECOG PS 0–1 vs 2 groups in terms of age, sex, tobacco use, histology, KRAS mutation status, presence of other potentially targetable driver mutations (BRAF, MET, HER2, RET), presence of brain metastases, and PD-L1 TPS distribution. Compared with patients with an ECOG PS of 0 or 1, patients with an ECOG PS of 2 had a significantly lower objective response rate (43.1% vs 25.6%; p=0.04), a numerically shorter median progression-free survival (6.6 months vs 4.0 months; HR 0.70 (95% CI 0.47 to 1.06); p=0.09), and a significantly shorter median overall survival (20.3 months vs 7.4 months; HR 0.42 (95% CI 0.26 to 0.68); p

Published

2020

46. Safety of combining thoracic radiation therapy with concurrent versus sequential immune checkpoint inhibition

Author

Donata von Reibnitz, BS, Jamie E. Chaft, MD, Abraham J. Wu, MD, Robert Samstein, MD, PhD, Matthew D. Hellmann, MD, Andrew J. Plodkowski, MD, Zhigang Zhang, PhD, Weiji Shi, MS, Rosalind Dick-Godfrey, BS, Kelly H. Panchoo, BA, Christopher A. Barker, MD, and Andreas Rimner, MD

Subjects

Medical physics. Medical radiology. Nuclear medicine, R895-920, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Purpose: The objective of this study was to evaluate adverse events (AEs) in patients who received both immune checkpoint inhibitors and thoracic radiation therapy (RT). In particular, we compared the rate of toxicities of concurrent versus sequential delivery of thoracic RT and checkpoint inhibitors. Methods and Materials: Patient and treatment characteristics were collected on all patients at our institution who were treated with programmed cell death protein 1 (PD-1), programmed death-ligand 1 (PD-L1), and/or cytotoxic T-lymphocyte-associated protein 4 (CTLA-4) inhibitors and underwent thoracic RT (n = 79). Receiving both treatments within 1 month was considered concurrent (n = 35; 44%), and any treatment up to 6 months apart was considered sequential (n = 44; 56%). The primary endpoint of this study was the rate of Grade ≥2 AEs from combination therapy (immunotherapy and RT), specifically those that are relevant to thoracic RT: Pneumonitis, other pulmonary events, esophagitis, dermatitis, and fatigue. Further univariate analysis was performed to compare AE rates with clinical and therapy-related variables. Results: A total of 79 patients were identified, with lung cancer (n = 45) and melanoma (n = 15) being the most common primary histology. Sixty-two (78%) patients were treated with anti-PD-1 or anti-PD-L1 antibodies, 12 (15%) with anti-CTLA-4 antibodies, and 5 (6%) received both anti-PD-1/PD-L1 and anti-CTLA-4 antibodies. The median follow-up for survivors was 5.9 months (range, 2.4-55.6 months). Grade ≥2 AEs included pneumonitis (n = 5; 6%), esophagitis (n = 6; 8%), and dermatitis (n = 8; 10%). No statistically significant correlation was found between these AEs when comparing concurrent versus sequential treatment. The only significant variable was a correlation of immunotherapy drug category with Grade ≥2 esophagitis (P = .04). Conclusions: Overall, Grade ≥2 AE rates of thoracic RT and immunotherapy appeared as expected and acceptable. The lack of significant differences in AE rates with concurrent versus sequential treatment suggests that even concurrent immunotherapy and thoracic RT may be safe.

Published

2018

47. Outcomes of Combination Platinum-Doublet Chemotherapy and Anti-PD(L)-1 Blockade in KRASG12C-Mutant Non-Small Cell Lung Cancer

Author

Elkrief, Arielle, primary, Riccuiti, Biagio, additional, Alessi, Joao V, additional, Fei, Teng, additional, Kalvin, Hannah L, additional, Egger, Jacklynn V, additional, Rizvi, Hira, additional, Thummalapalli, Rohit, additional, Lamberti, Guiseppe, additional, Plodkowski, Andrew, additional, Hellmann, Matthew D, additional, Kris, Mark G, additional, Arcila, Maria E, additional, Baine, Marina K, additional, Rudin, Charles M, additional, Lito, Piro, additional, Ladanyi, Marc, additional, Schoenfeld, Adam J, additional, Riely, Gregory J, additional, Awad, Mark M, additional, and Arbour, Kathryn C, additional

Published

2023

48. Radiogenomic evaluation of lung cancer — Are there imaging characteristics associated with lung adenocarcinomas harboring BRAF mutations?

Author

Halpenny, Darragh F, Plodkowski, Andrew, Riely, Gregory, Zheng, Junting, Litvak, Anya, Moscowitz, Chaya, and Ginsberg, Michelle S

Published

2017

49. Cabozantinib in patients with advanced RET-rearranged non-small-cell lung cancer: an open-label, single-centre, phase 2, single-arm trial

Author

Drilon, Alexander, Rekhtman, Natasha, Arcila, Maria, Wang, Lu, Ni, Andy, Albano, Melanie, Van Voorthuysen, Martine, Somwar, Romel, Smith, Roger S, Montecalvo, Joseph, Plodkowski, Andrew, Ginsberg, Michelle S, Riely, Gregory J, Rudin, Charles M, Ladanyi, Marc, and Kris, Mark G

Published

2016

50. Prognostic utility of differential tissue characterization of cardiac neoplasm and thrombus via late gadolinium enhancement cardiovascular magnetic resonance among patients with advanced systemic cancer

Author

Angel T. Chan, Andrew J. Plodkowski, Shawn C. Pun, Yuliya Lakhman, Darragh F. Halpenny, Jiwon Kim, Samantha R. Goldburg, Mathew J. Matasar, Chaya S. Moskowitz, Dipti Gupta, Richard Steingart, and Jonathan W. Weinsaft

Subjects

Cardio-oncology, Cardiac metastases, Cardiac thrombus, Cardiac mass, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Abstract Background Late gadolinium enhancement (LGE-) cardiovascular magnetic resonance (CMR) is well-validated for cardiac mass (CMASS) tissue characterization to differentiate neoplasm (CNEO) from thrombus (CTHR): Prognostic implications of CMASS subtypes among systemic cancer patients are unknown. Methods CMASS + patients and controls (CMASS -) matched for cancer diagnosis and stage underwent a standardized CMR protocol, including LGE-CMR (IR-GRE) for tissue characterization and balanced steady state free precession cine-CMR (SSFP) for cardiac structure/function. CMASS subtypes (CNEO, CTHR) were respectively defined by presence or absence of enhancement on LGE-CMR; lesions were quantified for tissue properties (contrast-to-noise ratio (CNR); signal-to-noise ratio (SNR) and size. Clinical follow-up was performed to evaluate prognosis in relation to CMASS etiology. Results The study population comprised 126 patients with systemic neoplasms referred for CMR, of whom 50% (n = 63) had CMASS + (CNEO = 32%, CTHR = 18%). Cancer etiology differed between CNEO (sarcoma = 20%, lung = 18%) and CTHR (lymphoma = 30%, GI = 26%); cardiac function (left ventricular ejection fraction: 63 ± 9 vs. 62 ± 10%; p = 0.51∣ right ventricular ejection fraction: 53 ± 9 vs. 54 ± 8%; p = 0.47) and geometric indices were similar (all p = NS). LGE-CMR tissue properties assessed by CNR (13.1 ± 13.0 vs. 1.6 ± 1.0; p

Published

2017