Your search keyword '"Joshua K. Sabari"' showing total 100 results

1. Multiple synchronous primary lung adenocarcinomas with distinct epidermal growth factor receptor mutations: A case report

Author

Matthew Siskin and Joshua K. Sabari

Subjects

Lung cancer, EGFR, Osimertinib, Case report, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

An 83-year-old woman presents with two synchronous primary lung adenocarcinomas each harboring unique EGFR mutations, one classical and the other rare. She was treated with adjuvant Osimertinib following surgical lobectomy and remains well 44 months from the time of her diagnosis. Her case demonstrates the potential value in using EGFR third generation TKI monotherapy in patients with early-stage disease, harboring rare mutations and in patients with multiple primary cancers harboring targetable mutations. Further research into the use of targeted therapy in these areas is needed.

Published

2022

2. Dynamic Management of Lung Cancer Care During Surging COVID-19

Author

Annie Wang, Stephanie H. Chang, Eric J. Kim, Jamie L. Bessich, Joshua K. Sabari, Benjamin Cooper, Travis C. Geraci, and Robert J. Cerfolio

Subjects

lung cancer, thoracic surgery, COVID-19, radiation oncology, screening, Surgery, RD1-811

Abstract

Management of patients with lung cancer continues to be challenging during the COVID-19 pandemic, due to the increased risk of complications in this subset of patients. During the COVID-19 surge in New York City, New York University Langone Health adopted triage strategies to help with care for lung cancer patients, with good surgical outcomes and no transmission of COVID-19 to patients or healthcare workers. Here, we will review current recommendations regarding screening and management of lung cancer patients during both a non-surge phase and surge phase of COVID-19.

Published

2021

3. Next-generation sequencing based detection of germline and somatic alterations in a patient with four metachronous primary tumors

Author

Madhuri Martin, Joshua K. Sabari, Gulisa Turashvili, Darragh F. Halpenny, Hira Rizvi, Natalie Shapnik, and Vicky Makker

Subjects

Gynecology and obstetrics, RG1-991, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Introduction: Multiple primary tumors (MPTs) are defined as two or more separate synchronous or metachronous neoplasms occurring in different sites in the same individual. These tumors differ in histology, as well as primary sites from which they arise. Risk factors associated with the occurrence of MPTs include germline alterations, exposure to prior cancer therapies, occupational hazards, and lifestyle and behavioral influences. Case report: We present a case of a patient who was diagnosed with four metachronous primary tumors. In 2013, she was diagnosed with serous proliferations associated with psammomatous bodies of primary peritoneal origin (pT3NxM0). This was followed by invasive ductal carcinoma of the breast (stage pT2N0Mx, histological grade III/III) in 2014, melanoma (stage pT2bNxMx) in 2016 that further advanced to the lung and brain in 2017, and a low-grade lung carcinoid in 2017. To better understand the biology of this patient's MPTs, we performed next-generation sequencing (NGS) to assess for both somatic and germline alterations. The treatment course for this patient aims to target the tumor with the strongest prognostic value, namely her malignant melanoma, and has contributed favorably to the overall survival of this patient. Conclusion: We report the clinical and genomic landscape of a patient with MPTs who had no identifiable unique somatic or germline mutations to explain her predilection to cancer. The treatment course and overall prognosis for this patient is important for understanding future cases with unrelated, metachronous MPTs, the occurrence of which cannot always be explained by underlying genetic mechanisms. Keywords: Multiple primary tumors, Next-generation sequencing, Tumor mutational burden, Immunotherapy

Published

2018

4. Management of infusion-related reactions (IRRs) in patients receiving amivantamab in the CHRYSALIS study

Author

Keunchil Park, Joshua K. Sabari, Eric B. Haura, Catherine A. Shu, Alexander Spira, Ravi Salgia, Karen L. Reckamp, Rachel E. Sanborn, Ramaswamy Govindan, Joshua M. Bauml, Joshua C. Curtin, John Xie, Amy Roshak, Patricia Lorenzini, Dawn Millington, Meena Thayu, Roland E. Knoblauch, and Byoung Chul Cho

Subjects

Pulmonary and Respiratory Medicine, Cancer Research, Oncology

Published

2023

5. Seeing Beyond the Smoke: Reclassifying Lung Cancer by Smoking-Related Mutational Signatures

Author

Andre L. Moreira and Joshua K. Sabari

Subjects

Pulmonary and Respiratory Medicine, Oncology

Published

2023

6. First-in-Human Phase I/IB Dose-Finding Study of Adagrasib (MRTX849) in Patients With Advanced KRASG12C Solid Tumors (KRYSTAL-1)

Author

Sai-Hong Ignatius Ou, Pasi A. Jänne, Ticiana A. Leal, Igor I. Rybkin, Joshua K. Sabari, Minal A. Barve, Lyudmila Bazhenova, Melissa L. Johnson, Karen L. Velastegui, Cornelius Cilliers, James G. Christensen, Xiaohong Yan, Richard C. Chao, and Kyriakos P. Papadopoulos

Subjects

Cancer Research, Oncology

Abstract

PURPOSE Adagrasib (MRTX849) is an oral, highly selective, small-molecule, covalent inhibitor of KRASG12C. We report results from a phase I/IB study of adagrasib in non–small-cell lung cancer, colorectal cancer, and other solid tumors harboring the KRAS G12C mutation. MATERIALS AND METHODS Patients with advanced KRAS G12C-mutant solid tumors were treated with adagrasib 150 mg orally once daily, 300 mg once daily, 600 mg once daily, 1,200 mg once daily, or 600 mg orally twice a day using an accelerated titration design, which transitioned to a modified toxicity probability interval design when a predefined degree of toxicity was observed or target adagrasib exposure was achieved. Safety, pharmacokinetics, and clinical activity were evaluated. RESULTS Twenty-five patients were enrolled and received at least one dose of adagrasib. The recommended phase II dose (RP2D) was 600 mg twice a day on the basis of safety, tolerability, and observed pharmacokinetics properties. No maximum tolerated dose was formally defined. After a median follow-up of 19.6 months, eight of 15 patients (53.3%; 95% CI, 26.6 to 78.7) with RECIST-evaluable KRAS G12C-mutant non–small-cell lung cancer treated at 600 mg twice a day achieved a confirmed partial response. The median duration of response was 16.4 months (95% CI, 3.1 to not estimable). The median progression-free survival was 11.1 months (95% CI, 2.6 to not estimable). One of two patients with KRAS G12C-mutant colorectal cancer treated at 600 mg twice a day achieved a partial response (duration of response, 4.2 months). At the RP2D, the most common treatment-related adverse events (any grade) were nausea (80.0%), diarrhea (70.0%), vomiting (50.0%), and fatigue (45.0%). The most common grade 3-4 treatment-related adverse event was fatigue (15.0%). CONCLUSION Adagrasib 600 mg twice a day was well tolerated and exhibited antitumor activity in patients with advanced solid tumors harboring the KRAS G12C mutation.

Published

2022

7. Adagrasib in Non–Small-Cell Lung Cancer Harboring a KRASG12C Mutation

Author

Pasi A. Jänne, Gregory J. Riely, Shirish M. Gadgeel, Rebecca S. Heist, Sai-Hong I. Ou, Jose M. Pacheco, Melissa L. Johnson, Joshua K. Sabari, Konstantinos Leventakos, Edwin Yau, Lyudmila Bazhenova, Marcelo V. Negrao, Nathan A. Pennell, Jun Zhang, Kenna Anderes, Hirak Der-Torossian, Thian Kheoh, Karen Velastegui, Xiaohong Yan, James G. Christensen, Richard C. Chao, and Alexander I. Spira

Subjects

General Medicine

Published

2022

8. Adagrasib in Advanced Solid Tumors Harboring a KRASG12C Mutation

Author

Tanios S. Bekaii-Saab, Rona Yaeger, Alexander I. Spira, Meredith S. Pelster, Joshua K. Sabari, Navid Hafez, Minal Barve, Karen Velastegui, Xiaohong Yan, Aditya Shetty, Hirak Der-Torossian, and Shubham Pant

Subjects

Cancer Research, Oncology

Abstract

PURPOSE Adagrasib, a KRASG12C inhibitor, has demonstrated clinical activity in patients with KRASG12C-mutated non-small cell lung cancer (NSCLC) and colorectal cancer (CRC). KRASG12C mutations occur rarely in other solid tumor types. We report evaluation of the clinical activity and safety of adagrasib in patients with other solid tumors harboring a KRASG12C mutation. METHODS In this phase II cohort of the KRYSTAL-1 study (NCT03785249; https://www.clinicaltrials.gov/ct2/show/NCT03785249 ; phase Ib cohort), we evaluated adagrasib (600 mg orally twice daily) in patients with KRASG12C-mutated advanced solid tumors (excluding NSCLC and CRC). The primary endpoint was objective response rate. Secondary endpoints included duration of response, progression-free survival, overall survival, and safety. RESULTS As of October 1, 2022, 64 patients with KRASG12C-mutated solid tumors were enrolled and 63 patients treated (median follow-up, 16.8 months). The median number of prior lines of systemic therapy was 2. Among 57 patients with measurable disease at baseline, objective responses were observed in 20 (35.1%) patients (all partial responses), including 7/21 (33.3%) responses in pancreatic and 5/12 (41.7%) in biliary tract cancers. The median duration of response was 5.3 months (95% confidence interval [CI], 2.8 to 7.3) and median progression-free survival was 7.4 months (95% CI, 5.3 to 8.6). Treatment-related adverse events (TRAEs) of any grade were observed in 96.8% of patients and grade 3 to 4 in 27.0%; there were no grade 5 TRAEs. TRAEs did not lead to treatment discontinuation in any patients. CONCLUSION Adagrasib demonstrates encouraging clinical activity and is well tolerated in this rare cohort of pretreated patients with KRASG12C-mutated solid tumors.

Published

2023

9. Activity of Adagrasib (MRTX849) in Brain Metastases: Preclinical Models and Clinical Data from Patients with KRASG12C-Mutant Non–Small Cell Lung Cancer

Author

Joshua K. Sabari, Vamsidhar Velcheti, Kazuhide Shimizu, Matthew R. Strickland, Rebecca S. Heist, Mohini Singh, Naema Nayyar, Anita Giobbie-Hurder, Subba R. Digumarthy, Justin F. Gainor, Anant P. Rajan, Edwin Nieblas-Bedolla, Aaron C. Burns, Jill Hallin, Peter Olson, James G. Christensen, Sylvia C. Kurz, Priscilla K. Brastianos, and Hiroaki Wakimoto

Subjects

Proto-Oncogene Proteins p21(ras), Mice, Cancer Research, Acetonitriles, Lung Neoplasms, Pyrimidines, Oncology, Brain Neoplasms, Carcinoma, Non-Small-Cell Lung, Animals, Humans, Piperazines, Retrospective Studies

Abstract

Purpose: Patients with KRAS-mutant non–small cell lung cancer (NSCLC) with brain metastases (BM) have a poor prognosis. Adagrasib (MRTX849), a potent oral small-molecule KRASG12C inhibitor, irreversibly and selectively binds KRASG12C, locking it in its inactive state. Adagrasib has been optimized for favorable pharmacokinetic properties, including long half-life (∼24 hours), extensive tissue distribution, dose-dependent pharmacokinetics, and central nervous system penetration; however, BM-specific antitumor activity of KRASG12C inhibitors remains to be fully characterized. Experimental Design: A retrospective database query identified patients with KRAS-mutant NSCLC to understand their propensity to develop BM. Preclinical studies assessed physiochemical and pharmacokinetic properties of adagrasib. Mice bearing intracranial KRASG12C-mutant NSCLC xenografts (LU99-Luc/H23-Luc/LU65-Luc) were treated with clinically relevant adagrasib doses, and levels of adagrasib in plasma, cerebrospinal fluid (CSF), and brain were determined along with antitumor activity. Preliminary clinical data were collected from 2 patients with NSCLC with untreated BM who had received adagrasib 600 mg twice daily in the phase Ib cohort of the KRYSTAL-1 trial; CSF was collected, adagrasib concentrations measured, and antitumor activity in BM evaluated. Results: Patients with KRAS-mutant NSCLC demonstrated high propensity to develop BM (≥40%). Adagrasib penetrated into CSF and demonstrated tumor regression and extended survival in multiple preclinical BM models. In 2 patients with NSCLC and untreated BM, CSF concentrations of adagrasib measured above the target cellular IC50. Both patients demonstrated corresponding BM regression, supporting potential clinical activity of adagrasib in the brain. Conclusions: These data support further development of adagrasib in patients with KRASG12C-mutant NSCLC with untreated BM. See related commentary by Kommalapati and Mansfield, p. 3179

Published

2022

10. Data from Activation of KRAS Mediates Resistance to Targeted Therapy in MET Exon 14–mutant Non–small Cell Lung Cancer

Author

Romel Somwar, Marc Ladanyi, Alexander Drilon, William W. Lockwood, Maria E. Arcila, Mark G. Kris, Charles M. Rudin, Elisa de Stanchina, Inna Khodos, Marissa Mattar, Huichun Tai, Joshua K. Sabari, Roger S. Smith, Morana Vojnic, Christopher Kurzatkowski, Daniel Lu, Michael Offin, and Ken Suzawa

Abstract

Purpose:MET exon 14 splice site alterations that cause exon skipping at the mRNA level (METex14) are actionable oncogenic drivers amenable to therapy with MET tyrosine kinase inhibitors (TKI); however, secondary resistance eventually arises in most cases while other tumors display primary resistance. Beyond relatively uncommon on-target MET kinase domain mutations, mechanisms underlying primary and acquired resistance remain unclear.Experimental Design:We examined clinical and genomic data from 113 patients with lung cancer with METex14. MET TKI resistance due to KRAS mutation was functionally evaluated using in vivo and in vitro models.Results:Five of 113 patients (4.4%) with METex14 had concurrent KRAS G12 mutations, a rate of KRAS cooccurrence significantly higher than in other major driver-defined lung cancer subsets. In one patient, the KRAS mutation was acquired post-crizotinib, while the remaining 4 METex14 patients harbored the KRAS mutation prior to MET TKI therapy. Gene set enrichment analysis of transcriptomic data from lung cancers with METex14 revealed preferential activation of the KRAS pathway. Moreover, expression of oncogenic KRAS enhanced MET expression. Using isogenic and patient-derived models, we show that KRAS mutation results in constitutive activation of RAS/ERK signaling and resistance to MET inhibition. Dual inhibition of MET or EGFR/ERBB2 and MEK reduced growth of cell line and xenograft models.Conclusions:KRAS mutation is a recurrent mechanism of primary and secondary resistance to MET TKIs in METex14 lung cancers. Dual inhibition of MET or EGFR/ERBB2 and MEK may represent a potential therapeutic approach in this molecular cohort.

Published

2023

11. Supplemental Tables from Comprehensive Molecular and Clinicopathologic Analysis of 200 Pulmonary Invasive Mucinous Adenocarcinomas Identifies Distinct Characteristics of Molecular Subtypes

Author

Natasha Rekhtman, Alexander Drilon, Marc Ladanyi, William D. Travis, Maria E. Arcila, Alison M. Schram, Bob T. Li, Laetitia Borsu, Khedoudja Nafa, Ryma Benayed, Joshua K. Sabari, Sarah Teed, Valerie W. Rusch, Prasad S. Adusumilli, Kyuichi Kadota, Patrice Desmeules, Joseph Montecalvo, Sharon Amir, Helen H. Won, Vasilisa A. Rudneva, Fanli Meng, Brian R. Houck-Loomis, David Brown, Christina Falcon, Michael Offin, and Jason C. Chang

Abstract

Supplemental Tables 1-11

Published

2023

12. Supplementary Figure from Activity of Adagrasib (MRTX849) in Brain Metastases: Preclinical Models and Clinical Data from Patients with KRASG12C-Mutant Non–Small Cell Lung Cancer

Author

Hiroaki Wakimoto, Priscilla K. Brastianos, Sylvia C. Kurz, James G. Christensen, Peter Olson, Jill Hallin, Aaron C. Burns, Edwin Nieblas-Bedolla, Anant P. Rajan, Justin F. Gainor, Subba R. Digumarthy, Anita Giobbie-Hurder, Naema Nayyar, Mohini Singh, Rebecca S. Heist, Matthew R. Strickland, Kazuhide Shimizu, Vamsidhar Velcheti, and Joshua K. Sabari

Abstract

Supplementary Figure from Activity of Adagrasib (MRTX849) in Brain Metastases: Preclinical Models and Clinical Data from Patients with KRASG12C-Mutant Non–Small Cell Lung Cancer

Published

2023

13. Supplemental Methods 2 from Comprehensive Molecular and Clinicopathologic Analysis of 200 Pulmonary Invasive Mucinous Adenocarcinomas Identifies Distinct Characteristics of Molecular Subtypes

Author

Natasha Rekhtman, Alexander Drilon, Marc Ladanyi, William D. Travis, Maria E. Arcila, Alison M. Schram, Bob T. Li, Laetitia Borsu, Khedoudja Nafa, Ryma Benayed, Joshua K. Sabari, Sarah Teed, Valerie W. Rusch, Prasad S. Adusumilli, Kyuichi Kadota, Patrice Desmeules, Joseph Montecalvo, Sharon Amir, Helen H. Won, Vasilisa A. Rudneva, Fanli Meng, Brian R. Houck-Loomis, David Brown, Christina Falcon, Michael Offin, and Jason C. Chang

Abstract

Supplemental Methods 2

Published

2023

14. Figure S6 from Activation of KRAS Mediates Resistance to Targeted Therapy in MET Exon 14–mutant Non–small Cell Lung Cancer

Author

Romel Somwar, Marc Ladanyi, Alexander Drilon, William W. Lockwood, Maria E. Arcila, Mark G. Kris, Charles M. Rudin, Elisa de Stanchina, Inna Khodos, Marissa Mattar, Huichun Tai, Joshua K. Sabari, Roger S. Smith, Morana Vojnic, Christopher Kurzatkowski, Daniel Lu, Michael Offin, and Ken Suzawa

Abstract

Tumor volume changes and body weight changes in vivo in treated LUAD12C xenografts.

Published

2023

15. Supplemental Figure 1 from Comprehensive Molecular and Clinicopathologic Analysis of 200 Pulmonary Invasive Mucinous Adenocarcinomas Identifies Distinct Characteristics of Molecular Subtypes

Author

Natasha Rekhtman, Alexander Drilon, Marc Ladanyi, William D. Travis, Maria E. Arcila, Alison M. Schram, Bob T. Li, Laetitia Borsu, Khedoudja Nafa, Ryma Benayed, Joshua K. Sabari, Sarah Teed, Valerie W. Rusch, Prasad S. Adusumilli, Kyuichi Kadota, Patrice Desmeules, Joseph Montecalvo, Sharon Amir, Helen H. Won, Vasilisa A. Rudneva, Fanli Meng, Brian R. Houck-Loomis, David Brown, Christina Falcon, Michael Offin, and Jason C. Chang

Abstract

Supplemental Figure 1. Consort diagram summarizing the molecular workflow of cases.

Published

2023

16. Supplemental Figure 3 from Comprehensive Molecular and Clinicopathologic Analysis of 200 Pulmonary Invasive Mucinous Adenocarcinomas Identifies Distinct Characteristics of Molecular Subtypes

Author

Natasha Rekhtman, Alexander Drilon, Marc Ladanyi, William D. Travis, Maria E. Arcila, Alison M. Schram, Bob T. Li, Laetitia Borsu, Khedoudja Nafa, Ryma Benayed, Joshua K. Sabari, Sarah Teed, Valerie W. Rusch, Prasad S. Adusumilli, Kyuichi Kadota, Patrice Desmeules, Joseph Montecalvo, Sharon Amir, Helen H. Won, Vasilisa A. Rudneva, Fanli Meng, Brian R. Houck-Loomis, David Brown, Christina Falcon, Michael Offin, and Jason C. Chang

Abstract

Supplemental Figure 3. Comparison of overall and recurrence-free survival in TP53-wild type and TP53-mutant IMAs

Published

2023

17. Supplementary Tables from Activation of KRAS Mediates Resistance to Targeted Therapy in MET Exon 14–mutant Non–small Cell Lung Cancer

Author

Romel Somwar, Marc Ladanyi, Alexander Drilon, William W. Lockwood, Maria E. Arcila, Mark G. Kris, Charles M. Rudin, Elisa de Stanchina, Inna Khodos, Marissa Mattar, Huichun Tai, Joshua K. Sabari, Roger S. Smith, Morana Vojnic, Christopher Kurzatkowski, Daniel Lu, Michael Offin, and Ken Suzawa

Abstract

Supplementary Tables 1A and 1B

Published

2023

18. Supplemental Methods 1 from Comprehensive Molecular and Clinicopathologic Analysis of 200 Pulmonary Invasive Mucinous Adenocarcinomas Identifies Distinct Characteristics of Molecular Subtypes

Author

Natasha Rekhtman, Alexander Drilon, Marc Ladanyi, William D. Travis, Maria E. Arcila, Alison M. Schram, Bob T. Li, Laetitia Borsu, Khedoudja Nafa, Ryma Benayed, Joshua K. Sabari, Sarah Teed, Valerie W. Rusch, Prasad S. Adusumilli, Kyuichi Kadota, Patrice Desmeules, Joseph Montecalvo, Sharon Amir, Helen H. Won, Vasilisa A. Rudneva, Fanli Meng, Brian R. Houck-Loomis, David Brown, Christina Falcon, Michael Offin, and Jason C. Chang

Abstract

Supplemental Methods 1

Published

2023

19. Data from Comprehensive Molecular and Clinicopathologic Analysis of 200 Pulmonary Invasive Mucinous Adenocarcinomas Identifies Distinct Characteristics of Molecular Subtypes

Author

Natasha Rekhtman, Alexander Drilon, Marc Ladanyi, William D. Travis, Maria E. Arcila, Alison M. Schram, Bob T. Li, Laetitia Borsu, Khedoudja Nafa, Ryma Benayed, Joshua K. Sabari, Sarah Teed, Valerie W. Rusch, Prasad S. Adusumilli, Kyuichi Kadota, Patrice Desmeules, Joseph Montecalvo, Sharon Amir, Helen H. Won, Vasilisa A. Rudneva, Fanli Meng, Brian R. Houck-Loomis, David Brown, Christina Falcon, Michael Offin, and Jason C. Chang

Abstract

Purpose:Invasive mucinous adenocarcinoma (IMA) is a unique subtype of lung adenocarcinoma, characterized genomically by frequent KRAS mutations or specific gene fusions, most commonly involving NRG1. Comprehensive analysis of a large series of IMAs using broad DNA- and RNA-sequencing methods is still lacking, and it remains unclear whether molecular subtypes of IMA differ clinicopathologically.Experimental Design:A total of 200 IMAs were analyzed by 410-gene DNA next-generation sequencing (MSK-IMPACT; n = 136) or hotspot 8-oncogene genotyping (n = 64). Driver-negative cases were further analyzed by 62-gene RNA sequencing (MSK-Fusion) and those lacking fusions were further tested by whole-exome sequencing and whole-transcriptome sequencing (WTS).Results:Combined MSK-IMPACT and MSK-Fusion testing identified mutually exclusive driver alterations in 96% of IMAs, including KRAS mutations (76%), NRG1 fusions (7%), ERBB2 alterations (6%), and other less common events. In addition, WTS identified a novel NRG2 fusion (F11R–NRG2). Overall, targetable gene fusions were identified in 51% of KRAS wild-type IMAs, leading to durable responses to targeted therapy in some patients. Compared with KRAS-mutant IMAs, NRG1-rearranged tumors exhibited several more aggressive characteristics, including worse recurrence-free survival (P < 0.0001).Conclusions:This is the largest molecular study of IMAs to date, where we demonstrate the presence of a major oncogenic driver in nearly all cases. This study is the first to document more aggressive characteristics of NRG1-rearranged IMAs, ERBB2 as the third most common alteration, and a novel NRG2 fusion in these tumors. Comprehensive molecular testing of KRAS wild-type IMAs that includes fusion testing is essential, given the high prevalence of alterations with established and investigational targeted therapies in this subset.

Published

2023

20. Supplementary Data from Activity of Adagrasib (MRTX849) in Brain Metastases: Preclinical Models and Clinical Data from Patients with KRASG12C-Mutant Non–Small Cell Lung Cancer

Author

Hiroaki Wakimoto, Priscilla K. Brastianos, Sylvia C. Kurz, James G. Christensen, Peter Olson, Jill Hallin, Aaron C. Burns, Edwin Nieblas-Bedolla, Anant P. Rajan, Justin F. Gainor, Subba R. Digumarthy, Anita Giobbie-Hurder, Naema Nayyar, Mohini Singh, Rebecca S. Heist, Matthew R. Strickland, Kazuhide Shimizu, Vamsidhar Velcheti, and Joshua K. Sabari

Abstract

Supplementary Data from Activity of Adagrasib (MRTX849) in Brain Metastases: Preclinical Models and Clinical Data from Patients with KRASG12C-Mutant Non–Small Cell Lung Cancer

Published

2023

21. Data from Activity of Adagrasib (MRTX849) in Brain Metastases: Preclinical Models and Clinical Data from Patients with KRASG12C-Mutant Non–Small Cell Lung Cancer

Author

Hiroaki Wakimoto, Priscilla K. Brastianos, Sylvia C. Kurz, James G. Christensen, Peter Olson, Jill Hallin, Aaron C. Burns, Edwin Nieblas-Bedolla, Anant P. Rajan, Justin F. Gainor, Subba R. Digumarthy, Anita Giobbie-Hurder, Naema Nayyar, Mohini Singh, Rebecca S. Heist, Matthew R. Strickland, Kazuhide Shimizu, Vamsidhar Velcheti, and Joshua K. Sabari

Abstract

Purpose:Patients with KRAS-mutant non–small cell lung cancer (NSCLC) with brain metastases (BM) have a poor prognosis. Adagrasib (MRTX849), a potent oral small-molecule KRASG12C inhibitor, irreversibly and selectively binds KRASG12C, locking it in its inactive state. Adagrasib has been optimized for favorable pharmacokinetic properties, including long half-life (∼24 hours), extensive tissue distribution, dose-dependent pharmacokinetics, and central nervous system penetration; however, BM-specific antitumor activity of KRASG12C inhibitors remains to be fully characterized.Experimental Design:A retrospective database query identified patients with KRAS-mutant NSCLC to understand their propensity to develop BM. Preclinical studies assessed physiochemical and pharmacokinetic properties of adagrasib. Mice bearing intracranial KRASG12C-mutant NSCLC xenografts (LU99-Luc/H23-Luc/LU65-Luc) were treated with clinically relevant adagrasib doses, and levels of adagrasib in plasma, cerebrospinal fluid (CSF), and brain were determined along with antitumor activity. Preliminary clinical data were collected from 2 patients with NSCLC with untreated BM who had received adagrasib 600 mg twice daily in the phase Ib cohort of the KRYSTAL-1 trial; CSF was collected, adagrasib concentrations measured, and antitumor activity in BM evaluated.Results:Patients with KRAS-mutant NSCLC demonstrated high propensity to develop BM (≥40%). Adagrasib penetrated into CSF and demonstrated tumor regression and extended survival in multiple preclinical BM models. In 2 patients with NSCLC and untreated BM, CSF concentrations of adagrasib measured above the target cellular IC50. Both patients demonstrated corresponding BM regression, supporting potential clinical activity of adagrasib in the brain.Conclusions:These data support further development of adagrasib in patients with KRASG12C-mutant NSCLC with untreated BM.See related commentary by Kommalapati and Mansfield, p. 3179

Published

2023

22. Supplemental Figure 4 from Comprehensive Molecular and Clinicopathologic Analysis of 200 Pulmonary Invasive Mucinous Adenocarcinomas Identifies Distinct Characteristics of Molecular Subtypes

Author

Natasha Rekhtman, Alexander Drilon, Marc Ladanyi, William D. Travis, Maria E. Arcila, Alison M. Schram, Bob T. Li, Laetitia Borsu, Khedoudja Nafa, Ryma Benayed, Joshua K. Sabari, Sarah Teed, Valerie W. Rusch, Prasad S. Adusumilli, Kyuichi Kadota, Patrice Desmeules, Joseph Montecalvo, Sharon Amir, Helen H. Won, Vasilisa A. Rudneva, Fanli Meng, Brian R. Houck-Loomis, David Brown, Christina Falcon, Michael Offin, and Jason C. Chang

Abstract

Supplemental Figure 4. Comparison of overall and recurrence-free survival in CDKN2A-wild type and CDKN2A-mutant IMAs.

Published

2023

23. Supplementary Methods from Activation of KRAS Mediates Resistance to Targeted Therapy in MET Exon 14–mutant Non–small Cell Lung Cancer

Author

Romel Somwar, Marc Ladanyi, Alexander Drilon, William W. Lockwood, Maria E. Arcila, Mark G. Kris, Charles M. Rudin, Elisa de Stanchina, Inna Khodos, Marissa Mattar, Huichun Tai, Joshua K. Sabari, Roger S. Smith, Morana Vojnic, Christopher Kurzatkowski, Daniel Lu, Michael Offin, and Ken Suzawa

Abstract

Supplementary Methods

Published

2023

24. Supplemental Figure 2 from Comprehensive Molecular and Clinicopathologic Analysis of 200 Pulmonary Invasive Mucinous Adenocarcinomas Identifies Distinct Characteristics of Molecular Subtypes

Author

Natasha Rekhtman, Alexander Drilon, Marc Ladanyi, William D. Travis, Maria E. Arcila, Alison M. Schram, Bob T. Li, Laetitia Borsu, Khedoudja Nafa, Ryma Benayed, Joshua K. Sabari, Sarah Teed, Valerie W. Rusch, Prasad S. Adusumilli, Kyuichi Kadota, Patrice Desmeules, Joseph Montecalvo, Sharon Amir, Helen H. Won, Vasilisa A. Rudneva, Fanli Meng, Brian R. Houck-Loomis, David Brown, Christina Falcon, Michael Offin, and Jason C. Chang

Abstract

Supplemental Figure 2. Detailed graphical visualizations of the F11R-NRG2 fusion.

Published

2023

25. Hitting the Right Spot: Advances in the Treatment of NSCLC With Uncommon EGFR Mutations

Author

Joshua K, Sabari, John V, Heymach, and Beth, Sandy

Subjects

ErbB Receptors, Lung Neoplasms, Oncology, Carcinoma, Non-Small-Cell Lung, Mutation, Humans, Protein Kinase Inhibitors, Early Detection of Cancer

Abstract

An understanding of the biology of uncommon epidermal growth factor receptor (EGFR) mutations in non–small cell lung cancer (NSCLC) is evolving. These mutations are important for the selection of targeted therapy and the development of resistance. The advent of genomic profiling has led to guideline-recommended molecular testing to identify patients with NSCLC who carry uncommonEGFRmutations to aid in the selection of appropriate targeted therapy. This article discusses the efficacy and safety of current and emerging targeted therapies for the treatment of uncommonEGFRmutations in NSCLC to aid in developing patient-specific treatment plans.

Published

2021

26. Presentation, Diagnosis and Management of Innominate Artery Thromboembolism

Author

Joshua K. Sabari, Navneet Narula, Heepeel Chang, Karan Garg, and Caron B. Rockman

Subjects

medicine.medical_specialty, business.industry, Subclavian Artery, medicine.disease, Treatment Outcome, medicine.anatomical_structure, Thromboembolism, Internal medicine, medicine.artery, medicine, Cardiology, Brachiocephalic artery, Humans, Female, Radiology, Nuclear Medicine and imaging, Surgery, Thromboembolic disease, Presentation (obstetrics), Cardiology and Cardiovascular Medicine, business, Stroke, Brachiocephalic Trunk, Aged, Thrombectomy, Artery

Abstract

Purpose: Acute thromboembolic disease of the innominate artery (IA) poses a unique set of therapeutic challenges, owing to its contribution to both the cerebral and upper extremity circulation, and risks of distal embolization via the carotid and subclavian arteries, respectively. Herein, we present a 74-year-old female who presents with acute IA thrombus treated successfully with right axillary and common carotid exposure and aspiration catheter-directed mechanical thrombectomy (CDT). Furthermore, an emerging use of CDT and its application in acute thromboembolism are outlined. Case report: A 74-year-old female with history of right lung transplant for pulmonary fibrosis with severe pulmonary hypertension, and stage IIIA left lung adenocarcinoma status post left lower lobectomy undergoing adjuvant chemotherapy presented with acute IA thrombus and right-sided stroke. She was treated successfully with right axillary and common carotid exposure and aspiration CDT. Computed tomography angiography performed 1 month postoperatively confirmed patent IA with no evidence of residual or recurrent thrombus. Conclusion: There are currently no standard guidelines on the management of acute IA thromboembolism, with mostly individual cases reported in the literature describing this rare entity. Nevertheless, this unique clinical entity mandates expeditious diagnostic and therapeutic approaches in order to avoid permanent neurologic deficits from distal embolization. Our case demonstrates that aspiration CDT may be an effective treatment modality for patients with acute IA thrombus.

Published

2021

27. Amivantamab in EGFR Exon 20 Insertion–Mutated Non–Small-Cell Lung Cancer Progressing on Platinum Chemotherapy: Initial Results From the CHRYSALIS Phase I Study

Author

Meena Thayu, A. Roshak, Jose Manuel Trigo, Jong Seok Lee, Keunchil Park, Santiago Viteri, Ramaswamy Govindan, Natasha B. Leighl, Ji-Youn Han, Paul Mitchell, Nahor Haddish-Berhane, James Chih-Hsin Yang, Chee Khoon Lee, Roland Elmar Knoblauch, Patricia Lorenzini, Byoung Chul Cho, Dawn Millington, Nicolas Girard, Alexander I. Spira, Tsung-Ying Yang, Rachel E. Sanborn, Eric B. Haura, J.C. Curtin, Matthew G Krebs, Pilar Garrido, Koichi Goto, Sang-We Kim, Dong Wan Kim, Karen L. Reckamp, Ki Hyeong Lee, Joshua Bauml, Joshua K. Sabari, Catherine A. Shu, and John Xie

Subjects

Adult, Diarrhea, Male, 0301 basic medicine, Cancer Research, Lung Neoplasms, Neutropenia, Organoplatinum Compounds, Hypokalemia, 03 medical and health sciences, Exon, Antineoplastic Agents, Immunological, 0302 clinical medicine, Carcinoma, Non-Small-Cell Lung, Antibodies, Bispecific, Platinum chemotherapy, Humans, Medicine, Epidermal growth factor receptor, Paronychia, Lung cancer, Aged, Aged, 80 and over, Manchester Cancer Research Centre, biology, business.industry, ResearchInstitutes_Networks_Beacons/mcrc, Exons, Middle Aged, medicine.disease, Progression-Free Survival, Injection Site Reaction, Phase i study, ErbB Receptors, Mutagenesis, Insertional, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Retreatment, Disease Progression, Cancer research, biology.protein, Female, Drug Eruptions, Non small cell, Pulmonary Embolism, business, Tyrosine kinase

Abstract

PURPOSE Non–small-cell lung cancer (NSCLC) with epidermal growth factor receptor ( EGFR) exon 20 insertion (Exon20ins) mutations exhibits inherent resistance to approved tyrosine kinase inhibitors. Amivantamab, an EGFR-MET bispecific antibody with immune cell–directing activity, binds to each receptor's extracellular domain, bypassing resistance at the tyrosine kinase inhibitor binding site. METHODS CHRYSALIS is a phase I, open-label, dose-escalation, and dose-expansion study, which included a population with EGFR Exon20ins NSCLC. The primary end points were dose-limiting toxicity and overall response rate. We report findings from the postplatinum EGFR Exon20ins NSCLC population treated at the recommended phase II dose of 1,050 mg amivantamab (1,400 mg, ≥ 80 kg) given once weekly for the first 4 weeks and then once every 2 weeks starting at week 5. RESULTS In the efficacy population (n = 81), the median age was 62 years (range, 42-84 years); 40 patients (49%) were Asian, and the median number of previous lines of therapy was two (range, 1-7). The overall response rate was 40% (95% CI, 29 to 51), including three complete responses, with a median duration of response of 11.1 months (95% CI, 6.9 to not reached). The median progression-free survival was 8.3 months (95% CI, 6.5 to 10.9). In the safety population (n = 114), the most common adverse events were rash in 98 patients (86%), infusion-related reactions in 75 (66%), and paronychia in 51 (45%). The most common grade 3-4 adverse events were hypokalemia in six patients (5%) and rash, pulmonary embolism, diarrhea, and neutropenia in four (4%) each. Treatment-related dose reductions and discontinuations were reported in 13% and 4% of patients, respectively. CONCLUSION Amivantamab, via its novel mechanism of action, yielded robust and durable responses with tolerable safety in patients with EGFR Exon20ins mutations after progression on platinum-based chemotherapy.

Published

2021

28. Clinicopathologic Features and Response to Therapy ofNRG1Fusion–Driven Lung Cancers: The eNRGy1 Global Multicenter Registry

Author

Michael Duruisseaux, Philippe Brun, Valérie Gounant, Alison M. Schram, Maria E. Arcila, Yonina R. Murciano-Goroff, Miguel Angel Molina, Masaoki Ito, Morihito Okada, Joshua K. Sabari, Denis Moro-Sibilot, Clarisse Dupont, Christina Falcon, Lucia Anna Muscarella, Alexa B. Schrock, Torsten Blum, Alexander Drilon, Marie Wislez, Robert C. Doebele, Haiquan Chen, Eva Brandén, Siraj M. Ali, Fanny Magne, Misako Nagasaka, D. Ross Camidge, Sai-Hong Ignatius Ou, Giulio Rossi, Jin-Yuan Shih, Viola W. Zhu, Jacques Cadranel, Soo-Ryum Yang, Maurice Pérol, Isabelle Monnet, Stephen V. Liu, Rafael Rosell, and Ji Youn Han

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Lung, Response to therapy, business.industry, MEDLINE, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Text mining, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Internal medicine, medicine, Multiple tumors, business

Abstract

PURPOSEAlthough NRG1 fusions are oncogenic drivers across multiple tumor types including lung cancers, these are difficult to study because of their rarity. The global eNRGy1 registry was thus established to characterize NRG1 fusion–positive lung cancers in the largest and most diverse series to date.METHODSFrom June 2018 to February 2020, a consortium of 22 centers from nine countries in Europe, Asia, and the United States contributed data from patients with pathologically confirmed NRG1 fusion–positive lung cancers. Profiling included DNA-based and/or RNA-based next-generation sequencing and fluorescence in situ hybridization. Anonymized clinical, pathologic, molecular, and response (RECIST v1.1) data were centrally curated and analyzed.RESULTSAlthough the typified never smoking (57%), mucinous adenocarcinoma (57%), and nonmetastatic (71%) phenotype predominated in 110 patients with NRG1 fusion–positive lung cancer, further diversity, including in smoking history (43%) and histology (43% nonmucinous and 6% nonadenocarcinoma), was elucidated. RNA-based testing identified most fusions (74%). Molecularly, six (of 18) novel 5′ partners, 20 unique epidermal growth factor domain–inclusive chimeric events, and heterogeneous 5′/3′ breakpoints were found. Platinum-doublet and taxane-based (post–platinum-doublet) chemotherapy achieved low objective response rates (ORRs 13% and 14%, respectively) and modest progression-free survival medians (PFS 5.8 and 4.0 months, respectively). Consistent with a low programmed death ligand-1 expressing (28%) and low tumor mutational burden (median: 0.9 mutations/megabase) immunophenotype, the activity of chemoimmunotherapy and single-agent immunotherapy was poor (ORR 0%/PFS 3.3 months and ORR 20%/PFS 3.6 months, respectively). Afatinib achieved an ORR of 25%, not contingent on fusion type, and a 2.8-month median PFS.CONCLUSIONNRG1 fusion–positive lung cancers were molecularly, pathologically, and clinically more heterogeneous than previously recognized. The activity of cytotoxic, immune, and targeted therapies was disappointing. Further research examining NRG1-rearranged tumor biology is needed to develop new therapeutic strategies.

Published

2021

29. KRYSTAL-1: Activity and safety of adagrasib (MRTX849) in patients with advanced solid tumors harboring a KRASG12C mutation

Author

Shubham Pant, Rona Yaeger, Alexander I. Spira, Meredith Pelster, Joshua K. Sabari, Navid Hafez, Minal A. Barve, Karen Velastegui, Xiaohong Yan, Hirak Der-Torossian, and Tanios S. Bekaii-Saab

Subjects

Cancer Research, Oncology

Abstract

425082 Background: KRAS, a mediator of signalling pathways essential for cellular growth, proliferation, and survival, is the most frequently mutated oncogene in cancer. Notably, KRAS mutations occur in ~90% of pancreatic cancers, of which ~2% are KRASG12C mutations. Other gastrointestinal (GI) tumors also harbor KRASG12C mutations, such as biliary tract cancer (BTC; 1%) and appendiceal cancer (3–4%), and they are also seen in non-GI tumors, such as endometrial and ovarian cancer (1–2%). Adagrasib, a covalent KRASG12C inhibitor that irreversibly and selectively binds KRASG12C in its inactive state, was selected for favorable properties, including long half-life (23 h), dose-dependent pharmacokinetics, and central nervous system penetration. Methods: KRYSTAL-1 is a multicohort phase 1/2 study (NCT03785249) evaluating adagrasib in patients (pts) with advanced solid tumors harboring a KRASG12C mutation. Here we report data from a phase 2 cohort evaluating adagrasib monotherapy administered orally at 600 mg BID in pts with unresectable or metastatic KRASG12C-mutated solid tumors (excluding non-small cell lung cancer and colorectal cancer), including pancreatic ductal adenocarcinoma (PDAC), BTC, other GI, and non-GI tumors. Study objectives include evaluation of clinical activity (ORR, DCR, DOR, PFS, OS) and safety. Results: As of October 1, 2022, 64 pts with KRASG12C-mutated solid tumors were enrolled and 63 were treated with adagrasib (median follow-up, 16.8 months); of these, 21 pts had PDAC, 12 BTC, 16 other GI tumors (9 appendiceal, 4 gastro-esophageal junction/esophageal, 3 small bowel), and 14 non-GI tumors (5 ovarian, 4 unknown primary, 3 endometrial, 1 breast, 1 glioblastoma). Overall, median age was 65 years, 61% had ECOG PS 1, and median prior lines of systemic therapy was 2. Among 57 pts with measurable disease (blinded independent central review), ORR was 35.1% (20/57; all partial responses); DCR was 86.0% (49/57); median DOR was 5.3 months (n=20; 95% CI 2.8–7.3); median PFS was 7.4 months (95% CI 5.3–8.6); and median OS was 14.0 months (n=64; 95% CI 8.5–18.6). Among 21 pts with PDAC, ORR was 33.3% (7/21); DCR was 81.0% (17/21); median PFS was 5.4 months (95% CI 3.9–8.2); and median OS was 8.0 months (95% CI 5.2–11.8). Among 12 pts with BTC, ORR was 41.7% (5/12); DCR was 91.7% (11/12); median PFS was 8.6 months (95% CI 2.7–11.3); and median OS was 15.1 months (95% CI 8.6–not estimable). Overall (n=63), treatment-related adverse events (TRAEs) of any grade were observed in 96.8% of pts (most commonly [≥20%] nausea [49.2%], diarrhea [47.6%], fatigue [41.3%], vomiting [39.7%]), grade 3 TRAEs in 25.4%, and grade 4 TRAEs in 1.6%. No grade 5 TRAE occurred. Conclusions: Adagrasib is well tolerated and demonstrates promising clinical activity in pretreated pts with PDAC, BTC, and other solid tumors harboring a KRASG12C mutation. Clinical trial information: NCT03785249 .

Published

2023

30. Common Germline Mutations in a Patient With Multiple Primary Lung Cancers

Author

Abraham Chachoua, Samuel Cytryn, Andre L. Moreira, and Joshua K. Sabari

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Cancer Research, Population, Bioinformatics, medicine.disease_cause, Germline, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Medicine, Stage (cooking), Lung cancer, education, Genetic testing, Mutation, education.field_of_study, medicine.diagnostic_test, business.industry, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, TSC1, business

Abstract

We report a case of a patient with multiple primary lung cancers (MPLC) each with a unique somatic mutation, but also with underlying germline mutations of BRCA2 and TSC1. Given the improvements in screening modalities and advances in therapies leading to longer survival, the incidence of MPLC has increased. This case highlights the possibility that patients with multiple primary malignancies, each with distinct driver mutations, may have an underlying, identifiable predisposition. Next generation sequencing (NGS) and germline genetic testing has not been well studied in early stage cancers. However, given the findings in this patient, it may be reasonable to consider those with MPLC for additional testing as the implications of identifying such an underlying mutation will help guide treatment as well as inform screening for affected family members, though further investigation in this population is warranted.

Published

2020

31. The incidence and predictors of new brain metastases in patients with non-small cell lung cancer following discontinuation of systemic therapy

Author

Dennis London, Dev N. Patel, Bernadine Donahue, Ralph E. Navarro, Jason Gurewitz, Joshua S. Silverman, Erik Sulman, Kenneth Bernstein, Amy Palermo, John G. Golfinos, Joshua K. Sabari, Elaine Shum, Vamsidhar Velcheti, Abraham Chachoua, and Douglas Kondziolka

Subjects

General Medicine

Abstract

OBJECTIVE Patients with non–small cell lung cancer (NSCLC) metastatic to the brain are living longer. The risk of new brain metastases when these patients stop systemic therapy is unknown. The authors hypothesized that the risk of new brain metastases remains constant for as long as patients are off systemic therapy. METHODS A prospectively collected registry of patients undergoing radiosurgery for brain metastases was analyzed. Of 606 patients with NSCLC, 63 met the inclusion criteria of discontinuing systemic therapy for at least 90 days and undergoing active surveillance. The risk factors for the development of new tumors were determined using Cox proportional hazards and recurrent events models. RESULTS The median duration to new brain metastases off systemic therapy was 16.0 months. The probability of developing an additional new tumor at 6, 12, and 18 months was 26%, 40%, and 53%, respectively. There were no additional new tumors 22 months after stopping therapy. Patients who discontinued therapy due to intolerance or progression of the disease and those with mutations in RAS or receptor tyrosine kinase (RTK) pathways (e.g., KRAS, EGFR) were more likely to develop new tumors (hazard ratio [HR] 2.25, 95% confidence interval [CI] 1.33–3.81, p = 2.5 × 10−3; HR 2.51, 95% CI 1.45–4.34, p = 9.8 × 10−4, respectively). CONCLUSIONS The rate of new brain metastases from NSCLC in patients off systemic therapy decreases over time and is uncommon 2 years after cessation of cancer therapy. Patients who stop therapy due to toxicity or who have RAS or RTK pathway mutations have a higher rate of new metastases and should be followed more closely.

Published

2021

32. Immune checkpoint inhibitors for patients with advanced lung cancer and oncogenic driver alterations: results from the IMMUNOTARGET registry

Author

Alexis B. Cortot, Sébastien Couraud, M. van den Heuvel, Julie Milia, Benjamin Besse, S-H.I. Ou, Sacha I. Rothschild, Mickaël Lattuca-Truc, Laura Mezquita, Joel W. Neal, Rafael Rosell, Amélie Lusque, R.D. Schouten, Terry L. Ng, Martin Früh, Marcel Wiesweg, Benjamin Solomon, D.R. Camidge, Nir Peled, C. Mascaux, Gérard Zalcman, Alexander Drilon, Alessandra Curioni-Fontecedro, Heather A. Wakelee, Alex Martinez-Marti, Paolo Bironzo, Julien Mazieres, Sanjay Popat, Valérie Gounant, Laurent Mhanna, Remi Veillon, Viola W. Zhu, Oliver Gautschi, Fabrice Barlesi, Joshua K. Sabari, Silvia Novello, A. Thai, Joachim Diebold, Rangueil-Larrey University Hospital, Université Toulouse III - Paul Sabatier (UT3), Université Fédérale Toulouse Midi-Pyrénées-Université Fédérale Toulouse Midi-Pyrénées, Centre de Recherche en Cancérologie de Marseille (CRCM), Aix Marseille Université (AMU)-Institut Paoli-Calmettes, Fédération nationale des Centres de lutte contre le Cancer (FNCLCC)-Fédération nationale des Centres de lutte contre le Cancer (FNCLCC)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Service de pneumologie [Centre Hospitalier Lyon Sud - HCL], Centre Hospitalier Lyon Sud [CHU - HCL] (CHLS), Hospices Civils de Lyon (HCL)-Hospices Civils de Lyon (HCL), CHU Tenon [AP-HP], Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Intergroupe Francophone de Cancérologie Thoracique [Paris] (IFCT), Intergroupe Francophone de Cancérologie thoracique, Service d'oncologie multidisciplinaire innovations thérapeutiques [Hôpital Nord - APHM], Assistance Publique - Hôpitaux de Marseille (APHM)- Hôpital Nord [CHU - APHM], Centre Hospitalier Universitaire de Toulouse (CHU Toulouse), and Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)

Subjects

0301 basic medicine, Oncology, Male, Lung Neoplasms, [SDV]Life Sciences [q-bio], Programmed Cell Death 1 Receptor, Medizin, medicine.disease_cause, B7-H1 Antigen, Antineoplastic Agents, Immunological, 0302 clinical medicine, Carcinoma, Non-Small-Cell Lung, Antineoplastic Combined Chemotherapy Protocols, 80 and over, Registries, Non-Small-Cell Lung, Lung, Cancer, Aged, 80 and over, Tumor, Hematology, Middle Aged, Chemotherapy regimen, Progression-Free Survival, 3. Good health, Immunotherapy-lung cancer-oncogenic addiction, Editorial Commentary, Immunological, Response Evaluation Criteria in Solid Tumors, 5.1 Pharmaceuticals, 030220 oncology & carcinogenesis, Adenocarcinoma, Female, KRAS, immunotherapy, Development of treatments and therapeutic interventions, hormones, hormone substitutes, and hormone antagonists, Adult, medicine.medical_specialty, Clinical Trials and Supportive Activities, Oncology and Carcinogenesis, Context (language use), Antineoplastic Agents, and over, [SDV.BC]Life Sciences [q-bio]/Cellular Biology, Rare cancers Radboud Institute for Molecular Life Sciences [Radboudumc 9], 03 medical and health sciences, Clinical Research, Internal medicine, Biomarkers, Tumor, medicine, ROS1, Humans, Progression-free survival, Oncology & Carcinogenesis, Lung cancer, oncogenic addiction, neoplasms, Retrospective Studies, Aged, Thoracic tumor, business.industry, Carcinoma, Oncogenes, medicine.disease, respiratory tract diseases, lung cancer, 030104 developmental biology, Good Health and Well Being, Mutation, business, Biomarkers

Abstract

Contains fulltext : 215810.pdf (Publisher’s version ) (Closed access) BACKGROUND: Anti-PD1/PD-L1 directed immune checkpoint inhibitors (ICI) are widely used to treat patients with advanced non-small-cell lung cancer (NSCLC). The activity of ICI across NSCLC harboring oncogenic alterations is poorly characterized. The aim of our study was to address the efficacy of ICI in the context of oncogenic addiction. PATIENTS AND METHODS: We conducted a retrospective study for patients receiving ICI monotherapy for advanced NSCLC with at least one oncogenic driver alteration. Anonymized data were evaluated for clinicopathologic characteristics and outcomes for ICI therapy: best response (RECIST 1.1), progression-free survival (PFS), and overall survival (OS) from ICI initiation. The primary end point was PFS under ICI. Secondary end points were best response (RECIST 1.1) and OS from ICI initiation. RESULTS: We studied 551 patients treated in 24 centers from 10 countries. The molecular alterations involved KRAS (n = 271), EGFR (n = 125), BRAF (n = 43), MET (n = 36), HER2 (n = 29), ALK (n = 23), RET (n = 16), ROS1 (n = 7), and multiple drivers (n = 1). Median age was 60 years, gender ratio was 1 : 1, never/former/current smokers were 28%/51%/21%, respectively, and the majority of tumors were adenocarcinoma. The objective response rate by driver alteration was: KRAS = 26%, BRAF = 24%, ROS1 = 17%, MET = 16%, EGFR = 12%, HER2 = 7%, RET = 6%, and ALK = 0%. In the entire cohort, median PFS was 2.8 months, OS 13.3 months, and the best response rate 19%. In a subgroup analysis, median PFS (in months) was 2.1 for EGFR, 3.2 for KRAS, 2.5 for ALK, 3.1 for BRAF, 2.5 for HER2, 2.1 for RET, and 3.4 for MET. In certain subgroups, PFS was positively associated with PD-L1 expression (KRAS, EGFR) and with smoking status (BRAF, HER2). CONCLUSIONS: : ICI induced regression in some tumors with actionable driver alterations, but clinical activity was lower compared with the KRAS group and the lack of response in the ALK group was notable. Patients with actionable tumor alterations should receive targeted therapies and chemotherapy before considering immunotherapy as a single agent.

Published

2019

33. Tumour exosomal CEMIP protein promotes cancer cell colonization in brain metastasis

Author

Etienne Meylan, David R. Jones, Navneet Narula, Jinxiang Dai, Shahin Rafii, Yuan Liu, Henrik Molina, Irene Casanova-Salas, Han Sang Kim, Irina Matei, David J. Pisapia, Alberto Benito-Martin, Quincey LaPlant, Joshua K. Sabari, Milica Tesic Mark, David Lyden, Candia M. Kenific, Daniela Freitas, Sandra J. Shin, Xinran Jiang, Nasser K. Altorki, Yonathan Ararso, Katharine Offer, Paula S. Ginter, Brian D. Dill, Loïc Steiner, Vinagolu K. Rajasekhar, Brunilde Gril, Huajuan Wang, Maria de Sousa, Gonçalo Rodrigues, Chaitanya R. Badwe, Héctor Peinado, Shizhen Emily Wang, Tyler M. Lu, Bruno Costa-Silva, Haiying Zhang, Patricia S. Steeg, Cyrus M. Ghajar, Ayuko Hoshino, Weston Buehring, John H. Healey, Charles M. Rudin, Peter R. Oxley, Linda Bojmar, Ilana Scandariato, and Jacqueline Bromberg

Subjects

Angiogenesis, Chemokine CXCL1, Nude, Cell, Inbred C57BL, Exosomes, Medical and Health Sciences, Metastasis, angiogenesis, Mice, Chemokine CCL1, 0302 clinical medicine, Cell Movement, Tumor Microenvironment, 2.1 Biological and endogenous factors, Neoplasm Metastasis, Aetiology, Cancer, 0303 health sciences, Tumor, Neovascularization, Pathologic, Brain Neoplasms, Brain, Biological Sciences, Tumor Burden, Cell biology, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, 030220 oncology & carcinogenesis, medicine.symptom, extracellular vesicles, Signal Transduction, growth, Mice, Nude, Hyaluronoglucosaminidase, Inflammation, Article, Cell Line, 03 medical and health sciences, Rare Diseases, Cell Line, Tumor, medicine, Animals, Humans, gene, Neovascularization, Cell Proliferation, 030304 developmental biology, Pathologic, Neoplastic, Tumor Necrosis Factor-alpha, Cell growth, business.industry, Neurosciences, Endothelial Cells, Cell Biology, medicine.disease, Survival Analysis, Xenograft Model Antitumor Assays, Microvesicles, Mice, Inbred C57BL, Gene Expression Regulation, Cyclooxygenase 2, kiaa1199, Cancer cell, Cancer research, business, Developmental Biology, Brain metastasis

Abstract

The development of effective therapies against brain metastasis is currently hindered by limitations in our understanding of the molecular mechanisms driving it. Here we define the contributions of tumour-secreted exosomes to brain metastatic colonization and demonstrate that pre-conditioning the brain microenvironment with exosomes from brain metastatic cells enhances cancer cell outgrowth. Proteomic analysis identified cell migration-inducing and hyaluronan-binding protein (CEMIP) as elevated in exosomes from brain metastatic but not lung or bone metastatic cells. CEMIP depletion in tumour cells impaired brain metastasis, disrupting invasion and tumour cell association with the brain vasculature, phenotypes rescued by pre-conditioning the brain microenvironment with CEMIP+ exosomes. Moreover, uptake of CEMIP+ exosomes by brain endothelial and microglial cells induced endothelial cell branching and inflammation in the perivascular niche by upregulating the pro-inflammatory cytokines encoded by Ptgs2, Tnf and Ccl/Cxcl, known to promote brain vascular remodelling and metastasis. CEMIP was elevated in tumour tissues and exosomes from patients with brain metastasis and predicted brain metastasis progression and patient survival. Collectively, our findings suggest that targeting exosomal CEMIP could constitute a future avenue for the prevention and treatment of brain metastasis.

Published

2019

34. Stage IV lung carcinoids: spectrum and evolution of proliferation rate, focusing on variants with elevated proliferation indices

Author

Marc Ladanyi, Wei-Chu Lai, Ai Ni, David S. Klimstra, Isabel Ruth Preeshagul, Anna Maria Litvak, Jason C. Chang, Maria Lauren Santos-Zabala, Charles M. Rudin, M.C. Pietanza, Natasha Rekhtman, Patrice Desmeules, Joseph Montecalvo, Amanda Beras, William D. Travis, and Joshua K. Sabari

Subjects

Adult, Male, carcinoid, 0301 basic medicine, Pathology, medicine.medical_specialty, Lung Neoplasms, Mitotic index, Mitosis, Carcinoid Tumor, Article, lung, Pathology and Forensic Medicine, Diagnosis, Differential, 03 medical and health sciences, 0302 clinical medicine, Predictive Value of Tests, Proliferation rate, Biomarkers, Tumor, Mitotic Index, Humans, Medicine, In patient, small cell carcinoma, large cell neuroendocrine carcinoma, Aged, Cell Proliferation, Neoplasm Staging, Aged, 80 and over, MIB1, Lung, business.industry, Middle Aged, medicine.disease, Primary tumor, 3. Good health, Neuroendocrine Carcinomas, Neuroendocrine Tumors, Ki-67 Antigen, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Predictive value of tests, Disease Progression, Ki-67, Female, Stage iv, business

Abstract

The spectrum and evolution of proliferation rates in stage IV lung carcinoids is poorly defined. In particular, there are limited data on the prevalence and characteristics of tumors exceeding the standard upper proliferative criteria—as defined largely based on early-stage carcinoids—in metastatic setting. Sixty-six patients with stage IV lung carcinoids were identified, and all evaluable samples (n = 132; mean 2 samples per patient) were analyzed for mitotic counts and Ki-67 rate. Clinicopathologic and genomic features associated with elevated proliferation rates (>10 mitoses per 2 mm2 and/or >20% hot-spot Ki-67), and evolution of proliferation rates in serial specimens were analyzed. We found that mitoses and/or Ki-67 exceeded the standard criteria in 35 of 132 (27%) samples, primarily (31/35 cases) at metastatic sites. Although neuroendocrine neoplasms with >10 mitoses per 2 mm2 are currently regarded as de facto neuroendocrine carcinomas, the notion that these cases are part of the spectrum of carcinoids was supported by (1) well-differentiated morphology, (2) conventional proliferation rates in other samples from same patient, (3) genetic characteristics, including the lack of RB1/TP53 alterations in all tested samples (n = 19), and (4) median overall survival of 2.7 years, compared to

Published

2019

35. Comprehensive Molecular and Clinicopathologic Analysis of 200 Pulmonary Invasive Mucinous Adenocarcinomas Identifies Distinct Characteristics of Molecular Subtypes

Author

Brian Houck-Loomis, Joshua K. Sabari, Ryma Benayed, Laetitia Borsu, Kyuichi Kadota, Helen Won, Prasad S. Adusumilli, Alison M. Schram, Maria E. Arcila, Jason C. Chang, Vasilisa A. Rudneva, Natasha Rekhtman, Sarah Teed, Valerie W. Rusch, Christina Falcon, Khedoudja Nafa, Marc Ladanyi, Patrice Desmeules, Michael Offin, Fanli Meng, Bob T. Li, William D. Travis, Alexander Drilon, David N Brown, Sharon Amir, and Joseph Montecalvo

Subjects

0301 basic medicine, Adult, Male, Cancer Research, Lung Neoplasms, medicine.medical_treatment, Biology, medicine.disease_cause, Mutually exclusive events, Article, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Neoplasm Invasiveness, Gene, Genotyping, Aged, Aged, 80 and over, High prevalence, Middle Aged, medicine.disease, Adenocarcinoma, Mucinous, Mucinous Adenocarcinomas, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Mutation, Cancer research, Adenocarcinoma, Female, KRAS

Abstract

Purpose:Invasive mucinous adenocarcinoma (IMA) is a unique subtype of lung adenocarcinoma, characterized genomically by frequent KRAS mutations or specific gene fusions, most commonly involving NRG1. Comprehensive analysis of a large series of IMAs using broad DNA- and RNA-sequencing methods is still lacking, and it remains unclear whether molecular subtypes of IMA differ clinicopathologically.Experimental Design:A total of 200 IMAs were analyzed by 410-gene DNA next-generation sequencing (MSK-IMPACT; n = 136) or hotspot 8-oncogene genotyping (n = 64). Driver-negative cases were further analyzed by 62-gene RNA sequencing (MSK-Fusion) and those lacking fusions were further tested by whole-exome sequencing and whole-transcriptome sequencing (WTS).Results:Combined MSK-IMPACT and MSK-Fusion testing identified mutually exclusive driver alterations in 96% of IMAs, including KRAS mutations (76%), NRG1 fusions (7%), ERBB2 alterations (6%), and other less common events. In addition, WTS identified a novel NRG2 fusion (F11R–NRG2). Overall, targetable gene fusions were identified in 51% of KRAS wild-type IMAs, leading to durable responses to targeted therapy in some patients. Compared with KRAS-mutant IMAs, NRG1-rearranged tumors exhibited several more aggressive characteristics, including worse recurrence-free survival (P < 0.0001).Conclusions:This is the largest molecular study of IMAs to date, where we demonstrate the presence of a major oncogenic driver in nearly all cases. This study is the first to document more aggressive characteristics of NRG1-rearranged IMAs, ERBB2 as the third most common alteration, and a novel NRG2 fusion in these tumors. Comprehensive molecular testing of KRAS wild-type IMAs that includes fusion testing is essential, given the high prevalence of alterations with established and investigational targeted therapies in this subset.

Published

2021

36. The Common Thread: A Case of Synchronous Lung Cancers and a Germline CHEK2 Mutation

Author

Edward T. Carey, Virginia Ferreira, Joshua K. Sabari, Fang Zhou, and Elaine Shum

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Oncology, Cancer Research, medicine.medical_specialty, Lung Neoplasms, Adenocarcinoma of Lung, medicine.disease_cause, Germline, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Internal medicine, Biopsy, medicine, Biomarkers, Tumor, Humans, skin and connective tissue diseases, Lung cancer, CHEK2, Germ-Line Mutation, Lung, medicine.diagnostic_test, business.industry, Cancer, Middle Aged, medicine.disease, Checkpoint Kinase 2, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Female, KRAS, business

Abstract

Patients with one form of cancer are at increased risk for another, and this is true for lung cancer, where synchronous primary lung cancers are an increasing multifaceted challenge.1,2 Here, we present the case of a middle age woman who was found to have bilateral lung masses. Biopsy and subsequent testing revealed unique synchronous lung adenocarcinomas, each with unique genetic signatures. Despite having two unique tumors, she was found to have CHEK2 mutations in both tumors and in germline testing. Because of this extensive testing that showed unique tumors, she was ultimately diagnosed with stage IIIb and IA2 lung cancers, and this changed her treatment options. Consideration of unique primary tumors leads to thorough diagnostics, which changed this patient's diagnosis, prognosis, and treatment. We hope this case raises awareness for multiple primary tumors, as well as CHEK2 as an important oncogene.

Published

2021

37. P10.08 Comparing Lung Cancer in Never Smokers and Ever Smokers in Asian or Asian American Patients Treated at a Tertiary Urban Public Hospital in New York

Author

Joshua K. Sabari, Abraham Chachoua, G. Kroening, Vamsidhar Velcheti, Kwok K. Wong, and Elaine Shum

Subjects

Pulmonary and Respiratory Medicine, Never smokers, medicine.medical_specialty, Oncology, business.industry, Asian americans, Family medicine, Public hospital, medicine, Lung cancer, medicine.disease, business

Published

2021

38. Dynamic Management of Lung Cancer Care During Surging COVID-19

Author

Robert J. Cerfolio, Stephanie H. Chang, Eric Kim, Benjamin T. Cooper, Travis C. Geraci, Jamie L. Bessich, Joshua K. Sabari, and Annie Wang

Subjects

medicine.medical_specialty, 2019-20 coronavirus outbreak, Coronavirus disease 2019 (COVID-19), lcsh:Surgery, Review, 030204 cardiovascular system & hematology, 03 medical and health sciences, 0302 clinical medicine, Health care, Pandemic, medicine, Intensive care medicine, Lung cancer, business.industry, screening, COVID-19, radiation oncology, lcsh:RD1-811, medicine.disease, Triage, thoracic surgery, lung cancer, Increased risk, 030220 oncology & carcinogenesis, Dynamic management, Surgery, business

Abstract

Management of patients with lung cancer continues to be challenging during the COVID-19 pandemic, due to the increased risk of complications in this subset of patients. During the COVID-19 surge in New York City, New York University Langone Health adopted triage strategies to help with care for lung cancer patients, with good surgical outcomes and no transmission of COVID-19 to patients or healthcare workers. Here, we will review current recommendations regarding screening and management of lung cancer patients during both a non-surge phase and surge phase of COVID-19.

Published

2021

39. Activity of adagrasib (MRTX849) in patients with KRASG12C-mutated NSCLC and active, untreated CNS metastases in the KRYSTAL-1 trial

Author

Joshua K. Sabari, Alexander I. Spira, Rebecca Suk Heist, Pasi A. Janne, Jose M. Pacheco, Jared Weiss, Shirish M. Gadgeel, Hirak Der-Torossian, Karen Velastegui, Thian Kheoh, James G Christensen, and Marcelo Vailati Negrao

Subjects

Cancer Research, Oncology

Abstract

LBA9009 Background: CNS metastases (mets) occur in 27–42% of NSCLC harboring KRASG12C mutations and are associated with poor prognosis. Adagrasib (ada), an investigational agent, is a KRASG12C inhibitor that irreversibly and selectively binds KRASG12C, locking it in its inactive state, and is optimized for favorable PK properties, including a long half-life (̃24 h) and dose-dependent PK. Ada has demonstrated dose-dependent CNS penetration and intracranial (IC) tumor regression in preclinical models of CNS mets. Methods: KRYSTAL-1 (NCT03785249) is a multicohort Phase 1/2 study evaluating ada as monotherapy or in combination with selected agents in patients (pts) with advanced solid tumors harboring a KRASG12C mutation. In a Phase 1b cohort, pts with KRASG12C-mutant NSCLC and active, untreated CNS mets were treated with ada 600 mg BID. The objectives for this Phase 1b cohort were to evaluate safety and clinical activity, including systemic and IC objective response rate (ORR) by blinded independent central review (BICR), duration of response (DOR), progression-free survival (PFS), and overall survival (OS). Systemic responses were assessed by RECIST 1.1; IC responses were assessed by modified RANO criteria and IC RECIST. Cerebrospinal fluid (CSF) was collected when feasible and was used to measure ada concentrations for optional evaluation. Results: As of 31 December 2021, 25 pts with NSCLC were enrolled and treated. Median follow-up was 6.6 months at the cutoff date. Median age was 66 years, 52% were female, 28%/72% had ECOG PS 0/1, and median lines of prior systemic therapy was one (range 0–4+). IC ORR per modified RANO criteria by BICR was 31.6% (6/19; 3 CRs, 2 PRs, 1 unconfirmed PR); IC disease control rate (DCR) was 84.2% (16/19, including 10 SDs). Median IC DOR was not reached (95% CI 4.1–NE); median IC PFS was 4.2 months (95% CI 3.8–NE). CSF samples were obtained for two pts for whom regression of CNS mets was observed and ada CSF concentrations exceeded the CNS penetrance partition coefficients observed for other therapies with demonstrated CNS penetration and CNS antitumor activity (Kp,uu 0.47). Systemic ORR by BICR was 35.0% (7/20), DCR was 80.0% (16/20) and median DOR was 9.6 months (95% CI 2.7–9.6); median PFS was 5.6 months (95% CI 3.8–11.0). For all pts enrolled, OS was immature, and the median had not been reached at the time of analysis. Safety was consistent with that previously reported with ada; any grade TRAEs occurred in 96% of pts, grade 3 TRAEs in 36%, and there were no grade 4/5 TRAEs. Further data describing IC activity assessed by IC RECIST will be presented. Conclusions: Ada was well tolerated, and these preliminary data demonstrate CNS penetration and encouraging IC activity in pretreated pts with NSCLC harboring a KRASG12C mutation and active, untreated CNS mets. These are the first clinical data demonstrating CNS-specific activity of a KRASG12C inhibitor in this population. Clinical trial information: NCT03785249.

Published

2022

40. KRYSTAL-1: Activity and safety of adagrasib (MRTX849) in patients with advanced/metastatic non–small cell lung cancer (NSCLC) harboring a KRASG12C mutation

Author

Alexander I. Spira, Gregory J. Riely, Shirish M. Gadgeel, Rebecca Suk Heist, Sai-Hong Ignatius Ou, Jose Maria Pacheco, Melissa Lynne Johnson, Joshua K. Sabari, Konstantinos Leventakos, Edwin Yau, Lyudmila Bazhenova, Marcelo Vailati Negrao, Nathan A. Pennell, Jun Zhang, Karen Velastegui, James G Christensen, xiaohong yan, Kenna Lynn Anderes, Richard C. Chao, and Pasi A. Janne

Subjects

Cancer Research, Oncology

Abstract

9002 Background: KRAS is a key mediator of the RAS/MAPK signaling cascade that promotes cellular growth and proliferation. KRASG12C mutation occurs in ̃14% of NSCLC. Adagrasib, an investigational agent, is a KRASG12C inhibitor that irreversibly and selectively binds KRASG12C, locking it in its inactive state. Adagrasib is optimized for favorable pharmacokinetic (PK) properties, including long half-life (̃24 h), dose-dependent PK, and central nervous system penetration; it has demonstrated objective response and favorable tolerability in the Phase 1/1b setting. Methods: KRYSTAL-1 (NCT03785249) is a multicohort Phase 1/2 study evaluating adagrasib as monotherapy or in combination regimens in patients with advanced solid tumors harboring a KRASG12C mutation. Here we report the first disclosure from all patients enrolled in Cohort A, a Phase 2 cohort with registrational intent, evaluating adagrasib given 600 mg orally BID in patients with NSCLC previously treated with platinum-based chemotherapy and anti-PD-1/L1 therapy. Study objectives include evaluating efficacy (objective response rate [ORR], duration of response [DOR], progression-free survival [PFS], overall survival [OS]), safety, PK, and exploratory correlative analyses. Objective tumor response was assessed per RECIST v1.1 by blinded independent central review (BICR). Results: As of the 15 October 2021 data cutoff, 116 patients with NSCLC harboring a KRASG12C mutation were enrolled and treated, with a median follow-up of 12.5 months. Baseline characteristics include median age 64 years, 65% female, and 15.5%/83.6% with ECOG PS 0/1; 98.3% of patients received adagrasib following prior treatment with immunotherapy and chemotherapy, with a median of 2 prior systemic therapies. The ORR (by BICR) was 42.9% (48/112) and the disease control rate was 79.5% (89/112); 31 patients remain on treatment. Median DOR was 8.5 months (95% CI 6.2–13.8), median PFS was 6.5 months (95% CI 4.7–8.4), median OS was 12.6 months (95% CI 9.2–NE). Treatment-related AEs (TRAEs) of any grade occurred in 97.4% of patients, grade ≥3 TRAEs in 45.7%, 2 grade 5 TRAEs, and 8 (6.9%) TRAEs led to discontinuation. The most commonly reported (≥25%) TRAEs (any grade) were diarrhea (62.9%), nausea (62.1%), vomiting (47.4%), fatigue (40.5%), ALT/AST increased (27.6%/25%), blood creatinine increased (25.9%); the most commonly reported (≥5%) TRAEs (grade 3/4) were lipase increased (6%) and anemia (5.2%). Additional subgroup analyses will be presented, including selected demographics, molecular markers and sites of metastases. Conclusions: Adagrasib is well tolerated and demonstrates promising efficacy in pretreated patients with NSCLC harboring a KRASG12C mutation. A Phase 3 trial evaluating adagrasib monotherapy versus docetaxel in previously treated patients with KRASG12C-mutant NSCLC is ongoing (NCT04685135). Clinical trial information: NCT03785249.

Published

2022

41. A phase 1/2 study of REGN5093-M114, a METxMET antibody-drug conjugate, in patients with mesenchymal epithelial transition factor (MET)-overexpressing NSCLC

Author

Alexander E. Drilon, Mark M. Awad, Shirish M. Gadgeel, Liza C Villaruz, Joshua K. Sabari, Javier Perez, Christopher Daly, Shraddha Patel, Siyu Li, Frank A. Seebach, Israel Lowy, Heather D. Magnan, and Petra Rietschel

Subjects

Cancer Research, Oncology

Abstract

TPS8593 Background: MET, also called hepatocyte growth factor receptor (HGFR), is a high-affinity transmembrane protein receptor for HGF. MET is overexpressed in various malignancies, including non-small cell lung cancer (NSCLC). MET overexpression can accompany MET exon 14 alteration or de novo/acquired MET amplification. REGN5093-M114 is an antibody drug conjugate composed of a novel linker-payload (M114, carrying the maytansine derivative M24, a potent inhibitor of microtubule assembly) covalently bound to lysine residues on a MET-targeting human IgG4p bispecific antibody, REGN5093. In preclinical models of MET overexpressing cancers, REGN5093-M114 demonstrated significant dose-dependent antitumor activity. Methods: This is an open label, phase 1/2, first-in-human, multicenter dose-escalation study with cohort expansion evaluating REGN5093-M114 in patients with MET-overexpressing NSCLC (NCT04982224). Patients must have advanced stage NSCLC for which there are no approved therapies available expected to confer clinical benefit, with tumor overexpressing MET (≥75% tumor cell staining at 2+) as centrally confirmed by immunohistochemistry. For the expansion phase, patients must have at least one lesion that is measurable by RECIST 1.1. REGN5093-M114 will be administered intravenously once every 3 weeks over 30 minutes until disease progression, intolerable adverse events, withdrawal of consent, or study withdrawal. The primary objectives in dose escalation are to evaluate safety, tolerability, PK, and maximum tolerated dose and/or recommended phase 2 dosing regimen of REGN5093-M114. PKs will include the assessment of REGN5093-M114, total antibody, and payload M24 concentrations. The primary objective in dose expansion is to assess preliminary anti-tumor activity of REGN5093-M114 in MET-overexpressing NSCLC as measured by the objective response rate. The secondary objectives of both phases of the study include an evaluation of treatment durability, and the immunogenicity of REGN5093-M114. This study is currently open to enrollment. Clinical trial information: NCT04982224.

Published

2022

42. Examination of speakership gender disparity at an international oncology conference

Author

Jessica Caro, Christina Boatwright, Xiaochun Li, Constance Fiocco, Jessica M Stempel, James Hart Stoeckle, James W. Smithy, Allison Betof Warner, Elaine Shum, Joshua K. Sabari, Jyoti Malhotra, Nancy Chan, Kristen Renee Spencer, Pamela L. Kunz, Judith D. Goldberg, and Janice M. Mehnert

Subjects

Cancer Research, Oncology

Abstract

11002 Background: Gender disparity is an important issue in medicine, as women occupy a minority of academic leadership positions despite increased representation in the physician workforce. One important aspect is the gender gap of speakers at academic meetings, which limits opportunities for career advancement and mentorship. This underrepresentation of women is largely anecdotal in oncology. We hypothesized that original research is less frequently presented by women at the annual ASCO meeting. We sought to examine presentation patterns from recently featured ASCO speakers, categorized by presentation type and gender. Methods: We conducted a retrospective, observational review of data from the 2018-2021 ASCO annual meetings. Mixed-gender coders extracted data from the ASCO Annual Meeting library and institutional public websites. Speaker-identified gender was unavailable; binary gender was determined by presenter name, pronouns, and video files. For original research, we collected data on last authors as well as these roles are also considered meritorious. Cochran–Mantel–Haenszel tests were used to investigate the association of gender and roles adjusted for each stratification variable individually. Common odds ratios (ORs) were estimated for each association. Breslow-Day Tests were used to test the homogeneity of these ORs among the different levels of each stratification variable. No adjustments for multiple testing were used. Results: We reviewed 4267 unique presentations, including those which highlighted original research (Poster Discussion, Oral Abstract, Clinical Science Symposium, Plenary) vs. education (Case-Based Panel, Education Sessions, Highlights of the Day). For original research, women were significantly more likely to have an ASCO-appointed role (discussant, speaker, or chair) than a first or last author role (48% vs. 32.7% of presentations, p < 0.0001), even after adjusting for conference year (OR 0.53, 95% CI: 0.45-0.61), session type (0.52, 0.45-0.61), degree (0.50, 0.43-0.58), academic rank (0.55, 0.47-0.64), and geographic region (0.58, 0.50-0.68). There was no difference between in-person and virtual conferences (p = 0.584). For education sessions, women comprised 46.1% (n = 626), nearly half, of these speaking roles (all ASCO-appointed) compared with men. 38% of the data was independently re-reviewed to confirm accuracy; 96.4% concordance was observed in presenter gender. Conclusions: Women are less likely to present highlighted original research and are more likely to have an appointed educational role at ASCO annual meetings. This likely reflects broader gender disparity within academia. Future analyses could be improved by examining speaker-identified gender. As high-profile original research can elevate careers, examining factors contributing to this observed disparity may reveal important approaches to address gender leadership gaps in oncology.

Published

2022

43. The Selective Personalized Radio-immunotherapy for Locally Advanced NSCLC Trial (SPRINT): Initial results

Author

Nitin Ohri, Shruti Jolly, Benjamin T. Cooper, Rafi Kabarriti, William Raymond Bodner, Jonathan Klein, Shankar Viswanathan, Elaine Shum, Joshua K. Sabari, Haiying Cheng, Rasim A. Gucalp, Enrico Castellucci, Angel Qin, Shirish M. Gadgeel, and Balazs Halmos

Subjects

Cancer Research, Oncology

Abstract

8510 Background: Standard therapy for unresectable locally advanced non-small cell lung cancer (LA-NSCLC) is concurrent chemoradiotherapy followed by adjuvant durvalumab. We performed a prospective trial testing sequential pembrolizumab and risk-adapted radiotherapy without chemotherapy for biomarker-selected LA-NSCLC patients. Methods: Patients with stage III NSCLC or unresectable stage II NSCLC, ECOG performance status 0-1, and no contraindications to protocol-specified therapy were eligible for this trial. Subjects with PD-L1 tumor proportion score (TPS) ≥ 50% underwent baseline FDG-PET/CT, received three cycles of induction pembrolizumab (200 mg, every 21 days), underwent restaging FDG-PET/CT, received risk-adapted thoracic radiotherapy (55 Gy delivered to tumors or lymph nodes with metabolic tumor volume exceeding 20 cc and 48 Gy delivered to smaller lesions, all in 20 daily fractions), and then received up to 13 cycles of additional pembrolizumab. The primary study endpoint was one-year progression-free survival (PFS). Here we report response rates following induction pembrolizumab, PFS and overall survival (OS) rates, and adverse event rates (CTCAE v. 4.03). Results: Twenty-five subjects with PD-L1 TPS ≥ 50% from three institutions were enrolled between August 2018 and November 2021. Median age was 71 (interquartile range [IQR] 62 to 77). One subject had stage II disease, 13 had stage IIIA disease, nine had stage IIIB disease, and two had stage IIIC disease. Median PD-L1 TPS was 75% (IQR 60 to 80%). Two subjects (8%) developed disease progression during induction pembrolizumab, and two subjects discontinued pembrolizumab after one infusion due to immune-related adverse events. Using RECIST 1.1 criteria, 12 subjects (48%) exhibited a partial (n = 11) or complete (n = 1) response following induction pembrolizumab on CT. Using PERCIST criteria, 12 subjects (48%) exhibited a partial response following induction pembrolizumab on PET. Four subjects had responses on PET but not on CT, and four had responses on CT but not on PET. With a median follow-up duration of 13 months, the actuarial 1-year PFS rate is 74%, and the actuarial 1-year OS rate is 95%. Grade 3 adverse events have been limited to single cases of anemia, arthritis, diarrhea, esophagitis, and pneumonitis, and no grade 4-5 adverse events have occurred. Exploratory analyses suggest that response to induction pembrolizumab on PET predicts efficacy of this treatment approach, with a 1-year PFS rate of 100% for responders, compared to 61% for non-responders (logrank p = 0.007). Conclusions: Treatment with pembrolizumab and risk-adapted radiotherapy is a promising treatment approach for LA-NSCLC patients with PD-L1 TPS ≥ 50%. Response on PET following induction pembrolizumab may be useful for identifying patients who can be treated successfully without chemotherapy. Clinical trial information: NCT03523702.

Published

2022

44. 1247P Management of infusion-related reactions (IRRs) in patients receiving amivantamab

Author

Rachel E. Sanborn, Roland Elmar Knoblauch, Catherine A. Shu, Patricia Lorenzini, J.C. Curtin, A. Roshak, Ravi Salgia, Karen L. Reckamp, Alexander I. Spira, Dawn Millington, Byoung Chul Cho, Ramaswamy Govindan, Meena Thayu, E.B. Haura, Joshua Bauml, John Xie, K. Park, and Joshua K. Sabari

Subjects

medicine.medical_specialty, Oncology, business.industry, Internal medicine, medicine, In patient, Hematology, business

Published

2021

45. KRYSTAL-1: Updated activity and safety of adagrasib (MRTX849) in patients (Pts) with unresectable or metastatic pancreatic cancer (PDAC) and other gastrointestinal (GI) tumors harboring a KRASG12C mutation

Author

Tanios S. Bekaii-Saab, Alexander I. Spira, Rona Yaeger, Gary L Buchschacher, Autumn Jackson McRee, Joshua K. Sabari, Melissa Lynne Johnson, Minal A. Barve, Navid Hafez, Karen Velastegui, James G Christensen, Thian Kheoh, Hirak Der-Torossian, and Igor I. Rybkin

Subjects

Cancer Research, Oncology

Abstract

519 Background: KRAS, the most frequently mutated oncogene in cancer, is a key mediator of the RAS/MAPK signaling cascade that promotes cellular growth and proliferation. KRAS mutations occur in approximately 90% of pancreatic cancer, and approximately 2% of these are KRASG12C mutations. Adagrasib, an investigational agent, is a KRASG12C inhibitor that irreversibly and selectively binds KRASG12C, locking it in its inactive state; adagrasib has been optimized for favorable pharmacokinetic (PK) properties, including long half-life (̃24 h), extensive tissue distribution, dose-dependent PK, as well as CNS penetration. Methods: KRYSTAL-1 (NCT03785249) is a multicohort Phase 1/2 study evaluating adagrasib as monotherapy or in combinations in pts with advanced solid tumors harboring a KRASG12C mutation. Here we report preliminary data from pts enrolled in a Phase 2 cohort evaluating single-agent adagrasib administered orally at 600 mg BID in previously treated pts with unresectable or metastatic solid tumors (excluding NSCLC and CRC), including pancreatic and other GI cancers. Study endpoints include clinical activity, safety, and PK. Results: The data cutoff was 10 September 2021. A total of 42 pts were enrolled in this cohort (median age 63.5 years, range 21–89; 52% female; 71% white; 29%/71% ECOG PS 0/1; median 2 prior lines of therapy, range 1–7; median follow-up 6.3 months), of whom 30 pts had KRASG12C-mutant GI tumors (12 PDAC, 8 biliary tract, 5 appendiceal, 2 gastro-esophageal junction, 2 small bowel, and 1 esophageal). In a preliminary analysis, 27 pts with GI tumors were evaluable for clinical activity; partial responses (PRs) were seen in 41% (11/27, including 3 unconfirmed PRs); the disease control rate (DCR) was 100% (27/27). Of the 12 pts with PDAC (median 3 prior lines of therapy; median follow-up 8.1 months), 10 were evaluable for clinical activity; PRs were seen in 50% (5/10, including 1 unconfirmed PR); the DCR was 100% (10/10). Median progression-free survival (PFS) was 6.6 months (95% CI 1.0–9.7), and treatment was ongoing in 50% of pts with PDAC. Among the 17 evaluable pts with other GI tumors, 6 achieved PR (35%; 2 unconfirmed) with a DCR of 100% (17/17); 11 pts were still receiving treatment. In the overall cohort, treatment-related adverse events of any grade occurred in 91% (38/42), the most frequent being nausea (48%), diarrhea (43%), vomiting (43%), and fatigue (29%); grade 3/4 events occurred in 21% of pts, with no grade 5 events. Conclusions: Adagrasib monotherapy is well tolerated and demonstrates encouraging clinical activity in pretreated pts with PDAC and other GI tumors harboring a KRASG12C mutation. Further exploration of adagrasib is ongoing in this pt population (NCT03785249). Clinical trial information: NCT03785249.

Published

2022

46. A Prospective Study of Circulating Tumor DNA to Guide Matched Targeted Therapy in Lung Cancers

Author

Marc Ladanyi, Sutirtha Datta, Dan DiPasquo, Alex Makhnin, Paul K. Paik, Alexander Drilon, Jamie E. Chaft, Mackenzie L. Myers, David R. Jones, Mark G. Kris, Andres Martinez, Jeong O Jeon, Bob T. Li, Charles M. Rudin, Adrian Lee, Dennis Stephens, Nidhi Tandon, Nick Pavlakis, Maria E. Arcila, Gregory J. Riely, James M. Isbell, Connie I. Diakos, Ysleni Leger, Joshua K. Sabari, Laetitia Borsu, Jennifer Hernandez, Matthew D. Hellmann, Michael Offin, Mark Li, Tristan Shaffer, Kavita Garg, Andy Ni, Helena A. Yu, Samantha Henderson, Lee P. Lim, Andreas Rimner, Christopher K. Raymond, Valerie W. Rusch, and Stephen Clarke

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Treatment response, Lung, business.industry, medicine.medical_treatment, Concordance, Articles, medicine.disease, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Circulating tumor DNA, 030220 oncology & carcinogenesis, Internal medicine, medicine, Liquid biopsy, Lung cancer, Prospective cohort study, business

Abstract

BACKGROUND: Liquid biopsy for plasma circulating tumor DNA (ctDNA) next-generation sequencing (NGS) is commercially available and increasingly adopted in clinical practice despite a paucity of prospective data to support its use. METHODS: Patients with advanced lung cancers who had no known oncogenic driver or developed resistance to current targeted therapy (n = 210) underwent plasma NGS, targeting 21 genes. A subset of patients had concurrent tissue NGS testing using a 468-gene panel (n = 106). Oncogenic driver detection, test turnaround time (TAT), concordance, and treatment response guided by plasma NGS were measured. All statistical tests were two-sided. RESULTS: Somatic mutations were detected in 64.3% (135/210) of patients. ctDNA detection was lower in patients who were on systemic therapy at the time of plasma collection compared with those who were not (30/70, 42.9% vs 105/140, 75.0%; OR = 0.26, 95% CI = 0.1 to 0.5, P

Published

2018

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

Author

Mizuki Nishino, Andrew J. Plodkowski, Joseph Montecalvo, Chebli Mrad, Charles M. Rudin, Lynette M. Sholl, Wei-Chu Victoria Lai, Mark G. Kris, Giulia Costanza Leonardi, Ai Ni, Renato Umeton, Mark M. Awad, Joshua K. Sabari, N. Rekhtman, Michael Offin, A. Drilon, Bob T. Li, Ruqin Chen, Darragh Halpenny, Catherine A. Shu, Kathryn C. Arbour, Matthew D. Hellmann, G. J. Riely, Isabella Bergagnini, Jules L. Dienstag, and Paul K. Paik

Subjects

Adult, Male, 0301 basic medicine, Oncology, medicine.medical_specialty, Lung Neoplasms, medicine.medical_treatment, Adenocarcinoma, B7-H1 Antigen, Cohort Studies, 03 medical and health sciences, Exon, Antineoplastic Agents, Immunological, 0302 clinical medicine, Carcinoma, Non-Small-Cell Lung, Internal medicine, Biomarkers, Tumor, medicine, Humans, Stage (cooking), Aged, Aged, 80 and over, Lung, business.industry, High-Throughput Nucleotide Sequencing, Original Articles, Exons, Hematology, Immunotherapy, Middle Aged, Proto-Oncogene Proteins c-met, Prognosis, MET Exon 14 Skipping Mutation, Immune checkpoint, Survival Rate, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Mutation, Cohort, Immunohistochemistry, Female, business, Follow-Up Studies

Abstract

BACKGROUND: MET exon 14 alterations are actionable oncogenic drivers. Durable responses to MET inhibitors are observed in patients with advanced MET exon 14-altered lung cancers in prospective trials. In contrast, the activity of immunotherapy, PD-L1 expression and tumor mutational burden (TMB) of these tumors and are not well characterized. PATIENTS AND METHODS: Patients with MET exon 14-altered lung cancers of any stage treated at two academic institutions were identified. A review of clinicopathologic and molecular features, and an analysis of response to single-agent or combination immune checkpoint inhibition were conducted. PD-L1 immunohistochemistry was carried out and TMB was calculated by estimation from targeted next-generation sequencing panels. RESULTS: We identified 147 patients with MET exon 14-altered lung cancers. PD-L1 expression of 0%, 1%–49%, and ≥50% were 37%, 22%, and 41%, respectively, in 111 evaluable tumor samples. The median TMB of MET exon 14-altered lung cancers was lower than that of unselected non-small-cell lung cancers (NSCLCs) in both independently evaluated cohorts: 3.8 versus 5.7 mutations/megabase (P

Published

2018

48. Response to ERBB3-Directed Targeted Therapy in NRG1-Rearranged Cancers

Author

Anja Ruusulehto, Andrew J. Plodkowski, Victor D. Martinez, Roger S. Smith, Jason C. Chang, Marc Ladanyi, Maria E. Arcila, Henrik Edgren, Kenneth K.-S. Ng, Gopinath Ganji, Charles M. Rudin, Christopher Matheny, Joshua K. Sabari, Joseph Montecalvo, Huichun Tai, Romel Somwar, Lukas Delasos, Natasha Rekhtman, Alexander Drilon, Ryma Benayed, Gregory J. Riely, Biju Mangatt, Mark G. Kris, Morana Vojnic, William W. Lockwood, and Patrice Desmeules

Subjects

0301 basic medicine, business.industry, Afatinib, medicine.medical_treatment, Exceptional Responder, Targeted therapy, Clinical trial, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Oncology, Drug development, Prostate, 030220 oncology & carcinogenesis, mental disorders, Monoclonal, medicine, Cancer research, ERBB3, business, medicine.drug

Abstract

NRG1 rearrangements are oncogenic drivers that are enriched in invasive mucinous adenocarcinomas (IMA) of the lung. The oncoprotein binds ERBB3–ERBB2 heterodimers and activates downstream signaling, supporting a therapeutic paradigm of ERBB3/ERBB2 inhibition. As proof of concept, a durable response was achieved with anti-ERBB3 mAb therapy (GSK2849330) in an exceptional responder with an NRG1-rearranged IMA on a phase I trial (NCT01966445). In contrast, response was not achieved with anti-ERBB2 therapy (afatinib) in four patients with NRG1-rearranged IMA (including the index patient post-GSK2849330). Although in vitro data supported the use of either ERBB3 or ERBB2 inhibition, these clinical results were consistent with more profound antitumor activity and downstream signaling inhibition with anti-ERBB3 versus anti-ERBB2 therapy in an NRG1-rearranged patient-derived xenograft model. Analysis of 8,984 and 17,485 tumors in The Cancer Genome Atlas and MSK-IMPACT datasets, respectively, identified NRG1 rearrangements with novel fusion partners in multiple histologies, including breast, head and neck, renal, lung, ovarian, pancreatic, prostate, and uterine cancers. Significance: This series highlights the utility of ERBB3 inhibition as a novel treatment paradigm for NRG1-rearranged cancers. In addition, it provides preliminary evidence that ERBB3 inhibition may be more optimal than ERBB2 inhibition. The identification of NRG1 rearrangements across various solid tumors supports a basket trial approach to drug development. Cancer Discov; 8(6); 686–95. ©2018 AACR. See related commentary by Wilson and Politi, p. 676. This article is highlighted in the In This Issue feature, p. 663

Published

2018

49. Next-generation sequencing based detection of germline and somatic alterations in a patient with four metachronous primary tumors

Author

Hira Rizvi, Darragh Halpenny, Joshua K. Sabari, Madhuri Martin, Vicky Makker, Natalie Shapnik, and Gulisa Turashvili

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, Somatic cell, lcsh:Gynecology and obstetrics, lcsh:RC254-282, Germline, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Internal medicine, medicine, Stage (cooking), lcsh:RG1-991, business.industry, Melanoma, Obstetrics and Gynecology, Cancer, Histology, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Serous fluid, 030104 developmental biology, 030220 oncology & carcinogenesis, business

Abstract

Introduction: Multiple primary tumors (MPTs) are defined as two or more separate synchronous or metachronous neoplasms occurring in different sites in the same individual. These tumors differ in histology, as well as primary sites from which they arise. Risk factors associated with the occurrence of MPTs include germline alterations, exposure to prior cancer therapies, occupational hazards, and lifestyle and behavioral influences. Case report: We present a case of a patient who was diagnosed with four metachronous primary tumors. In 2013, she was diagnosed with serous proliferations associated with psammomatous bodies of primary peritoneal origin (pT3NxM0). This was followed by invasive ductal carcinoma of the breast (stage pT2N0Mx, histological grade III/III) in 2014, melanoma (stage pT2bNxMx) in 2016 that further advanced to the lung and brain in 2017, and a low-grade lung carcinoid in 2017. To better understand the biology of this patient's MPTs, we performed next-generation sequencing (NGS) to assess for both somatic and germline alterations. The treatment course for this patient aims to target the tumor with the strongest prognostic value, namely her malignant melanoma, and has contributed favorably to the overall survival of this patient. Conclusion: We report the clinical and genomic landscape of a patient with MPTs who had no identifiable unique somatic or germline mutations to explain her predilection to cancer. The treatment course and overall prognosis for this patient is important for understanding future cases with unrelated, metachronous MPTs, the occurrence of which cannot always be explained by underlying genetic mechanisms. Keywords: Multiple primary tumors, Next-generation sequencing, Tumor mutational burden, Immunotherapy

Published

2018

50. Pulmonary large cell neuroendocrine carcinoma with adenocarcinoma-like features: napsin A expression and genomic alterations

Author

Charles M. Rudin, Prasad S. Adusumilli, Marc Ladanyi, Hangjun Wang, Catherine M. Pietanza, Kyuichi Kadota, Natasha Rekhtman, Omar Habeeb, Philippe Joubert, Joshua K. Sabari, Joseph Montecalvo, and William D. Travis

Subjects

carcinoid, Male, 0301 basic medicine, Pathology, medicine.medical_specialty, Lung Neoplasms, pulmonary, STK11, Adenocarcinoma of Lung, Biology, Malignancy, medicine.disease_cause, Article, lung, Pathology and Forensic Medicine, 03 medical and health sciences, 0302 clinical medicine, napsin A, KRAS, Biomarkers, Tumor, medicine, Carcinoma, Aspartic Acid Endopeptidases, Humans, large cell neuroendocrine carcinoma, Aged, Lung, Middle Aged, Large cell neuroendocrine carcinoma of the lung, medicine.disease, Carcinoma, Neuroendocrine, 3. Good health, small cell lung carcinoma, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Synaptophysin, biology.protein, Carcinoma, Large Cell, Adenocarcinoma, Female

Abstract

Pulmonary large cell neuroendocrine carcinoma (LCNEC) is a highly aggressive malignancy, which was recently found to comprise three major genomic subsets: small cell carcinoma-like, non-small cell carcinoma (predominantly adenocarcinoma)-like and carcinoid-like. To further characterize adenocarcinoma-like subset, here we analyzed the expression of exocrine marker napsin A, along with TTF-1, in a large series of LCNECs (n=112), and performed detailed clinicopathologic and genomic analysis of napsin A-positive cases. For comparison, we analyzed napsin A expression in other lung neuroendocrine neoplasms (177 carcinoids, 37 small cell carcinomas) and lung adenocarcinomas (n=60). We found that napsin A was expressed in 15% of LCNEC (17/112), whereas all carcinoids and small cell carcinomas were consistently negative. Napsin A reactivity in LCNEC was focal in 12/17 cases, and weak or moderate in intensity in all cases, which was significantly lower in the extent and intensity than seen in adenocarcinomas (p

Published

2018