Small-cell Lung Cancer Clinical Trial
— ATLANTISOfficial title:
Phase III Randomized Clinical Trial of Lurbinectedin (PM01183)/Doxorubicin Versus Cyclophosphamide, Doxorubicin and Vincristine (CAV) or Topotecan as Treatment in Patients With Small-Cell Lung Cancer (SCLC) Who Failed One Prior Platinum-containing Line (ATLANTIS)
| Verified date | August 2021 |
| Source | PharmaMar |
| Contact | n/a |
| Is FDA regulated | No |
| Health authority | |
| Study type | Interventional |
Phase III randomized clinical trial of lurbinectedin (PM01183)/doxorubicin (DOX) versus cyclophosphamide (CTX), doxorubicin (DOX) and vincristine (VCR) (CAV) or topotecan as treatment in patients with small-cell lung cancer (SCLC) who failed one prior platinum-containing line.
| Status | Completed |
| Enrollment | 613 |
| Est. completion date | February 24, 2020 |
| Est. primary completion date | February 24, 2020 |
| Accepts healthy volunteers | No |
| Gender | All |
| Age group | 18 Years and older |
| Eligibility | Inclusion Criteria: 1. Voluntary written informed consent 2. Adult patients = 18 years 3. Histologically or cytologically confirmed diagnosis of limited or extensive stage SCLC which failed one prior platinum-containing regimen and with a chemotherapy-free interval (CTFI, time from the last dose of first-line chemotherapy to the occurrence of progressive disease) = 30 days. Small-cell carcinoma of unknown primary site with or without neuroendocrine features confirmed in histology test(s) performed on metastatic lesion(s) are eligible, if Ki-67/MIB-1 is expressed in >50% of tumor cells. 4. Eastern Cooperative Oncology Group Performance Status (ECOG PS) = 2. 5. Adequate hematological, renal, metabolic and hepatic function within 7-10 days prior to randomization 6. At least three weeks since last prior anticancer treatment and adequate recovery from prior treatment toxicity 7. Prior radiotherapy (RT): At least four weeks since completion of whole-brain irradiation, at least two weeks since completion of prophylactic cranial irradiation, and to any other site. 8. Evidence of non-childbearing status for women of childbearing potential (WOCBP). WOCBP must agree to use a highly effective contraceptive measure up to six weeks after treatment discontinuation. Fertile male patients with WOCBP partners should use condoms during treatment and for four months following the last investigational medicinal product dose. Exclusion Criteria: 1. More than one prior chemotherapy-containing line(re-challenge with the same initial regimen is not allowed) 2. Patients who never received platinum-containing regimen for Small-cell Lung Cancer (SCLC) 3. Prior treatment with PM01183, topotecan or anthracyclines. 4. Limited-stage patients who are candidates for local or regional therapy 5. Impending need for palliative RT or surgery for pathological fractures and/or for medullary compression within four weeks prior to randomization. 6. Symptomatic or progressing or steroid requiring Central Nervous System (CNS) involvement disease at least four weeks prior to randomization 7. Concomitant diseases/conditions: Angina, myocardial infarction, congestive heart failure or clinically significant valvular heart disease, arrhythmia, immunodeficiency (including known HIV seropositive), ongoing or treatment-requiring chronic liver disease, active infection, oxygen requirement within two weeks prior to randomization, diffuse interstitial lung disease (ILD) or pulmonary fibrosis, second invasive malignancy treated with chemotherapy and/or radiotherapy, invasive fungal infections requiring systemic treatment within 12 weeks of randomization. 8. Pregnant or breast feeding women |
| Country | Name | City | State |
|---|---|---|---|
| Argentina | Instituto Médico Especializado Alexander Fleming | C.a.b.a. | Buenos Aires |
| Argentina | Instituto Oncológico de Córdoba (IONC) | Córdoba | |
| Argentina | CORI - Centro Oncológico Riojano Integral | La Rioja | |
| Argentina | Centro para la Atención Integral del Paciente Oncológico (CAIPO) | San Miguel de Tucumán | Tucumán |
| Argentina | ISIS Centro Especializado de Luce S.A. | Santa Fe | |
| Austria | Universitätsklinik für Innere Medizin III der PMU | Salzburg | |
| Austria | Medizinische Universität Wien / AKH Wien, Universitätsklinik für Innere Medizin I, Abteilung für klinische Onkologie | Wien | |
| Belgium | AZ Maria Middelares | Gent | |
| Belgium | Clinique André Renard | Herstal | |
| Belgium | CHR de la citadelle | Liege | |
| Belgium | CHU de Liege - Sart Tilman | Liege | |
| Belgium | CHU Ambroise Paré | Mons | |
| Belgium | AZ Delta Campus Wilgenstraat | Roeselare | |
| Brazil | Fundação PlO XII - Hospital de Câncer de Barretos | Barretos | São Paulo |
| Brazil | lOP- Instituto de oncologia do paraná | Curitiba | Paraná |
| Brazil | Associação Hospital de Caridade de Ijuí | Ijui | RS |
| Brazil | Hospital São Lucas da PUCRS | Porto Alegre | RS |
| Brazil | lrmandade da Santa Casa de Misericórdia de Porto Alegre | Porto Alegre | RS |
| Brazil | Hospital de clínicas de Porto alegre | Pôrto Alegre | RS |
| Brazil | Coordenação de Pesquisa Clínica / Instituto Nacional de Câncer | Rio de Janeiro | RJ |
| Brazil | Instituto COl de Pesquisa, Educação e Gestão | Rio de Janeiro | RJ |
| Brazil | Nucleo de Oncologia da Bahia | Salvador | BA |
| Brazil | lnstituto de Ensino e Pesquisa Säo Lucas - IEP Säo Lucas | Sao Paulo | São Paulo |
| Bulgaria | Multiprofile Hospital for Active Treatment - Uni Hospital, Panagyurishte | Panagyurishte | |
| Bulgaria | Acibadem City Clinic University Multiprofile Hospital for Active Treatment. EOOD, Sofia; Clinic of Medical Oncology | Sofia | |
| Bulgaria | Multiprofile Hospital for Active Treatment of Women Health - "Nadezhda", Sofia; Clinic of Medical Oncology | Sofia | |
| Bulgaria | University Multiprofile Hospital for Active Treatment "Sv. Ivan Rilski", Sofia | Sofia | |
| Canada | Centre intégré de santé et de services sociaux de la Montérégie Centre | Greenfield Park | Quebec |
| Canada | Biron (Clinique René Laennec) | Mont-Royal | Quebec |
| Canada | Montreal Oncology Research Inc. | Montreal | Quebec |
| Canada | McGill University Health Centre | Montréal | Quebec |
| Canada | Southlake Regional Health Centre - Stronach Regional Cancer Centre | Newmarket | Ontario |
| Canada | R.S. Mc Laughlin Durham Regional Cancer Centre, Lakeridge Health | Oshawa | Ontario |
| Czechia | Vitkovicka nemocnice, a.s., Plicni oddeleni | Ostrava | |
| Czechia | Krajska zdravotni a.s. Masarykova nemocnice o.z. | Usti nad Labem | |
| France | Institut Bergonié | Bordeaux | |
| France | Centre François Baclesse | Caen | |
| France | Centre Hospitalier Intercommunal de Créteil | Creteil | |
| France | Centre Hospitalier Lyon Sud - Service de Pneumologie | Lyon | |
| France | Hôpital Nord - Service Oncologie Multidisciplinaire et Innovations Thérapeutiques | Marseille | |
| France | Centre Antoine Lacassagne | Nice Cedex 2 | |
| France | CHU de Rennes Hôpital Pontchaillou | Rennes | |
| Germany | Central Clinic of Bad Berka | Bad Berka | |
| Germany | Evangelische Lungenklinik Berlin | Berlin | |
| Germany | Vivantes Klinikum am Urban, Hämatologie und Onkologie | Berlin | |
| Germany | Uniklinik Freiburg, Hämatologie, Onkologie & Stammzellransplantation | Freiburg | |
| Germany | Asklepios-Fachkliniken München Gauting | Gauting | |
| Germany | Center for Pneumology and Thoracic Surgery | Gerlingen | |
| Germany | Thoraxklinik Heidelberg GmbH | Heidelberg | |
| Germany | Lungenklinik Hemer | Hemer | |
| Germany | VIDIA Christliche Kliniken Karlsruhe | Karlsruhe | |
| Germany | Katholisches Klinikum Koblenz-Montabaur, Marienhof Koblenz | Koblenz | |
| Germany | Onkologische Schwerpunktpraxis Leer-Emden | Leer | |
| Germany | Klinik Löwenstein gGmbH, Med. Klinik II Onkologie | Löwenstein | |
| Germany | Uniklinikum Mannheim, TTZ, Medizinische Fakultät Mannheim | Mannheim | |
| Germany | Johannes Wesling Klinikum Minden, Klinik für Hämatologie, Onkologie und Palliativmedizin | Minden | |
| Germany | Klinikum Bogenhausen, Städt. Klinikum München GmbH, Klinik für Pneumologie und Pneumologische Onkologie | Munchen | |
| Germany | Städtisches Krankenhaus München Neuperlach | Munchen | |
| Germany | University of Munich LMU, Dpt. of Medicine V | Munchen | |
| Germany | Klinikum Nürnberg Nord - Pneumologische Onkologie | Nuremberg | |
| Germany | Universitätsklinikum Ulm - Klinik für Innere Medizin II, Pneumologie | Ulm | |
| Germany | Medizinische Klinik I | Wuppertal | |
| Greece | General Hospital of Chest Diseases of Athens "Sotiria" | Athens | |
| Greece | General Oncology Hospital of Kifissia "Agioi Anargiroi", 2nd Internal Medicine-Oncology Clinic | Athens | |
| Greece | University General Hospital of Heraklion - General Hospital "Venizeleio" | Heraklion | Crete |
| Greece | General Hospital of Thessaloniki "G. Papanikolaou", Pulmonary Clinic, Aristotle University of Thessaloniki | Thessaloniki | |
| Hungary | Országos Korányi TBC és Pulmonológiai Intézet, 6. Pulmonológia és Bronchologia | Budapest | |
| Hungary | Országos Korányi TBC és Pulmonológiai lntézet, 14. Pulmonológia | Budapest | |
| Hungary | Veszprém Megyei Tüdögyógyintézet, 3. Pulmonológiai Osztály | Farkasgyepu | |
| Hungary | Mátrai Gyógyintézet, Bronchológia | Matrahaza | |
| Hungary | Miskolci Semmelweis Kórház és Egyetemi Oktatókórház, Pulmonológiai Osztály | Miskolc | |
| Hungary | Fejér Megyei Szent György Egyetemi Oktató Kórház, I. Pulmonológiai Osztály | Szekesfehervar | |
| Hungary | Markusovszky Egyetemi Oktatókórház, Pulmonológiai Osztály | Szombathely | |
| Hungary | Szent Borbála Kórház, Pulmonológiai osztály | Tatabanya | |
| Hungary | Zala Megyei Kórház, Pulmonologia | Zalaegerszeg | |
| Italy | Centro di Riferimento Oncologico di Aviano | Aviano | |
| Italy | Azienda Ospedaliero - Universitaria "Policlinico - Vittorio Emanuele" - Presidio G. Rodolico | Catania | |
| Italy | ASST Grande Ospedale Metropolitano Niguarda | Milano | MI |
| Italy | AOU Maggiore della Carità - SC Oncologia | Novara | |
| Italy | Istituto Oncologico Veneto | Padova | |
| Italy | lRCCS-Arcispedale Santa Maria Nuova | Reggio Emilia | |
| Italy | IRCCS CROB (Istituto di Ricovero e Cura a Carattere Scientifico) | Rionero in Vulture | PZ |
| Italy | Policlinico Universitario Campus Bio-Medico | Roma | |
| Italy | ASST della Valtellina e dell' Alto Lario P.O. Di Sondrio | Sondrio | |
| Lebanon | Ain Wazein Hospital | Ain Wazein | El Chouf |
| Lebanon | American University of Beirut Medical Center | Beirut | |
| Lebanon | Hotel Dieu de France | Beirut | |
| Lebanon | Centre Hospitalier Universitaire Notre Dame de Secours | Biblos | |
| Lebanon | Hammoud Hospital University Medical Center | Sidon | |
| Netherlands | The Netherlands Cancer Institute - Antoni van Leeuwenhoek Hospital | Amsterdam | |
| Netherlands | Spaarne Gasthuis | Hoofddorp | |
| Netherlands | MUMC | Maastricht | |
| Netherlands | Maxima Medisch Centrum | Veldhoven | |
| Poland | Bialostockie Centrum Onkologii im. Marii Sklodowskiej-Curie; Oddzial Onkologii Klinicznej im. dr Ewy Pileckiej z pododdzialem | Bialystok | |
| Poland | Szpitale Pomorskie Sp. z o.o., Oddzial Onkologii Klinicznej, Oddzial Onkologii i Radioterapii | Gdynia | |
| Poland | Mazowieckie Centrum Leczenia Chorób Pluc i Gruzlicy Oddzial III Chorób Pluc z Pododdzialem Onkologicznym | Otwock | |
| Poland | Szpital Kliniczny Przemienienia Panskiego Uniwersytetu Medycznego im. K.Marcinkowskiego w Poznaniu, Oddzial Chemioterapii | Poznan | |
| Portugal | Centro Clínico Champalimaud - Fundação Champalimaud | Lisboa | |
| Portugal | Centro Hospitalar Lisboa Norte, EPE- Hospital Pulido Valente | Lisboa | |
| Portugal | Centro Hospitalar de São João, EPE | Porto | |
| Portugal | Centro Hospitalar do Porto, EPE - Hospital de Santo António | Porto | |
| Portugal | Hospital CUF Porto | Porto | |
| Portugal | Instituto Português de Oncologia do Porto Francisco Gentil, EPE | Porto | |
| Romania | Spitalul Judetean de Urgenta "Dr. Constantin Opris", Sectia Oncologie Medicala | Baia Mare | Maramures |
| Romania | Institutul Oncologic "Prof. Dr. Ion Chiricuta" Cluj-Napoca, Departament Oncologie Medicala | Cluj | |
| Romania | Institutul Oncologic "Prof. Dr. lon Chiricuta" Cluj-Napoca, Dcpartamentul Oncologie Medicala | Cluj | |
| Romania | Institutul Oncologic "Prof. Dr. lon Chiricuta" Cluj-Napoca, Sectia Oncologic Medicala | Cluj | |
| Romania | Spitalul Clinic Judetean de Urgenta "Sf. Apostol Andrei" | Constanta | Judet Constanta |
| Romania | SC Centrul de Oncologie Sf. Nectarie SRL, Departament Oncologie Medícala | Craiova | Dolj |
| Romania | SC Oncolab SRL | Craiova | Judet Dolj |
| Spain | Hospital Universitari Germans Trias i Pujol ICO | Badalona | Barcelona |
| Spain | Hospital Universitari Vall d' Hebron | Barcelona | |
| Spain | Hospital Universitario Reina Sofia | Cordoba | |
| Spain | Hospital Universitario 12 de Octubre | Madrid | |
| Spain | Hospital Universitario Clínico San Carlos | Madrid | |
| Spain | Hospital Universitario Fundación Jiménez Díaz | Madrid | |
| Spain | Hospital Universitario Ramón y Cajal | Madrid | |
| Spain | MD Anderson Cancer Center Madrid | Madrid | |
| Spain | Hospital Universitario Puerta de Hierro Majadahonda | Majadahonda | Madrid |
| Spain | Hospital Regional Universitario de Malaga | Malaga | |
| Spain | Corporació Sanitaria Parc Taulí-Hospital de Sabadell | Sabadell | Barcelona |
| Spain | Complejo hospitalario regional virgen rocío | Sevilla | |
| Spain | Hospital General Universitario de Valencia | Valencia | |
| Spain | Hospital Universitario La Fe de Valencia | Valencia | |
| Spain | Hospital Universitario Miguel Servet | Zaragoza | |
| United Kingdom | The Clatterbridge Cancer Centre NHS Foundation Trust | Bebington | Wirral |
| United Kingdom | Bristol Cancer Institute, UHB NHS Foundation Trust | Bristol | |
| United Kingdom | Sarah Cannon Research Institute UK | London | |
| United Kingdom | University College London Hospitals NHS Foundation Trust | London | |
| United Kingdom | The Christie NHS Fundation Trust | Manchester | Greater Manchester |
| United Kingdom | Worcestershire Acute Hospitals NHS Trust | Worcester | |
| United States | Anne Arundel Medical Center Oncology and Hematology | Annapolis | Maryland |
| United States | Alabama Oncology | Birmingham | Alabama |
| United States | Boca Raton Regional Hospital Lynn Cancer Institute | Boca Raton | Florida |
| United States | Massachusetts General Hospital | Boston | Massachusetts |
| United States | Gabrail Cancer Center Research | Canton | Ohio |
| United States | Ironwood Physicians P.C. dba Ironwood Cancer & Research Centers | Chandler | Arizona |
| United States | Summit Medical Group, P.A. | Florham Park | New Jersey |
| United States | Holy Cross Hospital - Michael and Dianne Bienes Comprehensive Cancer Center | Fort Lauderdale | Florida |
| United States | The Center for Cancer and Blood Disorders | Fort Worth | Texas |
| United States | St Jude Hospital Yorba Linda dba St Joseph Heritage Healthcare | Fullerton | California |
| United States | Joliet Oncology-Hematology Associates, Ltd. | Joliet | Illinois |
| United States | Comprehensive Cancer Centers of Nevada | Las Vegas | Nevada |
| United States | Dartmouth-Hitchcock Medical Center/Mary Hitchcock Memorial Hospital | Lebanon | New Hampshire |
| United States | Loma Linda University Medica! Center | Loma Linda | California |
| United States | Norton Cancer Institute | Louisville | Kentucky |
| United States | East Jefferson Hematology-Oncology Metairie Physicians Services, Inc | Metairie | Louisiana |
| United States | Froedtert Hospital & the Medical College of Wisconsin | Milwaukee | Wisconsin |
| United States | Montgomery Cancer Center | Mount Sterling | Kentucky |
| United States | FirstHealth Outpatient Cancer Center | Pinehurst | North Carolina |
| United States | QUEST Research Institute | Royal Oak | Michigan |
| United States | Medical Oncology Associates PS (dba Summit Cancer Centers) | Spokane | Washington |
| United States | MultiCare Institute for Research & Innovation | Tacoma | Washington |
| United States | H. Lee Moffitt Cancer Center & Research Institute | Tampa | Florida |
| United States | Healthcare Research Network III, LLC | Tinley Park | Illinois |
| United States | Oklahoma Cancer Specialists and Research Institute, LLC | Tulsa | Oklahoma |
| United States | Tyler Hematology-Oncology PA | Tyler | Texas |
| United States | Associates in Hematology and Oncology, P.C. | Upland | Pennsylvania |
| United States | Carle Cancer Center | Urbana | Illinois |
| United States | Innovative Clinical Research Institute (ICRI) | Whittier | California |
| Lead Sponsor | Collaborator |
|---|---|
| PharmaMar |
United States, Argentina, Austria, Belgium, Brazil, Bulgaria, Canada, Czechia, France, Germany, Greece, Hungary, Italy, Lebanon, Netherlands, Poland, Portugal, Romania, Spain, United Kingdom,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Overall Survival (OS) | Overall survival (OS) will be calculated from the date of randomization to the date of death (death event) or last contact(in this case, survival will be censored on that date). | Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Difference in Overall Survival Between Lurbinectedin/Doxorubicin (DOX) and CAV in Patients With CAV as Best Investigator's Choice: Overall Survival Rate at 12 Months | Overall survival (OS) will be calculated from the date of randomization to the date of death (death event) or last contact(in this case, survival will be censored on that date). | At 12 months | |
| Secondary | Difference in Overall Survival Between Lurbinectedin/DOX and CAV in Patients With CAV as Best Investigator's Choice: Overall Survival Rate at 18 Months | Overall survival (OS) will be calculated from the date of randomization to the date of death (death event) or last contact(in this case, survival will be censored on that date). | At 18 months | |
| Secondary | Difference in Overall Survival Between Lurbinectedin/DOX and CAV in Patients With CAV as Best Investigator's Choice: Overall Survival Rate at 24 Months | Overall survival (OS) will be calculated from the date of randomization to the date of death (death event) or last contact(in this case, survival will be censored on that date). | At 24 months | |
| Secondary | Progression-free Survival (PFS) by Independent Review Committee | Progression-free survival (PFS) is defined as the time from the date of randomization to the date of documented progression per RECIST v.1.1 or death (regardless of the cause of death). If the patient receives further antitumor therapy or is lost to follow-up before PD, PFS will be censored at the date of last tumor assessment before the date of subsequent antitumor therapy. | Every six weeks up to progression disease, a period of approximately 3.5 years | |
| Secondary | Progression-free Survival Rate at 6 Months by Independent Review Committee | Progression-free survival (PFS) is defined as the time from the date of randomization to the date of documented progression per RECIST v.1.1 or death (regardless of the cause of death). If the patient receives further antitumor therapy or is lost to follow-up before PD, PFS will be censored at the date of last tumor assessment before the date of subsequent antitumor therapy. | At 6 months | |
| Secondary | Progression-free Survival Rate at 12 Months by Independent Review Committee | Progression-free survival (PFS) is defined as the time from the date of randomization to the date of documented progression per RECIST v.1.1 or death (regardless of the cause of death). If the patient receives further antitumor therapy or is lost to follow-up before PD, PFS will be censored at the date of last tumor assessment before the date of subsequent antitumor therapy. | at 12 months | |
| Secondary | Best Antitumor Response by Independent Review Committee | Best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Overall Response Rate by Independent Review Committee | Overall response rate is defined as the proportion of patients who have a partial or complete response in the best antitumor response. The best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Duration of Response by Independent Review Committee | Duration of Response is defined as the time that patients who have a partial or complete response in the best antitumor response. The best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Overall Survival in Patients With Chemotherapy-free Interval = 90 Days | Overall survival (OS) will be calculated from the date of randomization to the date of death (death event) or last contact(in this case, survival will be censored on that date). | Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Progression-free Survival in Patients With Chemotherapy-free Interval =90 Days | Progression-free survival (PFS) is defined as the time from the date of randomization to the date of documented progression per RECIST v.1.1 or death (regardless of the cause of death). If the patient receives further antitumor therapy or is lost to follow-up before PD, PFS will be censored at the date of last tumor assessment before the date of subsequent antitumor therapy. | Every six weeks up to progression disease, a period of approximately 3.5 years | |
| Secondary | Best Antitumor Response in Patients With Chemotherapy-free Interval = 90 Days | Best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Overall Response Rate in Patients With Chemotherapy-free Interval = 90 Days | Overall response rate is defined as the proportion of patients who have a partial or complete response in the best antitumor response. The best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Duration of Response in Patients With Chemotherapy-free Interval = 90 Days | Duration of Response is defined as the time that patients who have a partial or complete response in the best antitumor response. The best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Overall Survival in Patients With Chemotherapy-free Interval < 90 Days | Overall survival (OS) will be calculated from the date of randomization to the date of death (death event) or last contact(in this case, survival will be censored on that date). | Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Progression-free Survival in Patients With Chemotherapy-free Interval <90 Days | Progression-free survival (PFS) is defined as the time from the date of randomization to the date of documented progression per RECIST v.1.1 or death (regardless of the cause of death). If the patient receives further antitumor therapy or is lost to follow-up before PD, PFS will be censored at the date of last tumor assessment before the date of subsequent antitumor therapy. | Every six weeks up to progression disease, a period of approximately 3.5 years | |
| Secondary | Best Antitumor Response in Patients With Chemotherapy-free Interval <90 Days | Best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Overall Response Rate in Patients With Chemotherapy-free Interval <90 Days | Overall response rate is defined as the proportion of patients who have a partial or complete response in the best antitumor response. The best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Duration of Response in Patients With Chemotherapy-free Interval <90 Days | Duration of Response is defined as the time that patients who have a partial or complete response in the best antitumor response. The best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Overall Survival in Patients Without Central Nervous System Involvement at Baseline | Overall survival (OS) will be calculated from the date of randomization to the date of death (death event) or last contact(in this case, survival will be censored on that date). | Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Progression-free Survival in Patients Without Central Nervous System Involvement at Baseline | Progression-free survival (PFS) is defined as the time from the date of randomization to the date of documented progression per RECIST v.1.1 or death (regardless of the cause of death). If the patient receives further antitumor therapy or is lost to follow-up before PD, PFS will be censored at the date of last tumor assessment before the date of subsequent antitumor therapy. | Every six weeks up to progression disease, a period of approximately 3.5 years | |
| Secondary | Best Antitumor Response in Patients Without Central Nervous System Involvement at Baseline | Best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Overall Response Rate in Patients Without Central Nervous System Involvement at Baseline | Overall response rate is defined as the proportion of patients who have a partial or complete response in the best antitumor response. The best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Duration of Response in Patients Without Central Nervous System Involvement at Baseline | Duration of Response is defined as the time that patients who have a partial or complete response in the best antitumor response. The best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Overall Survival in Patients With Central Nervous System Involvement at Baseline | Overall survival (OS) will be calculated from the date of randomization to the date of death (death event) or last contact(in this case, survival will be censored on that date). | Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Progression-free Survival in Patients With Central Nervous System Involvement at Baseline | Progression-free survival (PFS) is defined as the time from the date of randomization to the date of documented progression per RECIST v.1.1 or death (regardless of the cause of death). If the patient receives further antitumor therapy or is lost to follow-up before PD, PFS will be censored at the date of last tumor assessment before the date of subsequent antitumor therapy. | Every six weeks up to progression disease, a period of approximately 3.5 years | |
| Secondary | Best Antitumor Response in Patients With Central Nervous System Involvement at Baseline | Best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Overall Response Rate in Patients With Central Nervous System Involvement at Baseline | Overall response rate is defined as the proportion of patients who have a partial or complete response in the best antitumor response. The best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years | |
| Secondary | Duration of Response in Patients With Central Nervous System Involvement at Baseline | Duration of Response is defined as the time that patients who have a partial or complete response in the best antitumor response. The best antitumor response will be the best response obtained in any evaluation according to RECIST v.1.1.
CR, complete response: disappearance of all lesions; PD, disease progression: =10% increase in target lesion size and does not meet tumor density criteria of PR density; PR, partial response: =10% decrease in target lesion size or =15% decrease in tumor density; SD, stable disease: none of the CR, PR, or PD criteria met; UK,unknown |
Every three months up to death or study termination, a period of approximately 3.5 years |
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