Neoplasms Clinical Trial
— ARCS-MultiOfficial title:
Phase 1b Multi-indication Study of Anetumab Ravtansine (BAY94-9343) in Patients With Mesothelin Expressing Advanced or Recurrent Malignancies
| Verified date | June 2022 |
| Source | Bayer |
| Contact | n/a |
| Is FDA regulated | No |
| Health authority | |
| Study type | Interventional |
The key purpose of the main part of the study is to assess efficacy and safety of anetumab ravtansine as monotherapy or combination therapy for mesothelin expressing advanced solid tumors. The main purpose of the safety lead-in (dose-finding) part of the study is to determine the safety and tolerability of anetumab ravtansine in combination with cisplatin and in combination with gemcitabine, and to determine the MTD of anetumab ravtansine in combination with cisplatin for mesothelin expressing advanced cholangiocarcinoma and in combination with gemcitabine for mesothelin expressing advanced adenocarcinoma of the pancreas. Patients will receive anetumab ravtansine every three weeks in monotherapy for most indications. In cholangiocarinoma and adenocarinoma of the pancreas, 3-weekly anetumab ravtansine is administered in combination with cisplatin or gemcitabine respectively (both administered in a 2 week on / 1 week off schedule). Treatment will continue until disease progression or until another criterion for withdrawal is met. .Efficacy will be measured by evaluating the tumor's objective response rate. Radiological tumor assessments will be performed at defined time points until the patient's disease progresses. Blood samples will be collected for safety, pharmacokinetic and biomarker analysis. Archival or fresh biopsy tissue will also be collected for mesothelin expression testing and biomarker analyses.
| Status | Completed |
| Enrollment | 173 |
| Est. completion date | July 26, 2021 |
| Est. primary completion date | September 16, 2020 |
| Accepts healthy volunteers | No |
| Gender | All |
| Age group | 18 Years and older |
| Eligibility | Inclusion Criteria: - Availability of tumor tissue for mesothelin expression testing and for further biomarker analysis - Histologically-confirmed, mesothelin-expressing metastatic or advanced non-metastatic disease (tumour type specific inclusion criteria) - At least one measurable lesion according to Response Evaluation Criteria in Solid Tumors (RECIST 1.1) (or for thymic carcinoma, at least one measurable lesion per International Thymic Malignancy Interest Group (ITMIG) modified RECIST 1.1 criteria - Adequate bone marrow, liver, renal and coagulation function - Left ventricular ejection fraction (LVEF) = 50% of the lower limit of normal (LLN) according to local institutional ranges - Eastern Cooperative Oncology Group (ECOG) 0 or 1 Exclusion Criteria: - Exposure to more than one prior anti-tubulin/microtubule agent - Corneal epitheliopathy or any eye disorder that may predispose the patients to this condition - Symptomatic Central nervous system (CNS) metastases and/or carcinomatous meningitis - Contraindication to both CT and MRI contrast agents - Active hepatitis B or C infection - Pregnant or breast-feeding patients - Tumor type specific exclusion criteria |
| Country | Name | City | State |
|---|---|---|---|
| Australia | Flinders Medical Centre | Adelaide | South Australia |
| Australia | Blacktown Cancer & Haematology Centre | Blacktown | New South Wales |
| Australia | Mid North Coast Cancer Institute | Coffs Harbour | New South Wales |
| Australia | Kinghorn Cancer Centre | Darlinghurst | New South Wales |
| Australia | Sir Charles Gairdner Hospital | Nedlands | Western Australia |
| Australia | Epworth HealthCare | Richmond | Victoria |
| Australia | Northern Cancer Institute | St Leonards | New South Wales |
| Australia | St John of God Healthcare | Subiaco | Western Australia |
| Belgium | Hôpital Erasme/Erasmus Ziekenhuis | Bruxelles - Brussel | |
| Belgium | UZ Antwerpen | Edegem | |
| Belgium | UZ Leuven Gasthuisberg | Leuven | |
| Belgium | CHU de Liège | Liege | |
| Canada | Cross Cancer Institute | Edmonton | Alberta |
| Canada | McGill University Health Center | Montreal | Quebec |
| Canada | Sir Mortimer B. Davis Jewish General Hospital | Montreal | Quebec |
| Canada | Princess Margaret Cancer Centre - UHN | Toronto | Ontario |
| France | Hopital Jean Minjoz | Besancon | |
| France | Hôpital Henri Mondor | Creteil | |
| France | Centre Oscar Lambret - Lille | Lille Cedex | |
| France | Centre Léon Bérard | Lyon Cedex | |
| France | C.H.U. Timone | Marseille | |
| France | Centre René Gauducheau | Nantes | |
| France | Centre Antoine Lacassagne | Nice Cedex 2 | |
| France | Centre Hospitalier Lyon Sud | Pierre Benite | |
| France | Hôpital de la Milétrie | POITIERS cedex | |
| France | Centre Eugène Marquis - Rennes Cedex | Rennes Cedex | |
| France | Hôpital Pontchaillou | Rennes Cedex | |
| France | Institut Gustave Roussy | Villejuif Cedex | |
| Italy | A.O.U. di Bologna Policlinico S.Orsola Malpighi | Bologna | Emilia-Romagna |
| Italy | ASST Grande Ospedale Metropolitano Niguarda | Milano | Lombardia |
| Italy | Fondazione IRCCS Istituto Nazionale dei Tumori | Milano | Lombardia |
| Italy | Istituto Clinico Humanitas - Humanitas Mirasole S.p.A. | Milano | Lombardia |
| Italy | A.O.U. di Modena - Policlinico | Modena | Emilia-Romagna |
| Italy | A.O.U.I. Verona | Verona | Veneto |
| Korea, Republic of | Asan Medical Center | Seoul | |
| Korea, Republic of | Samsung Medical Center | Seoul | |
| Korea, Republic of | Seoul National University Hospital | Seoul | |
| Korea, Republic of | Severance Hospital, Yonsei University Health System | Seoul | |
| Netherlands | Nederlands Kanker Instituut | Amsterdam | |
| Netherlands | Maastricht UMC | Maastricht | |
| Singapore | National Cancer Center Singapore | Singapore | |
| Singapore | National University Hospital | Singapore | |
| Spain | Ciutat Sanitària i Universitaria de la Vall d'Hebron | Barcelona | |
| Spain | Hospital Clínic i Provincial de Barcelona | Barcelona | |
| Spain | Hospital del Mar | Barcelona | |
| Spain | Centro Integral Oncológico Clara Campal | Madrid | |
| Spain | Hospital General Universitario Gregorio Marañón | Oncología | Madrid | |
| Spain | Hospital Ramón y Cajal | Oncología | Madrid | |
| Spain | Hospital Universitario 12 de Octubre | Madrid | |
| Spain | Hospital Virgen de la Victoria | Málaga | |
| Spain | Hospital Universitario Quirón de Madrid | Pozuelo de Alarcón | Madrid |
| Switzerland | Ospedale Regionale Bellinzona | Bellinzona | Ticino |
| Switzerland | Kantonsspital Graubünden | Chur | Graubünden |
| United Kingdom | Belfast City Hospital | Belfast | North Ireland |
| United Kingdom | Leicester Royal Infirmary | Leicester | Leicestershire |
| United Kingdom | Guy's Hospital | London | |
| United Kingdom | Royal Marsden Hospital (London) | London | |
| United Kingdom | Christie Hospital | Manchester | |
| United Kingdom | Royal Marsden NHS Trust (Surrey) | Sutton | Surrey |
| United States | National Cancer Institute - Maryland | Bethesda | Maryland |
| United States | Texas Oncology, PA | Dallas | Texas |
| United States | Barbara Ann Karmanos Cancer Institute | Farmington Hills | Michigan |
| United States | University of Texas MD Anderson Cancer Center | Houston | Texas |
| United States | Indiana University School of Medicine | Indianapolis | Indiana |
| United States | University of Southern California | Los Angeles | California |
| United States | Vanderbilt University Medical Center | Nashville | Tennessee |
| United States | Ochsner Medical Center - New Orleans | New Orleans | Louisiana |
| United States | Mayo Clinic Hospital | Phoenix | Arizona |
| United States | Mayo Clinic - Rochester | Rochester | Minnesota |
| United States | Washington University School of Medicine | Saint Louis | Missouri |
| United States | Stanford Health Care | Stanford | California |
| United States | MedStar Georgetown University Hospital | Washington | District of Columbia |
| Lead Sponsor | Collaborator |
|---|---|
| Bayer | ImmunoGen, Inc., MorphoSys AG |
United States, Australia, Belgium, Canada, France, Italy, Korea, Republic of, Netherlands, Singapore, Spain, Switzerland, United Kingdom,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Number of patients in the safety lead-in (SLI) phase who completed Cycle 1 or had a DLT and were not replaced. | During SLI, patients with cholangiocarcinoma received anetumab ravtansine in combination with cisplatin and patients with pancreatic adenocarcinoma received anetumab ravtansine in combination with gemcitabine. The highest dose of anetumab ravtansine that can be given so that not more than 1 out of 6 patients experiences a dose-limiting toxicity (DLT) during the DLT evaluation period were declared as the MTD for anetumab ravtansine in combination with cisplatin or with gemcitabine. | At least 3 weeks after the last patient starts treatment | |
| Primary | Objective response (qualitative improvement from baseline) of anetumab ravtansine for monotherapy and combination therapy in mesothelin expressing advanced solid tumors | A patient is a responder if the patient has a best response compared to baseline of complete response (CR) or partial response (PR) among all post-baseline tumor assessments, as determined per RECIST 1.1 criteria (ITMIG modified RECIST 1.1 criteria for thymic carcinoma) | Up to approximately 26 months after patient starts treatment | |
| Primary | Durable disease control (lack of progression from baseline) of anetumab ravtansine in indications pancreatic and gastric cancer (co-primary endpoint) | A patient experiences durable disease control if the patient has a tumor response compared to baseline of CR, PR or stable disease (SD) among the post-baseline tumor assessments made at least 180 days from first treatment, without prior disease progression | Up to approximately 26 months after patient starts treatment | |
| Secondary | Number of serious and non-serious adverse events (AEs) | Include treatment-emergent AEs, SAEs, treatment-related AEs, AEs of special interest, and deaths. | Approximately 26 months (Until 30 days after the last day of study treatment, or until later resolution of adverse events or determination by the investigator that the event will not improve) | |
| Secondary | Disease control rate (DCR) | The DCR is defined as the number of patients with disease control divided by the number of treated patients. | Up to approximately 24 months after last patient starts treatment, or until earlier disease progression [assessed every 6 weeks for the first 6 months, every 9 weeks until end of year 1 and every 12 weeks thereafter] | |
| Secondary | Duration of response (DOR) | DOR is defined in responders as the time from documentation of tumor response (CR or PR) to earlier of disease progression or death | Up to approximately 24 months after last patient starts treatment, or until earlier disease progression [assessed every 6 weeks for the first 6 months, every 9 weeks until end of year 1 and every 12 weeks thereafter] | |
| Secondary | Durable response rate (DRR) | A durable responder is defined as a responder (CR or PR) with a duration of response per RECIST 1.1 criteria (ITMIG modified RECIST 1.1 criteria for thymic carcinoma) of 180 days or more. The DRR is the number of durable responders divided by the number of treated patients. | Up to approximately 24 months after last patient starts treatment, or until earlier disease progression [assessed every 6 weeks for the first 6 months, every 9 weeks until end of year 1 and every 12 weeks thereafter] | |
| Secondary | Progression free survival (PFS) | PFS is defined as time from start of treatment until disease progression according to RECIST 1.1 (ITMIG modified RECIST 1.1 criteria for thymic carcinoma) or death. | Up to approximately 24 months after last patient starts treatment, or until earlier disease progression [assessed every 6 weeks for the first 6 months, every 9 weeks until end of year 1 and every 12 weeks thereafter] | |
| Secondary | Durable disease control rate (DDCR) of anetumab ravtansine in indications other than pancreatic and gastric cancer | A patient experiences durable disease control if the patient has a tumor response of CR, PR or SD with CR, PR or SD assessed at least 180 days from first treatment, without prior progression. | Up to approximately 24 months after last patient starts treatment, or until earlier disease progression [assessed every 6 weeks for the first 6 months, every 9 weeks until end of year 1 and every 12 weeks thereafter] |
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