A Trial of Romidepsin for Progressive or Relapsed Peripheral T-cell Lymphoma

Phase 2

Completed

• Conditions: Peripheral T-cell Lymphoma
• Interventions: Drug: Romidepsin

• Registration Number: NCT00426764
• Lead Sponsor: Celgene

Brief Summary

The purpose of this study is to evaluate the activity of romidepsin in patients with progressive or relapsed peripheral T-cell lymphoma (PTCL) who have already been treated with systemic therapy.

Detailed Description

This is a Phase II, non-randomized, open-label, single-arm trial. This study is designed on the basis of complete response (CR) or unconfirmed CR \[CR(u)\] as the measure of efficacy, based on the best overall response of each patient. The sample size of 65 patients evaluable for efficacy would yield lower 95% confidence limits on the rate of CR + CR(u) that would range from 2.2% to 7.7%, if the observed rate of CR + CR(u) ranges from 8% to 15%. The study was amended to include an Extension Phase, during which patients at non-US sites who are benefitting from treatment can continue to receive romidepsin. The Extension Study Phase is active in EU countries where currently no Marketing Authorisation exists for romidepsin. Patients may remain on study until progressive disease occurs or they withdraw their consent and only serious adverse events and study drug administration data will continue to be collected and reported for these patients.

Study Timeline

• Study First Submitted: 2007-01-23
• Study First Submitted QC: 2007-01-23
• Study First Posted: 2007-01-25
• Study Start: 2007-06-19
• Primary Completion: 2010-11-11
• Results First Submitted: 2012-07-05
• Results First Submitted QC: 2012-07-05
• Results First Posted: 2012-08-13
• Study Completion: 2018-05-17
• Status Verified: 2020-01
• Last Update Submitted: 2020-01-29
• Last Update Posted: 2020-02-11

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 131

Inclusion Criteria

Patients must fulfill all of the following criteria to be eligible for study participation and have:

• Histologically confirmed PTCL not otherwise specified, angioimmunoblastic T-cell lymphoma, extranodal natural killer (NK)/T-cell lymphoma nasal type, enteropathy- type T-cell lymphoma, subcutaneous panniculitis-like T-cell lymphoma, cutaneous γδ T-cell lymphoma (excludes mycosis fungoides or Sezary syndrome), transformed mycosis fungoides, hepatosplenic T-cell lymphoma, anaplastic large cell lymphoma (ALCL; anaplastic lymphoma kinase [ALK]-1 negative), or patients with ALK 1 expressing ALCL (ALK-1 positive) who have relapsed disease after autologous stem cell transplant (ASCT);
• Age ≥18 years;
• Written informed consent;
• Progressive disease following at least one systemic therapy or refractory to at least one prior systemic therapy;
• Measurable disease according to the International Workshop Response (IWC) criteria and/or measurable cutaneous disease;
• Eastern Cooperative Oncology Group (ECOG) performance status of 0-2;
• Serum potassium ≥3.8 mmol/L and magnesium ≥0.85 mmol/L (electrolyte abnormalities can be corrected with supplementation to meet inclusion criteria);
• Negative urine or serum pregnancy test on females of childbearing potential; and
• All women of childbearing potential must use an effective barrier method of contraception (either an intrauterine contraceptive device [IUCD] or double barrier method using condoms or a diaphragm plus spermicide) during the treatment period and for at least 1 month thereafter. Male patients should use a barrier method of contraception during the treatment period and for at least 1 month thereafter. Hormonal methods of contraception such as the contraceptive pill or patch (particularly those containing ethinyl-estradiol) should be avoided due to a potential drug interaction.

Exclusion Criteria

Patients are ineligible for entry if any of the following criteria are met:

• Known central nervous system (CNS) lymphoma [computed tomography (CT) or magnetic resonance imaging (MRI) scans are required only if brain metastasis is suspected clinically];

• Chemotherapy or immunotherapy within 4 weeks of study entry (6 weeks if nitrosoureas given);

• Initiation of corticosteroids during study (defined as 7 days prior to Cycle 1 Day 1[C1D1] until study drug discontinuation)

  • Patients treated with a pulse of steroids were to discontinue steroid use 7 days prior to C1D1 and have a repeat CT scan and disease assessment after discontinuation of corticosteroids and before starting romidepsin;

• Concomitant use of any other anti-cancer therapy;

• Concomitant use of any investigational agent;

• Use of any investigational agent within 4 weeks of study entry;

• Any known cardiac abnormalities such as:

  • Congenital long QT syndrome;
  • QTc interval >480 milliseconds (msec);
  • A myocardial infarction within 6 months of C1D1. Patients with a history of myocardial infraction between 6 and 12 months prior to C1D1 who are asymptomatic and have had a negative cardiac risk assessment (treadmill stress test, nuclear medicine stress test, or stress echocardiogram) since the event may participate;
  • Other significant electrocardiogram (ECG) abnormalities including 2nd degree atrio-ventricular (AV) block type II, 3rd degree AV block, or bradycardia (ventricular rate less than 50 beats/min).
  • Symptomatic coronary artery disease (CAD), e.g., angina Canadian Class II-IV. In any patient in whom there is doubt, the patient should be referred to a cardiologist for evaluation;
  • An ECG recorded at screening showing significant ST depression (ST depression of ≥2 mm, measured from isoelectric line to the ST segment at a point 60 msec at the end of the QRS complex). If in any doubt, the patient should have a stress imaging study and, if abnormal, angiography to define whether or not CAD is present;
  • Congestive heart failure (CHF) that meets New York Heart Association (NYHA) Class II to IV definitions and/or ejection fraction <40% by MUGA scan or <50% by echocardiogram and/or MRI;
  • A known history of sustained ventricular tachycardia (VT), ventricular fibrillation (VF), Torsade de Pointes, or cardiac arrest unless currently addressed with an automatic implantable cardioverter defibrillator (AICD);
  • Hypertrophic cardiomyopathy or restrictive cardiomyopathy from prior treatment or other causes (if in doubt, see ejection fraction criteria above);
  • Uncontrolled hypertension, i.e., blood pressure (BP) of ≥160/95; patients who have a history of hypertension controlled by medication must be on a stable dose (for at least one month) and meet all other inclusion criteria;
  • Any cardiac arrhythmia requiring anti-arrhythmic medication;

• Serum potassium <3.8 mmol/L or serum magnesium <0.85 mmol/L (electrolyte abnormalities can be corrected with supplementation to meet inclusion criteria);

• Concomitant use of drugs that may cause a significant prolongation of the QTc;

• Concomitant use of CYP3A4 significant or moderate inhibitors;

• Concomitant use of therapeutic warfarin or another anticoagulant due to a potential drug interaction. Use of a small dose of a anticoagulant to maintain patency of venous access port and cannulas is permitted;

• Clinically significant active infection;

• Known infection with human immunodeficiency virus (HIV), hepatitis B, or hepatitis C;

• Previous extensive radiotherapy involving ≥30% of bone marrow (e.g., whole pelvis, half spine), excluding patients who have had total body irradiation as part of a conditioning regimen for ASCT;

• Major surgery within 2 weeks of study entry;

• Previous allogeneic stem cell transplant;

• Inadequate bone marrow or other organ function as evidenced by:

  • Hemoglobin <9 g/dL (transfusions and/or erythropoietin are permitted);
  • Absolute neutrophil count (ANC) ≤1.0 × 10^9 cells/L [patients with neutropenia (ANC 1-1.5 10^9 cells/L) as a function of their disease may be supported with granulocyte-colony stimulating factor (G-CSF)];
  • Platelet count <100 × 10^9 cells/L or platelet count <75 × 10^9 cells/L if bone marrow disease involvement is documented;
  • Total bilirubin >2.0 × upper limit of normal (ULN) or >3.0 × ULN in the presence of demonstrable liver metastases;
  • Aspartate transaminase/serum glutamic oxaloacetic transaminase (AST/SGOT) and alanine transaminase/serum glutamic pyruvic transaminase (ALT/SGPT) >2.0 × ULN or >3.0 × ULN in the presence of demonstrable liver metastases; or
  • Serum creatinine >2.0 × ULN;

• Patients who are pregnant or breast-feeding;

• Coexistent second malignancy or history of prior solid organ malignancy within previous 3 years (excluding basal or squamous cell carcinoma of the skin, and in situ carcinoma of the cervix (CIN 1) that has been treated curatively);

• Any prior history of a hematologic malignancy (other than T-cell lymphoma);

• Any significant medical or psychiatric condition that might prevent the patient from complying with all study procedures; or

• Prior exposure to romidepsin (other histone deacetylase inhibitors are allowed).

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: SINGLE_GROUP

Arm && Interventions

Group	Intervention	Description
Romidepsin	Romidepsin	Participants received romidepsin 14 mg/m\^2 administered intravenously over 4 hours on Days 1, 8, and 15 of a 28-day cycle. Participants continued on monthly cycles of romidepsin. The planned duration of study therapy was 6 cycles. Patients who responded could continue beyond 6 cycles until disease progression or other withdrawal criteria were met. For participants treated for 12 or more cycles, maintenance dosing (2 doses per cycle) was permitted.

Primary Outcome Measures

Name	Time	Method
Percentage of Participants With a Complete Response According to the International Workshop Response Criteria (IWC) for Non-Hodgkin's Lymphomas (NHL) Assessed by an Independent Review Committee	Response was assessed after every 2 cycles of treatment and at completion of therapy, up until 30 September 2012 (data cutoff for analysis). Maximum duration on study was 1931 days.	Complete Response (CR): \>75% decrease in size aggregate of nodal index lesions (large and small), complete disappearance of extranodal and non-index lesions; total disappearance of clinical disease including skin involvement; disease-related signs and symptoms, normalization of biochemical abnormalities and reduction in size of spleen or liver so no longer palpable. Unconfirmed CR: all above criteria except all nodal index lesions must have regressed \>75% in the sum of the product diameters (SPD) from baseline. Individual nodes previously confluent must have regressed by \>75% in their SPD.

Secondary Outcome Measures

Name	Time	Method
Time to Disease Progression	Response was assessed after every 2 cycles of treatment and at completion of therapy, up until 30 September 2012 (data cutoff for analysis). Maximum duration on study was 1931 days.	Time to progression (≥50% increase from the nadir in the individual sum of the products of the diameters of any index lesion; the reappearance of pathology, enlargement of liver/spleen, or unequivocal progression of non-measurable disease or appearance of any new lesions) was defined as the duration from the date of the first study drug dose to the date of relapse or progression as reported by the independent review committee and was determined using Kaplan-Meier product-limit estimates.
Percentage of Participants With Objective Disease Response	Response was assessed after every 2 cycles of treatment and at completion of therapy, up until 30 September 2012 (data cutoff for analysis). Maximum duration on study was 1931 days.	Objective disease response was defined as patients with a Complete Response, Unconfirmed Complete Response or a Partial Response (PR) according to the IWC 1999 assessed by an independent review committee: CR, Cru defined above, PR defined as ≥50% decrease in size of 6 largest dominant nodes and/or nodal masses \& extranodal index lesions and no increase of non-index lesions, liver, or spleen; no new sites of disease evident; skin lesions decreased by ≥50%.
Duration of Objective Disease Response	Response was assessed after every 2 cycles of treatment and at completion of therapy, up until 30 September 2012 (data cutoff for analysis). Maximum duration on study was 1931 days.	Duration of response was defined as the number of days from the date of the first disease response (Complete, Unconfirmed Complete or Partial Response) until the date of progression and was determined using Kaplan-Meier product-limit estimates. Progression was defined as: a ≥50% increase from the nadir in the individual sum of the products of the diameters of any index lesion; the reappearance of pathology, enlargement of liver/spleen, or unequivocal progression of non-measurable disease or appearance of any new lesions.
Duration of Complete Disease Response	Response was assessed after every 2 cycles of treatment and at completion of therapy, up until 30 September 2012 (data cutoff for analysis). Maximum duration on study was 1931 days.	Duration of response was defined as the number of days from the date of the first disease response (Complete or Unconfirmed Complete) until the date of progression and was determined using Kaplan-Meier product-limit estimates. Progression was defined as: a ≥50% increase from the nadir in the individual sum of the products of the diameters of any index lesion; the reappearance of pathology, enlargement of liver/spleen, or unequivocal progression of non-measurable disease or appearance of any new lesions.
Change in Eastern Cooperative Oncology Group (ECOG) Performance Status	From Baseline up until 30 September 2012 (data cutoff for analysis). Maximum duration on study was 1931 days.	The ECOG scale is as follows: Grade 0: Fully active, able to perform all pre-disease activities without restriction; Grade 1: Restricted in physically strenuous activity, ambulatory, able to carry out light work; Grade 2: Ambulatory and capable of all self-care but unable to work. Up and about more than 50% of waking hours; Grade 3: Capable of only limited self-care, confined to bed or chair \> 50% of waking hours; Grade 4: Completely disabled. Cannot carry on any self-care. Confined to bed or chair. Data reported is the shift from Baseline ECOG score to best on-study assessment score.
Number of Participants With Treatment Emergent Adverse Events (TEAEs)	From first dose of study treatment until the final study visit, which occurred 30 days after receiving the last dose. Mean duration of treatment up until 30 September 2012 (data cutoff for analysis) was 169 days.	An adverse event or experience (AE) is defined as any untoward medical occurrence, which does not necessarily have to have a causal relationship with this treatment. A serious AE is any untoward medical occurrence that at any dose: results in death; is life-threatening; requires inpatient hospitalization or prolongation of existing hospitalization; results in persistent or significant disability/incapacity; is a congenital anomaly/birth defect; is an important medical event or condition. Related AEs are defined as those considered by the Investigator to have a possible, probable, or very likely/certain relationship to the study drug. AEs were graded as mild (1), moderate (2), severe (3), lifethreatening (4), or death (5). TEAEs occurred from the first dose of study medication through the end of the study (30 days post last dose) or any event that was present at baseline but worsened in intensity or was subsequently considered drug-related by the Investigator through end of study.

Trial Locations

Locations (90)

Hematology Oncology Assoc. of IL Orchard Research LLC; 🇺🇸 Chicago, Illinois, United States

Charite Universitatsmedizin Berlin campus Virchow Klinikum Centrum fur Tumormedizin; 🇩🇪 Berlin, Germany

Hospital Universitario Vall D Hebron; 🇪🇸 Barcelona, Spain

Charles University General Hospital; 🇨🇿 Prague 2, Czechia

Lund University Hosptial; 🇸🇪 Lund, Sweden

CHU Nantes Hotel Dieu; 🇫🇷 Nantes, France

Hospital Universitario La Paz; 🇪🇸 Madrid, Spain

Centre Hospitalier Lyon Sud; 🇫🇷 Pierre Bénite, France

Wojewodzki Szpital Specjalistczny im. Mikolaja Kopernika; 🇵🇱 Lodz, Poland

Hopital Claude Huriez; 🇫🇷 Lille, France

Krankenhaus Nordwest; 🇩🇪 Frankfurt a.M., Germany

Hopital Saint-Louis; 🇫🇷 Paris, France

University Hospital Brno; 🇨🇿 Brno, Czechia

Klinikum Nurnberg Nord; 🇩🇪 Nürnberg, Germany

University Hospital of Kralovske Vinohrady; 🇨🇿 Prague 10, Czechia

Klinika Hematologii Akademickie Centrum Kliniczne Akademii Medycznej w Gdansku; 🇵🇱 Gdansk, Poland

University Hospital Hradec Kralove; 🇨🇿 Hradec Kralove, Czechia

Polyclinique Bordeaux Nord Aquitaine; 🇫🇷 Bordeaux, France

Oddzial Kliniczny Kliniki Hematologii; 🇵🇱 Kraków, Poland

Uniklinik Koln; 🇩🇪 Köln, Germany

Hospital de La Princesa; 🇪🇸 Madrid, Spain

Hopital Henri Mondor; 🇫🇷 Créteil, France

Service des Maladies du Sang; 🇫🇷 Pessac, France

St. Vincent Hospital; 🇦🇺 Fitzroy, Australia

Hospital Marques de Valdecilla; 🇪🇸 Santandar, Spain

Hospital Universitario de Salamanca; 🇪🇸 Salamanca, Spain

Royal North Shore Hospital; 🇦🇺 St Leonards, Australia

Centre Eugene Marquis; 🇫🇷 Rennes, France

Peter MacCallum Cancer Centre; 🇦🇺 East Melbourne, Australia

Georg-August-Universität Göttingen; 🇩🇪 Göttingen, Germany

Guy's and St. Thomas' Hospital; 🇬🇧 London, United Kingdom

Dnipropetrovsk State Medical Academy; 🇺🇦 Dnipropetrovsk, Ukraine

Barts Cancer Institute, Queen Mary University of London, Charterhouse Square; 🇬🇧 London, United Kingdom

Royal Free Hospital; 🇬🇧 London Hampstead, United Kingdom

Somers Cancer Research Building; 🇬🇧 Southampton, United Kingdom

Klinika Nowotworow Ukladu Chlonnego; 🇵🇱 Warszawa, Poland

Institute of Blood Pathology and Transfusion Medicine of the AMS of Ukraine; 🇺🇦 Lviv, Ukraine

Centre Henri Becquerel; 🇫🇷 Rouen Cedex, France

UKT Universitaetsklinikum Tuebingen; 🇩🇪 Tuebingen, Germany

Klinikum der Universitat Munchen-Grosshadern; 🇩🇪 Muenchen, Germany

UCLA Division of Hematology Oncology; 🇺🇸 Los Angeles, California, United States

Moore UCSD Cancer Center; 🇺🇸 La Jolla, California, United States

Rocky Mountain Cancer Centers-Aurora; 🇺🇸 Aurora, Colorado, United States

Georgetown University IRB; 🇺🇸 Washington, District of Columbia, United States

Washington Hospital Center; 🇺🇸 Washington, District of Columbia, United States

Cancer Centers of Florida, PA; 🇺🇸 Orlando, Florida, United States

H. Lee Moffitt Cancer Center and Research Institute; 🇺🇸 Tampa, Florida, United States

University of California, San Francisco; 🇺🇸 San Francisco, California, United States

Tyler Cancer Center; 🇺🇸 Tyler, Texas, United States

Winship Cancer Institute of Emory University; 🇺🇸 Atlanta, Georgia, United States

Augusta Oncology Associates, P.C.; 🇺🇸 Augusta, Georgia, United States

Central Georgia Cancer Care; 🇺🇸 Macon, Georgia, United States

Cancer Care and Hematology Specialists of Chicagoland; 🇺🇸 Arlington Heights, Illinois, United States

Rush University Medical Center; 🇺🇸 Chicago, Illinois, United States

Consultants in Blood Disorders and Cancer; 🇺🇸 Louisville, Kentucky, United States

St. Agnes - Medical Center; 🇺🇸 Baltimore, Maryland, United States

Center for Cancer And Blood Disorders; 🇺🇸 Bethesda, Maryland, United States

Tufts Medical Center; 🇺🇸 Boston, Massachusetts, United States

Center for Cancer Research CAMC; 🇺🇸 Bethesda, Maryland, United States

Henry Ford Hospital; 🇺🇸 Detroit, Michigan, United States

Minnesota Oncology Hematology, PA; 🇺🇸 Burnsville, Minnesota, United States

St. Joseph Oncology, Inc; 🇺🇸 Saint Joseph, Missouri, United States

Nebraska Cancer Specialists; 🇺🇸 Omaha, Nebraska, United States

Arch Medical Services; 🇺🇸 Saint Louis, Missouri, United States

Hackensack University Medical Center; 🇺🇸 Hackensack, New Jersey, United States

Memorial Sloan-Kettering Cancer Center; 🇺🇸 New York, New York, United States

Taussig Cancer Center Cleveland Clinic Foundation; 🇺🇸 Cleveland, Ohio, United States

Northwest Cancer Specialists, P.C.; 🇺🇸 Portland, Oregon, United States

Accelerated Community Oncology Research Network Inc ACORN; 🇺🇸 Memphis, Tennessee, United States

Mamie McFadden Ward Center; 🇺🇸 Beaumont, Texas, United States

Methodist Charlton Cancer Center; 🇺🇸 Dallas, Texas, United States

UT Southwestern Medical Center Simmons Comprehensive Cancer Center; 🇺🇸 Dallas, Texas, United States

El Paso Cancer Treatment Center; 🇺🇸 El Paso, Texas, United States

Texas Oncology, P.A.-Fort Worth; 🇺🇸 Fort Worth, Texas, United States

Allison Cancer Center; 🇺🇸 Midland, Texas, United States

UT MD Anderson Cancer Center; 🇺🇸 Houston, Texas, United States

University of Texas Health Science Center at San Antonio; 🇺🇸 San Antonio, Texas, United States

US Oncology; 🇺🇸 Plano, Texas, United States

HOAST; 🇺🇸 San Antonio, Texas, United States

Texas Oncology, PA; 🇺🇸 Waco, Texas, United States

Fred Hutchinson Cancer Research Center; 🇺🇸 Seattle, Washington, United States

Clinica Universitaria de Navarra; 🇪🇸 Pamplona, Spain

Akademiska Sjukhuset; 🇸🇪 Uppsala, Sweden

National Cancer Institute Department Of Conservative Methods Of Treatment; 🇺🇦 Kyiv, Ukraine

R.E.Kavetsky Institute of Experimental Pathology, Oncology and Radiobiology; 🇺🇦 Kyiv, Ukraine

Catherine Lewis Centre - Hematology Department; 🇬🇧 London, United Kingdom

Weill Cornell Medical College; 🇺🇸 New York, New York, United States

Columbia University Medical Center; 🇺🇸 New York, New York, United States

Yale University; 🇺🇸 New Haven, Connecticut, United States

Mater Private Medical Centre - Haematology and Oncology Clinics of Australasia Research Centre; 🇦🇺 South Brisbane, Queensland, Australia