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Clinical Trial Details — Status: Terminated

Administrative data

NCT number NCT03801525
Other study ID # U2-VEN-207
Secondary ID
Status Terminated
Phase Phase 2/Phase 3
First received
Last updated
Start date May 16, 2019
Est. completion date December 20, 2022

Study information

Verified date April 2024
Source TG Therapeutics, Inc.
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

ULTRA-V: Study to Assess the Efficacy and Safety of Ublituximab in Combination with Umbralisib and Venetoclax (U2-V) Compared to Ublituximab and Umbralisib (U2) in Subjects with Chronic Lymphocytic Leukemia (CLL)


Description:

This is an open-label, multicenter, Phase 2/3 study to evaluate the efficacy and safety of the combination of ublituximab + umbralisib + venetoclax (U2-V) compared to the combination of ublituximab + umbralisib (U2) in participants with either treatment naïve or previously treated CLL/ small lymphocytic lymphoma (SLL).


Recruitment information / eligibility

Status Terminated
Enrollment 277
Est. completion date December 20, 2022
Est. primary completion date December 20, 2022
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: - Chronic lymphocytic leukemia (CLL)/ small lymphocytic lymphoma (SLL) that warrants treatment - Adequate organ system function as specified in the protocol - Ability to follow protocol procedures. Exclusion Criteria: - Subjects receiving cancer therapy or any investigational drug within 21 days of Cycle 1, Day 1 - Prior exposure to any PI3K inhibitor or venetoclax - Autologous hematologic stem cell transplant within 6 months of study entry. Prior allogeneic hematologic stem cell transplant is excluded - Active Hepatitis B or Hepatitis C.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Ublituximab
recombinant chimeric anti-CD20 (cluster of differentiation 20) monoclonal antibody administered as an IV infusion
Umbralisib
inhibitor of phosphoinositide 3-kinase (PI3K) delta and casein kinase 1 epsilon (CK1e) Tablet form
Venetoclax
B-cell lymphoma 2 (BCL-2) inhibitor Tablet form

Locations

Country Name City State
United States TG Therapeutics Investigational Trial Site Ann Arbor Michigan
United States TG Therapeutics Investigational Trial Site Atlanta Georgia
United States TG Therapeutics Investigational Trial Site Aurora Colorado
United States TG Therapeutics Investigational Trial Site Austin Texas
United States TG Therapeutics Investigational Trial Site Bethesda Maryland
United States TG Therapeutics Investigational Trial Site Birmingham Alabama
United States TG Therapeutics Investigational Trial Site Blacksburg Virginia
United States TG Therapeutics Investigational Trial Site Boca Raton Florida
United States TG Therapeutics Investigational Trial Site Charleston South Carolina
United States TG Therapeutics Investigational Trial Site Charlotte North Carolina
United States TG Therapeutics Investigational Trial Site Chattanooga Tennessee
United States TG Therapeutics Investigational Trial Site Columbia Maryland
United States TG Therapeutics Investigational Trial Site Columbus Ohio
United States TG Therapeutics Investigational Trial Site Decatur Illinois
United States TG Therapeutics Investigational Trial Site Des Moines Iowa
United States TG Therapeutics Investigational Trial Site Detroit Michigan
United States TG Therapeutics Investigational Trial Site Detroit Michigan
United States TG Therapeutics Investigational Trial Site Duarte California
United States TG Therapeutics Investigational Trial Site Eugene Oregon
United States TG Therapeutics Investigational Trial Site Fort Myers Florida
United States TG Therapeutics Investigational Trial Site Fort Wayne Indiana
United States TG Therapeutics Investigational Trial Site Gainesville Virginia
United States TG Therapeutics Investigational Trial Site Greenville South Carolina
United States TG Therapeutics Investigational Trial Site Hackensack New Jersey
United States TG Therapeutics Investigational Trial Site Huntsville Alabama
United States TG Therapeutics Investigational Trial Site Indianapolis Indiana
United States TG Therapeutics Investigational Trial Site Jacksonville Florida
United States TG Therapeutics Investigational Trial Site Knoxville Tennessee
United States TG Therapeutics Investigational Trial Site La Jolla California
United States TG Therapeutics Investigational Trial Site Lebanon New Hampshire
United States TG Therapeutics Investigational Site Louisville Kentucky
United States TG Therapeutics Investigational Trial Site Morristown New Jersey
United States TG Therapeutics Investigational Trial Site Nashville Tennessee
United States TG Therapeutics Investigational Trial Site New York New York
United States TG Therapeutics Investigational Trial Site Niles Illinois
United States TG Therapeutics Investigational Trial Site Ogden Utah
United States TG Therapeutics Investigational Trial Site Omaha Nebraska
United States TG Therapeutics Investigational Site Peoria Illinois
United States TG Therapeutics Investigational Trial Site Philadelphia Pennsylvania
United States TG Therapeutics Investigational Trial Site Rochester Minnesota
United States TG Therapeutics Investigational Trial Site Saint Petersburg Florida
United States TG Therapeutics Investigational Trial Site Salt Lake City Utah
United States TG Therapeutics Investigational Trial Site San Antonio Texas
United States TG Therapeutics Investigational Trial Site Seattle Washington
United States TG Therapeutics Investigational Trial Site Seattle Washington
United States TG Therapeutics Investigational Trial Site Stamford Connecticut
United States TG Therapeutics Investigational Trial Site Tampa Florida
United States TG Therapeutics Investigational Trial Site Tucson Arizona
United States TG Therapeutics Investigational Trial Site Tyler Texas
United States TG Therapeutics Investigational Trial Site Westwood Kansas

Sponsors (1)

Lead Sponsor Collaborator
TG Therapeutics, Inc.

Country where clinical trial is conducted

United States, 

Outcome

Type Measure Description Time frame Safety issue
Primary Phase 2: Complete Response (CR) Rate as Per International Workshop on Chronic Lymphocytic Leukemia (iwCLL) 2018 Criteria CR rate=percent of participants who achieved CR or complete response with incomplete marrow recovery(CRi).CR=no evidence of new disease,absolute lymphocyte count(ALC) in peripheral blood<4x10^9 per liter(/L),regression of nodal masses to normal size <1.5 centimeters(cm) in longest diameter(LD),normal spleen and liver size,no constitutional symptoms,cytological/pathological evaluation of bone marrow(BM) smear/biopsy must be at least normocellular for age without evidence for typical chronic lymphocytic leukemia(CLL)/small lymphocytic lymphoma(SLL) lymphocytes by morphological criteria,peripheral blood counts with absolute neutrophil count(ANC)=1.5x10^9/L or platelet=100x10^9/L or hemoglobin=110 grams per liter(g/L) without red blood cell(RBC) transfusions,all without need for exogenous growth factors.CRi=all CR criteria but with persistent anemia,thrombocytopenia,or neutropenia or hypocellular BM that is related to prior/ongoing drug toxicity(and not to CLL/SLL). Up to 43.2 months
Primary Phase 2: Overall Response Rate (ORR) Per iwCLL 2018 Criteria ORR=percent of participants who achieve CR,CRi,partial response(PR) or PR with lymphocytosis(PR-L).CR=no evidence of new disease;ALC<4x10^9/L;regression of nodal masses to<1.5cm LD;normal spleen,liver size;no constitutional symptoms;cytological/pathological evaluation of BM smear/biopsy must be at least normocellular for age;ANC=1.5x10^9/L,platelet=100x10^9/L,Hb=110g/L.CRi=CR criteria but with persistent anemia,thrombocytopenia,or neutropenia/hypocellular BM related to prior/ongoing drug toxicity.PR=no evidence of new disease,meets=2 criteria:=50% decrease from baseline(BL) in ALC(or decrease to<4x10^9/L) or sum of products(SPD) of target nodal lesions or CLL/SLL marrow infiltrate/Blymphoid;no target,splenic,liver,or non-target disease with worsening that meets criteria for definitive progressive disease(PD);platelet>100x10^9/L or Hb=110g/L or =50% increase from BL in each.PR-L=PR criteria but not had =50% decrease from BL in ALC/decrease to<4x10^9/L. Up to 43.2 months
Primary Phase 3: Progression-Free Survival (PFS) Per iwCLL 2018 Criteria PFS was assessed in participants treated with U2-V compared with U2. PFS was defined as the interval between randomization and the date of definitive PD (as confirmed by the IRC) or death due to any cause, whichever occurs first. Participants who had no event (progression or death) were censored at the day of their last adequate disease assessment. PD= appearance of new nodes >1.5 cm in the LD, >50% increase in greatest diameter, new or recurrent hepatomegaly or splenomegaly, new unequivocal extra-nodal lesion, new non-target disease, =50% increase from the nadir in the sum of products of diameters (SPD) of target lesions, =50% increase in the LD of an individual node or extra-nodal mass, splenic/hepatic enlargement of =50% from nadir, unequivocal increase in the size of non-target disease, transformation to a more aggressive histology, decrease in platelet count or Hgb, >50% decrease from the highest on-study platelet count, >20 g/L decrease from the highest on-study Hgb. Up to 43.2 months
Secondary Minimal Residual Disease (MRD) Negativity Rate The MRD negativity rate was defined as the percentage of participants who achieved MRD negative status post-baseline, defined as a quantitative detection of less than one CLL/SLL cell in 10000 leukocytes by flow cytometry (MRD level, 10^-4) in blood or bone marrow (BM). If a participant was determined to be MRD negative by peripheral blood, a bone marrow aspirate was obtained to assess MRD in the bone marrow. Participants who did not have an MRD assessment at any post-baseline visits were considered non-responders and were included in the denominator when calculating MRD negativity rate. Up to 43.2 months
Secondary Number of Participants Experiencing at Least One Treatment-Emergent Adverse Event (TEAE) An adverse event (AE) is any untoward medical occurrence in a clinical investigation participant administered a pharmaceutical product. An AE does not necessarily have to have a causal relationship with this treatment. An AE can therefore be any unfavorable and unintended sign (including an abnormal laboratory finding, for example), symptom, or disease temporarily associated with the use of a medicinal product, whether or not considered related to the medicinal product. TEAE is any AE that occur after first dosing of study medication and through the end of the study or through 30 days after the last dose of study treatment, or is considered treatment-related regardless of the start date of the event, or is present before first dosing of study medication but worsens in intensity or the investigator subsequently considers treatment-related. Up to 43.2 months
Secondary Phase 2: Time to Response (TTR) Per iwCLL 2018 Criteria TTR was defined as the interval from enrollment to first documentation of CR, CRi, PR, or PR-L. TTR was analyzed via Kaplan-Meier method. CR=no evidence of new disease; ALC<4x10^9/L; regression of nodal masses to <1.5cm LD; normal spleen ,liver size; no constitutional symptoms; cytological/pathological evaluation of BM smear/biopsy must be at least normocellular for age; ANC=1.5x10^9/L, platelet=100x10^9/L, Hb=110g/L. CRi=CR criteria but with persistent anemia, thrombocytopenia, or neutropenia/hypocellular BM related to prior/ongoing drug toxicity.PR=no evidence of new disease,meets=2 criteria:=50% decrease from BL in ALC (or decrease to<4x10^9/L) or SPD of target nodal lesions or CLL/SLL marrow infiltrate/B-lymphoid; no target, splenic, liver, or non-target disease with worsening that meets criteria for definitive PD; platelet>100x10^9/L or Hb=110g/L or =50% increase from BL in each.PR-L=PR criteria but not had =50% decrease from BL in ALC/decrease to<4x10^9/L. Up to 43.2 months
Secondary Phase 2: Duration of Response (DOR) Per iwCLL 2018 Criteria DOR=interval from 1st documentation of CR,CRi,PR or PR-L to earlier of 1st documentation of definitive PD or death from any cause.CR=no evidence of new disease;ALC<4x10^9/L;regression of nodal masses to<1.5cm LD;normal spleen,liver size;no constitutional symptoms;cytological/pathological evaluation of BM smear/biopsy must be at least normocellular for age;ANC=1.5x10^9/L,platelet=100x10^9/L,Hb=110g/L.CRi=CR criteria but with persistent anemia,thrombocytopenia,neutropenia/hypocellular BM related to prior/ongoing drug toxicity.PR=no evidence of new disease,meets=2 criteria:=50% decrease from BL in ALC(or decrease to<4x10^9/L) or SPD of target nodal lesions or CLL/SLL marrow infiltrate/Blymphoid;no target,splenic,liver,or non-target disease with worsening that meets criteria for definitive PD;platelet>100x10^9/L or Hb=110g/L or =50% increase from BL in each.PR-L=PR criteria;not=50% decrease from BL in ALC/decrease to<4x10^9/L.PD=evidence of new disease per protocol-specififed criteria. Up to 43.2 months
Secondary Phase 3: CR Rate as Assessed by an Independent Review Committee (IRC) Per iwCLL 2018 Criteria CR rate=percent of participants who achieved CR or CRi. CR=no evidence of new disease; ALC<4x10^9/L; regression of nodal masses to <1.5 cm LD; normal spleen, liver size; no constitutional symptoms; cytological/pathological evaluation of BM smear/biopsy must be at least normocellular for age; ANC =1.5x10^9/L, platelet =100x10^9/L, Hb =110g/L. CRi=CR criteria but with persistent anemia,thrombocytopenia,or neutropenia/hypocellular BM related to prior/ongoing drug toxicity. CR assessment was subject to independent confirmation by the IRC in participants enrolled to the Phase 3 stage of the study. Up to 43.2 months
Secondary Phase 3: ORR as Assessed by IRC Per iwCLL 2018 Criteria ORR=percent of participants who achieve CR, CRi, PR or PR-L.CR=no evidence of new disease; ALC<4x10^9/L; regression of nodal masses to<1.5cm LD; normal spleen and liver size; no constitutional symptoms; cytological/pathological evaluation of BM smear/biopsy must be at least normocellular for age; ANC=1.5x10^9/L, platelet=100x10^9/L, Hb=110g/L. CRi=CR criteria but with persistent anemia, thrombocytopenia, or neutropenia/hypocellular BM related to prior/ongoing drug toxicity.PR=no evidence of new disease,meets=2 criteria:=50% decrease from baseline (BL) in ALC (or decrease to<4x10^9/L) or SPD of target nodal lesions or CLL/SLL marrow infiltrate/B-lymphoid; no target, splenic, liver, or non-target disease with worsening that meets criteria for definitive PD; platelet>100x10^9/L or Hb=110g/L or =50% increase from BL in each.PR-L=PR criteria but not had =50% decrease from BL in ALC/decrease to<4x10^9/L. Up to 43.2 months
Secondary Phase 3: Overall Survival (OS) Overall Survival (OS) was defined as the interval from randomization to death from any cause. OS data was censored at the last documented date that the participant was confirmed alive for participants who withdrew consent or were lost to follow-up prior to the end of the study, and for participants whose vital status in the study could not be determined. Up to 43.2 months
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