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Purpose

This is a Phase 2, Multi-Arm, Multi-Cohort, Open-Label Study to Evaluate the Safety and Efficacy of Cretostimogene Grenadenorepvec in Participants with High-Risk Non-Muscle-Invasive Bladder Cancer.

Condition

Eligibility

Eligible Ages
Over 18 Years
Eligible Genders
All
Accepts Healthy Volunteers
No

Inclusion Criteria

  • Pathologically confirmed BCG-naïve high-risk high-grade NMIBC (i.e., CIS with or without Ta/T1 disease or high-grade Ta/T1 papillary-only disease without CIS) within 90 days of treatment allocation. - All visible disease must be resected, and all CIS resected or fulgurated, as feasible within 90 days prior to treatment allocation. - Acceptable baseline organ function. Cohort B Key Inclusion Criteria: - Pathologically confirmed BCG-exposed high-risk high-grade NMIBC (i.e., CIS with or without Ta/T1 disease or high-grade Ta/T1 papillary-only disease without CIS) within 90 days of treatment allocation. - All visible disease must be resected, and all CIS resected or fulgurated, as feasible within 90 days prior to treatment allocation. - Acceptable baseline organ function. Cohort CX Inclusion Criteria - Pathologically confirmed high-risk high-grade BCG-unresponsive or BCG-exposed NMIBC (i.e., CIS with or without Ta/T1 disease or high-grade Ta/T1 papillary-only disease without CIS) within 90 days of treatment allocation. - All visible disease must be resected, and all CIS resected or fulgurated, as feasible within 90 days prior to treatment allocation. - Acceptable baseline organ function.

Exclusion Criteria

(Both Cohorts): - Current or past history of muscle-invasive, locally advanced or metastatic bladder cancer. - High-grade urothelial carcinoma in the upper urinary tract or prostatic urethra within 24 months or T2 in upper tract within 48 months or any history of locally advanced/ nodal or metastatic disease in the upper urinary tract. - Significant immunodeficiency. - Pregnant or breastfeeding. - Cohort CX Only: serial intravesical gemcitabine within 24 months

Study Design

Phase
Phase 2
Study Type
Interventional
Allocation
Randomized
Intervention Model
Parallel Assignment
Primary Purpose
Treatment
Masking
None (Open Label)

Arm Groups

ArmDescriptionAssigned Intervention
Experimental
Experimental: Cohort A, Arm 1 		Cretostimogene (1 x 1012 vp) will be administered intravesically via the current instillation method
  • Drug: Cretostimogene Grenadenorepvec
    Respective Cohort
    Other names:
    • CG0070
Experimental
Experimental: Cohort A, Arm 2 		Cretostimogene (1 x 1012 vp) will be administered intravesically via an alternative instillation method.
  • Drug: Cretostimogene Grenadenorepvec
    Respective Cohort
    Other names:
    • CG0070
Experimental
Experimental: Cohort A, Arm 3 		Cretostimogene (1 x 1012 vp) will be administered intravesically via an alternative instillation method.
  • Drug: Cretostimogene Grenadenorepvec
    Respective Cohort
    Other names:
    • CG0070
Experimental
Experimental: Cohort B, Arm 1 		Cretostimogene (1 x 1012 vp) will be administered intravesically via an alternative instillation method.
  • Drug: Cretostimogene Grenadenorepvec
    Respective Cohort
    Other names:
    • CG0070
Experimental
Experimental: Cohort B, Arm 2 		Cretostimogene (1 x 1012 vp) will be administered intravesically via an alternative instillation method.
  • Drug: Cretostimogene Grenadenorepvec
    Respective Cohort
    Other names:
    • CG0070
Experimental
Experimental: Cohort CX, Arm 1 		At all treatment visits cretostimogene (1 x 1012 vp) will be administered intravesically via an alternative instillation method followed by gemcitabine instilled intravesically
  • Drug: Cretostimogene Grenadenorepvec
    Respective Cohort
    Other names:
    • CG0070
Experimental
Experimental: Cohort CX, Arm 2 		Cretostimogene (1 x 1012 vp) will be administered intravesically via an alternative instillation method for two consecutive weeks, followed by gemcitabine administered intravesically in the third week on a cyclic 2:1 visit schedule basis
  • Drug: Cretostimogene Grenadenorepvec
    Respective Cohort
    Other names:
    • CG0070

Recruiting Locations

Mayo Clinic Arizona
Phoenix, Arizona 85054
Contact:
Mark Tyson, MD
tyson.mark@mayo.edu

Arkansas Urology
Little Rock, Arkansas 72211
Contact:
Jon Henderson, MD
501-219-8900
Jon@arkansasurology.com

Michael G Oefelein, MD Clinical Trials
Bakersfield, California 93301
Contact:
Michael G Oefelein, MD
661-310-1063

Genesis Research (Greater Los Angeles)
Los Alamitos, California 90720
Contact:
Sepehr Nowfar, MD
424-667-2280
Sepehr.Nowfar@uniohp.com

Advanced Urology
Los Angeles, California 90045
Contact:
Faisal Ahmed, MD
drahmed@urologyla.com

Urology Center of Southern California
Murrieta, California 92563
Contact:
Madhumitha Reddy, MD
mreddy@ucosc.com

University of California, Irvine
Orange, California 92868
Contact:
Edward Uchio, MD
euchio@uci.edu

Univeristy of Southern California
San Diego, California 92123
Contact:
Siamak Daneshmand, MD
daneshma@med.usc.edu

Genesis Research (Greater Los Angeles)
Torrance, California 90503
Contact:
Timothy Lesser, MD
424-667-2565
Timothy.Lesser@uniohp.com

Urology Associates, Lone Tree
Lone Tree, Colorado 80124
Contact:
Daniel Mazur, MD
D.Mazur@uradenver.com

Mayo Clinic Florida
Jacksonville, Florida 32224
Contact:
Andrew Zganjar, MD
Zganjar.Andrew@mayo.edu

Advanced Urology Institute (Solaris)
Largo, Florida 33771
Contact:
Matthew Truesdale, MD
matthew.truesdale@auihealth.com

Advanced Urology Institute
Oxford, Florida 34484
Contact:
Edward King, MD
352-259-4400
edward.king@auihealth.com

Advanced Urogoloy Institute - Tallahassee (Solaris)
Tallahassee, Florida 32308
Contact:
Scott Sellinger
Scott.sellinger@auihealth.com

Emory University
Atlanta, Georgia 30322
Contact:
Shreyas Joshi, MD
shreyas.joshi@emory.edu

Associated Urological Specialists
Chicago Ridge, Illinois 60415
Contact:
Aaron Berger, MD
a.berger@auspecialists.com

Uropartners
Glenview, Illinois 60026
Contact:
Jeffrey Pearl, MD
JPearl@uropartners.com;

Urology of Indiana - Carmel
Carmel, Indiana 46032
Contact:
Chad Reichard, MD
creichard@urologyin.com

Urology of Indiana, LLC (US Urology Partners)
Greenwood, Indiana 46143
Contact:
Eugene Cone, MD
317-564-5573
econe@urologyin.com

First Urology, PSC
Jeffersonville, Indiana 47130
Contact:
Ryan Malone, MD
812-206-8164
rmalone@1sturology.com

Urologic Specialists of Northwest Indiana (Solaris)
Merrillville, Indiana 46410
Contact:
Manoj Rao, MD
314-443-1168
mrao@urologic-specialists.com

Urology Center of Iowa Research
Clive, Iowa 50325
Contact:
Brian Gallagher, MD
515-992-7718
brian.gallagher@objective.health

Wichita Urology Group
Wichita, Kansas 67226
Contact:
Philippe Nabbout, MD
pnabbout@wichitaurology.com

Southern Urology (Urology America)
Lafayette, Louisiana 70508
Contact:
Jason Bourque, MD
337-422-3738
jasonbourque@gmail.com

Michigan Institute of Urology (Solaris)
Troy, Michigan 48084
Contact:
Jason Hafron, MD
248-786-0467
HafronJ@michiganurology.com

Mayo Clinic Rochester
Rochester, Minnesota 55905
Contact:
Paras Shah, MD
Shah.Paras@mayo.edu

Specialty Clinical Research of St. Louis
Saint Louis, Missouri 63141
Contact:
Gregory Auffenberg, MD
Gregory.Auffenberg@objective.health

Integrated Medical Professionals, PLLC (Solaris)
New York, New York 10016
Contact:
Jed Kaminetsky, MD
jkaminetsky@imppllc.com

Associated Medical Professionals of NY, PLLC (US Urology Partners)
Syracuse, New York 13210
Contact:
Christopher Pieczonka, MD
315-478-4185
cpieczonka@ampofny.com

The Urology Group (Solaris)
Cincinnati, Ohio 45212
Contact:
Marc Pliskin, MD
mpliskin@urologygroup.com

Central Ohio Urology Group (US Urology Partners)
Gahanna, Ohio 43230
Contact:
Benjamin Martin, MD
614-396-2684
bmartin@centralohiourology.com

Midlantic Urology (Solaris)
Bala-Cynwyd, Pennsylvania 19004
Contact:
Laurence Belkoff, MD
lbelkoff@midlanticurology.com

Keystone Urology Specialists
Lancaster, Pennsylvania 17604
Contact:
Paul Sieber, MD
psieber@keystoneurology.com

University of Pennsylvania
Philadelphia, Pennsylvania 19104
Contact:
Trinity Bivalacqua, MD
trinity.bivalacqua@pennmedicine.upenn.edu

Charleston Area Medical Center
Charleston, South Carolina 25304
Contact:
Michael Stencel, MD
Michael.stenceldo@gmail.com

Carolina Urologic Research Center, LLC
Myrtle Beach, South Carolina 229572
Contact:
Neal Shore, MD
nshore@gsuro.com

Lowcountry Urology (Solaris)
North Charleston, South Carolina 29406
Contact:
Justin Ellett, MD
jellett@lcurology.com

The Conrad Pearson Clinic (Urology America)
Germantown, Tennessee 38138
Contact:
Michael Granieri, MD
901-236-0957
mgranieri@conradpearson.com

Urology Associates, PC
Nashville, Tennessee 37209
Contact:
Gautam Jayram, MD
615-250-9208
gtjayram@ua-pc.com

Amarillo Urology Research
Amarillo, Texas 79106
Contact:
David Wilheim, MD
david.wilhelm@objective.health

UPNT Research Institute, LLC
Arlington, Texas 76017
Contact:
Michael Collini, MD
682-205-8396
michael.collini@objective.health

Urology Austin, PLLC (Urology America)
Austin, Texas 78745
Contact:
Brian Mazzarella, MD
512-410-3773
brian.mazzarella@urologyaustin.com

Urology Clinics of North Texas, PLLC
Dallas, Texas 75231
Contact:
Jacob Taylor, MD
214-556-8337
jtaylor@urologyclinics.com

Urology San Antonio, PA dba USA Clinical Trials
San Antonio, Texas 78229
Contact:
Daniel Zainnfeld, MD
210-617-4116
Daniel.Zainfeld@urologysa.com

Urology of Virginia
Virginia Beach, Virginia 23462
Contact:
Michael Williams, MD
mwilliams@urologyofva.net

Spokane Urology
Spokane, Washington 99202
Contact:
Shane Pearce, MD
509-747-3147
pearce.shane@gmail.com

More Details

NCT ID
NCT06567743
Status
Recruiting
Sponsor
CG Oncology, Inc.

Study Contact

Rebecca Tregunna, MD
+1.949.419.6105
Rebecca.Tregunna@cgoncology.com

Detailed Description

In Cohort A, up to 125 participants will be enrolled with pathologically confirmed, high-risk high-grade non-muscle invasive bladder cancer (NMIBC) NMIBC (i.e., CIS with or without concomitant Ta or T1 disease OR HG Ta/T1 disease without CIS) which is naïve to Bacillus Calmette-Guerin (BCG) treatment. Participants with CIS with or without concomitant Ta/T1 NMIBC at baseline will be randomized 1:1 to receive cretostimogene via the current (Arm 1) or an alternative instillation procedure (Arm 2). Participants with papillary-only high-risk NMIBC (i.e., HG Ta/T1 without CIS) at baseline (Arm 3) will receive cretostimogene via the alternative instillation procedure. In Cohort B, up to 150 participants will be enrolled with pathologically confirmed, high-risk high-grade NMIBC (i.e., CIS with or without concomitant Ta or T1 disease OR HG Ta/T1 disease without CIS) which has previously been exposed to BCG treatment. Participants with CIS-containing pathology at baseline will be recruited into Arm 1 and participants with papillary-only pathology at baseline will be recruited into Arm 2. Both Cohort B Arms 1 and 2 will receive cretostimogene via the alternative instillation procedure. In Cohort CX, up to 50 participants will be enrolled with pathologically confirmed, high-risk high-grade NMIBC (i.e., CIS with or without concomitant Ta or T1 disease OR HG Ta/T1 disease without CIS) which has previously been exposed to or is unresponsive to BCG treatment. Participants will be randomized 1:1 to receive cretostimogene and gemcitabine either concurrently or sequentially. In all cohorts, study treatment will be administered as a weekly induction course for the first 6 weeks with a reinduction course administered to patients who have CIS and/or high-grade Ta disease at the 3-month evaluation. Following induction, if no high-grade disease is detected, maintenance treatment will begin. This consists of a cycle of three weekly treatments every three months during the first year, and every six months during the second year, with an optional extension to the third year following the same six-month schedule. Disease status will be assessed using urine cytology, complete bladder visualization (e.g., cystoscopy), upper tract assessment and directed resection/biopsy (if indicated) every 3 months for the first 2 years and then every 6 months for a further 2 years or until disease recurrence.

Notice

Study information shown on this site is derived from ClinicalTrials.gov (a public registry operated by the National Institutes of Health). The listing of studies provided is not certain to be all studies for which you might be eligible. Furthermore, study eligibility requirements can be difficult to understand and may change over time, so it is wise to speak with your medical care provider and individual research study teams when making decisions related to participation.

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