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Dose-Escalation and Efficacy Study of LAE001/Prednisone Plus Afuresertib Patients With m-CRPC

Sponsor
Laekna Limited (Industry)
Overall Status
Recruiting
CT.gov ID
NCT04060394
Collaborator
(none)
74
Enrollment
17
Locations
6
Arms
36.6
Anticipated Duration (Months)
4.4
Patients Per Site
0.1
Patients Per Site Per Month

Study Details

Study Description

Brief Summary

The combination treatment of protein kinase B (AKT) inhibitor, afuresertib, with androgen synthesis enzyme inhibitor, LAE001, may provide an effective treatment for metastatic castration resistant prostate cancer (m-CRPC) patients who have progressed/drug resistant following prior standard care treatments of any anti-androgen. This study intends to identify the most appropriate combined doses of LAE001/prednisone and afuresertib in m-CRPC patients who have progressive disease or are intolerant of 2 prior standard treatments of any anti-androgen or anti-androgen treatment plus chemotherapy.

Condition or Disease Intervention/Treatment Phase
  • Drug: Phase I and Phase II: LAE001/prednisone + afuresertib
 Phase 1/Phase 2

Detailed Description

The Phase I part of this study will perform a dose-escalation to identify the recommended Phase II dose of LAE001/prednisone plus afuresertib in m-CRPC patients.

In the Phase II part of this study, the anti-tumor efficacy of LAE001/prednisone plus afuresertib and docetaxel/prednisone plus afuresertib will be assessed in mCRPC patients with PTEN loss and/or PIK3CA/AKT/PTEN alteration who have progressed on, or who are intolerant of, 1-3 prior standard treatments for mCSPC, or nmCRPC, or mCRPC, including at least one antiandrogen treatment and no more than one chemotherapy. Participants will be assigned to one of the two study cohorts, based on the investigator's clinical judgement. Cohort 1 will receive LAE001/prednisone plus afuresertib using RP2D established in the Phase I study. Cohort 2 will receive docetaxel/prednisone plus afuresertib, with a safety run-in period during the first cycle in the first 6 patients. These study results will provide preliminary efficacy and safety information of the combination of LAE001/prednisone plus afuresertib and docetaxel/prednisone plus afuresertib as requested in the Food and Drug Administration (FDA) combined therapy guideline. Whether to move one or both combination therapies to the pivotal study will be based on the PFS improvements of the combination therapy versus historical controls of abiraterone or docetaxel monotherapies in mCRPC patients who failed 1-3 lines of standard of care therapies.

Study Design

Study Type:
Interventional
Anticipated Enrollment :
74 participants
Allocation:
Randomized
Intervention Model:
Sequential Assignment
Intervention Model Description:
Phase 1 Dose Escalation to determine Recommended Phase II Dose (RP2D) of LAE001/Prednisone plus Afuresertib in m-CRPC patients. Once RP2D is determined, Phase II will evaluate LAE001/Prednisone plus Afuresertib vs and Docetaxel/Prednisone plus Afuresertib in m-CRPC patients.Phase 1 Dose Escalation to determine Recommended Phase II Dose (RP2D) of LAE001/Prednisone plus Afuresertib in m-CRPC patients. Once RP2D is determined, Phase II will evaluate LAE001/Prednisone plus Afuresertib vs and Docetaxel/Prednisone plus Afuresertib in m-CRPC patients.
Masking:
None (Open Label)
Primary Purpose:
Treatment
Official Title:
A Phase I/II Dose-Escalation and Efficacy Study of LAE001/Prednisone Plus Afuresertib in Patients With Metastatic Castration-resistant Prostate Cancer Following Standard of Care Treatment
Actual Study Start Date :
Sep 13, 2019
Anticipated Primary Completion Date :
Sep 1, 2022
Anticipated Study Completion Date :
Oct 1, 2022

Arms and Interventions

Arm Intervention/Treatment
Experimental: Phase I Cohort 1

LAE001 (capsules) 75mg Twice Daily (BID) + prednisone (tablet) 5mg BID +afuresertib (tablet) 100mg Once Daily (QD) will be administered in Cycles of 28 days.

Drug: Phase I and Phase II: LAE001/prednisone + afuresertib
In the Phase I portion of the study will identify the RPD2 of the combined therapy. In the Phase II will evaluate LAE001/prednisone + afuresertib at the RP2D (Cohort 1) and docetaxel/prednisone + afuresertib (Cohort 2).
Other Names:
  • Phase II: Afuresertib

    		•
    Experimental: Phase I Cohort 2

    LAE001 (capsules) 100mg BID + prednisone (tablet) 5mg BID +afuresertib (tablet) 100mg QD will be administered in Cycles of 28 days.

    Drug: Phase I and Phase II: LAE001/prednisone + afuresertib
    In the Phase I portion of the study will identify the RPD2 of the combined therapy. In the Phase II will evaluate LAE001/prednisone + afuresertib at the RP2D (Cohort 1) and docetaxel/prednisone + afuresertib (Cohort 2).
    Other Names:
  • Phase II: Afuresertib

    		•
    Experimental: Phase I Cohort 3

    LAE001 (capsules) 100mg BID + prednisone (tablet) 5mg BID +afuresertib (tablet) 125mg QD will be administered in Cycles of 28 days.

    Drug: Phase I and Phase II: LAE001/prednisone + afuresertib
    In the Phase I portion of the study will identify the RPD2 of the combined therapy. In the Phase II will evaluate LAE001/prednisone + afuresertib at the RP2D (Cohort 1) and docetaxel/prednisone + afuresertib (Cohort 2).
    Other Names:
  • Phase II: Afuresertib

    		•
    Experimental: Phase I Cohort 4

    LAE001 (capsules) 100mg BID + prednisone (tablet) 5mg BID +afuresertib (tablet) 150mg QD will be administered in Cycles of 28 days.

    Drug: Phase I and Phase II: LAE001/prednisone + afuresertib
    In the Phase I portion of the study will identify the RPD2 of the combined therapy. In the Phase II will evaluate LAE001/prednisone + afuresertib at the RP2D (Cohort 1) and docetaxel/prednisone + afuresertib (Cohort 2).
    Other Names:
  • Phase II: Afuresertib

    		•
    Experimental: Phase II Cohort 1

    LAE001 (capsules) + prednisone (tablet) +afuresertib at the Recommended Phase II Dose (RP2D)

    Drug: Phase I and Phase II: LAE001/prednisone + afuresertib
    In the Phase I portion of the study will identify the RPD2 of the combined therapy. In the Phase II will evaluate LAE001/prednisone + afuresertib at the RP2D (Cohort 1) and docetaxel/prednisone + afuresertib (Cohort 2).
    Other Names:
  • Phase II: Afuresertib

    		•
    Experimental: Phase II Cohort 2

    Docetaxel/prednisone + afuresertib

    Drug: Phase I and Phase II: LAE001/prednisone + afuresertib
    In the Phase I portion of the study will identify the RPD2 of the combined therapy. In the Phase II will evaluate LAE001/prednisone + afuresertib at the RP2D (Cohort 1) and docetaxel/prednisone + afuresertib (Cohort 2).
    Other Names:
  • Phase II: Afuresertib

    		•

    Outcome Measures

    Primary Outcome Measures

    1. Phase II: Radiological progression free survival (rPFS) based on change in tumor per Response Evaluation Criteria in Solid Tumors (RECIST) 1.1 [At the end of each 28 day treatment cycle and within 15 days of last treatment]

      Based on investigator reviewed radiographic tumor assessment.

    2. Phase I: Demonstrate safety and tolerability of LAE001/prednisone and afuresertib as combination therapy. [Through study completion for an average of 12 months]

      Frequency and severity of AEs.

    3. Phase II: Radiological progression free survival (rPFS) based changes per Prostate Cancer Working Group 3 (PCWG3) [At the end of each 28 day treatment cycle and within 15 days of last treatment]

      Based on investigator reviewed radiographic tumor assessment.

    Secondary Outcome Measures

    1. Phase II: Overall Response Rate (ORR) based tumor changes per RECIST 1.1 [At the end of each 28 day treatment cycle and within 15 days of last treatment]

      Based on investigator reviewed radiographic tumor assessments and death from any cause.

    2. Phase II: Overall Response Rate (ORR) based tumor changes per PCWG3 [At the end of each 28 day treatment cycle and within 15 days of last treatment]

      Based on investigator reviewed radiographic tumor assessments and death from any cause.

    3. Phase II: Duration of Response (DOR) based on tumor changes per RECIST 1.1 [At the end of each 28 day treatment cycle and within 15 days of last treatment]

      Based on investigator reviewed radiographic tumor assessment and death.

    4. Phase I: Duration of Response (DOR) based on tumor changes per RECIST 1.1 [At the end of the 28 day treatment cycle for cycles 2,4 and 6 and then every 3 cycles after cycle 6 and within 15 days of last treatment]

      Based on investigator reviewed radiographic tumor assessment and death.

    5. Phase II: Duration of Response (DOR) based on tumor changes per PCWG3 [At the end of each 28 day treatment cycle and within 15 days of last treatment]

      Based on investigator reviewed radiographic tumor assessment and death.

    6. Phase I: Duration of Response (DOR) based on tumor changes per PCWG3 [At the end of the 28 day treatment cycle for cycles 2,4 and 6 and then every 3 cycles after cycle 6 and within 15 days of last treatment]

      Based on investigator reviewed radiographic tumor assessment and death.

    7. Phase II: Disease Control Rate (DCR) based on tumor changes per RECIST 1.1 [At the end of each 28 day treatment cycle and within 15 days of last treatment]

      Based on investigator reviewed radiographic tumor assessment and death.

    8. Phase II: Disease Control Rate (DCR) based on tumor changes per PCWG3 [At the end of each 28 day treatment cycle and within 15 days of last treatment]

      Based on investigator reviewed radiographic tumor assessment and death.

    9. Phase II: Overall Survival (OS) [At the end of each 28 day treatment cycle and within 15 days of last treatment]

      Based on investigator reviewed radiographic tumor assessment and death.

    10. Phase II: Changes in Prostate Specific Antigen (PSA) levels [End of Treatment as compared to baseline]

      Analysis of blood samples to be drawn at baseline and end of treatment

    11. Phase I: Changes in Prostate Specific Antigen (PSA) levels [Day 1 Cycle 2 (each cycle is 28 days) and all subsequent cycle and End of Treatment for an avergae of 12 months as compared to baseline]

      Analysis of blood samples to be drawn at baseline and end of treatment

    12. Phase II: PSA response [From date of randomization until the date of first documented progression or date of death from any cause, whichever came first, assessed up to 24 months]

      A >/=50% reduction in PSA from baseline

    13. Phase I: PSA response [From date of randomization until the date of first documented progression or date of death from any cause, whichever came first, assessed up to 24 months]

      A >/=50% reduction in PSA from baseline

    14. Phase I: Secondary PSA response [Baseline to>/=12 weeks after study treatment; confirmed 4 weeks later]

      A >/=30% reduction

    15. Phase II: Best PSA response [Through study completion for an avergae of 12 months]

      According to PCWG3

    16. Phase I: Best PSA response [Through study completion for an average of 12 months]

      According to PCWG3

    17. Phase II: Time to PSA progression [Through study completion for an average of 12 months]

      According to PCWG3

    18. Phase I: Time to PSA progression [Through study completion for an average of 12 months]

      According to PCWG3

    19. Phase II: % patients with PSA progression or death from any cause [At 12 weeks from start of study treatment]

      Patients with PSA progression or have died 12 weeks after treatment

    20. Phase II: Frequency and severity of AEs [Through study completion for an average of 12 months]

      Findings on physical examination, ECGs, vital signs and laboratory results based on CTCAE v5.0

    21. Phase I: Evaluate PK characteristics of study drug in combination treatment [Cycle 1 (each cycle is 28 days) Day 1 and Cycle 1 Day 15]

      Assess PK parameters as various timepoints

    22. Phase I: Describe pharmacodynamics of study drugs [Cycle 1 (each cycle is 28 days) Days 1,8,15 and 22 and Day 1 of subsequent cycles]

      Based on changes in blood levels on adrenal hormone and testosterone levels

    23. Phase I: Radiographic tumor response based on Prostate Cancer Working Group 3 (PCWG3) [At the end of each 28 day treatment cycle for cycles 2,4 and 6 and then every 3 cycles after cycle 6 and within 15 days of last treatment]

      Based on investigator reviewed radiographic tumor assessment.

    24. Phase I: Radiographic tumor response based on RECIST 1.1 [At the end of each 28 day treatment cycle for cycles 2,4 and 6 and then every 3 cycles after cycle 6 and within 15 days of last treatment]

      Based on investigator reviewed radiographic tumor assessment.

    Other Outcome Measures

    1. Phase I: Relationship between PSA levels and testosterone levels [Cycle 1 (each cycle is 28 days) Days 1,8,15 and 22 and Day 1 of subsequent cycles]

      Correlation between testosterone decreasing and PSA level changes

    2. Phase I: Explore correlation between anti-tumor activity and patient's PTEN status [At the end of each 28 day treatment cycle and within 15 days of last treatment]

      Anti-tumor activity (rPFS, DOR, ORR, PSA) in patients with PTEN loss

    3. Phase I: Explore correlation between anti-tumor activity and patient's BRCA mutation status [At the end of each 28 day treatment cycle and within 15 days of last treatment]

      Anti-tumor activity (rPFS, DOR, ORR, PSA) in patients with BRCA Mutations

    Eligibility Criteria

    Criteria

    Ages Eligible for Study:
    18 Years and Older
    Sexes Eligible for Study:
    Male
    Accepts Healthy Volunteers:
    No
    Inclusion Criteria:

    1. Patients, males ≥18 years of age, must be able to provide written informed consent.

    2. Patients must have documented histological or cytological evidence of adenocarcinoma of the prostate (excluding neuroendocrine differentiation or small cell histology).

    3. Patients must have radiographic evidence of metastatic disease for mCRPC based on the 'Guideline of American Urological Association for Prostate Cancer' before study enrollment. (https://www.auanet.org/guidelines/prostate-cancer-castration-resistant11 guideline)

    4. For PTEN and PIK3CA/AKT status test:

    Phase I: The PTEN/PIK3CA/AKT status test is optional and the result could be either positive, negative, undetermined or invalid. Phase II: Patients will be allowed to enroll regardless of the biomarker status, medical monitor review is necessary before enrollment. The biomarker status tests will be performed with the following order. The biomarker results of all enrolled patients will be used for retrospective analysis purposes.

    • Patients that have a documentation of "PTEN LOSS" and/or PTEN/PIK3CA/AKT alteration from a previous test on either tissue or liquid biopsy (e.g., IHC or next generation sequencing NGS), no further biomarker tests are needed in this study.

    • Patients who have PTEN or PI3KPIK3CA/AKT alteration status reported other than "PTEN LOSS", "PIK3CA/AKT alterations" or never completed any PTEN/PIK3CA/AKT test before, could either provide the archival tumor samples collected at any time before study enrollment or do a fresh core tumor biopsy.

    • As the last option, patients can perform a liquid biopsy for PTEN LOSS and PTEN/PIK3CA/AKT alteration tests by NGS of cfDNA if they have no archival tissue to provide, no tumor lesion for biopsy or a fresh biopsy is not feasible.

    1. Patients must have progressive disease based on the PCWG3 criteria:

    • Patients who progressed based solely on total PSA rising, should have had a sequence of rising values on 3 consecutive occasions of at least 1-week intervals (if the third measurement is not greater than the second measurement, a fourth measurement at least a week apart must be taken and must be greater than the second measurement) and should have 2.0 ng/mL minimum level for entry. Note: Patient must have had a prior PSA response, followed by documented PSA progression on prior hormone treatment.

    • Patients who have documented disease progression per RECIST 1.1 are eligible independent of PSA.

    • Patients with bone only progression according to PCWG3 (i.e., bone scan showing

    appearance of ≥2 new lesions).

    1. Patients must have castration levels of testosterone (<50 ng/dL or 1.7 nmol/L). Note: Patients must have undergone androgen deprivation therapy (ADT), such as orchiectomy, or have been on luteinizing hormone releasing hormone (LHRH) agonists or antagonists, for at least 3 months prior to study enrollment. Patients on LHRH agonists/antagonists must remain on these agents for the duration of the study.

    2. Patients must have an Eastern Cooperative Oncology Group (ECOG) performance status of ≤ 2.

    3. Patients must have adequate hematopoietic function by local laboratory within the 28 days before enrollment, as evidenced by:

    • Absolute neutrophil count ≥1,500/μL

    • Platelet count ≥75,000/μL

    • Hemoglobin ≥9 g/dL

    1. Note: Criteria must be met without growth factors or transfusion within 10 days prior to the screening lab tests. Total serum bilirubin ≤1.5 × ULN within the 28 days before enrollment (in patients with known Gilbert's syndrome, total bilirubin ≤3 × ULN with direct bilirubin ≤1.5 × ULN).

    2. Aspartate aminotransferase and alanine aminotransferase ≤2.5 × ULN except for patients with tumor involvement of the liver who must have AST and ALT ≤5 × ULN within the 28 days before enrollment.

    3. Patients must have adequate renal function as evidenced by a serum creatinine of

    ≤1.5 × ULN for the reference laboratory or creatinine clearance ≥30 mL/min within the 28 days before enrollment (calculated from Cockcroft-Gault formula or 24-hour urine collection).

    1. Serum potassium ≥3.5 mmol/L and < ULN within the 28 days before enrollment.

    2. Fasting plasma glucose (fasting is defined as no caloric intake for at least 8 hours):

    • ≤126 mg/dL for those patients without a pre-existing diagnosis of Type 1 or Type 2 diabetes mellitus

    • ≤167 mg/dL for those patients with a pre-existing diagnosis of Type 2 diabetes mellitus AND glycosylated haemoglobin (HbA1C) ≤8%

    1. Phase I: Patients who have mCRPC progressed or are intolerant after receiving at least 1 prior treatments of any anti-androgen (such as abiraterone, enzalutamide, apalutamide, or any other AR antagonists that are approved later), and/or chemotherapy. Patients must have at least 3 weeks of treatment of any antiandrogen and/or completed at least 4 Cycles of docetaxel or cabazitaxel treatment before their screening visit.

    Phase II: Patients who have mCRPC progressed or are intolerant after receiving 1-3 prior standard treatments for mCSPC, or nmCRPC, or mCRPC, including at least one second-generation antiandrogen treatment (i.e., abiraterone, enzalutamide, apalutamide, or darolutamide), and no more than one chemotherapy. Patients must have at least 3 weeks of treatment of any antiandrogen and/or completed at least 3 Cycles of docetaxel or cabazitaxel treatment and/or at least 3 injections of R223 and/or at least 2 injections of sipuleucel-T to be counted as one prior therapy. Patient's current diagnosis at screening must be mCRPC.

    1. Concomitant use of bisphosphonates and other bone supportive agents is allowed if the dose and renal function have been stable for at least 12 weeks before enrollment and no related ≥Grade 2 side effects are present for at least 4 weeks prior to study drug treatment. The minimum washout period is 4 weeks for prostate cancer therapy (cytotoxic, biologics, antiandrogens, etc.) before enrollment, starting from the day the therapies were stopped.

    2. Patients with a female partner of childbearing potential must agree to use condoms plus an additional contraceptive method to avoid conception until the end of relevant systemic exposure plus 90 days following the Clinical Trial Facilitation Group contraception guideline from September 2014.

    3. Patient should be suitable for oral medication and should not have any known gastrointestinal diseases that may interfere with drug absorption.

    4. Life expectancy of at least 6 months.

    Exclusion Criteria:
    1. Major surgery within 28 days before study treatment and/or have not adequately (Grade
    1. recovered from the adverse effects of any major surgical procedures before study treatment.

    1. Patients that received other second-line ADT (including but not limited to ketoconazole and amino glutethimide) within 6 weeks before enrollment.

    2. Patients who have completed sipuleucel-T (Provenge®) treatment within 6 weeks of enrollment.

    3. Patients who have received antiandrogens such as flutamide (EULEXIN®), bicalutamide (CASODEX®), or nilutamide (NILANDRON®) for >3 months must be off treatment for 6 weeks prior to enrollment and should demonstrate a continued rise in PSA after withdrawal.

    4. Patients who have received Radium Ra 223 dichloride (XOFIGO®) must be off therapy for 7 weeks prior to enrollment or Samarium Sm 153 lexidronam (QUADRAMET®) must be off therapy for at least 2 weeks prior to enrollment.

    5. Patients that are currently receiving increasing or chronic treatment (>5 days) with corticosteroids or another immunosuppressive agent, other than the following: daily use of up to 10 mg prednisone (or equivalent) or low-dose steroid for the control of nausea and vomiting, topical steroid, or inhaled steroid use.

    6. Patients who require potassium-wasting diuretics.

    7. Patients who have received any investigational agent beyond those indicated for the treatment of prostate cancer within 5 half-lives of the agent; if the half-life of the agent is not known, the patients must be off investigational therapy for 4 weeks prior to enrollment (whichever is shorter of the two should be preferred).

    8. Patients who have received palliative and other radiotherapy for the target lesion within 4 weeks of study enrollment.

    9. Patients with symptomatic or known central nervous system metastases from prostate cancer or who are at high risk for spinal cord compression, per investigator's judgment.

    10. Patients with a history of hypothalamus, pituitary or adrenal insufficiency.

    11. Patients with >grade 2 neuropathy at study enrollment.

    12. History of another primary malignancy that is currently clinically significant or currently requires active intervention.

    13. Inadequately controlled hypertension (eg, systolic blood pressure ≥160 mmHg or diastolic blood pressure ≥95 mmHg) or hypotension (eg, systolic blood pressure ≤ 80 mmHg or diastolic blood pressure ≤50 mmHg) after up to 3 measurements with at least 5 minutes apart during 28 days before study enrollment.

    14. Patients with active cardiac disease or a history of cardiac dysfunction including any of the following:

    • Severe or unstable angina pectoris or acute coronary syndrome or stroke within 6 months prior to study enrollment.

    • Symptomatic pericarditis.

    • Documented myocardial infarction or arterial thrombotic events within 6 months prior to study enrollment.

    • History of documented congestive heart failure (New York Health Association functional classification III to IV).

    • Documented history of cardiomyopathy.

    • Known left ventricular ejection fraction <50% as determined by multiple gated acquisition scan or echocardiogram within 28 days prior to enrollment.

    • History of clinically significant cardiac arrhythmias unsuitable to participate, as determined by the investigator.

    1. Patients with a Fridericia-corrected QT (QTcF) interval of >470 msec on the screening ECG (using the QTcF formula), has a short/long QT syndrome, or history of QT prolongation/Torsades de Pointes, unless prolonged QTc interval is due to (right or left) bundle branch block and/or pacemaker rhythm. If wide QRS complex is present, cardiology consultation is required to assess the risk for Torsade de Pointes.

    2. Patients with a history of an active infection (viral, bacterial, or fungal) requiring systemic therapy within 10 days before enrollment, including but not limited to tuberculosis.

    3. Patients who have active human immunodeficiency virus (HIV), hepatitis B, or hepatitis C infections.

    4. Patients that are currently receiving treatment with drugs known to be moderate or strong inhibitors or inducers of isoenzyme CYP1A (including but not limited:

    α-Naphthoflavone, Furafylline, Omeprazole, Lansoprazole) and isoenzyme CYP3A (including but not limited: Itraconazole, Ketoconazole, Azamulin, Troleandomycin, Verapamil, Rifampicin). The patients must have discontinued moderate or strong inducers for at least 2 weeks prior to study enrollment and must have discontinued moderate or strong inhibitors for at least 1 week before study enrollment. Spironolactone Strong bile salt export pump (BSEP) inhibitors, grapefruit juice, herbal medicines such as St. John's wort, Kava, ephedra, gingko biloba, dehydroepiandrosterone, yohimbe, saw palmetto and ginseng should be discontinued.

    1. Sexually active males not willing to use a condom during the whole course of the study and for 16 weeks after stopping treatment. Male patients must not father a child in this period. A condom is required to be used also by vasectomized men as well as during intercourse with a male partner in order to prevent delivery of the drug via seminal fluid.

    2. Patients with any other medical, psychiatric, or social condition, including substance abuse, which in the opinion of the investigator, would preclude participation in the study.

    3. Patients with a history of upper gastrointestinal bleeding or uncontrolled peptic disease in the previous 3 months which in Investigator's opinion may impact patient's participation in the study.

    4. Patients have previously received AKT or PI3 kinase pathway or mTOR inhibitors

    Contacts and Locations

    Locations

    Site City State Country Postal Code
    1 Urological Associates of Southern Arizona Tucson Arizona United States 85741
    2 California Cancer Associates for Researh & Excellence, Inc Encinitas California United States 92024
    3 Eastern Connnecticut Hematology/Oncology Associates Norwich Connecticut United States 06360
    4 Piedmont Columbus Regional Research Institute Columbus Georgia United States 31901
    5 University of Chicago Chicago Illinois United States 60637
    6 Cotton-O'Neil Clinical Research Center Topeka Kansas United States 66606
    7 Associated Medical Professionals of NY Syracuse New York United States 13215
    8 Oregon Urology Institute Florence Oregon United States 97439
    9 Greenville Hospital System Greenville South Carolina United States 29605
    10 Mary Crowley Cancer Research Centers Dallas Texas United States 75251
    11 Baylor Scott and White Health Temple Texas United States 76508
    12 Northwest Medical Specialties, PLLC Tacoma Washington United States 98405
    13 National Cancer Center Goyang-si Gyeonggido Korea, Republic of 10408
    14 Seoul National University Bundang Hospital Seongnam-si Gyunggido Korea, Republic of 13605
    15 Seoul National University Hospital Seoul Korea, Republic of 03080
    16 Severance Hospital Seoul Korea, Republic of 03722
    17 Asan Medical Center Seoul Korea, Republic of 05505

    Sponsors and Collaborators

    • Laekna Limited

    Investigators

    • Study Chair: Yong Yue, MD, Laekna Therapeutics

    Study Documents (Full-Text)

    None provided.

    More Information

    Publications

    None provided.
    Responsible Party:
    Laekna Limited
    ClinicalTrials.gov Identifier:
    NCT04060394
    Other Study ID Numbers:
    • LAE201INT2101
    First Posted:
    Aug 19, 2019
    Last Update Posted:
    Aug 5, 2022
    Last Verified:
    Aug 1, 2022
    Studies a U.S. FDA-regulated Drug Product:
    Yes
    Studies a U.S. FDA-regulated Device Product:
    No
    Additional relevant MeSH terms:
    Prostatic Neoplasms
    Prednisone

    Study Results

    No Results Posted as of Aug 5, 2022