Primary Outcomes

Description: The maximum dose at which no more than 1 of 6 patients at same dose level experience a drug related toxicity (DLT), as defined in the protocol.

Measure: Establish the maximum tolerated dose (MTD) in Phase I of AZD5069 administered in combination with enzalutamide at 160mg OD.

Time: 12 months

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Description: Prostate specific antigen (PSA) decline ≥ 50% criteria confirmed 4 weeks or later and/or, Confirmed soft tissue objective response by RECIST (v1.1) in patients with measurable disease and/or, ONLY for patients with detectable circulating tumour cell count (CTC) of ≥ 5/7.5ml blood at baseline, conversion of CTC <5/7.5ml blood nadir.

Measure: Antitumour activity of AZD5069 in combination with enzalutamide as measured by response rate in Phase II

Time: 12 months

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Description: For disease progression (see section 3.6) the Prostate Cancer Working Group 2 (PCWG2) criteria and RECIST (v1.1) criteria will be used. Treatment failure will be defined as: Progression of soft tissue/visceral disease by RECIST (v1.1) and/or, Progression of bone disease by PCWG2 bone scan criteria and/or Progression of PSA by PCWG2 PSA criteria.

Measure: Antitumour activity of AZD5069 in combination with enzalutamide as measured by response rate in Phase II

Time: 12 months

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Secondary Outcomes

Description: Maximal PSA decline at any time during the trial and PSA decline after 12 weeks (as per PCWG2 criteria) of combination treatment.

Measure: PSA decline

Time: 24 months

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Description: Overall survival will be measured from the date of AZD5069 addition to enzalutamide to the date of death (whatever cause). Survival time of living patients will be censored on the last date of patient is known to be alive or lost to follow up.

Measure: Overall survival of patients in Phase II

Time: 24 months

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Description: rPFS will be measured from the date of AZD5069 addition to enzalutamide until: Progression of soft tissue/visceral disease by RESIST and/or, Progression of bone disease by PCWG2 bone scan criteria and/or, Death of any cause Patients withdrawn for any reason prior to radiological progression then the patient should be assessed until radiological progression has occurred. If however they have started another treatment then they will be censored at the start of the new treatment.

Measure: To estimate the radiologic progression free survival (rPFS) on the combination in Phase II

Time: 24 months

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Description: CTC fall by >30% will be expressed as the proportion of patients that have demonstrated a CTC fall of >30% after 12 weeks of combination treatment.

Measure: To assess the effects of AZD5069 and enzalutamide on the number of circulating tumour cells in Phase II

Time: 24 months

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Description: Recording the population exposure to the AZD5069 and enzalutamide combination will summarise safety. Adverse events will be graded according to the Common Terminology Criteria for Adverse Events (CTCAE) v4.0.

Measure: To further evaluate the safety and tolerability of the combination in patients who progress on enzalutamide in Phase II

Time: 24 months

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Description: Number of patients with a neutrophil to lymphocyte ratio (NLR) ≥ 3 (at baseline) that convert to an NLR < 3 (blood nadir) with AZD5069 and enzalutamide in combination.

Measure: To further characterise the PD profile of AZD5069 and enzalutamide when administered in combination in Phase II

Time: 24 months

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Description: Plasma concentration of enzalutamide and AZD5069 in whole blood

Measure: To characterise the pharmacokinetic (PK) profile of enzalutamide and AZD5069 when administered in combination in Phase I

Time: 24 months

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Description: Number of patients with a neutrophil to lymphocyte ratio (NLR) ≥ 3 (at baseline) that convert to an NLR < 3 (blood nadir) with AZD5069 and enzalutamide in combination.

Measure: To characterise the pharmacodynamic (PD) profile of AZD5069 and enzalutamide when administered in combination in Phase I

Time: 24 months

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Description: Antitumour activity will be defined by response rate on the basis of the following outcomes; if any of these occur, patients will be considered to have responded: PSA decline ≥ 50% criteria confirmed 4 weeks or later and/or, Confirmed soft tissue objective response by RECIST (v1.1) in patients with measurable disease and/or, ONLY for patients with detectable circulating tumour cell count (CTC) of ≥ 5/7.5ml blood at baseline, conversion of CTC <5/7.5ml blood nadir.

Measure: To estimate the antitumour activity of AZD5069 in combination with enzalutamide as measured by response rate in Phase I.

Time: 24 months

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Description: Number of patients patients whose circulating myeloid derived suppressor cells (MDSCs) and intratumoral MDSCs reduce by 50% with AZD5069 and enzalutamide in combination.

Measure: To further characterise the PD profile of AZD5069 and enzalutamide when administered in combination in Phase II

Time: 24 months

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Description: Number of patients whose circulating myeloid derived suppressor cells (MDSCs) and intratumoral MDSCs reduce by 50% with AZD5069 and enzalutamide in combination.

Measure: To characterise the pharmacodynamic (PD) profile of AZD5069 and enzalutamide when administered in combination in Phase I

Time: 24 months

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Description: For disease progression (see section 3.6) the PCWG2 criteria and RECIST (v1.1) criteria will be used. Treatment failure will be defined as: Progression of soft tissue/visceral disease by RECIST (v1.1) and/or, Progression of bone disease by PCWG2 bone scan criteria and/or Progression of PSA by PCWG2 PSA criteria.

Measure: To estimate the antitumour activity of AZD5069 in combination with enzalutamide as measured by response rate in Phase I.

Time: 24 months

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Primary Outcomes

Description: Defined by radiographic response by Response Evaluation Criteria in Solid Tumors (RECIST) 1.1 or prostate specific antigen [PSA] response of > 50%). Will be conducted using the Cochran-Mantel-Haenszel test, with one-sided p-value of =< 0.05 considered significant.

Measure: Response rate (complete response + partial response)

Time: Up to 2 years

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Secondary Outcomes

Description: Assessed by Prostate Cancer Working Group (PCWG)3. PFS to be estimated with the Kaplan Meier methodology. Median and event-free rate at selected time points will be provided with 95% confidence interval.

Measure: Progression-free survival (PFS)

Time: From the time of randomization up to 2 years

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Description: Assessed by PCWG2. PSA progression will be estimated with the Kaplan Meier methodology. Median and event-free rate at selected time points will be provided with 95% confidence interval. Comparison of time to PSA progression between arms will be conducted using the log-rank test.

Measure: Time to PSA progression

Time: From the time of randomization up to 2 years

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Description: Assessed by RECIST 1.1. rPFS will be estimated with the Kaplan Meier methodology. Median and event-free rate at selected time points will be provided with 95% confidence interval.

Measure: Radiographic progression-free survival (rPFS)

Time: From the time of randomization up to 2 years

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Description: Will be summarized according to treatment arm. For toxicity reporting, all adverse events will be graded and analyzed using Common Terminology Criteria for Adverse Events (CTCAE) version 5.0. Type of adverse events, intensity (grading), and attribution will be provided in a listing. All adverse events resulting in discontinuation, dose modification, and/or dosing interruption, and/or treatment delay of drug will also be summarized. Laboratory test results will be classified according to the CTCAE version 5.0.

Measure: Incidence of adverse events

Time: Up to 2 years

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Other Outcomes

Description: OS will be estimated with the Kaplan Meier methodology. Comparison of OS between arms will be conducted using the log-rank test base on the intention-to-treat approach, where two treatment arms will be compared regardless of cross-over or any subsequent therapy.

Measure: Overall survival (OS)

Time: From the time of randomization up to 2 years

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Description: Gene mutation frequencies and mean +/- standard deviation of quantitative biomarkers will be summarized by arm and in overall population at baseline and/or at end of study.

Measure: Gene mutation frequencies

Time: Baseline up to 2 years

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Primary Outcomes

Description: Safety is based on evaluation of adverse events (AEs) and serious adverse events (SAEs) from the time of study drug administration through the End of Study visit.

Measure: Incidence of Adverse Events of MGC018 and MGC018 + MGA012 as assessed by CTCAE v4.03

Time: 30 days after last dose

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Description: Maximum tolerated or maximum administered dose of MGC018 and MGC018 + MGA012

Measure: Maximum Tolerated Dose

Time: up to 42 days from first dose

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Secondary Outcomes

Description: Efficacy assessed as best overall response rate using Response Evaluation Criteria in Solid Tumors version 1.1 (RECIST v1.1)

Measure: Preliminary anti-tumor activity of MGC018 and MGC018+MGA012

Time: 24 months

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Description: Percent of prostate cancer patients with at least 50% reduction in prostate-specific antigen (PSA)

Measure: PSA response rate

Time: 24 months

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Description: For prostate cancer patients, time from first dose to first radiographic progression in soft tissue or bone, or death from any cause

Measure: Radiographic progression-free survival

Time: 24 months

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Description: For prostate cancer patients, change from baseline in pain intensity as measured by the Brief Pain Inventory-Short Form scale

Measure: Patient-reported Outcome

Time: 24 months

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Description: Area under the plasma concentration versus time curve of MGC018 and MGC018+MGA012

Measure: Area under the curve

Time: 24 months

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Description: Maximum Plasma Concentration of MGC018 and MGC018+MGA012

Measure: Cmax

Time: 24 months

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Description: Time to reach maximum (peak) plasma concentration of MGC018 and MGC018+MGA012

Measure: Tmax

Time: 24 months

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Description: Trough plasma concentration of MGC018 and MGC018+MGA012

Measure: Ctrough

Time: 24 months

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Description: Total body clearance of the drug from plasma of MGC018 and MGC018+MGA012

Measure: CL

Time: 24 months

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Description: Apparent volume of distribution at steady state of MGC018 and MGC018+MGA012

Measure: Vss

Time: 24 months

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Description: Terminal half life of MGC018 and MGC018+MGA012

Measure: t1/2

Time: 24 months

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Description: Percent of patients with anti-drug antibodies against MGC018 and MGA012

Measure: Immunogenicity

Time: 24 months

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Primary Outcomes

Description: Response Evaluation Criteria In Solid Tumors (RECIST) 1.1 criteria; circulating tumor cell (CTC) conversion from >5/7.5 mL to <5/7.5 mL12; and a greater than 50% prostate-specific antigen (PSA) decline from baseline.

Measure: Estimate the composite response rate of the combination of BXCL701 + PEMBRO

Time: up to 36 months

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Secondary Outcomes

Description: The median time frame with progression-free survival with the use of BXCL701 in combination with Pembro determined by radiographic evidence.

Measure: Estimate the median radiographic progression-free survival (rPFS) of the combination of BXCL701 and PEMBRO in Cohort A and B

Time: up to 36 months

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Description: The median time frame with progression-free survival with the use of BXCL701 in combination with Pembro

Measure: Estimate the median PSA progression-free survival (PSA PFS) of the combination of BXCL701 and PEMBRO in Cohort A and B.

Time: up to 36 months

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Description: The median time frame with overall survival with the use of BXCL701 in combination with Pembro

Measure: Estimate the median overall survival (OS) of the combination of BXCL701 and PEMBRO in Cohort A and B.

Time: up to 36 months

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Description: The timeframe in which the tumor reacts to BXCL701 in combination with Pembro

Measure: Estimate the median duration of response (DOR) of the combination of BXCL701 and PEMBRO in Cohort A and B.

Time: up to 36 months

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Description: Determines the frequency and severity of known and unknown adverse events with the use of BXCL701 in combination with Pembro

Measure: Determine the risk profile of the use of BXCL701 in combination with PEMBRO.

Time: up to 36 months

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Primary Outcomes

Description: Cmax will be recorded from the pharmacokinetic (PK) plasma samples collected.

Measure: Pharmacokinetics (PK) of Digoxin in combination with rosuvastatin in plasma: maximum concentration (Cmax)

Time: Up to Day 71

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Description: AUClast will be recorded from the pharmacokinetic (PK) plasma samples collected.

Measure: Pharmacokinetics (PK) of Digoxin in combination with rosuvastatin in plasma: area under the concentration-time curve from the time of dosing to the last measurable concentration (AUClast)

Time: Up to Day 71

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Description: AUCinf will be recorded from the pharmacokinetic (PK) plasma samples collected.

Measure: Pharmacokinetics (PK) of Digoxin in combination with rosuvastatin in plasma: area under the concentration time curve from the time of dosing extrapolated to time infinity (AUCinf)

Time: Up to Day 71

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Secondary Outcomes

Description: Adverse events (AEs) will be coded using medical dictionary for regulatory activities (MedDRA). An AE is any untoward medical occurrence in a participant administered an Investigational Product (IP), and which 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), symptom, or disease temporally associated with the use of IP whether or not considered related to the IP. An AE is considered "serious" if the event: results in death; is life-threatening; results in persistent or significant disability/incapacity or substantial disruption of the ability to conduct normal life functions; results in congenital anomaly or birth defect; requires inpatient hospitalization (except for planned procedures)or leads to prolongation of hospitalization (except if prolongation of planned hospitalization is not caused by an AE); or other medically important events.

Measure: Number of participants with Adverse Events (AEs)

Time: Up to Day 101

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Description: Number of participants with potentially clinically significant laboratory values.

Measure: Number of participants with laboratory value abnormalities and/or adverse events (AEs)

Time: Up to Day 101

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Description: Number of participants with potentially clinically significant vital sign values.

Measure: Number of participants with vital sign abnormalities and /or adverse events (AEs)

Time: Up to Day 101

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Description: Number of participants with potentially clinically significant ECG values.

Measure: Number of participants with routine 12-lead electrocardiogram (ECG) abnormalities and/or Adverse Events (AEs)

Time: Up to Day 101

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Description: Cmax will be recorded from the pharmacokinetic (PK) plasma samples collected.

Measure: Pharmacokinetics (PK) of enzalutamide and its metabolite (N-desmethyl) in plasma: maximum concentration (Cmax)

Time: Up to Day 71

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Description: AUCtau will be recorded from the pharmacokinetic (PK) plasma samples collected.

Measure: Pharmacokinetics (PK) of enzalutamide and its metabolite (N-desmethyl) in plasma: area under the concentration-time curve during a dosing interval, where tau (τ) is the length of the dosing interval (AUCtau)

Time: Up to Day 71

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Description: Ctrough will be recorded from the pharmacokinetic (PK) plasma samples collected.

Measure: Pharmacokinetics (PK) of enzalutamide and its metabolite (N-desmethyl) in plasma: concentration immediately prior to dosing at multiple dosing (Ctrough)

Time: Up to Day 71

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Primary Outcomes

Description: To determine a maximum tolerated dose (MTD) of tildrakizumab by establishing the dose at which the DLT rate is as close to the target DLT rate of 15% as possible, in combination with abiraterone at 1000 mg OD with prednisolone at 5 mg bid, and is deemed to be tolerable by the Safety Review Committee. This will be the RP2D for tildrakizumab.

Measure: Phase I - To describe the safety and tolerability of abiraterone acetate and tildrakizumab when given in combination. To establish a RP2D for tildrakizumab, in combination with abiraterone.

Time: 12 months

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Description: Antitumour activity will be defined by response rate on the basis of the following outcomes. If any of the following occur, patients will be considered to have responded: PSA decline ≥ 50% criteria confirmed 4-weeks or later and/or, Confirmed soft tissue objective response by RECIST (v1.1) in patients with measurable disease and/or, ONLY for patients with detectable circulating tumour cell (CTC) count of ≥ 5/7.5ml blood at baseline, conversion of CTC count to <5/7.5ml blood nadir.

Measure: Phase II - To determine the antitumour activity of tildrakizumab (at RP2D) in combination with abiraterone in men with mCRPC.

Time: 12 months

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