Targeted Alpha Therapy Using Astatine (At-211) Against Differentiated Thyroid Cancer
Primary Purpose
Thyroid Cancer
Status
Recruiting
Phase
Phase 1
Locations
Japan
Study Type
Interventional
Intervention
Targeted alpha therapy
Sponsored by
About this trial
This is an interventional treatment trial for Thyroid Cancer focused on measuring Targeted alpha therapy, Astatine (At-211)
Eligibility Criteria
Inclusion Criteria:
- Patients with differentiated thyroid cancer (papillary cancer, follicular cancer) after total thyroidectomy who meet the following conditions (1) resistance to standard treatment or (2) difficulty in continuing standard treatment (1) Patients who are refractory to standard treatment such as 131I-NaI treatment Insufficient therapeutic effect after 3 or more 131I-NaI treatments. 131I-NaI treatment resistance and difficulty in performing or continuing tyrosine kinase inhibitor (TKI) treatment (2) Patients who have difficulty continuing standard treatment such as 131I-NaI treatment Ablation for residual thyroid or 131I-NaI treatment for relapsed / metastatic lesions has been performed, but relapsed / metastatic lesions were observed at the time of participation in this study, and 131I-NaI is the standard treatment. If it is difficult to continue treatment or if local radiation therapy (including addition) is not indicated (if it is not 131I-NaI treatment resistant, TKI treatment is not indicated).
- Patients aged 18 years or older at the time of consent acquisition
- Patients with stable general condition with PS (Performance status) of 0 to 2 in ECOG (Eastern Cooperative Oncology Group)
- Patients who can be expected to survive for 6 months or more, judging from clinical symptoms and medical examination findings
- Patients with no or controlled brain metastases with symptoms
- Patients with no clinically significant abnormal findings in electrocardiogram, respiratory rate, and blood oxygen saturation within 30 days before registration
- Patients whose laboratory values within 30days before the enrollment are within the range specified in the protocol
- Patients who thoroughly listened to the explanation of the clinical trial, agreed to the examination, visit during the observation period and follow-up survey, contraception during the clinical trial period, etc. according to the clinical trial protocol, and signed the consent document.
Exclusion Criteria:
- Patients who need fertility preservation
- Pregnant or potentially pregnant women, lactating patients
- Patients with active double cancer (simultaneous double cancer and ectopic double cancer with a disease-free period of 5 years or less)
- Patients who received other investigational or unapproved drugs within 5 weeks prior to enrollment
- Patients who received chemotherapy, immunotherapy or radiation therapy within 8 weeks prior to enrollment in this study
- Patients with uncontrollable active infections
- HBsAg positive, HCV antibody positive or HIV antibody positive patients
- Patients with mental illness or psychiatric symptoms who are judged to be difficult to participate in clinical trials
- Other patients who are judged to be inappropriate by the investigator, etc.
Sites / Locations
- Osaka University HospitalRecruiting
Arms of the Study
Arm 1
Arm Type
Other
Arm Label
Treatment group
Arm Description
Outcomes
Primary Outcome Measures
Treatment-related adverse events as assessed by CTCAE v5.0
Type, severity, frequency of occurrence and duration of adverse events
Dose Limiting Toxicity
Toxicity is defined as one or more of the following items for which a causal relationship with the investigational drug cannot be ruled out.
Grade 3 * hematological toxicity that lasts for 7 days or more
Hematological toxicity of Grade 4 * or higher regardless of duration
Febrile neutropenia regardless of duration
Thrombocytopenia with bleeding tendency or requiring platelet transfusion
Anemia requiring red blood cell transfusion
Neutropenia with infection
Non-hematological toxicity of Grade 3 * or higher that does not improve with symptomatic treatment and lasts for 7 days or longer. However, the following are excluded.
Abnormal laboratory test values that are not clinically significant
Toxicity that can be controlled to Grade 2 * or less with maximum supportive care
Due to exacerbation of the underlying disease (*: Grade specified in CTCAE v.5.0J COG version)
Secondary Outcome Measures
Blood pressure
Systolic and diastolic blood pressure (mmHg)
Heart rate
Pulse (bpm)
Blood oxygen saturation
Percutaneous oxygen saturation (%)
Respiratory rate
Respiratory rate (times/min)
Body temperature
Body temperature (°C)
Body weight
Weight (kg)
Symptoms and examination findings
Subjective symptoms and medical examination findings
Hematological examination
White blood cell count (/μL), red blood cell count (×10^4/μL), hemoglobin (g/dL), hematocrit (%), platelet count (×10^4/μL)
Blood biochemical test
Total protein (g/dL), albumin (g/dL), total bilirubin (mg/dL), AST (U/L), ALT (U/L), ALP (U/L), γ-GTP (U/L), LDH (U/L), total cholesterol (mg/dL), triglyceride (mg/dL), uric acid (mg/dL), BUN (mg/dL), creatinine (mg/dL), CK (U/L), Na (mmol/L), K (mmol/L), Cl (mmol/L), Ca (mmol/L), CRP (mg/dL)
Urinalysis
Urinary protein, urine sugar, urineous blood, urobilinogen (qualitative test)
12-lead ECG
Presence or absence of abnormal findings in waveform
Pharmacokinetic parameters 1)
AUC (Area under the plasma concentration versus time curve, Bq·min/mL)
Pharmacokinetic parameters 2)
AUC / D (Area under the plasma concentration versus time curve divided by injected dose, min/mL)
Pharmacokinetic parameters 3)
Cmax (Peak plasma concentration, Bq/mL)
Pharmacokinetic parameters 4)
Cmax / D (Peak plasma concentration divided by injected dose, /mL)
Pharmacokinetic parameters 5)
Tmax (Time to maximum plasma concentration, min)
Pharmacokinetic parameters 6)
T1 / 2 (Time from Tmax to half of maximum plasma concentration, min)
Pharmacokinetic parameters 7)
CL (Clearance, L/hr/kg)
Pharmacokinetic parameters 8)
Vss (Volume of distribution in steady state, L/kg)
Excretion 1) urinary
Urine volume (mL) and radioactivity (Bq): Radioactivity and volume will be combined to report radioactivity concentration (Bq/mL).
Excretion 2) fecal
Stool weight (g) and radioactivity (Bq): Radioactivity and weight will be combined to report radioactivity concentration (Bq/g).
Excretion 3) exhaled
Exhaled volume (mL) and radioactivity (Bq): Radioactivity and volume will be combined to report radioactivity concentration (Bq/mL).
Radioactivity concentration in major organs
Changes in radioactivity concentration (Bq/mL) in major organs over time: Whole-body imaging (planar and SPECT/CT) is performed to evaluate the distribution in the body at 1 hour, 3 hours, 24 hours after the administration.
Residence time of major organs
Residence time (hr) of each organ
Absorbed dose of major organs
Absorbed dose (mGy / MBq) of each organ
Preliminary effectiveness assessment 1)
Evaluation of treatment effect on CT images by referring to the Revised RECIST guideline (version 1.1): CR (Complete response), PR (Partial response), SD (Stable disease), or PD (Progressive disease)
Preliminary effectiveness assessment 2)
Evaluation of uptake change in diagnostic [131I] NaI scans: CR , PR, SD, or PD
Preliminary effectiveness assessment 3)
Evaluation of changes in tumor markers: blood thyroglobulin (ng/mL)
Full Information
1. Study Identification
Unique Protocol Identification Number
NCT05275946
Brief Title
Targeted Alpha Therapy Using Astatine (At-211) Against Differentiated Thyroid Cancer
Official Title
Phase I Investigator-initiated Clinical Trial in Patients With Differentiated Thyroid Cancer (Papillary Cancer, Follicular Cancer) by the Targeted Alpha Therapy Drug TAH-1005 ([211At] NaAt) (Alpha-T1 Study)
Study Type
Interventional
2. Study Status
Record Verification Date
March 2023
Overall Recruitment Status
Recruiting
Study Start Date
November 20, 2021 (Actual)
Primary Completion Date
March 31, 2024 (Anticipated)
Study Completion Date
September 30, 2024 (Anticipated)
3. Sponsor/Collaborators
Responsible Party, by Official Title
Principal Investigator
Name of the Sponsor
Osaka University
4. Oversight
Studies a U.S. FDA-regulated Drug Product
No
Studies a U.S. FDA-regulated Device Product
No
5. Study Description
Brief Summary
Single intravenous administration of TAH-1005 is performed in patients with differentiated thyroid cancer (papillary cancer, follicular cancer) who cannot obtain therapeutic effect with standard treatment or who have difficulty in implementing and continuing standard treatment. The safety, pharmacokinetics, absorbed dose, and efficacy will be evaluated to determine the recommended dose for Phase II clinical trial.
Detailed Description
Radioactive iodine (I-131) has long been used clinically for patients with metastatic differentiated thyroid cancer. However, some patients are refractory to repetitive I-131 treatment, despite the targeted regions showing sufficient iodine uptake. In such patients, beta-particle therapy using I-131 is inadequate and another strategy is needed using more effective radionuclide targeting the sodium/iodide symporter (NIS). Astatine (At-211) is receiving increasing attention as an alpha-emitter for targeted radionuclide therapy. At-211 is a halogen element with similar chemical properties to iodine. Alpha particles emitted from At-211 has higher linear energy transfer as compared to beta particles from I-131 and exert a better therapeutic effect by inducing DNA double strand breaks and free radical formation. Thus, targeted alpha therapy using At-211 is highly promising for the treatment of advanced differentiated thyroid cancer.
6. Conditions and Keywords
Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Thyroid Cancer
Keywords
Targeted alpha therapy, Astatine (At-211)
7. Study Design
Primary Purpose
Treatment
Study Phase
Phase 1
Interventional Study Model
Single Group Assignment
Masking
None (Open Label)
Allocation
N/A
Enrollment
11 (Anticipated)
8. Arms, Groups, and Interventions
Arm Title
Treatment group
Arm Type
Other
Intervention Type
Drug
Intervention Name(s)
Targeted alpha therapy
Intervention Description
Single intravenous administration
Primary Outcome Measure Information:
Title
Treatment-related adverse events as assessed by CTCAE v5.0
Description
Type, severity, frequency of occurrence and duration of adverse events
Time Frame
From the start of iodine restriction to 6 months after administration
Title
Dose Limiting Toxicity
Description
Toxicity is defined as one or more of the following items for which a causal relationship with the investigational drug cannot be ruled out.
Grade 3 * hematological toxicity that lasts for 7 days or more
Hematological toxicity of Grade 4 * or higher regardless of duration
Febrile neutropenia regardless of duration
Thrombocytopenia with bleeding tendency or requiring platelet transfusion
Anemia requiring red blood cell transfusion
Neutropenia with infection
Non-hematological toxicity of Grade 3 * or higher that does not improve with symptomatic treatment and lasts for 7 days or longer. However, the following are excluded.
Abnormal laboratory test values that are not clinically significant
Toxicity that can be controlled to Grade 2 * or less with maximum supportive care
Due to exacerbation of the underlying disease (*: Grade specified in CTCAE v.5.0J COG version)
Time Frame
within 4 weeks after administration
Secondary Outcome Measure Information:
Title
Blood pressure
Description
Systolic and diastolic blood pressure (mmHg)
Time Frame
within 4 weeks after administration
Title
Heart rate
Description
Pulse (bpm)
Time Frame
within 4 weeks after administration
Title
Blood oxygen saturation
Description
Percutaneous oxygen saturation (%)
Time Frame
within 4 weeks after administration
Title
Respiratory rate
Description
Respiratory rate (times/min)
Time Frame
within 4 weeks after administration
Title
Body temperature
Description
Body temperature (°C)
Time Frame
within 4 weeks after administration
Title
Body weight
Description
Weight (kg)
Time Frame
within 4 weeks after administration
Title
Symptoms and examination findings
Description
Subjective symptoms and medical examination findings
Time Frame
within 4 weeks after administration
Title
Hematological examination
Description
White blood cell count (/μL), red blood cell count (×10^4/μL), hemoglobin (g/dL), hematocrit (%), platelet count (×10^4/μL)
Time Frame
within 4 weeks after administration
Title
Blood biochemical test
Description
Total protein (g/dL), albumin (g/dL), total bilirubin (mg/dL), AST (U/L), ALT (U/L), ALP (U/L), γ-GTP (U/L), LDH (U/L), total cholesterol (mg/dL), triglyceride (mg/dL), uric acid (mg/dL), BUN (mg/dL), creatinine (mg/dL), CK (U/L), Na (mmol/L), K (mmol/L), Cl (mmol/L), Ca (mmol/L), CRP (mg/dL)
Time Frame
within 4 weeks after administration
Title
Urinalysis
Description
Urinary protein, urine sugar, urineous blood, urobilinogen (qualitative test)
Time Frame
within 4 weeks after administration
Title
12-lead ECG
Description
Presence or absence of abnormal findings in waveform
Time Frame
within 4 weeks after administration
Title
Pharmacokinetic parameters 1)
Description
AUC (Area under the plasma concentration versus time curve, Bq·min/mL)
Time Frame
until 24 hours after administration
Title
Pharmacokinetic parameters 2)
Description
AUC / D (Area under the plasma concentration versus time curve divided by injected dose, min/mL)
Time Frame
until 24 hours after administration
Title
Pharmacokinetic parameters 3)
Description
Cmax (Peak plasma concentration, Bq/mL)
Time Frame
until 24 hours after administration
Title
Pharmacokinetic parameters 4)
Description
Cmax / D (Peak plasma concentration divided by injected dose, /mL)
Time Frame
until 24 hours after administration
Title
Pharmacokinetic parameters 5)
Description
Tmax (Time to maximum plasma concentration, min)
Time Frame
until 24 hours after administration
Title
Pharmacokinetic parameters 6)
Description
T1 / 2 (Time from Tmax to half of maximum plasma concentration, min)
Time Frame
until 24 hours after administration
Title
Pharmacokinetic parameters 7)
Description
CL (Clearance, L/hr/kg)
Time Frame
until 24 hours after administration
Title
Pharmacokinetic parameters 8)
Description
Vss (Volume of distribution in steady state, L/kg)
Time Frame
until 24 hours after administration
Title
Excretion 1) urinary
Description
Urine volume (mL) and radioactivity (Bq): Radioactivity and volume will be combined to report radioactivity concentration (Bq/mL).
Time Frame
until 24 hours after administration
Title
Excretion 2) fecal
Description
Stool weight (g) and radioactivity (Bq): Radioactivity and weight will be combined to report radioactivity concentration (Bq/g).
Time Frame
until 24 hours after administration
Title
Excretion 3) exhaled
Description
Exhaled volume (mL) and radioactivity (Bq): Radioactivity and volume will be combined to report radioactivity concentration (Bq/mL).
Time Frame
until 24 hours after administration
Title
Radioactivity concentration in major organs
Description
Changes in radioactivity concentration (Bq/mL) in major organs over time: Whole-body imaging (planar and SPECT/CT) is performed to evaluate the distribution in the body at 1 hour, 3 hours, 24 hours after the administration.
Time Frame
until 24 hours after administration
Title
Residence time of major organs
Description
Residence time (hr) of each organ
Time Frame
until 24 hours after administration
Title
Absorbed dose of major organs
Description
Absorbed dose (mGy / MBq) of each organ
Time Frame
until 24 hours after administration
Title
Preliminary effectiveness assessment 1)
Description
Evaluation of treatment effect on CT images by referring to the Revised RECIST guideline (version 1.1): CR (Complete response), PR (Partial response), SD (Stable disease), or PD (Progressive disease)
Time Frame
3 and 6 months after administration
Title
Preliminary effectiveness assessment 2)
Description
Evaluation of uptake change in diagnostic [131I] NaI scans: CR , PR, SD, or PD
Time Frame
3 and 6 months after administration
Title
Preliminary effectiveness assessment 3)
Description
Evaluation of changes in tumor markers: blood thyroglobulin (ng/mL)
Time Frame
3 and 6 months after administration
10. Eligibility
Sex
All
Maximum Age & Unit of Time
18 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria:
Patients with differentiated thyroid cancer (papillary cancer, follicular cancer) after total thyroidectomy who meet the following conditions (1) resistance to standard treatment or (2) difficulty in continuing standard treatment (1) Patients who are refractory to standard treatment such as 131I-NaI treatment Insufficient therapeutic effect after 3 or more 131I-NaI treatments. 131I-NaI treatment resistance and difficulty in performing or continuing tyrosine kinase inhibitor (TKI) treatment (2) Patients who have difficulty continuing standard treatment such as 131I-NaI treatment Ablation for residual thyroid or 131I-NaI treatment for relapsed / metastatic lesions has been performed, but relapsed / metastatic lesions were observed at the time of participation in this study, and 131I-NaI is the standard treatment. If it is difficult to continue treatment or if local radiation therapy (including addition) is not indicated (if it is not 131I-NaI treatment resistant, TKI treatment is not indicated).
Patients aged 18 years or older at the time of consent acquisition
Patients with stable general condition with PS (Performance status) of 0 to 2 in ECOG (Eastern Cooperative Oncology Group)
Patients who can be expected to survive for 6 months or more, judging from clinical symptoms and medical examination findings
Patients with no or controlled brain metastases with symptoms
Patients with no clinically significant abnormal findings in electrocardiogram, respiratory rate, and blood oxygen saturation within 30 days before registration
Patients whose laboratory values within 30days before the enrollment are within the range specified in the protocol
Patients who thoroughly listened to the explanation of the clinical trial, agreed to the examination, visit during the observation period and follow-up survey, contraception during the clinical trial period, etc. according to the clinical trial protocol, and signed the consent document.
Exclusion Criteria:
Patients who need fertility preservation
Pregnant or potentially pregnant women, lactating patients
Patients with active double cancer (simultaneous double cancer and ectopic double cancer with a disease-free period of 5 years or less)
Patients who received other investigational or unapproved drugs within 5 weeks prior to enrollment
Patients who received chemotherapy, immunotherapy or radiation therapy within 8 weeks prior to enrollment in this study
Patients with uncontrollable active infections
HBsAg positive, HCV antibody positive or HIV antibody positive patients
Patients with mental illness or psychiatric symptoms who are judged to be difficult to participate in clinical trials
Other patients who are judged to be inappropriate by the investigator, etc.
Central Contact Person:
First Name & Middle Initial & Last Name or Official Title & Degree
Tadashi Watabe, M.D., Ph.D.
Phone
+81-6-6879-3461
Email
watabe@tracer.med.osaka-u.ac.jp
Facility Information:
Facility Name
Osaka University Hospital
City
Suita
ZIP/Postal Code
565-0871
Country
Japan
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Tadashi Watabe, M.D., Ph.D.
Phone
+81-6-6879-3461
Email
watabe@tracer.med.osaka-u.ac.jp
First Name & Middle Initial & Last Name & Degree
Tadashi Watabe, M.D., Ph.D.
12. IPD Sharing Statement
Plan to Share IPD
Undecided
Learn more about this trial
Targeted Alpha Therapy Using Astatine (At-211) Against Differentiated Thyroid Cancer
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