search
Back to results

124I-p5+14 Injection Safety in Subjects With Systemic Amyloidosis

Primary Purpose

Systemic Amyloidosis

Status
Completed
Phase
Phase 1
Locations
United States
Study Type
Interventional
Intervention
124I-p5+14 Injection
Sponsored by
University of Tennessee Graduate School of Medicine
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional diagnostic trial for Systemic Amyloidosis focused on measuring Amyloidosis, AL, ATTR, ALect2

Eligibility Criteria

18 Years - undefined (Adult, Older Adult)All SexesDoes not accept healthy volunteers

Subjects included in this trial are volunteers with a confirmed diagnosis of systemic amyloidosis, a genetically well-defined mutation of the TTR gene but without clinical evidence of active disease, and at an age typical of development of symptomology ≥ 50, or healthy control subjects (≥30 years).

Prior to participation in Parts 1 or 2 of the trial (n = 73), the following inclusion criteria must be met

Subjects included in this trial are volunteers with a confirmed diagnosis of systemic amyloidosis, a genetically well-defined mutation of the TTR gene but without clinical evidence of active disease, and at an age typical of development of symptomology ≥ 50, or healthy control subjects (≥30 years).

Prior to participation in Parts 1 or 2 of the trial (n = 73), the following inclusion criteria must be met:

  1. Patients must have a confirmed diagnosis of systemic amyloidosis, based on either a histologic confirmation that a biopsy contains deposits of apple-green birefringent, Congophilic material or genetic screening and presence of amyloid-related pathology, or amyloid-specific imaging study. Additionally, the type of amyloidosis (AL, ATTR, ALect2, or other) should be characterized.
  2. Patients enrolled in Part 1 (n = 3) must have widespread AL amyloidosis, defined as biopsy proven or clinically detectable involvement, of at least two organs (excluding the peripheral nervous system).
  3. All patients in Parts 1 and 2 will be 18 years of age or older. There are no gender or racial restrictions.
  4. Women of child bearing potential (those who have not been surgically sterilized, are not postmenopausal [typically understood to mean last menstrual period >2 y ago without pharmaceutical intervention], and women who are fertile) must test negative for pregnancy in a laboratory test administered by the site physician.
  5. Patients who have had or are currently receiving therapy or other drug based anti-amyloid regimens can be included on study (Parts 1 and 2).
  6. Patients must provide signed, written, informed consent and be willing to comply with eligibility requirements, scheduled visits, and follow-up studies.
  7. Due to annual dosimetry limitations, patients who have participated in another nuclear medicine amyloid imaging clinical trial protocol can be included in this study no earlier than 12 months after the previous radiotracer injection.
  8. In Part 2, inclusion of patients with amyloid subsets AL, ATTR, and ALect2 will continue until the trial has achieved recruitment goals for each subset: 30 AL; 20 ATTR; 5 ALect2; and 10 15 "Other".

Prior to participation in Part 3 (n = 10 subjects) of the trial, the following inclusion criteria must be met:

  1. Patients must have a well-defined germline mutation of the transthyretin (TTR) gene rendering them at risk for amyloidosis, and be free of clinical evidence of SA.
  2. All patients in Part 3 will be >50 years of age. There are no gender or racial restrictions.
  3. Women of child bearing potential (those who have not been surgically sterilized, are not postmenopausal [typically understood to mean last menstrual period >2 y ago without pharmaceutical intervention], and women who are fertile) must test negative for pregnancy in a laboratory test administered by the site physician.
  4. Subjects must provide signed, written, informed consent and be willing to comply with eligibility requirements, scheduled visits, and follow-up studies.
  5. Due to annual dosimetry limitations, subjects who have participated in another nuclear medicine amyloid imaging clinical trial protocol can be included in this study no earlier than 12 months after the previous radiotracer injection.

Prior to participation Part 4 of the trial (n = 5), the following inclusion criteria must be met:

  1. Healthy Control Subjects (HC) will be generally healthy adults, either male or female, and will not have a diagnosis of amyloidosis, will not have a first- or second-degree relative (parent, sibling, child, aunt, uncle, niece, nephew) with confirmed or suspected familial amyloidosis, and will not have diabetes mellitus (type 2).
  2. All Part 4 subjects will be > 30 years of age or older.
  3. Women of child bearing potential (those who have not been surgically sterilized, are not postmenopausal [typically understood to mean last menstrual period >2 y ago without pharmaceutical intervention], and women who are fertile) must test negative for pregnancy in a laboratory test administered by the site physician.
  4. Patients must provide signed, written, informed consent and be willing to comply with eligibility requirements, scheduled visits, and follow-up studies.
  5. Due to annual dosimetry limitations, patients who have participated in another nuclear medicine imaging clinical trial protocol can be included in this study no earlier than 12 months after the previous radiotracer injection.

Prior to participation in Part 5 of the trial, the following inclusion criteria must be met:

  1. Patients must have successfully completed participation in Part 2 or Part 3 of this trial with CT/PET images confirming the presence of abnormal amyloid deposits in thoracoabdominal organs.
  2. Patients must have received a 2 mCi dose of 124I-p5+14 Injection during Part 2 or 3 of this trial with visual evidence of uptake of radiotracer in abdominothoracic organs associated with amyloid.
  3. The repeat exposure to the study agent must occur at least 6 months after the first exposure.
  4. Patients must submit a serum specimen for exploratory evaluation of the presence of anti-p5+14 peptide antibodies, with results reviewed by the Principal Investigator prior to a second exposure to the study agent.
  5. The patient must meet all of the Inclusion criteria for participation in Part 2 or Part 3 outlined in Sections 5.2 or Section 5.3 (as applicable), including the signing of an informed consent for Part 5.

In addition, the following criteria will exclude candidates from participation in the trial, Parts 1 and 2:

  1. Those with significant co-morbidity (e.g., Eastern Cooperative Oncology Group [ECOG] score of 3 or greater), uncontrolled infection, or other serious illness.
  2. Patients with a sustained SpO2 of ≤ 92% as noted in the medical record.
  3. Patients that require renal dialysis.
  4. Women who are of child bearing potential (those who have not been surgically sterilized, are not postmenopausal [typically understood to mean last menstrual period >2 y ago without pharmaceutical intervention], and women who are fertile) who test positive for pregnancy in a laboratory test administered by the site physician, are pregnant, or are nursing
  5. Patients who have received any amyloidophilic radiotracer as part of a research clinical trial (not standard of care) within the past 12 months.
  6. Patients with exposure to heparin, or heparin-based medications, within 7 days prior to the imaging study.
  7. Patients who have a known allergy to acetaminophen or iOSAT iodine treatment.

The following criteria will exclude candidates from participation in Part 3 of the trial:

  1. Those with significant co-morbidity (e.g., Eastern Cooperative Oncology Group [ECOG] score of 3 or greater), uncontrolled infection, or other serious illness.
  2. Subjects with a sustained SpO2 of ≤ 92% as noted in the medical record.
  3. Women who are of child bearing potential (those who have not been surgically sterilized, are not postmenopausal [typically understood to mean last menstrual period >2 y ago without pharmaceutical intervention], and women who are fertile) who test positive for pregnancy in a laboratory test administered by the site physician, are pregnant, or are nursing.
  4. Subjects who have clinical evidence of amyloidosis based on standard clinical criteria.
  5. Subjects with polyneuropathy of unknown origin.
  6. Subjects who have received any amyloidophilic radiotracer as part of a research clinical trial (not standard of care) within the past 12 months.
  7. Subjects with exposure to heparin, or heparin-based medications, within 7 days prior to the imaging study.
  8. Subjects who have a known allergy to acetaminophen or iOSAT iodine treatment.
  9. Subjects with clinical signs of SA based on routine investigation of serum and urine biomarkers, radiographic or nuclear imaging studies, or peripheral nerve evaluations.

The following criteria will exclude subjects from participation in Part 4:

  1. Those with significant co-morbidity (e.g., Eastern Cooperative Oncology Group [ECOG] score of 2 (Restricted in physically strenuous activity but ambulatory and able to carry out work of a light or sedentary nature, e.g. light house work, office work) or greater), uncontrolled infection, or other serious illness.
  2. Individuals with a sustained SpO2 of ≤ 92% as noted in the medical record.
  3. Women who are of child bearing potential (those who have not been surgically sterilized, are not postmenopausal [typically understood to mean last menstrual period >2 y ago without pharmaceutical intervention], and women who are fertile) who test positive for pregnancy in a laboratory test administered by the site physician, are pregnant, or are nursing.
  4. Subjects who have received any amyloidophilic radiotracer as part of a research clinical trial (not standard of care) within the past 12 months.
  5. Subjects with exposure to heparin, or heparin-based medications, within 30 days prior to the imaging study.
  6. Subjects who have a known allergy to acetaminophen or iOSAT iodine treatment.
  7. Subjects with a diagnosis of Type 2 diabetes mellitus or who are taking medication for management of Type 2 diabetes mellitus.
  8. Active infection requiring systemic antiviral or antimicrobial therapy that will not be completed prior to Study Day 1.
  9. Known history of or positive test for human immunodeficiency virus (HIV), hepatitis C or chronic hepatitis.
  10. Uncontrolled hypertension (BP > 160/100 mm Hg).
  11. Smokes >20 cigarettes a day.
  12. A diagnosis of heart failure with preserved ejection fraction.
  13. Has any other conditions, which, in the opinion of the Investigator would make the subject unsuitable for inclusion, or could interfere with the subject participating in or completing the study

The following criteria will exclude subjects from participation in Part 5.

  1. Any patient who experienced a clinically significant adverse event related to prior exposure to the study agent.
  2. Any subject who meets any of the Exclusion Criteria for Part 2 or Part 3 (as applicable), described in Section 5.3.1 and Section 5.3.2.

Sites / Locations

  • University of Tennessee Medical Center

Arms of the Study

Arm 1

Arm Type

Experimental

Arm Label

124I-p5+14 Injection

Arm Description

A single-injection dose of 124I-p5+14 adequate for imaging amyloid deposits by using PET/CT imaging in subjects with confirmed systemic amyloidosis of several sub-types.

Outcomes

Primary Outcome Measures

Organ-specific radioactivity dosimetry (Part 1).
Localization of 124I-p5+14 will be taken from PET/CT images performed at intervals during the 48 hours after injection. Organ-specific dosimetry and whole body dose measurements will be made using Olinda software (Olinda/Exp; Organ Level Internal Dose Assessment/Exponential Modeling)

Secondary Outcome Measures

Absolute values and changes from baseline in clinical laboratory values.
Laboratory assessments will include hematology and clinical chemistry.
Clinically defined amyloidosis organ involvement.
For each subject, the clinician/investigator will designate each organ as involved or not involved with amyloidosis, based on available medical history including prior imaging, prior biopsy results, and clinical laboratory values.
Measure of background radioactivity uptake.
For each subject, a background radioactivity uptake measure will be derived from the PET images at an uninvolved anatomic site (the lumen of a large blood vessel).
Measure of radioactivity uptake by each organ
Uptake of 124I-p5+14 will be derived from PET/CT scans performed at 6 hours and 24 hours after injection. Any organ with >=2-fold higher accumulation of radiotracer, relative to the background uptake, will be considered positive.
Concentration of radiotracer in specific anatomic sites, for each subject and anatomic site
Concentration of 124I-p5+14 will be derived from PET/CT scans performed at 6 hours and 24 hours after injection.
Organ and tissue-specific sensitivity of the 124I-p5+14 Injection radiotracer
Sensitivity for each organ will be derived from the list of clinically involved organs (Secondary Measure 1) and the list of organ radioactivity uptake (Secondary Measure 4), using the formula, true positive rate = [True positive/(True positive + False negative)].
Correlation between concentration of the radiotracer (Bq/cc) in the kidney with organ-associated clinical biomarkers.
Statistical correlation of kidney radiotracer uptake with proteinuria, albuminuria, creatinine, and blood urea nitrogen (BUN).
Correlation between concentration of the radiotracer (Bq/cc) in the heart with organ-associated clinical biomarkers.
Statistical correlation of heart radiotracer uptake with N-terminal-pro-brain natriuretic peptide (NT-BNP) or Brain Natriuretic Peptide (BNP) serum levels, intraventricular septal thickness, and ejection fraction (measures as available from medical history)
Peptide uptake in the heart.
Peptide uptake will be recorded as the Standard Uptake Value (SUV) or as Bq/cc of organ volume; obtained from the Region of Interest (ROI) analysis
Peptide uptake in the kidney
Peptide uptake will be recorded as the Standard Uptake Value (SUV) or as Bq/cc of organ volume; obtained from the Region of Interest (ROI) analysis.
Peptide uptake in organ(s) other than kidney or heart if clinically relevant
Peptide uptake will be recorded as the Standard Uptake Value (SUV) or as Bq/cc of organ volume; obtained from the Region of Interest (ROI) analysis
Correlation between uptake of peptide and clinical status of kidney, heart and other organs
Correlation between uptake of peptide (from ROI measurements) and the clinical status of kidney, heart, and other organs if indicated (clinical status defined as in Secondary Endpoint 1).

Full Information

First Posted
July 30, 2018
Last Updated
March 23, 2022
Sponsor
University of Tennessee Graduate School of Medicine
search

1. Study Identification

Unique Protocol Identification Number
NCT03678259
Brief Title
124I-p5+14 Injection Safety in Subjects With Systemic Amyloidosis
Official Title
Evaluation of 124I-p5+14 Injection as an Imaging Agent for the Detection of Systemic Amyloidosis
Study Type
Interventional

2. Study Status

Record Verification Date
July 2021
Overall Recruitment Status
Completed
Study Start Date
October 1, 2018 (Actual)
Primary Completion Date
October 1, 2021 (Actual)
Study Completion Date
October 1, 2021 (Actual)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor
Name of the Sponsor
University of Tennessee Graduate School of Medicine

4. Oversight

Studies a U.S. FDA-regulated Drug Product
Yes
Studies a U.S. FDA-regulated Device Product
No
Data Monitoring Committee
No

5. Study Description

Brief Summary
This is a single-center, exploratory, Phase 1 Positron Emission Tomography/x-ray Computed Tomography (PET/CT) imaging study to detect amyloidosis that will enroll patients with a confirmed diagnosis of systemic amyloidosis. The purpose of this exploratory trial is to assess the safety and efficacy of 124I-p5+14 Injection at a single-injection dose adequate for imaging amyloid deposits by using PET/CT imaging in subjects with confirmed systemic Immunoglobulin Light Chain-associated Amyloidosis (AL), Transthyretin-associated Amyloidosis (ATTR), Leukocyte Chemotactic Factor 2-associated Amyloidosis (ALect2) as well as other types.
Detailed Description
The rationale for this study is the discovery of a synthetic polypeptide, designated p5+14, a synthetic 45 amino acid peptide that binds many forms of amyloid, including human AL-, ATTR- and ALect2-associated amyloid, as well as human and murine serum amyloid protein A-associated (AA) amyloid. In preclinical studies, using SPECT and PET imaging, as well as microautoradiography, it has been shown that radioiodinated p5+14 binds rapidly and specifically to all amyloid deposits in abdominothoracic organs and tissues. This is a single site, exploratory, open-label Phase I PET/CT imaging and dosimetry study. The investigational drug product (designated 124I-p5+14 Injection) is an amyloid-reactive synthetic peptide, p5+14 (also known as APi1832), radiolabeled with iodine-124 (I-124 or 124I). All patients enrolled in this exploratory trial will be outpatients with a confirmed diagnosis of systemic amyloidosis. The first three patients enrolled in the trial (Part 1) will take part in a dose-escalation dosimetry study and will receive a single intravenous (IV) dose of 11.1 Megabecquerel (MBq) (0.3 millicuries (mCi); n = 1), 37 MBq (1 mCi; n = 1) or 74 MBq (2 mCi; n = 1) of 124I-p5+14 Injection for the purpose of determining estimates of organ-associated and whole body radioactive dosimetry. The trial then will be opened to include another 54 patients who will receive a single IV bolus injection of 2 mCi 124I-p5+14 Injection. Every patient participating will receive < 2 mg of peptide p5+14. The study comprises five parts. In Part 2, the trial will enroll SA patients with confirmed AL, ATTR, ALECT2, or other forms of amyloidosis. In Part 3, the trial will study asymptomatic subjects with genetically confirmed mutation of the transthyretin gene. Part 4 will include five healthy control subjects. Part 5 will recruit previously enrolled subjects from Parts 2 or 3 who received a 2 mC dose of 124I-p5+14 Injection and had images confirming the presence of abnormal amyloid deposits for a second exposure to 124I p5+14 Injection and second PET/CT scan.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Systemic Amyloidosis
Keywords
Amyloidosis, AL, ATTR, ALect2

7. Study Design

Primary Purpose
Diagnostic
Study Phase
Phase 1, Phase 2
Interventional Study Model
Single Group Assignment
Model Description
The first three patients enrolled in the trial (Part 1) will take part in a dose-escalation study and will receive a single IV dose 11.1 MBq (0.3 mCi; n = 1), 37 MBq (1 mCi; n = 1) or 74 MBq (2 mCi; n = 1) of 124I-p5+14 Injection. The trial then will be opened to include another 54 patients who will receive a single IV bolus injection of 2 mCi 124I-p5+14 Injection. Every patient participating will receive < 2 mg of peptide p5+14. The study comprises five parts.In Part 2, the trial will enroll SA patients with confirmed AL, ATTR, ALECT2, or other forms of amyloidosis.In Part 3, the trial will study asymptomatic subjects with genetically confirmed mutation of the transthyretin gene.Part 4 will include five healthy control subjects.Part 5 will recruit previously enrolled subjects from Parts 2 or 3 who received a 2 mC dose of 124I-p5+14 Injection and had images confirming the presence of abnormal amyloid deposits for a second exposure to 124I p5+14 Injection and second PET/CT scan.
Masking
None (Open Label)
Masking Description
open-label
Allocation
N/A
Enrollment
57 (Actual)

8. Arms, Groups, and Interventions

Arm Title
124I-p5+14 Injection
Arm Type
Experimental
Arm Description
A single-injection dose of 124I-p5+14 adequate for imaging amyloid deposits by using PET/CT imaging in subjects with confirmed systemic amyloidosis of several sub-types.
Intervention Type
Drug
Intervention Name(s)
124I-p5+14 Injection
Other Intervention Name(s)
APi1832
Intervention Description
124I-p5+14 Injection which is a formulation of a synthetic, all natural, 45 amino acid peptide (MW = 4766.4) with a net +12 positive charge
Primary Outcome Measure Information:
Title
Organ-specific radioactivity dosimetry (Part 1).
Description
Localization of 124I-p5+14 will be taken from PET/CT images performed at intervals during the 48 hours after injection. Organ-specific dosimetry and whole body dose measurements will be made using Olinda software (Olinda/Exp; Organ Level Internal Dose Assessment/Exponential Modeling)
Time Frame
Through 48 hours
Secondary Outcome Measure Information:
Title
Absolute values and changes from baseline in clinical laboratory values.
Description
Laboratory assessments will include hematology and clinical chemistry.
Time Frame
Baseline and 24 hours
Title
Clinically defined amyloidosis organ involvement.
Description
For each subject, the clinician/investigator will designate each organ as involved or not involved with amyloidosis, based on available medical history including prior imaging, prior biopsy results, and clinical laboratory values.
Time Frame
Baseline
Title
Measure of background radioactivity uptake.
Description
For each subject, a background radioactivity uptake measure will be derived from the PET images at an uninvolved anatomic site (the lumen of a large blood vessel).
Time Frame
6 hours and 24 hours
Title
Measure of radioactivity uptake by each organ
Description
Uptake of 124I-p5+14 will be derived from PET/CT scans performed at 6 hours and 24 hours after injection. Any organ with >=2-fold higher accumulation of radiotracer, relative to the background uptake, will be considered positive.
Time Frame
6 hours and 24 hours
Title
Concentration of radiotracer in specific anatomic sites, for each subject and anatomic site
Description
Concentration of 124I-p5+14 will be derived from PET/CT scans performed at 6 hours and 24 hours after injection.
Time Frame
6 hours and 24 hours
Title
Organ and tissue-specific sensitivity of the 124I-p5+14 Injection radiotracer
Description
Sensitivity for each organ will be derived from the list of clinically involved organs (Secondary Measure 1) and the list of organ radioactivity uptake (Secondary Measure 4), using the formula, true positive rate = [True positive/(True positive + False negative)].
Time Frame
6 hours and 24 hours
Title
Correlation between concentration of the radiotracer (Bq/cc) in the kidney with organ-associated clinical biomarkers.
Description
Statistical correlation of kidney radiotracer uptake with proteinuria, albuminuria, creatinine, and blood urea nitrogen (BUN).
Time Frame
6 hours and 24 hours
Title
Correlation between concentration of the radiotracer (Bq/cc) in the heart with organ-associated clinical biomarkers.
Description
Statistical correlation of heart radiotracer uptake with N-terminal-pro-brain natriuretic peptide (NT-BNP) or Brain Natriuretic Peptide (BNP) serum levels, intraventricular septal thickness, and ejection fraction (measures as available from medical history)
Time Frame
6 hours and 24 hours
Title
Peptide uptake in the heart.
Description
Peptide uptake will be recorded as the Standard Uptake Value (SUV) or as Bq/cc of organ volume; obtained from the Region of Interest (ROI) analysis
Time Frame
6 hours and 24 hours
Title
Peptide uptake in the kidney
Description
Peptide uptake will be recorded as the Standard Uptake Value (SUV) or as Bq/cc of organ volume; obtained from the Region of Interest (ROI) analysis.
Time Frame
6 hours and 24 hours
Title
Peptide uptake in organ(s) other than kidney or heart if clinically relevant
Description
Peptide uptake will be recorded as the Standard Uptake Value (SUV) or as Bq/cc of organ volume; obtained from the Region of Interest (ROI) analysis
Time Frame
6 hours and 24 hours
Title
Correlation between uptake of peptide and clinical status of kidney, heart and other organs
Description
Correlation between uptake of peptide (from ROI measurements) and the clinical status of kidney, heart, and other organs if indicated (clinical status defined as in Secondary Endpoint 1).
Time Frame
Baseline and 24 hours

10. Eligibility

Sex
All
Minimum Age & Unit of Time
18 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Subjects included in this trial are volunteers with a confirmed diagnosis of systemic amyloidosis, a genetically well-defined mutation of the TTR gene but without clinical evidence of active disease, and at an age typical of development of symptomology ≥ 50, or healthy control subjects (≥30 years). Prior to participation in Parts 1 or 2 of the trial (n = 73), the following inclusion criteria must be met Subjects included in this trial are volunteers with a confirmed diagnosis of systemic amyloidosis, a genetically well-defined mutation of the TTR gene but without clinical evidence of active disease, and at an age typical of development of symptomology ≥ 50, or healthy control subjects (≥30 years). Prior to participation in Parts 1 or 2 of the trial (n = 73), the following inclusion criteria must be met: Patients must have a confirmed diagnosis of systemic amyloidosis, based on either a histologic confirmation that a biopsy contains deposits of apple-green birefringent, Congophilic material or genetic screening and presence of amyloid-related pathology, or amyloid-specific imaging study. Additionally, the type of amyloidosis (AL, ATTR, ALect2, or other) should be characterized. Patients enrolled in Part 1 (n = 3) must have widespread AL amyloidosis, defined as biopsy proven or clinically detectable involvement, of at least two organs (excluding the peripheral nervous system). All patients in Parts 1 and 2 will be 18 years of age or older. There are no gender or racial restrictions. Women of child bearing potential (those who have not been surgically sterilized, are not postmenopausal [typically understood to mean last menstrual period >2 y ago without pharmaceutical intervention], and women who are fertile) must test negative for pregnancy in a laboratory test administered by the site physician. Patients who have had or are currently receiving therapy or other drug based anti-amyloid regimens can be included on study (Parts 1 and 2). Patients must provide signed, written, informed consent and be willing to comply with eligibility requirements, scheduled visits, and follow-up studies. Due to annual dosimetry limitations, patients who have participated in another nuclear medicine amyloid imaging clinical trial protocol can be included in this study no earlier than 12 months after the previous radiotracer injection. In Part 2, inclusion of patients with amyloid subsets AL, ATTR, and ALect2 will continue until the trial has achieved recruitment goals for each subset: 30 AL; 20 ATTR; 5 ALect2; and 10 15 "Other". Prior to participation in Part 3 (n = 10 subjects) of the trial, the following inclusion criteria must be met: Patients must have a well-defined germline mutation of the transthyretin (TTR) gene rendering them at risk for amyloidosis, and be free of clinical evidence of SA. All patients in Part 3 will be >50 years of age. There are no gender or racial restrictions. Women of child bearing potential (those who have not been surgically sterilized, are not postmenopausal [typically understood to mean last menstrual period >2 y ago without pharmaceutical intervention], and women who are fertile) must test negative for pregnancy in a laboratory test administered by the site physician. Subjects must provide signed, written, informed consent and be willing to comply with eligibility requirements, scheduled visits, and follow-up studies. Due to annual dosimetry limitations, subjects who have participated in another nuclear medicine amyloid imaging clinical trial protocol can be included in this study no earlier than 12 months after the previous radiotracer injection. Prior to participation Part 4 of the trial (n = 5), the following inclusion criteria must be met: Healthy Control Subjects (HC) will be generally healthy adults, either male or female, and will not have a diagnosis of amyloidosis, will not have a first- or second-degree relative (parent, sibling, child, aunt, uncle, niece, nephew) with confirmed or suspected familial amyloidosis, and will not have diabetes mellitus (type 2). All Part 4 subjects will be > 30 years of age or older. Women of child bearing potential (those who have not been surgically sterilized, are not postmenopausal [typically understood to mean last menstrual period >2 y ago without pharmaceutical intervention], and women who are fertile) must test negative for pregnancy in a laboratory test administered by the site physician. Patients must provide signed, written, informed consent and be willing to comply with eligibility requirements, scheduled visits, and follow-up studies. Due to annual dosimetry limitations, patients who have participated in another nuclear medicine imaging clinical trial protocol can be included in this study no earlier than 12 months after the previous radiotracer injection. Prior to participation in Part 5 of the trial, the following inclusion criteria must be met: Patients must have successfully completed participation in Part 2 or Part 3 of this trial with CT/PET images confirming the presence of abnormal amyloid deposits in thoracoabdominal organs. Patients must have received a 2 mCi dose of 124I-p5+14 Injection during Part 2 or 3 of this trial with visual evidence of uptake of radiotracer in abdominothoracic organs associated with amyloid. The repeat exposure to the study agent must occur at least 6 months after the first exposure. Patients must submit a serum specimen for exploratory evaluation of the presence of anti-p5+14 peptide antibodies, with results reviewed by the Principal Investigator prior to a second exposure to the study agent. The patient must meet all of the Inclusion criteria for participation in Part 2 or Part 3 outlined in Sections 5.2 or Section 5.3 (as applicable), including the signing of an informed consent for Part 5. In addition, the following criteria will exclude candidates from participation in the trial, Parts 1 and 2: Those with significant co-morbidity (e.g., Eastern Cooperative Oncology Group [ECOG] score of 3 or greater), uncontrolled infection, or other serious illness. Patients with a sustained SpO2 of ≤ 92% as noted in the medical record. Patients that require renal dialysis. Women who are of child bearing potential (those who have not been surgically sterilized, are not postmenopausal [typically understood to mean last menstrual period >2 y ago without pharmaceutical intervention], and women who are fertile) who test positive for pregnancy in a laboratory test administered by the site physician, are pregnant, or are nursing Patients who have received any amyloidophilic radiotracer as part of a research clinical trial (not standard of care) within the past 12 months. Patients with exposure to heparin, or heparin-based medications, within 7 days prior to the imaging study. Patients who have a known allergy to acetaminophen or iOSAT iodine treatment. The following criteria will exclude candidates from participation in Part 3 of the trial: Those with significant co-morbidity (e.g., Eastern Cooperative Oncology Group [ECOG] score of 3 or greater), uncontrolled infection, or other serious illness. Subjects with a sustained SpO2 of ≤ 92% as noted in the medical record. Women who are of child bearing potential (those who have not been surgically sterilized, are not postmenopausal [typically understood to mean last menstrual period >2 y ago without pharmaceutical intervention], and women who are fertile) who test positive for pregnancy in a laboratory test administered by the site physician, are pregnant, or are nursing. Subjects who have clinical evidence of amyloidosis based on standard clinical criteria. Subjects with polyneuropathy of unknown origin. Subjects who have received any amyloidophilic radiotracer as part of a research clinical trial (not standard of care) within the past 12 months. Subjects with exposure to heparin, or heparin-based medications, within 7 days prior to the imaging study. Subjects who have a known allergy to acetaminophen or iOSAT iodine treatment. Subjects with clinical signs of SA based on routine investigation of serum and urine biomarkers, radiographic or nuclear imaging studies, or peripheral nerve evaluations. The following criteria will exclude subjects from participation in Part 4: Those with significant co-morbidity (e.g., Eastern Cooperative Oncology Group [ECOG] score of 2 (Restricted in physically strenuous activity but ambulatory and able to carry out work of a light or sedentary nature, e.g. light house work, office work) or greater), uncontrolled infection, or other serious illness. Individuals with a sustained SpO2 of ≤ 92% as noted in the medical record. Women who are of child bearing potential (those who have not been surgically sterilized, are not postmenopausal [typically understood to mean last menstrual period >2 y ago without pharmaceutical intervention], and women who are fertile) who test positive for pregnancy in a laboratory test administered by the site physician, are pregnant, or are nursing. Subjects who have received any amyloidophilic radiotracer as part of a research clinical trial (not standard of care) within the past 12 months. Subjects with exposure to heparin, or heparin-based medications, within 30 days prior to the imaging study. Subjects who have a known allergy to acetaminophen or iOSAT iodine treatment. Subjects with a diagnosis of Type 2 diabetes mellitus or who are taking medication for management of Type 2 diabetes mellitus. Active infection requiring systemic antiviral or antimicrobial therapy that will not be completed prior to Study Day 1. Known history of or positive test for human immunodeficiency virus (HIV), hepatitis C or chronic hepatitis. Uncontrolled hypertension (BP > 160/100 mm Hg). Smokes >20 cigarettes a day. A diagnosis of heart failure with preserved ejection fraction. Has any other conditions, which, in the opinion of the Investigator would make the subject unsuitable for inclusion, or could interfere with the subject participating in or completing the study The following criteria will exclude subjects from participation in Part 5. Any patient who experienced a clinically significant adverse event related to prior exposure to the study agent. Any subject who meets any of the Exclusion Criteria for Part 2 or Part 3 (as applicable), described in Section 5.3.1 and Section 5.3.2.
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Jonathan Wall, Ph.D.
Organizational Affiliation
UTHSC Graduate School of Medicine
Official's Role
Principal Investigator
Facility Information:
Facility Name
University of Tennessee Medical Center
City
Knoxville
State/Province
Tennessee
ZIP/Postal Code
37920
Country
United States

12. IPD Sharing Statement

Plan to Share IPD
Undecided
Citations:
PubMed Identifier
34786667
Citation
Wall JS, Martin EB, Endsley A, Stuckey AC, Williams AD, Powell D, Whittle B, Hall S, Lambeth TR, Julian RR, Stabin M, Lands RH, Kennel SJ. First in Human Evaluation and Dosimetry Calculations for Peptide 124I-p5+14-a Novel Radiotracer for the Detection of Systemic Amyloidosis Using PET/CT Imaging. Mol Imaging Biol. 2022 Jun;24(3):479-488. doi: 10.1007/s11307-021-01681-2. Epub 2021 Nov 16.
Results Reference
derived

Learn more about this trial

124I-p5+14 Injection Safety in Subjects With Systemic Amyloidosis

We'll reach out to this number within 24 hrs