INTERCEPT Safety Evaluation in Anemic Patients

Not Applicable

Withdrawn

• Conditions: Anemia
• Interventions: Device: INTERCEPT; Device: Standard of Care

• Registration Number: NCT03486054
• Lead Sponsor: Swiss Transfusion SRC

Brief Summary

The pathogen reduction (PR) system for Whole Blood (WB) using Amustaline (S-303) and Glutathione (GSH) has a potential to decrease transfusion-transmitted infection. There is scientific basis to hypothesize, that cells containing DNA and RNA such as bacteria, viruses and parasites that could be present in blood collected from asymptomatic infected donors are inactivated in the treated whole blood and therefore reduce the risk of transfusion-transmitted infections. The aim of the study is to gather data to support the safety of whole blood products that underwent treatment with amustaline and glutathione and data to support a larger sufficiently powered efficacy study. This study will evaluate the safety of the system for whole blood in adult patients with anemia.

This study is designed as a randomized, controlled, open-label study. The aim is to explore the safety of the whole blood product treated with a PR system using amustaline and glutathione.

The study will enroll 20 patients with anemia. 20 patients will be randomized either to treated WB (Test) or Standard of Care, either Red Blood Cells or Whole Blood (Control).

Detailed Description

Screening:

All potentially eligible patients at the participating institution will be approached for study consent prior to study transfusion. Enrolled patients will be asked for consent to the storage of their samples for a future project in TTI Project. Illiterate patients can be consented by an impartial witness.

Patients who consent to the study will be assigned a study ID number and undergo screening.

Screening data collection and procedures will include: Demographics (age, sex), vital signs, height, weight, indication for anticipated transfusion, medical history including history of bleeding and transfusion and concomitant medications. A physical examination, including skin inspection, will be performed. Blood samples will be drawn for a hematological panel (including complete blood count, blood chemistry, blood type, coagulation (aPTT, PT and/or INR) and pregnancy test (if applicable). Immunohematology tests will be performed in a patient's sample at the blood transfusion center. This includes the Direct Antibody Test (DAT), immune reactivity to RBCs that have been processed with the INTERCEPT Blood System (IBS RBC), red cell alloantibody screen (Indirect Antibody Test (IAT) / Indirect Coombs).

Blood samples (pre/post-treatment) for future research on transfusion-transmitted infections will be archived in a biobank of the Institut Pasteur de Côte d'Ivoire (IPCI)

Randomization:

After successful screening, eligible patients will be assigned to a treatment arm by randomization. Randomization will be performed in the blood center by sequentially selecting a randomization envelope starting with the lowest number (e.g., 1 for the first eligible subject in ascending order up to envelope number 20 for the 20th subject).

The ratio of patients assigned to the Test and Control group will be 1:1. Each subject will receive a Test product or SOC. The assigned blood product number must be noted on the randomization assignment envelope and on the release form. The product number will also be entered into the case report form (CRF).

The replacement strategy in this Phase I clinical trial is based on the aim to reach twenty evaluable patients ("evaluable patients" is defined as those patients who are randomized and receive any study transfusion).

If a randomized subject withdraws or is withdrawn from the study prior to the administration of any study transfusion, or does not receive any study transfusion through 7-days post-randomization, this subject will be replaced by the next eligible subject using the same randomization envelope. If a randomized subject receives a conventional (untreated) blood transfusion prior to study transfusion, the patient will be replaced as described above.

All patients who received at least one study product will be included into the analysis of evaluable patients and followed up to the final study visit on Day 58.

All used and unused randomization envelopes will be kept in the Site File for reconciliation.

Pre-transfusion visit:

Vital signs, height, weight, hemoglobin will be assessed and urine dipstick test for detection of blood will be performed. If the patient consented to future research on TTI, a sample is drawn.

Treatment:

Patients will be transfused with one investigational product or SOC on Day 1. In case he or she requires further transfusion support to treat anemia, enrolled patients may be treated with a second study transfusion. A patient who requires a second blood component will receive a second treatment with a study product from the assigned treatment arm. This patient will be included into the analysis of evaluable patients and followed up to Day 58, the end of study visit.

Post-transfusion visit(s):

Patients will be hospitalized for 24 hours after each study transfusion to allow close monitoring and data collection uniquely for the study purpose since their condition would allow an outpatient treatment. 3 hours and 6 hours after initiating each study transfusion vital signs, skin inspection, and urine dipstick will be performed.

24-hours post-transfusion vital signs, concomitant medication/intervention will be assessed, laboratory samples for hemoglobin, coagulation assays (aPTT, PT and/or INR) and potassium and a sample for determination of residual S-300 will be taken.

If a subject consented to future research on TTI, a second blood sample (post-transfusion) will be taken and archived in the biobank.

In case clinical symptoms of transfusion-related bacterial contamination occur, a blood sample will be taken during the post-transfusion period and sent for microbiological analysis. Those patients will be treated according to local SOC.

Safety Follow-up visit Day 28 (+/-3 days after last study transfusion):

At day 28 (+/-3 days) a physical examination, vitals and blood samples will be collected for laboratory analysis of safety variables (e.g., complete blood count, coagulation, blood chemistry) and urine dipstick.

All Adverse Events (AE), Transfusion Reactions (TR) and unanticipated adverse device effects will be reviewed and recorded for the period from the first study transfusion through day 28 after the last study transfusion.

The Investigators will assess each AE/TR for relation to the study transfusion. Available clinical diagnostic tools will be used to classify occurring transfusion reactions by the definitions of Swissmedic grading scale.

Final study visit Day 58 (+/-7 days after last study transfusion) At the final study visit, the immune reactivity of patient serum to RBCs treated with amustaline/GSH and a DAT test will be performed.

SAEs will be reviewed and recorded for the period of 58 days up to the final study visit.

The Investigators will assess each Serious Adverse Event (SAE) for relation to the study transfusion. Depending on the availability of clinical diagnostic tools, the transfusion reactions will be classified by the definitions of Swissmedic grading scale.

Study Timeline

• Study First Submitted: 2018-03-06
• Study First Submitted QC: 2018-03-26
• Study First Posted: 2018-04-03
• Study Start: 2019-06
• Status Verified: 2019-12
• Last Update Submitted: 2019-12-12
• Last Update Posted: 2019-12-13
• Primary Completion: 2020-03
• Study Completion: 2020-06

Recruitment & Eligibility

• Status: WITHDRAWN
• Sex: All
• Target Recruitment: Not specified

Inclusion Criteria

Not provided

Exclusion Criteria

Not provided

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Experimental Arm A	INTERCEPT	Whole blood treated with amustaline and glutathione, a pathogen reduction technology (PRT), ordered and administered to study patients by their treating physicians
Control Arm B	Standard of Care	Standard of Care (either red blood cells or whole blood)

Primary Outcome Measures

Name	Time	Method
Severe Transfusion Reactions	24 hours	The primary safety outcome will be assessed by the occurrence of transfusion reactions \>= grade 2 according to the Swissmedic transfusion reaction grading and causality criteria (Appendix 1), during the first 24 hours following administration of each study transfusion, with probable, possible or certain causality to the transfused product

Secondary Outcome Measures

Name	Time	Method
Treatment-emergent antibodies	58 (+/-7)	Treatment-induced antibodies to amustaline/GSH treated RBCs within 58 (+/-7) days after last study transfusion
Adverse events	58 (+/-7)	All adverse events including all transfusion reactions within 28 (+/-3) days and all SAEs within 58 (+/- 7) days after last study transfusion.
Treatment-emergent auto-antibodies	58 (+/-7)	Treatment emergent auto-antibody within 58 (+/-7) days after study transfusion
Hemoglobin increment	24 hours	The hemoglobin increment 24h post transfusion will be calculated as the difference between the hemoglobin value most proximate before the transfusion and approximately 24h post transfusion, adjusted by hemoglobin content transfused.