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Clinical Trial Details — Status: Enrolling by invitation

Administrative data

NCT number NCT05629338
Other study ID # IDE 27346
Secondary ID
Status Enrolling by invitation
Phase Phase 1
First received
Last updated
Start date December 1, 2022
Est. completion date May 15, 2024

Study information

Verified date April 2024
Source Velico Medical
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This study in healthy volunteers is designed to assess the safety of infusing increasing doses of spray dried plasma (FrontlineODP).


Description:

This study in healthy volunteers is designed to assess the safety of infusing increasing doses of spray dried plasma (FrontlineODP). Volunteers will have their plasma collected, spray dried, and then rehydrated for infusion. Volunteers will be infused with their own (autologous) rehydrated plasma. Cohort 1 will receive 1 FrontlineODP unit that is rehydrated to approximately 200 mL. Cohort 2 will receive 2 FrontlineODP units of approximately 400 mL. Cohort 3 volunteers will receive 2 separate infusions of 4 units of approximately 800 mL of either FrontlineODP (experimental) or frozen plasma (PF24). Order of receipt of plasma product will be randomized with 14 days between infusion.


Recruitment information / eligibility

Status Enrolling by invitation
Enrollment 24
Est. completion date May 15, 2024
Est. primary completion date May 15, 2024
Accepts healthy volunteers Accepts Healthy Volunteers
Gender All
Age group 18 Years to 65 Years
Eligibility Inclusion Criteria: - Males and nonpregnant/nonbreastfeeding females - For females, a minimum weight of 140 pounds and maximum weight of 220 pounds; for males, a minimum weight of 140 pounds and a maximum weight of 250 pounds - Subject is 18 to 65 years of age, inclusive - Subject self-reports that he or she feels well and healthy - Subject scores =35 on the Duke Activity Status Index - Subject is able to donate a unit of plasma by plasmapheresis based on the AABB Donor History Questionnaire with modifications indicated: subjects with history of travel, which puts them at risk for Creutzfeldt-Jakob Disease or malaria, are eligible to participate - Subject has completed a vaccination course for severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), with the final vaccine injection administered at least 2 weeks before enrollment - Subject has read the educational materials on donating blood and has had his or her questions answered - Subject is able and willing to provide written informed consent - Females of childbearing potential should either be surgically sterile (hysterectomy or tubal ligation) or should use a highly effective medically accepted contraceptive regimen. Highly effective methods of birth control are defined as those which result in a low failure rate (ie, less than 1% per year) when used consistently and correctly such as implants, injectables, combined oral contraceptives, some intrauterine devices, sexual abstinence, condoms with spermicide, or vasectomized partner - All females must have a negative urine or serum pregnancy test - Subject understands the English language Exclusion Criteria: - Subject has known liver, kidney, cardiovascular, neurologic, gastrointestinal, blood, endocrine/metabolic, autoimmune, or pulmonary disease, or treated or untreated hypertension - Subject has cancer of any kind, under treatment or resolved - Subject has known or past coagulopathy conditions - Subject has any conditions, uses medications, etc. on the AABB medical deferral list - Subject has a history of asthma (defined as use of a prescribed daily asthma controller medication or required asthma medication in the past 2 weeks) - Subject has a previous diagnosis of stroke, deep vein thrombosis (DVT), venous or arterial thrombosis, blood clots, or transient ischemic attack - Subject has a family history of venous or arterial thrombosis before the age of 50 years in first degree relatives (ie, biological parents, full siblings, or children) - Subject has a D-dimer test result =0.5 FEU/mL - Subject has a recent (within 1 year of Screening) history of an abnormal electrocardiogram of clinical significance as determined by the site PI - Subject has known HIV or AIDS-related illness or received a positive test result for HIV infection - Subject has a positive test result for HBV, hepatitis C virus (HCV), or human T-cell lymphotropic virus - Subject has a history of significant treated or untreated mental health issues - Subject is currently taking an antibiotic or another medication for an infection - Subject has received aspirin or other platelet-inhibiting agents within 14 days of study donation and infusion visits. Prior and concomitant medication information will be recorded beginning 30 days before enrollment through the final follow-up visit - Subject is currently using any medications for anticoagulant therapy - Subject has used clotting factor concentrates(s) (eg, FVIIa) - Subject has received blood or blood products within the past 12 months - Subject has had concurrent headache and fever in the past week - Subject has systolic blood pressure (current) greater than 140 mm Hg - Subject has diastolic blood pressure (current) greater than 90 mm Hg - Subject has an oral temperature greater than 100°F - Subject has known hematocrit =39% for male donors and =38% for female donors - Subject has a positive DAT result - Subject has received any investigational agent within 1 month before treatment infusion for this study - Subject is participating in any phase of any other investigational studies while participating in this study - Subject is unwilling or unable to comply with the requirements of this protocol, including the presence of any condition (physical, mental, or social) that is likely to affect the subject's return for follow-up visits as scheduled - Subject has other unspecified reasons that, in the opinion of the site PI, make the subject unsuitable for enrollment - Subject is institutionalized because of legal or regulatory order - Subject has a positive urine drug screen

Study Design


Related Conditions & MeSH terms


Intervention

Combination Product:
Autologous Spray Dried Plasma
Evaluation of the Safety of Ascending Doses of Autologous Spray Dried Plasma in Healthy Volunteers

Locations

Country Name City State
United States Hoxworth Blood Center Cincinnati Ohio
United States Versiti Blood Center of Wisconsin Milwaukee Wisconsin
United States Spaulding Clinical Research LLC West Bend Wisconsin

Sponsors (1)

Lead Sponsor Collaborator
Velico Medical

Country where clinical trial is conducted

United States, 

Outcome

Type Measure Description Time frame Safety issue
Primary Occurrence of Treatment-Emergent Adverse Events (TEAEs) Conclusions about safety will be based on the occurrence of TEAEs in Cohort 1 (1 unit of FrontlineODP, 200 mL) and Cohort 2 (2 units of FrontlineODP, 400 mL). Start of plasma infusion through 28 day follow up (Day 29).
Primary Occurrence of Treatment-Emergent Adverse Events (TEAEs) Conclusions about safety will be based on the occurrence of TEAEs in Cohort 3 with infusions of 4 units (800 mL) of FrontlineODP compared to 4 units (800 mL) of PF24. Start of first plasma infusion through 28 day follow up of the second infusion (Day 43).
Secondary Changes in PT changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in INR changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in aPTT changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in Factor I changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in Factor II changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in Factor V changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in Factor VII changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in Factor VIII changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in Factor IX changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in Factor X changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in Factor XI changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in D-dimer changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in von Willebrand Ristocetin Cofactor (vWF:RCo) activity changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in von Willebrand (vWF) antigen changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in protein S changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
Secondary Changes in protein C changes between pre-infusion baseline and 4 hours post-infusion values after infusion of 4 units of FrontlineODP compared with infusion of the same dose of PF24. Start of first plasma infusion through 28-day follow up of second infusion (Day 43).
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