SUBSCI II: Cord Blood Cells in Patients With Acute SCI

Sponsor

Sklifosovsky Institute of Emergency Care (Other)

Overall Status

Recruiting

CT.gov ID

NCT05693181

Collaborator

State-Financed Health Facility "Samara Regional Medical Center Dinasty" (Other), K.L. Hetagurov North-Osetian State University (Other)

Enrollment

Location

Arms

32.8

Anticipated Duration (Months)

2.4

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

This is a prospective, single-blinded, single-center, randomized, comparative, interventional clinical study of systemic mononuclear multiple allogenic cord blood cells administration safety and efficiency in patients having acute severe contusion spinal cord injury (ASIA A/B), phase I/II

Condition or Disease	Intervention/Treatment	Phase
Spinal Cord Injury, Acute	Biological: Multiple systemic (i.v.) administration of allogenic non-related group- and rhesus-compatible mononuclear cord blood cells Other: Control vehicle (sterile saline)	Phase 1/Phase 2

Detailed Description

Phase I/II of the SUBSCI II (Systemic Umbilical Cord Blood Administration in Patients with Acute Severe Contusion Spinal Cord Injury II) study is focused on safety and primary efficacy of multiple systemic infusions of allogeneic unrelated human umbilical cord blood mononuclear cells in patients with severe acute spinal cord contusion having severe neurologic deficit (ASIA A/B).

In a previous clinical study (SUBSCI I/IIa) complete safety and significant efficiency of systemic administration of human umbilical cord blood cells (HUCBCs) was demonstrated. Current study is established to confirm and verify the obtained results in a larger group of patients.

SUBSCI II study includes 80 patients with acute severe contusion spinal cord injury (SCI) and American Spinal Injury Association (ASIA) level A/B deficit divided into 2 groups (experimental and control groups, 40 patients in each). Patients will be treated with 4 infusions of group-matched and rhesus-matched cord blood samples following primary decompressive and stabilizing surgery within 7 days after SCI. All patients will be followed up for 12 months after SCI.

Study Design

Study Type:

Interventional

Anticipated Enrollment :

80 participants

Allocation:

Randomized

Intervention Model:

Parallel Assignment

Masking:

Single (Participant)

Masking Description:

Participants in the experimental group will obtain 4 systemic (i.v.) infusions of allogenic group- and rhesus-compatible non-related mononuclear cord blood cell samples (500 +/- 50 x 10'6 cells each). Participants in the control group will obtain the similar volume of vehicle (sterile saline). Participant's devision will be performed in a randomized manner. Randomization will be performed using standard randomization computer table. All participants will be blinded concerning the therapy mode.

Primary Purpose:

Treatment

Official Title:

Systemic Administration of Allogenic Mononuclear Cord Blood Cells in Patients With Acute Severe Contusion Spinal Cord Injury: Safety and Efficiency Evaluation, Stages I/II

Actual Study Start Date :

Dec 5, 2022

Anticipated Primary Completion Date :

Dec 31, 2024

Anticipated Study Completion Date :

Aug 30, 2025

Arms and Interventions

Arm	Intervention/Treatment
Experimental: Cell Therapy Patients having acute severe contusion spinal cord injury (cervical, thoracic or upper-lumbar) and ASIA A/B neurological deficit, within 7 days post-SCI, after primary decompressive and stabilizing surgery. All participants meet inclusion and exclusion criteria. All participants obtain 4 infusions of allogenic non-related group- and rhesus-compatible mononuclear cord blood cells samples (500 +/- 50 x 10*6 cells each) with a 1-week interval. All participants are followed up for 12 months post-SCI.	Biological: Multiple systemic (i.v.) administration of allogenic non-related group- and rhesus-compatible mononuclear cord blood cells Each HUCBCs sample contain 500 +/- 50 x 10*6 allogenic non-related group- and rhesus-compatible mononuclear cord blood cells
Placebo Comparator: Vehicle Patients having acute severe contusion spinal cord injury (cervical, thoracic or upper-lumbar) and ASIA A/B neurological deficit, within 7 days post-SCI, after primary decompressive and stabilizing surgery. All participants meet inclusion and exclusion criteria. All participants obtain 4 infusions of vehicle (sterile saline) with a 1-week interval. All participants are followed up for 12 months post-SCI.	Other: Control vehicle (sterile saline) Sterile saline infusion in control patients

Arm

Intervention/Treatment

Experimental: Cell Therapy

Patients having acute severe contusion spinal cord injury (cervical, thoracic or upper-lumbar) and ASIA A/B neurological deficit, within 7 days post-SCI, after primary decompressive and stabilizing surgery. All participants meet inclusion and exclusion criteria. All participants obtain 4 infusions of allogenic non-related group- and rhesus-compatible mononuclear cord blood cells samples (500 +/- 50 x 10*6 cells each) with a 1-week interval. All participants are followed up for 12 months post-SCI.

Biological: Multiple systemic (i.v.) administration of allogenic non-related group- and rhesus-compatible mononuclear cord blood cells

Each HUCBCs sample contain 500 +/- 50 x 10*6 allogenic non-related group- and rhesus-compatible mononuclear cord blood cells

Placebo Comparator: Vehicle

Patients having acute severe contusion spinal cord injury (cervical, thoracic or upper-lumbar) and ASIA A/B neurological deficit, within 7 days post-SCI, after primary decompressive and stabilizing surgery. All participants meet inclusion and exclusion criteria. All participants obtain 4 infusions of vehicle (sterile saline) with a 1-week interval. All participants are followed up for 12 months post-SCI.

Other: Control vehicle (sterile saline)

Sterile saline infusion in control patients

Outcome Measures

Primary Outcome Measures

Adverse events [Continuously for 12 months post-SCI]
All adverse events (AEs) are registered within follow-up period. All registered AEs are classified using CTCAE classification and relation to the performed therapy.
Motor function [Change from Baseline 12 months post-SCI]
Evaluation of motor function dynamics in upper (UEMS), lower (LEMS) and all (GEMS) limbs
Neurological deficit [Change from Baseline 12 months post-SCI]
Evaluation of general neurological deficit dynamics using ASIA scale

Secondary Outcome Measures

Sensory function [Change from Baseline 12 months post-SCI]
Evaluation of pain, tactile, temperature and proprioceptive sensory function dynamics below SCI level and comparison between two groups
Neuropathic pain syndrome [12 months post-SCI]
Evaluation of neuropathic pain syndrome dynamics and comparison between two groups
Independent verticalization and motion ability [Change from Baseline 12 months post-SCI]
Evaluation of Independent verticalization and motion ability dynamics and comparison between two groups
Limb muscle spasticity [Change from Baseline 12 months post-SCI]
Evaluation of limb muscle spasticity level dynamics using modified Ashworth or Tardieu scales and comparison between two groups
Psychological status [Change from Baseline 12 months post-SCI]
Evaluation of psychological status dynamics using Beck depression and anxiety scales and comparison between two groups
Pelvic functions [Change from Baseline 12 months post-SCI]
Evaluation of pelvic functions dynamics (bladder fulfillment feeling, independent urination ability, urodynamic examination)
Life quality [Change from Baseline 12 months post-SCI]
Evaluation of life quality level in two groups using FIM (Functional Independence Measurement) scale and SF36 questionnaire
Electrophysiology parameters [12 months post-SCI]
Assessment of electrophysiology objective parameters (electroneuromyography parameters with transcranial magnetic stimulation - full block, partial block or no block; somatosensory evoked potentials, motor evoked potentials)
Cell immunization [12 months post-SCI]
Assessment of patient's immunization to infused cell samples

Eligibility Criteria

Criteria

Ages Eligible for Study:

18 Years to 75 Years

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

Inclusion Criteria:

Both males and females, 18 to 75 years old
Contusion spinal cord injury (SCI) at cervical, thoracic or upper lumbar (cone level) levels
admission by 7 days post-SCI
spinal cord contusion confirmed using MRI (T1- and T2-weighted images, STIR)
ASIA A/B neurological deficit
identical level of neurological deficit at admission and at the moment of patient inclusion
primary decompressive and stabilizing surgery performed within 5 days post-SCI and prior to the first cell sample infused
patient is ready to participate and fulfill the requirements of the study protocol
informed consent signed by the patient or his legal representative

Exclusion Criteria:

motor function preserved in lower limbs at admission (LEMS > 0 points) corresponding to ASIA C, D or E deficit level
any spinal cord injury different from contusion (tear, defibering, concussion, SCIWORA, SCIWONA) confirmed using MRI
severe combined trauma (ISS > 35 points)
inability to perform primary decompressive and stabilizing surgery within 5 days post-SCI and prior to the first cell sample infused
persistent systolic arterial pressure (AP) > 185 mmHg or diastolic AP > 105 mmHg or need of aggressive AP lowering using systemic antihypertensive medication at the moment of patient inclusion
acute myocardial infarction
blood glucose level < 3.5 Mmol/L or >21 Mmol/L or ineffective antidiabetic therapy for 24 hours
acute or deterioration of chronic diseases of central nervous system (CNS) (e.g. stroke, non-traumatic subarachnoid hemorrhages and others at the discretion of investigator)
hypotension or cardiovascular shock AND systolic AP < 90 mmHg OR need for intensive systemic inotropic therapy at the moment of patient inclusion
objective need for artificial ling ventilation (ALV) at admission or prior to the stage I surgery
acute kidney failure or deterioration of chronic kidney failure (creatinin level > 250 mumol/L or carbamide level > 25 Mmol/L)
liver failure (general bilirubin level > 25 mumol/L, alanine aminotransferase (ALT) and aspartate aminotransferase (AST) levels > 4 times exceeding upper reference limit)
other significant disorders of vital functions
acute of deterioration of chronic diseases of internal organs preventing from cell samples infusion
autoimmune diseases (active or anamnestic) preventing from cell samples infusion
allergic reactions of any type for any component of HUCBC samples
pregnancy or lactation
significant surgeries or severe traumas within 3 months prior to patient inclusion
acute or chronic infection diseases (tuberculosis, lues, HIV, hepatitis B, hepatitis C etc.)
moderate or severe hematological and/or oncohematological diseases preventing from the cell samples infusion
any malignant tumors (both operated and not operated) or benign tumors (not operated or not totally removed) at the moment of patient inclusion
neurological and/or psychiatric diseases preventing patient from complete understanding of study protocol or fulfillment of the study protocol requirements
other reasons preventing patient from complete understanding of study protocol or fulfillment of the study protocol requirements
patient's participation in any other clinical trials or studies within 6 months prior to inclusion
immunosuppressive therapy obtained by the patient for any reason at admission
allergic reaction for full blood or blood component transfusion in the past
need for extracorporal detoxication methods application (hemodialysis, plasmapheresis, sorption etc.)
bone marrow or internal organs (both donor and relative) transplantation in the past
patient's participation in any studies applying regenerative technologies (grow factors, cytokines, cell therapy, gene therapy etc.) within 1 year prior to inclusion
patient's rejection to sign the informed consent
any other reasons preventing patient's inclusion according to the investigator's opinion