Placebo-controlled Study to Evaluate Rexlemestrocel-L Alone or Combined With Hyaluronic Acid in Participants With Chronic Low Back Pain

Phase 3

Completed

Conditions: Degenerative Disc Disease

Interventions: Drug: Rexlemestrocel-L + HA Mixture
Drug: Placebo
Drug: Rexlemestrocel-L

Registration Number: NCT02412735

Lead Sponsor: Mesoblast, Ltd.

Brief Summary: This is a prospective, multicenter, randomized, double-blind, placebo-controlled Phase 3 study designed to evaluate the safety and efficacy of Mesoblast's rexlemestrocel-L alone or combined with hyaluronic acid (HA) in participants with chronic low back pain (\> 6 months) associated with moderate radiographic degenerative changes of a disc.

Detailed Description: Not available

Recruitment & Eligibility

Status: COMPLETED

Sex: All

Target Recruitment: 404

Inclusion Criteria

Male and female participants 18 years of age and older
If female of childbearing potential, participant is non-pregnant, non-nursing, and agrees to use highly effective methods of contraception for a minimum of 24 months post-treatment
Signed informed consent and country-appropriate privacy forms indicating participant is willing to undergo treatment and willing to be available for each examination scheduled over the study duration
Have documented diagnosis of moderate radiographic degeneration of an intervertebral disc from L1 to S1, with a disc suspected of causing chronic low back pain (CLBP) associated with moderate radiographic degeneration at a lumbar disc is defined as the following (participant must meet all of the listed conditions):
1. Chronic low back pain for at least 6 months
2. Have failed 6 months of conservative back pain care. (Conservative treatment regimens may include any or all of the following: initial rest, medications [e.g., anti-inflammatory, analgesics, narcotics/opioids, muscle relaxants], massage, acupuncture, chiropractic manipulations, activity modification, home-directed lumbar exercise program, and non-invasive pain control treatments or procedures)
3. Have at a minimum undergone supervised physical therapy, such as daily walking routines, therapeutic exercises, and back education programs specifically for the treatment of low back pain and taken a pain medication for back pain (e.g. non-steroidal anti-inflammatory drug (NSAID) and/or opioid medication).
4. Change from normal disc morphology of the index disc as defined by radiographic evaluation by the core imaging evaluation provider. Radiographs must show all of the following:
A modified Pfirrmann score of 3, 4, 5 or 6 on magnetic resonance imaging (MRI) at the index disc
Modic Grade II changes or less on MRI at the index disc
With or without contained disc protrusion at the index disc on MRI

e. Low back pain of at least 40mm and not more than 90mm of 100mm on low back pain visual analogue scale (VAS) (average pain over 24 hours)

f. Leg pain ≤20mm in both legs on a 100mm VAS scale

g. Oswestry disability index (ODI) score of at least 30 and no more than 90 on a 100 point scale.

Exclusion Criteria

Female participants who are pregnant or nursing, or women planning to become pregnant in the first 24 months post-treatment
Extreme obesity, as defined by National Institutes of Health (NIH) Clinical Guidelines Body Mass Index (BMI > 40)
Have undergone a surgical procedure (e.g. discectomy, intradiscal electrothermal therapy, intradiscal radiofrequency, artificial disc replacement, interbody fusion) on the disc at the index or adjacent level
Osteoporosis, as defined by dual-energy X-ray absorptiometry (DEXA) scan. A DEXA T-score of ≤ -2.5 will exclude the participant.
Any lumbar intradiscal injection, including steroids, into the index or adjacent discs prior to treatment injection, with the exception of the following injections performed at least 2 weeks prior to study treatment:
1. Contrast medium (discography or other diagnostic injection)
2. NSAIDs
3. Nerve-blocking anesthetics (e.g., lidocaine, bupivacaine)
4. Antibiotics
5. Saline
Have undergone a procedure affecting the structure/biomechanics of the index disc level (e.g., posterolateral fusion)
Active malignancy or tumor as source of symptoms or history of malignancy within the 5 years prior to enrolment on study
Have been a recipient of prior allogeneic stem cell/progenitor cell therapy for any indication or autologous stem cell/progenitor cell therapy or other biological intervention to repair the index intervertebral disc
An average baseline morphine equivalent dose (MED) of >75mg/day as determined by e-diary entries during the screening period
Taking systemic immunosuppressants
A medical condition, serious intercurrent illness, or extenuating circumstance that would preclude participation in the study or potentially decrease survival or interfere with ambulation or rehabilitation.
Participants involved in spinal litigation, including workman's compensation, unless litigation is complete
Are transient or has a severe alcohol or substance abuse problem
Clinically significant nerve pain (e.g., chronic radiculopathy or neuropathy)
Clinically significant sacroiliac joint pain
Compressive pathology due to stenosis or disc protrusion on MRI with associated clinical symptoms defined as leg pain VAS>20mm out of 100mm or neurologic deficit on neurologic exam
Disc extrusion with a maximum dimension greater or equal to twice the posterior height of the disc, or disc sequestration in the lumbar spine on MRI as determined by radiographic core lab
Modified Pfirrmann score of 7 or 8 at any lumbar level (L1-S1) on MRI evaluation as determined by radiographic core lab
Symptomatic involvement of more than one lumbar disc
Symptomatic central vertebral canal stenosis as defined by neurogenic claudication
Spondylolisthesis or retrolisthesis Grade 2 and above or Spondylolysis at the index or adjacent level(s)
Lumbar spondylitis or other undifferentiated spondyloarthropathy affecting the index disc
Spinal deformity defined as lumbar scoliosis with a Cobb angle of the lumbar spine greater than 15 degrees
Any fracture of the spine at the index or adjacent levels that has not healed, or clinically compromised vertebral bodies at the index level due to current or past trauma
Facet pain at the index level or adjacent segments as determined by a diagnostic medial branch block (a facet block injection is not acceptable for making this determination) to rule out facet joint involvement.
Full thickness annular tears in the index level as determined by free flowing contrast media through the annulus fibrosis.

Study & Design

Study Type: INTERVENTIONAL

Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Rexlemestrocel-L + HA	Rexlemestrocel-L + HA Mixture	Participants received rexlemestrocel-L 2.0 mL injection of approximately 6 million rexlemestrocel-L cells in freeze media mixed in a 1:1 by-volume ratio with hyaluronic acid (HA) solution on Day 0 (Visit 2).
Placebo	Placebo	Participants received saline solution as matching-placebo on Day 0 (Visit 2).
Rexlemestrocel-L	Rexlemestrocel-L	Participants received rexlemestrocel-L 2.0 mL injection of approximately 6 million rexlemestrocel-L cells in freeze media mixed in a 1:1 by-volume ratio with saline on Day 0 (Visit 2).

Primary Outcome Measures

Name	Time	Method
Overall Treatment Success: Bayesian Estimated Response Rate	Up to 24 months	Overall treatment success was determined based on number of responders who had composite response at both months 12 and 24 evaluated per specified criteria. A treatment responder with treatment success was defined as a participant who met the 3 criteria of a composite responder analysis as: 50% or greater reduction in the lower-back pain visual analogue scale (VAS) score; 15-point or greater reduction in the Oswestry Disability Index (ODI) score; and lack of post-treatment interventions at the treated level as of the study visit (Visits 6 \[12 months post-treatment\] and 8 \[24 months post-treatment\]). The average response rate (proportion of participants with response presented as Bayesian estimate\[BE\]) was based upon the average of multiple Bayesian simulations.

Secondary Outcome Measures

Name	Time	Method
Effectiveness Based on Functional Responders: Bayesian Estimated Response Rate	Up to 24 months	A participant was defined as a functional responder for a given study visit if they achieved at least a 15-point reduction from Baseline in ODI score, as reported during in-clinic assessment. The participant should be qualified as a functional responder at both 12 and 24 months post-treatment, and must not have received a post-treatment intervention through 24 months' follow-up; any participant that did not have a minimum of a visit at 3 months (Study Visit 4) was considered a non-responder for this outcome measure. The average response rate (proportion of participants with response presented as BE) was based upon the average of multiple Bayesian simulations.
Effectiveness Based on Treatment Success at 24 Months: Bayesian Estimated Response Rate	Month 24	A treatment responder with treatment success was defined as a participant who met the 3 conditions of a composite responder analysis as: 50% or greater reduction in the lower-back pain VAS score; 15-point or greater reduction in ODI score; and lack of post-treatment interventions at the treated level as of the study visit. The participants qualified as responders if they satisfied the above conditions at the 24-month follow-up visit alone. Any participant that did not have a minimum of a visit at 3 months (Study Visit 4) was considered a non-responder for this outcome measure. The average response rate (proportion of participants with response presented as BE) was based upon the average of multiple Bayesian simulations.
Effectiveness Based on Minimal Pain Responders at 24 Months: Bayesian Estimated Response Rate	Month 24	A minimal pain responder was defined as a participant who achieved a lower-back pain VAS score (average pain over 24 hours) of 20 mm or less at the given study visit. The participants qualified as responders if they satisfied the above condition at 24 months post-treatment, and did not receive a post-treatment intervention through 24 months' follow-up. Any participant that did not have a minimum of a visit at 3 months (Study Visit 4) was considered a non-responder for this outcome measure. The average response rate (proportion of participants with response presented as BE) was based upon the average of multiple Bayesian simulations.
Effectiveness Based on Pain Responders: Bayesian Estimated Response Rate	Up to 24 months	A participant was defined as a pain responder for a given study visit if they achieved at least a 50% reduction from Baseline in the lower-back pain VAS score (average pain over 24 hours), as reported during in-clinic assessment. The participant should be qualified as a pain responder at both 12 and 24 months post-treatment, and must not have received a post-treatment intervention through 24 months' follow-up. Any participant that did not have a minimum of a visit at 3 months (Study Visit 4) was considered a non-responder for this outcome measure. The average response rate (proportion of participants with response presented as BE) was based upon the average of multiple Bayesian simulations.
Effectiveness Based on Minimal Disability Responders at 24 Months: Bayesian Estimated Response Rate	Month 24	A minimal disability responder was defined as a participant who achieved an ODI score of 20% or less at the given study visit. The participants qualified as responders if they satisfied the above condition at 24 months post-treatment, and did not receive a post-treatment intervention through 24 months' follow-up. Any participant that did not have a minimum of a visit at 3 months (Study Visit 4) was considered a non-responder for this outcome measure. The average response rate (proportion of participants with response presented as BE) was based upon the average of multiple Bayesian simulations.
Effectiveness Based on Time to First Intervention Over 24 Months	Up to Month 24	The effectiveness of the study drug was evaluated based on its ability in increasing the time to additional interventions at the treated level over 24 months post-treatment. Kaplan-Meier estimates for the probability (expressed as a percentage) of participants to receive an intervention are presented.

Trial Locations

Locations (48): Tennessee Valley Pain Consultants
🇺🇸
Huntsville, Alabama, United States
Integrated Pain Management
🇺🇸
Walnut Creek, California, United States
Holy Cross Orthopedics Institute
🇺🇸
Oakland Park, Florida, United States
Otrimed Clinical Research
🇺🇸
Edgewood, Kentucky, United States
Emory Orthopaedics & Spine Center
🇺🇸
Atlanta, Georgia, United States
George Washington University Medical Center
🇺🇸
Washington, District of Columbia, United States
Arizona Pain Specialists
🇺🇸
Scottsdale, Arizona, United States
Summit Pain Alliance
🇺🇸
Santa Rosa, California, United States
University Clinical Research
🇺🇸
Somerset, New Jersey, United States
DOC Clinical Research
🇺🇸
Dayton, Ohio, United States
Clinical Investigations, LLC
🇺🇸
Edmond, Oklahoma, United States
Spine Team Texas
🇺🇸
Southlake, Texas, United States
Coastal Clinical Research Specialists
🇺🇸
Fernandina Beach, Florida, United States
Precision Spine Care
🇺🇸
Tyler, Texas, United States
Ericksen Research & Development, LLC
🇺🇸
Bountiful, Utah, United States
the SMART Clinic
🇺🇸
Draper, Utah, United States
Rochester Regional Health
🇺🇸
Rochester, New York, United States
On Site Clinical Solutions, LLC
🇺🇸
Morrisville, North Carolina, United States
RI Hospital-Comprehensive Spine Center
🇺🇸
Providence, Rhode Island, United States
Monash Medical Center
🇦🇺
Clayton, Victoria, Australia
Millennium Pain Center
🇺🇸
Bloomington, Illinois, United States
MAPS Applied Research Center
🇺🇸
Shakopee, Minnesota, United States
Carolina Neurosurgery and Spine Associates
🇺🇸
Charlotte, North Carolina, United States
Hope Research Institute
🇺🇸
Saint George, Utah, United States
Ainsworth Institute of Pain Management
🇺🇸
New York, New York, United States
Injury Care Medical Center
🇺🇸
Boise, Idaho, United States
Physicians Research Group
🇺🇸
Tempe, Arizona, United States
Newport Beach Headache and Pain
🇺🇸
Newport Beach, California, United States
Orthopedic Pain Specialists
🇺🇸
Santa Monica, California, United States
The Spine Institute
🇺🇸
Santa Monica, California, United States
Georgia Institute for Clinical Research, LLC
🇺🇸
Marietta, Georgia, United States
Orthopedic Specialists of Louisiana
🇺🇸
Shreveport, Louisiana, United States
Cleveland Clinic
🇺🇸
Cleveland, Ohio, United States
Innovative Pain Care Center
🇺🇸
Las Vegas, Nevada, United States
Alabama Clinical Therapeutics, LLC
🇺🇸
Birmingham, Alabama, United States
Mayo Clinic
🇺🇸
Rochester, Minnesota, United States
UC Davis Spine Center
🇺🇸
Sacramento, California, United States
Institute for Regenerative Medicine and Clinical Research
🇺🇸
Pasadena, California, United States
TriWest Research Associates, LLC
🇺🇸
El Cajon, California, United States
Memorial Orthopaedics Surgical Group
🇺🇸
Long Beach, California, United States
Shrock Orthopedic Research, LLC
🇺🇸
Fort Lauderdale, Florida, United States
Denver Back Pain Specialists, LLC
🇺🇸
Greenwood Village, Colorado, United States
Orthopaedic and Spine Specialists
🇺🇸
York, Pennsylvania, United States
Texas Back Institute
🇺🇸
Plano, Texas, United States
The Center for Clinical Research/ Carolinas Pain Institute
🇺🇸
Winston-Salem, North Carolina, United States
Virginia iSpine Physicians, PC
🇺🇸
Richmond, Virginia, United States
Clinical Trials of South Carolina
🇺🇸
Charleston, South Carolina, United States
Greenville Pharmaceutical Research, Inc.
🇺🇸
Charleston, South Carolina, United States