P-15 Peptide Enhanced Bone Graft in Transforaminal Lumbar Interbody Fusion

James S. Harrop; John E. O’Toole; Michael P. Steinmetz; Rick C. Sasso; Christopher D. Chaput; K. Brandon Strenge; Greg Maislin; Jeffrey P. Mullin; Thomas B. Freeman; Anthony Guanciale; Howard Lantner; Michael E. Janssen; David G. Schwartz; John M. Small; Wellington K. Hsu; Paul M. Arnold

doi:10.1097/BRS.0000000000005579

P-15 Peptide Enhanced Bone Graft in Transforaminal Lumbar Interbody Fusion

James S. Harrop
, John E. O’Toole
, Michael P. Steinmetz
, Rick C. Sasso
, Christopher D. Chaput
, K. Brandon Strenge
, Greg Maislin
, Jeffrey P. Mullin
, Thomas B. Freeman
, Anthony Guanciale
, Howard Lantner
, Michael E. Janssen
, David G. Schwartz
, John M. Small
, Wellington K. Hsu
, Paul M. Arnold

Research output: Contribution to journal › Article › peer-review

Abstract

Study Design. – Prospective, multicenter, single-blind, randomized, controlled pivotal study. Objective. – To evaluate whether P-15L (PearlMatrix^TM P-15 Peptide Enhanced Bone Graft) is non-inferior in effectiveness to local autograft when applied in single level instrumented transforaminal lumbar interbody fusion (TLIF). Summary of Background Data. – P-15L, an FDA-designated Breakthrough Drug-Device, is a composite drug-device combination bone graft containing P-15, a 15-amino acid polypeptide, which enhances cell binding, proliferation, and differentiation resulting in bone formation. Methods. – Skeletally mature patients, aged 22-80 years, with degenerative disc disease (DDD) were randomized 1:1 to P-15L (investigational) or to the local autograft (control) during single-level TLIF with a polyetheretherketone (PEEK) cage and supplemental pedicle screw fixation. The primary outcome was Composite Clinical Success (CCS) at 24 months, defined as: no index level secondary surgical procedures; achievement of fusion; ≥15-point improvement in Oswestry Low Back Pain Disability Questionnaire (ODI) from baseline; no new or worsening persistent neurological deficit relative to baseline; and no device-related serious adverse events (SAEs). Results. – 290 patients were enrolled at 33 sites: 141 (48.6%) received P-15L, and 149 (51.3%) received local autograft. P-15L was non-inferior (P<0.0001) and superior (P=0.002) to autograft with respect to CCS, with 55.5% of the investigational group achieving composite clinical success compared with 37.5% of the control group. P-15L had a 25.8% higher fusion rate as compared to autograft for the CCS at 24 months (84.3% vs. 58.5%, respectively). Device-related SAE rates were similar in both groups. Conclusion. – P-15L was superior to local autograft in achieving clinical success at 24 months. Furthermore, P-15L produced a significantly higher fusion rate as compared to autograft. No meaningful clinical differences were found in the incidence of device-related SAEs. P-15L appears to be a safe and effective option for TLIF. Level of Evidence.

Original language	English (US)
Journal	Spine
Volume	Publish Ahead of Print
DOIs	https://doi.org/10.1097/BRS.0000000000005579
State	Published - 2025

Keywords

ABM/P-15 Matrix
Bone Graft
Fusion
P-15
PearlMatrix
TLIF
autograft
peptide

ASJC Scopus subject areas

Orthopedics and Sports Medicine
Clinical Neurology

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10.1097/BRS.0000000000005579

Cite this

Harrop, J. S., O’Toole, J. E., Steinmetz, M. P., Sasso, R. C., Chaput, C. D., Strenge, K. B., Maislin, G., Mullin, J. P., Freeman, T. B., Guanciale, A., Lantner, H., Janssen, M. E., Schwartz, D. G., Small, J. M., Hsu, W. K., & Arnold, P. M. (2025). P-15 Peptide Enhanced Bone Graft in Transforaminal Lumbar Interbody Fusion. Spine, Publish Ahead of Print. https://doi.org/10.1097/BRS.0000000000005579

@article{f59a8fbb557e41b584126ecedc2203ad,

title = "P-15 Peptide Enhanced Bone Graft in Transforaminal Lumbar Interbody Fusion",

abstract = "Study Design. – Prospective, multicenter, single-blind, randomized, controlled pivotal study. Objective. – To evaluate whether P-15L (PearlMatrixTM P-15 Peptide Enhanced Bone Graft) is non-inferior in effectiveness to local autograft when applied in single level instrumented transforaminal lumbar interbody fusion (TLIF). Summary of Background Data. – P-15L, an FDA-designated Breakthrough Drug-Device, is a composite drug-device combination bone graft containing P-15, a 15-amino acid polypeptide, which enhances cell binding, proliferation, and differentiation resulting in bone formation. Methods. – Skeletally mature patients, aged 22-80 years, with degenerative disc disease (DDD) were randomized 1:1 to P-15L (investigational) or to the local autograft (control) during single-level TLIF with a polyetheretherketone (PEEK) cage and supplemental pedicle screw fixation. The primary outcome was Composite Clinical Success (CCS) at 24 months, defined as: no index level secondary surgical procedures; achievement of fusion; ≥15-point improvement in Oswestry Low Back Pain Disability Questionnaire (ODI) from baseline; no new or worsening persistent neurological deficit relative to baseline; and no device-related serious adverse events (SAEs). Results. – 290 patients were enrolled at 33 sites: 141 (48.6\%) received P-15L, and 149 (51.3\%) received local autograft. P-15L was non-inferior (P<0.0001) and superior (P=0.002) to autograft with respect to CCS, with 55.5\% of the investigational group achieving composite clinical success compared with 37.5\% of the control group. P-15L had a 25.8\% higher fusion rate as compared to autograft for the CCS at 24 months (84.3\% vs. 58.5\%, respectively). Device-related SAE rates were similar in both groups. Conclusion. – P-15L was superior to local autograft in achieving clinical success at 24 months. Furthermore, P-15L produced a significantly higher fusion rate as compared to autograft. No meaningful clinical differences were found in the incidence of device-related SAEs. P-15L appears to be a safe and effective option for TLIF. Level of Evidence.",

keywords = "ABM/P-15 Matrix, Bone Graft, Fusion, P-15, PearlMatrix, TLIF, autograft, peptide",

author = "Harrop, \{James S.\} and O{\textquoteright}Toole, \{John E.\} and Steinmetz, \{Michael P.\} and Sasso, \{Rick C.\} and Chaput, \{Christopher D.\} and Strenge, \{K. Brandon\} and Greg Maislin and Mullin, \{Jeffrey P.\} and Freeman, \{Thomas B.\} and Anthony Guanciale and Howard Lantner and Janssen, \{Michael E.\} and Schwartz, \{David G.\} and Small, \{John M.\} and Hsu, \{Wellington K.\} and Arnold, \{Paul M.\}",

note = "Publisher Copyright: {\textcopyright} 2025",

year = "2025",

doi = "10.1097/BRS.0000000000005579",

language = "English (US)",

volume = "Publish Ahead of Print",

journal = "Spine",

issn = "0362-2436",

publisher = "Wolters Kluwer Health",

}

TY - JOUR

T1 - P-15 Peptide Enhanced Bone Graft in Transforaminal Lumbar Interbody Fusion

AU - Harrop, James S.

AU - O’Toole, John E.

AU - Steinmetz, Michael P.

AU - Sasso, Rick C.

AU - Chaput, Christopher D.

AU - Strenge, K. Brandon

AU - Maislin, Greg

AU - Mullin, Jeffrey P.

AU - Freeman, Thomas B.

AU - Guanciale, Anthony

AU - Lantner, Howard

AU - Janssen, Michael E.

AU - Schwartz, David G.

AU - Small, John M.

AU - Hsu, Wellington K.

AU - Arnold, Paul M.

PY - 2025

Y1 - 2025

N2 - Study Design. – Prospective, multicenter, single-blind, randomized, controlled pivotal study. Objective. – To evaluate whether P-15L (PearlMatrixTM P-15 Peptide Enhanced Bone Graft) is non-inferior in effectiveness to local autograft when applied in single level instrumented transforaminal lumbar interbody fusion (TLIF). Summary of Background Data. – P-15L, an FDA-designated Breakthrough Drug-Device, is a composite drug-device combination bone graft containing P-15, a 15-amino acid polypeptide, which enhances cell binding, proliferation, and differentiation resulting in bone formation. Methods. – Skeletally mature patients, aged 22-80 years, with degenerative disc disease (DDD) were randomized 1:1 to P-15L (investigational) or to the local autograft (control) during single-level TLIF with a polyetheretherketone (PEEK) cage and supplemental pedicle screw fixation. The primary outcome was Composite Clinical Success (CCS) at 24 months, defined as: no index level secondary surgical procedures; achievement of fusion; ≥15-point improvement in Oswestry Low Back Pain Disability Questionnaire (ODI) from baseline; no new or worsening persistent neurological deficit relative to baseline; and no device-related serious adverse events (SAEs). Results. – 290 patients were enrolled at 33 sites: 141 (48.6%) received P-15L, and 149 (51.3%) received local autograft. P-15L was non-inferior (P<0.0001) and superior (P=0.002) to autograft with respect to CCS, with 55.5% of the investigational group achieving composite clinical success compared with 37.5% of the control group. P-15L had a 25.8% higher fusion rate as compared to autograft for the CCS at 24 months (84.3% vs. 58.5%, respectively). Device-related SAE rates were similar in both groups. Conclusion. – P-15L was superior to local autograft in achieving clinical success at 24 months. Furthermore, P-15L produced a significantly higher fusion rate as compared to autograft. No meaningful clinical differences were found in the incidence of device-related SAEs. P-15L appears to be a safe and effective option for TLIF. Level of Evidence.

AB - Study Design. – Prospective, multicenter, single-blind, randomized, controlled pivotal study. Objective. – To evaluate whether P-15L (PearlMatrixTM P-15 Peptide Enhanced Bone Graft) is non-inferior in effectiveness to local autograft when applied in single level instrumented transforaminal lumbar interbody fusion (TLIF). Summary of Background Data. – P-15L, an FDA-designated Breakthrough Drug-Device, is a composite drug-device combination bone graft containing P-15, a 15-amino acid polypeptide, which enhances cell binding, proliferation, and differentiation resulting in bone formation. Methods. – Skeletally mature patients, aged 22-80 years, with degenerative disc disease (DDD) were randomized 1:1 to P-15L (investigational) or to the local autograft (control) during single-level TLIF with a polyetheretherketone (PEEK) cage and supplemental pedicle screw fixation. The primary outcome was Composite Clinical Success (CCS) at 24 months, defined as: no index level secondary surgical procedures; achievement of fusion; ≥15-point improvement in Oswestry Low Back Pain Disability Questionnaire (ODI) from baseline; no new or worsening persistent neurological deficit relative to baseline; and no device-related serious adverse events (SAEs). Results. – 290 patients were enrolled at 33 sites: 141 (48.6%) received P-15L, and 149 (51.3%) received local autograft. P-15L was non-inferior (P<0.0001) and superior (P=0.002) to autograft with respect to CCS, with 55.5% of the investigational group achieving composite clinical success compared with 37.5% of the control group. P-15L had a 25.8% higher fusion rate as compared to autograft for the CCS at 24 months (84.3% vs. 58.5%, respectively). Device-related SAE rates were similar in both groups. Conclusion. – P-15L was superior to local autograft in achieving clinical success at 24 months. Furthermore, P-15L produced a significantly higher fusion rate as compared to autograft. No meaningful clinical differences were found in the incidence of device-related SAEs. P-15L appears to be a safe and effective option for TLIF. Level of Evidence.

KW - ABM/P-15 Matrix

KW - Bone Graft

KW - Fusion

KW - P-15

KW - PearlMatrix

KW - TLIF

KW - autograft

KW - peptide

UR - https://www.scopus.com/pages/publications/105027441051

UR - https://www.scopus.com/pages/publications/105027441051#tab=citedBy

U2 - 10.1097/BRS.0000000000005579

DO - 10.1097/BRS.0000000000005579

M3 - Article

C2 - 41307110

AN - SCOPUS:105027441051

SN - 0362-2436

VL - Publish Ahead of Print

JO - Spine

JF - Spine

ER -

P-15 Peptide Enhanced Bone Graft in Transforaminal Lumbar Interbody Fusion

Abstract

Keywords

ASJC Scopus subject areas

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