Does recombinant human bone morphogenetic protein-2 use in adult spinal deformity increase complications and are complications associated with location of rhBMP-2 use? A prospective, multicenter study of 279 consecutive patients.

dc.contributor.author

Bess, Shay

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Line, Breton G

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Lafage, Virginie

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Schwab, Frank

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Shaffrey, Christopher I

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Hart, Robert A

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Boachie-Adjei, Oheneba

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Akbarnia, Behrooz A

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Ames, Christopher P

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Burton, Douglas C

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Deverin, Vedat

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Fu, Kai-Ming G

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Gupta, Munish

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Hostin, Richard

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Kebaish, Khaled

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Klineberg, Eric

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Mundis, Gregory

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O'Brien, Michael

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Shelokov, Alexis

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Smith, Justin S

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International Spine Study Group ISSG

dc.date.accessioned

2023-07-20T20:43:24Z

dc.date.available

2023-07-20T20:43:24Z

dc.date.issued

2014-02

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2023-07-20T20:43:22Z

dc.description.abstract

Study design

Multicenter, prospective analysis of consecutive patients with adult spinal deformity (ASD).

Objective

Evaluate complications associated with recombinant human bone morphogenetic protein-2 (rhBMP-2) use in ASD.

Summary of background data

Off-label rhBMP-2 use is common; however, underreporting of rhBMP-2 associated complications has been recently scrutinized.

Methods

Patients with ASD consecutively enrolled into a prospective, multicenter database were evaluated for type and timing of acute perioperative complications.

Inclusion criteria

age 18 years and older, ASD, spinal arthrodesis of more than 4 levels, and 3 or more months of follow-up. Patients were divided into those receiving rhBMP-2 (BMP) or no rhBMP-2 (NOBMP). BMP divided into location of use: posterior (PBMP), interbody (IBMP), and interbody + posterior spine (I + PBMP). Correlations between acute perioperative complications and rhBMP-2 use including total dose, dose/level, and location of use were evaluated.

Results

A total of 279 patients (mean age: 57 yr; mean spinal levels fused: 12.0; and mean follow-up: 28.8 mo) met inclusion criteria. BMP (n = 172; average posterior dose = 2.5 mg/level, average interbody dose = 5 mg/level) had similar age, smoking history, previous spine surgery, total spinal levels fused, estimated blood loss, and duration of hospital stay as NOBMP (n = 107; P > 0.05). BMP had greater Charlson Comorbidity Index (1.9 vs. 1.2), greater scoliosis (43° vs. 38°), longer operative time (488.2 vs. 414.6 min), more osteotomies per patient (4.0 vs. 1.6), and greater percentage of anteroposterior fusion (APSF; 20.9% vs. 8.4%) than NOBMP, respectively (P < 0.05). BMP had more total complications per patient (1.4 vs. 0.6) and more minor complications per patient (0.9 vs. 0.2) than NOBMP, respectively (P < 0.05). NOBMP had more complications requiring surgery per patient than BMP (0.3 vs. 0.2; P < 0.05). Major, neurological, wound, and infectious complications were similar for NOBMP, BMP, PBMP, IBMP, and I + PBMP (P > 0.05). Multivariate analysis demonstrated small to nonexistent correlations between rhBMP-2 use and complications.

Conclusion

RhBMP-2 use and location of rhBMP-2 use in ASD surgery, at reported doses, do not increase acute major, neurological, or wound complications. Research is needed for higher rhBMP-2 dosing and long-term follow-up.

Level of evidence

2.
dc.identifier

00007632-201402010-00012

dc.identifier.issn

0362-2436

dc.identifier.issn

1528-1159

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https://hdl.handle.net/10161/28537

dc.language

eng

dc.publisher

Ovid Technologies (Wolters Kluwer Health)

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Spine

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10.1097/brs.0000000000000104

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International Spine Study Group ISSG

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Humans

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Scoliosis

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Postoperative Complications

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Transforming Growth Factor beta

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Recombinant Proteins

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Spinal Fusion

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Follow-Up Studies

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Prospective Studies

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Adolescent

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Adult

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Aged

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Aged, 80 and over

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Middle Aged

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Female

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Male

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Bone Morphogenetic Protein 2

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Young Adult

dc.title

Does recombinant human bone morphogenetic protein-2 use in adult spinal deformity increase complications and are complications associated with location of rhBMP-2 use? A prospective, multicenter study of 279 consecutive patients.

dc.type

Journal article

duke.contributor.orcid

Shaffrey, Christopher I|0000-0001-9760-8386

pubs.begin-page

233

pubs.end-page

242

pubs.issue

3

pubs.organisational-group

Duke

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School of Medicine

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Clinical Science Departments

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Orthopaedic Surgery

pubs.organisational-group

Neurosurgery

pubs.publication-status

Published

pubs.volume

39

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