Probability of severe frailty development among operative and nonoperative adult spinal deformity patients: an actuarial survivorship analysis over a 3-year period.

dc.contributor.author

Passias, Peter G

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Segreto, Frank A

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Bortz, Cole A

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Horn, Samantha R

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Pierce, Katherine E

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Naessig, Sara

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Brown, Avery E

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Jackson-Fowl, Brendan

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Ahmad, Waleed

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Oh, Cheongeun

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Lafage, Virginie

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Lafage, Renaud

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Smith, Justin S

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Daniels, Alan H

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Line, Breton G

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Kim, Han Jo

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Uribe, Juan S

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Eastlack, Robert K

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Hamilton, D Kojo

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Klineberg, Eric O

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Burton, Douglas C

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Hart, Robert AA

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Schwab, Frank J

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Shaffrey, Christopher I

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Ames, Christopher P

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Bess, Shay

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International Spine Study Group

dc.date.accessioned

2023-06-19T19:59:46Z

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2023-06-19T19:59:46Z

dc.date.issued

2020-08

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2023-06-19T19:59:45Z

dc.description.abstract

Background

Little is known of how frailty, a dynamic measure of physiological age, progresses relative to age or disability status. Operative treatment of adult spinal deformity (ASD) may play a role in frailty remediation and maintenance.

Purpose

Compare frailty status, severe frailty development, and factors influencing severe frailty development among ASD patients undergoing operative or nonoperative treatment.

Design

Retrospective review with maximum follow-up of 3 years.

Setting

Prospective, multicenter, ASD database.

Participants

Patients were consecutively enrolled from 13 participating centers.

Inclusion criteria

≥18 years undergoing either operative or nonoperative treatment for ASD, exclusion criteria: spinal deformity of neuromuscular etiology, presence of active infection, or malignancy. The mean age of the participants analyzed were 54.9 for the operative cohort and 55.0 for the nonoperative cohort.

Outcomes measures

Frailty status, severe frailty development, and factors influencing severe frailty development.

Methods

ASD patients (coronal scoliosis ≥20°, sagittal vertical axis (SVA) ≥5 cm, Pelvic Tilt (PT) ≥25°, or thoracic kyphosis ≥60°) >18 y/o, with Base Line (BL) frailty scores were included. Frailty was scored from 0 to 1 (not frail: <0.3, frail 0.3-0.5, severe frailty >0.5) through the use of ASD-frailty index (FI) which has been validated using the International Spine Study Group (ISSG) ASD database, European Spine Study Group ASD database, and the Scoli-RISK-1 Patient Database. The ISSG is funded through research grants from DePuy Synthes and individual donations and supported the current work. Operative (Op) and Nonoperative (Non-Op) patients were propensity matched. T-tests compared frailty among treatment groups and BL, 1, 2, and ≥3 years. An actuarial Kaplan-Meier survivorship analysis with log-rank (Mantel-Cox) test, adjusting for patients lost to follow-up, determined probability of severe frailty development. Multivariate Cox Regressions gauged the effect of sagittal malalignment, patient and surgical details on severe frailty development.

Results

The analysis includes 472 patients (236 Op, 236 Non-Op) selected by propensity score matching from a cohort of 1,172. Demographics and comorbidities were similar between groups (p>.05). Op exhibited decreased frailty at all follow-up intervals compared with BL (BL: 0.22 vs Y1: 0.18; Y2: 0.16; Y3: 0.15, all p<.001). Non-Op displayed similar frailty from BL to 2Y follow up, and increased frailty at 3Y follow up (0.23 vs 0.25, p=.014). Compared with Non-Op, Op had lower frailty at 1Y (0.18 vs 0.24), 2Y (0.16 vs 0.23), and 3Y (0.15 vs 0.25; all p<.001). Cumulative probability of maintaining nonsevere frailty was (Op: 97.7%, Non-Op: 94.5%) at 1Y, (Op: 95.1%, Non-Op: 90.4%) at 2Y, and (Op: 95.1%, Non-Op: 89.1%) at ≥3Y, (p=.018). Among all patients, baseline depression (hazard ratio: 2.688[1.172-6.167], p=.020), Numeric Rating Scale (NRS) back pain scores (HR: 1.247[1.012-1.537], p=.039), and nonoperative treatment (HR: 2.785[1.167-6.659], p=.021) predicted severe frailty development with having a HR>1.0 and p value<.05. Among operative patients, 6-week postoperative residual SVA malalignment (SRS-Schwab SVA+modifier) (HR: 15.034[1.922-116.940], p=.010) predicted severe frailty development indicated by having a HR>1.0 and p value <.05.

Conclusions

Non-Op patients were more likely to develop severe frailty, and at a quicker rate. Baseline depression, increased NRS back pain scores, nonoperative treatment, and postoperative sagittal malalignment at 6-week follow-up significantly predicted severe frailty development. Operative intervention and postoperative sagittal balance appear to play significant roles in frailty remediation and maintenance in ASD patients. Frailty is one factor, in a multifactorial conservation, that may be considered when determining operative or nonoperative values for ASD patients. Operating before the onset of severe frailty, may result in a lower complication risk and better long-term clinical outcomes.
dc.identifier

S1529-9430(20)30145-5

dc.identifier.issn

1529-9430

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1878-1632

dc.identifier.uri

https://hdl.handle.net/10161/28139

dc.language

eng

dc.publisher

Elsevier BV

dc.relation.ispartof

The spine journal : official journal of the North American Spine Society

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10.1016/j.spinee.2020.04.010

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International Spine Study Group

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Humans

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Lordosis

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Probability

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Retrospective Studies

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Prospective Studies

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Quality of Life

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Adult

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Frailty

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Survivorship

dc.title

Probability of severe frailty development among operative and nonoperative adult spinal deformity patients: an actuarial survivorship analysis over a 3-year period.

dc.type

Journal article

duke.contributor.orcid

Passias, Peter G|0000-0002-1479-4070|0000-0003-2635-2226

duke.contributor.orcid

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

pubs.begin-page

1276

pubs.end-page

1285

pubs.issue

8

pubs.organisational-group

Duke

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School of Medicine

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Clinical Science Departments

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Orthopaedic Surgery

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Neurosurgery

pubs.publication-status

Published

pubs.volume

20

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