# Novel parathyroid hormone-based bone graft substitute, KUR-111, in treatment of tibial plateau fractures: a prospective, randomised, open-label, multicenter study

**Authors:** Nikolaos K Kanakaris, Michael J Raschke, Joe M Lane, James T Ryaby, Brent L Atkinson, Peter V Giannoudis

PMC · DOI: 10.1007/s00590-025-04645-2 · 2026-01-14

## TL;DR

A new bone graft substitute called KUR-111 was tested in treating tibial plateau fractures and showed promising healing results compared to traditional methods.

## Contribution

This study introduces KUR-111, a novel PTH-based bone graft substitute, and demonstrates its efficacy in treating tibial plateau fractures in a clinical trial.

## Key findings

- KUR-111-high achieved non-inferior union rates compared to autograft at 16 weeks.
- KUR-111-high significantly increased union rates compared to KUR-111-low.
- KUR-111-high resulted in less pain and reduced analgesic and opioid use compared to autograft.

## Abstract

The treatment of closed tibial plateau fractures (TPF) is complex and carries a risk of malunion. Parathyroid hormone (PTH) plays a key role in bone metabolism, and a PTH-peptide (PTH1 − 34) promotes bone healing. The objective was to evaluate the safety and efficacy of a novel PTH-based bone-graft-substitute (KUR-111) in the treatment of TPF.

The study was a randomised, controlled, multicenter, open-label (dose-blinded), and dose-finding clinical trial. Subjects were randomised into 3 groups (iliac crest autograft (control); KUR-111-low; and high-dose TGplPTH1-34). The primary efficacy endpoint was the rate of union by computed tomography (CT) at 16weeks, as assessed by the Independent Radiologist Evaluation Panel (IREP).

A total of 183 TPF were enrolled and treated. The primary endpoint was met, as statistical non-inferiority was demonstrated for KUR-111-high compared with autograft at 16weeks. KUR-111-high significantly (p = 0.03) increased union rates compared to KUR-111-low (83.6%vs66.1%). IREP and a clinician-assessed composite score of fracture healing showed higher healing rates for KUR-111-high than KUR-111-low or autograft. Loss of reduction was minimal (0.4–0.9 mm) without significant differences (p > 0.10) among groups. Mean pain of the treated knee improved from baseline, with the least pain for KUR-111-high at all timepoints. Clinically significant donor-site pain was reported by 61.8% at discharge and remained in 12.2% of subjects at 104weeks. By 104weeks, analgesic use following KUR-111-high was less than one-half (9.8%vs24.1%), and opioid use was approximately 7-fold lower (1.6%vs12.1%) as compared to autograft.

KUR-111-high has the potential to be a promising adjunctive therapy in the treatment of closed TPFs.

Therapeutic Level I.

## Full-text entities

- **Genes:** PTH (parathyroid hormone) [NCBI Gene 5741] {aka FIH1, PTH1}
- **Diseases:** malunion (MESH:D017759), fracture (MESH:D050723), pain (MESH:D010146), TPF (MESH:D000092463)
- **Chemicals:** KUR-111 (-)

## Figures

4 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12804197/full.md

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Source: https://tomesphere.com/paper/PMC12804197