Cell-permeable bone morphogenetic protein 2 facilitates bone regeneration by promoting osteogenesis

Mingu Kang; Seokwon Lee; Jong-pil Seo; Eun-bee Lee; Daye Ahn; Jisoo Shin; Young-Ki Paik; Daewoong Jo

Materials Today Bio (Apr 2024)

Cell-permeable bone morphogenetic protein 2 facilitates bone regeneration by promoting osteogenesis

Mingu Kang,
Seokwon Lee,
Jong-pil Seo,
Eun-bee Lee,
Daye Ahn,
Jisoo Shin,
Young-Ki Paik,
Daewoong Jo

Affiliations

Mingu Kang: Cellivery R&D Institute, Cellivery Therapeutics, Inc., Seoul, 03929, South Korea
Seokwon Lee: Cellivery R&D Institute, Cellivery Therapeutics, Inc., Seoul, 03929, South Korea
Jong-pil Seo: College of Veterinary Medicine and Veterinary Medical Research Institute, Jeju National University, Jeju, 63243, South Korea
Eun-bee Lee: College of Veterinary Medicine and Veterinary Medical Research Institute, Jeju National University, Jeju, 63243, South Korea
Daye Ahn: Cellivery R&D Institute, Cellivery Therapeutics, Inc., Seoul, 03929, South Korea
Jisoo Shin: Cellivery R&D Institute, Cellivery Therapeutics, Inc., Seoul, 03929, South Korea
Young-Ki Paik: Cellivery R&D Institute, Cellivery Therapeutics, Inc., Seoul, 03929, South Korea; Corresponding author. Cellivery Therapeutics, Inc., K-BIZ DMC Tower F9, 189 Sungam-Ro, Mapo-Gu, Seoul, 03929, South Korea.
Daewoong Jo: Cellivery R&D Institute, Cellivery Therapeutics, Inc., Seoul, 03929, South Korea; Corresponding author.

Journal volume & issue: Vol. 25
p. 100983

Abstract

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The use of the FDA-approved osteoinductive growth factor BMP2 is widespread for bone regeneration. However, its clinical application has been hindered by limitations in cell permeability and a short half-life in circulation. To address this issue, we have developed a modified version of BMP2, referred to as Cell Permeable (CP)-BMP2, which possesses improved cell permeability. CP-BMP2 incorporates an advanced macromolecular transduction domain (aMTD) to facilitate transfer across the plasma membrane, a solubilization domain, and recombinant human BMP2. Compared to traditional rhBMP2, CP-BMP2 exhibits enhanced cell permeability, solubility, and bioavailability, and activates Smad phosphorylation through binding to BMP receptor 2. The effectiveness of CP-BMP2 was evaluated in three animal studies focusing on bone regeneration. In the initial study, mice and rabbits with critical-size calvarial defects received subcutaneous (SC) injections of CP-BMP2 and rhBMP2 (7.5 mg/kg, 3 injections per week for 8 weeks).Following 8 weeks of administration, CP-BMP2 demonstrated a remarkable 65 % increase in bone formation in mice when compared to both the vehicle and rhBMP2. Moreover, rabbits exhibited faster bone formation, characterized by a filling pattern originating from the center. In a subsequent study involving injured horses, hind limb bones treated with CP-BMP2 exhibited an 85 % higher bone regeneration rate, as evidenced by Micro-CT results, in contrast to horses treated with the vehicle or rhBMP2 (administered at 150 μg/defect, subcutaneously, once a week for 8 weeks, without a scaffold). These results underscore the potential of CP-BMP2 to facilitate rapid and effective healing. No noticeable adverse effects, such as ectopic bone formation, were observed in any of the studies. Overall, our findings demonstrate that CP-BMP2 holds therapeutic potential as a novel and effective osteogenic agent.

Published in Materials Today Bio

ISSN: 2590-0064 (Online)
Publisher: Elsevier
Country of publisher: Netherlands
LCC subjects: Medicine: Medicine (General); Science: Biology (General)
Website: https://www.journals.elsevier.com/materials-today-bio

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