Mitochondrial transplantation as a novel therapeutic approach in idiopathic inflammatory myopathy
- Authors
- Kim, Jeong Yeon; Kang, Young Cheol; Kim, Min Jung; Kim, Seon Uk; Kang, Hae Rim; Yeo, Jeong Seon; Kim, Yujin; Yu, Shin-Hye; Song, Byeongwook; Hwang, Jung Wook; Lee, Yun-Sang; Byun, Jung Woo; Yoo, Dae Hyun; Kim, Hyun Sook; Han, Kyuboem; Kim, Chun-Hyung; Lee, Eun Young
- Issue Date
- Apr-2025
- Publisher
- BMJ Publishing Group
- Citation
- Annals of the Rheumatic Diseases, v.84, no.4, pp 609 - 619
- Pages
- 11
- Indexed
- SCIE
SCOPUS
- Journal Title
- Annals of the Rheumatic Diseases
- Volume
- 84
- Number
- 4
- Start Page
- 609
- End Page
- 619
- URI
- https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/209963
- DOI
- 10.1016/j.ard.2024.11.005
- ISSN
- 0003-4967
1468-2060
- Abstract
- Objectives
This study aimed to investigate the efficacy of mitochondrial transplantation as a therapeutic intervention for idiopathic inflammatory myopathy (IIM). This study used a comprehensive approach, incorporating both in vitro and in vivo IIM models, and conducted a first-in-human clinical trial to assess the effectiveness and safety of mitochondria isolated from human umbilical cord mesenchymal stem cells (PN-101).
Methods
Mitochondria isolated from umbilical cord mesenchymal stem cells were designated as PN-101. The efficacy of PN-101 was assessed using myoblasts derived from patients with IIM and C2C12 mouse perforin/granzyme B–treated myoblasts as an in vitro IIM model. PN-101’s effect on IIM was examined using C protein–induced myositis (CIM) mice as an in vivo model. The efficacy and safety of PN-101 were evaluated in a phase 1/2a clinical trial involving 9 adult patients with refractory polymyositis or dermatomyositis.
Results
The myoblasts derived from patients with IIM exhibited defects in mitochondrial function and myogenesis. PN-101 transplantation enhances muscle differentiation and mitochondrial function in IIM myoblasts. PN-101 also enhanced intracellular adenosine triphosphate content, cell viability, and myogenesis in C2C12 perforin/granzyme B–treated myoblasts. In an in vivo model, PN-101 reduced myositis severity by exhibiting anti-inflammatory effects and restoring the CIM-induced metabolic shift. In a phase 1/2a prospective clinical trial involving adult patients with refractory IIM, PN-101 demonstrated no severe adverse drug reactions and showed at least minimal improvement in the International Myositis Assessment and Clinical Studies Group (IMACS)–Total Improvement Scores (TISs) compared with baseline.
Conclusions
PN-101 transplantation could serve as a novel treatment for IIM by enhancing mitochondrial repair and reducing inflammation in muscle tissues.
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