Transplantation with autologous bone marrow‐derived mesenchymal stem cells for alcoholic cirrhosis: Phase 2 trial

Ki Tae Suk; Jung‐Hwan Yoon; Moon Young Kim; Chang Wook Kim; Ja Kyung Kim; Hana Park; Seong Gyu Hwang; Dong Joon Kim; Byung Seok Lee; Sae Hwan Lee; Hong Soo Kim; Jae Young Jang; Chang‐Hyeong Lee; Byung Seok Kim; Yoon Ok Jang; Mee-Yon Cho; Eun Sun Jung; Yong Man Kim; Si Hyun Bae; Soon Koo Baik

doi:10.1002/hep.28693

Transplantation with autologous bone marrow‐derived mesenchymal stem cells for alcoholic cirrhosis: Phase 2 trial

Ki Tae Suk(Hallym University), Jung‐Hwan Yoon(Seoul National University), Moon Young Kim(Yonsei University), Chang Wook Kim(The Catholic University of Korea Uijeongbu St. Mary's Hospital), Ja Kyung Kim(Gangnam Severance Hospital), Hana Park(CHA University Bundang Medical Center), Seong Gyu Hwang(CHA University Bundang Medical Center), Dong Joon Kim(Hallym University), Byung Seok Lee(Chungnam National University), Sae Hwan Lee(Soonchunhyang University), Hong Soo Kim(Soonchunhyang University), Jae Young Jang(Soonchunhyang University), Chang‐Hyeong Lee(Daegu Catholic University), Byung Seok Kim(Daegu Catholic University), Yoon Ok Jang(Yonsei University), Mee-Yon Cho(Yonsei University), Eun Sun Jung(Seoul National University), Yong Man Kim(Hallym University), Si Hyun Bae(Hallym University), Soon Koo Baik(Yonsei University)

Hepatology

June 23, 2016

10.1002/hep.28693

Cited by 309Open Access

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Abstract

Bone marrow‐derived mesenchymal stem cell (BM‐MSC) transplantation has been suggested as an effective therapy for liver cirrhosis. The efficacy and safety of autologous BM‐MSC transplantation in the treatment of alcoholic cirrhosis were investigated. Seventy‐two patients with baseline biopsy‐proven alcoholic cirrhosis who had been alcohol‐abstinent for more than 6 months underwent a multicenter, randomized, open‐label, phase 2 trial. Patients were randomly assigned to three groups: one control group and two autologous BM‐MSC groups that underwent either one‐time or two‐time hepatic arterial injections of 5 × 10 7 BM‐MSCs 30 days after BM aspiration. A follow‐up biopsy was performed 6 months after enrollment, and adverse events were monitored for 12 months. The primary endpoint was improvement in fibrosis quantification based on picrosirius red staining. The secondary endpoints included liver function tests, Child‐Pugh score, and Model for End‐stage Liver Disease score. Outcomes were analyzed by per‐protocol analysis. In terms of fibrosis quantification (before versus after), the one‐time and two‐time BM‐MSC groups were associated with 25% (19.5 ± 9.5% versus 14.5 ± 7.1%) and 37% (21.1 ± 8.9% versus 13.2 ± 6.7%) reductions in the proportion of collagen, respectively ( P < 0.001). In the intergroup comparison, two‐time BM‐MSC transplantation in comparison with one‐time BM‐MSC transplantation was not associated with improved results in fibrosis quantification ( P > 0.05). The Child‐Pugh scores of both BM‐MSC groups (one‐time 7.6 ± 1.0 versus 6.3 ± 1.3 and two‐time 7.8 ± 1.2 versus 6.8 ± 1.6) were also significantly improved following BM‐MSC transplantation ( P < 0.05). The proportion of patients with adverse events did not differ among the three groups. Conclusion : Autologous BM‐MSC transplantation safely improved histologic fibrosis and liver function in patients with alcoholic cirrhosis. (H epatology 2016;64:2185‐2197)

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