Autologous Bone Marrow Mononuclear Cell Transplantation in Patients with Decompensated Alcoholic Liver Disease: A Randomized Controlled Trial | Zendy

Laurent Spahr | Zendy; Yves Chalandon | Zendy; Sylvain Terraz | Zendy; Vincent Kindler | Zendy; Laura RubbiaBrandt | Zendy; JeanLouis Frossard | Zendy; Romain Bréguet | Zendy; Nicolas Lanthier | Zendy; Annarita Farina | Zendy; Jakob Passweg | Zendy; Christoph D. Becker | Zendy; Antoine Hadengue | Zendy

Open Access

Autologous Bone Marrow Mononuclear Cell Transplantation in Patients with Decompensated Alcoholic Liver Disease: A Randomized Controlled Trial

Author(s) -

Laurent Spahr,

Yves Chalandon,

Sylvain Terraz,

Vincent Kindler,

Laura RubbiaBrandt,

JeanLouis Frossard,

Romain Bréguet,

Nicolas Lanthier,

Annarita Farina,

Jakob Passweg,

Christoph D. Becker,

Antoine Hadengue

Publication year - 2013

Publication title -

plos one

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.99

H-Index - 332

ISSN - 1932-6203

DOI - 10.1371/journal.pone.0053719

Subject(s) - medicine , alcoholic liver disease , liver biopsy , gastroenterology , clinical endpoint , cirrhosis , transplantation , liver function , liver function tests , bone marrow , liver transplantation , alcoholic hepatitis , model for end stage liver disease , steatohepatitis , liver disease , biopsy , randomized controlled trial , fatty liver , surgery , disease

Objective Impaired liver regeneration is associated with a poor outcome in patients with decompensated alcoholic liver disease (ALD). We assessed whether autologous bone marrow mononuclear cell transplantation (BMMCT) improved liver function in decompensated ALD. Design 58 patients (mean age 54 yrs; mean MELD score 19, all with cirrhosis, 81% with alcoholic steatohepatitis at baseline liver biopsy) were randomized early after hospital admission to standard medical therapy (SMT) alone (n = 30), including steroids in patients with a Maddrey’s score ≥32, or combined with G-CSF injections and autologous BMMCT into the hepatic artery (n = 28). Bone marrow cells were harvested, isolated and reinfused the same day. The primary endpoint was a ≥3 points decrease in the MELD score at 3 months, corresponding to a clinically relevant improvement in liver function. Liver biopsy was repeated at week 4 to assess changes in Ki67+/CK7+ hepatic progenitor cells (HPC) compartment. Results Both study groups were comparable at baseline. After 3 months, 2 and 4 patients died in the BMMCT and SMT groups, respectively. Adverse events were equally distributed between groups. Moderate alcohol relapse occurred in 31% of patients. The MELD score improved in parallel in both groups during follow-up with 18 patients (64%) from the BMMCT group and 18 patients (53%) from the SMT group reaching the primary endpoint (p = 0.43 (OR 1.6, CI 0.49–5.4) in an intention to treat analysis. Comparing liver biopsy at 4 weeks to baseline, steatosis improved (p<0.001), and proliferating HPC tended to decrease in both groups (−35 and −33%, respectively). Conclusion Autologous BMMCT, compared to SMT is a safe procedure but did not result in an expanded HPC compartment or improved liver function. These data suggest either insufficient regenerative stimulation after BMMCT or resistance to liver regenerative drive in patients with decompensated alcoholic cirrhosis. Trial Registration Controlled-Trials.com ISRCTN83972743 .

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