A Subpopulation of Bone Marrow Cells Depleted by a Novel Antibody, Anti-Liv8, is Useful for Cell Therapy to Repair Damaged Liver

Overview

Journal Biochem Biophys Res Commun

Publisher Elsevier

Specialty Biochemistry

Date 2004 Jan 7

PMID 14706657

Citations 11

Authors

Naoki Yamamoto

Shuji Terai

Shinya Ohata

Tomomi Watanabe

Kaoru Omori

Koh Shinoda

Koji Miyamoto

Toshiaki Katada

Isao Sakaida

Hiroshi Nishina

Kiwamu Okita

Affiliations

Soon will be listed here.

Abstract

We previously reported a new in vivo model named as "GFP/CCl(4) model" for monitoring the transdifferentiation of green fluorescent protein (GFP) positive bone marrow cell (BMC) into albumin-positive hepatocyte under the specific "niche" made by CCl(4) induced persistent liver damage, but the subpopulation which BMCs transdifferentiate into hepatocytes remains unknown. Here we developed a new monoclonal antibody, anti-Liv8, using mouse E 11.5 fetal liver as an antigen. Anti-Liv8 recognized both hematopoietic progenitor cells in fetal liver at E 11.5 and CD45-positive hematopoietic cells in adult bone marrow. We separated Liv8-positive and Liv8-negative cells and then transplanted these cells into a continuous liver damaged model. At 4 weeks after BMC transplantation, more efficient repopulation and transdifferentiation of BMC into hepatocytes were seen with Liv8-negative cells. These findings suggest that the subpopulation of Liv8-negative cells includes useful cells to perform cell therapy on repair damaged liver.

Citing Articles

Migration of human umbilical cord blood cells into rat liver.

Ismail A, Hassan E, Seleem M, Hassan M, ElDeen F, Salah A Int J Stem Cells. 2014; 3(2):154-60.

PMID: 24855553 PMC: 4021809. DOI: 10.15283/ijsc.2010.3.2.154.

Application of stem cells in orthopedics.

Schmitt A, van Griensven M, Imhoff A, Buchmann S Stem Cells Int. 2012; 2012:394962.

PMID: 22550505 PMC: 3328166. DOI: 10.1155/2012/394962.

Splenectomy enhances the anti-fibrotic effect of bone marrow cell infusion and improves liver function in cirrhotic mice and patients.

Iwamoto T, Terai S, Mizunaga Y, Yamamoto N, Omori K, Uchida K J Gastroenterol. 2011; 47(3):300-12.

PMID: 22065159 DOI: 10.1007/s00535-011-0486-7.

Efficacy of mesenchymal stem cells in suppression of hepatocarcinorigenesis in rats: possible role of Wnt signaling.

Abdel Aziz M, El Asmar M, Atta H, Mahfouz S, Fouad H, Roshdy N J Exp Clin Cancer Res. 2011; 30:49.

PMID: 21545718 PMC: 3113743. DOI: 10.1186/1756-9966-30-49.

Stem cells for end stage liver disease: how far have we got?.

Lorenzini S, Gitto S, Grandini E, Andreone P, Bernardi M World J Gastroenterol. 2008; 14(29):4593-9.

PMID: 18698672 PMC: 2738783. DOI: 10.3748/wjg.14.4593.