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Hepatic targeting of transplanted liver sinusoidal endothelial cells in intact mice
Author(s) -
Benten Daniel,
Follenzi Antonia,
Bhargava Kuldeep K.,
Kumaran Vinay,
Palestro Christopher J.,
Gupta Sanjeev
Publication year - 2005
Publication title -
hepatology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 5.488
H-Index - 361
eISSN - 1527-3350
pISSN - 0270-9139
DOI - 10.1002/hep.20746
Subject(s) - liver transplantation , microbiology and biotechnology , biology , medicine , pathology , transplantation
Abstract Targeting of cells to specific tissues is critical for cell therapy. To study endothelial cell targeting, we isolated mouse liver sinusoidal endothelial cells (LSEC) and examined cell biodistributions in animals. To identify transplanted LSEC in tissues, we labeled cells metabolically with DiI‐conjugated acetylated low density lipoprotein particles (DiI‐Ac‐LDL) or 111 Indium‐oxine, used LSEC from Rosa26 donors expressing β‐galactosidase or Tie‐2‐GFP donors with green fluorescent protein (GFP) expression, and tranduced LSEC with a GFP‐lentiviral vector. LSEC efficiently incorporated 111 Indium and DiI‐Ac‐LDL and expressed GFP introduced by the lentiviral vector. Use of radiolabeled LSEC showed differences in cell biodistributions in relation to the cell transplantation route. After intraportal injection, LSEC were largely in the liver (60 ± 13%) and, after systemic intravenous injection, in lungs (67 ± 9%); however, after intrasplenic injection, only some LSEC remained in the spleen (29 ± 10%; P < .01), whereas most LSEC migrated to the liver or lungs. Transplanted LSEC were found in the liver, lungs, and spleen shortly after transplantation, whereas longer‐term cell survival was observed only in the liver. Transplanted LSEC were distinct from Kupffer cells with expression of Tie‐2 promoter‐driven GFP and of CD31, without F4/80 reactivity. In further studies using radiolabeled LSEC, we established that the manipulation of receptor‐mediated cell adhesion in liver sinusoids or the manipulation of blood flow–dependent cell exit from sinusoids improved intrahepatic retention of LSEC to 89 ± 7% and 89 ± 5%, respectively ( P < .01). In conclusion , the targeting of LSEC to the liver and other organs is directed by vascular bed–specific mechanisms, including blood flow–related processes, and cell‐specific factors. These findings may facilitate analysis of LSEC for cell and gene therapy applications. (H EPATOLOGY 2005.)