Overexpression of the cholesterol-binding protein MLN64 induces liver damage in the mouse

To examine the in vivo phenotype associated with hepatic metastatic lymph node 64 (MLN64) over-expression. Recombinant-adenovirus-mediated MLN64 gene transfer was used to overexpress MLN64 in the livers of C57BL/6 mice. We measured the effects of MLN64 overexpression on hepatic cholesterol content,...

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Veröffentlicht in:World journal of gastroenterology : WJG 2007-06, Vol.13 (22), p.3071-3079
Hauptverfasser: Tichauer, Juan-Enrique, Morales, Maria-Gabriela, Amigo, Ludwig, Galdames, Leopoldo, Klein, Andres, Quinones, Veronica, Ferrada, Carla, Alvarez, Alejandra-R, Rio, Marie-Christine, Miquel, Juan-Francisco, Rigotti, Attilio, Zanlungo, Silvana
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Sprache:eng
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Zusammenfassung:To examine the in vivo phenotype associated with hepatic metastatic lymph node 64 (MLN64) over-expression. Recombinant-adenovirus-mediated MLN64 gene transfer was used to overexpress MLN64 in the livers of C57BL/6 mice. We measured the effects of MLN64 overexpression on hepatic cholesterol content, bile flow, biliary lipid secretion and apoptosis markers. For in vitro studies cultured CHO cells with transient MLN64 overexpression were utilized and apoptosis by TUNEL assay was measured. Livers from Ad.MLN64-infected mice exhibited early onset of liver damage and apoptosis. This response correlated with increases in liver cholesterol content and biliary bile acid concentration, and impaired bile flow. We investigated whether liver MLN64 expression could be modulated in a murine model of hepatic injury. We found increased hepatic MLN64 mRNA and protein levels in mice with chenodeoxycholic acid-induced liver damage. In addition, cultured CHO cells with transient MLN64 overexpression showed increased apoptosis. In summary, hepatic MLN64 over-expression induced damage and apoptosis in murine livers and altered cholesterol metabolism. Further studies are required to elucidate the relevance of these findings under physiologic and disease conditions.
ISSN:1007-9327
2219-2840
DOI:10.3748/wjg.v13.i22.3071