Myc-transformed epithelial cells down-regulate clusterin, which inhibits their growth in vitro and carcinogenesis in vivo

Myc-transformed epithelial cells down-regulate clusterin, which inhibits their growth in vitro and carcinogenesis in vivo

Effective treatment of malignant carcinomas requires identification of proteins regulating epithelial cell proliferation. To this end, we compared gene expression profiles in murine colonocytes and their c-Myc-transformed counterparts, which possess enhanced proliferative potential. A surprisingly s...

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Veröffentlicht in:Cancer research (Chicago, Ill.) Ill.), 2004-05, Vol.64 (9), p.3126-3136
Hauptverfasser: THOMAS-TIKHONENKO, Andrei, VIARD-LEVEUGLE, Isabelle, SAURAT, Jean-Hilaire, FRENCH, Lars E, DEWS, Michael, WEHRLI, Philippe, SEVIGNANI, Cinzia, DUONAN YU, RICCI, Stacey, EL-DEIRY, Wafik, ARONOW, Bruce, KAYA, Gürkan
Format: Artikel
Sprache:eng
Schlagworte:
Adenovirus
Animals
Antineoplastic agents
Biological and medical sciences
Cell Division - drug effects
Cell Division - physiology
Cell Transformation, Neoplastic
Clusterin
Down-Regulation
Epithelial Cells - cytology
Epithelial Cells - drug effects
Epithelial Cells - physiology
Genes, myc - physiology
Glycoproteins - biosynthesis
Glycoproteins - genetics
Glycoproteins - pharmacology
Glycoproteins - physiology
Humans
Keratinocytes - cytology
Keratinocytes - drug effects
Keratinocytes - metabolism
Keratinocytes - physiology
Medical sciences
Mice
Mice, Knockout
Molecular Chaperones - biosynthesis
Molecular Chaperones - genetics
Molecular Chaperones - pharmacology
Molecular Chaperones - physiology
Pharmacology. Drug treatments
Recombinant Proteins - pharmacology
Skin Neoplasms - genetics
Skin Neoplasms - metabolism
Skin Neoplasms - pathology
Skin Neoplasms - prevention & control
Thrombospondin 1 - antagonists & inhibitors
Thrombospondin 1 - biosynthesis
Thrombospondin 1 - genetics
Tumors
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Zusammenfassung:Effective treatment of malignant carcinomas requires identification of proteins regulating epithelial cell proliferation. To this end, we compared gene expression profiles in murine colonocytes and their c-Myc-transformed counterparts, which possess enhanced proliferative potential. A surprisingly short list of deregulated genes included the cDNA for clusterin, an extracellular glycoprotein without a firmly established function. We had previously demonstrated that in organs such as skin, clusterin expression is restricted to differentiating but not proliferating cell layers, suggesting a possible negative role in cell division. Indeed, its transient overexpression in Myc-transduced colonocytes decreased cell accumulation. Furthermore, clusterin was down-regulated in rapidly dividing human keratinocytes infected with a Myc-encoding adenovirus. Its knockdown via antisense RNA in neoplastic epidermoid cells enhanced proliferation. Finally, recombinant human clusterin suppressed, in a dose-dependent manner, DNA replication in keratinocytes and other cells of epithelial origin. Thus, clusterin appears to be an inhibitor of epithelial cell proliferation in vitro. To determine whether it also affects neoplastic growth in vivo, we compared wild-type and clusterin-null mice with respect to their sensitivity to 7, 12-dimethylbenz(a)anthracene /12-Otetradecanoylphorbol-13-acetate (DMBA/TPA)-induced skin carcinogenesis. We observed that the mean number of papillomas/mouse was higher in clusterin-null animals. Moreover, these papillomas did not regress as readily as in wild-type mice and persisted beyond week 35. The rate of progression toward squamous cell carcinoma was not altered, although those developing in clusterin-null mice were on average better differentiated. These data suggest that clusterin not only suppresses epithelial cell proliferation in vitro but also interferes with the promotion stage of skin carcinogenesis.
ISSN:0008-5472
1538-7445
DOI:10.1158/0008-5472.CAN-03-1953