BIOMAT Database Logo BIOMAT Database Logo

The metabolic processing of glycosphingolipids in HT-29 cells is differentiation-dependent. 1994

J J Houri, and A Falbo, and G Vignali, and P Codogno, and R Ghidoni
INSERM U410, Paris, France.

The metabolism of two radiolabelled glycosphingolipids, lactosylceramide and GM1 ganglioside, in differentiated and undifferentiated HT-29 cells is reported. Both lactosylceramide and GM1 ganglioside were demonstrated to be extensively catabolized in undifferentiated cells, as deduced by the relative amount of the compounds formed along the degradative pathway. Conversely, in differentiated cells both precursors were utilized as substrates for sugar-chain elongation. Furthermore we were unable to detect any significant difference in the activity of CMP-NeuAc:GM1 alpha 2-->3 sialyltransferase, a Golgi key enzyme for the glycosylation of glycosphingolipids, between the two cell populations. Taken together with our previous results on the differentiation-dependent trimming of high-mannose N-linked glycoproteins in HT-29 cells, one can suggest that common steps control the anabolic/catabolic balance of these two classes of glycoconjugates as a function of differentiation.

UI MeSH Term Description Entries
D007790 Lactosylceramides Glycosphingolipids which contain as their polar head group a lactose moiety bound in glycosidic linkage to the hydroxyl group of ceramide. Their accumulation in tissue, due to a defect in lactosylceramide beta-galactosidase, is the cause of lactosylceramidosis. Lactosyl Ceramides,Ceramides, Lactosyl
D002454 Cell Differentiation Progressive restriction of the developmental potential and increasing specialization of function that leads to the formation of specialized cells, tissues, and organs. Differentiation, Cell,Cell Differentiations,Differentiations, Cell
D003110 Colonic Neoplasms Tumors or cancer of the COLON. Cancer of Colon,Colon Adenocarcinoma,Colon Cancer,Cancer of the Colon,Colon Neoplasms,Colonic Cancer,Neoplasms, Colonic,Adenocarcinoma, Colon,Adenocarcinomas, Colon,Cancer, Colon,Cancer, Colonic,Cancers, Colon,Cancers, Colonic,Colon Adenocarcinomas,Colon Cancers,Colon Neoplasm,Colonic Cancers,Colonic Neoplasm,Neoplasm, Colon,Neoplasm, Colonic,Neoplasms, Colon
D005677 G(M1) Ganglioside A specific monosialoganglioside that accumulates abnormally within the nervous system due to a deficiency of GM1-b-galactosidase, resulting in GM1 gangliosidosis. GM1 Ganglioside,Monosialosyl Tetraglycosyl Ceramide,GM1a Monosialoganglioside,Ceramide, Monosialosyl Tetraglycosyl,Ganglioside, GM1,Monosialoganglioside, GM1a,Tetraglycosyl Ceramide, Monosialosyl
D006028 Glycosphingolipids Lipids containing at least one monosaccharide residue and either a sphingoid or a ceramide (CERAMIDES). They are subdivided into NEUTRAL GLYCOSPHINGOLIPIDS comprising monoglycosyl- and oligoglycosylsphingoids and monoglycosyl- and oligoglycosylceramides; and ACIDIC GLYCOSPHINGOLIPIDS which comprises sialosylglycosylsphingolipids (GANGLIOSIDES); SULFOGLYCOSPHINGOLIPIDS (formerly known as sulfatides), glycuronoglycosphingolipids, and phospho- and phosphonoglycosphingolipids. (From IUPAC's webpage) Asialoganglioside,Asialogangliosides,Glycosphingolipid,Sphingoglycolipid,Sphingoglycolipids
D006031 Glycosylation The synthetic chemistry reaction or enzymatic reaction of adding carbohydrate or glycosyl groups. GLYCOSYLTRANSFERASES carry out the enzymatic glycosylation reactions. The spontaneous, non-enzymatic attachment of reducing sugars to free amino groups in proteins, lipids, or nucleic acids is called GLYCATION (see MAILLARD REACTION). Protein Glycosylation,Glycosylation, Protein
D006056 Golgi Apparatus A stack of flattened vesicles that functions in posttranslational processing and sorting of proteins, receiving them from the rough ENDOPLASMIC RETICULUM and directing them to secretory vesicles, LYSOSOMES, or the CELL MEMBRANE. The movement of proteins takes place by transfer vesicles that bud off from the rough endoplasmic reticulum or Golgi apparatus and fuse with the Golgi, lysosomes or cell membrane. (From Glick, Glossary of Biochemistry and Molecular Biology, 1990) Golgi Complex,Apparatus, Golgi,Complex, Golgi
D006801 Humans Members of the species Homo sapiens. Homo sapiens,Man (Taxonomy),Human,Man, Modern,Modern Man
D012799 Sialyltransferases A group of enzymes with the general activity CMP-N-acetylneuraminate:acceptor N-acetylneuraminyl transferase. They catalyze the transfer of N-ACETYLNEURAMINIC ACID from CMP-N-ACETYLNEURAMINIC ACID to an acceptor, which is usually the terminal sugar residue of an oligosaccharide, a glycoprotein, or a glycolipid. Glycoprotein Sialyltransferases,Glycosyltransferase Family 29,Sialyltransferase,Ectosialyltransferase,Glycoprotein Sialyltransferase,Sialyltransferase, Glycoprotein,Sialyltransferases, Glycoprotein
D014407 Tumor Cells, Cultured Cells grown in vitro from neoplastic tissue. If they can be established as a TUMOR CELL LINE, they can be propagated in cell culture indefinitely. Cultured Tumor Cells,Neoplastic Cells, Cultured,Cultured Neoplastic Cells,Cell, Cultured Neoplastic,Cell, Cultured Tumor,Cells, Cultured Neoplastic,Cells, Cultured Tumor,Cultured Neoplastic Cell,Cultured Tumor Cell,Neoplastic Cell, Cultured,Tumor Cell, Cultured

Related Publications

J J Houri, and A Falbo, and G Vignali, and P Codogno, and R Ghidoni
Energy state in HT-29 cells is linked to differentiation.
April 1997, In vitro cellular & developmental biology. Animal,
J J Houri, and A Falbo, and G Vignali, and P Codogno, and R Ghidoni
Processing of asparagine-linked oligosaccharides is an early biochemical marker of the enterocytic differentiation of HT-29 cells.
September 1989, Journal of cellular biochemistry,
J J Houri, and A Falbo, and G Vignali, and P Codogno, and R Ghidoni
The metabolism of sphingo(glyco)lipids is correlated with the differentiation-dependent autophagic pathway in HT-29 cells.
April 1996, European journal of biochemistry,
J J Houri, and A Falbo, and G Vignali, and P Codogno, and R Ghidoni
The posttranslational processing of sucrase-isomaltase in HT-29 cells is a function of their state of enterocytic differentiation.
May 1987, The Journal of cell biology,
J J Houri, and A Falbo, and G Vignali, and P Codogno, and R Ghidoni
The N-glycan processing in HT-29 cells is a function of their state of enterocytic differentiation. Evidence for an atypical traffic associated with change in polypeptide stability in undifferentiated HT-29 cells.
November 1991, The Journal of biological chemistry,
J J Houri, and A Falbo, and G Vignali, and P Codogno, and R Ghidoni
Butyrate rapidly induces growth inhibition and differentiation in HT-29 cells.
June 1993, Cell growth & differentiation : the molecular biology journal of the American Association for Cancer Research,
J J Houri, and A Falbo, and G Vignali, and P Codogno, and R Ghidoni
Maintenance of differentiation capacity of HT-29 cells after radiation exposure.
March 2005, International journal of radiation biology,
J J Houri, and A Falbo, and G Vignali, and P Codogno, and R Ghidoni
[Expression of O-glycans during enterocytic differentiation of HT-29 cells].
January 1989, Comptes rendus de l'Academie des sciences. Serie III, Sciences de la vie,
J J Houri, and A Falbo, and G Vignali, and P Codogno, and R Ghidoni
Metallothionein 1G promotes the differentiation of HT-29 human colorectal cancer cells.
May 2017, Oncology reports,
J J Houri, and A Falbo, and G Vignali, and P Codogno, and R Ghidoni
Increased phospholipase D activity in butyrate-induced differentiation of HT-29 cells.
October 1998, Cancer letters,
Copied contents to your clipboard!