monensin and Niemann-Pick-Diseases

monensin has been researched along with Niemann-Pick-Diseases* in 2 studies

Other Studies

2 other study(ies) available for monensin and Niemann-Pick-Diseases

Article	Year
Cholesterol movement in Niemann-Pick type C cells and in cells treated with amphiphiles. The Journal of biological chemistry, 2000, Jun-09, Volume: 275, Issue:23 Cholesterol accumulates to massive levels in cells from Niemann-Pick type C (NP-C) patients and in cells treated with class 2 amphiphiles that mimic NP-C disease. This behavior has been attributed to the failure of cholesterol released from ingested low density lipoproteins to exit the lysosomes. However, we now show that the rate of movement of cholesterol from lysosomes to plasma membranes in NP-C cells is at least as great as normal, as was also found previously for amphiphile-treated cells. Furthermore, the lysosomes in these cells filled with plasma membrane cholesterol in the absence of lipoproteins. In addition, we showed that the size of the endoplasmic reticulum cholesterol pool and the set point of the homeostatic sensor of cell cholesterol were approximately normal in NP-C cells. The plasma membrane cholesterol pools in both NP-C and amphiphile-treated cells were also normal. Furthermore, the build up of cholesterol in NP-C lysosomes was not a physiological response to cholesterol overload. Rather, it appeared that the accumulation in NP-C lysosomes results from an imbalance in the brisk flow of cholesterol among membrane compartments. In related experiments, we found that NP-C cells did not respond to class 2 amphiphiles (e.g. trifluoperazine, imipramine, and U18666A); these agents may therefore act directly on the NPC1 protein or on its pathway. Finally, we showed that the lysosomal cholesterol pool in NP-C cells was substantially and preferentially reduced by incubating cells with the oxysterols, 25-hydroxycholesterol and 7-ketocholesterol; these findings suggest a new pharmacological approach to the treatment of NP-C disease. Topics: Androstenes; Anticholesteremic Agents; Cell Line; Cell Membrane; Cells, Cultured; Cholesterol; Culture Media; Endoplasmic Reticulum; Fibroblasts; Homeostasis; Humans; Imipramine; Kinetics; Lipoproteins; Lysosomes; Membrane Lipids; Monensin; Niemann-Pick Diseases; Skin; Trifluoperazine	2000
Impaired cholesterol esterification in cultured skin fibroblasts from patients with I-cell disease and pseudo-Hurler polydystrophy. Biochemistry international, 1989, Volume: 18, Issue:6 Cholesterol esterification was examined in cultured skin fibroblasts from patients with I-cell disease and pseudo-Hurler polydystrophy by incubating cells pretreated without fetal calf serum for 48h, with (14C) cholesterol for 24h. Impaired cholesterol esterification was found in these cells and free cholesterol was accumulated in plasma membrane and Golgi fractions. This impairment was also induced in control cells by adding leupeptin (20 micrograms/ml) or monensin (2 micrograms/ml). These findings suggest the importance of the role of lysosomes for esterification of cholesterol and give a hint as to the basic defect in type C Niemann-Pick disease. Topics: Autoradiography; Cell Fractionation; Cells, Cultured; Cholesterol Esters; Esterification; Fibroblasts; Humans; Leupeptins; Lysosomes; Monensin; Mucolipidoses; Niemann-Pick Diseases	1989

Article

Year

Cholesterol movement in Niemann-Pick type C cells and in cells treated with amphiphiles.

The Journal of biological chemistry, 2000, Jun-09, Volume: 275, Issue:23

Cholesterol accumulates to massive levels in cells from Niemann-Pick type C (NP-C) patients and in cells treated with class 2 amphiphiles that mimic NP-C disease. This behavior has been attributed to the failure of cholesterol released from ingested low density lipoproteins to exit the lysosomes. However, we now show that the rate of movement of cholesterol from lysosomes to plasma membranes in NP-C cells is at least as great as normal, as was also found previously for amphiphile-treated cells. Furthermore, the lysosomes in these cells filled with plasma membrane cholesterol in the absence of lipoproteins. In addition, we showed that the size of the endoplasmic reticulum cholesterol pool and the set point of the homeostatic sensor of cell cholesterol were approximately normal in NP-C cells. The plasma membrane cholesterol pools in both NP-C and amphiphile-treated cells were also normal. Furthermore, the build up of cholesterol in NP-C lysosomes was not a physiological response to cholesterol overload. Rather, it appeared that the accumulation in NP-C lysosomes results from an imbalance in the brisk flow of cholesterol among membrane compartments. In related experiments, we found that NP-C cells did not respond to class 2 amphiphiles (e.g. trifluoperazine, imipramine, and U18666A); these agents may therefore act directly on the NPC1 protein or on its pathway. Finally, we showed that the lysosomal cholesterol pool in NP-C cells was substantially and preferentially reduced by incubating cells with the oxysterols, 25-hydroxycholesterol and 7-ketocholesterol; these findings suggest a new pharmacological approach to the treatment of NP-C disease.

Topics: Androstenes; Anticholesteremic Agents; Cell Line; Cell Membrane; Cells, Cultured; Cholesterol; Culture Media; Endoplasmic Reticulum; Fibroblasts; Homeostasis; Humans; Imipramine; Kinetics; Lipoproteins; Lysosomes; Membrane Lipids; Monensin; Niemann-Pick Diseases; Skin; Trifluoperazine

2000

Impaired cholesterol esterification in cultured skin fibroblasts from patients with I-cell disease and pseudo-Hurler polydystrophy.

Biochemistry international, 1989, Volume: 18, Issue:6

Cholesterol esterification was examined in cultured skin fibroblasts from patients with I-cell disease and pseudo-Hurler polydystrophy by incubating cells pretreated without fetal calf serum for 48h, with (14C) cholesterol for 24h. Impaired cholesterol esterification was found in these cells and free cholesterol was accumulated in plasma membrane and Golgi fractions. This impairment was also induced in control cells by adding leupeptin (20 micrograms/ml) or monensin (2 micrograms/ml). These findings suggest the importance of the role of lysosomes for esterification of cholesterol and give a hint as to the basic defect in type C Niemann-Pick disease.

Topics: Autoradiography; Cell Fractionation; Cells, Cultured; Cholesterol Esters; Esterification; Fibroblasts; Humans; Leupeptins; Lysosomes; Monensin; Mucolipidoses; Niemann-Pick Diseases

1989