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Literature DB >> 18655184

O-acetylation of GD3 prevents its apoptotic effect and promotes survival of lymphoblasts in childhood acute lymphoblastic leukaemia.

Kankana Mukherjee¹, Anil Kumar Chava, Chandan Mandal, Sailendra Nath Dey, Bernhard Kniep, Sarmila Chandra, Chitra Mandal.

Abstract

We have previously demonstrated induction of O-acetylated sialoglycoproteins on lymphoblasts of childhood acute lymphoblastic leukaemia (ALL). These molecules promote survival of lymphoblasts by preventing apoptosis. Although O-acetylated sialoglycoproteins are over expressed, the status of O-acetylation of gangliosides and their role in lymphoblasts survival remains to be explored in ALL patients. Here, we have observed enhanced levels of 9-O-acetylated GD3 (9-O-AcGD3) in the lymphoblasts of patients and leukaemic cell line versus disialoganglioside GD3 in comparison to the normal cells. Localization of GD3 and 9-O-AcGD3 on mitochondria of patient's lymphoblasts has been demonstrated by immuno-electron microscopy. The exogenous administration of GD3-induced apoptosis in lymphoblasts as evident from the nuclear fragmentation and sub G0/G1 apoptotic peak. In contrast, 9-O-AcGD3 failed to induce such apoptosis. We further explored the mitochondria-dependent pathway triggered during GD3-induced apoptosis in lymphoblasts. GD3 caused a time-dependent depolarization of mitochondrial membrane potential, release of cytochrome c and 7.4- and 8-fold increased in caspase 9 and caspase 3 activity respectively. However, under identical conditions, an equimolar concentration of 9-O-AcGD3 failed to induce similar effects. Interestingly, 9-O-AcGD3 protected the lymphoblasts from GD3-induced apoptosis when administered in equimolar concentrations simultaneously. In situ de-O-acetylation of 9-O-AcGD3 with sodium salicylate restores the GD3-responsiveness to apoptotic signals. Although both GD3 and 9-O-acetyl GD3 localize to mitochondria, these two structurally related molecules may play different roles in ALL-disease biology. Taken together, our results suggest that O-acetylation of GD3, like that of O-acetylated sialoglycoproteins, might be a general strategy adopted by leukaemic blasts towards survival in ALL. (c) 2008 Wiley-Liss, Inc.

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Year: 2008 PMID： 18655184 DOI： 10.1002/jcb.21867

Source DB: PubMed Journal: J Cell Biochem ISSN： 0730-2312 Impact factor: 4.429

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Cited

20 in total

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2. Human coronavirus-induced neuronal programmed cell death is cyclophilin d dependent and potentially caspase dispensable.

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Review 3. Glycosphingolipids and cell death: one aim, many ways.

Authors: Carmen Garcia-Ruiz; Albert Morales; José C Fernández-Checa
Journal: Apoptosis Date: 2015-05 Impact factor: 4.677

4. Targeting the GD3 acetylation pathway selectively induces apoptosis in glioblastoma.

Authors: Suzanne M Birks; John Owusu Danquah; Linda King; Reinhardt Vlasak; Dariusz C Gorecki; Geoffrey J Pilkington
Journal: Neuro Oncol Date: 2011-07-31 Impact factor: 12.300

5. Identification of 9-O-acetyl-N-acetylneuraminic acid (Neu5,9Ac₂) as main O-acetylated sialic acid species of GD2 in breast cancer cells.

Authors: Sumeyye Cavdarli; Justine H Dewald; Nao Yamakawa; Yann Guérardel; Mickaël Terme; Jean-Marc Le Doussal; Philippe Delannoy; Sophie Groux-Degroote
Journal: Glycoconj J Date: 2019-01-05 Impact factor: 2.916

6. A monoclonal antibody to O-acetyl-GD2 ganglioside and not to GD2 shows potent anti-tumor activity without peripheral nervous system cross-reactivity.

Authors: Nidia Alvarez-Rueda; Ariane Desselle; Denis Cochonneau; Tanguy Chaumette; Béatrice Clemenceau; Stéphanie Leprieur; Gwenola Bougras; Stéphane Supiot; Jean-Marie Mussini; Jacques Barbet; Julie Saba; François Paris; Jacques Aubry; Stéphane Birklé
Journal: PLoS One Date: 2011-09-22 Impact factor: 3.240

O-acetylation of GD3 prevents its apoptotic effect and promotes survival of lymphoblasts in childhood acute lymphoblastic leukaemia.

1. The role of 9-O-acetylated ganglioside D3 (CD60) and {alpha}4{beta}1 (CD49d) expression in predicting the survival of patients with Sezary syndrome.

2. Human coronavirus-induced neuronal programmed cell death is cyclophilin d dependent and potentially caspase dispensable.

Review 3. Glycosphingolipids and cell death: one aim, many ways.

4. Targeting the GD3 acetylation pathway selectively induces apoptosis in glioblastoma.

5. Identification of 9-O-acetyl-N-acetylneuraminic acid (Neu5,9Ac₂) as main O-acetylated sialic acid species of GD2 in breast cancer cells.

6. A monoclonal antibody to O-acetyl-GD2 ganglioside and not to GD2 shows potent anti-tumor activity without peripheral nervous system cross-reactivity.

7. 9-O-Acetylation of sialic acids is catalysed by CASD1 via a covalent acetyl-enzyme intermediate.

Review 8. Cancer-Associated Glycosphingolipids as Tumor Markers and Targets for Cancer Immunotherapy.

9. O-acetylated N-acetylneuraminic acid as a novel target for therapy in human pre-B acute lymphoblastic leukemia.

Review 10. Sphingolipids: key regulators of apoptosis and pivotal players in cancer drug resistance.