Pal, Santanu ; Chatterjee, Mitali ; Bhattacharya, Dilip Kumar ; Bandhyopadhyay, Santu ; Mandal, Chhabinath ; Mandal, Chitra (2001) O-acetyl sialic acid specific IgM in childhood acute lymphoblastic leukaemia Glycoconjugate Journal, 18 (7). pp. 529-537. ISSN 02820080
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Official URL: http://doi.org/10.1023/A:1019692329568
Related URL: http://dx.doi.org/10.1023/A:1019692329568
Abstract
Initial studies have revealed an enhanced surface expression of O-acetylated sialoglycoconjugates (O-AcSGs) on lymphoblasts concomitant with high titres of IgG in childhood Acute Lymphoblastic Leukaemia (ALL) (Mandal C, Chatterjee M, Sinha D, Br J Haematol 110, 801–12, 2000). In our efforts to identify disease specific markers for ALL, we have affinity-purified IgM directed against O-AcSGs that reacts with three disease specific O-AcSGs present on membrane proteins derived from peripheral blood mononuclear cells (PBMC) of ALL patients. Antibody specificity towards O-AcSGs was confirmed by selective binding to erythrocytes bearing surface O-AcSGs, decreased binding with de-O-acetylated BSM and following pretreatment with O-acetyl esterase. Competitive inhibition ELISA demonstrated a higher avidity of IgM for O-AcSG than IgG. Flow cytometry demonstrated the diagnostic potential of purified O-AcSA IgM as binding was specific with ALL patients and minimal with other haematological disorders and normal individuals. It therefore may be adopted as a non-invasive approach for detection of childhood ALL. Taken together, the data indicates that carbohydrate epitopes having terminal O-AcSA α2 → 6 GalNAc determinants induce disease specific IgG and IgM, potentially useful molecular markers for childhood ALL.
Item Type: | Article |
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Source: | Copyright of this article belongs to Springer Nature Switzerland AG |
Keywords: | acute lymphoblastic leukaemia (ALL);O-acetylated sialic acids;minimal residual disease;IgM;antibodies against O-acetylated sialic acids |
ID Code: | 133038 |
Deposited On: | 26 Dec 2022 05:39 |
Last Modified: | 26 Dec 2022 05:39 |
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