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IgA With altered carbohydrate structure as a tumor-associated marker in serum of cancer patients

✍ Scribed by Jerry G. Henslee; Harry G. Rittenhouse; Matthew S. Matias; G. Michael Hass; Jay R. Schenck; Joseph T. Tomita


Publisher
John Wiley and Sons
Year
1988
Tongue
English
Weight
728 KB
Volume
2
Category
Article
ISSN
0887-8013

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✦ Synopsis


Serum lgAl contains 0-linked carbohydrate structures, whereas other immunoglobulins contain only N-linked structures. An assay was developed which detects lgAl by measuring the DGalP(1-3) DGalNAc structures 0-linked to the lgAl hinge region. Fifty percent of the serum specimens from cancer patients tested were elevated compared to 1% of the total normal serum specimens tested by this assay. The assay combines antibody (antihuman IgA) and lectin and measures the DGalp(1-3)DGalNAc structure in the lgAl molecule accessible to lectin binding. Three lectins were compared-the lectins from Bauhinia purpurea alba, Maclura pomifera, and peanut agglutinin (PNA). PNA in the assay discriminated best between serum specimens from normal subjects and cancer patients and was chosen as the lectin component in the assay. The anti-lgA-PNA enzyme immunoassay was evaluated in a retrospective study of can-cer patients. A panel of 845 serum specimens was tested and the results analyzed at three cutoff R values. The R value of a specimen is the ratio of the assay absorbance obtained for that test specimen with respect to the assay absorbance obtained for a pool of normal human sera. At a cutoff R value of 2.38, 1% normals and 26% benigns were elevated. The following cancer specimens had elevated R values: 52% lung, 60% colon, 43% head and neck, 35% breast, 64% kidney, 38% bladder, 43% prostate, 8% ovarian, and 67% pancreas. Further testing showed a significant percentage of serum specimens from patients with cirrhosis, pancreatitis, or ulcerative colitis also had elevated R values. No correlation of this assay was observed with CEA levels. The results suggest that the carbohydrate structure of serum lgAl is altered by malignancies and that measurement of this altered IgA may supplement CEA testing.


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