Expression of Neural Cell Adhesion Molecule-related Sialoglycoprotein in Small Cell Lung Cancer and Neuroblastoma Cell Lines H69 and CHP-212

Overview

Journal Cancer Res

Specialty Oncology

Date 1990 Feb 15

PMID 2153450

Citations 40

Authors

C E Moolenaar

E J Muller

D J Schol

C G Figdor

E Bock

D Bitter-Suermann

R J Michalides

Affiliations

Soon will be listed here.

Abstract

Monoclonal antibodies (MAbs) 123C3 and 123A8 generated against a membrane preparation of a small cell lung carcinoma (SCLC) specimen recognize not only SCLC and bronchial carcinoids but also a significant portion of non-small cell lung carcinomas (non-SCLC) of various histological types. Together with 13 other monoclonal antibodies, which show preference for SCLC, they have been ranked as SCLC cluster 1 (SC-1) Mabs. In this study we show that SC-1 MAbs are directed against a restricted number of epitopes, and that SC-1 MAbs and a polyclonal antiserum directed against the neural cell adhesion molecule (NCAM) recognize identical glycoproteins, indicating that SC-1 antigens are closely related to or identical with NCAM. Long polysialic acid units composed of alpha-(2,8)-linked N-acetylneuraminic acid units, which in mammals are found exclusively on NCAM, were present on SC-1 antigens in SCLC. This provides further evidence that SC-1 MAbs recognize NCAM. The SC-1 antigens in the SCLC cell line H69 were present in two forms, NCAM-containing alpha-(2,8)-polysialic acid units identified by antiserum 735, the NCAM-H form, and the less sialylated NCAM-L form. The NCAM-H form consisted of diffusely migrating sialoglycoproteins with a molecular weight of 200,000-250,000, which resolved after neuraminidase treatment into two proteins with molecular weights of 140,000 and 180,000. Since the NCAM-H form is expressed in the lung tumor type with a poor prognosis, our results suggest that NCAM might be implicated in the invasive behavior of these NCAM-positive lung tumors.

Citing Articles

Small Cell Lung Cancer Neuronal Features and Their Implications for Tumor Progression, Metastasis, and Therapy.

Hartmann G, Sage J Mol Cancer Res. 2024; 22(9):787-795.

PMID: 38912893 PMC: 11374474. DOI: 10.1158/1541-7786.MCR-24-0265.

Glycation Leads to Increased Polysialylation and Promotes the Metastatic Potential of Neuroblastoma Cells.

Scheer M, Bork K, Simon F, Nagasundaram M, Horstkorte R, Gnanapragassam V Cells. 2020; 9(4).

PMID: 32252464 PMC: 7226752. DOI: 10.3390/cells9040868.

Noncatalytic Endosialidase Enables Surface Capture of Small-Cell Lung Cancer Cells Utilizing Strong Dendrimer-Mediated Enzyme-Glycoprotein Interactions.

Hsu H, Palka-Hamblin H, Bhide G, Myung J, Cheong M, Colley K Anal Chem. 2018; 90(6):3670-3675.

PMID: 29473730 PMC: 7038578. DOI: 10.1021/acs.analchem.8b00427.

Is Polysialylated NCAM Not Only a Regulator during Brain Development But also during the Formation of Other Organs?.

Galuska C, Lutteke T, Galuska S Biology (Basel). 2017; 6(2).

PMID: 28448440 PMC: 5485474. DOI: 10.3390/biology6020027.

Glycobiology of neuroblastoma: impact on tumor behavior, prognosis, and therapeutic strategies.

Berois N, Osinaga E Front Oncol. 2014; 4:114.

PMID: 24904828 PMC: 4033258. DOI: 10.3389/fonc.2014.00114.