Expression of the small cell carcinoma antigens of cluster-5 and cluster-5A in primary lung tumours

Maier, Andrea B.; Schmidt, Ulrike; Waibel, Robert; Hartung, Wolfgang; Stahel, R.

doi:10.1038/bjc.1989.144

Cited by 11 publications

(11 citation statements)

References 10 publications

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“…This antigen could be an appropriate target for the development of ricin A chain ITs with therapeutic potential designed to react with a high proportion of human SCLC tumours. The cluster 5A antigen recognised by SWA20 is a sialoglycoprotein that is highly selectively expressed by human SCLC and is present in about 50% of primary SCLC tumours Maier et al, 1989). Our studies indicate that ricin A chain ITs directed to this antigen could exert selective cytotoxic effects against the fraction of tumour cells that express the target antigen.…”

Section: Resultsmentioning

confidence: 82%

Cytotoxic activity of ricin A chain immunotoxins recognising cluster 1, w4 and 5A antigens associated with human small cell lung cancer

1991

Lung Cancer

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Section: Resultsmentioning

confidence: 82%

Cytotoxic activity of ricin A chain immunotoxins recognising cluster 1, w4 and 5A antigens associated with human small cell lung cancer

1991

Lung Cancer

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“…SGP,-,,, is a membrane sialoglycoprotein with high selectivity of expression in small-cell carcinoma, and little or no expression in normal tissues (Stahel et al, 1986;Maier et al, 1989;Bernal et al, 1988). To facilitate investigations on the structural relationship between antigen and anti-idiotype and to have the high specificity of a uniform reagent, a monoclonal approach was chosen to obtain a P-type anti-idiotypic antibody which could substitute for the antigen.…”

Section: Discussionmentioning

confidence: 98%

Monoclonal anti‐idiotypic antibody mimicking a tumor‐associated sialoglycoprotein antigen induces humoral immune response against human small‐cell lung carcinoma

Barth

Waibel

Stahel

1989

Intl Journal of Cancer

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We have previously described the tumor-associated sialoglycoprotein antigen sGP90-135 defined by the murine LAM8 MAb. The antigen is characterized by strong membrane expression in a proportion of small-cell carcinomas of the lung, but little or no expression on normal tissues of epithelial or neural origin or on blood cells. With the aim of obtaining anti-idiotypic antibodies which might be useful as surrogates for sGP90-135 in vaccination studies, LOU rats were immunized with LAM8 MAb and their spleen cells fused with Y3 rat myeloma cells. The LY8-229 hybrid was selected by an anti-idiotype competition radioimmunoassay on antigen-positive target cells. LY8-229 was shown to be a rat IgG1 with high specificity for LAM8 combining site. Solubilized small-cell carcinoma extract, as well as antibody SEN16, which recognizes the same tumor-associated antigen sGP90-135, selectively inhibited 125I-LY8-229 binding to LAM8. Serum from BALB/c mice and DA rats immunized with anti-idiotypic antibody LY8-229 showed reactivity with antigen-positive target cell lines, but not with antigen-negative control cell lines. The induction of a specific immune response in 2 different species by the anti-idiotypic antibody LY8-229 suggests that LY8-229 bears the internal image of the antigen sGP90-135 and that it might be a candidate for immunotherapy trials in cancer patients.

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“…Both cluster-5 and -5A antigens are strongly expressed on 45%-50% of SCLC tumours and co-ordinately expressed in about 35% [5]. Expression of these antigens is practically absent from other pulmonary and extrapulmonary tumours and occurs only at low levels in bronchial epithelium and other normal tissues [5,10].…”

Section: Introductionmentioning

confidence: 99%

Cytotoxic properties of a ricin A chain immunotoxin recognising the cluster-5A antigen associated with human small-cell lung cancer

Derbyshire

Stahel

Wawrzynczak

1992

Cancer Immunol Immunother

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The cytotoxic properties of a ricin A chain immunotoxin made with the mouse monoclonal antibody SWA20, recognising a family of sialoglycoprotein antigens selectively expressed by human small-cell lung cancer (SCLC), were examined using a panel of tumour cell lines in tissue culture. SWA20-ricin-A-chain was selectively toxic to the SW2, NCI-H69 and GLC-8 SCLC cell lines, inhibiting the incorporation of [3H]leucine by 50% at a concentration of 0.2-2 nM, but had no selective activity against the NCI-H23 and NCI-H125 lung adenocarcinoma or the control CEM T-lymphoblastoid cell lines. The SWA20 immunotoxin intoxicated the SW2 cell line rapidly, inhibiting [3H]leucine incorporation by 50% within 2 h compared with 0.5 h for ricin. Analysis of the effects of SWA20-ricin-A-chain on the growth of SW2 cells using a limiting-dilution clonogenic assay revealed that the immunotoxin could eliminate 95% of clonogenic malignant cells. Although SWA20-ricin-A-chain was found to be rapidly active against the majority of tumour cells, its action was limited by the presence of insensitive cells expressing low levels of the target antigen.

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Expression of the small cell carcinoma antigens of cluster-5 and cluster-5A in primary lung tumours

Cited by 11 publications

References 10 publications

Cytotoxic activity of ricin A chain immunotoxins recognising cluster 1, w4 and 5A antigens associated with human small cell lung cancer

Cytotoxic activity of ricin A chain immunotoxins recognising cluster 1, w4 and 5A antigens associated with human small cell lung cancer

Monoclonal anti‐idiotypic antibody mimicking a tumor‐associated sialoglycoprotein antigen induces humoral immune response against human small‐cell lung carcinoma

Cytotoxic properties of a ricin A chain immunotoxin recognising the cluster-5A antigen associated with human small-cell lung cancer

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