G Lüben scite author profile

Three murine monoclonal antibodies (MAbs) reactive to different epitopes on CEA were selected according to their ability to bind to various human tissue sections. The most selective MAb, BW 431/31, bound to the majority of colon carcinomas but only faintly to normal colon mucosa. In addition to the tissues stained by MAb BW 431/31, MAb BW 250/183 reacted with granulocytes, colon mucosa and faintly with pancreatic ducts. The third MAb, BW 374/14, reacted with granulocytes, colon mucosa, strongly with pancreatic ducts and with alveolar and bronchial epithelium. The antigenic determinants recognized by the 3 MAbs in human tissue sections were resistant to formaldehyde fixation and paraffin embedding as well as to periodic acid oxidation and neuraminidase treatment. The last two treatments suggest that the epitopes are protein in nature. Using MAb affinity chromatography, 3 antigen preparations were isolated from a human colon carcinoma xenograft with an approximate molecular weight of 180 kd. These preparations were shown to bear the epitopes from each of the MAbs and from a polyclonal antiserum specific for purified CEA. Furthermore, the ability of MAb BW 431/31 to localize its antigenic determinant in vivo on a human colon carcinoma xenograft is evaluated and its possible application in the patient is suggested.

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The Discovery, Isolation, Elucidation of Structure, and Synthesis of Antamanide

Wieland

Lüben

Ottenheym

et al. 1968

Angew. Chem. Int. Ed. Engl.

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Antamanide is the name we have given to a constituent of the fungus Amanita phalloides. This substance counteracts the lethal action of the Amanita toxins phalloidine and u-amanatine if administered to the white mouse before, or simultaneously with, the poisons. Its concentration in the fungus is, however, so low that the toxic action of the latter predominates. Antamanide is a cyclic decapeptide formed from the L-amino acids alanine, phenylalanine, proline, and valine in the molar ratio 1:4:4:f. The amino-acid sequence was determined by a combination of gas chromatography and mass spectrometry. The structural formula assigned was confirmed by synthesis according to a classic route of peptide chemistry.

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Radioimmunoassay of SP₁(Pregnancy-specificβ₁-glycoprotein) in maternal blood and in amniotic fluid in normal and pathologic pregnancies

Würz¹,

Geiger²,

Künzig³

et al. 1981

Journal of Perinatal Medicine

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A monoclonal antibody with binding and inhibiting activity towards human pancreatic carcinoma cells

Bosslet

Kern

Kanzy

et al. 1986

Cancer Immunol Immunother

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The murine monoclonal antibody (MAb) BW 494 was characterized in relation to its tissue specificity, the epitope recognized, in vitro and in vivo radiolocalization and its potential to mediate antibody dependent cellular cytotoxicity (ADCC) and complement mediated cytolysis (CMC). The MAb defined carbohydrate epitope located on a greater than 200 k daltons glycoprotein was mainly expressed on the majority of well differentiated adenocarcinomas of the pancreas. Furthermore, the epitope is accessible to MAb BW 494 in vivo, allowing an enrichment of radioactive antibody at the tumor site in nude mice. Additionally, MAb BW 494 is able to use human peripheral blood lymphocytes as effector cells for ADCC reactions against appropriate tumor target cells in vitro. In contrast, the antibody does not mediate human or rabbit CMC.

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Quantitative considerations supporting the irrelevance of circulating serum CEA for the immunoscintigraphic visualization of CEA expressing carcinomas

Bosslet

Steinsträsser²,

Schwarz³

et al. 1988

Eur J Nucl Med

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Starting from the phenomenon that the amount of circulating CEA in patients' sera did not significantly influence immunoscintigraphic visualization of CEA expressing tumors, we built up an in vitro model to explain this phenomenon. Blocking experiments in this model system showed that the CEA specific MAbs BW 431/26 and BW 431/31 could not be inhibited in their binding to cell associated CEA, if they were preincubated with a 20 molar excess of serum CEA. In contrast, the CEA-NCA cross reactive MAbs could be inhibited in their binding to tumor associated CEA under identical conditions. These data combined with western blotting analysis of patients' sera and affinity constant determinations argue that conformational changes in serum CEA cause a decreased affinity of the CEA specific MAbs to serum CEA allowing a preferential binding to tumor associated CEA.

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G Lüben

Immunohistochemical localization and molecular characteristics of three monoclonal antibody‐defined epitopes detectable on carcinoembryonic antigen (CEA)

The Discovery, Isolation, Elucidation of Structure, and Synthesis of Antamanide

Radioimmunoassay of SP₁(Pregnancy-specificβ₁-glycoprotein) in maternal blood and in amniotic fluid in normal and pathologic pregnancies

A monoclonal antibody with binding and inhibiting activity towards human pancreatic carcinoma cells

Quantitative considerations supporting the irrelevance of circulating serum CEA for the immunoscintigraphic visualization of CEA expressing carcinomas

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G Lüben

Immunohistochemical localization and molecular characteristics of three monoclonal antibody‐defined epitopes detectable on carcinoembryonic antigen (CEA)

The Discovery, Isolation, Elucidation of Structure, and Synthesis of Antamanide

Radioimmunoassay of SP1(Pregnancy-specificβ1-glycoprotein) in maternal blood and in amniotic fluid in normal and pathologic pregnancies

A monoclonal antibody with binding and inhibiting activity towards human pancreatic carcinoma cells

Quantitative considerations supporting the irrelevance of circulating serum CEA for the immunoscintigraphic visualization of CEA expressing carcinomas

Contact Info

Product

Resources

About

Radioimmunoassay of SP₁(Pregnancy-specificβ₁-glycoprotein) in maternal blood and in amniotic fluid in normal and pathologic pregnancies