Clinical Profile of a New Monoclonal Antibody-Based Immunoassay for Tissue Polypeptide Antigen

Author:

Correale M.1,Arnberg H.2,Blockx P.3,Bombardieri E.4,Castelli M.5,Encabo G.6,Gion M.7,Klapdor R.8,Martin M.3,Nilsson S.2,Reutgen H.9,Ruggeri G.10,Safi F.11,Stegmuller M.12,Vering A.12

Affiliation:

1. Istituto Oncologico, Bari - Italy

2. Akademiska Sjukhuset Uppsala - Sweden

3. UIA Nuclear Medicine Department, Edegem - Belgium

4. Dipartimento di Medicina Nucleare, Istituto Nazionale per la Cura e lo Studio dei Tumori, Milano - Italy

5. Istituto dei Tumori “Regina Elena”, Centro Ricerche Sperimentali Oncologia, Roma - Italy

6. Valle Hebron Hospital, Barcelona - Spain

7. Centro Regionale per lo Studio degli Indicatori Biochimici di Tumore, Ospedale Civile, Venezia - Italy

8. Universitätskrankenhaus Eppendorf I. Medizinische Klinik, Hamburg - Germany

9. Fachkrankenhaus für Lungenheilkunde, Berlin - Germany

10. III Laboratorio Analisi Chimico-Cliniche, Spedali Civili, Brescia - Italy

11. Uniwide range of clinical apversitätsklinik Ulm-Safranberg, Chirurgische Abteilung, Ulm - Germany

12. Universitätsfrauenklinik, Frankfurt am Main - Germany

Abstract

Our preliminary evaluation of a new monoclonal antibody-based assay for tissue polypeptide antigen (TPA) has shown it to be clinically equivalent to the polyclonal antibody-based assay for TPA. The new assay (TPA-M) employs three monoclonal antibodies to epitopes on cytokeratins 8, 18 and 19. This multicenter, multinational study included 266 patients with newly diagnosed carcinomas of the lung, breast, large bowel and urinary bladder. TPA values from the two assays were compared with three other cytokeratin markers (TPS, CYFRA 21–1 and TPACyk) and with the established reference markers for these malignancies (CEA and NSE for lung, CA 15–3 for breast, CEA and CA 19–9 for colorectal tumors). Analysis of receiver operating characteristic (ROC) curves in lung, colorectal and bladder cancer showed similar sensitivities for the two assays, ranging from 50% to 80% with a specificity of 95%. In breast cancer all the markers studied showed poor sensitivity. However, TPA determination by either method could discriminate advanced stage (stages III and IV) from early stage disease (stages 0 to II). TPA showed similar discriminating ability in bladder cancer. On the basis of the results obtained in our patient series, it seems that of the cytokeratin markers studied, TPA and TPA-M are the most sensitive and offer a wide range of clinical applications.

Publisher

SAGE Publications

Subject

Cancer Research,Clinical Biochemistry,Oncology,Pathology and Forensic Medicine

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