Circulating chromogranin A in the assessment of patients with neuroendocrine tumours. A single institution experience

doi:10.1093/annonc/12.suppl_2.S73

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Annals of Oncology 12:S73-S77, 2001
© 2001 European Society for Medical Oncology

Circulating chromogranin A in the assessment of patients with neuroendocrine tumours. A single institution experience

M. Stivanello¹, A. Berruti¹, M. Torta¹, A. Termine², M. Tampellini¹, G. Gorzegno¹, A. Angeli¹ and L. Dogliotti¹

¹ Dipartimento di Scienze Cliniche e Biologiche Università di Torino, Oncologia Medica Orbassano (Torino), Italy
² Dipartimento di Scienze Cliniche e Biologiche Università di Torino, Medicina Interna, Azienda Ospedaliera San Luigi Orbassano (Torino), Italy

Correspondence to: Prof. Luigi Dogliotti Oncologia Medica Azienda Ospedaliera San Luigi Regione Gonzole 10 10043 Orbassano Italy E-mail: luigi.dogliotti{at}unito.it

Background: Chromogranin A (CgA) is a secretory protein presentin dense-core vesicles of neuroendocrine (NE) cells. Its ubiquitouspresence in NE tissues makes it a suitable circulating markerof neoplasms of NE origin.

Patients and methods: Plasma CgA was determined in 178 patientswith NE tumors and in 36 patients with non-endocrine malignancies.Circulating CgA was also serially evaluated in 39 NE cancerpatients with advanced disease submitted to systemic therapyand in 14 patients with no evidence of disease (NED).

Results: Supranormal CgA values were found in 81% of patientswith advanced NE tumors and in only 91% of NED cases. PlasmaCgA in patients with well differentiated NE tumors, such ascarcinoids, carcinoma of gastrointestinal tract, pheocromocytoma,pancreatic NE carcinoma (either functioning or not functioning),medullary thyroid carcinoma and NE tumors from various primarysites, was higher and more frequently elevated than in patientswith small-cell lung cancer (P < 0.001). Plasma CgA did notdiscriminate patients with NE from those with non NE neoplasmssince it was found elevated in 44% of the latter cases. PlasmaCgA pattern correlated with the disease response in patientssubmitted to cytotoxic treatment and with changes in clinicalsymptomathology in patients receiving somatostatin analogs.

Conclusions: Our data confirm that CgA is the best circulatingneuroendocrine marker available up to now available for themanagement of differentiated neuroendocrine malignancies irrespectiveof tumor location and functional status. CgA plasma levels couldalso identify the coexistence of neuroendocrine differentiationin the context of non-endocrine malignancies. Circulating CgAseems to be less useful in undifferentiated tumors such as small-celllung cancer.

chromogranin A, neuroendocrine tumours

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