Medullary thyroid microcarcinoma: A clinicopathologic retrospective study of 38 patients with no prior familial disease

Thirty-eight patients (25 women, 13 men; mean age, 57.8 [32 to 91]) showing one or more medullary thyroid microcarcinomas (ie, < 1 cm), with no prior MEN II or medullary thyroid carcinoma history in their family, were reviewed. Follow-up was available for 29 patients (mean, 53.6 months [1 to 147]...

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Veröffentlicht in:Human pathology 1999-08, Vol.30 (8), p.957-963
Hauptverfasser: Guyétant, Serge, Dupre, Florence, Bigorgne, Jean-Claude, Franc, Brigitte, Dutrieux-Berger, Nicole, Lecomte-Houcke, Martine, Patey, Martine, Caillou, Bernard, Viennet, Gabriel, Guerin, Olivier, Saint-Andre, Jean-Paul
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Sprache:eng
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Zusammenfassung:Thirty-eight patients (25 women, 13 men; mean age, 57.8 [32 to 91]) showing one or more medullary thyroid microcarcinomas (ie, < 1 cm), with no prior MEN II or medullary thyroid carcinoma history in their family, were reviewed. Follow-up was available for 29 patients (mean, 53.6 months [1 to 147]). 21 patients (72.4%) are alive and free of disease, four patients (13.8%) died during follow-up without disease, 2 patients are alive with disease (local recurrence and persistent hypercalcitoninemia) after 80 and 99 months, respectively, and 2 patients died of disease after 24 and 46 months. Most tumors were incidental pathological findings (19 of 38) or were discovered by systematic blood calcitonin measurement for a nodular thyroid disease (15 of 38). Only the four patients who had an unfavorable outcome were symptomatic cases (palpable micro-MTC, diarrhea, cervical lymph node metastasis and pulmonary metastatic disease). The two patients with metastatic disease at diagnosis died during follow-up. In univariate analysis, a symptomatic medullary thyroid carcinoma was a strong predictor of an unfavourable outcome ( p < .00008), as were the preoperative calcitonin level ( P = .007) and an elevated postoperative calcitonin level ( P = .004). Among 30 histopathological criteria, only the presence of amyloid correlated with an unfavorable outcome ( P = .018).
ISSN:0046-8177
1532-8392
DOI:10.1016/S0046-8177(99)90250-2