Detection of High Mobility Group I HMGI(Y) Protein in the Diagnosis of Thyroid Tumors: HMGI(Y) Expression Represents a Potential Diagnostic Indicator of Carcinoma
Articolo
Data di Pubblicazione:
1998
Abstract:
Hyperplastic or neoplastic proliferativi' lésions of thyroid follicular
epithelium consist of a spectrum, ranging from nodular hyperplasia to
undifferentiated (anaplastic) carcinoma, and usually present as palpable
thyroid nodules. Thyroid nodules are a common occurrence in the general
population, but only a small proportion of them are eventually diagnosed
as carcinoma. The difficulty in objectively identifying those thyroid nod
ules that are malignant to avoid unnecessary surgery, combined with the
range and effectiveness of the available therapeutic options in those
patients who do, indeed, have thyroid carcinoma, has prompted the search
for tumor markers and prognostic indicators. The high mobility group I
(HMGI) proteins represent a class of nuclear proteins involved in the
regulation of chromatin structure and function. HMGI(Y), one of the
members of this class, is expressed at high levels during embryogenesis
and in malignant tumors but at generally low levels in normal adult
human tissues. Previous work on a limited number of thyroid samples
suggested that the detection of the HMGI(Y) proteins may provide a
clinically useful diagnostic tool. To verify this assumption, we analyzed
HMGI(Y) expression by a combination of immunohistochemistry and
reverse transcription-PCR in 358 thyroid tissue samples that were repre
sentative of the spectrum of thyroid tumor pathology. HMGI(Y) was
detectable in 18 of 19 follicular carcinomas, 92 of 96 papillary carcinomas,
and 11 of 11 undifferentiated (anaplastic) carcinomas but in only 1 of 20
hyperplastic nodules, 44 of 200 follicular adenomas, and 0 of 12 normal
tissue samples. The correlation between HMGI(Y) expression and a diag
nosis of carcinoma was highly significant (P < 0.0001). We also prospectively
collected and analyzed for HMGI(Y) expression by immunohisto
chemistry and reverse transcription-PCR in 12 fine needle aspiration
biopsies from 10 patients who subsequently underwent surgical removal
of a solitary thyroid nodule. HMGI(Y) was detectable only in the four fine
needle aspiration biopsies, corresponding to the thyroid nodules that were
definitively diagnosed as carcinomas after surgery (two follicular carci
nomas and two papillary carcinomas). The remaining eight samples (six
follicular adenomas and two samples consisting of normal follicular cells)
were negative. The findings of this study confirm the differential expres
sion of HMGl(Y) in thyroid neoplasia and indicate the HMGI(Y) protein
as a potential marker for thyroid carcinoma.
Tipologia CRIS:
01.01 Articolo in rivista
Elenco autori:
Fusco, Alfredo; Fedele, Monica
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