CD99 immunoreactivity in gastrointestinal and pulmonary neuroendocrine tumours

被引:0
|
作者
G. Pelosi
Filippo Fraggetta
Angelica Sonzogni
Nicola Fazio
Alessandra Cavallon
Giuseppe Viale
机构
[1] Divisione di Anatomia Patologica e Medicina di Laboratorio,
[2] Istituto Europeo di Oncologia,undefined
[3] Via G. Ripamonti,undefined
[4] 435,undefined
[5] 20141 Milano,undefined
[6] Italy e-mail: giuseppe.pelosi@ieo.it Tel.: +39-02-57489414,undefined
[7] Fax: +39-02-57489417,undefined
[8] Department of Pathology and Laboratory Medicine,undefined
[9] European Institute of Oncology and the University of Milan School of Medicine,undefined
[10] Milan,undefined
[11] Italy,undefined
[12] Department of Medical Oncology,undefined
[13] European Institute of Oncology and the University of Milan School of Medicine,undefined
[14] Milan,undefined
[15] Italy,undefined
来源
Virchows Archiv | 2000年 / 437卷
关键词
Keywords CD99 antigen; Neuroendocrine tumours; Immunohistochemistry; Cell-to-cell adhesion; Proliferative activity;
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摘要
Although considered a specific marker for Ewing’s sarcoma/peripheral neuroectodermal tumour, the MIC2 gene product (CD99) has been immunolocalised in a variety of human tumours. The present study evaluated immunohistochemically the prevalence of CD99 expression in a series of 68 neuroendocrine tumours of different gastrointestinal and pulmonary sites. We now report on membrane and/or granular cytoplasmic immunoreactivity in 25% of these tumours, independent of their anatomical sites. In lung neuroendocrine tumours, CD99 was preferentially confined to typical carcinoids (P=0.009). A statistically significant relationship was observed between the number of CD99 positive cells but not the immunostaining patterns and the presence of local invasion and/or distant metastases (P<0.001). Moreover, there was a tendency for CD99-reactive tumours to show a reduced proliferative activity expressed by a Ki67 index of 2% (P=0.119). The number of CD99 immunoreactive cells or patterns of immunoreactivity did not correlate with the presence of associated clinical syndrome or particular hormonal immunostaining. Although the molecular basis underlying CD99 expression in neuroendocrine tumours is still poorly understood, our data suggest that CD99 may be involved in cell-to-cell adhesion of neuroendocrine tumour cells and in downregulation of their proliferative activity.
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页码:270 / 274
页数:4
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