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Immunohistochemical analysis of p16INK4a, p14ARF, p18INK4c, p21CIP1, p27KIP1 and p73 expression in 271 meningiomas correlation with tumor grade and clinical outcome

✍ Scribed by Andrey Korshunov; Lyudmila Shishkina; Andrey Golanov


Publisher
John Wiley and Sons
Year
2003
Tongue
French
Weight
185 KB
Volume
104
Category
Article
ISSN
0020-7136

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✦ Synopsis


Abstract

Routine pathological examination cannot distinctively predict the clinical course of meningiomas because even histologically benign tumors may recur after gross total resection. Numerous efforts have been made for the evaluation of different immunohistochemical assays in meningioma prognosis. We investigated the prognostic significance of p16INK4a, p14ARF, p18INK4c, p21CIP1, p27KIP1 and p73 expression by immunohistochemical analysis of 271 meningiomas. All tumors were additionally stained for the proliferation markers Ki‐67 and DNA topoisomerase II alpha (TopoIIα). Significant differences between the number of p16INK4a‐, p18INK4c‐ and p21CIP1‐positive cases were noted among the 3 grades of meningiomas. p16INK4a‐ and p21CIP‐positive tumors were found to prevail among benign meningiomas, whereas p18INK4c immunostaining was closely associated to anaplastic meningiomas. The number of p16INK4a‐ and p21CIP‐positive cases was significantly lower in the cohort of recurrent meningiomas. In contrast, p18INK4c‐positive cases were clustered among recurrent meningiomas regardless of tumor grade. Immunoreactivity of p14ARF, p27KIP1 and p73 did not show any differences between meningiomas of various histology and clinical outcomes. Multivariate analysis revealed that only tumor grade and TopoIIα index are independent criteria for predicting meningioma recurrence. Thus, the immunohistochemical assessment of p16INK4a, p14ARF, p18INK4c, p21CIP1, p27KIP1 and p73 expression in meningiomas does not appear to provide prognostically useful information. Further studies are needed to identify more reliable prognostic markers and to address in more detail the role of cell cycle aberrations in these tumors. © 2003 Wiley‐Liss, Inc.


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