Mitosin and pHH3 predict poorer survival in astrocytomas WHO grades II and III.

Abstract	AIMS: The limitations of the current WHO classification of astrocytomas call for a sustained effort to improve diagnostic and prognostic accuracy. The relationship between tumour growth and clinical outcome suggests that proliferative activity should be examined. The objective of this study was to evaluate the diagnostic and prognostic value of the proliferation markers mitosin and phosphohistone H3 (pHH3) in infiltrative astrocytomas WHO grades II and III and compare the findings with mitotic count and Ki-67/MiB-1 immunostaining. METHODS: Fifty-nine and thirty-three infiltrative astrocytomas WHO grades II and III, respectively, were immunostained with the proliferation markers mitosin and pHH3 using standard immunohistochemical procedures. The expression was quantified as a proliferative index (PI) and statistically evaluated with Spearman's rank correlation test, Wilcoxon-Mann-Whitney U test, and univariable and multivariable COX regression survival analyses. RESULTS: Significant positive correlations were found between these proliferation markers. The number of mitoses, pHH3 mitotic figures (MFs), the Ki-67/MiB-1 PI and the mitosin PI were greater in WHOgrade III anaplastic astrocytomas compared to WHO grade II diffuse astrocytomas, while pHH3 PI only showed a trend. All proliferation markers were associated with poorer prognosis, but mitotic count was not. Ki-67/MiB-1, mitosin and pHH3 MF achieved statistical significance in the univariable analyses of both time to relapse (TTR) and overall survival (OS). Only mitosin remained significant in both multivariable analyses. pHH3 was significant in the multivariable analysis of OS but not of TTR. Clinical factors including age, extent of surgical resection and WHO performance status were also significantly correlated with survival. CONCLUSIONS: In conclusion, mitosin and pHH3 immunostaining have prognostic and diagnostic value in the clinical assessment of patients with infiltrative astrocytomas. The inclusion of proliferation markers in a layered diagnosis should be considered in the upcoming revision of the WHO classification system.
Authors	R K Varughese, T Lind-Landström, A H Habberstad, Ø Salvesen, C S Haug, S Sundstrøm, S H Torp
Journal	Journal of clinical pathology (J Clin Pathol) Vol. 69 Issue 1 Pg. 26-34 (Jan 2016) ISSN: 1472-4146 [Electronic] England
PMID	26188054 (Publication Type: Comparative Study, Evaluation Study, Journal Article)
Copyright	Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://www.bmj.com/company/products-services/rights-and-licensing/
Chemical References	Biomarkers, Tumor Chromosomal Proteins, Non-Histone Histones Ki-67 Antigen Microfilament Proteins centromere protein F
Topics	Adult Aged Astrocytoma (chemistry, classification, mortality, pathology, therapy) Biomarkers, Tumor (analysis) Brain Neoplasms (chemistry, classification, mortality, pathology, therapy) Cell Proliferation Chromosomal Proteins, Non-Histone (analysis) Disease Progression Female Histones (analysis) Humans Immunohistochemistry Kaplan-Meier Estimate Ki-67 Antigen (analysis) Male Microfilament Proteins (analysis) Middle Aged Mitosis Mitotic Index Multivariate Analysis Neoplasm Grading Neoplasm Recurrence, Local Phosphorylation Proportional Hazards Models Retrospective Studies Risk Factors Time Factors Treatment Outcome Young Adult

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