Journal of Clinical Oncology, Vol 15, 2456-2466, Copyright © 1997 by American Society of Clinical Oncology
Prognostic value of the expression of p53, bcl-2, and bax oncoproteins, and neovascularization in patients with radically resected non-small- cell lung cancer
RM Apolinario, P van der Valk, JS de Jong, W Deville, J van Ark-Otte, AM Dingemans, JC van Mourik, PE Postmus, HM Pinedo and G Giaccone
Department of Medical Oncology, Vrije Universiteit and University Hospital, Amsterdam, the Netherlands.
PURPOSE: To assess the prognostic value of p53, bcl-2, bax, and
neovascularization in radically resected non-small-cell lung cancer (NSCLC)
patients. PATIENTS AND METHODS: Tumors from 116 patients were assessed by
immunohistochemistry for expression of p53 (DO7 and PAb1081), bcl-2, and
the quantification of microvessel density (CD-31). In addition, the
expression of bax was assessed in 61 stage I tumors. The median levels of
expression of each marker were used as cutoff points. RESULTS: p53 was not
correlated to any patient or tumor characteristic, whereas bcl-2 showed
higher expression in squamous cell carcinomas (P < .001). bax expression
was significantly related with male sex (P = .006) and adenocarcinoma type
(P = .0013). p53 status, assessed with one monoclonal antibody (MoAb), was
not predictive for survival; however, the combination of staining results
obtained with two MoAbs identified the DO7-/PAb1801+ tumors as those with
the worst prognosis. bcl-2 expression was associated with longer survival
in stage I patients (P = .0169). The combined group expressing
p53+(PAb1801)/bcl-2- had the worst survival in stage I patients (P = .034)
and in the whole series in comparison with the other combinations of the
two oncoproteins. bax expression alone had no influence on survival of
stage I patients, but patients with bax+/bcl-2- tumors had the worst
prognosis (P = .02 in comparison with bax+/bcl-2+). Tumor
neovascularization was not related with other factors, and patients with
CD-31+ tumors had a shorter survival duration than those with CD- 31-
tumors only in stage II (P = .0283). By multivariate analysis including all
patients, the presence of p53+/ bcl-2- tumor expression and large tumor
diameter (> or = 4cm) were independent prognostic factors for shorter
survival duration. For stage I, only the presence of bax+/ bcl-2- tumor
expression had a significant negative influence on survival. CONCLUSION:
The interaction and the regulation of new biologic markers, such as those
involved in the apoptotic pathway, are complex. Combinations of the
expression of several of them may give more valuable information than the
study of just one. Prognostic influence of p53 staining varied depending on
the choice of antibody and the combination of bcl-2- together with p53+
(PAb1801) or with bax+ had the worst influence on survival for patients
with stage I NSCLC.
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