TUMOR ANGIOGENESIS CORRELATES WITH HISTOLOGIC TYPE AND METASTASIS IN NON-SMALL-CELL LUNG-CANCER

Authors
YUAN A YANG PC YU CJ LEE YC YAO YT CHEN CL LEE LN KUO SH LUH KT
Citation
A. Yuan et al., TUMOR ANGIOGENESIS CORRELATES WITH HISTOLOGIC TYPE AND METASTASIS IN NON-SMALL-CELL LUNG-CANCER, American journal of respiratory and critical care medicine, 152(6), 1995, pp. 2157-2162
Citations number
27
Categorie Soggetti
Emergency Medicine & Critical Care","Respiratory System
Journal title
American journal of respiratory and critical care medicineACNP
ISSN journal
1073449X
Volume
152
Issue
6
Year of publication
1995
Pages
2157 - 2162
Database
ISI
SICI code
1073-449X(1995)152:6<2157:TACWHT>2.0.ZU;2-S
Abstract
This study investigated the clinico-pathologic correlation of tu mor a ngiogenesis in non-small-cell lung cancers. Formalin-fixed, paraffin-e mbedded surgical specimens of 55 consecutive patients with primary non -small-cell lung cancers were examined. Included were 26 squamous cell carcinomas and 29 adenocarcinomas. Twenty-five patients had stage I d isease, eight patients had stage II disease, and 22 patients had stage IIIA or IIIB disease. Among them, 28 had nodal metastasis and 27 did not. The microvessel was demonstrated by immunocytochemical staining f or factor VIII and platelet endothelial cell adhesion molecules (PECAM -1). The microvessels in the areas of highest neovascularization were counted under light microscopy in 200x field by two independent observ ers without knowledge of clinical information. At least three separate fields were counted for each specimen. The Mann-Whitney U test was us ed for statistical analysis. The microvessel counts in adenocarcinoma were significantly higher than in the squamous cell carcinoma (54.4 +/ - 35.65 versus 26.16 +/- 20.46 in factor VIII staining and 80.52 +/- 4 8.42 versus 40.04 +/- 32.33 in PECAM-1 staining; p < 0.001). The micro vessel counts in patients with Stages I-II disease were significantly lower than that of stages IIIA-IIIB disease (23.63 +/- 16.21 versus 65 .36 +/- 31.92 in factor VIII staining and 41.85 +/- 36.76 versus 93.00 +/- 43.08 in PECAM-1; p < 0.001). Patients with nodal metastasis had higher microvessel density than those without nodal metastasis (56.67 +/- 35.55 versus 23.44 +/- 15.77 in factor VIII staining and 86.89 +/- 46.46 versus 36.30 +/- 25.83 in PECAM-1 staining; p < 0.001). The mic rovessel counts in patients with early postoperative metastasis were h igher than those without early metastasis (64.47 +/- 34.60 versus 27.5 3 +/- 20.48 in factor VIII staining and 96.79 +/- 48.14 versus 44.39 /- 38.0 in PECAM-1 staining; p < 0.001). Our results suggest that micr ovessel density correlates with histologic types, stages of disease, n odal status, and postoperative metastasis in non-small-cell lung cance r. The high microvessel counts in adenocarcinoma may contribute to the higher metastatic potential compared with squamous cell carcinoma.