Immuno-Expression of Endoglin and Smooth Muscle Actin in the Vessels of Brain Metastases. Is There a Rational for Anti-Angiogenic Therapy?

Immuno-Expression of Endoglin and Smooth Muscle Actin in the Vessels of Brain Metastases. Is There a Rational for Anti-Angiogenic Therapy?

Despite ongoing clinical trials, the efficacy of anti-angiogenic drugs for the treatment of brain metastases (BM) is still questionable. The lower response rate to anti-angiogenic therapy in the presence of BM than in metastatic disease involving other sites suggests that BM may be insensitive to t...

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Main Authors: Valeria Barresi, Giovanni Branca, Maria Caffo, Rosario Caltabiano, Antonio Ieni, Enrica Vitarelli, Salvatore Lanzafame, Giovanni Tuccari
Format: Article
Language:English
Published: MDPI AG 2014-04-01
Series:International Journal of Molecular Sciences
Subjects:
brain metastasis
endoglin
MVD
pericytes
angiogenesis
Online Access:http://www.mdpi.com/1422-0067/15/4/5663
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spelling doaj-064e63e8d1864aaa97d16c5abf4987d82020-11-25T01:41:05ZengMDPI AGInternational Journal of Molecular Sciences1422-00672014-04-011545663567910.3390/ijms15045663ijms15045663Immuno-Expression of Endoglin and Smooth Muscle Actin in the Vessels of Brain Metastases. Is There a Rational for Anti-Angiogenic Therapy?Valeria Barresi0Giovanni Branca1Maria Caffo2Rosario Caltabiano3Antonio Ieni4Enrica Vitarelli5Salvatore Lanzafame6Giovanni Tuccari7Department of Human Pathology "G. Barresi", University of Messina, Messina 98125, ItalyDepartment of Human Pathology "G. Barresi", University of Messina, Messina 98125, ItalyDepartment of Neurosciences, University of Messina, Messina 98125, ItalyDepartment G.F. Ingrassia, Section of Anatomic Pathology, University of Catania, Catania 95123, ItalyDepartment of Human Pathology "G. Barresi", University of Messina, Messina 98125, ItalyDepartment of Human Pathology "G. Barresi", University of Messina, Messina 98125, ItalyDepartment G.F. Ingrassia, Section of Anatomic Pathology, University of Catania, Catania 95123, ItalyDepartment of Human Pathology "G. Barresi", University of Messina, Messina 98125, ItalyDespite ongoing clinical trials, the efficacy of anti-angiogenic drugs for the treatment of brain metastases (BM) is still questionable. The lower response rate to anti-angiogenic therapy in the presence of BM than in metastatic disease involving other sites suggests that BM may be insensitive to these drugs, although the biological reasons underlining this phenomenon are still to be clarified. With the aim of assessing whether the targets of anti-angiogenic therapies are actually present in BM, in the present study, we analyzed the microvessel density (MVD), a measure of neo-angiogenesis, and the vascular phenotype (mature vs. immature) in the tumor tissue of a series of BM derived from different primary tumors. By using immunohistochemistry against endoglin, a specific marker for newly formed vessels, we found that neo-angiogenesis widely varies in BM depending on the site of the primary tumor, as well as on its histotype. According to our results, BM from lung cancer displayed the highest MVD counts, while those from renal carcinoma had the lowest. Then, among BM from lung cancer, those from large cell and adenocarcinoma histotypes had significantly higher MVD counts than those originating from squamous cell carcinoma (p = 0.0043; p = 0.0063). Of note, MVD counts were inversely correlated with the maturation index of the endoglin-stained vessels, reflected by the coverage of smooth muscle actin (SMA) positive pericytes (r = −0.693; p < 0.0001). Accordingly, all the endoglin-positive vessels in BM from pulmonary squamous cell carcinoma and renal carcinoma, displayed a mature phenotype, while vessels with an immature phenotype were found in highly vascularized BM from pulmonary large cell and adenocarcinoma. The low MVD and mature phenotype observed in BM from some primary tumors may account for their low sensitivity to anti-angiogenic therapies. Although our findings need to be validated in correlative studies with a clinical response, this should be taken into account in therapeutic protocols in order to avoid the adverse effects of useless therapies.http://www.mdpi.com/1422-0067/15/4/5663brain metastasisendoglinMVDpericytesangiogenesis
collection DOAJ
language English
format Article
sources DOAJ
author Valeria Barresi
Giovanni Branca
Maria Caffo
Rosario Caltabiano
Antonio Ieni
Enrica Vitarelli
Salvatore Lanzafame
Giovanni Tuccari
spellingShingle Valeria Barresi
Giovanni Branca
Maria Caffo
Rosario Caltabiano
Antonio Ieni
Enrica Vitarelli
Salvatore Lanzafame
Giovanni Tuccari
Immuno-Expression of Endoglin and Smooth Muscle Actin in the Vessels of Brain Metastases. Is There a Rational for Anti-Angiogenic Therapy?
International Journal of Molecular Sciences
brain metastasis
endoglin
MVD
pericytes
angiogenesis
author_facet Valeria Barresi
Giovanni Branca
Maria Caffo
Rosario Caltabiano
Antonio Ieni
Enrica Vitarelli
Salvatore Lanzafame
Giovanni Tuccari
author_sort Valeria Barresi
title Immuno-Expression of Endoglin and Smooth Muscle Actin in the Vessels of Brain Metastases. Is There a Rational for Anti-Angiogenic Therapy?
title_short Immuno-Expression of Endoglin and Smooth Muscle Actin in the Vessels of Brain Metastases. Is There a Rational for Anti-Angiogenic Therapy?
title_full Immuno-Expression of Endoglin and Smooth Muscle Actin in the Vessels of Brain Metastases. Is There a Rational for Anti-Angiogenic Therapy?
title_fullStr Immuno-Expression of Endoglin and Smooth Muscle Actin in the Vessels of Brain Metastases. Is There a Rational for Anti-Angiogenic Therapy?
title_full_unstemmed Immuno-Expression of Endoglin and Smooth Muscle Actin in the Vessels of Brain Metastases. Is There a Rational for Anti-Angiogenic Therapy?
title_sort immuno-expression of endoglin and smooth muscle actin in the vessels of brain metastases. is there a rational for anti-angiogenic therapy?
publisher MDPI AG
series International Journal of Molecular Sciences
issn 1422-0067
publishDate 2014-04-01
description Despite ongoing clinical trials, the efficacy of anti-angiogenic drugs for the treatment of brain metastases (BM) is still questionable. The lower response rate to anti-angiogenic therapy in the presence of BM than in metastatic disease involving other sites suggests that BM may be insensitive to these drugs, although the biological reasons underlining this phenomenon are still to be clarified. With the aim of assessing whether the targets of anti-angiogenic therapies are actually present in BM, in the present study, we analyzed the microvessel density (MVD), a measure of neo-angiogenesis, and the vascular phenotype (mature vs. immature) in the tumor tissue of a series of BM derived from different primary tumors. By using immunohistochemistry against endoglin, a specific marker for newly formed vessels, we found that neo-angiogenesis widely varies in BM depending on the site of the primary tumor, as well as on its histotype. According to our results, BM from lung cancer displayed the highest MVD counts, while those from renal carcinoma had the lowest. Then, among BM from lung cancer, those from large cell and adenocarcinoma histotypes had significantly higher MVD counts than those originating from squamous cell carcinoma (p = 0.0043; p = 0.0063). Of note, MVD counts were inversely correlated with the maturation index of the endoglin-stained vessels, reflected by the coverage of smooth muscle actin (SMA) positive pericytes (r = −0.693; p < 0.0001). Accordingly, all the endoglin-positive vessels in BM from pulmonary squamous cell carcinoma and renal carcinoma, displayed a mature phenotype, while vessels with an immature phenotype were found in highly vascularized BM from pulmonary large cell and adenocarcinoma. The low MVD and mature phenotype observed in BM from some primary tumors may account for their low sensitivity to anti-angiogenic therapies. Although our findings need to be validated in correlative studies with a clinical response, this should be taken into account in therapeutic protocols in order to avoid the adverse effects of useless therapies.
topic brain metastasis
endoglin
MVD
pericytes
angiogenesis
url http://www.mdpi.com/1422-0067/15/4/5663
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