AI Article Synopsis

  • CD105 (endoglin) is significantly expressed in activated endothelial cells and tumor microvessels, and its expression may have clinical relevance based on a study of 929 patients.
  • Univariate analysis revealed that the number of CD105+ microvessels correlates with poor overall survival, particularly in node-negative patients, and high CD105 expression is linked to an increased risk of metastasis.
  • The study concluded that CD105 immunodetection serves as an independent prognostic indicator, potentially guiding the selection of node-negative patients for targeted antiangiogenic therapy.

Article Abstract

CD105 (endoglin) is expressed significantly in activated endothelial cells in culture and in tumor microvessels. Quantification of CD105 immunocytochemical expression that may be clinically relevant has not been accurately evaluated. We studied CD105 expression on frozen tissue sections by using immunohistochemical assays in a series of 929 patients and correlated the findings with long-term follow-up (median, 11.3 years). Univariate (Kaplan-Meier) analysis showed that the number of CD105+ microvessels (cutoff, 15 vessels) correlated significantly with poor overall survival among all patients (P = .001). This correlation was less significant in node-negative patients (P = .035). Marked CD105 expression also correlated with a high risk for metastasis among all patients (P = .006) and among node-negative patients (P = .001). Multivariate analysis (Cox model) identified CD105 immunodetection as an independent prognostic indicator. Our results suggest that immunohistochemical expression of CD105 has practical clinical relevance for identifying node-negative patients with a poor prognosis. Moreover, immunodetection of CD105 also may be considered a potential tool for selecting patients who could benefit from specific antiangiogenic therapy, using anti-CD105 conjugates.

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Source
http://dx.doi.org/10.1309/1kf54l6rb625556wDOI Listing

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