Association of collagen architecture with glioblastoma patient survival

Author:

Pointer Kelli B.123,Clark Paul A.1,Schroeder Alexandra B.345,Salamat M. Shahriar67,Eliceiri Kevin W.23457,Kuo John S.1278

Affiliation:

1. Departments of Neurological Surgery and

2. Cellular and Molecular Biology Graduate Program;

3. Laboratory for Optical and Computational Instrumentation;

4. Medical Physics Graduate Program;

5. Morgridge Institute for Research; and

6. Pathology and Laboratory Medicine;

7. Carbone Cancer Center, University of Wisconsin, Madison, Wisconsin; and

8. Department of Surgery, National University of Singapore, Singapore

Abstract

OBJECTIVEGlioblastoma (GBM) is the most malignant primary brain tumor. Collagen is present in low amounts in normal brain, but in GBMs, collagen gene expression is reportedly upregulated. However, to the authors' knowledge, direct visualization of collagen architecture has not been reported. The authors sought to perform the first direct visualization of GBM collagen architecture, identify clinically relevant collagen signatures, and link them to differential patient survival.METHODSSecond-harmonic generation microscopy was used to detect collagen in a GBM patient tissue microarray. Focal and invasive GBM mouse xenografts were stained with Picrosirius red. Quantitation of collagen fibers was performed using custom software. Multivariate survival analysis was done to determine if collagen is a survival marker for patients.RESULTSIn focal xenografts, collagen was observed at tumor brain boundaries. For invasive xenografts, collagen was intercalated with tumor cells. Quantitative analysis showed significant differences in collagen fibers for focal and invasive xenografts. The authors also found that GBM patients with more organized collagen had a longer median survival than those with less organized collagen.CONCLUSIONSCollagen architecture can be directly visualized and is different in focal versus invasive GBMs. The authors also demonstrate that collagen signature is associated with patient survival. These findings suggest that there are collagen differences in focal versus invasive GBMs and that collagen is a survival marker for GBM.

Publisher

Journal of Neurosurgery Publishing Group (JNSPG)

Subject

Genetics,Animal Science and Zoology

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