Research May Lead to New Treatment for Type of Brain Cancer

Study Pinpoints a Genetic Cause of Most Lethal Brain Tumor— May Lead to New Treatment

New York, NY (July 26, 2012) — Researchers at Columbia University Medical Center (CUMC) have discovered that some cases of glioblastoma, the most common and aggressive form of primary brain cancer, are caused by the fusion of two adjacent genes. The study also found that drugs that target the protein produced by this genetic aberration can dramatically slow the growth of glioblastomas in mice. The findings were published today in the online edition of the journal Science.

Figure 1

Figure 1: FGFR-TACC fusion protein disrupts cellular division (mitosis) by localizing aberrantly at the mid-body of dividing cells. Here, FGFR-TACC (shown in red) can be seen interacting with tubulin bundles (green), structures that support mitosis, at the point connecting the two daughter cells (whose nuclei are colored blue).

“Our findings are doubly important,” said study leader Antonio Iavarone, MD, professor of pathology and neurology at CUMC, and a member of the Herbert Irving Comprehensive Cancer Center (HICCC) at NewYork-Presbyterian Hospital/Columbia University Medical Center. “From a clinical perspective, we have identified a druggable target for a brain cancer with a particularly dismal outcome. From a basic research perspective, we have found the first example of a tumor-initiating mutation that directly affects how cells divide, causing chromosomal instability. This discovery has implications for the understanding of glioblastoma as well as others types of solid tumors.”

The fusion of these two genes was observed in just three percent of tumors studied, so any therapy based on this particular genetic aberration would apply to only a small subset of glioblastoma patients. “It’s unlikely that we will find a gene fusion responsible for most glioblastomas. But we may be able to discover a number of other gene fusions, each accounting for a small percentage of tumors, and each with its own specific therapy,” said co-senior author Anna Lasorella, MD, associate professor of pathology and pediatrics at CUMC and a member of the Columbia Stem Cell Initiative and the HICCC.

“This is a very exciting advance in our understanding of cancer, and perhaps a first step toward a personalized, precision approach to the treatment of glioblastoma,” said Stephen G. Emerson, MD, PhD, director of the HICCC and the Clyde ’56 and Helen Wu Professorship in Immunology at the Columbia University College of Physicians and Surgeons.

Figure 2

Figure 2: Abnormal accumulation of the FGFR-TACC fusion protein (red) in glioblastoma stem cells isolated from a primary human glioblastoma with fused FGFR- TACC genes. Cellular nuclei are colored blue.

Glioblastomas are tumors that arise from astrocytes, star-shaped cells that make up the brain’s supportive tissue. Since astrocytes reproduce quickly and are supported by a large network of blood vessels, glioblastomas are usually highly malignant. It is estimated that these tumors affect about 10,000 people in the United States each year. Glioblastoma is typically treated with surgery, followed by radiation and chemotherapy. However, the disease is invariably fatal, with a median survival of about 14 months after diagnosis, even with aggressive therapy. Glioblastomas took the lives of Senator Edward Kennedy in 2009 and New York Mets all-star catcher Gary Carter in 2012.

Several common single-gene alterations have been observed in glioblastoma. “However, therapies targeting these alterations have not improved clinical outcomes, most likely because they have systematically failed to eradicate the proteins to which the tumor is ‘addicted,’” said Dr. Iavarone.

Dr. Iavarone and his colleagues suspected that glioblastomas might be addicted to proteins produced by gene fusions. Such fusions have been implicated in other cancers, notably chronic myelogenous leukemia (CML). Novartis AG’s (NYSE: NVS) drug Gleevec (imatinib), which targets a fusion protein responsible for CML, has proved to be highly effective in arresting the disease.

Figure 3

Figure 3: Graphic representation of the collaboration between experimental and computational biology. The outer ring represents results of next-generation genetic sequencing of the glioblastoma genome, showing expression of the FGFR-TACC fusion gene (red peaks). In the center, FGFR-TACC fusion protein (red) can be seen disrupting tubulin bundles (green), structures that support cell division, or mitosis, at the point connecting the two daughter cells (whose nuclei are colored blue). Photo credit: Antonio Iavarone, MD/Columbia University Medical Center

In the current study, the CUMC researchers conducted genetic analyses of glioblastomas from nine patients, looking specifically for gene fusions. The most common fusion they observed involved the genes FGFR (fibroblast growth factor receptor) and TACC (transforming acidic coiled-coil).

Although each gene plays a specific role in the cell, sometimes errors in the DNA cause two ordinary genes to fuse into a single entity, with novel characteristics that can lead to a tumor," said co-senior author Raul Rabadan, PhD, assistant professor in the department of Biomedical Informatics and the Center for Computational Biology and Bioinformatics, Columbia Initiative in Systems Biology.

"We developed a new method for analyzing the cell's genomic material," he said. "First we looked at pieces of the glioblastoma genome from several samples, and then we extended the analysis to a large set of glioblastomas from the Cancer Genome Atlas project, sponsored by the National Cancer Institute."

The researchers discovered that the protein produced by FGFR-TACC acts by disrupting the mitotic spindle, the cellular structure that guides mitosis (the division of a cell into two identical daughter cells). “If this process happens incorrectly, you get uneven distribution of the chromosomes. This condition, which is known as aneuploidy, is thought to be the hallmark of tumorigenesis,” said Dr. Iavarone.

When FGFR-TACC was introduced into the brain cells of healthy mice, aggressive brain tumors developed in 90 percent of the animals, confirming that this gene fusion can lead to glioblastoma.

In another experiment, mice with this form of glioblastoma were given a drug that inhibits FGFR kinase, an enzyme essential for the protein produced by FGRF-TACC to do its work. The drug was found to prevent abnormal mitosis and double survival time, compared with a control group of mice that did not receive the drug.

Dr. Iavarone is currently establishing a cooperative study group, including CUMC and other brain tumor centers around the country, to conduct the trials of FGFR kinase inhibitors. Preliminary trials of these drugs (for treatment of other forms of cancer) have shown that they have a good safety profile, which should accelerate testing in patients with glioblastoma.

“This work is the result of an ongoing collaboration between a traditional and a computational lab. The synergy between the two approaches allows us to tackle complex biological problems in a high throughput fashion, providing a global view to the genome of glioblastoma,” said Dr. Rabadan.

Dr. Iavarone’s paper is titled, “Transforming Fusions of FGFR and TACC Genes in Human Glioblastoma.” The other contributors are Devendra Singh (CUMC), Joseph Minhow Chan (CUMC), Pietro Zoppoli CUMC), Francesco Niola (CUMC), Ryan Sullivan (CUMC), Angelica Castano (CUMC), Eric Minwei Liu (CUMC), Jonathan Reichel (CUMC and Weill Cornell Medical College, New York, NY), Paola Porrati (Fondazione I.R.C.C.S Istituto Neurologico C. Besta, Milan, Italy), Serena Pellegatta (Fondazione I.R.C.C.S Istituto Neurologico C. Besta), Kunlong Qiu (Bioinformatics Center, BGI, Shenzhen, China) Zhibo Gao (Bioinformatics Center, BGI), Michele Ceccarelli (Biogem, Ariano Irpino (AV) and Dipartimento di Scienze Biologiche ed Ambientali, Università del Sannio, Benevento, Italy), Riccardo Riccardi (Catholic University, Rome, Italy), Daniel J. Brat (Emory University School of Medicine, Atlanta, Ga.), Abhijit Guha (University of Toronto, Toronto, Canada), Ken Aldape (M.D. Anderson Cancer Center, Houston, Tex.), John G. Golfinos (NYU Langone Medical Center, New York, N.Y.), David Zagzag (NYU Langone Medical Center), Tom Mikkelsen (Henry Ford Health System, Detroit, Mich.), and Gaetano Finocchiaro (Fondazione I.R.C.C.S Istituto Neurologico C. Besta).

This research was supported by National Cancer Institute grants R01CA101644, R01CA131126, R01CA085628, R01CA127643, and U54 CA121852-05; National Library of Medicine grant 1R01LM010140-01; National Institute of Neurological Disorders and Stroke grant R01NS061776; Partnership for Cure grant 7-78947; and grants from the Chemotherapy Foundation, the Associazione Italiana per la Ricerca sul Cancro, and the Italian Ministry of Health. Additional support was provided by Giuseppe Bruno, Marianne Mebane, and Denise and David Chase.

Drs. Iavarone, Lasorella, and Rabadan and CUMC have filed a patent application related to the diagnostic and therapeutic use of FGFR-TACC gene fusions. Otherwise, the authors declare no financial or other conflicts of interest.

Columbia University Medical Center provides international leadership in basic, pre-clinical and clinical research, in medical and health sciences education, and in patient care. The medical center trains future leaders and includes the dedicated work of many physicians, scientists, public health professionals, dentists, and nurses at the College of Physicians and Surgeons, the Mailman School of Public Health, the College of Dental Medicine, the School of Nursing, the biomedical departments of the Graduate School of Arts and Sciences, and allied research centers and institutions. Established in 1767, Columbia's College of Physicians and Surgeons was the first institution in the country to grant the M.D. degree and is among the most selective medical schools in the country. Columbia University Medical Center is home to the largest medical research enterprise in New York City and State and one of the largest in the United States.

The Herbert Irving Comprehensive Cancer Center at Columbia University Medical Center and NewYork-Presbyterian Hospital encompasses pre-clinical and clinical research, treatment, prevention and education efforts in cancer. The Cancer Center was initially funded by the NCI in 1972 and became a National Cancer Institute (NCI)–designated comprehensive cancer center in 1979. The designation recognizes the Center’s collaborative environment and expertise in harnessing translational research to bridge scientific discovery to clinical delivery, with the ultimate goal of successfully introducing novel diagnostic, therapeutic and preventive approaches to cancer. For more information, visit www.hiccc.columbia.edu.

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Media Contact: Karin Eskenazi, 212-342-0508, ket2116@columbia.edu

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