Showing posts with label tumor. Show all posts
Showing posts with label tumor. Show all posts

Wednesday, 14 August 2013

Tumor suppressor may provide clues for improved treatment for neuroblastoma

Main Category: Neurology / Neuroscience
Also Included In: Cancer / Oncology;  Stem Cell Research
Article Date: 14 Aug 2013 - 0:00 PDT Current ratings for:
Tumor suppressor may provide clues for improved treatment for neuroblastoma
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Loss of a gene required for stem cells in the brain to turn into neurons may underlie the most severe forms of neuroblastoma, a deadly childhood cancer of the nervous system, according to a Ludwig Cancer Research study. Published in Developmental Cell, the findings also provide clues about how to improve the treatment of this often-incurable tumor.

Neuroblastoma can appear in nervous tissue in the abdomen, chest and spine, among other regions of the body, and can spawn body-wracking metastasis. The most severe tumors respond poorly to treatment, and the disease accounts for 15 percent of cancer deaths in children.

Johan Holmberg, PhD, at the Ludwig Institute for Cancer Research Stockholm took a close look at the role of the CHD5 tumor suppressor during normal nervous system development. Previous studies had shown that the gene CHD5 is often inactivated in the most severe forms of neuroblastoma, but little was known about its function in healthy tissue or how it operates. The study, which was conducted in close collaboration with colleagues at Trinity College, Dublin, Ireland, addressed these two key issues.

The researchers found that CHD5 is required for the cellular transition from a stem cell to a mature neuron. In one experiment, the researchers knocked down the CHD5 gene by injecting a small RNA into the brains of fetal mice while in the womb.

"The result was a complete absence of neurons," says Ludwig researcher Holmberg who is based at the Karolinska Institutet. "Instead of becoming neurons, the cells with CHD5 knocked down stayed in a limbo-like state between an actively-dividing stem cell and a mature nerve cell. It was a very robust effect," added Holmberg.

The researchers also dissected how CHD5 operates, showing that it sticks to certain modifications of histone proteins. These modifications help control how genes are turned on and off. In the absence of CHD5, key stem cell genes are not turned off, and genes required for neuronal maturation are not turned on. The findings highlight how the failure of a cell to properly mature into its terminal state can underlie cancer, a relatively understudied area of research.

"It is necessary for cells in the healthy nervous tissue to be able to go from stem cells to neurons," explains Holmberg. "If you lose this capacity, these cells become locked in an immature state, which might yield quite dangerous tumor cells, especially in combination with additional cancer-promoting cellular events."

The research could also lead to new ways to treat neuroblastoma, perhaps using currently approved drugs. One component of neuroblastoma treatment is retinoic acid, a drug that can drive neuronal maturation. Holmberg and his colleagues found that knocking down the expression of CHD5 in more benign neuroblastoma cells blocked their capacity to mature in response to retinoic acid treatment. "These cells were completely insensitive to treatment, no matter how much we gave them, mirroring the same unresponsiveness to retinoic acid in the more malignant CHD5-negative neuroblastoma cells," says Holmberg.

The results of these cell-based experiments are consistent with clinical findings that retinoic acid is often unsuccessful in patients with severe forms of the disease. Holmberg reasons that if CHD5 could be re-activated in such hard-to-treat patients, it might increase responsiveness to retinoic acid. The findings may also have relevance for other types of tumors. For instance, CHD5 is often inactivated in glioblastoma multiforme, the most common and most aggressive form of brain cancer in adults.

Article adapted by Medical News Today from original press release. Click 'references' tab above for source.
Visit our neurology / neuroscience section for the latest news on this subject.

Funding for this research came in part from Science Foundation Ireland; the Health Research Board; the Swedish Cancer Society, the Swedish Research Council, the Lilian Sagen and Curt Eriksson Research Foundation; DBRM; the Swedish Childhood Cancer Foundation; the Danish National Research Foundation; the Lundbeck Foundation; and the Novo Nordisk Foundation.

CHD5 Is Required for Neurogenesis and Has a Dual Role in Facilitating Gene Expression and Polycomb Gene Repression

Developmental Cell, Volume 26, Issue 3, 223-236, 12 August 2013. 10.1016/j.devcel.2013.07.008

Ludwig Institute for Cancer Research

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Monday, 5 August 2013

Virginia Tech researcher uses micro-fabricated blood vessels to study tumor growth and anti-angiogenic cancer therapy

Main Category: Cancer / Oncology
Also Included In: Blood / Hematology
Article Date: 02 Aug 2013 - 1:00 PDT Current ratings for:
Virginia Tech researcher uses micro-fabricated blood vessels to study tumor growth and anti-angiogenic cancer therapy
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Researchers have established a 3-D microfluidic system to study a biological process known as endothelial sprouting. This process represents an early step in new blood vessel growth called angiogenesis.

Breakthroughs in an integrated understanding of angiogenesis will benefit researchers in broad biomedical fields, including cancer, vascular science, and tissue engineering. The reason for this interest in the cancer field is that tumors must access the host blood supply to obtain nutrients essential for growth. They do this by co-opting nearby blood vessels, causing them to sprout into and vascularize the tumor bulk in angiogenesis. The progression of the tumor results in fatal cancer.

Scott Verbridge, assistant professor in the School of Biomedical Engineering and Sciences at Virginia Tech, along with senior investigators at the Cornell University Physical Sciences-Oncology Center, developed the system using in vitro models, or living engineered tissues, with support from the National Cancer Institute's Physical Sciences in Oncology.

In the scientific community, relatively little is known about the integrated physico-chemical processes involved in angiogenesis. Blood vessel intrinsic processes can augment or inhibit cell sprouting initially driven by chemical signals from the tumor cells, such that drugs designed to block these tumor-derived chemical triggers may not always be effective. However tools to study these important details have been lacking.

"Angiogenesis has been extensively studied in this field and is one of the areas where innovative microenvironment-targeted therapies have actually made it to patients. However these treatments do not work nearly as well as people hoped," said Verbridge. "Developing in vitro models will help us understand the various regulators of angiogenesis, how these may influence the efficacy of current treatments, and motivate new treatment ideas."

The system uses natural tissue materials, consisting of three defined microchannels embedded in type I collagen hydrogels, designed to imitate the structural support into which new blood vessels regenerate. Two parallel side channels provide the means to create biochemical gradients that cross the endothelial cell-coated central channel.

New blood vessel sprouting transpires when gradients of vascular endothelial growth factor (VEGF) are applied across the central channel, however blood vessel geometry and density were also unexpectedly found to strongly regulate sprouting dynamics.

The results are described in a paper published in the Journal of Biomedical Materials Research Part A and highlight the importance of mechanical factors, as well as biochemical ones. Verbridge's laboratory, a multidisciplinary research group collaborating with Virginia Tech labs in biomedical engineering, electrical and computer engineering, and chemical engineering; and the Wake Forest Comprehensive Cancer Center, work to develop innovative paradigms for more effective treatment of currently incurable forms of cancer. Tumor metabolism, experimental tumor evolution, energy-based cancer therapies, and graphene nano-bio interfaces are a few of the projects being pursued by lab investigators.

The College of Engineering at Virginia Tech is internationally recognized for its excellence in 14 engineering disciplines and computer science. The college's 6,000 undergraduates benefit from an innovative curriculum that provides a "hands-on, minds-on" approach to engineering education, complementing classroom instruction with two unique design-and-build facilities and a strong Cooperative Education Program. With more than 50 research centers and numerous laboratories, the college offers its 2,000 graduate students opportunities in advanced fields of study such as biomedical engineering, state-of-the-art microelectronics, and nanotechnology. Virginia Tech, the most comprehensive university in Virginia, is dedicated to quality, innovation, and results to the commonwealth, the nation, and the world.

Article adapted by Medical News Today from original press release. Click 'references' tab above for source.
Visit our cancer / oncology section for the latest news on this subject.

"Physicochemical regulation of endothelial sprouting in a 3D microfluidic angiogenesis model", Scott S. Verbridge, Anirikh Chakrabarti, Peter DelNero, Brian Kwee, Jeffrey D. Varner, Abraham D. Stroock, Claudia Fischbach, Article first published online: 5 APR 2013, DOI: 10.1002/jbm.a.34587

Virginia Tech

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Tech, Virginia. "Virginia Tech researcher uses micro-fabricated blood vessels to study tumor growth and anti-angiogenic cancer therapy." Medical News Today. MediLexicon, Intl., 2 Aug. 2013. Web.
3 Aug. 2013. APA

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'Virginia Tech researcher uses micro-fabricated blood vessels to study tumor growth and anti-angiogenic cancer therapy'

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Please send any medical news or health news press releases to:

Note: Any medical information published on this website is not intended as a substitute for informed medical advice and you should not take any action before consulting with a health care professional. For more information, please read our terms and conditions.



View the original article here