Taking A Sideswipe at High-Risk Neuroblastoma

0

This originally appeared on Vector, Boston Children’s Hospital’s blog.

Cancer and other diseases are now understood to spring from a complex interplay of biological factors rather than any one isolated origin. New research reveals that an equally-nuanced approach to treating high-risk neuroblastoma may be the most effective way to curb tumor growth.

One challenge in treating pediatric cancers like neuroblastoma is that they are not initiated from the same kinds of genetic mutations as adult cancers, which usually arise from mutations related to an accumulation of DNA replication errors or environmental factors. In contrast, childhood cancers more often stem from genetic duplications, deletions or translocations, the latter of which occurs when a gene sequence switches its location from one chromosome to another.

Human neuroblastoma cells.

Human neuroblastoma cells.

On top of this, pediatric cancers that develop from these types of genetic alterations often involve genes called “transcription factors”, which encode for production of proteins that regulate the transcription of specific DNA sequences.

“Transcription factors have been notoriously difficult to make drugs against and they are frequently translocated or amplified in pediatric cancers,” says Kimberly Stegmaier, MD, who is co-director of the pediatric hematologic malignancy program at Dana-Farber/Boston Children’s Cancer and Blood Disorders Center and also a member of the Broad Institute’s Cancer Program.

A Tale of Two Genes

In pediatric high-risk neuroblastoma, for example, a transcription factor known as MYCN becomes amplified with many copies inside each cancer cell. So far, it has not been possible to target MYCN pharmacologically.

But now, a team led by Stegmaier has discovered a roundabout way to stave off the effects of MYCN amplification through a link with another gene, called EZH2. Their findings were published this month in the Journal of Clinical Investigation.

In their experiments, the team found that the MYCN protein directly controls the expression of the EZH2gene, which encodes for the EZH2 protein, a known tumor cell proliferator across various types of cancers. When MYCN is amplified, over-production of the EZH2 protein blocks tumor suppressor activity and normal differentiation programs in the neuroblastoma cells and prevents them from growing into mature neurons, according to a story about the research by the Broad.

Strikingly, by blocking EZH2 through genetic repression and chemical inhibitors, the researchers were able to impair neuroblastoma growth.

Setting the Stage for a Clinical Trial

The findings are all the more interesting because an EZH2 inhibitor is already being evaluated in children with certain cancers.

Called tazemetostat, it’s being clinically tested in two studies led by Susan Chi, MD, of Dana-Farber/Boston Childrens: A phase 1 clinical trial for children with certain relapsed/refractory malignancies and a phase 2 nationwide precision medicine study sponsored by the National Institute of Cancer (NCI) and the Children’s Oncology Group (COG).

“Given these initial findings with other EZH2 inhibitors, we are now evaluating tazemetostat as a potential molecule to treat MYCN-amplified neuroblastoma,” says Stegmaier. “It is my hope that our publication and a growing body of other data supporting the role of EZH2 in high-risk neuroblastoma will fuel the development of a clinical trial to test EZH2 inhibitors for the treatment of children with this type of cancer.”

Learn more about Dana-Farber/Boston Children’s research.

Comments Sort By Newest

Leave a Reply

Your email address will not be published. Required fields are marked *

Blue Captcha Image
Refresh

*

Make An Appointment

For adults: 877-960-1562

Quick access: Appointments as soon as the next day for new adult patients

For children: 888-733-4662

All content in these blogs is provided by independent writers and does not represent the opinions or advice of Dana-Farber Cancer Institute or its partners.

Latest Tweets

Dana-Farber @danafarber
Since 2014, more than 40 of Carol Snyder Halberstadt’s poems, including those focused on her ongoing care at Dana-F… https://t.co/NufLBIE2mk
Dana-Farber @danafarber
WATCH: Laurie H. Glimcher, MD, president and chief executive officer of Dana-Farber, at the World Economic Forum di… https://t.co/M9jAdexxAB

Republish our posts on your blog

Interested in sharing one of our stories on your blog? Feel free to republish this content! We just ask that you credit Dana-Farber, link to the original article, and refrain from making edits that change the original context. Questions? Email the editors at insight_blog@dfci.harvard.edu.