Grants Search Results

Langerhans cell histiocytosis (LCH) is a rare cancer of the immune cells that can cause a wide range of symptoms, ranging from a rash to lethal multi-organ disease. Dr. Zinn hypothesizes that a patient's symptoms are determined by a combination of the patient's specific mutation and the specific immune cell that becomes mutated. Dr. Zinn is investigating the causes of LCH in order to develop the most effective and safe therapies for each patient.

Children's cancer can spread through the body by hiding from the bodys immune system. There are certain cells, called regulatory T cells, that make it easier for cancer to hide by turning down the bodys immune system. Children with cancer who have a higher number of these cells seem to have a poorer outcome. Additionally, some cancers have these cells inside them. Dr. Mathias's lab has made a drug that can kill regulatory T cells, and will test this drug in a model to see the effects of killing the regulatory T cells, hopefully helping the body to improve the immune system's ability to kill cancer cells.

Based on progress to date, Dr. Mavers was awarded a new grant in 2018 to fund an additional year of this Fellow award. Many children with cancer cannot be cured with chemotherapy alone and must undergo bone marrow transplantation. This treatment permits very high doses of chemotherapy to cure the cancer then rebuilds the immune system, which is destroyed by such high chemotherapy doses. In many cases, rebuilding a new immune system causes the new immune cells to attack the body, which is called graft-versus-host disease. Graft-versus-host disease can damage many organs. Dr. Mavers is studying ways to use special cell types to stop graft-versus-host disease and make stem cell transplantation a safer way to cure cancer.

This grant is made with generous support from the Rays of Hope Hero Fund that honors the memory of Rayanna Marrero by giving hope through research funding. She is remembered for her infectious smile and energetic spirit that continue to inspire so many.

Based on progress to date, Dr. Deel was awarded a new grant in 2018 to fund an additional year of this Fellow award. Rhabdomyosarcoma is a childhood cancer of the muscle that has two major subtypes. Children with the alveolar type do very poorly, as these are frequently recurrent and metastatic. Alveolar rhabdomyosarcoma cells have a specific fusion protein that is a powerful cancer driver and that does not yet have a pharmaceutical treatment. Dr. Deel and his team recently found that the Hippo pathway, normally functions to suppress tumor growth, is not correctly regulated in alveolar rhabdomyosarcoma, which leads to TAZ (a co-activator) activating pro-tumoric gene transcription.

As the Aiden's Army St. Baldrick's Fellow, Dr. Deel is studying the interaction between the protein and the co-activator TAZ as a novel therapeutic target. Aiden Binkley was diagnosed with Stage IV rhabdomyosarcoma at age 8. This bright, funny and courageous little boy believed he got cancer so he could grow up to find a cure for it. His vision is being carried on by Aiden’s Army through the funding of research. They will march until there is a cure!

Based on progress to date, Dr. John was awarded a new grant in 2018 to fund an additional year of this Fellow award. Unfortunately, even with intensive treatment, only 60% of children with acute myeloid leukemia (AML) will survive the disease. Intensifying standard therapies have failed to improve survival rates, so a new approach is needed. Dr. John is creating a novel receptor that will specifically target a marker on AML cells. He will put this new receptor on T-cells of the body, which will then target and kill the leukemia cells. Dr. John hopes to improve outcomes for pediatric AML with this grant.

This grant is generously supported by Super Soph's Pediatric Cancer Research Fund. Sophie Rossi was diagnosed with AML at 3 months of age. Throughout her courageous battle, she was always smiling, always joyful. This fund was created to honor her spunky, sweet spirit by funding research to find cures for AML and all childhood cancers.

Juvenile myelomonocytic leukemia (JMML) is an aggressive blood cancer of young children. The only current curative treatment is bone marrow transplantation. Yet, about 50% of children do not survive despite this very aggressive therapy. An improved understanding of the mechanisms that cause JMML is critical to developing new treatments. Dr. Cantor is studying a protein called GATA2, which normally turns on and off white blood cell genes, to determine if it is incorrectly activated in JMML. If so, the results of this project will support development of medicines to inhibit GATA2 for the treatment of JMML.

Neuroblastoma is a common type of childhood cancer that arises from nerve-like cells and causes tumors just outside the brain. Dr. George is studying tumor cells from patients to discover new molecular targets for treatment of neuroblastoma. Dr. George and his team are growing tumor cells from patients and examining their electrical properties in order to identify specific proteins that carry electrical current that may be new targets for treating neuroblastoma using existing non-cancer drugs.

Relatively little is currently known about the cellular and molecular mechanisms of medulloblastoma spread throughout the spinal fluid. Dr. Keller's preliminary findings show that medulloblastoma tumor cells actively migrate to the surface of the covering of the brain and spine, rather than arriving passively. Dr. Keller is investigating the efficacy of stopping the tumor cells from migrating to the brain and spine surfaces, which, if successful, will provide a rationale for future clinical trials.

Dr. Wechsler and his team study how normal white blood cells turn into leukemia cells. They have discovered that a protein called CRM1 is directly involved in turning on specific genes that cause leukemia to develop. Dr. Wechsler is studying this previously unrecognized function of CRM1 by identifying other proteins that are required for CRM1 to turn on. This research aims to allow Dr. Wechsler to design new drugs that can selectively target leukemia cells and increase cure rates.

Ewing sarcoma is a cancer of bone and soft tissue in children and young adults, which is fatal if untreated. While often successful, therapies for Ewing sarcoma have severe long-term side effects for survivors. Dr. Lombard is testing a new means of treating Ewing sarcoma, by targeting the mitochondrion, the metabolic hub of the cell. Dr. Lombard and his team have early results to suggest that this new approach may provide a way to efficiently kill Ewing sarcoma cells, with little impact on normal cells and organs.

This grant is named for Love Your Melon, an apparel brand dedicated to giving a hat to every child battling cancer in America as well as supporting nonprofit organizations who lead the fight against pediatric cancer.

Progress in improving therapy for Acute myeloid leukemia (AML) has been slow and survival rates for patients remain quite low. Thus, there is a great need for more effective and less toxic therapies for AML. Dr. DeGregori has identified a new molecule called MCJ, the loss of which is associated with the resistance of cancers to therapies. Dr. DeGregori has developed novel drugs that can restore MCJ function in cancer cells, and is investigating whether these MCJ activating drugs can be used improve therapies for AML.

Genes instruct cells to do their jobs through making specific proteins. In the human body, all cells store these "instructions" in the chromosomes. When chromosomes break off, the broken pieces sometimes change places and create new chromosomes. These changes are called chromosomal translocations. Dr. Su is studying how chromosomal translocations cause deadly diseases in children and young adults, and more importantly, is investigating possible clinical options to correct these abnormal conditions.

Childhood brain tumors are frequently quite different than those of adults. Dr. Eck's For the Love of Jack St. Baldrick''s Research Grant aims to find new 'targeted' therapies for low-grade astrocytomas (a type of brain tumor) in children that are caused by a mutation in a protein called BRAF. BRAF mutations are common in cancer, and drugs have been developed that are effective in some tumors caused by one type of BRAF mutation. Unfortunately, these drugs do not work on the BRAF mutation found most often in pediatric brain tumors. Dr. Eck is using detailed information about the molecular structure of the BRAF mutation found in pediatric brain tumors to discover new drugs that specifically target this cause of brain tumors in children. Jack Tweedy was diagnosed with brain and spinal cancer when he was two. Since then he has endured multiple surgeries and 270 weeks of chemotherapy but never fails to uplift those around him. Together with his family, he inspires others to help fund the best research to ensure that all cancer warriors have better treatment options.

The interaction between two important cancer-related proteins called MDM4 and TOP2A may cause cancer and contribute to disease progression. Dr. Zhou is studying the regulation of MDM4 and TOP2A to identify small-molecule inhibitors (agents) that can block the MDM4-TOP2A interaction, leading to inhibition of these two proteins. The results of these studies will provide important clues to help scientists develop novel methods and drugs to specifically and simultaneously target TOP2A and MDM4 for treatment of pediatric cancer patients.

Treatment of childhood acute lymphoblastic leukemia (ALL) using chemoradiation can be successful, but it is difficult to manage treatment-associated side events and secondary cancers. Furthermore, in relapsed/refractory patients, the overall prognosis remains dismal. Direct inhibition of the main proteins promoting cancer (the 'oncogenes') is not successful in ALL. Dr. Ntziachristos's "Just Do It...and be done with it" St. Baldrick's Research Grant will study certain oncogene-supporting mechanisms that might be specific to a diseased state, and not to a healthy state. Dr. Ntziachristos has selected one of these mechanisms to target in ALL models, and is assessing the anti-cancer activity that results. Such experiments could pave the way for clinical trials for high-risk disease.

This grant is named for the "Just Do It...and be done with it" Hero Fund created in honor of Sara Martorano who doesn''t let anything dim her sparkle and has a compassionate heart and smile. It also celebrates the courage of all cancer kids through treatment and the support of their family and friends.

Diffuse Intrinsic Pontine Glioma is a type of incurable brain tumor that affects young children. Despite treatment with radiation and chemotherapy, the tumor exhibits resistance to current treatments and grows back. Dr. Beroukhim is studying the tumors at a single-cell level to determine how they become resistant to treatments, which will help guide the development of combination therapies to improve outcomes.

This grant is made with generous support from the McKenna Claire Foundation established by the Wetzel family in memory of their daughter, McKenna. Their mission is to cure pediatric brain cancer by raising awareness, increasing community involvement and funding research.

Medulloblastoma (MB) is a highly aggressive pediatric brain tumor for which safer and more effective therapies are needed. Recent studies have identified four major forms of MB that differ in terms of molecular characteristics and patient outcomes. Dr. Wechsler-Reya is working to identify genes that drive Group 4 MB tumor formation, the most prevalent form of MB, to develop new strategies for treatment of this devastating disease.

Medulloblastoma (MB) is the most common malignant pediatric brain tumor, yet currently has no optimal treatment options. Medulloblastoma has been classified into 4 major subgroups, and Dr. Chen is targeting methylation mutations to develop improved therapeutics for two highly-aggressive subgroups of medulloblastoma. To facilitate this, Dr. Chen is establishing precision models of this disease to screen and test for therapeutics. To systematically identify protein targets required for survival of MB cells, Dr. Chen and colleagues are performing a genome screen to look for possible targets, in order to enhance understanding of this disease and lead to novel therapeutic routes.

Targeted therapy works by attacking an abnormal gene product that is specific to the cancer type. Only a minority of neuroblastoma types show genetic drivers, which makes it difficult to develop targeted therapy. Most neuroblastomas show too many or too few copies of large chromosomal regions, called CNAs. Dr. Weiss is studying the connection between CNAs and neuroblastoma, to determine if it CNA is a possible candidate for targeted therapy. Dr. Weiss is engineering CNAs to create CNA-driven models of neuroblastoma, which he will then use to identify CNA-specific therapies to treat neuroblastoma.

Neuroblastoma is the second most common solid tumor in children, and is a cancer that frequently metastasizes to the bone marrow. Dr. DeClerck is studying how neuroblastoma cells "teach" bone marrow cells to promote tumor growth.