Literature DB >> 16774296

Treatments for astrocytic tumors in children: current and emerging strategies.

Stanislaw R Burzynski1.   

Abstract

Strategies for the treatment of childhood cancer have changed considerably during the last 50 years and have led to dramatic improvements in long-term survival. Despite these accomplishments, CNS tumors remain the leading cause of death in pediatric oncology. Astrocytic tumors form the most common histologic group among childhood brain tumors. They are a heterogeneous group that from a practical therapeutic point of view can be subdivided into low-grade astrocytomas (LGA), optic pathway gliomas (OPG), high-grade astrocytomas (HGA), and brainstem gliomas (BSG). This article focuses on the practical application of treatments that lead to long-term survival, improved quality of life, and reduced long-term complications. Improvement in therapy has led to better outcomes for patients with LGA and OPG. Careful follow-up without any treatment is indicated for a small percentage of patients diagnosed with LGA with an indolent course including children with neurofibromatosis type 1 (NF1). Surgery is the main recommended treatment for children with resectable LGA. Radiation therapy is generally recommended for children with progressive LGA, or after failure of chemotherapy, accomplishing tumor control at 10 years in over 60% of patients. Cytotoxic chemotherapy is usually reserved for children who have had treatment failure with surgery and radiation therapy. It is also offered for children who are too young to be treated with radiation or to defer or avoid radiotherapy. Carboplatin and vincristine achieve 5% complete and 28% partial responses but the use of vincristine is criticized due to poor penetration of the CNS. A regimen of tioguanine, procarbazine, mitolactol, lomustine, and vincristine is frequently administered as an alternative to carboplatin and vincristine in LGA. The introduction of temozolomide has allowed better responses, including a 24% complete response rate compared with 0-5% complete response rates with the previous regimens. OPG are usually histologically LGA, and are treated with similar chemotherapy regimens. OPG is the most common type of brain tumor associated with NF1. Tumor growth in some of these patients is slow with no treatment recommended for an extended period of time. The prognosis for children with the remaining types of astrocytomas remains poor. Surgical resection is typically the first step in the treatment of HGA followed in older children by radiation therapy. The data regarding chemotherapy are mixed. Combination chemotherapy before or after radiation, including cisplatin, carmustine, cyclophosphamide, and vincristine or carboplatin, ifosfamide, cyclophosphamide, and etoposide has provided disappointing results. Clinical trials with temozolomide and agents directed against single targets have not shown substantially better results, but it is hoped that currently conducted studies will provide better outcomes. Diffuse intrinsic BSG are among the most difficult-to-treat brain tumors. Surgical treatment is not recommended for diffuse intrinsic BSG and standard radiation therapy is typically given in children aged >3 years. None of the numerous chemotherapy regimens, including temozolomide, has provided a significant response rate or an improvement in survival. It is expected that newer agents affecting multiple targets such as AEE-788 and antineoplastons, and combinations of single-targeted agents with chemotherapy will provide better results. Careful evaluation of histology, location of the tumor, patient age, and consideration of treatment-related morbidity play an important part in selecting between clinical observation, surgery, radiation, chemotherapy, or investigational agents. The goals of treatment for astrocytic tumors should extend well beyond objective responses and increased survival. Improvement of quality of life is an equally important objective of treatment. Radiation therapy and chemotherapy result in serious late toxicities.

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Year:  2006        PMID: 16774296     DOI: 10.2165/00148581-200608030-00003

Source DB:  PubMed          Journal:  Paediatr Drugs        ISSN: 1174-5878            Impact factor:   3.022


  125 in total

1.  A detrimental effect of a combined chemotherapy-radiotherapy approach in children with diffuse intrinsic brain stem gliomas?

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4.  Low grade chiasmatic-hypothalamic glioma-carboplatin and vincristin chemotherapy effectively defers radiotherapy within a comprehensive treatment strategy -- report from the multicenter treatment study for children and adolescents with a low grade glioma -- HIT-LGG 1996 -- of the Society of Pediatric Oncology and Hematology (GPOH).

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Journal:  Curr Neurol Neurosci Rep       Date:  2001-03       Impact factor: 5.081

7.  Vinca alkaloid-induced cardiovascular autonomic neuropathy.

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8.  Temozolomide is active in childhood, progressive, unresectable, low-grade gliomas.

Authors:  Dennis J Kuo; Howard L Weiner; Jeffrey Wisoff; Douglas C Miller; Edmond A Knopp; Jonathan L Finlay
Journal:  J Pediatr Hematol Oncol       Date:  2003-05       Impact factor: 1.289

9.  Current neurosurgical management and the impact of the extent of resection in the treatment of malignant gliomas of childhood: a report of the Children's Cancer Group trial no. CCG-945.

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Journal:  J Neurosurg       Date:  1998-07       Impact factor: 5.115

10.  Ocular toxicity associated with high-dose carmustine.

Authors:  B J Shingleton; D C Bienfang; D M Albert; W D Ensminger; W F Chandler; H S Greenberg
Journal:  Arch Ophthalmol       Date:  1982-11
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  9 in total

1.  Incidence of vasculopathy in children with hypothalamic/chiasmatic gliomas treated with brachytherapy.

Authors:  U Tacke; D Karger; J Spreer; A Berlis; G Nikkhah; R Korinthenberg
Journal:  Childs Nerv Syst       Date:  2011-03-17       Impact factor: 1.475

2.  Interpreting mammalian target of rapamycin and cell growth inhibition in a genetically engineered mouse model of Nf1-deficient astrocytes.

Authors:  Sutapa Banerjee; Scott M Gianino; Feng Gao; Uwe Christians; David H Gutmann
Journal:  Mol Cancer Ther       Date:  2011-01-07       Impact factor: 6.261

3.  Phase II trial of tipifarnib and radiation in children with newly diagnosed diffuse intrinsic pontine gliomas.

Authors:  Daphne A Haas-Kogan; Anuradha Banerjee; Tina Young Poussaint; Mehmet Kocak; Michael D Prados; J Russell Geyer; Maryam Fouladi; Alberto Broniscer; Jane E Minturn; Ian F Pollack; Roger J Packer; James M Boyett; Larry E Kun
Journal:  Neuro Oncol       Date:  2011-03       Impact factor: 12.300

4.  Temozolomide-mediated radiosensitization of human glioma cells in a zebrafish embryonic system.

Authors:  Geoffrey A Geiger; Weili Fu; Gary D Kao
Journal:  Cancer Res       Date:  2008-05-01       Impact factor: 12.701

5.  Treatment Outcomes and Prognostic Factors in Pediatric Non-brainstem Astrocytoma in North East of Iran.

Authors:  Kazem Anvari; Mehdi Seilanian Toussi; Gholamreza Bahadorkhan; Motahare Bitaghsir; Mozhgan Heidari; Mitra Fazl Ersi; Soodabeh Shahidsales
Journal:  Iran J Cancer Prev       Date:  2014

6.  The response and survival of children with recurrent diffuse intrinsic pontine glioma based on phase II study of antineoplastons A10 and AS2-1 in patients with brainstem glioma.

Authors:  Stanislaw R Burzynski; Tomasz J Janicki; Gregory S Burzynski; Ania Marszalek
Journal:  Childs Nerv Syst       Date:  2014-04-10       Impact factor: 1.475

7.  Novel drugs in pediatric gliomas.

Authors:  Dongli Zhang; Xiaoming Liu; Conghai Fan; Jiao Chen
Journal:  Oncol Lett       Date:  2017-03-06       Impact factor: 2.967

8.  Long-term survival (>13 years) in a child with recurrent diffuse pontine gliosarcoma: a case report.

Authors:  Stanislaw R Burzynski; Tomasz J Janicki; Gregory S Burzynski; Ania Marszalek
Journal:  J Pediatr Hematol Oncol       Date:  2014-10       Impact factor: 1.289

9.  Drug repositioning via matrix completion with multi-view side information.

Authors:  Yunda Hao; Menglan Cai; Limin Li
Journal:  IET Syst Biol       Date:  2019-10       Impact factor: 1.615

  9 in total

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