1.Temozolomide Chemotherapy for the Treatment of a Recurrent and Progressive Malignant Glioma.
Seung Ho YANG ; Yong Kil HONG ; Tae Kyu LEE ; Moon Chan KIM
Journal of Korean Neurosurgical Society 2004;35(3):235-239
OBJECTIVE: Temozolomide is a novel oral alkylating agent, which has been reported to be effective in treating patients with recurrent malignant gliomas. This study report an analysis of the activity and toxicity of temozolomide as second-line therapy for patients with recurrent and progressive malignant gliomas after surgery and standard radiation therapy with or without chemotherapy. METHODS: Twenty patients with malignant gliomas of which thirteen(65%) had glioblastoma multiforme(GBM), five(25%) with anaplastic astrocytoma(AA), and two(10%) with anaplastic oligodendroglioma(AO) were enrolled in this study. They had been treated in our institution since July, 2000 and had been previously irradiated with or without chemotherapy. For the patients with recurrent and progressive disease, temozolomide(150-200mg/m2/d x5 days) was administered every 28 days until the progression of the tumor or toxicity developed. RESULTS: The median number of treatment cycles was 3(total 86). Of the 20 patients, 2(10%) achieved a complete response(CR), 5(25%) achieved a partial response(PR), 5(25%) had stable disease(SD), and 8(40%) had progressive disease(PD). One patient achieved a CR, 3 patients achieved a PR, 2 patients had SD and 7 patients had PD in GBM, and 1 patient achieved a CR, 2 patients achieved a PR, 3 patients had SD, 1 patient had PD in the non-GBM patients. Median progression free survival(PFS) was 8 weeks in GBM and 22 weeks in the non-GBM patients. No hematological toxicity greater than grade 2 was observed, and hepatotoxicity of grade 2 was encountered in 1(5%) patient. CONCLUSION: Temozolomide demonstrate moderate activity in recurrent and progressive malignant brain tumors, and the response rate and PFS were better in the non-GBM tumors than in the GBM tumors. The treatment is well tolerated without any serious toxicity.
Brain Neoplasms
;
Drug Therapy*
;
Glioblastoma
;
Glioma*
;
Humans
2.Phase III Randomized Trial of ACNU in Addition to Surgery and Radiotherapy for Patients with Supratentorial Malignant Gliomas.
Hee Won JUNG ; Chang Wan OH ; Chun Kee CHUNG ; Hee Jin YANG ; Kil Soo CHOI ; Dae Hee HAN ; Je G CHI ; Yung Jue BANG ; Dae Seog HEO ; Noe Kyeong KIM ; Yoon Ok AHN ; Il Han KIM
Journal of the Korean Cancer Association 1997;29(4):608-615
No abstract available
Drug Therapy
;
Glioma*
;
Humans
;
Nimustine*
;
Radiotherapy*
4.Surgical Treatment of the Intracranial Gliomas.
Journal of Korean Neurosurgical Society 1990;19(3):307-315
In the treatment of the intracranial gliomas surgical intervention is recommended as the standard procedure which should be performed in all cases when the tumor is accessible. While surgery will not bring about a cure and clearly, radiation therapy and chemotherapy have made a significant impact of long-term survival in the treatment of the malignant gliomas, nevertheless surgery still remains the single most effective method for achieving a rapid reduction of tumor burden reducing increased intracranial pressure and provides a tissue diagnosis. Following surgery, the other antitumor programs have the best chance of achieving a significant increment of tumor cell kill, therefore, surgery has a distinct role to play in the multidisciplinable approach to the treatment of these highly aggressive malignant tumors. It is very unlikely that future advances will obviate the necessity for conventional surgery in the treatment of benign gliomas. The surgical management of gliomas with major emphasis on malignant ones is presented including the pathophysiology, radiological diagnosis, aim of surgery, surgical procedure and some different possibility of surgical treatment. Prospective future development of surgical treatment of brain tumor is also considered.
Brain Neoplasms
;
Diagnosis
;
Drug Therapy
;
Glioma*
;
Intracranial Pressure
;
Tumor Burden
5.Clinical Outcome of the Mixed Glioma: Preliminary Analysis.
Seung Jin CHOI ; Kwan Sung LEE ; Yong Kil HONG ; Hyung Kyun RHA ; Sang Won LEE ; Min Woo BAEK ; Moon Chan KIM ; Joon Ki KANG
Journal of Korean Neurosurgical Society 1998;27(12):1700-1709
The authors analyzed preliminary outcome of 10 patients with mixed glioma(3 patients with low-grade oligoastrocytoma and 7 patients with anaplastic oligoastrocytoma) who underwent surgical resection and were treated or are in treatment with or without adjuvant therapy at our institute since May 1993. In the low-grade oligoastrocytoma group, gross total tumor resection was done in all three cases and postoperative radiation therapy was performed in 2 cases. In the anaplastic oligoastrocytoma group, all seven cases were divided as to the amount of tumor removal(gross total resection; 4 cases, subtotal resection; 1 case, partial resection; 2 cases) and clinical course and prognosis were analyzed as to performing postoperative radiation therapy with or without chemotherapy. In the low-grade oligoastrocytoma group, one patient who didn't undergo postoperative radiation therapy suffered from tumor recurrence that showed histopathologically malignant transformation. In the anaplastic oligoastrocytoma group, 2 patients who underwent subtotal tumor resection and partial tumor resection with postoperative radiation therapy showed tumor progression and histopathologically more malignant transformation. The authors propose that gross total tumor resection with postoperative radiation therapy in low-grade oligoastrocytoma and adding chemotherapy(especially with procarbazine, lomustine, vincristine; PCV regimen) in anaplastic oligoastrocytoma appear to be associated with more prolongation of patient's survival.
Drug Therapy
;
Glioma*
;
Humans
;
Lomustine
;
Procarbazine
;
Prognosis
;
Recurrence
;
Vincristine
6.Phase III Randomized Trial of ACNU in Addition to Surgery and Radiotherapy for Patients with Malignant Glioma of the Brain: A Preliminary Report.
Hee Won JUNG ; Chun Kee CHUNG ; Je G CHI ; Yung Jue BANG ; Dae Seog HEO ; Yoon Ok AHN ; Il Han KIM ; Noe Kyeong KIM ; Kil Soo CHOI ; Dae Hee HAN
Journal of Korean Neurosurgical Society 1992;21(9):1095-1101
No abstract available.
Astrocytoma
;
Brain*
;
Drug Therapy
;
Glioblastoma
;
Glioma*
;
Humans
;
Nimustine*
;
Radiotherapy*
7.Treatment of Recurrent Gliomas with PCV Chemotherapy : A Preliminary Report.
Ji Soo JANG ; Jae Wook SONG ; Sang Min YOUN ; Chang Hun RHEE ; Seung Hoon LEE
Journal of Korean Neurosurgical Society 1996;25(11):2229-2233
Twelve patients with recurrent malignant glioma were treated with combination chemotherapy, consisting of procarbazine(60mg/m2, 8th-21th day), CCNU(110mg/m2, 1st day), and vincristine(1.4mg/m2, 8th and 29th day) every 6 weeks. Most patients had undergone initial resection of primary tumor, postoperative radiotherapy, and another form of chemotherapy. Response or progression was defined as improvement or deterioration in MRI scan. Assessment of response followed evaluation of MRI obtained after the completion of each two cycles of chemotherapy, if possible. Partial(more than 50% reduction of tumor mass) response at 15+ to 47+ weeks after chemotherapy was noted in three(60%) of the five patients with recurrent oligodendrogliomas. But in patients with recurrent anaplastic astrocytoma or gllioblastoma, partial response at 8+ weeks after chemotherapy was noted in one(14%) of the seven patients. It is suggested that PCV chemotherapy is more effective for patients with recurrent oligodendrogliomas than other recurre nt gliomas.
Astrocytoma
;
Drug Therapy*
;
Drug Therapy, Combination
;
Glioma*
;
Humans
;
Magnetic Resonance Imaging
;
Oligodendroglioma
;
Radiotherapy
8.Advances in the Immunotherapeutic Potential of Isocitrate Dehydrogenase Mutations in Glioma.
Feng TANG ; Zhiyong PAN ; Yi WANG ; Tian LAN ; Mengyue WANG ; Fengping LI ; Wei QUAN ; Zhenyuan LIU ; Zefen WANG ; Zhiqiang LI
Neuroscience Bulletin 2022;38(9):1069-1084
Isocitrate dehydrogenase (IDH) is an essential metabolic enzyme in the tricarboxylic acid cycle (TAC). The high mutation frequency of the IDH gene plays a complicated role in gliomas. In addition to affecting gliomas directly, mutations in IDH can also alter their immune microenvironment and can change immune-cell function in direct and indirect ways. IDH mutations mediate immune-cell infiltration and function by modulating immune-checkpoint gene expression and chemokine secretion. In addition, IDH mutation-derived D2-hydroxyglutarate can be absorbed by surrounding immune cells, also affecting their functioning. In this review, we summarize current knowledge about the effects of IDH mutations as well as other gene mutations on the immune microenvironment of gliomas. We also describe recent preclinical and clinical data related to IDH-mutant inhibitors for the treatment of gliomas. Finally, we discuss different types of immunotherapy and the immunotherapeutic potential of IDH mutations in gliomas.
Brain Neoplasms/therapy*
;
Glioma/therapy*
;
Humans
;
Immunotherapy
;
Isocitrate Dehydrogenase/genetics*
;
Mutation/genetics*
;
Tumor Microenvironment
9.High-grade gliomas: reality and hopes.
Chinese Journal of Cancer 2014;33(1):1-3
In this issue of the Chinese Journal of Cancer, European experts review current standards, trends, and future prospects in the difficult domain of high-grade glioma. In all fields covered by the different authors, the progress has been impressive. For example, discoveries at the molecular level have already impacted imaging, surgery, radiotherapy, and systemic therapies, and they are expected to play an increasing role in the management of these cancers. The European Organization for Research and Treatment of Cancer (EORTC) has pioneered new treatment strategies and contributed to new standards. The articles in this issue will cover basic molecular biological principles applicable today, novel surgical approaches, innovations in radiotherapy planning and delivery, evidence-based standards for radiotherapy alone or combined with chemotherapy, current standards and novel approaches for systemic treatments, and the important but often neglected field of health-related quality of life. Despite the advances described in these articles, the overall prognosis of high-grade glioma, especially glioblastoma, remains poor, and more research is needed to address this problem.
Brain Neoplasms
;
pathology
;
therapy
;
Combined Modality Therapy
;
Glioblastoma
;
pathology
;
therapy
;
Glioma
;
pathology
;
therapy
;
Humans
;
Neoplasm Grading
;
Quality of Life
10.Study in the killing effect of Myxoma virus to C6 glioma cell in vitro.
Meng ZANG ; Qiu-Sheng ZHANG ; Shi-Jie LIANG ; Tao JI ; Heng-Zhou LIN ; Wei-Ping LI
Chinese Journal of Experimental and Clinical Virology 2012;26(1):43-45
OBJECTIVETo evaluate the susceptibility of C6 glioma cells to Myxoma virus and the killing effect of Myxoma virus to the C6 glioma cells in vitro.
METHODSC6 glioma cells were infected with myxoma virus, used death virus as the negative control, 5-FU as the positive control, DEMD as blank control. The number of living cells were counted every 24 h, and Western-Blot method, inverted microscope and MTT assay were applicated to observe the cell morphology and survival rate in each group.
RESULTSThe cell number were decreased rapidly in virus effected group and 5-FU group, with significant differences to the negative and blank control groups. And cells in virus effected group appeared cytopathic effect.
CONCLUSIONSC6 glioma cells were susceptible to myxoma virus and myxoma virus had killing effect to C6 glioma cells in vitro.
Cell Line, Tumor ; Glioma ; therapy ; Humans ; Myxoma virus ; Oncolytic Virotherapy ; Proto-Oncogene Proteins c-akt ; physiology