Cancer Therapy Vol 5, page 243 Cancer Therapy Vol 5, 243-252, 2007 Management of recurrent high-grade gliomas Research Article !ihomir N. Eftimov1, Ivan D. Ivanov1, Alexander P. Petkov1, Emil Nakov2 1 2 Clinic of Neurosurgery Laboratory of Pathomorphology, Military Medical Academy-Sofia, Bulgaria __________________________________________________________________________________ *Correspondence: Tihomir Eftimov, M.D., Ph.D., Clinic of Neurosurgery, Military Medical Academy, 3, “Georgi Sofiiski” blvd., 1606, Sofia, Bulgaria; e-mail: t_eftimov @ hotmail.com Key words: recurrent high-grade gliomas, repeated surgical resection, chemotherapy, radiotherapy, interstitial chemotherapy, Gliadel, Karnofsky Performance Scale (KPS), Quality of Life Questionnaire QLQ-C30 Abbreviations: anaplastic astrocytomas, (AAs); Computed Tomography, (CT); glioblastoma multiforme, (GBM); intracranial pressure, (ICP); Karnofsky Performance Scale, (KPS); Magnetic Resonance Imaging, (MRI) Received: 9 September 2007; Revised: 25 October 2007 Accepted: 29 October 2007; electronically published: November 2007 Summary The biological behavior and clinical symptoms of high-grade gliomas are extremely variable. Treatment options in cases of recurrence are usually limited after initial therapy. The objective of our study is to present the results of the multimodal treatment in patients with recurrent high-grade gliomas and discuss some prognostic factors. Thirtytwo patients in five-year period (2001-2005) were treated with repeated surgery, chemotherapy, and re-irradiation in the case of recurrent high-grade gliomas. Based on the histopathological examination the patients were divided into two groups: 12 (37.5%) with recurrent anaplastic astrocytomas (AAs) and 20 (62.5%) with recurrent glioblastoma multiforme (GBM). The volume of surgical resection was assessed by comparing the preoperative and control Computed Tomography (CT) and(or Magnetic Resonance Imaging (MRI) findings. All patients were assessed pre- and postoperatively by Karnofsky Performance Scale (KPS). The quality of life in all survived patients was measured by EORTC QLQ-C30. Five of patients with recurrent GBM were treated with Temozolomide after first operation and one patient obtained interstitial chemotherapy with Gliadel. Twelve (37.5%) operated patients with recurrent high-grade gliomas had good results (KPS=80-100), 10 patients (31%) had different morbidity (KPS=60-70), and 6 (19%) had poor outcome (KPS<50). Four patients (12.5%) died. The following surgical complications were diagnosed by the control CT in the early postoperative period: hematoma in loco of the excised tumor - in 5 patients (15.6%); brain edema with dislocation and herniation syndrome - in 4 (12.5%), and hydrocephaly - in 2 (6%) patients. Surgical treatment of recurrent high-grade gliomas is appropriate in young patients with solid or cystic part of the tumor without infiltration of eloquent area and deep brain structures and longer interval between the primary operation and tumor recurrence. remain asymptomatic (Vecht et al, 1990; Huber et al, 1993; Harsh, 1995, 1999; Lote et al, 1998; Hou et al, 2006). The indications and choice for optimal treatment in cases of tumor recurrence are controversial, and still disputable. The new operative strategies and treatment algorithms for recurrent high-grade gliomas are sought, because the possibilities for treatment are limited after the primary treatment (Ransohoff et al, 1978; Young et al, 1981; Ammirati et al, 1987; Harsh et al, 1987; Fadul et al, 1988; Voynov et al, 2002; Hou et al, 2006; Westphal et al, 2006). Gross total surgical resection is, however, associated with serious postoperative morbidity considering the localization, sizes and the infiltrative nature of tumor. I. Introduction The biological behavior and clinical symptoms of high-grade gliomas are extremely variable (Muller et al, 1977; Burger et al, 1985; Kaluza and Pyrich, 1994; Harsh, 1995, 1999; Alba et al, 1999). Irrespective of the aggressive primary treatment (radicalism of surgical resection and multimodal adjuvant chemotherapy and radiotherapy) high-grade gliomas tend to reoccur within averagely 6 to 11 months after the primary treatment (Vick et al, 1989; Vecht et al, 1990; Dirks et al, 1993; Rostomily et al, 1994; Gomori et al, 2002; Salvati et al, 1998). Recurrent high-grade gliomas demonstrate different clinical symptoms. Epilepsy alone can be controlled by drugs therapy, while patients with focal neurological deficit and increased intracranial pressure (ICP) demand operative treatment. Some of recurrent high-grade gliomas 243 Eftimov et al: Management of recurrent high-grade gliomas interval between the two operative interventions was recorded. The diagnosis was defined on the base of neurological examination, CT and MRI findings and histopathological results. The tumor localization was identified as „superficial” (cortical and subcortical) in 11 (34%) patients and „profound” (basal ganglia, corpus callosum, ventricular infiltration) in 21 (66%) patients. Median time to recurrence was in AAs group 49, 3 weeks and in GBM group - 20,7 weeks after the initial operation. The extension of surgical resection was assessed by comparing the preoperative and control CT and MRI findings. In all patents early postoperative CT scans were done: Postoperative MRI in the first month after reoperation was provided in 12 (37,5%) patients. According to the results of early postoperative neuroimaging investigations the patients were divided into three groups: 1. with partial tumor resection (< 50%); 2. with subtotal tumor resection (50% - 90%) and 3. with “gross total” tumor resection (> 90%). All patients were assessed pre- and postoperatively by Karnofsky Performance Scale (KPS): 1. minor disability (80-100 points); 2. moderate disability (60-70 points) and 3. severe disability (10-50 points). The quality of life in all survived patients was measured by QLQ-C30 comparing preoperative and postoperative scores. The postoperative complications were divided into surgical (edema with “mass effect" and herniation syndromes, hematoma in loco of tumor resection, hydrocephaly, deterioration or new neurological deficit etc.) and non-surgical ones. The radiotherapy (including stereotaxic radiosurgery) may be contraindicated because the maximum tolerable dose was already reached with preceding exposures. The chemotherapy is an alternative, despite the limited drugs available for these types of tumors and the possible onset of acquired drug resistance. Interstitial chemotherapy with Gliadel and interstitial radiotherapy are not a routine treatment options. It is extremely difficult to determine the indications for re-operation in patients with recurrent high-grade gliomas as the main goal is to prolong and safe the quality of life in treated patients. When deciding for repeated surgical interventions, the potential surgical complications, including lethal outcome should be taken into consideration. Would a new reoperation be appropriate in patients without clinical symptoms, but with CT and MRI evidence for a tumor recurrence? Are the clinical symptoms and neuroimaging evidence rather directly related to the tumor recurrence or a result of a radionecrotic or inflammatory process? What other therapy following the operative treatment could be proposed? The objective of our study is to present the results of the reoperative treatment in patients with recurrent highgrade gliomas and discuss some prognostic factors: pathomorphology of the primary and recurrent tumor, patients’ age, preoperative neurological and performing status, intervals between the first and second operation, volume of the operative intervention etc. III. Results All patients with recurrent high-grade gliomas were operated on. Two operative interventions underwent 24 (75%) patients (14 with AAs and 10 with GBM). Three and more operations were done in 8 (25%) patients (6 with AAs and 2 with GBM). The volume of tumor resection at first reoperation is shown on Figure 1. In 14 (44%) patients neuronavigation control was used during the first reoperation and in 6 (19) patients during the second reoperation, with satisfactory postoperative results (Figures 2, 3, 4). The adjuvant postoperative chemotherapy with Temodal was achieved in 5 (25%) of reoperated patients with recurrent GBM. Other patients were treated with CCNU. Radiotherapy alone was administered in 3 (9%) II. Material and Methods Thirty-two patients with recurrent high-grade gliomas have been hospitalized and operated on at the Clinic of Neurosurgery of the Military Medical Academy-Sofia over a five-year period (2001-2005). The mean age of patients with recurrent high-grade gliomas was 56.28 years +(- 10.54 with sex ratio: men/women = 1.3. Based on the histopathological examination after reoperation the patients were divided into two groups: 12 (37.5%) with recurrent anaplastic astrocytomas (AAs) and 20 (62.5%) with recurrent glioblastoma multiforme (GBM). The Figure 1. Volume of tumor resection of the recurrent high-grade gliomas at the first reoperation. 244 Cancer Therapy Vol 5, page 245 Figure 2. Deep situated recurrent GBM in corpus callosum (a) and basal ganglions (b) and (c) with partial tumor resection. Figure 3. Clinical case 1. 32 year-old man who underwent reoperation due to recurrent GBM of the corpus callosum. One year later, control MRI was performed on which tumor recurrence was found (a), (b), (c). The control CT (d) and MRI (e), (f) after the reoperation showed partial tumor excision. The outcome was lethal 18 months after the first operation. Figure 4. Clinical case 2. A 37 year-old man who underwent reoperation due to recurrent GBM 6 months after the first operation – prereoperative MRI (a), (b) and early CT-control after the reoperation - subtotal tumor resection (c). 245 Eftimov et al: Management of recurrent high-grade gliomas patients. Combined adjuvant chemotherapy and fractioned radiotherapy was administered in 8 (25%) patients to the maximum tolerated dose of 60 Gy with the concurrent administration of Temodal - 75 mg/m2 over 6 weeks, in 5 consecutive days. The adjuvant radiotherapy (alone or in conjunction with Temodal) was administered in those patients who had not been administered radiotherapy after the first operation. In one of our patients we were able to perform the interstitial chemotherapy by intraoperative application of Gliadel, in conjunction with postoperative systemic chemotherapy with Temodal (Figure 5). One month after the reoperation, however, we observed pronounced adverse effects (skin rush and acute abdominal pains), which are generally reported at the administration of Gliadel (Figure 6a). The chemotherapy with Temozolomide was administrated. In 2 months MRIcontrol showed a tumor recurrence, great in size, with pronounced grow infiltrativeness. After the third operation the histopathology confirmed GBM. The lethal outcome set in 10,2 months after the primary diagnostics (Figure 6b). Figure 5. Clinical case 3. A 47 year-old man who underwent reoperation due to recurrent GBM 8 months after the first operation – prereoperative MRI (a). Intraoperatively Gliadel Implant 61,6 mg was placed into resection cavity (b). Early postoperative CT-imaging showed subtotal tumor resection and Gliadel placement into resection cavity (c). Figure 6. Rush-syndrome after implantation of Gliadel (a). Control MRI-imaging in 2 months after reoperation and interstitial chemotherapy with Gliadel. The following surgical complications were diagnosed by the control CT in the early postoperative period: hematoma in loco of the excised tumor recurrence - in 5 patients (15.6%); brain edema with dislocation and herniation syndrome - in 4 (12.5%), and hydrocephaly - in 2 (6%) patients. No lethal surgical complications were observed. Twelve (37.5%) operated patients with recurrent high-grade gliomas had good results (KPS=80-90), 10 patients (31%) had different morbidity (KPS=60-70), and 6 (19%) had poor outcome (KPS<50). Four patients (12.5%) had lethal outcome due to somatic complications (pulmonary thromboembolism, cardio-vascular insufficiency, gastro-intestinal hemorrhage) in early postoperative period (Table 1). Patients over 60 years age with KPS below 50 score formed the greatest absolute number and relative share in comparison to the younger patients with poor outcome (p<0.05) (Figure 7). The postoperative results show that the rate of patients with KPS<60-70 points is lower than the preoperative rate, on the account of increased relative share of the patients with good results (KPS=80-100), and those whose neurological status has deteriorated postoperatively (KPS<50) (Figure 8). Good postoperative results (KPS=80-100) are related to “superficial” (cortical and subcortical) tumor localization, and are limited to the temporal, frontal and occipital lobe, whereas bad results, leading to high disability rate, are related to deep (basal ganglia) and 246 Cancer Therapy Vol 5, page 247 bilateral (corpus callosum) localization of the recurrent tumor. Measuring quality of life by EORTC QLQ-C30 in all survived patients after and before reoperation we found an improvement in 12(37,5%) and deteriorating in 16(50%) retreated patients (Table 2). Statistically significant differences were observed for 5 of the QLQ-C30 scales: physical functioning (p<0.001), role functioning (p<0.001), fatigue (p<0.01), nausea and vomiting (p<0.05) and global quality of life (p<0.01). Kaplan-Mayer curves show 4,6 months median survival in patients with recurrent GBM and 6,7 months in patients with recurrent AAs (p=0,1256) after the last operation (Figure 9). The management of recurrent high-grade gliomas varies from repeated efforts at aggressive surgical resection combined with chemotherapy and radiotherapy to no therapeutic intervention at all (Young et al, 1981; Ammirati et al, 1987; Harsh et al, 1987; Vecht et al, 1990; Dirks et al, 1993; Voynov et al, 2002; Chang et al, 2006; Hou et al, 2006). Regardless of the used surgical technique, however, “superfluous aggressiveness” of the surgeon in profound recurrent gliomas cannot be justified. Cytoreductive therapy is a fundamental part of the treatment of most systematic malignant diseases; therefore, there exists a significant correlation between the volume of excised neoplasm and the outcome of operative treatment (Salcman, 1994). In high-grade gliomas the dependency between the residual tumor size and postoperative results (interval for tumor recurrence, quality of life and survival time) has not been clearly determined yet (Ciric et al, 1989; Salcman et al, 1982; Devita, 1983; Harsh, 1999; Hou et al, 2006). Some studies (Devita, 1983; Ammirati et al, 1987; Burger et al, 1985; Ciric et al, 1989; Vick et al, 1989; Winger et al, 1989; Vecht et al, 1990; Salcman, 1994; Alba et al, 1999) confirm that the surgical intervention volume is an important prognostic factor (AAs 76 - 90 weeks in total resection vs. 19-43 weeks in subtotal; GBM 39.5 - 50.6 weeks vs. 21 - 33 weeks for subtotal excision). This is consistent with our results too, i.e. high-grade gliomas treated by partial resection tend to recur in shorter period. IV. Discussion Recurrent high-grade gliomas are evidence for the failure of even primarily aggressive multimodal treatment - surgery, chemotherapy and radiotherapy (Devita, 1983; Burger et al, 1985; Garcia et al, 1985; Kaluza and Pyrich, 1994; Rostomily et al, 1994; Alba et al, 1999; Harsh, 1999; Chang et al, 2006). There are different factors limiting their effectiveness, e.g. the surgical access to the recurrent tumor which determines the risk of serious postoperative morbidity, gliomas’ infiltrative nature etc. Regardless of the “gross total” tumor excision the control CT and MRI, as well as the stereotactic biopsy in adjacent to the tumor areas show presence of microscopic infiltrations with tumor cells (Ciric et al, 1989; Dirks et al, 1993; Salcman, 1994; Gomori et al, 2002). Table 1. Patients’ outcome assessed by distinction in postoperative and preoperative KPS score. Distinction in postoperative and preoperative Karnofsky score + 20 + 10 0 -10 -20 death N = 32 1 6 16 3 2 4 % 3% 19% 50% 9.3% 6.2% 12.5% Figure 7. Dependency between treatment outcome and patients’ age. 247 Eftimov et al: Management of recurrent high-grade gliomas Figure 8. Pre- and postoperative results in reoperated patients assessed by KPS. Table 2. Analysis (ANOVA) of EORTC QLQ-C30 scores before and after retreatment. Reproduced from Aaronson et a, 1993. IMPROVED PATIENTS (N=12) PRETREATMENT POSTTREATMENT MEAN SD MEAN SD Functioning scales Physical 58.1 (p<0.001) Role (p<0.001) 55.9 Cognitive 79.9 Emotional 63.3 Social 78.1 Global quality of 53.3 life Symptom scales/items Fatigue (p<0.01) 43.1 Nausea and 11.8 vomiting Pain 32.8 Dyspnea 48.0 Sleep disturbance 29.4 Appetite loss 30.4 Constipation 28.4 DETERIORATED PATIENTS (N=16) PRETREATMENT POSTTREATMENT MEAN SD MEAN SD 27.1 67.5 22.6 67.8 27.6 54.7 32.0 36.4 22.0 26.2 29.5 21.8 67.6 80.9 74.5 79.7 62.9 34.6 21.4 18.1 28.9 19.4 60.1 78.1 69.8 73.6 56.2 38.7 22.5 21.3 29.8 25.5 44.3 74.2 72.5 67.9 50.5 39.2 27.2 23.1 30.8 25.0 27.6 20.7 40.1 14.7 26.0 20.8 42.6 9.9 25.7 18.4 53.2 26.4 27.7 29.2 31.1 28.7 33.6 37.0 36.8 15.7 41.2 20.6 30.4 22.5 20.9 29.7 28.4 38.8 31.5 32.7 44.4 33.8 31.2 24.5 34.0 31.6 33.3 37.9 33.2 25.2 40.6 33.8 40.9 28.7 28.4 30.7 35.0 39.2 36.5 Recurrent high-grade gliomas (especially AAs) show faster infiltrative growth in contrast to the primary tumor (Figure 10). This change in the gliomas’ biological behavior makes them resistant to any subsequent treatment. The shorter interval between the first operation and expressed clinical symptoms are often related to fast tumor regrowth and pessimistic prognosis (Muller et al, 1977; Vertosick et al, 1991; Dirks et al, 1993; Kaluza and Pyrich, 1994; Harsh, 1999; Gomori et al, 2002). Prognostic factors in recurrent high-grade gliomas are related to the tumor biology (histology, invasiveness, proliferate activity), tumor resectability (anatomical access and physiological permissiveness); the results from the primary chemotherapy and radiotherapy; patients’ age and preoperative performing status KPS. The important prognostic factors for recurrent high-grade gliomas are: Histological finding. Recurrent high-grade gliomas show more aggressive growth. Most authors find statistically significant dependency on the histological finding after the second operation and life duration of the operated patients (Muller et al, 1977; Young et al, 1981; Gomori et al, 2002). Time to tumor recurrence. The time between the first and second operation is an important prognostic factor, which better explains the biological tumor activity, as well as its sensitiveness and resistibility to chemotherapy and radiotherapy. The longer the interval, the longer life duration after the second operation is (Wilson, 1975; Muller et al, 1977; Burger et al, 1985; Fadul et al, 1988; Alba et al, 1999; Huber et al, 1993). Patient’s preoperative status. Patients with recurrent high-grade gliomas and Karnofsky score > 60 have better prognosis, which is confirmed by our results too (Salcman et al, 1982; Salvati et al, 1998; Alba et al, 1999; Hou et al, 2006). 248 Cancer Therapy Vol 5, page 249 Figure 10. Time for doubling of tumor cell population. Reproduced from Harsh, 1999. Patient’s age is a statistically significant factor. Elderly have poorer postoperative results (Burger et al, 1985; Winger et al, 1989; Vecht et al, 1990; Huber et al, 1993). Tumor recurrence localization - patients with cortical and subcortical localization of the tumor recurrence have better prognosis in comparison to extensive tumor invasion of basal ganglia (Ammirati et al, 1987; Fadul et al, 1988; Vertosick et al 1991; Hou et al, 2006). Macroscopic characteristics of tumor recurrence - in recurrent high-grade gliomas with cystic component optimal postoperative results could be achieved after a new operative intervention (Garfield, 1986; Kaluza and Pyrich, 1994, Harsh, 1999). Most authors advocate second operative intervention in young patients with good preoperative status (KPS > 60) with local tumor recurrence in anatomically accessible place and long period after the first operation (Alba et al, 1999; Ammirati et al, 1987; Burger et al, 1985; Hou et al, 2006; Huber et al, 1993; Winger et al, 1989). Others (Garfield, 1986; Harsh et al, 1987; Fadul et al, 1988; Vecht et al, 1990) have published results of operative treatment in recurrent high-grade gliomas with low morbidity and lethality (0-5.1%), which are comparable with the results after the first intervention. Naturally, a new surgical intervention is connected with a real risk of: intracranial infections (0-21%), wound healing (0-13%) and intraoperative problems with hemostasis (0-4%). Hematomas in loco of tumor resection were CT diagnosed in 5 (15.6%) operated patients in our study. If the neurological deterioration is a result of invasion of deep structures, then the possibilities for surgical treatment are seriously limited. If, however, the neurological deficit is caused by increased intracranial pressure (ICP) or compression without destruction, then we would anticipate improvement in the patients’ status after the tumor resection (Wilson, 1975; Young et al, 1981; Vecht et al, 1990; Harsh, 1999; Hou et al, 2006). The results of this study and literature data suggest that possibilities for an adequate multimodal treatment of recurrent gliomas are still limited. Because malignant growth of gliomas is infiltrative, the reoperation, like an initial resection, is not curative. The justification for reoperation is the clinical palliation that results in tumor cytoreduction and enhancement of the effect of subsequent chemotherapy and radiotherapy against a reduced population of neoplastic cells. The operative risks appear no greater and the benefits are substantial. Some impending randomized trials (Westphal et al, 2006) have to define the effect of new options for multimodal treatment in patients with recurrent high-grade gliomas. New chemotherapeutic agents (Temozolomide and antiangiogenesis targeting agents - Genfitinib, Erlotinib) in combination with interstitial chemotherapy (Gliadel) or interstitial radiotherapy (GliaSite Radiation Therapy System) are some new investigated treatment options (Figure 11). In conclusion the surgical treatment of recurrent high-grade gliomas is appropriate in young patients with solid or cystic part of the recurrent tumor without infiltration of eloquent area and deep brain structures and longer interval between the first operation and tumor reappearance. In contrast, high-grade recurrent gliomas infiltrating deep brain structures in short time after first operation and in old patients with poor performing status (KPS<60) are related with negative prognosis and poor outcome. 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