Article Text
Abstract
Objectives: To analyse the results of gamma knife radiosurgery (GKS) for the trreatment of intracranial meningiomas and to assess possible factors related to the outcome and complications of such treatment.
Methods: The authors retrospectively reviewed the clinical and radiological data of 179 patients (194 lesions) treated with GKS for meningiomas between May 1992 and October 2000. The mean follow up duration was 37.3 months (range 6.4 to 86.3 months). The study determined the correlation between radiosurgical outcome including imaging changes after GKS and multiple factors such as tumour location and size, patient characteristics, venous sinus status, pre-GKS degree of oedema, other treatment modalities, and radiosurgical parameters.
Results: The radiological control rate was 97.1%. Magnetic resonance imaging (MRI) showed complications after GKS in 35 lesions (25.0%) among the 140 lesions followed up with MRI. Complications were divided into peritumorous imaging changes (33 lesions; 23.6%) and transient cranial nerve dysfunction (two lesions; 1.4%). Radiation induced imaging changes were seen mostly in convexity, parasagittal, and falx meningiomas that were deeply embedded in the cortex. About 60% of these were asymptomatic and the overall rate of symptomatic imaging changes was 9.3%. Neurological deficit related to imaging changes developed in only three patients, and all the symptoms were transient.
Conclusion: GKS for intracranial meningiomas seems to be a safe and effective treatment. However, meningiomas of the convexity, parasagittal region, or falx cerebri have a higher incidence of peritumorous imaging changes after GKS than those of the skull base. Therefore, the use of GKS needs to be considered very cautiously in cerebral hemispheric meningiomas, taking into consideration patient age and general condition, tumour size and location, pattern of cortical embedding, relation between the tumour and venous sinuses, presenting symptoms, and patient preference.
- meningioma
- gamma knife
- GKS, gamma knife radiosurgery
- MRI, magnetic resonance imaging
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Although more than 90% of intracranial meningiomas are histopathologically benign, they frequently recur if removal is incomplete.1–,9 While surgical approaches and techniques for these tumours have undergone continual development, their complete removal remains difficult, especially for parasellar, cavernous, orbital, and petroclival meningiomas and meningiomas adjacent to the major venous sinuses. As a result, the role of radiosurgery has been increasing in importance as a primary or adjuvant treatment modality.1–6,8–,16 Meningiomas are suitable for radiosurgery, because they are encapsulated and often small at time of diagnosis, usually do not invade the brain, and are well defined by computed tomography or magnetic resonance imaging (MRI). These features allow steep radiation fall off and precise definition of target volume. Because their blood supply usually arises from the dura, it can be included in the treatment volume, and this can cause tumour infarction and necrosis.5
Recent advances in high resolution imaging technique and sophisticated three dimensional workstations have improved the accuracy of dose planning during gamma knife radiosurgery (GKS).6 Nevertheless, there have been major and minor complications after GKS, so proper selection of meningiomas for GKS is still very important. We, therefore, analysed the radiosurgical outcomes and complications resulting from treatment of benign meningiomas with GKS and further evaluated potential aetiologies of treatment complications.
METHODS
Between May 1992 and October 2000, 187 patients with meningiomas were treated with GKS at our institution. This group represented 28.5% of all brain tumours treated with GKS. After we excluded one atypical meningioma and seven malignant meningiomas from this study, we retrospectively reviewed the clinical and radiological data in 194 lesions of 179 patients treated with GKS for intracranial meningiomas. There were nine patients with multiple meningiomas. We used the KULA dose planning system (version 5.4, Elekta, Sweden; 164 lesions) until September 1999, when we began using the GammaPlan (version 5.30, Elekta, Sweden; 30 lesions).
Among the 194 lesions, 140 lesions (72.2%) were radiologically followed up for more than six months with MRI and the mean follow up duration was 37.3 months (range 6.4 to 86.3 months). When the volume of a tumour decreased by more than 20% of pre-GKS volume on follow up MRI, it was defined as shrinkage and represented as the volume response of a tumour to GKS. When it changed by less than 20%, or increased by more than 20%, it was defined as stasis or enlargement, respectively. Shrinkage and stasis were defined as radiological controls. The degree of peritumorous oedema was graded by first subtracting the maximal diameter (cm) of the tumour from that of the peritumorous oedema on the T2 weighted MR image and then rounding off the result to the nearest whole number (fig 1⇓). The grade 0 indicates that there was no peritumorous oedema and increasing grade indicates increasing severity of the peritumorous oedema.
A Cox proportional hazards model was used to evaluate the correlation between radiosurgical outcomes and imaging changes after GKS and various factors such as tumour location, lobar location and size, patient age, sex, and presenting symptom, relation to major venous sinus, pre-GKS degree of oedema, treatment modality, and various radiosurgical parameters (maximum tumour dose, tumour margin dose, and type of software used for dose planning). Significance was assigned as p less than 0.05.
RESULTS
Patient characteristics
The mean age of the patients at the time of radiosurgery was 50.4 years (range 7.4 to 82.2 years). The ratio of male to female patients was 1:3.5 (40 male and 139 female patients). The most common presenting symptoms were headache in 55 patients (30.7%), trigeminal neuralgia in 18 (10.1%), and visual disturbance in 13 (7.3%). In 49 patients (27.4%), the meningiomas were incidentally detected.
Radiological findings
Most of the tumours were located in the skull base (n=112; 57.7%), and cerebral hemispheres (n=72; 37.1%). The rest were in the ventricles, pineal region, or sylvian fissure (n=10; 5.2%). Cerebral hemispheric meningiomas included convexity, parasagittal, and falx meningiomas. Among the 72 hemispheric meningiomas, 42 (58.3%) were located in the frontal region, 18 (25.0%) in the parietal region, four (5.6%) in the occipital region, three (4.2%) in the temporal region, and five (6.9%) in the cerebellar convexity.
The relation between tumour and major venous sinus was classified into three groups: complete occlusion of venous sinus due to tumour invasion (n=2, 1.0%); partial occlusion of venous sinus (n=21, 10.8%); and no venous sinus invasion (n=171, 88.1%).
Pre-GKS peritumorous oedema, grade 1 to 6, was found in 26 lesions (13.4%).
Treatment modalities
Of the 179 patients, GKS was performed as a primary treatment in 109 (60.9%) and as an adjuvant treatment for residual or recurrent lesions after surgical resection in the other 70 (39.1%). No patient received conventional radiation therapy.
Radiosurgical parameters
The volume of tumour was estimated by the area within the isodose curve during dose planning. The mean volume of tumours was 10.1 cc (range 0.6 to 45 cc). The tumour was covered within 40% to 90% (mean 50.5%) of the isodose curve; the mean tumour margin dose was 15.1 Gy (range 9.5 to 24.5 Gy); the mean maximum tumour dose was 30.0 Gy (range 19 to 45 Gy); and the mean number of isocentres was 6.3 (range 1 to 15).
Radiological response
Of the 140 lesions (72.2%) followed up for more than six months with MRI, shrinkage was found in 77 (55.0%), stasis in 59 (42.1%), and enlargement in four (2.9%). Radiological control, either shrinkage or stasis was achieved in 136 of 140 lesions, giving a radiological control rate of 97.1%. The probability of radiological control after GKS was analysed with Kaplan-Meier analysis (fig 2⇓). We have provided additional data on the four intracranial meningiomas that failed GKS (table 1⇓). We were unable to identify statistically significant factors related to radiological control of meningiomas or failure of treatment after GKS.
Complications
Complications after GKS for meningiomas were found in 35 lesions (25.0%) among the 140 lesions followed up with MRI. Complications were divided into peritumorous imaging changes on follow up MRI in 33 lesions (23.6%) and transient cranial nerve dysfunction in the other two (1.4%). Peritumourous imaging changes included newly developed imaging changes and aggravation of pre-existing imaging changes on follow up MRI after GKS (fig 3⇓). Among the 33 peritumorous lesions, 13 (39.4%) produced either headaches, caused by increased intracranial pressure (six lesions); seizures (four lesions); or other neurological deficits (three lesions). The symptoms were all transient. The overall rate of symptomatic oedema was 9.3%. Imaging changes developed at a mean of 7.8 months (range 2.8 to 48.9 months) after GKS and were sustained for 13.5 months (range 3.0 to 28.0 months). Imaging changes were evident in four (5.1%) of the 79 skull base meningiomas and 26 (50.0%) of the 52 hemispheric meningiomas. The symptomatic imaging changes occurred more frequently in hemispheric meningiomas (table 2⇓).
The cranial nerve dysfunction seen in two patients was also transient. The first patient had undergone GKS for a cavernous meningioma extending to the orbital fossa. The tumour margin dose was 16.5 Gy and the estimated dose to the lateral wall of the cavernous sinus was 16.5 Gy. Decreased hemifacial sensation developed six months after GKS and was present for one month. The second patient with a cavernous meningioma had undergone GKS with 13.3 Gy of tumour margin dose. The estimated dose to the cavernous sinus was 18.6 Gy. The patient developed an abducens nerve palsy at 18 months after GKS but improved two months later.
We analysed the factors related to peritumorous imaging changes on MRI after GKS. In univariate analysis, tumour location (p<0.001), maximum tumour dose (p=0.0002), and tumour margin dose (p=0.037) were significantly related to imaging changes after GKS. However, in multivariate analysis, only tumour location was significant. Cerebral hemispheric meningiomas had a higher rate of peritumorous imaging changes after GKS than tumours at other locations such as the skull base, ventricles, pineal region, or sylvian fissure.
DISCUSSION
The role of radiosurgery has been gaining importance as a primary or adjuvant treatment modality for meningiomas and many authors have reported excellent outcome for meningiomas treated with GKS.1,3–6,8,10–,19 We identified peritumorous imaging changes on MRI after GKS in 23.6% of lesions. Most of these did not exhibit any symptoms, and all of the symptomatic patients (9.3%) completely recovered. The detailed mechanism and pathophysiology of perilesional imaging changes after radiosurgery are unclear. Most peritumorous imaging changes are believed to be attributable to vasogenic oedema. Whether this is attributable to vascular endothelial growth factor (VEGF)/vascular permeability factor (VPF), an angiogenic growth factor present in most meningiomas,20–,24 or radiation injury to the vasculature is unknown.
There have been many reports about the risk factors for oedema development after radiosurgery. Kalapurakal et al reported that parasagittal location, presence of pretreatment oedema, sagittal sinus occlusion, and radiation doses above 6 Gy per fraction, were significant risk factors for oedema development after radiation therapy.25 In a multicentre review, Kondziolka et al identified 18 of 185 patients with symptomatic oedema that required treatment after GKS.3 They suggested that the presence of a pre-GKS neurological deficit was the most important factor for subsequent symptomatic oedema and that the tumour margin dose was not related to onset of oedema after GKS. Several groups have also reported that non-skull base meningiomas have a higher risk of peritumorous oedema after GKS.8,17,26 Ganz et al suggested that oedema developed preferentially in non-basal tumours, especially those around the midline and sagittal sinus and in cases with a margin tumour dose more than 18 Gy.17 Besides the factors described above, patient age, histological finding, tumour growth, oestrogen and progesterone receptor positivity, and presence of secretory and excretory granules by electron microscopy were suggested as possible risk factors for peritumorous oedema.18,25,26
In our study, post-GKS peritumorous imaging changes developed mostly in cerebral hemispheric meningiomas of the convexity, parasagittal region, or falx cerebri. In univariate analysis, tumour location (skull base or cerebral hemisphere), maximum tumour dose, and tumour margin dose were correlated with the occurrence of imaging changes after GKS. However, in multivariate analysis tumour location was the only significant factor. Other factors reported as significant by other investigators, such as pre-existing oedema, occlusion of venous sinus, or patient age, did not influence the occurrence of imaging changes after GKS.
The influence of tumour location on the rate of occurrence of imaging changes—that is, peritumorous oedema, seems to be related to the different growth patterns of skull base and hemispheric meningiomas (fig 4⇓). While skull base meningiomas spread laterally along the cistern, maintaining a wide base on the dura at the base of the skull, cerebral hemispheric meningiomas are embedded in the brain, and, therefore, have a wider contact area with the brain parenchyma than skull base meningiomas. Unlike skull base meningiomas, which are surrounded by cisterns, hemispheric meningiomas lack any intervening arachnoid or cerbral spinal fluid barrier between the tumour and cortical surface. Therefore, the brain parenchyma surrounding hemispheric meningiomas seems to be more easily affected by the oedema fluid.
GKS has played an important part in the treatment of skull base meningiomas, because the surgical approach carries a high risk of complications and recurrence.1,4–6,9–15,26 Skull base meningiomas were over-represented in our study of GKS treated meningiomas (57.7%), compared with their prevalence in the whole meningioma population. There are many cranial nerves and critical structures around the skull base, especially the cavernous sinus, and careful dose planning is required.6,12,14,15,27
The most critical structure is the optic pathway, which many authors believe tolerates a radiation dose of less than 8 to 10 Gy.4,6,14,27,28 Girkin et al reported that optic neuropathy developed 7 to 30 months after GKS for perichiasmal tumours as an abrupt change in the visual field to a homonymous hemianopic defect.29 MRI showed swelling and contrast enhancement of the affected portion of the visual apparatus. They suggested that risk factors for the development of radiation optic neuropathy after GKS included dose to the optic apparatus of greater than 8 Gy, previous conventional radiation therapy, pre-existing anterior visual pathway dysfunction secondary to previous surgery or tumour compression, treatment plans based on computed tomography rather than MRI, large tumour volume, and treatment isocentres within 5 mm of the anterior visual pathways. Kondziolka et al insisted that only a 1 mm gap between tumour margin and the chiasm might be necessary, if this proximity occurred only at one point, as verified with current high resolution imaging techniques.4 Another report suggested that even more than 10 Gy was safe for the optic apparatus.12 However, we believe that the radiation dose to the optic pathway should not exceed 10 Gy. In our studies, the dose to the optic pathway was less than 9.6 Gy and there were no visual complications. Recent advances in neuroradiological imaging and radiosurgical technique have permitted effective and safe control for tumours with a closer contact to the optic pathway.6
Beyond the optic pathway, attention also should be paid to the radiation dose to the cranial nerves running along the wall of the cavernous sinus, Meckel’s cave, hypothalamus, pituitary gland and stalk, and brain stem.6,12,14,27,28 We previously suggested the optimal radiation dose for critical juxtasellar structures.27 While 48 patients with radiosurgically treated juxtasellar tumours with a dose of less than 16 Gy to the cavernous sinus had no cranial nerve deficits, two other patients with a dose of more than 16 Gy experienced cranial nerve dysfunction. In this study, both of the patients with transient cranial nerve dysfunctions, received more than 16.0 Gy to the cranial nerves.
While 12 Gy to 15 Gy has been recommended as the minimal dose for the meningioma margin,6,8,12,15,17 low dose radiosurgery has been tried by several groups to avoid complications associated with radiation therapy.8,10,19 While a lower dose may be sufficient for effective tumour control with decreased complication rate, the follow up durations of these low dose radiosurgery studies are comparatively short. The minimal dose for tumour margin remains controversial and longer follow up studies are needed.
In our study, we identified four failed cases of meningioma after GKS. One patient had undergone GKS for a residual convexity meningioma after surgical resection. The tumour had nearly disappeared three years after GKS, but recurred on follow up MRI taken at seven years after GKS. The recurrence was thought to arise from the peritumorous dural extension not included within a proper isodose curve. We believe it is essential to irradiate the peritumorous dural extension optimally to achieve long term tumour control.
In conclusion, GKS for intracranial meningiomas is a safe and effective form of primary or adjuvant treatment after incomplete surgical resection. However, patients with cerebral hemispheric meningiomas of convexity, parasagittal region, or falx cerebri have a higher incidence of peritumorous imaging changes after GKS than those with skull base meningiomas. These imaging changes are probably explained by postradiosurgical peritumorous oedema. Therefore, patient age and general condition, tumour size and location, pattern of cortical embedding, relation between the tumour and venous sinuses, presenting symptoms and patient preference need to be considered when treating hemispheric meningiomas with GKS.
Acknowledgments
We thank Drs Steven M Rothman and Michael Wong (Department of Neurology, Washington University School of Medicine, St Louis, MO) for helpful discussions.
REFERENCES
Footnotes
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Competing interests: none declared.