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Case Studies |
Arthur and Sonia Labatt Brain Tumor Center, Hospital for Sick Children Research Institute, Toronto, ON M5T-2S8, Canada (A.B., A.G.); Department of Neurosurgery, National Institute of Mental Health and Neurosciences, Bangalore, 560029 India (A.B.); Department of Pathology (P.S.) and Division of Neurosurgery (M.H., A.G.), Western Hospital, University Health Network, Toronto, ON, M5T-2S8 Canada; and Departments of Radiation Oncology (N.L.) and Clinical Physics (H.M.), Princess Margaret Hospital, University Health Network, Toronto, ON, M5G-2M9 Canada
Address correspondence to Abhijit Guha, Arthur and Sonia Labatt Brain Tumor Center, Hospital for Sick Children, University of Toronto, 399 Bathurst St., 4W-446, Toronto, ON M5T-2S8, Canada (Abhijit.Guha{at}uhn.on.ca).
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Abstract |
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Key Words: acoustic neuroma • neurofibromatosis-2 • radiation-induced GBM • radiosurgery
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Introduction |
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The minimal up-front risks of focused radiotherapy, especially compared to surgery, are highly attractive. The long-term benign risks of radiation-induced neuropathy, vasculopathy, and CNS necrosis are acknowledged. These risks are usually minimal and often delayed. However, the potential long-term carcinogenic risks of focused radiotherapy, especially those associated with development of secondary de novo malignant tumors or malignant conversion of a benign primary, are of concern. Although a significant literature exists on carcinogenic risks of conventional radiation,1-9 similar risks after focused radiotherapy have been considered unlikely by many who regularly use this treatment modality. Cited reasons why the carcinogenic risks are theoretically low after focused versus conventional radiotherapy include that the small irradiated perilesional normal structures receive extremely low-dose scatter radiation, and that the targeted lesion would receive such a high radiation dose that it is cytotoxic, rather than allowing survival of mutagenized and potentially transformed cells.10
However, as focused radiotherapy enters its fourth decade, with increased use and increase in potential indications, the comment by Heros and Korosue11 regarding the carcinogenic risks of focused radiotherapy for arteriovenous malformations (AVMs), that "this should always be a source of concern when radiation is used to treat conditions compatible with prolonged survival," is bearing true. Our review of the literature yielded 19 cases of malignant progression or secondary radiation-induced tumors after focused radiotherapy for benign intracranial pathologies (Table 1). The vast majority of these tumors occurred in patients being treated for acoustic neuromas (AN), with most of the secondary tumors being malignant in nature. This report represents our second single-institutional experience of a patient who succumbed to a glioblastoma multiforme (GBM), which fulfills all of Cahan's criteria for radiation-induced tumors,12 after focused radiotherapy for an AN. Adapted criteria from Cahan's original report include the following: the new tumor must arise within the previously radiated tissue, must be histologically distinct from the prior tumor, and must arise at least several years following the prior course of radiotherapy. The first patient developed GBM after SRS,13 whereas the patient described here received SFRT. We present this case to highlight the need of judicious and individualized decision toward use of focused radiotherapy, in consultation with the patient.
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Case History |
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About 9 years postdiagnosis of AN (5 years after SFRT), the patient was diagnosed with breast carcinoma. Routine metastatic surveillance MRI of the brain revealed a new 1.5-cm asymptomatic right temporal lobe lesion on fluid-attenuated inversion recovery images. Repeat MRI in 2 weeks demonstrated progression of the lesion, leading to excision biopsy and pathological verification of a GBM (Fig. 2A,B).
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Discussion |
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The radiation dose to the right temporal lobe site of the GBM was low (mean, 4.46 Gy; Fig. 2C); however, the minimal carcinogenic dose to the brain, if one exists at all, has not been firmly established. Radiation doses as low as 1 Gy have been associated with an increased relative risk of a secondary tumor of 1.57-8.75, a figure that increases to 18.4 after an interval of 20-25 years.25 In support, long-term follow-up for brain tumor development after childhood exposure to ionizing radiation for taenia capitis estimated the mean radiation dose delivered to the brain to be 1.5 Gy.6 Experimental evidence also suggests that low nonlethal-dose radiation is more carcinogenic than higher dose radiation. Nondividing primary human fibroblasts were not able to repair DNA double-strand breaks (DSBs) resulting from very low radiation (1 mGy) as efficiently as those resulting from higher radiation doses.26 Normally, these cells harboring DNA DSBs do not proliferate due to G1 cell-cycle arrest, secondary to p53 induction by the low-dose radiation. However, additional genetic alterations or environmental proliferative signals, which result in escape from G1 cell-cycle arrest, would make these cells receiving low-dose radiation and harboring DNA DSBs more prone to transformation.27,28
Among the 20 cases, it is not surprising that 14 of the primary tumors were ANs (Table 1). Cumulative data published on patients treated with the Gamma Knife until December 2005 for North and South America at the Leksell Gamma Knife Society Website (www.elekta.com/site_dbase.php?form_link_id=1090859) indicate that approximately 30% of the indications have been for benign tumors, with ANs accounting for almost one-third of these cases (
9,000 ANs treated by Gamma Knife). This represents only the Americas and does not include the rest of the world and, of course, does not include patients treated with linear accelerator technology. Of most interest, it is striking that 8 of 14 of these cases of AN, with carcinogenic complications associated with focused radiotherapy, were in the setting of neurofibromatosis-2 (NF2), a tumor predisposition syndrome that contributes to less than 5% of all ANs. Although de novo malignant gliomas did arise in these NF2 ANs, in six of eight cases there was progression to a malignant nerve sheath tumor, which was verified at second surgery in five cases and presumed in one case by rapid radiological growth of the AN, which led to the patient's death. The risk for malignant progression in NF2 ANs resulting from radiosurgery has not been formally examined; however, a survey accompanying the report of three cases of malignant nerve sheath tumors in NF2 ANs, which had initially been managed by focused radiotherapy29 (Table 1), is of interest. The survey estimated the incidence of malignant nerve sheath tumors in nonradiated NF2 AN to be less than 0.5%, compared to a 6% incidence in NF2 ANs that had received focused radiotherapy, suggesting a 12-fold increased radiotherapy-linked risk.29 Similarly, a suggestion of increased susceptibility to radiation-induced carcinogenesis and loss of the NF2 gene was suggested by Plowman et al.30 In strict adherence to Cahan's criteria,12 one may argue that the existence of a primary AN precludes the involvement of radiation induction in these cases of a malignant nerve sheath tumor; however, progression to malignant nerve sheath tumor occurs extremely rarely, if ever, in sporadic or NF2-associated peripheral schwannoma or AN.21 This is in contrast to plexiform neurofibromas in neurofibromatosis-1 (NF1) patients, where sporadic malignant progression is well recognized, with an approximately 10%-15% lifetime risk.31
The pathological alterations associated with AN following focused radiotherapy, although reported, are not clear.32-34 The requirement for surgery is not usually due to malignant transformation, but rather necessitated by continued growth, peritumoral swelling, and increased cyst formation, all resulting in local mass effect on the brainstem and/or hydrocephalus.32 Accompanying pathological differences compared to nonradiated ANs, other than those expected from the radiation effects on the tumor microvasculature, are scant.32 Limited studies have suggested an increase in the proliferative index with accompanying microsatellite instability in a minority of these postradiosurgery ANs,33,34 but not enough to diagnose conversion to a malignant nerve sheath tumor. Lack of precise clinical-pathological-molecular data makes the need for additional evidence from in vitro and in vivo models paramount. Unfortunately, these preclinical experiments have not been thoroughly undertaken for NF2, unlike the much more common NF1 syndrome. Deletion of both copies of the Nf2 or Nf1 gene in mice is embryonic lethal, whereas heterozygous mice for both genes are viable but develop tumors other than those associated with the respective syndromes at a higher rate than do normal control mice.35 Carcinogenic susceptibility with Nf2 heterozygous mice is suggested by double transgenics of Nf2 heterozygous and p53 mutant mice, which do develop malignant tumors of neural crest origin.36 Susceptibility to radiation- and chemotherapy-induced carcinogenesis has been demonstrated in Nf1 heterozygotes, in keeping with clinical observations,37 but similar, much-needed studies are lacking with the Nf2 heterozygous mice or NF2 null schwannomas or derivative Schwann cell cultures.
Although lacking definitive clinical or substantial preclinical data, the available data are highly supportive of caution in the use of focused radiotherapy in management of NF2 ANs. In addition to their germline tumor predisposition, NF2-associated ANs occur at a much earlier age, thereby cumulating the radiation carcinogenic risks over a longer period of time. NF2 patients do pose a difficult multifaceted management challenge, not only from their bilateral ANs and other multiple tumors, but also from critical issues regarding hearing and other cranial nerve preservation. One is therefore tempted to justify managing these NF2 ANs with focused radiotherapy, due to minimal short-term risks. However, we should be cognizant of the potential long-term carcinogenic risks, and perhaps observation for those NF2 patients with functional hearing and no clinically significant brainstem compression is prudent. For young NF2 patients with clinically significant mass effect from their AN, most of whom are functionally deaf in that side, microneurosurgical removal, even if subtotal to minimize risks on seventh cranial nerve, may be more desirable to avoid the long-term radiation risks.
In conclusion, our present case and those reported in the literature to date demonstrate that there is a definitive and increasing incidence of de novo malignant gliomas and malignant progression of ANs after focused radiotherapy using either SRS or SFRT for benign intracranial pathologies. This risk is extremely low, given the total number of cases of focused radiotherapy undertaken to date, and certainly should play a small role in our recommendation to the select group of patients where the surgical risks are high or natural life expectancy is relatively short. The primary lesion and associated risks for radiation-induced carcinogenesis are probably factors, but likely this risk is not restricted to ANs, with the increased representation of these cases reflecting our use and experience with focused radiotherapy to date. Although among the 20 cases, two cases involve a primary vascular malformation, reviews by centers with greater experience of treating AVMs with focused radiotherapy are highly suggestive that the risks in these patients may be even smaller than in AN patients.38,39 What the risks are with other benign pathologies, such as trigeminal neuralgia and seizures, needs to be carefully monitored and studied at the very least, as we increase accrual of these cases. Given this uncertainty, we still should practice caution using this treatment modality, especially in young patients and those with tumor predisposition syndromes, because certainly the patient will not benefit by exchanging a benign pathology for a malignant one. One must remember that despite development of instrumentation and refinement of delivery, the final emission of focused radiotherapy is ionizing radiation, a well-recognized carcinogen. Like other management options, it needs to be used judiciously with a thorough risk-benefit discussion with our patients.
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Acknowledgments |
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Received for publication August 7, 2006. Accepted for publication October 26, 2006.
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