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Management of Benign and Aggressive Intracranial Meningiomas
Die Behandlung von gutartigen und aggressiven intrakraniellen Meningeomen Teil 2
Edward W. Akeyson, MD, PhD and Ian E. Mccutcheon, MD, FRCS(C)
Quelle: ONCOLOGY Vol 10, No 5 (May 1996)
Department of Neurosurgery, The University of Texas M. D. Anderson Cancer Center, Houston
Brachytherapy
Direct and stereotactic placement of high-activity iodine-125 seeds into both recurrent and primary meningiomas has been reported [55-58]. This method has at least three theoretical advantages over conventional fractionated or single high-dose irradiation in the management of meningiomas [56,57]. First, continuous radiation may be more likely than discontinuous forms of radiation to damage slow-growing cells as they pass through the vulnerable period of the cell cycle, yet normal tissues are more resistant to this form of radiation. Second, a very tight dosimetry is possible using this isotope; this may have several benefits when treating tumors at the skull base in proximity to the brainstem, cranial nerves, and vessels. Third, the dose distribution can be tailored to fit an irregular tumor contour, and placement of each seed can be verified radiologically. As with radiosurgery, the number of patients treated with this modality is small, and follow-up is relatively short.
The largest single series of patients undergoing this form of radiation therapy is that of Kumar et al, who reported the results of interstitial brachytherapy in 15 patients with recurrent or primary meningiomas in whom other treatment options had been exhausted or who were medically unsuitable for more conventional treatment modalities [56,57]. The number of seeds implanted depended on the geometry of the tumors, with spherical tumors receiving a single seed; oval tumors, two seeds; and irregular tumors, three seeds. The dose administered to these patients was 100 to 500 Gy at a rate of 0.05 to 0.25 Gy/h over the life of the radionuclide, which averages 87 days.
In 11 (73%) of these patients, the meningiomas showed near-complete resolution at a median follow-up of 29 months; a limited response in 2 patients was attributed to significant calcification in the tumors, as only the noncalcified portion of the tumors responded to the treatment [56,57]. There were no complications in this series.
Some authors have expressed concern over the effects of seed migration and the delivery of unwanted radiation to nearby neurovascular structures [59]. However, these initially promising results indicate that, if technical problems such as seed migration can be adequately addressed, brachytherapy may become a useful adjunct for certain patients with meningiomas.
Medical Treatment
Medical treatment for meningiomas ranges from pharmacologic interventions for relief of symptoms referable to meningiomas to chemotherapeutic regimens that attempt to reduce tumor growth or cause tumor necrosis.
Symptomatic Medical Treatment
Many of the neurologic symptoms associated with meningiomas can be palliated with medical therapy alone, but all surgical patients should also have maximal medical therapy prior to surgery to minimize potential peri-operative complications. All patients with supratentorial meningiomas should be placed on anticonvulsant prophylaxis. Corticosteroids, such as dexamethasone, are routinely used to minimize brain edema associated with these tumors, either to palliate neurologic symptoms when surgery cannot be done or in the perioperative period to minimize brain swelling. When corticosteroids are administered, H2-antagonists are also routinely prescribed. Patients who are immobilized by neurologic deficits produced by their meningiomas should have antiembolism or pneumatic compression stockings placed to prevent pulmonary embolism.
Chemotherapy
Few data exist concerning the efficacy of traditional antineoplastic agents against either benign or malignant meningiomas. Traditional thinking would dictate that due to the slow growth pattern of benign meningiomas, agents that rely on cell replication for effectiveness would not be expected to be of significant benefit. In a recent retrospective review of 15 patients with aggressive meningeal neoplasms, Groves et al reported minimal success with a variety of chemotherapeutic agents, including cisplatin (Platinol), dacarbazine, doxorubicin, and interferon-alfa (Intron A, Roferon-A), given alone or in combination [60]. One patient who was given interferon-alfa had a positive response, and this is the basis for a phase II trial of interferon-alfa that is currently underway. The use of intra-arterial cisplatin and intravenous doxorubicin controlled tumor growth in two patients with inoperable recurrent meningiomas [61], and necrosis of an incidental meningioma was seen in a patient receiving multidrug chemotherapy for rectal carcinoma [62].
Sporadic evidence such as this indicates that there may be a role for multidrug chemotherapy. However, multicenter trials will be necessary to confirm these results on a larger scale.
Hormonal Therapy
Although surgery and radiation constitute the usual treatment modalities for meningiomas, adjuvant endocrinologic manipulation of these tumors could be beneficial both at initial presentation and at the time of recurrence when surgical resection is not possible, either due to advanced age of the patient or location of the tumor. Furthermore, hormonal therapy might represent another way to lower the rate of tumor recurrence following conventional surgery and radiotherapy.
Clinical epidemiologic studies suggest hormonal influences on meningioma growth and a potential role for hormonal modulation in the treatment of meningiomas. These clinical studies and in vitro investigations of meningioma cell biology are the basis for several clinical trials of hormonal agents in the treatment of meningiomas.
Epidemiologic and Physiologic Evidence
Three lines of evidence point to the sex hormones as growth factors in meningiomas. First, intracranial meningiomas are twice as common in women as men, and this female predominance is even greater for spinal meningiomas [39,63]. This 2:1 ratio is most evident in the fourth through seventh decades of life, presumably due to the unique hormonal milieu present in women in this age range [64].
Second, the exacerbation of neurologic symptoms during pregnancy in women known to have meningiomas, with resolution of these symptoms after delivery in some, is common. As of 1991, there were 223 cases of meningioma growth during pregnancy reported in the literature [65]. This phenomenon is most commonly seen during the third trimester, when circulating progesterone levels are highest, and in cases where the tumor is associated with vessels or cranial nerves at the skull base [64].
Third, meningiomas are associated with breast cancer, a tumor known for its dependence on steroid hormones. Women with breast cancer have a greater than twofold increased risk of developing meningiomas over the population as a whole [66], and the association between sphenoid wing meningiomas and either breast or reproductive tract carcinoma is particularly high [67].
Based on the results of the epidemiologic studies, investigations of steroid hormone responsiveness of meningiomas were undertaken with breast cancer as a model. The initial report of Donnell et al supported the contention that steroids may play a role in meningioma physiology by demonstrating significant amounts of estrogen-binding activity in four of six meningiomas tested [68]. Since this original report, many investigators have addressed the presence of steroid receptors in meningiomas, and have generally found a predominance of progesterone-binding proteins over those activated by estrogens (average, 70% vs 17.5%, respectively) [68-73]. In addition, the progesterone-binding site has characteristics that qualify it as a specific receptor in the classic sense, while the estrogen-binding site is much less specific and may be biologically inactive. Androgen receptors have also been found in a large fraction of meningiomas, and in one study the amount of androgen receptor was linearly related to the amount of progesterone receptor [74,75].
Controversy continues over whether these steroid-binding proteins truly represent receptors with a functional role in the physiology of meningiomas. However, a full discussion of these biologic issues is beyond the scope of this article. Moreover, the special case of aggressive meningiomas has not been addressed in these experimental studies.
Clinical Trials of Hormonal Manipulation
Clinical trials employing estrogen antagonists, progesterone supplementation or depletion, and progesterone antagonists have been performed. Using breast carcinoma as a model, a few investigators have explored the use of tamoxifen (an antiestrogen) in patients with unresectable meningiomas [76,77]. The results of these studies were disappointing; only a small number of patients demonstrated a positive response. Similarly disappointing results have been obtained in trials of progesterone supplementation with medroxyprogesterone acetate [78] or megestrol acetate [79]. A single case of symptomatic relief with progesterone depletion has been reported [80].
Mifepristone--Results from studies employing progesterone receptor blockade with the progesterone antagonist mifepristone (RU 486) are now available. In a trial of mifepristone (200 mg/d) at the University of Southern California Comprehensive Cancer Center, 8 of 28 patients experienced objective improvement, as judged by either reduction in tumor size on imaging studies or improvement in visual field deficits [81,82]. This was accompanied by subjective improvement in five patients.
Using a similar regimen of mifepristone, Lamberts et al reported reduction in tumor size in 3 of 10 patients with unresectable meningiomas [83]. Headache was reduced in five patients in that study. One of two postmenopausal women with unresectable meningiomas experienced a reduction in tumor growth in the mifepristone study of Haak et al [84]. Interestingly, vision deteriorated in both patients after cessation of therapy, but improved when the drug was reinstated.
Treatment regimens using mifepristone such as those cited above are generally well-tolerated by patients. Side effects of severe fatigue, nausea, vomiting, and anorexia are common but are easily managed with exogenous corticosteroid administration [82,83]. A large randomized, double-blind, placebo-controlled phase III trial of mifepristone in the treatment of unresectable meningiomas is now underway [81].
Conclusions
Because of the broad spectrum of behaviors exhibited by meningiomas and their poor response to traditional medical treatment regimens, the treatment algorithms for patients harboring meningiomas remain complex. An attempt should be made to completely characterize a particular meningioma, using all available grading schemes and cell kinetic data, so as to identify those tumors with a propensity for recurrent or aggressive behavior. Benign meningiomas should be completely resected when possible, and surgery should be followed by adjuvant radiotherapy when complete resection cannot be performed or the tumor recurs. Radical surgery followed by radiation therapy should be used in all aggressive or malignant meningiomas. Hormonal manipulation, although relatively new and incompletely tested, may provide additional benefit inoperable recurrent meningiomas or those exhibiting aggressive behavior.
Neurosurgeons and oncologists must continue to seek better methods of classifying and treating aggressive meningiomas, which remain a significant risk to life and function in patients that harbor them.
References
1. Cushing H, Eisenhardt L: Meningiomas: Their Classification, Regional Behavior, Life History and Surgical End Results. Springfield, Illinois, Charles C. Thomas, 1938.
2. Russell DS, Rubenstein LJ: Pathology of Tumors of the Nervous System, pp 449-532, Baltimore, Williams & Wilkins, 1989.
3. de la Monte SM, Flickinger J, Linggood RM: Histopathologic features predicting recurrence of meningiomas following subtotal resection. Am J Surg Pathol 10:836-843, 1986.
4. Zülch KJ: Histological typing of tumours of the central nervous system. International Histological Classification of Tumors, no. 21. Geneva, World Health Organization, pp 53-56, 1979.
5. Kleihues P, Burger PC, Scheithauer BW: Histological Typing of Tumours of the Central Nervous System. Berlin, Springer-Verlag, pp 33-37, 1993.
6. Jääskeläinen J, Haltia M, Laasonen E, et al: The growth rate of intracranial meningiomas and its relation to histology: An analysis of 43 patients. Surg Neurol 24:165-172, 1985.
7. Rohringer M, Sutherland GR, Louw GF, et al: Incidence and clinicopathological features of meningioma. J Neurosurg 71:665-672, 1989.
8. Mahmood A, Caccamo DV, Tomecek FJ, et al: Atypical and malignant meningiomas. A clinicopathological review. Neurosurgery 33:955-963, 1993.
9. Ironside JW, Battersby RDE, Lawry J, et al: DNA in meningioma tissues and explant cell cultures: A flow cytometric study with clinicopathological correlates. J Neurosurg 66:588-594, 1987.
10. Crone KR, Challa VR, Klute TE, et al: Relationship between flow cytometric features and clinical behavior of meningiomas. Neurosurgery 23:720-724, 1988.
11. May PL, Broome JC, Lawry J, et al: The prediction of recurrence in meningioma. A flow cytometric study of paraffin-embedded archival material. J Neurosurg 71:347-351, 1989.
12. Shibuya M, Hoshino T, Ito S, et al: Meningiomas. Clinical implications of a high proliferative potential determined by bromodeoxyuridine labeling. Neurosurgery 30:494-498, 1992.
13. Fukui M, Iwaki T, Sawa H, et al: Proliferative activity of meningiomas as evaluated by bromodeoxyuridine uptake examination. Acta Neurochir 81:135-141, 1986.
14. Jääskeläinen J, Haltia M, Servo A: Atypical and anaplastic meningiomas: Radiology, surgery, radiotherapy, and outcome. Surg Neurol 25:233-242, 1986.
15. Wilson CB: Meningiomas. Genetics, malignancy, and the role of radiation in induction and treatment. J Neurosurg 81:666-675, 1994.
16. Fabiani A, Trebini F, Favero M, et al: The significance of atypical mitoses in malignant meningiomas. Acta Neuropath 38:229-237, 1977.
17. Jellinger K, Slowik F: Histologic subtypes and prognostic problems in meningiomas. J Neurol 208:279-298, 1975.
18. Zülch KJ, Mennel HD: Malignant meningiomas, in Klug W, Brock M, Klinger M et al (eds): Advances in Neurosurgery, pp 3-11. New York, Springer-Verlag, 1975.
19. MacCarty CS, Taylor WF: Intracranial meningiomas: Experiences at the Mayo Clinic. Neurol Med Chir (Tokyo) 19:569-574, 1979.
20. Salcman M: Malignant meningiomas, in Al-Mefty O (ed): Meningiomas, pp 75-85. New York, Raven Press., 1991.
21. Wong G, Harper C: Atypical meningiomas. Clinical pathological correlation. Aust NZ J Surg 54:331-336, 1984.
22. Thomas HG, Dolman CL, Berry K: Malignant meningioma. Clinical and pathologic features. J Neurosurg 55:929-934, 1981.
23. Manelfe C, Lasjaunias P, Ruscalleda J: Preoperative embolization of intracranial meningiomas. Amer Jnl Neuroradiology 7:963-972, 1986.
24. Berenstein A, Kricheff I: Microembolization techniques of vascular occlusion: Radiologic, pathologic and clinical correlation. Am J Neuroradiol 2:261-267, 1981.
25. Rodesch G, Lasjaunias P: Embolization and meningiomas, in Al-Mefty O (ed): Meningiomas, pp 285-297. New York, Raven Press, 1991.
26. Black PM: Meningiomas. Neurosurgery 32:643-657, 1993.
27. Simpson D: The recurrence of intracranial meningiomas after surgical treatment. J Neurol Neurosurg Psychiatry 20:22-39, 1957.
28. Jan M, Bazeze V, Saudeau D, et al: Outcome of intracranial meningioma in adults: Retrospective study of a medicosurgical series of 161 meningiomas. Neurochirurgie 32:129-134, 1986.
29. Kallio M, Sankilla R, Hakulinen T: Factors affecting operative and excess long-term mortality in 935 patients with intracranial meningiomas. Neurosurgery 31:2-12, 1992.
30. Mirimanoff RO, Dosoretz DE, Linggood RM, et al: Meningiomas: Analysis of recurrence and progression following neurosurgical resection. J Neurosurg 62:18-24, 1985.
31. Pertuiset B, Farah S, Clayes L, et al: Operability of intracranial meningiomas: Personal series of 353 cases. Acta Neurochirurg 76:2-11, 1985.
32. Sankila R, Kallio M, Jääskeläinen J, et al: Long-term survival of 1986 patients with intracranial meningioma diagnosed from 1953 to 1984 in Finland: Comparison of the observed and expected survival rates in a population-based series. Cancer 70:1568-1576, 1992.
33. Chan RC, Thompson GB: Morbidity, mortality, and quality of life following surgery for intracranial meningiomas: A retrospective study in 257 cases. J Neurosurg 60:52-60, 1984.
34. Dolenc VV: The Cavernous Sinus: A Multidisciplinary Approach to Vascular and Tumorous Lesions. Vienna, Springer-Verlag, 1987.
35. Bricolo AP, Turazzi S, Talachhi A, et al: Microsurgical removal of petroclival meningiomas: A report of 33 patients. Neurosurgery 31:813-828, 1992.
36. Sekhar LN, Altschuler EM: Meningiomas of the cavernous sinus, in Al-Mefty O (ed): Meningiomas, pp 445-460. New York, Raven Press, 1991.
37. Sekhar LN, Janetta PJ, Burkhart LE, et al: Meningiomas involving the clivus: A six-year experience with 41 patients. Neurosurgery 27:764-781, 1990.
38. New PFJ, Hesselink JR, O'Carroll CP, et al: Malignant meningiomas: CT and histologic criteria. Amer Jnl Neuroradiology 3:267-276, 1982.
39. Kepes JJ: Meningiomas; Biology, Pathology, and Differential Diagnosis, pp 112-123. New York, Masson, 1982.
40. Adegbite AB, Khan MI, Paine KW, et al: The recurrence of intracranial meningiomas after surgical treatment. J Neurosurg 58:51-56, 1983.
41. Barbaro NM, Gutin PH, Wilson CB, et al: Radiation therapy in the treatment of partially resected meningiomas. Neurosurgery 20:525-528, 1987.
42. Bloom HJG: Intracranial tumors. Response and resistance to therapeutic endeavors, 1970-1980. Int J Radiat Oncol Biol Phys 8:1083-1113, 1982.
43. Carella RJ, Ransohoff J, Newall J: Role of radiation therapy in the management of meningioma. Neurosurg 10:332-339, 1982.
44. Forbes AR, Goldberg ID: Radiation therapy in the treatment of meningioma: The Joint Center for Radiation Therapy experience 1970 to 1982. J Clin Oncol 2:1139-1143, 1984.
45. Melamed S, Sahar A, Beller AJ: The recurrence of intracranial meningiomas. Neurochirurgica 22:47-51, 1979.
46. Petty AM, Kun LE, Meyer GA: Radiation therapy for incompletely resected meningiomas. J Neurosurg 62:502-507, 1985.
47. Taylor BW, Jr., Marcus RB, Jr, Friedman WA, et al: The meningioma controversy: Postoperative radiation therapy. Int J Radiat Oncol Biol Phys 15:299-304, 1988.
48. Wara WM: Radiation therapy for brain tumors. Cancer 55:2291-2295, 1985.
49. Yamashita J, Handa H, Iwaki K et al: Recurrence of intracranial meningiomas, with special reference to radiotherapy. Surg Neurol 14:33-40, 1980.
50. Goldsmith BJ, Wara WM, Wilson CB, et al: Postoperative irradiation for subtotally resected meningiomas: A retrospective analysis of 140 patients treated from 1967 to 1990. J Neurosurg 80:195-201, 1994.
51. Miralbell R, Linggood RM, de la Monte SM, et al: The role of radiotherapy in the treatment of subtotally resected benign meningiomas. J Neurooncol 13:157-164, 1992.
52. Salazar OM: Ensuring local control in meningiomas. Int J Radiat Oncol Biol Phys 15:501-504, 1988.
53. Solan MJ, Kramer S: The role of radiation therapy in the management of intracranial meningiomas. Int J Radiat Oncol Biol Phys 11:675-677, 1985.
54. Kondziolka D, Lunsford LD, Coffey RJ, et al: Stereotactic radiosurgery of meningiomas. J Neurosurg 74:552-559, 1991.
55. Gutin PH, Leibel SA, Hosobuchi Y, et al: Brachytherapy of recurrent tumors of the skull base and spine with iodine-125 sources. Neurosurgery 20:938-945, 1987.
56. Kumar PP, Patil AA, Syh HW, et al: Role of brachytherapy in the management of the skull base meningioma: Treatment of skull base meningiomas. Cancer 71:3726-3731, 1993.
57. Kumar PP, Patil AA, Leibrock LG, et al: Continuous low dose rate brachytherapy with high activity iodine-125 seeds in the management of meningiomas. Int J Radiat Oncol Biol Phys 25:325-328, 1993.
58. Kumar PP, Patil AA, Leibrock LG, et al: Brachytherapy: A viable alternative in the management of basal meningiomas. Neurosurgery 29:676-680, 1991.
59. Al-Mefty O, Schenck MP, and Smith RR: Petroclival meningiomas, in Rengachary SS, Wilkins RH (eds): Neurosurgical Operative Atlas, pp 339-350. Baltimore, Williams & Wilkins, 1991.
60. Groves MD, DeMonte F, Yung WAK: Chemotherapeutic treatment of aggressive meningeal tumors (abstract). Skull Base Surgery 5(suppl 1):2, 1995.
61. Stewart DJ, Dahrouge S, Wee M, et al: Intraarterial cisplatin plus intravenous doxorubicin for inoperable recurrent meningiomas. J Neurol Oncol 24:189-194, 1995.
62. Bernstein M, Villamil A, Davidson G, et al: Necrosis in a meningioma following systemic chemotherapy: Case report. J Neurosurg 81:284-287, 1994.
63. Sutherland GR, Florell R, Louw D, et al: Epidemiology of primary intracranial neoplasms in Manitoba, Canada. Can J Neurol Sci 14:586-1987.
64. Olson JJ: Laboratory evidence for the hormonal dependency of meningiomas. Hum Reprod 9(suppl 1):195-201, 1994.
65. McCormick PW, Coccia C: Coagulopathy, cerebrovascular disease, and other conditions associated with meningiomas, in Schmidek HH (ed): Meningiomas and Their Surgical Management, pp 22-33. Philadelphia, WB Saunders, 1991.
66. Schoenberg BS, Christine BW, Wisnant JP: Nervous system neoplasms and primary malignancies of other sites: The unique association between meningiomas and breast cancer. Neurology 25:705-712, 1975.
67. Jacobs DH, MacFarlane MJ, Holmes FF: Female patients with meningiomas of the sphenoid wing and additional neoplasms of the breast and genital tract. Cancer 60:3080-1987.
68. Donnell MS, Meyer GA, Donegan WL: Oestrogen-receptor proteins in intracranial meningiomas. J Neurosurg 50:499-502, 1979.
69. Cahill DW, Bashirelahi N, Solomon LW, et al: Oestrogen and progesterone receptors in meningiomas. J Neurosurg 60:985-993, 1984.
70. Lesch KP, Fahlbusch R: Simultaneous estradiol and progesterone receptor analysis in meningiomas. Surg Neurol 26:257-263, 1985.
71. Markwalder TM, Zava DT, Goldhirsch A, et al: Oestrogen and progesterone receptors in meningiomas in relation to clinical and pathologic features. Surg Neurol 20:42-47, 1983.
72. Schnegg JF, Gomez F, Lemarchand-Bauraud T, et al: Presence of sex steroid receptors in meningioma tissue. Surg Neurol 15:415-418, 1981.
73. Tilzer LL, Plapp FV, Evans JP, et al: Steroid receptor proteins in human meningiomas. Cancer 49:633-636, 1982.
74. Lesch KP, Engl HG, Gross S: Androgen receptor binding activity in meningiomas. Surg Neurol 28:176-180, 1987.
75. Olson JJ, Beck DW, MacIndoe JW, et al: Androgen receptors in meningiomas. Cancer 61:952-955, 1988.
76. Markwalder TM, Seiler RW, Zava DT: Antiestrogenic therapy of meningiomas: A pilot study. Surg Neurol 24:245-249, 1985.
77. Goodwin JW, Crowley J, Eyre JH, et al: A phase II evaluation of tamoxifen in unresectable or refractory meningiomas: A Southwest Oncology Group study. J Neuro Oncol 15:75-77, 1993.
78. Jääskeläinen J, Laasonen E, Karkkainen J, et al: Hormone treatment of meningiomas: Lack of response to medroxyprogesterone acetate (MPA): A pilot study of five cases. Acta Neurochir 80:35-41, 1986.
79. Grunberg SM, Weiss MH: Lack of efficacy of megestrol acetate in the treatment of unresectable meningioma. J Neuro-Oncol 8:61-65, 1990.
80. van Seters AP, van Dulken H, de Keizer RJW, et al: Symptomatic relief of meningioma by buserelin maintenance therapy. Lancet 1:564-565, 1989.
81. Grunberg SM: Role of antiprogestational therapy for meningiomas. Hum Reprod 9 (suppl 1):202-207, 1994.
82. Grunberg SM, Weiss MH, Spitz IM, et al: Treatment of unresectable meningiomas with the antiprogesterone agent mifepristone. J Neurosurg 74:861-866, 1991.
83. Lamberts SW, Tanghe HL, Avezaat CJ et al: Mifepristone (RU 486) treatment of meningiomas. J Neurol Neurosurg Psychiatry 55:486-490, 1992.
84. Haak HR, de Keizer RJ, Hagenouw-Taal JC, et al: Successful mifepristone treatment of recurrent, inoperable meningioma. Lancet 336:124-125, 1990.
85. Fukui M, Kitamura K, Nakagaki H, et al: Irradiated meningiomas: A clinical evaluation. Acta Neurochir 54:33-43, 1980.
The Akeyson/McCutcheon Article Reviewed
Steven M. Grunberg, MD, University of Vermont Burlington
Meningioma is a prime example of a tumor requiring a multimodality approach. This tumor is usually benign and often grows slowly. Under many circumstances, such a benign tumor would never attract the attention of the oncologist or even require treatment at all. However, a meningioma is a benign tumor in a malignant location. In the closed space of the skull, there is no room for expansion of even a benign lesion; thus, effective treatment of this potentially neurologically devastating lesion is necessary. Neurosurgeons, neuroradiologists, radiotherapists, and medical oncologists are all directly involved in treatment decisions. Rapidly expanding knowledge concerning the etiology and natural history of meningiomas may now also involve epidemiologists, molecular geneticists, and endocrinologists. Despite this concentration of expertise, numerous questions remain unanswered or incompletely answered.
The epidemiology of meningiomas has always been of great interest [1]. Observations that meningiomas are twice as common in women as in men, that they may wax and wane with pregnancy, and that they are positively associated with breast cancer opened the door to investigation of the role of sex hormone receptors in the growth of meningiomas and to a greater understanding of the pathways that control the expression and function of these receptors. However, other risk factors have also been identified. Trauma may be a factor in the induction of meningiomas; they may be the only tumors associated with participation in a competitive sport (head trauma from boxing) [2]. Radiation may also play a role in the induction of meningiomas, including either therapeutic radiation to the brain or scalp [3] or possible risk from excessive dental x-rays [2]. Description of deletions of chromosome 22 as a possible marker for meningiomas may help identify a common pathway of chromosomal damage for these various risk factors [3].
Treatment Options
Surgery remains the acknowledged mainstay for potentially curative treatment of meningiomas. Surgical results have improved both through technical advances and through the development of effective multispecialty surgical teams, particularly in the area of skull-base procedures. However, planning the extent of appropriate surgery depends upon appreciation of the malignant potential of the tumor in question, and this has been a special area of difficulty for meningioma.
Some meningiomas may be obviously histologically malignant or may present as malignant tumors by metastasizing to distant sites. However, the description of an aggressive meningioma is often based more on the clinical picture than on particular histologic or cytologic features. In addition, there is a propensity for meningiomas that intermittently recur over many years to demonstrate increasingly aggressive behavior. More extensive surgery is therefore finally needed at the time when previous interventions make such an approach more difficult. Improvement of techniques for early identification of malignant or aggressive potential through the definition of appropriate markers of proliferation or through metabolic imaging (such as the use of positron emission tomography) is thus a major requirement for improvement in long-term results.
A significant literature now supports the use of radiotherapy for the treatment of advanced meningiomas or for adjuvant treatment after tumor resection [4]. In much of neuro-oncology, the use of aggressive cranial radiotherapy with potential delayed toxicity can be justified, in part, by the poor expectations for long-term outcome. In the case of meningiomas, where survival for a decade or more can be expected in many cases, the question of persistent or late toxicity becomes more important. Further work to identify the subset of patients who may be at increased risk for deterioration in cognitive function after cranial radiotherapy is required. In addition, a greater appreciation of the possible delayed effects of cranial radiotherapy, such as hypothalamic-pituitary dysfunction resulting in hypothyroidism [5], is necessary for physicians involved in the long-term care of patients with meningiomas.
Although isolated reports of success with cytotoxic chemotherapy or embolization of meningiomas can be found, neither treatment has become a significant part of general care. In contrast, the role of various growth factors has been a fascinating area. The epidemiologic association of meningiomas with female gender led to the original description of female sex hormone receptors with potential proliferative function on meningioma cells. Since then, the realization that progesterone receptors on meningiomas may be expressed independently of estrogen receptor stimulation has led to potentially important insights into the regulation of these receptors (including the possibilities of either totally independent expression of progesterone receptors or expression induced by a constitutively activated modified estrogen receptor) [6].
The suggestive results of early trials of antiprogesterone manipulation of meningiomas (now being tested in larger phase III trials) have introduced a new form of hormonal manipulation to the antineoplastic armamentarium [7]. This line of research has advanced the idea that sex hormones and sex hormone receptors may function as growth factors and growth factor receptors, even in the absence of an obvious gender relationship of the organ in question. This concept may have far-reaching implications for the management of numerous medical conditions. Furthermore, the identification of additional hormone receptors that could potentially serve as growth factor receptors on meningiomas (including androgen and somatostatin receptors) may suggest an increasingly important role for biologics (rather than cytotoxics) in the medical management of meningiomas [1].
Although treatment of benign tumors should be simple (ie, resection), meningiomas, by virtue of their location and natural history, have turned this simple question into a multifaceted research and treatment challenge. In view of the expected long survival of patients with meningiomas, superb surgical and radiotherapeutic techniques for the avoidance of chronic and late toxicities are needed. Meningiomas also have provided the opportunity to gain greater insights into the role of hormonal and other growth factors, which may have widespread implications for the understanding and management of both malignant and nonmalignant conditions. Increased knowledge of these signalling pathways may be the most important contribution to emerge from the many ongoing avenues of meningioma research.
References
1. Grunberg SM: The role of progesterone receptors in meningioma. In: Muggia FM (ed), New Drugs, Concepts, and Results in Cancer Chemotherapy, pp 127-137. Boston, Kluwer Academic Publishers, 1991.
2. Preston-Martin S, Yu MC, Henderson BE, et al: Risk factors for meningiomas in men in Los Angeles county. J Natl Cancer Inst 70:863-866, 1983.
3. Black PM: Meningiomas. Neurosurgery 32:643-657, 1993.
4. Wilson CB: Meningiomas: Genetics, malignancy, and the role of radiation in induction and treatment: The Richard C. Schneider Lecture. J Neurosurg 81:666-675, 1994.
5. Constine LS, Woolf PD, Cann D, et al: Hypothalamic-pituitary dysfunction after radiation for brain tumors. N Engl J Med 328:87-94, 1993.
6. Blankenstein MA, Koehorst SGA, van der Kallen CJH, et al: Oestrogen receptor independent expression of progestin receptors in human meningioma--A review. J Steroid Biochem Mol Biol 53:361-365, 1995.
7. Grunberg SM, Weiss MH, Spitz IM, et al: Treatment of unresectable meningiomas with the antiprogestational agent mifepristone. J Neurosurg 74:861-866, 1991.
The Akeyson/McCutcheon Article Reviewed
Michael Mcdermott, MD, University of California San Francisco
Benign and aggressive intracranial meningiomas, as the authors state, are seemingly simple tumors (even with benign histology) that can behave in a clinically malignant fashion solely by location. Clinicians with experience in the management of patients with aggressive, recurrent, or malignant meningiomas are all too well aware of the difficulties of recommending effective therapy beyond surgery and radiation therapy. Clearly, there is much room for improvement in the treatment of recurrent or malignant meningiomas with local or systemic chemotherapy and/or biologic therapies.
A key to the uniform reporting and analysis of the results of the treatment of meningiomas is a standard classification system based on histopathologic features. Although many different schemes have been proposed since the time of Cushing and Eisenhardt [1], the scheme by Russell and Rubenstein [2], and the World Health Organization Classification of Tumors, Second Edition (WHO-2) [3], seem to be the most widely used. As the authors point out, these descriptors of pathologic type may be supplemented by the Helsinki grading system, which attributes either 0 or 3 points for the absence or presence of six features of anaplasia [4]. These features include loss of cell architecture, increased cellularity, nuclear pleomorphism, mitotic figures, focal necrosis, and brain infiltration. The sum of these points is then used to assign a grade from I to IV corresponding to descriptions of benign, atypical, anaplastic, and sarcomatous forms of meningiomas.
Although bromodeoxyuridine labeling indices (developed by Dr. Takao Hoshino at the Brain Tumor Research Center at the University of California, San Francisco) were used in the past, we have now turned to ex vivo labeling studies, including the use of Ki-67 and MIB-1 [5]. MIB-1 is commercially available and can be used on paraffin-embedded tumor sections; these sections can be recovered in such a fashion as to reactivate an epitope of Ki-67, which stains for the expression of several proliferation-associated nuclear proteins, and a proliferating cell index can be derived. Typically, with this technique, the labeling index is 2.4 to 1.8 times higher than it is with the bromodeoxyuridine labeling index. There is, however, a strong correlation among the bromodeoxyuridine, MIB-1, and Ki-67 proliferating cell indices [5]. These indices correlate with the proliferative potential of a tumor more accurately than do other tissue descriptive assessments. The results of the combination of histopathologic information, tumor grade, labeling index information, and the Simpson surgical grade, as discussed by the authors, should be available from future clinical series reporting on the treatment of meningiomas [6].
Surgical Treatment Options
Although surgical resection remains an important part of the treatment of both benign and malignant meningiomas, not all patients with intracranial meningiomas require surgery, especially elderly patients [7]. Now, for a variety of reasons, small dura-based tumors with imaging characteristics compatible with meningiomas are more often detected via imaging of the central nervous system. Beyond the determination of whether or not a meningioma is responsible for any signs or symptoms, patient and tumor factors must be weighed to determine the appropriateness, and benefit, of any recommended surgical procedure. It is not uncommon to see a patient with a heavily calcified meningioma that does grow appreciably for a considerable period. Clearly, if a decision is made not to intervene, the patient should agree with this approach and be available for regular clinical and radiologic follow-up, so if new symptoms or signs develop, or there is objective evidence of tumor growth, the situation can be reevaluated.
Preoperative medical therapy for patients with meningiomas does not necessarily have to include embolization, as the authors indicated. With a convexity meningioma, the dural blood supply can be exposed easily and interrupted during the exposure necessary for resection of the tumor. Furthermore, in certain locations, such as the olfactory groove, embolization may present too high a risk. In the case of a small falx meningioma, for which preoperative angiography is not necessary, we have found magnetic resonance venography to be an important adjunct in surgical decision-making regarding the side from which to approach the tumor, given the pattern of veins draining into the superior sagittal sinus. Any additional information that may reduce the potentially devastating consequences of interrupting a "safe" parasagittal draining vein should be considered.
There is no question that during the mid-to-late 1980s, the development of skull-base approaches allowed surgeons to remove tumors previously thought to be unapproachable. However, by their very nature, these procedures are complex and lengthy and may be associated with significant morbidity. In a recent seminal article, Larson et al pointed out the pathologic findings of infiltration of cranial nerves within the cavernous sinus by benign meningiomas, excluding any realistic possibility of "surgical cure" while maintaining extraocular muscle function and an acceptable rate of operative morbidity.8 Some impressive surgical results have been reported by surgeons accomplished in skull-base approaches; however, 5-year and 10-year rates of recurrence-free survival will be necessary to evaluate the efficacy of this complex surgical procedure.
Radiotherapy and Chemotherapy
It seems somewhat paradoxical that radiation therapy would be recommended as an adjuvant therapy for incompletely resected, recurrent, or malignant meningiomas when both low- and high-dose irradiation to large volumes of the scalp have been implicated in the development of meningiomas. Beyond the experience of Israeli children treated for tinea capitis with meningiomas, a recent review of the literature has revealed that the higher the dose and the younger the patient undergoing irradiation, the shorter the latency period for tumor development [9]. It must be understood that with conventional external-beam irradiation techniques and three-dimensional treatment planning, the volume of normal tissue irradiated to a significant dose has been greatly limited.
The authors have rightly assessed the utility of modern-day radiotherapy for subtotally resected and recurrent meningiomas. Series published since 1990 document 5-year progression-free survival rates for benign meningiomas of 84% to 89% [6]. In the University of California at San Francisco series published by Goldsmith et al, treatment complications, occurred in 5 patients (3.6%), 3 of whom had a sudden onset of blindness 20 to 22 months after treatment [10]. Others have reported such complications as hearing loss, memory impairment, pituitary dysfunction, and chronic otitis media. For surgeons and radiotherapists, information about microscopic rests of meningothelial cells at up to 3 cm from the margin of the original tumor in 57% of specimens is essential for treatment planning [11].
Although radiosurgery is a relatively new treatment for meningiomas, at least 2 series reported a median follow-up of at least 40 months. In the two series, tumor control rates were 76% and 80%, respectively [12,13]. As mentioned by the authors, reduction in tumor size is not the only end point in evaluating therapy, and no increase in tumor size is also an acceptable result. In our experience, only about 30% of meningiomas will become smaller after radiosurgery. Radiosurgery can be used for small, focal occurrences of benign meningiomas or as a boost for residual disease in malignant meningiomas.
In their discussion of interstitial brachytherapy, the authors refer to two series by the same author, who reported remarkable radiologic response rates without complications. Our experience is encouraging but not nearly as dramatic! In an evaluation of 21 patients with recurrent or malignant meningiomas treated with iodine-125, low-activity permanent implants at the time of reoperation, the median time to tumor progression was 96 weeks and the median survival was 124 weeks from the time of implantation [14]. Complications occurred in a significant number of patients (38%). These implants are usually reserved for patients with a significant mass of recurrent tumor and for patients in whom other treatment modalities have failed. Obviously, these patients still must be strong enough for an open surgical procedure.
Conventional chemotherapy for recurrent or malignant meningiomas has certainly been disappointing. We have not found a regimen of cyclophosphamide (Cytoxan, Neosar), doxorubicin, and vincristine to be of any significant benefit, given the side effects; in 11 patients, our failure rate was 73% at 1 year and 100% at 2 years after the start of treatment [15]. Clearly, some other approach is warranted, given these poor results.
Experimental Therapies
Experimental studies have demonstrated a number of receptors present in meningioma cells, including progestins, androgens, glucocorticoids, dopamine (DA1), interferon alpha, epidermal growth factor, and platelet-derived growth factor, to mention a few [6]. Experimental evidence in animal models does exist for the use of some receptor antagonists against these different receptors in controlling tumor growth. In one study, trapidil, a drug with antiplatelet-derived growth factor activity, was combined with bromocriptine (Parlodel), a DA1-dopamine receptor blocker; this combination of drugs inhibited tumor growth more than either agent alone [16]. Obviously, the clinical applications of such experiments require further study. Although the antiprogestational agent mifepristone has generated much excitement, the small amount of objective data documenting tumor control requires further investigation. In addition, high doses of tamoxifen may, in fact, act against meningioma cells by inhibiting protein kinase C activity, rather than by any effect on estrogen receptors, few as they are.
A potentially exciting area of current laboratory investigation is the use of novel biologic therapies for the treatment of meningiomas. In this regard, options include using modified attenuated live virus and infecting the proliferating tumor; the enzyme activity of these proliferating cells is directed toward replication of the virus, and cell death occurs through the normal mechanisms of virus-induced cell lysis [17]. As well, the introduction of a specific gene, such as herpes simplex virus I thymidine kinase, with a retroviral vector may permit the incorporation of a small amount of this gene in actively proliferating cells [18]. The administration of a prodrug such as ganciclovir (Cytovene) permits the phosphorylation of the drug through the activity of thymidine kinase; the triphosphate form of ganciclovir is toxic to the tumor cells. According to Fick et al current research now indicates that the bystander effect is likely related to the passage of phosphorylated forms of ganciclovir between tumor cells, and it appears that the efficiency of this bystander effect relates to the density of gap junctions that exist on the tumor cell surface [19]. Conveniently, meningioma cells happen to have abundant gap junctions. Therefore, these tumors may be well suited to this form of therapy. Obviously, if laboratory studies continue to indicate the effectiveness of this treatment, it will be some time before this therapy is brought to the clinical sphere.
Although it is true that the mainstay of therapy for meningiomas is surgery, clearly there are a significant number of patients for whom this option does not provide a cure, and other adjuvant therapies are necessary. Neurosurgeons, radiation oncologists, and medical oncologists with a special interest in these tumors have long been frustrated by their tenacity to resist conventional treatment. Advanced surgical techniques, improved radiotherapy using three-dimensional conformal treatment planning, and radiosurgery units have nearly reached their technical limits. Clearly, it is necessary to identify the most effective form of adjuvant chemotherapy, immunotherapy, or viral/genetic therapy for recurrent, aggressive, or malignant meningiomas.
References
1. Cushing H, Eisenhardt L: Meningiomas: Their Classification, Regional Behavior, Life History, and Surgical End Results. Springfield, OH, Charles C. Thomas, 1938.
2. Russell DS, Rubenstein LJ: Pathology of Tumors of the Nervous System, 5th ed. Baltimore, Williams & Wilkins, 1989.
3. Kleihues P, Burger PC, Scheithauer BW (eds): Histological Typing of Tumors of the Central Nervous System, pp 33-42. New York, Springer-Verlag, 1993.
4. Jaaskelainen J, Haltia M, Laasonen Erkki, et al: The growth rate of intracranial meningiomas and its relation to histology. Surg Neurol 24:165-172, 1985.
5. Onda K, Davis RL, Shibuya M, et al: Correlation between the bromodeoxyuridine labeling index and MIB-1 and Ki-67 proliferating cell indices in cerebral gliomas. Cancer 74:1921-1926, 1994.
6. McDermott MW, Wilson CB: Meningiomas. In: Youmans JR, ed. Neurological Surgery, 4th ed, pp 2782-2825. Philadelphia, WB Saunders, 1996.
7. Mastronardi L, Ferrante L, Qasho R, et al: Intracranial meningiomas in the ninth decade of life: A retrospective study of 17 surgical cases. Neurosurgery 36:270-274, 1995.
8. Larson JJ, van Loveren HR, Balko MG, et al: Evidence of meningioma infiltration into cranial nerves: Clinical implications for cavernous sinus meningiomas. J Neurosurg 83:596-599, 1995.
9. Harrison MJ, Wolfe DE, Lau TS, et al: Radiation-induced meningiomas: Experience at the Mount Sinai Hospital and review of the literature. J Neurosurg 75:564-574, 1991.
10. Goldsmith BJ, Wara WM, Wilson CB, et al: Postoperative irradiation for subtotally resected meningiomas: A retrospective analysis of 140 patients treated from 1967 to 1990. J Neurosurg 80:195-201, 1994.
11. Borovich B, Doron Y: Recurrence of intracranial meningiomas: The role played by regional multicentricity. J Neurosurg 64:58-63, 1986.
12. Engenhart R, Kimmig BN, Hover KH, et al: Stereotactic single high dose radiation therapy of benign intracranial meningiomas. Int J Radiat Oncol Biol Phys 19:1021-1026, 1990.
13. Kaplan ID, Castro JR, Phillips TL: Helium charged particle radiotherapy for meningioma: Experience at UCLBL. Int J Radiat Oncol Biol Phys 28:257-261, 1993.
14. Rogano LA, McDermott MW, Larson DA, et al: Permanent I-125 implants for recurrent malignant tumors. Proc Congress Neurol Surg, 45th Annual Meeting, p 382, 1995.
15. Wilson CB: Meningiomas: Genetics, malignancy, and the role of radiation in induction and treatment. J Neurosurg 81:666-675, 1994.
16. Todo T, Adams EF, Fahlbusch R: Inhibitory effect of trapidil on human meningioma cell proliferation via interruption of autocrine growth stimulation. J Neurosurg 78:463-469, 1993.
17. Yazaki T, Manz HJ, Rabkin SD, et al: Treatment of human malignant meningiomas by G207, a replication-competent multimutated herpes simplex virus 1. Cancer Res 55:4752-4756, 1995.
18. Culver KW, Ram Z, Wallbridge S, et al: In vivo gene transfer with retroviral vector-producer cells for treatment of experimental brain tumors. Science 256:1550-1552, 1992.
19. Fick J, Barker FG II, Dazin P, et al: The extent of heterocellular communication mediated by gap junctions is predictive of bystander tumor cytotoxicity in vitro. Proc Natl Acad Sci USA 92: 11071-11075, 1995.
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© 1996 by PRR, Inc. All rights reserved.
Thema: Behandlung von gutartigen und aggressiven Meningeomen (Gelesen 11617 mal)