The natural history of familial cavernous malformations: results of an ongoing study

Joseph M. ZabramskiDivisions of Neurological Surgery and Neuroradiology, Barrow Neurological Institute, St. Joseph's Hospital, Phoenix, Arizona; Division of Neuroradiology, Kaiser Permanente Hospital, Portland, Oregon; and Division of Neurological Surgery, University of Maryland Hospital, Baltimore, Maryland

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Thomas M. WascherDivisions of Neurological Surgery and Neuroradiology, Barrow Neurological Institute, St. Joseph's Hospital, Phoenix, Arizona; Division of Neuroradiology, Kaiser Permanente Hospital, Portland, Oregon; and Division of Neurological Surgery, University of Maryland Hospital, Baltimore, Maryland

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Robert F. SpetzlerDivisions of Neurological Surgery and Neuroradiology, Barrow Neurological Institute, St. Joseph's Hospital, Phoenix, Arizona; Division of Neuroradiology, Kaiser Permanente Hospital, Portland, Oregon; and Division of Neurological Surgery, University of Maryland Hospital, Baltimore, Maryland

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Blake JohnsonDivisions of Neurological Surgery and Neuroradiology, Barrow Neurological Institute, St. Joseph's Hospital, Phoenix, Arizona; Division of Neuroradiology, Kaiser Permanente Hospital, Portland, Oregon; and Division of Neurological Surgery, University of Maryland Hospital, Baltimore, Maryland

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John GolfinosDivisions of Neurological Surgery and Neuroradiology, Barrow Neurological Institute, St. Joseph's Hospital, Phoenix, Arizona; Division of Neuroradiology, Kaiser Permanente Hospital, Portland, Oregon; and Division of Neurological Surgery, University of Maryland Hospital, Baltimore, Maryland

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Burton P. DrayerDivisions of Neurological Surgery and Neuroradiology, Barrow Neurological Institute, St. Joseph's Hospital, Phoenix, Arizona; Division of Neuroradiology, Kaiser Permanente Hospital, Portland, Oregon; and Division of Neurological Surgery, University of Maryland Hospital, Baltimore, Maryland

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Ben BrownDivisions of Neurological Surgery and Neuroradiology, Barrow Neurological Institute, St. Joseph's Hospital, Phoenix, Arizona; Division of Neuroradiology, Kaiser Permanente Hospital, Portland, Oregon; and Division of Neurological Surgery, University of Maryland Hospital, Baltimore, Maryland

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Daniel RigamontiDivisions of Neurological Surgery and Neuroradiology, Barrow Neurological Institute, St. Joseph's Hospital, Phoenix, Arizona; Division of Neuroradiology, Kaiser Permanente Hospital, Portland, Oregon; and Division of Neurological Surgery, University of Maryland Hospital, Baltimore, Maryland

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Geraldine BrownDivisions of Neurological Surgery and Neuroradiology, Barrow Neurological Institute, St. Joseph's Hospital, Phoenix, Arizona; Division of Neuroradiology, Kaiser Permanente Hospital, Portland, Oregon; and Division of Neurological Surgery, University of Maryland Hospital, Baltimore, Maryland

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✓ Cavernous malformations are congenital abnormalities of the cerebral vessels that affect 0.5% to 0.7% of the population. They occur in two forms: a sporadic form characterized by isolated lesions, and a familial form characterized by multiple lesions with an autosomal dominant mode of inheritance. The management of patients with cavernous malformations, particularly those with the familial form of the disease, remains a challenge because little is known regarding the natural history.

The authors report the results of an ongoing study in which six families afflicted by familial cavernous malformations have been prospectively followed with serial interviews, physical examinations, and magnetic resonance (MR) imaging at 6- to 12-month intervals. A total of 59 members of these six families were screened for protocol enrollment; 31 (53%) had MR evidence of familial cavernous malformations. Nineteen (61%) of these 31 patients were symptomatic, with seizures in 12 (39%), recurrent headaches in 16 (52%), focal sensory/motor deficits in three (10%), and visual field deficits in two (6%). Twenty-one of these 31 patients underwent at least two serial clinical and MR imaging examinations. A total of 128 individual cavernous malformations (mean 6.5 ± 3.8 lesions/patient) were identified and followed radiographically. During a mean follow-up period of 2.2 years (range 1 to 5.5 years), serial MR images demonstrated 17 new lesions in six (29%) of the 21 patients; 13 lesions (10%) showed changes in signal characteristics, and five lesions (3.9%) changed significantly in size. The incidence of symptomatic hemorrhage was 1.1% per lesion per year.

The results of this study demonstrate that the familial form of cavernous malformations is a dynamic disease; serial MR images revealed changes in the number, size, and imaging characteristics of lesions consistent with acute or resolving hemorrhage. It is believed that the de novo development of new lesions in this disease has not been previously reported. These findings suggest that patients with familial cavernous malformations require careful follow-up monitoring, and that significant changes in neurological symptoms warrant repeat MR imaging. Surgery should be considered only for lesions that produce repetitive or progressive symptoms. Prophylactic resection of asymptomatic lesions does not appear to be indicated.

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