期刊名称:ePlasty: Open Access Journal of Plastic and Reconstructive Surgery
印刷版ISSN:1937-5719
出版年度:2015
卷号:15
语种:English
出版社:Open Science Co. LLC
摘要:DESCRIPTIONA 29-year-old man with neurofibromatosis type 1 (NF1) presented with a giant facial neurofibroma causing significant facial deformity and asymmetry. Ipsilateral paresis of the temporal branch of the facial nerve was evident. He had left-sided blindness secondary to visual axis obstruction. He underwent scalp neurofibroma resection as a child.QUESTIONSWhat is the etiology of this patient's facial neurofibroma?What additional clinical findings might be seen in NF1?What are considerations that must be taken into account prior to definitive treatment?What are the management options?DISCUSSIONNeurofibromatosis comprises a range of disorders sharing a main feature of benign peripheral nerve sheath tumors.1Ninety percent of cases are NF1, or von Recklinghausen disease.2The remainder consist of neurofibromatosis type 2 and schwannomatosis. Neurofibromatosis type 1 demonstrates autosomal dominant inheritance due to an inactivating mutation of neurofibromin.1Histological examination of tumors demonstrates proliferation of both nerve and local stromal elements. The morphological variants of NF1 are cutaneous, nodular plexiform, diffuse plexiform, and subcutaneous.3Craniofacial involvement is typically of the plexiform variant of NF1.2Plexiform neurofibromatosis is characterized by neural tissue hamartomas that grow along nerve sheaths within the subcutaneous fat or deeper tissues.1It carries a 10% risk of transformation into a malignant peripheral nerve sheath tumor.4Two of 7 cardinal clinical criteria, developed by the National Institutes of Health, must be present for a diagnosis of NF1. These include 6 or more café au lait spots more than 5 mm in diameter in prepubertal and more than 15 mm in diameter in postpubertal individuals, 2 or more Lisch nodules (pigmented iris hamartomas), axillary (Crowe sign) or inguinal freckling, optic glioma, 2 or more neurofibromas of any type or 1 plexiform neurofibroma, a distinctive osseous lesion, or an affected first-degree relative. Tumors may involve underlying fascia, muscle, bone, and potentially viscera leading to systemic symptoms. Subsequent deformities may occur primarily via direct tumor involvement or secondarily by traction on neighboring structures due to gravity.5Hypertrophy of adjacent connective tissue and underlying bone can occur.3Craniofacial lesions may lead to motor and sensory deficits due to cranial nerve disruption.2Because of the cosmetic and functional importance of one's face, patients with craniofacial lesions incur a high risk for psychological disturbances.5Complete tumor resection may not be feasible without risk for facial nerve injury or extensive muscle resection. In addition, as neurofibromas lack a capsule and have a substantial and friable blood supply, dissection is typically tedious with a high risk for substantial blood loss.6Conservative or partial excisions portend a concern of recurrence, whereas more radical excisions may require aggressive reconstruction of soft-tissue defects.7In cases of midface involvement, lateral structures should be addressed prior to midline structures.5Treatment of concomitant cheek and zygomatic lesions with preservation of canthal and levator function may provide superior outcomes in cases of periorbital involvement.8Critical regions for midface reconstruction include the nasolabial region and oral commissures.5As there is no cure for the disorder itself, the treatment of choice for neurofibromas associated with NF1 is surgical resection.3Medical interventions including antihistamines, maturation agents, and antiangiogenic drugs have had inconsistent results. Potential new therapies such as angiotensin-converting enzyme inhibitors and gene therapy are being investigated. Surgical techniques include partial and radical excisions with a variety of reconstruction options: adjacent tissue transfers, tissue expansion, free flap reconstruction, and composite tissue allotransplantation. Suspension using autologous materials may enable tumor ingrowth and recurrence; using a Teflon mesh netting may prevent this.7Composite tissue allotransplantation is a promising approach that permits radical excision with superior functional and cosmetic reconstruction. A handful of cases have been reported worldwide; such procedures must be performed at well-equipped facilities using a multidisciplinary approach due to the significant risks associated with composite tissue allotransplantation. Ultimately, management should focus on anticipatory guidance, genetic counseling, and symptomatic treatment. Although a period of stability may occur, hasty surgical intervention should be avoided, as rapid recurrence may occur early in the clinical course.3In addition to significant facial asymmetry, our patient developed ipsilateral blindness and facial nerve involvement. His large, ptotic lesion, severe brow, and upper lid ptosis led to significant disfigurement and psychological sequelae. After 2 staged resections, canthopexy, browpexy, and adjacent tissue transfer, the patient remains extremely satisfied, with improved symmetry and appearance 1 year postoperatively. Periorbital resection and reconstruction are planned as a next step of treatment.
