Localized (Sporadic) Neurofibroma

Localized neurofibromas occur most often as sporadic lesions in patients who do not have NF1. Their exact incidence is unknown because of the difficulty in excluding the diagnosis of NF1 in some patients, such as young persons, in whom the initial presentation of the disease may be a solitary neurofibroma, or patients who have no affected family members. Despite these problems, it appears that sporadic neurofibromas outnumber those occurring in NF1 by a considerable margin.

Clinical Findings

Localized sporadic neurofibromas, like their inherited counterparts, affect the genders equally. Most develop in persons between ages 20 and 30 years. Because most are superficial lesions of the dermis or subcutis, they are found evenly distributed over the body surface. They grow slowly as painless nodules that produce few symptoms. Grossly, they are glistening tan-white tumors that lack the secondary degenerative changes common to schwannomas. If they arise in major nerves, they expand the structure in a fusiform fashion, and normal nerves can be seen entering and exiting from the mass ( Fig. 26.14 ). If this lesion remains confined by the epineurium, it has a true capsule. More frequently, these tumors arise in small nerves and readily extend into soft tissue. These tumors appear circumscribed but not encapsulated.

Gross specimen of neurofibroma arising as fusiform expansion of nerve.

Case courtesy of Dr. Steve Bonsib.

Microscopic Findings

Histologically, neurofibromas vary, depending on their content of cells, stromal mucin, and collagen ( Figs. 26.15 to 26.18 ). In its most characteristic form, neurofibromas contain interlacing bundles of elongated cells with wavy, darkly stained nuclei. The cells are intimately associated with wirelike strands of collagen that have been likened to shredded carrots. Small to moderate amounts of mucoid material separate the cells and collagen. The stroma of the tumor is dotted with mast cells, lymphocytes, and rarely xanthoma cells. Less frequently, neurofibromas are highly cellular and consist of Schwann cells set in a uniform collagen matrix devoid of mucosubstances ( Fig. 26.16 ). The cells may be arranged in short fascicles, whorls, or even a storiform pattern. In certain respects, these cellular neurofibromas resemble Antoni A areas of a schwannoma. Unlike schwannomas, however, neurofibromas are not encapsulated and lack a clear partition into two zones. Moreover, small neurites can usually be demonstrated throughout these tumors. Least commonly, neurofibromas are highly myxoid and therefore often confused with myxomas ; this form of neurofibroma usually occurs on the extremities. These hypocellular neoplasms contain pools of acid mucopolysaccharide with widely spaced Schwann cells. In contrast to the cells of myxoma, neurofibroma cells usually have a greater degree of orientation. The vascularity is also more prominent, and with careful searching, features of specific differentiation (e.g., pseudomeissnerian bodies) may be found. Rare variations in neurofibromas are epithelioid change of the Schwann cells and skeletal muscle ( Fig. 26.19 ). Extraordinarily rare cases contain benign glands or rosettes. S-100 protein and SOX10 can be identified in these tumors but stain only a subset of cells, in keeping with the observation that neurofibromas contain a mixed population of cells (see Fig. 26.18 ).

Neurofibroma with myxoid matrix containing neoplastic cells and ropey collagen bundles.

Neurofibroma with dense collagen bundles.

Neurofibroma with Schwann cells of irregular shape, mononuclear cells, and occasional mast cells.

S-100 protein ( A ) and SOX 10 ( B ) immunostains of neurofibroma illustrating that only a subpopulation of cells express the respective antigens. S-100 protein is localized to nucleus and cytoplasm, whereas SOX10 localized to nucleus only.

Epithelioid neurofibroma arising in nerve of patient with neurofibromatosis 1 (NF1). A, Transition between epithelioid areas and those with appearance of conventional neurofibroma. B, High-power view of epithelioid areas.

Although solitary neurofibromas are not associated with the same incidence of malignant change as their inherited counterparts, the exact risk is unknown. It is probably vanishingly small. Simple excision of these tumors is considered adequate therapy.

Clinical Findings

Although, in principle, diagnosis of NF1 should be possible through genetic testing, the large size of the gene and the myriad of mutations have precluded this. Instead, a protein truncation assay to screen for stop mutations has been devised. Unfortunately, it detects only two-thirds of cases and does not predict severity of the disease. More recently, deep sequencing of all 60 NF1 exons, copy number analyses, and screening for intronic splicing site mutations have been reported to identify 95% of presumed NF1 mutations. Some commercial laboratories are also now performing complete sequencing of the entire NF1 gene; Longo et al., however, report that this approach has only been successful in 75% to 85% of candidate cases, for unclear reasons. Therefore the diagnosis of NF1 is still at least in part dependent on identification of the cardinal signs of the disease, two or more of which must be present to establish the diagnosis ( Box 26.1 ).

The severity of the disease varies widely from patient to patient and from family to family. Because of the complexity of the disease and size of the gene, it has been difficult to perform precise genotypic-phenotypic correlations. Only in patients with extremely severe forms of the disease who harbor large deletions have such correlations been possible. It is therefore likely that genetic modifiers outside the NF1 locus play a role in disease symptoms. Complete gene deletions are associated with severe symptoms of NF1, a large number of neurofibromas, and significantly higher lifetime risk for MPNST, whereas mutations at the 3’ end of the gene correlate with familial spinal neurofibromatosis. Segmental forms of neurofibromatosis may be explained by somatic mosaicism.

In the typical patient, NF1 becomes evident within the first few years of life when café au lait spots develop. These pigmented macular lesions resemble freckles, especially during the early stage when they are small. Typically, they become much larger and darker with age and occur mainly on unexposed surfaces of the body ( Fig. 26.20 ). One of the most characteristic locations for café au lait spots is the axilla ( axillary freckle sign ). Pathologically, the spots are characterized by an increase in melanin pigment in the basal layer of the epidermis. In adults, only lesions larger than 1.5 cm are considered café au lait spots for purposes of diagnosis. Because the number of café au lait spots increases with age, and more than 90% of patients with neurofibromatosis have these lesions, their number serves as a useful guideline when making the diagnosis. Not only do these lesions herald the onset of the disease, but in older patients they often give some indication as to the form and severity of the disease. For instance, patients with few café au lait spots tend to have either (1) late onset of palpable neurofibromas, (2) localization of neurofibromas to one segment of the body, or (3) NF2.

Café au Lait Spot.

These pigmented lesions often herald the onset of NF1. They are usually multiple, occur on unexposed surfaces, and are several centimeters in diameter.

Neurofibromas, the hallmark of the disease, make their appearance during childhood or adolescence after the café au lait spots. The time course varies greatly; some tumors emerge at birth, and others appear during late adult life ( Fig. 26.21 ). They may be found in virtually any location and in rare cases may be restricted to one area of the body ( segmental neurofibromatosis ). Unusual symptoms have been related to the presence of these tumors in various organs such as the GI tract. The tumors are usually slowly growing lesions. Acceleration of their growth rate has been noted during pregnancy and at puberty. A sudden increase in the size of one lesion should always suggest malignant change.

Male patient with neurofibromatosis of long duration.

In addition to peripheral neurofibromas, patients with NF1 also develop central nervous system (CNS) tumors, including optic nerve glioma, astrocytoma, and a variety of heterotopias. Vestibular schwannoma, the hallmark of NF2, is virtually never encountered in NF1. Unusual bright objects are detected by T2-weighted MRI in the brain in more than 60% of patients with NF1 and are thought to provide some indication of the degree of cognitive dysfunction.

Pigmented hamartomas of the iris ( Lisch nodules ) may also be found. These asymptomatic lesions are not present in normal individuals or in those with NF2 ( Figs. 26.22 and 26.23 ). Although Lisch nodules cannot be correlated with other specific manifestations of NF1, they are helpful for establishing the diagnosis.

Lisch nodule in patient with NF1. Pigmented areas are seen as brown areas in the iris.

Lisch nodule showing collections of pigment in the iris.

Skeletal abnormalities occur in almost 40% of patients with NF1. They include erosive defects secondary to impingement by soft tissue tumors and primary defects, such as scalloping of the vertebra, congenital bowing of long bones with pseudoarthrosis, unilateral orbital malformations, and cystic osteolytic lesions. The intraosseous cystic lesions were previously believed to be skeletal neurofibromas, but most of these lesions have the histologic appearance of nonossifying fibroma or fibrous cortical defect, characterized by fascicles of fibroblasts arranged in short, intersecting fascicles (sometimes in a storiform pattern) and punctuated with occasional giant cells.

Vascular abnormalities, specifically vascular stenoses, secondary to proliferation of intimal cells, are a significant cause of premature death from renovascular hypertension or stroke. Gynecomastia-like changes (pseudogynecomastia) consisting of stromal hyalinization with nerve fibers and fibroblasts, some of which are multinucleated, have been reported in young males with the disease. In addition to these well-recognized signs and symptoms, NF1 is associated with diverse symptoms not clearly referable to the presence of tumors. They include disorders of growth, sexual maturation, and cognition and abnormalities of the lung. Patients with NF1 are also prone to develop nonneural tumors, notably pheochromocytoma, myelogenous leukemia, and multifocal gastrointestinal stromal tumor (GIST).

Variants of NF1

In addition to classic NF1, there appear to be variant forms in which the features are atypical or incomplete. They include (1) segmental NF manifesting as neurofibromas in a segmental distribution caused by somatic mosaicism of NF1 mutations, (2) gastrointestinal NF, (3) familial spinal NF, and (4) familial café au lait spots.

Pathologic Findings

Several types of neurofibroma occur with NF1 and are distinguished on the basis of their gross and microscopic appearance.

Plexiform Neurofibroma

Plexiform neurofibroma is pathognomonic of NF1, provided that the definition of a plexiform neurofibroma is stringent ( Figs. 26.24 to 26.27 ). Plexiform neurofibromas always develop during early childhood, often before the cutaneous neurofibromas have fully developed. Those plexiform neurofibromas involving an entire extremity give rise to the condition known as elephantiasis neuromatosa, in which the extremity is enlarged ( Fig. 26.28 ). The overlying skin is loose, redundant, and hyperpigmented, and the underlying bone may be hypertrophied, a phenomenon probably related to the increased vascular supply to the limb. Macroscopically, plexiform neurofibromas are large lesions that affect large segments of a nerve, distorting it and contorting it into a “bag of worms” ( Fig. 26.29 ). Smaller lesions, which simply have a plexiform pattern when viewed microscopically rather than macroscopically, should not be interpreted as plexiform neurofibromas for purposes of establishing the diagnosis of NF1.

Plexiform neurofibroma in subcutis of scalp and involving upper eyelid. Note the irregular, tortuous contour of the tumor. Lesions of this type are virtually pathognomonic of NF1.

Plexiform neurofibroma of lower extremity in patient with NF1.

Gross appearance of plexiform neurofibroma. The nerve is converted to a thick, convoluted mass, which has been likened to a bag of worms.

Plexiform neurofibroma involving nerve and extending into hilum of lymph node. Apparent lymph node involvement does not indicate malignancy but simply reflects diffuseness of the process (×5).

Patient with NF1 and large neurofibroma of leg resulting in elephantiasis neuromatosa.

Plexiform neurofibroma with tortuous enlargement of nerves.

Microscopically, the lesion consists of a tortuous mass of expanded nerve branches, as seen when cut in various planes of section. In the early stages, the nerves may simply have an increase in the endoneurial matrix material, resulting in a wide separation of the small nerve fascicles ( Fig. 26.30 ). With continued growth, the cells spill out of the nerves into soft tissue, creating a diffuse backdrop of neurofibromatous tissue ( Fig. 26.31 ), so that NF1 lesions can have both plexiform and diffuse areas. Plexiform neurofibromas, like localized neurofibromas, may display nuclear atypia. Because these lesions are at greatest risk to undergo malignant transformation, care should be paid to lesions displaying heightened cellularity and atypia. The sequence of histologic changes and the inherent problems are discussed later. Occasionally, plexiform neurofibromas contain small schwannian nodules resembling a miniature schwannoma; such lesions have been described as “hybrid schwannoma-neurofibromas” (see Hybrid Benign Peripheral Nerve Sheath Tumors, later).

Plexiform neurofibroma with expansion of endoneurium by myxoid ground substance.

A and B, Portion of plexiform neurofibroma showing the lesion spilling into soft tissue. These areas may resemble areas of diffuse neurofibroma.

Diffuse Neurofibroma

Diffuse neurofibroma is an uncommon but distinctive form that occurs principally in children and young adults. A subset of patients with this lesion also has neurofibromatosis.

Clinically, this tumor is most common in the head and neck region and presents as a plaquelike elevation of the skin. On cut section, the entire subcutis between superficial fascia and dermis is thickened by firm, grayish tissue ( Fig. 26.32 ). As its name implies, this form of neurofibroma is poorly defined and spreads extensively along connective tissue septa and between fat cells. Despite its infiltrative growth, it does not destroy but rather envelops the normal structures that it encompasses, in much the same way as dermatofibrosarcoma protuberans (DFSP) ( Fig. 26.33 ). It differs from the conventional neurofibroma in that it has a uniform matrix of fine fibrillary collagen. The Schwann cells, which lie suspended in the matrix, are usually less elongated than those of conventional neurofibromas and have short fusiform or even round contours. Usually the cellularity is low in diffuse neurofibromas ( Fig. 26.34 ), but occasionally it is high enough to suggest the possibility of a round cell sarcoma ( Fig. 26.35 ). The tumor contains clusters of pseudomeissnerian body–like structures, a characteristic feature of this lesion that serves to distinguish it from the superficial aspect of DFSP ( Fig. 26.39 ). Some diffuse neurofibromas consist of a rather complex arrangement of several mesenchymal elements in addition to the neurofibromatous tissue ( Figs. 26.36 to 26.40 ). These tumors, which seem to be more common in neurofibromatosis, consist of neurofibromatous tissue admixed with mature fat or large ectatic vessels. The latter structures are so striking at times that they eclipse the neural component and can result in the erroneous impression of exuberant granulation tissue. Nuclear palisading may occasionally be present in diffuse neurofibromas. Extremely rarely, diffuse neurofibroma may progress to MPNST.

Diffuse neurofibroma presenting as poorly defined expansion of subcutaneous region of scalp.

Diffuse neurofibroma with extensive permeation of subcutaneous tissue similar to dermatofibrosarcoma protuberans.

Diffuse neurofibroma composed of small rounded cells in a delicate fibrillary background.

Highly cellular diffuse neurofibroma.

Areas of increased vascularity in large, diffuse neurofibroma.

Medium-power ( A ) and high-power ( B ) views of diffuse neurofibroma with characteristic short, fusiform or rounded, Schwann cells.

Nuclear atypia in diffuse neurofibroma.

Medium-power ( A ) and high-power ( B ) views of pseudomeissnerian bodies in diffuse neurofibroma.

A, Diffuse neurofibroma with extensive fatty overgrowth. B, Pseudomeissnerian bodies in fat identify neural nature of lesion.

Pigmented Neurofibroma

About 1% of all neurofibromas contain melanin-bearing pigmented cells. Most occur in patients with NF1 and are of the diffuse type, although some have features of both diffuse and plexiform types ( Fig. 26.41 ). The pigment is not usually appreciated on gross examination and requires histologic examination. The pigmented cells, which are dendritic or epithelioid in shape, are dispersed throughout the tumors but tend to cluster and localize toward the superficial portions of the lesion ( Fig. 26.42 ). They express both S-100 protein and melanin markers, in contrast to the surrounding nonpigmented cells, which express S-100 protein only. Because of the diffuse pattern of growth, these lesions may recur, but metastasis has not been recorded.

Pigmented neurofibroma developing in neurofibroma of diffuse type.

Pigmented Neurofibroma.

Melanin pigment is present in irregularly shaped Schwann cells.

These lesions should be distinguished from pigmented forms of DFSP ( Bednar tumor ), a tumor that in the past was sometimes referred to as a storiform pigmented neurofibroma . The uniform fibroblastic cells, repetitive storiform pattern, and lack of S-100 protein immunoreactivity seen in pigmented DFSP usually make this distinction apparent. The distinction between congenital pigmented nevi with neuroid features and pigmented neurofibroma is less clear-cut. The lack of a junctional or superficial nevoid component supports the diagnosis of a pigmented neurofibroma over that of a congenital neuroid nevus.

Malignant Change in Neurofibromas

In a subset of NF1 patients, an MPNST emerges from a preexisting neurofibroma, typically a deep-seated plexiform lesion ( Figs. 26.43 and 26.44 ). The histologic demarcation between a neurofibroma with atypical histologic features and a low-grade MPNST is difficult because, in effect, these lesions represent a histologic continuum (see Figs. 26.45 to 26.48 ). Furthermore, in neurofibromas that have undergone malignant transformation, it is common to see neurofibroma with a range of atypical features adjacent to areas of frank MPNST. To date, no large study has correlated the number and degree of atypical features in neurofibromas with either outcome or molecular alterations. Because progression of neurofibromas to MPNST is associated with additional mutational events (see later), IHC for p16/CDKN2A (lost in MPNST), Ki67 (high in MPNST), p53 (overexpressed in MPNST), EGFR (amplified in MPNST), and H3K27me3 (lost in 50%–60% of MPNSTs) can be of some assistance in this often challenging distinction. However, there is significant overlap in the expression patterns of these proteins in atypical neurofibromatous neoplasms and MPNSTs, and findings with these markers must always be correlated with light microscopy.

Neurofibroma with malignant transformation ( right ).

A, Plexiform neurofibroma with area of angiosarcoma (hemorrhagic zone). The tumor was an epithelioid angiosarcoma. B, This pattern of malignant transformation is rare and is discussed in Chapter 27 .

Neurofibroma with nuclear atypia of occasional cells without increased cellularity or mitotic activity.

Neurofibroma with moderate cellularity and nuclear atypia. The designation “neurofibroma with atypical features” is used for changes of this type. This change may be seen adjacent to areas of frank sarcoma.

Low-grade malignant peripheral nerve sheath tumor arising in neurofibroma. This neurofibromatous lesion is characterized by back-to-back cellularity throughout, diffuse nuclear enlargement, and low levels of mitotic activity.

Low-grade malignant peripheral nerve sheath tumor arising in neurofibroma. Generalized marked atypia and increased cellularity make the cells appear to be arranged in small fascicles. Low levels of mitotic activity were identified in the lesion.

A small study with short-term follow-up by Lin et al. suggested that cellularity, atypia, and low levels of mitotic activity were still associated with good outcome; others reported similar findings. Some believe the presence of mitotic figures in an otherwise innocuous neurofibroma is insufficient for a diagnosis of malignancy, but mitotic activity and cellularity seem to covary; it is unusual to encounter a mitotically active neurofibroma without some increase in cellularity. The following discussion represents a general approach to this problem. In the final analysis, although labels are convenient, borderline neurofibromatous lesions require careful sampling, dialogue with the clinician, and potentially complete removal, depending on the clinical setting. A recent consensus paper by Miettinen et al., proposing the term “atypical neurofibromatous neoplasm of uncertain biologic potential” (ANNUBP) for some of these tumors, discusses many of these difficult issues. Our own approach to these difficult lesions is similar to that advocated in this consensus statement.

The term neurofibroma should be used for conventional neurofibromas, including those with nuclear atypia only ( Fig. 26.45 ). The latter, as an isolated focal or diffuse change, is common in neurofibromas and does not correlate with malignancy. It is thought to be a degenerative phenomenon, akin to the changes that may be seen in “ancient” schwannoma, symplastic leiomyomas, and symplastic glomus tumors. Although some use the term “atypical neurofibroma” for these lesions, we strongly discourage this term because it could be misconstrued as reflecting concern about malignancy.

The term neurofibroma with atypical features (or “atypical neurofibromatous neoplasm of uncertain biologic potential”) is used for neurofibromas that have any combination of cellularity, nuclear atypia, and mitotic activity, but fall short of the minimum criteria for a diagnosis of low-grade MPNST ( Fig. 26.46 ). This category excludes lesions characterized by nuclear atypia only, as described previously. In general, these lesions are recognized first at low-power magnification, which shows areas having greater cellularity and a more pronounced fascicular growth pattern than seen in ordinary neurofibroma. These areas are the best places to then look for cytologic atypia, in particular monotonous, hyperchromatic cells or pleomorphic cells, as well as mitotic activity. Extensive scrutiny of otherwise typical-appearing neurofibromas for scattered mitotic figures is generally counterproductive, in our experience. Miettinen et al. proposed labeling as “ANNUBP” the tumors showing at least two of the following features: (1) cytologic atypia, (2) loss of neurofibroma architecture, (3) high cellularity, and/or (4) mitotic activity of more than 1 figure per 50 high-power fields but less than 3 figures per 10 hpf.

We recommend reserving the diagnosis of “low-grade MPNST arising in neurofibroma” for cases that show generalized nuclear atypia, diffuse cellularity, and low levels of mitotic activity ( Figs. 26.47 and 26.48 ). Nuclear atypia consists of nuclear enlargement and hyperchromatism. Some require that nuclear enlargement should be at least three times the size of a normal Schwann cell nucleus. The recent consensus paper suggested that the term low-grade MPNST be applied to tumors fulfilling criteria for ANNUBP and displaying 3 to 9 mitotic figures per 10 hpf, although it was recognized that this represented a purely empirical approach. It should be recognized that no outcome-based data support these mitotic figure–based cutoffs.

Discussion

Unlike solitary neurofibromas, those encountered in neurofibromatosis cause significant morbidity. The large number of lesions usually makes surgical therapy impossible. Therefore, surgery has traditionally been reserved for lesions that are large, painful, or located in strategic areas where continued expansion would compromise organ function. Even after attempted complete excision of these lesions, clinical recurrences occasionally develop, a phenomenon related to the poorly defined nature of the tumors. Targeted therapies may therefore prove to be extremely important. Treatment of plexiform neurofibromas with cis -retinoic acid, a maturational agent, and interferon-α, an antiangiogenic factor, have shown growth stabilization in a majority of patients. Some patients have also responded to thalidomide, known to have antiangiogenic properties.

A problem of greater importance is that of malignant transformation. The exact incidence is difficult to determine and has been estimated at 2% to 29% of patients with NF1, but seems dependent on the severity of disease among the population studied. A large follow-up study of a nationwide cohort of 212 Danish patients with neurofibromatosis found nine sarcomas and 16 gliomas but noted the tumors occurred in the proband group (84 patients), who by definition required hospitalization and were probably more severely affected by the disorder. The authors suggest that the natural history of neurofibromatosis may be more accurately reflected by the largest group of patients, relatives of the probands (128 patients) who did not require hospitalization and whose prognosis may have been better than previously thought. Both groups, however, had decreased survival rate after 40 years compared with the general population. A more recent study by Evans et al. documented an 8% to 13% lifetime risk for MPNST, and de Raedt et al. identified an association between large genomic deletions and malignancy in NF1 patients. The latter suggests that certain mutations may be more closely linked to the risk for malignant transformation. In general, patients with NF1 and MPNST have had the disease for many years and present with rapid enlargement or pain in a preexisting neurofibroma. Both symptoms, especially rapid enlargement, should always lead to biopsy. Unfortunately, the prognosis is poor for patients developing an MPNST in this setting (see Chapter 27 ).

With the identification of the NF1 gene in 1990, it has become possible to examine the molecular events underlying tumorigenesis in this disease. Because conventional mice knockout models in which NF1 is completely inactivated (NF1 ^−/− ) prove lethal in utero, conditional mice knockout models in which Schwann cell–specific NF1 is inactivated have been used. In this system, Zhu et al. have shown that Schwann cell–specific knockout mice (NF1 ^−/− ) develop Schwann cell hyperplasias but rarely neurofibromas, whereas Schwann cell–specific knockout mice having one mutant and one wild-type allele (NF1 ^+/− ) readily develop plexiform neurofibromas containing NF1 ^+/− mast cells. These observations have led to the hypothesis that neurofibromin-deficient Schwann cells (NF1 ^−/− ) require other haploinsufficient (NF1 ^+/− ) cells (e.g., mast cells, fibroblasts) in the microenvironment for tumorigenesis. Progression of neurofibromas to MPNST requires additional mutational events involving mitogenic and cell cycle regulatory pathways. Mutations in P53 , INK4 (p16 ^INK4a and p14 ^ARF genes), p27 ^kip1 , and amplification of EGFR have been reported in MPNSTs and suggest a synergistic effect with neurofibromatosis.

Clinical Findings

Schwannomas occur at all ages but are most common in persons 20 to 50 years old. They affect the genders in about equal numbers. The tumors have a predilection for the head, neck, and flexor surfaces of the upper and lower extremities. Consequently, the spinal roots and the cervical, sympathetic, vagus, peroneal, and ulnar nerves are most often affected. Deeply situated tumors predominate in the posterior mediastinum and the retroperitoneum. Schwannomas are usually solitary sporadic lesions. In a population-based study of schwannomas, about 90% were sporadic, 3% occurred in patients with NF2, 2% in those with schwannomatosis, and 5% in association with multiple meningiomas in patients with or without NF2. Rarely, schwannomas occur as part of NF1. About 60% of sporadic and NF2-associated schwannomas have inactivating mutations of the NF2 gene. These events are small frameshift mutations that occur throughout the coding sequence and predict a truncated product. Usually these mutations are accompanied by inactivation of the remaining wild-type allele on 22q. In about one-third of tumors, there is a loss of 22q without detectable mutations, and the remaining tumors seem to have no detectable NF2 alteration. Nevertheless, all schwannomas, whether sporadic or syndromic, lack the protein product merlin. This suggests that schwannomas with apparent intact NF2 gene have either undetectable mutations or epigenetic modification of the gene.

Schwannoma is a slowly growing tumor usually present several years before diagnosis. When it involves small nerves, it is freely movable except for a single point of attachment. In large nerves, the tumor is movable except along the long axis of the nerve, where the attachment restricts mobility. Pain and neurologic symptoms are uncommon unless the tumor becomes large. In some cases the patient is vaguely aware that the tumor waxes and wanes in size, a phenomenon that might be related to fluctuations in the amount of cystic change in the lesion. Of particular significance is the posterior mediastinal schwannoma , which often originates from or extends into the vertebral canal. Such lesions, termed dumbbell tumors or hourglass tumors, pose difficult management problems because patients may develop profound neurologic difficulties.

Gross Findings

Because these tumors arise in nerve sheaths, schwannomas are surrounded by a true capsule consisting of the epineurium. Depending on the size of the involved nerve, the appearance of the tumor varies. Tumors of small nerves may resemble neurofibromas because of their fusiform shape, and they often eclipse or obliterate the nerve of origin. In large nerves the tumors present as eccentric masses over which the nerve fibers are splayed.

On cut section these tumors have a pink, white, or yellow appearance and usually measure less than 5 cm ( Figs. 26.49 and 26.50 ). Tumors in the retroperitoneum and mediastinum are considerably larger. As a result, these tumors are more likely to manifest secondary degenerative changes such as cystification and calcification (see later, ancient schwannoma).

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