Neural, Neuroectodermal, and Neuroendocrine Neoplasms



Neural, Neuroectodermal, and Neuroendocrine Neoplasms





A variety of neural, neuroectodermal, and neuroendocrine neoplasms can occur throughout the region of the upper aerodigestive tract. These lesions may show overlapping histologic features and be difficult to distinguish from one another by small biopsy. Nonetheless distinction from one another and from other neoplasms is important as these tumors have widely different prognoses and require markedly different treatments. This chapter discusses the clinicopathologic features of these neoplasms and methods for accurately diagnosing them.


NEURAL LESIONS

Most neural lesions found throughout the peripheral nervous system can occur in the upper aerodigestive tract (Table 8.1).1 These include neurofibromas, schwannomas, granular cell tumors, neuromas, neurothekeomas, paragangliomas, and malignant peripheral nerve sheath tumors. Most may occur throughout the upper aerodigestive tract; however, many occur more frequently at particular sites in well-defined clinicopathologic circumstances. With small biopsies, it is not always possible to distinguish the lesions from one another, especially as knowing the overall architecture of the neoplasms is sometimes necessary for the diagnosis. In such cases, differential diagnoses can be supplied or more general diagnoses such as benign nerve sheath tumor or benign neural tumor can be used.

Traumatic neuromas can occur throughout the tract but most frequently arise in the lip, tongue, or mental nerve area.1,2 They present as small nodules which are often painful to palpation. Like their counterparts throughout the body, they are composed of tangles of neural tissue composed of axons and schwann cells, often accompanied with dense sclerotic tissue (Fig. 8.1, eFig. 8.1). Ganglion cells have been reported in some lesions. An S100 immunostain can be used to highlight the neural nature of these lesions.









TABLE 8.1 Neural Lesions of the Upper Aerodigestive Tract





Traumatic neuroma


Mucosal neuroma


Neurofibroma


Schwannoma


Granular cell tumor


Neurothekeoma


Nerve sheath myxoma


Palisaded, encapsulated neuroma (solitary, circumscribed neuroma)


Malignant peripheral nerve sheath tumor


Paraganglioma


Olfactory neuroblastoma


The mucosal neuromas of multiple endocrine neoplasia (MEN) type 2b resemble traumatic neuromas and are composed of convoluted neural tissue with numerous axons surrounded by a thickened perineurium.1,3 These lesions mostly involve the lips and tongue, but can also involve other oral and nasal sites. The syndrome is associated with familial mutations of the RET protooncogene and the development of medullary thyroid carcinoma and pheochromocytomas.3,4 It is important to distinguish these lesions from neurofibromas as the lesions occur in vastly different syndromes and have different risks for subsequent diseases.






FIGURE 8.1 Traumatic neuroma with complex well-formed nerve.







FIGURE 8.2 A plexiform neurofibroma infiltrating surrounding skeletal muscle.

Solitary and multiple neurofibromas can also occur throughout the upper aerodigestive tract and may be associated with neurofibromatosis type 1.1,5,6,7 The distinction of these lesions from other neural tumors is thus important, as the diagnosis can allow for the identification of the other stigmata of the disease. Neurofibromas appear either somewhat circumscribed or plexiform (Fig. 8.2); however, even when they appear circumscribed, the interface of the lesion with the surrounding soft tissue is usually not discrete. The lesions are composed of intermixed spindled cells with serpentine or wavy nuclei, collagenous fibers, and myxoid matrix (eFig. 8.2). A mixture of S100 protein and CD34 immunoreactive cells can be identified by immunohistochemistry. Neurofibromas can usually be distinguished from other neural tumors because of their classic, rather uniform histology.

Schwannomas or neurilemomas also occur throughout the upper aerodigestive tract.1,5,8,9 Aside from those which involve the ear, they appear to be most frequent in the sinonasal area. The tumors occur in older adults and usually present as polypoid masses with symptoms secondary to mass effect. Although benign, schwannomas may be associated with the destruction of surrounding bony tissues.8 When not resected in a piecemeal fashion, the lesions will sometimes appear circumscribed and encapsulated although this feature seems to be less common than with peripheral schwannomas, and infiltration adjacent to mucosal epithelium may be seen.8 Histologically, the tumors are similar to those seen at other sites of the body and are composed of variably cellular areas (cellular Antoni A and looser, less cellular Antoni B areas) (Fig. 8.3, eFig. 8.3). Cellular palisading or Verocay bodies can be identified in some cases,
and hyalinized blood vessels can be found in most examples (eFigs. 8.4 and 8.5).8,9 The tumors show strong and diffuse immunoreactivity with antibodies to S100. Although occasional cells may be immunoreactive with antibodies to CD34, such cells are much fewer in number than in neurofibromas.8,9






FIGURE 8.3 Schwannomas can be very cellular.

Granular cell tumors occur throughout the body, but the tongue is the most commonly involved anatomic site.10,11 The lesions usually present as painless submucosal nodules. Frequently, the overlying squamous epithelium will show a significant amount of pseudoepitheliomatous hyperplasia, a well-described pitfall that has led some cases to be erroneously diagnosed as squamous cell carcinomas.10,11 Granular cell tumors are circumscribed, but not encapsulated and neoplastic cells frequently infiltrate the surrounding soft tissues. The constituent cells are large and polygonal with abundant granular, eosinophilic cytoplasm (Fig. 8.4). Ultrastructurally, the granularity is due to numerous lysosomes filling the cytoplasm.10 Nuclei are small and centrally located and rare cells may be multinucleated. Mitotic figures are uncommon, but occasional typical forms can be identified. By immunohistochemistry, the neoplastic cells react strongly and diffusely with antibodies to S100 protein (eFig. 8.6) and other markers of antigens associated with peripheral nerves.12,13 Not surprisingly, the neoplastic cells react with antibodies to lysozyme and CD68.14 Rare granular cell tumors are malignant, and as such are characterized by a larger size, necrosis, increased mitotic activity, and cellular atypia. Distinction of malignant tumors and multifocal granular cell tumors may be difficult.







FIGURE 8.4 The large and polygonal cells of a granular cell tumor.

It is unclear how congenital epulis or congenital granular cell tumor relates to the typical adult granular cell tumor. These tumors present as large polypoid masses attached to the gingiva of newborns, almost always in girls.15 By conventional H&E histology, they are identical to adult granular cell tumors (eFig. 8.7). The neoplastic cells do not react with antibodies to S100 protein, however.16 Unlike nonneural granular cell tumors of the skin, congenital epulis does not appear to have ALK translocations.17

Nerve sheath myxomas and neurothekeomas are uncommon, benign tumors.18,19,20 Both may involve the head and neck and when reported in the upper aerodigestive tract, they have almost exclusively involved the mouth. Histologically, nerve sheath myxomas are lobular and well-circumscribed although they do not have a capsule.1,19 The lobules are composed of abundant myxoid stroma with intermixed spindled cells and are separated from one another by fibrous connective tissue that resembles perineurium (eFig. 8.8). These lesions show immunoreactivity with antibodies to S100 protein. Neurothekeomas are also typically well-circumscribed and grow as lobules of neoplastic cells separated by bands of collagen (Fig. 8.5). Frequently, some degree of myxoid matrix is present. The growth pattern is typically whirled although some fascicular growth may be present. Tumor cells are spindled and epithelioid with abundant eosinophilic cytoplasm. Only minimal to mild atypia is present in most cases and mitotic figures are usually infrequent. Osteoclastlike giant cells are sometimes present. Unlike nerve sheath myxomas, these lesions are not immunoreactive with antibodies to S100 protein. They are typically immunoreactive with antibodies
to NKI/C3, vimentin, and NSE. Frequently, they are immunoreactive with antibodies to MSA and SMA. Recently, some have suggested that these tumors may be related to fibrous histiocytomas.21






FIGURE 8.5 Neurothekeomas have a lobular and circumscribed growth pattern.

Palisaded, encapsulated neuroma or solitary circumscribed neuroma is a benign tumor of the peripheral nerve sheath that mostly occurs subcutaneously but may involve the mouth, especially in the region of the lips, gingiva, and palate.22,23,24 The lesions are described as slow growing and painless and are mostly identified in adults. Histologically, they are well-circumscribed and partially encapsulated (Fig. 8.6). Tumors are composed of broad fascicles of spindled cells with little intervening eosinophilic stroma. Although the nuclei can focally appear vaguely parallel, palisading Verocay bodies akin to those seen with schwannomas are not usually seen with this tumor, in spite of its name.22,24 Furthermore, hypocellular areas are also not seen. Small vessels are often noted, and hemorrhage and necrosis are not seen. Most tumor cells react with antibodies to S100 protein. Immunostaining for EMA will highlight the perineurium that surrounds the lesions.22,23

Malignant peripheral nerve sheath tumors (MPNSTs) also occur throughout the upper aerodigestive tract and have been frequently noted in the sinonasal area.25,26,27 These tumors develop in older individuals and most often occur in patients who do not have neurofibromatosis. Unlike schwannomas, MPNSTs are infiltrative and destructive and after resection, tend to recur and eventually metastasize.26,27 MPNSTs are usually highly cellular and generally have a histologic pattern reminiscent of a fibrosarcoma, although a prominent herringbone pattern is usually not seen and the nuclei tend to appear more irregular and wavy (Fig. 8.7).26,27
MPNSTs also have been noted to have alternating less cellular (eFig. 8.9) areas and rare nuclear palisading. Compared to benign neurogenic tumors, mitotic figures in MPNSTs are usually increased in number and geographic necrosis can sometimes be found (Fig. 8.8). To assist in the diagnosis, immunohistochemistry can be helpful, especially if the tumor
is immunoreactive with antibodies to S100 protein.26,27 Staining for CD56 is more sensitive but less specific (eFig. 8.10). Importantly, with small biopsies, positive staining with antibodies to S100 protein does not clinch a diagnosis of MPNST and malignant melanoma must be excluded.26 Also of note, up to 15% of MPNSTs are immunoreactive with antibodies to TLE1, an antibody generally used to diagnose synovial sarcoma.28 A significant portion of tumors originally classified as MPNSTs of the sinonasal tract likely represent biphenotypic sinonasal sarcoma and will thus express S100 and SMA and have PAX3 translocations (see Chapter 11).29,30,31






FIGURE 8.6 A solitary circumscribed neuroma of the lip.






FIGURE 8.7 A cellular area within a malignant peripheral nerve sheath tumor with somewhat wavy nuclei.






FIGURE 8.8 Geographic necrosis seen in a malignant peripheral nerve sheath tumor.

Most paragangliomas of the head and neck arise at the carotid body, the vagal body, or the middle ear. Those that arise in the upper aerodigestive tract usually arise within the nasal cavity and larynx.32,33,34 Occasional tumors, likely arising in the vagal body, will present as nasopharyngeal masses. Paragangliomas develop in both sexes, usually in adults. Those that arise in the head and neck present almost exclusively with mass-related symptoms, or other nonspecific symptoms related to their site of presentation (e.g., epistaxis when in the nasal cavity).32,34 Head and neck paragangliomas almost never produce symptoms secondary to hormone production, especially catecholamine production. Some pheochromocytomas and extra-adrenal paragangliomas are familial and can be seen with mutations of the VHL gene, RET proto-oncogene, and the genes encoding for subunits of succinate dehydrogenase (e.g., SDHB).35

The tumors have a typical histology, akin to that seen with pheochromocytomas of the adrenal gland.33,34 They tend to be well-circumscribed and partially encapsulated. The tumors are composed of nests of epithelioid
cells with finely granular, eosinophilic cytoplasm and round to oval nuclei (Fig. 8.9, eFig. 8.11). The nuclei may have granular chromatin, and occasional prominent nucleoli may be seen (Fig. 8.10). Atypia may be present and should not be considered a feature suggestive of malignancy. Mitotic figures are rare. Surrounding the nests are slender sustentacular cells and a rich network of capillaries. By immunohistochemistry,
neoplastic cells will react with antibodies to chromogranin, synaptophysin, and NSE.36,37 They do not react with antibodies to cytokeratins. Supporting sustentacular cells will react with antibodies to S100 protein (Fig. 8.11). Although some tumors will behave in a malignant fashion, histology provides little clues to distinguish benign and malignant tumors. Some have suggested that a lack of sustentacular cells, identified by an absence of S100 protein staining, may help to identify malignant tumors.38






FIGURE 8.9 A laryngeal paraganglioma showing an obvious nested pattern.






FIGURE 8.10 Most of the nuclei of paragangliomas have granular chromatin.






FIGURE 8.11 S100 immunostaining of a laryngeal paraganglioma highlights the sustentacular cells.

Olfactory neuroblastomas (ONBs) are rare tumors that develop in the upper nasal cavity in the area of the olfactory epithelium.39,40,41 The tumors show a bimodal age incidence and occur most frequently in adolescents and older adults. The tumors do not show a predilection for either sex or race. Patients with these malignancies present with nonspecific symptoms including nasal stuffiness, epistaxis, nasal discharge, headache, and anosmia. Occasionally, visual changes can be present.

The tumors are usually polypoid and occur high in the nasal cavity in the region of the cribriform plate, superior turbinate, and ethmoid sinuses.39,41 The location of the tumor and its phenotypic characteristics have led most to consider it to be a malignancy of the olfactory epithelium. As biopsy specimens are received piecemeal and as patients are usually treated prior to surgical resection, staging is usually performed clinically and radiographically, based on the extent of the tumor according to the method originally described by Kadish (Table 8.2).41 Molecular changes are complex, similar to most epithelial malignancies.42 ONB is not a member of the Ewing sarcoma group of tumors and the typical t(11;22) seen in
those tumors is not seen with ONBs, despite an early paper claiming the contrary.43,44,45 With current multimodality treatments, patients with ONB do quite well and some have reported survival rates at 10 years to be greater than 80%.46,47








TABLE 8.2 Kadish Staging System for Olfactory Neuroblastoma












Stage A


Limited to the nasal cavity


Stage B


Limited to the nasal cavity and paranasal sinuses


Stage C


Local or distant spread beyond the nasal cavity and paranasal sinuses


Microscopically, tumor cells grow either diffusely or in discrete, circumscribed nests that are separated by fibrous or edematous stroma (Figs. 8.12 and 8.13).39,41 About 25% of cases have definitive Homer Wright rosettes with annular arrays of neoplastic cells surrounding central, eosinophilic fibrils (Fig. 8.14, eFig. 8.12). Many more will show more equivocal rosette formations surrounding fibrillary material and the remainder lack even rudimentary rosettes. An eosinophilic fibrillary background can be found in most cases (Fig. 8.15, eFig. 8.13) and calcification will be seen with some cases (eFig. 8.14). Vascular invasion and necrosis, either as single-cell apoptosis or as large zones, are often seen. Mature ganglion cells are also identified in some cases (eFig. 8.15). The neoplastic cells are small and usually have minimal eosinophilic cytoplasm.
The nuclei often appear monomorphic and round with delicate granular chromatin. Prominent nucleoli and mitotic figures are usually absent. The tumor can, however, display a wide range of atypia and some cases may show marked variation in nuclear size and shape. Mitotic activity can also vary greatly and some cases have been noted to have more than 10
mitotic figures per high-powered field. ONBs have been graded according to the Hyams grading system (Table 8.3) which takes into account tumor architecture, nuclear atypia, mitotic activity, necrosis, and the presence or absence of background fibrillary material.48 There have been mixed reports regarding the utility of this grading system, and it should be noted that it was developed prior to the distinction of other high-grade neuroendocrine
tumors of the sinonasal tract, including sinonasal undifferentiated carcinoma (which may have originally been reported as grade 4 ONBs). As a result, most ONBs that we now see would be considered to be grade 1 or 2 neoplasms.






FIGURE 8.12 Olfactory neuroblastoma with a diffuse growth pattern.






FIGURE 8.13 Olfactory neuroblastoma with a nested growth pattern.






FIGURE 8.14 Homer Wright rosettes can be found in many olfactory neuroblastomas.






FIGURE 8.15 A neurofibrillary background can be seen with most cases of olfactory neuroblastoma.








TABLE 8.3 Hyams Grading Scheme for Olfactory Neuroblastoma





















































Histology


Grade 1


Grade 2


Grade 3


Grade 4


Lobular architecture


Predominant


Predominant


Occasional


Infrequent


Nuclear Pleomorphism


Minimal


Mild


Moderate


Marked


Mitotic figures


Rare


Occasional


Abundant


Abundant


Calcification


Sometimes present


Sometimes present


None


None


Necrosis


None


None


Some


Abundant


Fibrillary background


Abundant


Abundant


Less frequent


Not seen


H-W rosettes


Often seen


Often seen


Not seen


Not seen


H-W, Homer Wright.


Although many ONBs can be diagnosed based on histology alone, immunohistochemistry is often prudently used for a number of reasons (Table 8.5).40,49 The distinction of these lesions from other sinonasal tumors such as sinonasal undifferentiated carcinomas has significant prognostic value. Furthermore, biopsy specimens are often limited in both tumor quantity and quality, frequently exhibiting marked crush artifact. Most ONBs will show immunoreactivity with antibodies to synaptophysin or chromogranin, as well as with antibodies to less specific markers of neural or neuroendocrine differentiation such as NSE and CD56 (Fig. 8.16). Although most ONBs do not react with antibodies to cytokeratins, occasional tumors will display focal positivity and thus cytokeratin reactivity should not dissuade one from making the diagnosis. In our experience, strong reactivity with antibodies to cytokeratin is very rare with ONBs. S100 immunoreactivity, when present, is usually limited to the supporting or sustentacular cells that surround the neoplastic nests (Fig. 8.17). Occasional tumor cells may show limited reactivity with antibodies to S100; however, staining for other markers of melanoma, such as HMB45, should not be seen. Finally, membranous reactivity with antibodies to CD99 should not be seen nor should nuclear staining with antibodies to FLI1.






FIGURE 8.16 Olfactory neuroblastomas are generally immunoreactive with antibodies to synaptophysin.







FIGURE 8.17 Sustentacular cells of olfactory neuroblastomas can be highlighted with an S100 immunostain.


NEUROECTODERMAL LESIONS


Melanotic Neuroectodermal Tumor of Infancy

This rare tumor can occur throughout the head and neck but usually involves maxilla or, less commonly, the mandible.50,51,52,53,54 Patients are more often males and are usually younger than 1, although melanotic neuroectodermal tumors of infancy (MNTIs) sometimes present in older children. The prognosis for MNTI is good, and although tumors can recur, they only rarely metastasize.52 The lesions usually are less than 5 cm in greatest dimension and appear grossly lobulated and circumscribed although capsules are not present. On cut surface the tumors may appear gray-white to darkly pigmented.52

Histologically, two cell populations are present. Larger, epithelioid cells with vesicular nuclei and prominent nucleoli and abundant eosinophilic cytoplasm that contains dark brown granular melanin pigment arrange themselves together in loose alveolar or tubular structures while small, round to oval cells with hyperchromatic nuclei and scant cytoplasm form small nests, cords, or sheets usually surrounded by the larger, epithelioid cells (Figs. 8.18 and 8.19, eFigs. 8.16-8.18).51,52 Dense collagenous stroma separates the alveoli, pseudoglandular spaces, tubular structures, and small nests of neoplastic cells from one another. Occasionally, a more fibrillary stroma is identified within the islands of smaller cells. Neoplastic cells infiltrate into adjacent bone and soft tissue. Histologic features of a high-grade malignancy such as abundant mitotic figures or necrosis are not noted.

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Jan 24, 2021 | Posted by in PATHOLOGY & LABORATORY MEDICINE | Comments Off on Neural, Neuroectodermal, and Neuroendocrine Neoplasms

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