The 2007 WHO Classification of Tumours of the Central Nervous System

This newly identified tumour (Fig. 1) occurs predominantly in children and young adults (mean age at surgery, 17 years), with refractory epilepsy as the leading clinical symptom. A total of 28 cases has been reported from the United States [51], France [33], and Austria/Germany [41]. Angiocentric gliomas are located superficially, the most common sites being the fronto-parietal cortex and the temporal lobe as well as the hippocampal region. FLAIR images show well delineated, hyperintense, non-enhancing cortical lesions, often with a stalk-like extension to the subjacent ventricle [41]. The tumours are stable or slowly growing and histopathologically characterized by monomorphous bipolar cells, an angiocentric growth pattern and immunoreactivity for EMA, GFAP, S-100 protein and vimentin, but not for neuronal antigens. Despite frequent extension of angiocentric glioma to the ventricular wall and the presence of microscopic features suggestive of ependymal differentiation, the predominant clinical symptoms, cortical location, architectural pattern and outcome were considered insufficient to designate this entity as an ependymoma variant. Given the uncertainties regarding histogenesis, angiocentric glioma was grouped with astroblastoma and chordoid glioma of the third ventricle in the category of ‘Other neuroepithelial tumours’, previously designated ‘Tumours of uncertain origin’. Due to its benign clinical behaviour and the possibility of curative surgery, the neoplasm was assigned to WHO grade I.

Most intraventricular papillary neoplasms derived from choroid plexus epithelium are benign in nature and can be cured by surgery (choroid plexus papilloma, WHO Grade I, ICD-O 9390/0). At the other side of the spectrum is the choroid plexus carcinoma (WHO Grade III, ICD-O 9390/3) with frank signs of malignancy, including brisk mitotic activity, increased cellularity, blurring of the papillary pattern, necrosis and frequent invasion of brain parenchyma. The WHO Working group proposes to introduce an additional entity with intermediate features, designated ‘atypical choroid plexus papilloma’ which is primarily distinguished from the choroid plexus papilloma by increased mitotic activity. Curative surgery is still possible but the probability of recurrence appears to be significantly higher. To reflect this concern, the proposed ICD-O code is the same as for other choroid plexus tumours but carries the /1 extension (ICD-O 9390/1).

The term central neurocytoma describes a neuronal tumour with pathological features distinct from cerebral neuroblastoma, occurring in young adults, with preferential location in the lateral ventricles in the region of the foramen of Monro and a generally favourable prognosis. Central neurocytomas are composed of uniform round cells with immunohistochemical and ultrastructural evidence of neuronal differentiation. Additional features include fibrillary areas mimicking neuropil, and a low proliferation rate. During the past decade several reports have shown that neoplasms occur in brain parenchyma outside the ventricular system with similar biological behaviour and histopathological characteristics although the latter appear to exhibit a somewhat larger morphological spectrum. For these neoplasms, the 2007 WHO classification recommends the term ‘extraventricular neurocytoma’ and proposes an ICD-O code identical to that of central neurocytoma (9506/1).

The papillary glioneuronal tumour (Fig. 2) was established as a distinct clinico-pathologic entity by Komori et al. in 1998 [28]. Histopathologically similar tumours had previously been described as pseudopapillary ganglioglioneurocytoma [29] and pseudopapillary neurocytoma with glial differentiation [23]. PGNT manifests over a wide age range (mean 27 years) and is a clinically benign neoplasm that typically corresponds to WHO grade I. Its preferential location is the temporal lobe. On CT and MR images, it appears as a contrast-enhancing, well delineated mass, occasionally showing a cyst-mural nodule pattern. Histologically, it is characterized by a single or pseudostratified layer of flat to cuboidal, GFAP-positive astrocytes surrounding hyalinized vascular pseudopapillae and by synaptophysin-positive interpapillary sheets of neurocytes, large neurons and intermediate size “ganglioid” cells. This tumour is part of the growing list of relatively benign glioneuronal tumours.

This newly included entity, initially described as dysembryoplastic neuroepithelial tumour (DNT) of the cerebellum [32], was established as distinct disease entity in a report of 11 cases by Komori et al. in 2002 [30]. Since then, a total of 17 cases have been reported. Rosette-forming glioneuronal tumour of the fourth ventricle (RGNT) is defined as a rare, slowly growing tumour of the fourth ventriclular region that predominantly affects young adults (mean age 33 years) and causes obstructive hydrocephalus, ataxia being the most common clinical manifestation. RGNT typically arises in the midline and primarily involves the cerebellum and wall or floor of the fourth ventricle. It often occupies the fourth ventricle and/or aqueduct, and may show parenchymal extension. T2-weighted MR imaging reveal a well delineated, hyperintense tumour. Histopathologically, RGNTs are characterized by a biphasic neurocytic and glial architecture [18, 30, 40]. The neuronal component consists of neurocytes that form neurocytic rosettes with eosinophilic, synaptophysin-positive cores and/or perivascular pseudorosettes. The glial component dominates and typically exhibits features of pilocytic astrocytoma. Given its benign clinical behaviour with the possibility of surgical cure, the rosette-forming glioneuronal tumour (RGNT) corresponds to WHO grade I. It shares the new ICD-O code 9509/1 with the papillary glioneuronal tumour (PGNT).

This recently described rare neuroepithelial tumour (Fig. 3) of the pineal region manifests in children and adults (mean age 32 years), is relatively large (2.5–4 cm), and well-circumscribed, with MR imaging showing a low T1 and increased T2 signal as well as contrast enhancement. In addition to the initial 2003 report of six cases by Jouvet et al. [20], a total of 38 cases have been published to date. Histologically, papillary tumours of the pineal region are characterized by a papillary architecture and epithelial cytology, with immunoreactivity for cytokeratin and, focally, GFAP. Although macroscopically indistinguishable from pineocytoma, the histology is incompatible with a pineal parenchymal tumour. Ultrastructural features suggest ependymal differentiation and a possible origin from specialized ependymal cells of the subcommissural organ (SCO) has been suggested [20]. The biological behaviour of papillary tumour of the pineal region (PTPR) is variable and may correspond to WHO grades II or III, but precise histological grading criteria remain to be defined. The code 9395/3 has been proposed for the fourth edition of ICD-O.

Pituicytoma is a rare, solid, low grade, spindle cell, glial neoplasm of adults that originates in the neurohypophysis or infundibulum (Fig. 4). In the past, the term pituicytoma was also applied to other tumours in the sellar and suprasellar region, particularly granular cell tumours and pilocytic astrocytomas. Presently, it is reserved for low-grade glial neoplasms that originate in the neurohypophysis or infundibulum and are distinct from pilocytic astrocytoma. Less preferred terms for pituicytoma include ‘posterior pituitary astrocytoma’ and, for lesions arising in the pituitary stalk, ‘infundibuloma’. The WHO Working Group felt that inclusion of the diagnostic term pituicytoma would help to more clearly delineate neoplasms manifesting in the neurohypophysis and pituitary stalk.

To date, less than 30 bona fide examples have been described, often as case reports. Clinical signs and symptoms include visual disturbance, headache and features of hypopituitarism. Pituicytomas are well-circumscribed, solid masses that can measure up to several centimetres. Histologically, they show a compact architecture consisting of elongate, bipolar spindle cells arranged in interlacing fascicles or assuming a storiform pattern [2, 48]. Mitotic figures are absent or rare. Pituicytomas are generally positive for vimentin, S-100 protein and, to a variable degree, GFAP. In contrast to spindle cell oncocytoma (see below), oncocytic change is lacking. Due to their slow growth and the possibility of curative surgery, pituicytomas correspond to WHO grade I. The code 9432/1 has been proposed for the fourth edition of ICD-O.

Spindle cell oncocytoma (Fig. 5) is defined as an oncocytic, non-endocrine neoplasm of the anterior pituitary that manifests in adults (mean age 56 years). These tumours may macroscopically be indistinguishable from a non-functioning pituitary adenoma and follow a benign clinical course, corresponding to WHO grade I. The eosinophilic, variably oncocytic cytoplasm contains numerous mitochondria, is immunoreactive for the anti-mitochondrial antibody 113-I as well as to S-100 protein and EMA, but is negative for pituitary hormones. Since the initial 2002 report of five cases by Roncaroli et al. [43], five additional cases have been published from three institutions [4, 27, 49]. The code 8291/0 has been proposed for the fourth edition of ICD-O.

Originally described by Jänisch et al. in 1985 as ‘diencephalic pilocytic astrocytoma with clinical onset in infancy’ [19], the term pilomyxoid astrocytoma was introduced in 1999 by Tihan et al. [47] who also defined its characteristic histopathological features. Pilomyxoid astrocytoma (PMA) (Fig. 6) occurs typically in the hypothalamic/chiasmatic region, sites that are also affected by classical pilocytic astrocytomas. PMA is histologically characterized by a prominent myxoid matrix and angiocentric arrangement of monomorphous, bipolar tumour cells. The close relationship to pilocytic astrocytoma is underscored by a report of two cases that occurred in the setting of neurofibromatosis type 1 (NF1). PMA affects predominantly infants and children (median age, 10 months) and appears to have a less favourable prognosis. Local recurrences and cerebrospinal spread are more likely to occur in pilomyxoid than in pilocytic astrocytomas. The Working Group therefore recommended an assignment to WHO grade II and the new code 9425/3 has been proposed for the fourth edition of ICD-O.

This variant of medulloblastoma is characterized histologically by marked nuclear pleomorphism, nuclear moulding, cell–cell wrapping, and high mitotic activity, often with atypical forms. Although all medulloblastomas show some degree of atypia, these changes are particularly pronounced and widespread in the anaplastic variant. Histological progression from classic to anaplastic medulloblastomas may be observed, even within the same biopsy. The highly malignant large cell medulloblastomas and anaplastic medulloblastomas have considerable cytological overlap. The large cell variant features often spherical cells with round nuclei, open chromatin and prominent central nucleoli. The patterns may coexist. Indeed, in several studies a combined large cell/anaplastic category has been used. It is proposed that in the fourth edition of ICD-O anaplastic medulloblastoma and large cell medulloblastoma share the same code 9474/3.

The medulloblastoma with extensive nodularity is closely related to the desmoplastic/nodular medulloblastoma (9471/3) and was previously designated ‘cerebellar neuroblastoma’. It occurs in infants and differs from the desmoplastic nodular variant by exhibiting a markedly expanded lobular architecture, due to the fact that the reticulin-free zones become unusually large and rich in neuropil-like tissue. Such zones contain a population of small cells resembling those of a central neurocytoma and exhibit a streaming pattern. The internodular reticulin-rich component, which dominates in the desmoplastic/nodular variant, is markedly reduced. Following radiotherapy and/or chemotherapy, medulloblastomas with extensive nodularity may occasionally undergo further maturation to tumours dominated by ganglion cells. A more favourable outcome than for patients with classic medulloblastomas is recognized for both, the desmoplastic/nodular medulloblastoma variant and medulloblastoma with extensive nodularity. It is proposed that medulloblastoma with extensive nodularity and desmoplastic/nodular medulloblastoma share the same ICD-O code 9471/3.