QUATER-1-PE-HEALTH-LC2- this is just a sample of unpacked lesson
Case record...Neurofibromatosis type 2
1. CASE OF THE WEEK
PROFESSOR YASSER METWALLY
CLINICAL PICTURE
CLINICAL PICTURE:
A 22 years old male patient presented clinically with bilateral tinnitus, headache, bilateral diminution of hearing,
bilateral papilledema, bilateral facial nerve palsy, bulbar cranial nerves dysfunction, right sided cerebellar
manifestation and bilateral long tract dysfunction.
RADIOLOGICAL FINDINGS
RADIOLOGICAL FINDINGS:
Figure 1. Bilateral vestibular schwannomas. The bilateral cerebellopontine angle tumors are hypointense on the
precontrast MRI T1 images (Antoni B schwannomas). Notice that the brain stem is bilaterally compressed and
squeezed by the bilateral tumors. Also notice the CSF cleft that separates the bilateral tumors from the neural tissues
(The tumors are extra-axial). Moderate degree of hydrocephalus is present.
2. Figure 2. Bilateral vestibular schwannomas. Postcontrast MRI T1 images showing dense and uniform contrast
enhancement of the bilateral tumors.
Figure 3. Bilateral vestibular schwannomas. MRI T2 and FLAIR images. The tumors have heterogenous signal on
both T2 and FLAIR images with hyperintense zones which, most probably, represent cystic (fluid -filled) areas
(Antoni B tissues).
3. Figure 4. Bilateral vestibular schwannomas. MRI FLAIR images. Notice the moderate hydrocephalic changes and the
transependymal edema. Also notice the CSF cleft that separates the tumor from the brain stem. The tumor
hyperintensity is due to the existence of cystic changes (Antoni B tissues).
Figure 5. Bilateral vestibular Antoni B tissue schwannoma. Notice that the tumours are hypointense of precontrast
MRI T1 image, with intense contrast enhancement. The tumours are mainly hyperintense in MRI T2 image. Notice
the CSF cleft that separate the tumours from the brain stem,a sign which indicates the extraaxial location of the
tumours. The brain stem is compressed bilaterally. The T1,T2 signal changes are due to the higher water content of
Antoni B tissue.
4. DIAGNOSIS:
DIAGNOSIS: NEUROFIBROMATOSIS TYPE 2
Synonyms:
Bilateral acoustic neurofibromatosis
Bilateral vestibular schwannomas (Antoni B schwannomas, surgically confirmed)
DISCUSSION
DISCUSSION:
Benign nerve sheath tumors can be categorized into schwannoma and neurofibroma based on histopathologic
characteristics. Schwannomas are solitary encapsulated tumors located along cranial or spinal nerves or nerve roots.
These tumors consist of Schwann cells and do not contain nerve tissue. Histologically the tumor contains a mixture of
two clear-cut patterns: Antoni A tissue has a compact arrangement of cells and reticulin fibers. Antoni B tissue is loose
textured, mucinous, and free of fibrillary background. These lesions can be seen in association with neurofibromatosis.
Figure 6. Antoni A tissue [a] and Antoni B tissues [b]
Figure 7. A, Schwannoma. B, A schwannoma with
mixed Antoni A, dense cellular areas, and Antoni B,
loosely structured areas.
TISSUE TYPE DESCRIPTION
It consists of compact bipolar, elongated, spindle-shaped, lipid rich schwann
cells with twisted nuclei, indistinct cytoplasmic borders, and, occasionally,
5. clear intranuclear vacuoles. The cells are arranged in short bundles or
Antoni A tissue (Dense, fibrillary, solid interlacing fascicles with nuclear palisading, whorling of the cells, and
compact type) Verocay bodies. Verocay bodies are formed by 2 compact rows of well-
aligned nuclei and cell processes that are arranged in a roughly oval shape.
Is loose textured, mucinous and free of fibrillary background. Cells are
Antoni B tissue (Loose, reticulated,
separated by large amount of oedematous tissue that coalesce to form cystic
cystic type)
spaces. Cells are scanty and vacuolated
Neurofibromas are tumors of the cranial, spinal, or peripheral nerves and are intimately continuous with the nerve
proper. The affected nerve is circumferentially compressed and diffusely penetrated by elements of tumor.
Histopathologically neurofibromas contain all elements of the nerve, including Schwann cells, myelinated and
unmyelinated nerve fibers, and fibroblasts. Thus it is difficult to remove the tumor without sacrificing the nerve.
Plexiform neurofibromas are pathognomonic of von Recklinghausen's disease. These tumors appear as tortuous
entanglements or fusiform enlargements of the peripheral nerves. They often trap soft tissues, such as adipose tissue
and muscle. Malignant nerve sheath tumors are seen in association with neurofibromatosis.
Figure 8. Schwannoma, A, and neurofibroma, B
Figure 9. A, Schwannoma. Antoni A, densely
cellular area, no Verocay body. B
Schwannoma. Antoni A, densely cellular area
with nuclear palisading or Verocay body
Pathologically neurofibromas are composed of a central fibrocollagenous core and a peripheral myxomatous tissues.
These tissue characteristics frequently determines the MRI appearance of neurofibromas.
6. Figure 10. The peripheral myxomatous tissue (yellow) and the central fibrocollagenous core of neurofibromas (brown)
Schwannomas Neurofibromas
Usually single tumours (only multiple in
type II neurofibromatosis,bilateral Invariably multiple
acoustic schwannomas)
Composed of all nerve tissues (schwann cells, myelinated and non-
Composed of schwann cells only
myelinated nerve tissues and nerve axons)
The loose, myxomatous Antoni type B tissue of a neurilemoma may mimic
a neurofibroma. However, NFs lack the thick collagenous capsule of a
neurilemoma and instead are surrounded by a variably thickened
perineurium and epineurium. NFs also lack the Antoni type A and B
patterns, as well as Verocay bodies, typical of a neurilemoma. NFs are
Antoni A,B, tissues composed of a mucinous matrix containing scattered myelinated and
nonmyelinated axons along with a heterogeneous cell population including
Schwann cells, fibroblasts and perineural cells. Immunoreactivity for S-
100 protein consequently is observed in only a portion of the cells
comprising a NF, as opposed to uniform reactivity throughout a
neurilemoma.
CT SCAN IMAGING OF NERVE SHEATH TUMOURS
CT-Pathology correlation of schwannomas
Cell type CT scan picture
Schwannomas with Antoni A tissue containing lipid- rich Schwann cells
Schwannomas with Antoni A tissue
appear lucent on noncontrast CT scan.
Schwannomas with Antoni B tissue appear cystic on CT scan as a result of
loosely textured stroma that has a cystic component. The cells are separated
Schwannomas with Antoni B tissue by large amounts of edematous fluid, which coalesce to form cystic spaces.
Cystic changes are more common in the cranial schwannomas than in spinal
lesions (Antoni B schwannomas are more common intracranially)
7. Figure 11. A, Postcontrast CT showing bilateral vestibular schwannomas. Notice central cavitations (Antoni B tissues),
B, postmortem specimen showing vestibular schwannoma compressing the brain stem.
Figure 12. A. showing the cystic Antoni B schwannoma compressing the brain stem, B, showing the solid
neurofibroma
Figure 13. A, Vestibular schwannoma (arrows). B, Histologically, the tumor is made up of sheets of uniform spindle
cells, some of which are forming palisades called Verocay bodies.
8. Figure 14. The sheets of uniform spindle cells resemble normal
Schwann cells. In addition, a foamy, reticulated tissue is sometimes
seen in these tumors, which may represent degeneration of these cells.
The dense spindled areas are known as Antoni A areas while the looser
areas are Antoni B. Both types of tissue are seen in this figure.
CT-Pathology correlation of neurofibroma
Neurofibromas with predominantly lipid- rich Schwann cells are lucent on CT scan. Neurofibromas composed
predominantly of compactly arranged collections of fibroblasts with abundant production of dense bundles of collagen
appear dense on CT scan. Tumors show minimal to intense, homogeneous to inhomogeneous, or peripheral ringlike
enhancement on postcontrast study.
MRI IMAGING OF NERVE SHEATH TUMOURS
Imaging of schwannomas
Schwannomas arise from perineural Schwann cells. They are neoplasms that usually arise from sensory nerves. In the
intracranial compartment, approximately 80% of schwannomas involve the internal auditory canal. Bilateral acoustic
schwannomas are diagnostic of neurofibromatosis type 2. 1
Figure 15. Schwannoma. Antoni B, loosely cellular areas with
vacuolated cells and with round or oval nuclei.
9. Figure 16. Foramen magnum schwannoma. A, Contiguous off-midline sagittal unenhanced Tl- weighted MR images
demonstrate a circumscribed mass (arrows) at the foramen magnum. B, Coronal enhanced Tl -weighted MR image
shows avid enhancement of the schwannoma. Note central hypointensity consistent with necrosis (arrowhead),
widening of the ipsilateral cerebrospinal fluid (CSF) space (arrows), and displacement of the cervicomedullary
junction from right to left.
Calcification and reaction in the adjacent bone are unusual. The MR
Antoni type A tumors are composed of packed cells,
imaging appearance of schwannomas is dependent on their cellular resulting in a hypointense appearance (isointense to brain)
makeup. Antoni type A tumors are composed of packed cells, resulting on T2-weighted imaging. Antoni type B schwannomas
in a hypointense appearance (isointense to brain) on T2-weighted typically have a higher water content and a low cell ratio
imaging. Antoni type B schwannomas typically have a higher water resulting in a hyperintense appearance on T2-weighted
content and a low cell ratio resulting in a hyperintense appearance on imaging.
T2-weighted imaging. 2 A given acoustic neuroma may contain areas
with both Antoni A and Antoni B tissue. Most schwannomas enhance; however, the enhancement is frequently
heterogeneous. 3 This is largely related to the development of central necrosis, which occurs in most lesions that are
more than 2 cm in size. The presence of an enhancing dural tail is unusual with schwannomas, but may occasionally
be present.
Figure 17. Antony B schwannoma
Cell type MRI picture
Antoni type A schwannomas (solid hypercellular The tumours are composed of packed cells, resulting in a
tumours with high nuclear to cytoplasmic ratio and with hypointense appearance (isointense to brain) on T2-
minimal extracellular water) weighted imaging.
10. The tumours typically have a higher water content and a
Antoni type B schwannomas (cystic tumours) low cell ratio resulting in a hyperintense appearance on
T2-weighted imaging.
The other common region in the posterior fossa where extra-axial neoplasms occur is the cerebellopontine angle.
Enhancing masses that occur in the cerebellopontine angle in decreasing order of frequency include schwannomas,
meningiomas, and metastatic disease. 2 Other lesions that may occur here include aneurysms arising from the anterior
inferior cerebellar artery or the vertebral-basilar system. 2 Exophytic brainstem gliomas and fourth ventricular
ependymomas may extend into the cerebellopontine angle and foramen magnum, 2 but the origin of these masses from
the brain- stem and fourth ventricle, respectively, is usually evident.
Schwannomas in the cerebellopontine angle arise in most cases from
Schwannomas involve the internal auditory canal in
cranial nerve 8 (the vestibular division is more common than cochlear approximately 80% of cases, compared with meningiomas
nerve). The next most common nerves of origin are cranial nerve 5 where involvement of the internal auditory canal is
(trigeminal) followed by cranial nerve 7 (facial). Several imaging unusual, seen in approximately 5% of cases.
findings may help to distinguish a schwannoma from a meningioma in
the cerebellopontine angle. Schwannomas involve the internal Schwannomas make an acute angle with the petrous bone,
auditory canal in approximately 80% of cases, compared with compared with meningiomas, which make obtuse angles
owing to their dural origin.
meningiomas where involvement of the internal auditory canal is
unusual, seen in approximately 5% of cases. Schwannomas make an
Because schwannomas extend into the internal auditory
acute angle with the petrous bone, compared with meningiomas, canal, when large enough, there may be flaring or
which make obtuse angles owing to their dural origin. Because expansion of the porus acousticus (the opening of the
schwannomas extend into the internal auditory canal, when large internal auditory canal) as well as the canal itself.
enough, there may be flaring or expansion of the porus acousticus (the
opening of the internal auditory canal) as well as the canal itself. With With schwannomas, there is frequently obscuration of the
schwannomas, there is frequently obscuration of the seventh and seventh and eighth nerves, compared with meningiomas in
which these nerves often can be seen separate from the
eighth nerves, compared with meningiomas in which these nerves tumor on imaging. 5
often can be seen separate from the tumor on imaging. 2 In addition,
in approximately 10% of cases, schwannomas may be associated with In 10% of cases, schwannomas may be associated with a
a coexistent arachnoid cyst. Finally, although schwannomas usually coexistent arachnoid cyst.
are centered geographically at the internal auditory canal,
meningiomas frequently are centered anterior or posterior and Although schwannomas usually are centered
superior or inferior to it. geographically at the internal auditory canal, meningiomas
frequently are centered anterior or posterior and superior or
inferior to it.
Metastases involving the cerebellopontine angle are typically dural
based, en plaque lesions, caused by hematogenous spread, subarachnoid seeding along the cranial nerves, or extension
from an adjacent bone lesion.
Common metastases to affect the cerebellopontine angle include breast, lung, and prostate carcinoma, as well as
lymphoma. In the pediatric population, leukemia and neuroblastoma should be considered.
Figure 18. Bilateral vestibular schwannoma with intense contrast
enhancement.
11. Figure 19. A,B Left cerebellopontine angle schwannoma in a middle-aged man. A, Axial T2-weighted MR image
obtained at the level of the internal auditory canals. There is a heterogeneous, predominantly hypointense mass within
the left cerebellopontine angle. Central high signal intensity is consistent with necrosis. Note the CSF cleft (black
arrows) separating this extra-axial mass from the adjacent brainstem and cerebellum. There is widening of the
internal auditory canal (white arrowheads). B, Axial enhanced Tl -weighted MR image demonstrates heterogeneous
enhancement of the mass. Enhancement extends into the opening of the internal auditory canal. In addition, there are
small enhancing dural tails (arrows). C, Cerebellopontine cistern epidermoid cyst. Axial unenhanced T1 -weighted
image shows the mass conforming to the shape of the cerebellopontine cistern. The basilar artery is encased (white
arrow), and the posterior margin of the cyst is scalloped (black arrows).
Figure 20. A, small acoustic neuroma within the internal
auditory canal is easily seen on postgadolinium MRI. B,
MRI T2 image showing bilateral vestibular Antoni B
tissue schwannoma, the tumours are hyperintense.
12. Figure 21. Precontrast MRI T1 (A) and postcontrast MRI T1 (B) images showing a case with type II
neurofibromatosis (bilateral acoustic schwannomas). The tumours are hypointense on the precontrast MRI T1 image
(A) with intense and uniform postcontrast enhancement (B). Notice the clear CSF cleft that separated the tumours
from the brain stem, indicating the extraaxial nature of the tumours that are seen compressing the brain stem
bilaterally. C, The tumours were surgically removed with the histopathological diagnosis of Antoni B schwannomas.
Imaging of neurofibromas
Benign nerve sheath tumors are isointense to slightly hyperintense to muscle in TI-weighted pulse sequences. These
tumors show variable hyperintensity in T2-weighted images; Varma et al 4 have demonstrated a target sign (a
peripheral hyperintense rim and a central low intensity) in T2-weighted sequences. This target pattern is attributed to
peripheral myxomatous tissue and central fibrocollagenous tissue. This pattern was absent in lesions with cystic,
hemorrhagic, or necrotic degeneration.
13. Figure 22. Neurofibroma. These peripheral nerve tumors resemble Schwannomas and are differentiated from the
latter by histological criteria that are not always distinct. As a rule, however, neurofibromas are less cellular, lack
striking palisading, are more loosely packed than Schwannomas, and may have a much more striking collagenous
component (red bundles).
A target sign was not seen in malignant lesions. A mass with a target appearance if seen by MR imaging is a useful
sign in diagnosis of benign nerve sheath tumors. This sign is seen in both neurofibromas and schwannomas. Neither
CT nor MR imaging can always accurately differentiate benign from malignant nerve sheath tumors. If masses are
seen with irregular contour and disruption of soft tissue planes, however, findings favor malignant neoplasm.
Figure 23. MRI picture of the target sign
Spinal schwannoma & neurofibromas
Schwannomas and neurofibromas typically involve the dorsal sensory nerve roots. Depending upon their site of origin,
they can be intradural, extradural, or both, forming a quot;dumbbellquot; or hour-glass shaped mass. Rarely, schwannomas
may extend into the substance of the spinal cord and be entirely intramedullary in location. Plain radiographs may
show an enlarged neural foramen or spinal canal. There may be associated findings of neurofibromatosis (scoliosis,
vertebral dysplasia). CT-myelography will show the bony changes if present and an intradural, extramedullary mass
with rounded, well-defined margins. Schwannomas appear iso- to hypointense relative to spinal cord on TI-weighted
images and hyperintense on T2-weighted images (cystic Antoni B schwannoma). Areas of even greater signal
hyperintensity on T2-weighted images may represent cyst formation; conversely, areas of relatively decreased signal
intensity on T2-weighted images may relate to intratumoral hemorrhage, dense cellularity, or collagen deposition. The
tendency for cyst formation is greater in spinal tumors than in intracranial lesions.
In contrast, neurofibroma is a solid tumor; cystic areas are uncommon. They have more uniform signal intensity on
MR images, in keeping with their more uniform histologic appearance on the T2-weighted images, a target
appearance may be seen with relatively greater signal intensity peripherally, corresponding to peripheral myxomatous
tissue and central fibrocollagenous tissue seen histologically. Contrast- enhanced MR imaging may show a central
area of decreased signal intensity surrounded by enhancing tumor in either neurofibroma or schwannoma.
14. Figure 24. MRI T2 images showing a dumb-bell neurofibroma notice the T2 hypointensity (B) which could be due to
intralesional haemorrhage, , dense cellularity, or collagen deposition
These tumors show variable hyperintensity in T2-weighted images;the target sign is occasionally demonstrated (a
peripheral hyperintense rim and a central low intensity) in T2-weighted sequences This target pattern is attributed to
peripheral myxomatous tissue and central fibrocollagenous tissue. This pattern is absent in lesions with cystic,
hemorrhagic, or necrotic degeneration.
Figure 25. MRI T2 images showing the target sign,with central
hypointensity corresponding to the fibrocollagenous core and a
peripheral hyperintensity corresponding to the peripheral myxomatous
tissue
Plexiform neurofibroma is a distinct lesion that is characteristic of NFl. Although these are infiltrative lesions that
occur most commonly near the orbital apex or superior orbital fissure, they can occur anywhere in the body. On MR
imaging, the lesions appear hypointense relative to cord on TI-weighted images and hyperintense on T2-weighted
images with variable contrast enhancement.
SUMMARY
SUMMARY
Central neurofibromatosis or NF type 2 is a multisystem genetic disorder associated with bilateral vestibular
schwannomas, spinal cord schwannomas, meningiomas, gliomas, and juvenile cataracts with a paucity of cutaneous
features, which are seen more consistently in NF1. Although quite variable in its age of onset and severity of symptoms
in affected individuals, NF2 is associated with significant morbidity and decreased lifespan. Furthermore, diagnosis in
childhood is often difficult because of the absence of central nervous system involvement at a young age.
Table 1. Genetics of neurofibromatosis
Type Gene product Gene location Gene function
15. Type I neurofibromatosis Neurofibromin Long arm of chromosome 17 Putative tumor suppressor
Type II neurofibromatosis Merlin Long arm of chromosome 22 function
Addendum
A new version of this PDF file (with a new case) is uploaded in my web site every week (every Saturday and
remains available till Friday.)
To download the current version follow the link quot;http://pdf.yassermetwally.com/case.pdfquot;.
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To download the software version of the publication (crow.exe) follow the link:
http://neurology.yassermetwally.com/crow.zip
The case is also presented as a short case in PDF format, to download the short case follow the link:
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At the end of each year, all the publications are compiled on a single CD-ROM, please contact the author to
know more details.
Screen resolution is better set at 1024*768 pixel screen area for optimum display.
For an archive of the previously reported cases go to www.yassermetwally.net, then under pages in the right
panel, scroll down and click on the text entry quot;downloadable case records in PDF formatquot;
REFERENCES
References
1. Spagnoli MV, Goldberg HI, Grossman RI, et al: Intracranial meningiomas: High-field MR imaging. Radiology
161:369-375,1986
2. Press GA, Hesselink JR: MR imaging of cerebellopontine angle and internal auditory canal lesions at 1.5T. AJNR
Am j Neuroradiol 9:241-251,1988
3. Nguyen HD, Simonson TM, Fisher DJ, et al: MR evaluation of acoustic schwannoma with fractional contrast doses.
J Comput Assist Tomogr 19:23-27, 1995
4. Varma DGK, Moulopoulos A, Sara AS, et al: MR imaging of extracranial nerve sheath tumors. j Comput Assist
Tomogr 16:448, 1992
5. Metwally, MYM: Textbook of neuroimaging, A CD-ROM publication, (Metwally, MYM editor) WEB-CD agency
for electronic publication, version 9.2a April 2008