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Brain Tumors Classification and Biology of Brain Tumors M.R.Ehsaei M.D M.R.Ehsaei M.D Department of Department of Neurosurgery of MUMS Neurosurgery of MUMS
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Brain Tumors Classification and Biology of Brain Tumors M.R.Ehsaei M.D Department of Neurosurgery of MUMS.

Dec 15, 2015

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Page 1: Brain Tumors Classification and Biology of Brain Tumors M.R.Ehsaei M.D Department of Neurosurgery of MUMS.

Brain Tumors

Classification and Biology of Brain Tumors

M.R.Ehsaei M.DM.R.Ehsaei M.D

Department of Neurosurgery of Department of Neurosurgery of MUMSMUMS

Page 2: Brain Tumors Classification and Biology of Brain Tumors M.R.Ehsaei M.D Department of Neurosurgery of MUMS.

Methods for Tissue Sampling and Study

Open BiopsyNeedle BiopsyFrozen SectionImmunohistochemistryElectron MicroscopyCytologyCytogenetic and Molecular Biological StudiesQuantitation of Cell Proliferation

Page 3: Brain Tumors Classification and Biology of Brain Tumors M.R.Ehsaei M.D Department of Neurosurgery of MUMS.

Open Biopsy. For lesions that are favorably situated, open

cerebral resection can provide a true total resection of the tumor

for which classification and grading are of academic interest.

Page 4: Brain Tumors Classification and Biology of Brain Tumors M.R.Ehsaei M.D Department of Neurosurgery of MUMS.

Needle Biopsy. The size of such specimens ranges from small

fragments or only scattered cells when a thin needle is used to more substantial tissue fragments when a

large, hollow core needle with a cutting side port is employed.

Page 5: Brain Tumors Classification and Biology of Brain Tumors M.R.Ehsaei M.D Department of Neurosurgery of MUMS.

Frozen Section. Frozen sections of open or needle biopsy

specimens provide a means to ensure that adequate material is

obtained or to establish a specific histological diagnosis.

Page 6: Brain Tumors Classification and Biology of Brain Tumors M.R.Ehsaei M.D Department of Neurosurgery of MUMS.

Immunohistochemistry. As it has for pathological diagnoses for other organ systems, immunohistochemistry has

had a major impact on operative pathology of the nervous system. This

technique is employed to recognize antigens on or within neoplastic cells

by immunofluorescence or, more commonly, by the immunoperoxidase

method, which can be used on paraffin-embedded material.

Page 7: Brain Tumors Classification and Biology of Brain Tumors M.R.Ehsaei M.D Department of Neurosurgery of MUMS.

S-100 is a soluble protein found within the cytoplasm and nuclei

of cells of the central and peripheral nervous system. It is expressed strongly in Schwann

cells and is useful in establishing this cellular origin

for acoustic and spinal schwannomas.

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The strong S-100 staining of melanocytes is also helpful in

identifying amelanotic metastatic malignant melanomas. Other

applications of immunohistochemistry include the characterization of germ cell neoplasms in the pineal region,

characterization of the hormones produced by pituitary adenomas, and differentiation in medulloblastomas

Page 9: Brain Tumors Classification and Biology of Brain Tumors M.R.Ehsaei M.D Department of Neurosurgery of MUMS.

Cytogenetic and Molecular Biological Studies. There is increasing interest in

the chromosomal abnormalities of human neoplasms because of the possibility that such changes are

related etiologically to the neoplasms by means of certain oncogenes and

tumor suppressor genes.

Page 10: Brain Tumors Classification and Biology of Brain Tumors M.R.Ehsaei M.D Department of Neurosurgery of MUMS.

Quantitation of Cell Proliferation. The estimate of a neoplasm's proliferative potential is done inferentially by study

of the cytological characteristics of the cells or more directly by

determination of a mitotic index. A monoclonal antibody, MIB-1,

recognizes the same antigen as Ki-67 but retains strong reactivity in paraffin

sections (Fig. 113-1).

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Clinicopathological Entities

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FIBROUS DYSPLASIA

Fibrous dysplasia is a disorder of unknown etiology that usually is

manifested as an enlargement of the bones in and about the orbit.

Occasionally, more discrete lesions appear as isolated osteolytic areas in

the cranial vault. The natural history of fibrous dysplasia has not been studied

in detail; many lesions stabilize in adolescence.

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CHORDOMAThe chordoma is a destructive neoplasm generally arising at either end of the axial

skeleton, in the clivus or the sacrum. Evidence indicates that the lesion originates from notochordal nests, which are frequently

observed in the clivus, although it is not clear why these neoplasms are not more common along the thoracic and lumbar spine, where

these same nests are frequently encountered in the center of the intervertebral discs.

Chordomas in the clivus are often situated somewhat off the midline and can produce

unilateral cranial nerve deficits.

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LANGERHANS CELL HISTIOCYTOSIS

Langerhans cell histiocytosis is a uni- or multifocal disorder of bone or soft tissue, or

both, that most often comes to neurosurgical attention as a lytic lesion of

the skull. The common solitary lesion of the skull is known as an eosinophilic granuloma, and the multiple lesions of the skull that are often associated with diabetes insipidus are

part of the Hand-Schüller-Christian syndrome (Fig. 113-2). Extensive

involvement of soft tissue characterizes the historical but ill-defined entity of Letterer-

Siwe disease.

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The common solitary lesion of bone is a benign condition responding to

radiation therapy. The multifocal lesions of the base of the skull are in

many cases also cured by irradiation, although they may be

associated with variable morbidity.

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Histologically, the lesions are distinctive because of the mixture of

histiocytes (Langerhans cells), lymphocytes, and eosinophils (Fig.

113-3). In some cases, the histiocytes are engorged with fat, and the lesions

are macroscopically yellow. The Langerhans cells have markedly

convoluted nuclei and, by electron microscopy, contain the distinctive

Birbeck granule diagnostic of this cell type (Fig. 113-4).

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CRANIOPHARYNGIOMA

The craniopharyngioma is a radiographically discrete,

calcified, often cystic neoplasm that is seen most frequently in

childhood. A noncalcified lesion with a slightly different

histological pattern is usually seen in adults

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Microscopically, cells anastomose in ribbons to produce the adamantinomatous pattern (Fig. 113-5). Keratinized nodules, seen as

white flecks with the naked eye or operating microscope, are also typical. During

resection, pieces of the floor of the third ventricle can be avulsed, and microscopic

study often reveals infiltration of the neoplastic cells. It is not surprising that total excision is difficult and that late recurrences

can occur. The recurrent lesion is more widely adherent to local structures and is

difficult or impossible to remove.

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The histological pattern of the craniopharyngioma seen most frequently in adults has been

termed a "papillary craniopharyngioma" or

"suprasellar squamous papillary epithelioma" (Fig. 113-6)

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MENINGIOMA

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