Neuro-oncology

Neuro-oncology
Focus	Cancerous brain tumors
Significant tests	Tumor markers, TNM staging, CT scans, MRI
Specialist	Neurooncologist

Last updated August 18, 2023

Neuro-oncology is the study of brain and spinal cord neoplasms, many of which are (at least eventually) very dangerous and life-threatening (astrocytoma, glioma, glioblastoma multiforme, ependymoma, pontine glioma, and brain stem tumors are among the many examples of these). Among the malignant brain cancers, gliomas of the brainstem and pons, glioblastoma multiforme, and high-grade (highly anaplastic) astrocytoma/oligodendroglioma are among the worst.^[1] In these cases, untreated survival usually amounts to only a few months, and survival with current radiation and chemotherapy treatments may extend that time from around a year to a year and a half, possibly two or more, depending on the patient's condition, immune function, treatments used, and the specific type of malignant brain neoplasm. Surgery may in some cases be curative, but, as a general rule, malignant brain cancers tend to regenerate and emerge from remission easily, especially highly malignant cases. In such cases, the goal is to excise as much of the mass (tumor cells) and as much of the tumor margin as possible without endangering vital functions or other important cognitive abilities. The Journal of Neuro-Oncology is the longest continuously published journal in the field and serves as a leading reference to those practicing in the area of neuro-oncology.

General information
Primary tumors of the central nervous system
Metastatic tumors of the central nervous system
Mechanisms
Tumor factors
Initial patient evaluation and care
Diagnostic procedures
Diagnostic imaging of the brain and spinal cord
Lumbar puncture and cerebrospinal fluid analysis
Pathologic diagnosis
Commonly used treatments
References
External links

General information

Primary tumors of the central nervous system

Primary brain tumors can occur at any age, from infancy to late in life. These tumors often afflict people during their prime years. Factors such as age, tumor location, and clinical presentation are helpful in differential diagnosis. Most types of primary brain tumors are more common in men with the exception of meningiomas, which are more common in women.^[2]

Metastatic tumors of the central nervous system

Cancer spreads to the nervous system by direct invasion, compression, or metastasis. Direct invasion or compression from continuous tissues relates to the proximity of the nervous system to other structures, such as the brachial plexus, lumbosacral plexus, vertebral neuroforamina, base of skull, cranium, and pelvic bones.^[2]

Intracranial metastasis

There are three types of intracranial metastasis: brain metastasis, dural metastasis, and leptomeningeal metastasis. Brain metastasis can be single or multiple and involve any portion of the brain. Metastasis to dural structures generally occurs by hematogenous spread or direct invasion from a contiguous bone. Dural metastases can invade the underlying brain and cause focal edema and associated neurologic symptoms. These processes tend to cause seizures early in the course because of their cortical location. Metastasis to the leptomeninges is an uncommon but well-recognized clinical presentation in cancer patients. Leptomeningeal metastasis most commonly is due to breast, lung, or melanoma primary tumors.^[2]

Skull metastasis

Metastases to the skull are divided into two categories by general site: calvarium and skull base. Metastases to the calvarium usually are asymptomatic. Metastases to the skull base quickly become symptomatic because of their proximity to cranial nerves and vascular structures.^[2]

Spinal metastasis

The spine most often is affected by metastatic disease involving the epidural space. This usually occurs as direct tumor spread from a vertebral body (85%) or by invasion of paravertebral masses through a neuroforamin (10–15%).^[2]

Mechanisms

Tumor factors

Histology

Seizures are common in patients with low-grade tumors such as dysembryoblastic neuroepithelial tumors, gangligliomas, and oligodendrogliomas. The rapid growth of fast-growing high-grade brain tumors may damage the subcortical network essential for electrical transmission, whereas slow-growing tumors have been suggested to induce partial deafferentation of cortical regions, causing denervation hypersensitivity and producing an epileptogenic milieu. Studies strongly suggest that genetic factors may play a role in tumor development and tumor-related epilepsy.^[3]^[4]

Glutamate neurotransmission

Recent work has demonstrated a close link between seizure activity and high extracellular glutamate in tumor-related epilepsy. Glutamate activation of ionotropic receptors leads to a rapid excitatory signal based on cation influx that can cause release of calcium from intracellular stores.^[2]

Initial patient evaluation and care

1. Brain Tumor Presentations

In general, patients with primary brain tumors or single metastatic tumors can present with any of these signs and symptoms, whereas patients with multiple brain metastases tend to present with generalized symptoms and may lack localized findings.^[5]

Several clinical features warrant special comment:

Seizures (partial or generalized) are the presenting symptom in 15-20% of patients with intracranial tumors. Seizures occur in up to 50% of patients with melanoma metastases, oligodendrogliomas, and tumors that have a hemorrhagic component. Seizures also are more common with cortically based tumors.^[5]
Seizures are much less common in patients with infratentorial tumors than in those with supratentorial tumors.^[5]
"Stroke-like" onset of symptoms is due to hemorrhage within the tumor or, less commonly, macroscopic tumor embolus from systemic cancer.^[5]
Although intratumoral hemorrhage can occur in any primary or metastatic brain tumor, certain tumors have a greater tendency to bleed, including metastasis from melanoma, choriocarcinoma, and thyroid cancer and the primary brain tumors glioblastoma and oligodendroglioma.^[5]

2. Spinal Cord Tumor Presentations

Pain is the first symptom in >90% of patients presenting with epidural metastasis and occurs less frequently with intradural tumors.^[6]
Mechanisms of pain include spinal cord ischemia and traction on the periosteum, dura, nearby soft tissues, and nerve roots.^[6]
Pain occasionally can be absent in adults and more often is absent in childhood. If other neurologic symptoms suggestive of myelopathy are present, without pain, the clinician should evaluate for spinal cord tumor.^[6]
Changes in bowel and bladder habits, particularly urinary retention with overflow incontinence, usually occur late in the course of epidural spinal cord compression but are seen in a small percentage of patients at presentation.^[6]

3. Approach to the Evaluation of New Patients

The initial evaluation of a patient with a newly diagnosed tumor of the nervous system is a critical step toward appropriate management and patient care. The most important portions of the initial evaluation are a detailed history and a thorough examination. This process serves to identify the extent and nature of neurological deficit, provides diagnostic clues, can help disclose a source of metastasis, or may identify a genetic process associated with a primary central nervous system tumor.^[5]

4. Practical Strategies for Providing Appropriate Patient Care

There is no question that the clinical management of neurooncology patients is challenging. However, if we are to help patients and ultimately make advances in treating these tumors, meticulous and compassionate care of patients with neurological malignancies are crucial.^[5]

Give instructions both orally and in written form for the patient to take home.^[5]
Use a consistent format of written instructions, so that a patient can expect where to find information on the page.^[5]
Write down new or important diagnoses for the patient to refer to at home.^[5]
Identify one reliable caregiver to serve as a contact point.^[5]
Pictures and diagrams are helpful.^[5]
A team approach, using clinicians with different areas of expertise, is helpful.^[5]
Provide a reliable and simple method for the patient to seek help.^[5]
Minimize sedating drug use.^[5]

Diagnostic procedures

Diagnostic imaging of the brain and spinal cord

The imaging studies commonly used in neurooncology are computed tomography (CT) and magnetic resonance imaging (MRI). Less commonly used are myelography, positron emission tomography (PET), and diagnostic angiography.^[7]^[8]

Lumbar puncture and cerebrospinal fluid analysis

Lumbar puncture (LP) and cerebrospinal fluid (CSF) analysis are important for the evaluation of some primary tumors, metastatic conditions, and neurologic complications of cancer.^[7]

Pathologic diagnosis

Accurate histologic diagnosis is critical for treatment planning and patient counseling. Surgically obtained tissue usually is required to make a histologic diagnosis. For certain tumors, a definitive diagnosis can be accomplished by vitreous aspirate, cerebrospinal fluid (CSF) cytology, or suggested by the presence of certain tumor markers in the CSF.^[7]

Commonly used treatments

Radiotherapy
Radiotherapy is an important treatment for central nervous system tumors and has been demonstrated to extend survival and improve the quality of life for patients with many of the primary and metastatic brain tumors.^[7]
Chemotherapy
Chemotherapy, or the use of drugs in the treatment of cancer, can lead to the long-term control of many malignancies. Some tumors, such as testicular cancer of Hodgkin's disease, may be cured even when they are widespread. As chemotherapy may be associated with severe toxicity, it should be given under the supervision of one skilled in the administration and monitoring of such agents.^[7]
Corticosteroids
Corticosteroids (CS) are commonly used in patients with a variety of neuro-oncologic conditions. CS treatment often is required to control symptoms related to increased intracranial pressure (ICP) or peritumoral edema.^[9]
Neurosurgical interventions
Neurosurgical intervention is warranted in almost all cases of primary central nervous system tumors and for many metastatic tumors. A biopsy usually establishes a definitive histologic diagnosis. The role of surgery depends on the nature of the tumor. With modern neurosurgical techniques, most patients with extra-axial brain tumors are cured with minimal residual neurologic deficit.^[9]

Related Research Articles

A brain tumor occurs when abnormal cells form within the brain. There are two main types of tumors: malignant tumors and benign (non-cancerous) tumors. These can be further classified as primary tumors, which start within the brain, and secondary tumors, which most commonly have spread from tumors located outside the brain, known as brain metastasis tumors. All types of brain tumors may produce symptoms that vary depending on the size of the tumor and the part of the brain that is involved. Where symptoms exist, they may include headaches, seizures, problems with vision, vomiting and mental changes. Other symptoms may include difficulty walking, speaking, with sensations, or unconsciousness.

Metastasis is a pathogenic agent's spread from an initial or primary site to a different or secondary site within the host's body; the term is typically used when referring to metastasis by a cancerous tumor. The newly pathological sites, then, are metastases (mets). It is generally distinguished from cancer invasion, which is the direct extension and penetration by cancer cells into neighboring tissues.

<span class="mw-page-title-main">Glioma</span> Tumour of the glial cells of the brain or spine

A glioma is a type of tumor that starts in the glial cells of the brain or the spine. Gliomas comprise about 30 percent of all brain tumors and central nervous system tumours, and 80 percent of all malignant brain tumours.

Spinal tumors are neoplasms located in either the vertebral column or the spinal cord. There are three main types of spinal tumors classified based on their location: extradural and intradural. Extradural tumors are located outside the dura mater lining and are most commonly metastatic. Intradural tumors are located inside the dura mater lining and are further subdivided into intramedullary and extramedullary tumors. Intradural-intramedullary tumors are located within the dura and spinal cord parenchyma, while intradural-extramedullary tumors are located within the dura but outside the spinal cord parenchyma. The most common presenting symptom of spinal tumors is nocturnal back pain. Other common symptoms include muscle weakness, sensory loss, and difficulty walking. Loss of bowel and bladder control may occur during the later stages of the disease.

Oligodendrogliomas are a type of glioma that are believed to originate from the oligodendrocytes of the brain or from a glial precursor cell. They occur primarily in adults but are also found in children.

An ependymoma is a tumor that arises from the ependyma, a tissue of the central nervous system. Usually, in pediatric cases the location is intracranial, while in adults it is spinal. The common location of intracranial ependymomas is the fourth ventricle. Rarely, ependymomas can occur in the pelvic cavity.

Meningioma, also known as meningeal tumor, is typically a slow-growing tumor that forms from the meninges, the membranous layers surrounding the brain and spinal cord. Symptoms depend on the location and occur as a result of the tumor pressing on nearby tissue. Many cases never produce symptoms. Occasionally seizures, dementia, trouble talking, vision problems, one sided weakness, or loss of bladder control may occur.

Glioblastoma, previously known as glioblastoma multiforme (GBM), is the most aggressive and most common type of cancer that originates in the brain, and has very poor prognosis for survival. Initial signs and symptoms of glioblastoma are nonspecific. They may include headaches, personality changes, nausea, and symptoms similar to those of a stroke. Symptoms often worsen rapidly and may progress to unconsciousness.

<span class="mw-page-title-main">Oligoastrocytoma</span> Medical condition

Oligoastrocytomas are a subset of brain tumors that present with an appearance of mixed glial cell origin, astrocytoma and oligodendroglioma. However, the term "Oligoastrocytoma" is now considered obsolete by the National Comprehensive Cancer Network stating "the term should no longer be used as such morphologically ambiguous tumors can be reliably resolved into astrocytomas and oligodendrogliomas with molecular testing."

Pilocytic astrocytoma is a brain tumor that occurs most commonly in children and young adults. They usually arise in the cerebellum, near the brainstem, in the hypothalamic region, or the optic chiasm, but they may occur in any area where astrocytes are present, including the cerebral hemispheres and the spinal cord. These tumors are usually slow growing and benign, corresponding to WHO malignancy grade 1.

Spinal cord compression is a form of myelopathy in which the spinal cord is compressed. Causes can be bone fragments from a vertebral fracture, a tumor, abscess, ruptured intervertebral disc or other lesion.

Gliosarcoma is a rare type of glioma, a cancer of the brain that comes from glial, or supportive, brain cells, as opposed to the neural brain cells. Gliosarcoma is a malignant cancer, and is defined as a glioblastoma consisting of gliomatous and sarcomatous components. Primary gliosarcoma (PGS) is classified as a grade IV tumor and a subtype of glioblastoma multiforme in the 2007 World Health Organization classification system (GBM). Because of a lack of specific and clear diagnostic criteria, the word "gliosarcoma" was frequently used to refer to glial tumours with mesenchymal properties, such as the ability to make collagen and reticulin.

Leptomeningeal cancer is a rare complication of cancer in which the disease spreads from the original tumor site to the meninges surrounding the brain and spinal cord. This leads to an inflammatory response, hence the alternative names neoplastic meningitis (NM), malignant meningitis, or carcinomatous meningitis. The term leptomeningeal describes the thin meninges, the arachnoid and the pia mater, between which the cerebrospinal fluid is located. The disorder was originally reported by Eberth in 1870.

Bone metastasis, or osseous metastatic disease, is a category of cancer metastases that results from primary tumor invasion to bone. Bone-originating primary tumors such as osteosarcoma, chondrosarcoma, and Ewing sarcoma are rare; the most common bone tumor is a metastasis. Bone metastases can be classified as osteolytic, osteoblastic, or both. Unlike hematologic malignancies which originate in the blood and form non-solid tumors, bone metastases generally arise from epithelial tumors and form a solid mass inside the bone. Bone metastases, especially in a state of advanced disease, can cause severe pain, characterized by a dull, constant ache with periodic spikes of incident pain.

Metastatic breast cancer, also referred to as metastases, advanced breast cancer, secondary tumors, secondaries or stage IV breast cancer, is a stage of breast cancer where the breast cancer cells have spread to distant sites beyond the axillary lymph nodes. There is no cure for metastatic breast cancer; there is no stage after IV.

A brain metastasis is a cancer that has metastasized (spread) to the brain from another location in the body and is therefore considered a secondary brain tumor. The metastasis typically shares a cancer cell type with the original site of the cancer. Metastasis is the most common cause of brain cancer, as primary tumors that originate in the brain are less common. The most common sites of primary cancer which metastasize to the brain are lung, breast, colon, kidney, and skin cancer. Brain metastases can occur in patients months or even years after their original cancer is treated. Brain metastases have a poor prognosis for cure, but modern treatments are allowing patients to live months and sometimes years after the diagnosis.

Isabelle M. Germano is a neurosurgeon and professor of neurosurgery, neurology, and oncology at the Icahn School of Medicine at Mount Sinai Hospital. She is a Fellow of the American College of Surgeons and the American Association of Neurological Surgeons. Germano works with image-guided brain and spine surgery.

A central nervous system tumor is an abnormal growth of cells from the tissues of the brain or spinal cord. CNS tumor is a generic term encompassing over 120 distinct tumor types. Common symptoms of CNS tumors include vomiting, headache, changes in vision, nausea, and seizures. A CNS tumor can be detected and classified via neurological examination, medical imaging, such as x-ray imaging, magnetic resonance imaging (MRI) or computed tomography (CT), or after analysis of a biopsy.

<span class="mw-page-title-main">Anaplastic oligodendroglioma</span> Human brain tumor

Anaplastic oligodendroglioma is a neuroepithelial tumor which is believed to originate from oligodendrocytes, a cell type of the glia. In the World Health Organization (WHO) classification of brain tumors, anaplastic oligodendrogliomas are classified as grade III. In the course of the disease, they can degenerate into highly malignant oligodendroglioma, grade IV. The vast majority of oligodendrogliomas occur sporadically, without a confirmed cause and without inheritance within a family.

CNS metastasis is the spread and proliferation of cancer cells from their original tumour to form secondary tumours in portions of the central nervous system.

References

↑ Levin, VA (April 1999). "Neuro-oncology: an overview". Archives of Neurology. 56 (4): 401–4. doi:10.1001/archneur.56.4.401. PMID 10199326.
1 2 3 4 5 6 McAllister, L.D., Ward, J.H., Schulman, S.F., DeAngels, L.M. (2002). Practical Neuro-Oncology: A Guide to Patient Care. Woburn, MA: Butterworth-Heinemann.
↑ Smits, A. (2011). Seizures and the natural history of World Health Organization grade II gliomas: a review. Neurosurgery (2011): 1326-1333.
↑ Read, Tracy-Ann; Hegedus, Balazs; Wechsler-Reya, Robert; Gutmann, David H. (July 2006). "The neurobiology of neurooncology". Annals of Neurology. 60 (1): 3–11. doi:10.1002/ana.20912. PMID 16802285. S2CID 870084.
1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 Liu, James K.; Patel, Smruti K.; Podolski, Amanda J.; Jyung, Robert W. (September 2012). "Fascial sling technique for dural reconstruction after translabyrinthine resection of acoustic neuroma: technical note". Neurosurgical Focus. 33 (3): E17. doi: 10.3171/2012.6.FOCUS12168 . PMID 22937851.
1 2 3 4 Muller, H. L., Gebhardt, U., Warmuth-Metz, M., Pietsch, T., Sorensen, N., & Kortmann, R. D. (2012). Meningioma assecond malignant neoplasm after oncological treatment during childhood. 188, 438-441. Retrieved from ^[dead link ]
1 2 3 4 5 Ansari, Shaheryar F.; Terry, Colin; Cohen-Gadol, Aaron A. (September 2012). "Surgery for vestibular schwannomas: a systematic review of complications by approach". Neurosurgical Focus. 33 (3): E14. doi: 10.3171/2012.6.FOCUS12163 . PMID 22937848. S2CID 46630604.
↑ Cha, Soonmee (July 2009). "Neuroimaging in neuro-oncology". Neurotherapeutics. 6 (3): 465–477. doi:10.1016/j.nurt.2009.05.002. PMC 5084183 . PMID 19560737.
1 2 Duffau, H. (2012). The challenge to remove diffuse low-grade gliomas while preserving brain functions. 10(7), 569-574. ^{[ dead link ]}

External links

www.bnos.org.uk – British Neuro-Oncology Society (BNOS)
www.cochrane.org – Trusted evidence. Informed decisions. Better health.
www.soc-neuro-onc.org – Society for Neuro-Oncology

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[pmid10199326-1] Levin, VA (April 1999). "Neuro-oncology: an overview". Archives of Neurology. 56 (4): 401–4. doi:10.1001/archneur.56.4.401. PMID 10199326.

[practical-2] 1 2 3 4 5 6 McAllister, L.D., Ward, J.H., Schulman, S.F., DeAngels, L.M. (2002). Practical Neuro-Oncology: A Guide to Patient Care. Woburn, MA: Butterworth-Heinemann.

[3] Smits, A. (2011). Seizures and the natural history of World Health Organization grade II gliomas: a review. Neurosurgery (2011): 1326-1333.

[pmid16802285-4] Read, Tracy-Ann; Hegedus, Balazs; Wechsler-Reya, Robert; Gutmann, David H. (July 2006). "The neurobiology of neurooncology". Annals of Neurology. 60 (1): 3–11. doi:10.1002/ana.20912. PMID 16802285. S2CID 870084.

[seizures-5] 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 Liu, James K.; Patel, Smruti K.; Podolski, Amanda J.; Jyung, Robert W. (September 2012). "Fascial sling technique for dural reconstruction after translabyrinthine resection of acoustic neuroma: technical note". Neurosurgical Focus. 33 (3): E17. doi: 10.3171/2012.6.FOCUS12168 . PMID 22937851.

[muller-6] 1 2 3 4 Muller, H. L., Gebhardt, U., Warmuth-Metz, M., Pietsch, T., Sorensen, N., & Kortmann, R. D. (2012). Meningioma assecond malignant neoplasm after oncological treatment during childhood. 188, 438-441. Retrieved from ^[dead link ]

[Ansari-7] 1 2 3 4 5 Ansari, Shaheryar F.; Terry, Colin; Cohen-Gadol, Aaron A. (September 2012). "Surgery for vestibular schwannomas: a systematic review of complications by approach". Neurosurgical Focus. 33 (3): E14. doi: 10.3171/2012.6.FOCUS12163 . PMID 22937848. S2CID 46630604.

[pmid19560737-8] Cha, Soonmee (July 2009). "Neuroimaging in neuro-oncology". Neurotherapeutics. 6 (3): 465–477. doi:10.1016/j.nurt.2009.05.002. PMC 5084183 . PMID 19560737.

[brain-9] 1 2 Duffau, H. (2012). The challenge to remove diffuse low-grade gliomas while preserving brain functions. 10(7), 569-574. ^{[ dead link ]}

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Category Commons

Focus	Cancerous brain tumors
Significant tests	Tumor markers, TNM staging, CT scans, MRI
Specialist	Neurooncologist