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'''Original Editor '''- [[User:George Prudden|George Prudden]]  
'''Original Editor '''- [[User:George Prudden|George Prudden]]
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== Definition ==
'''Top Contributors''' -  {{Special:Contributors/{{FULLPAGENAME}}}}</div>  
Ependymomas are tumors of the central nervous system (CNS), which means that they originate in either the brain or spine. Tumors of glial cells are the most common and are known as gliomas. They effect both adults and children but are most common in children, Tumors are classified by the World Health Organization (WHO) Classification of Tumors of the Nervous System as grades I, II, and III based on their grade of anaplasia (cell disorganisation)<ref name=":0">Cern-foundation.org. (2017). ''Ependymoma Basics | CERN Foundation''. [online] Available at: <nowiki>http://www.cern-foundation.org/education/ependymoma-basics</nowiki> [Accessed 24 Aug. 2017].
</ref>


== Clinically Relevant Anatomy ==
==Introduction==
[[File:Ependymoma3.jpg|thumb|Anaplastic ependymoma in an adult patient]]
Ependymomas represent a broad group of [[Glial Cells|glial]] tumours most often arising from the lining of the ventricles of the [[Brain Anatomy|brain]] or the central canal of the [[Spinal cord anatomy|spinal cord]]. They account for ~5% of all neuroepithelial neoplasms, ~10% of all paediatric brain tumours and up to 33% of brain tumours occurring in those less than 3 years of age<ref name=":6">Radiopedia Ependymoma Available:https://radiopaedia.org/articles/ependymoma<nowiki/>(accessed 11.5.2022)</ref>.


=== Glial cells ===
Unlike other kinds of cancer, ependymomas usually don’t spread to other parts of the body, but can spread to more than one area of the brain or spine. In children, these tumors are likely to come back after treatment<ref>Web Md Ependymoma Available: https://www.webmd.com/cancer/brain-cancer/what-is-ependymoma (accessed 11.5.2022)</ref>.
Glial cells are a cell type that are found between nerve cells that share a general function of holding the CNS together. There are more glial cells than nerve cells and thereby constitute half of the total volume of the CNS. The four types of glial cells are: oligodenrocytes, microglia, epndymal cells and astrocytes.<ref>Palastanga, N., Field, D. and Soames, R. (2012). ''Anatomy and Human Movement: Structure and Function''. 6th ed. Burlington: Elsevier Science.</ref>
[[File:Tentorium cerebelli.jpeg|right|frameless]]
They can be divided into three groups depending on the anatomical compartment in which they are found:


=== Ventricals ===
# Posterior fossa (60%)
Ventricals and the central canal of the spinal cord are fluid-filled spaces within the CNS that contain cerebrospinal fluid. Both are common locations for tumours.<ref name=":0" />
# Supratentorial (30%) ie above the tentorium cerebelli
# Spinal cord (10%)<ref name=":6" />
==Clinically Relevant Anatomy==
[[Glial Cells|Glial cells]]:  cell type that are found between nerve cells that share a general function of holding the CNS together. Although there are about 86-100 billion neurons in the brain, there are about the same number of glial cells in the brain.<ref>Palastanga, N., Field, D. and Soames, R. (2012). ''Anatomy and Human Movement: Structure and Function''. 6th ed. Burlington: Elsevier Science.</ref>
[[File:Ventricles Brain.png|thumb|Ventricles Brain]]
Ventricals and the Central Canal of the Spinal Cord: fluid-filled spaces within the CNS that contain cerebrospinal fluid. Both are common locations for tumours.


=== Tentorium Cerebelli ===
Tentorium Cerebelli: extension of the [[Meninges|dura matter]] that separates the [[cerebellum]] from the inferior aspect of the occipital lobes. Tumour below the tentorium are called infratentorial and those above are called supratentorial.
Tentorium Cerebelli is an extension of the dura matter that separates the cerebellum from the inferior aspect of the occipital lobes. Tumour below the tentorium are called infratentorial and those above are called supratentorial.<ref name=":0" />


== Pathological Process ==
==Pathological Process:==
Ependymomas are traditionally thought to arise from oncogenetic events that transform normal ependymal cells into tumor phenotypes. The precise nature and order of these genetic events are unknown.<ref name=":1">Emedicine.medscape.com. (2017). ''Ependymoma: Practice Essentials, Background, Pathophysiology''. [online] Available at: <nowiki>http://emedicine.medscape.com/article/277621-overview</nowiki> [Accessed 30 Aug. 2017].</ref>


== Clinical Presentation  ==
== Epidemiology ==
[[File:Ependymal Cells.png|thumb|Ependymal Cells Ventricle]]
Ependymomas affect all age groups, with a higher frequency in children, being the third most common brain tumor in pediatric patients. As per the Central Brain Tumor Registry of the United States (CBTRUS) Statistical Report for CNS tumors from the years 2011 to 2015, ependymal tumors represent 1.7% of all brain and CNS tumors, with a median age of 44 years.


add text here relating to the clinical presentation of the condition<br>  
Children: It represents around 6% to 12% of children brain tumor and 2% of all childhood cancer<ref name=":3">Kilday JP, Rahman R, Dyer S, Ridley L, Lowe J, Coyle B, Grundy R. Pediatric ependymoma: biological perspectives. Molecular Cancer Research. 2009 Jun 1;7(6):765-86.</ref>. The prognosis for pediatric ependymomas remains relatively poor when compared with other brain tumors in children,despite advances in neurosurgery, neuroimaging techniques, and postoperative adjuvant therapy.<ref name=":3" /> The 5-year survival rate ranges from 39% to 64%.<ref name=":3" />


== Diagnostic Procedures  ==
Adults: the most common primary glial neoplasm of spinal cord representing 50%–60% of all intramedullary cord neoplasms.<ref name=":4">Helseth A, Mørk SJ. Primary intraspinal neoplasms in Norway, 1955 to 1986: a population-based survey of 467 patients. Journal of neurosurgery. 1989 Dec 1;71(6):842-5</ref><ref>Mohammed W, Farrell M, Bolger C. Spinal cord ependymoma–Surgical management and outcome. Journal of Neurosciences in Rural Practice. 2019 Apr 1;10(2):316.</ref>; Most commonly occur in the spinal cord<ref name=":0">Cern-foundation.org. (2017). ''Ependymoma Basics | CERN Foundation''. [online] Available at: <nowiki>http://www.cern-foundation.org/education/ependymoma-basics</nowiki> [Accessed 24 Aug. 2017].
</ref>; Ependymomas are believed to be slow-growing tumors and exhibit benign pathology behavior<ref name=":4" />.


Tumors are classified and graded according to their appearance when viewed through the microscope with the most severe tumour associated with a higher grade.
== Clinical Presentation  ==
 
[[File:Ependymoma4.jpg|thumb|4th ventricular ependymoma]]
=== World Health Organization (WHO) Classification of Tumors of the Nervous System ===
'''Brain tumor symptoms include:'''
 
* Headache or pressure in the head
==== Myxopapillary ependymoma (WHO grade I) ====
* Nausea or vomiting
This entity is characterised by cuboidal tumour cells, with GFAP expression and lack of cytokeratin expression, surrounding blood vessels in a mucoid matrix. Mitotic activity is very low or absent. 2.1.2.
* Blurred vision
 
* Weakness or numbness and tingling
==== Subependymoma (WHO grade I) ====
'''Spinal cord symptoms include:'''
Subependymoma has isomorphic nuclei in an abundant and dense fibrillary matrix with frequent microcysts; mitoses are very rare or absent. 2.1.3.
* Back pain
 
* Weakness in the arms or legs
==== Ependymoma (WHO grade II) ====
* Numbness or tingling in the arms, legs or trunk
This neoplasm has moderate cellularity; mitoses are rare or absent and nuclear morphology is monomorphic. Key histological features are perivascular pseudorosettes and ependymal rosettes[14]. Four histological variants have been described: cellular ependymoma, which has hypercellularity and increased mitotic rate, papillary ependymoma, clear cell ependymoma and tanycytic ependymoma.
* Problems going to the bathroom or controlling bowel or bladder function<ref name=":0" /><ref>Sofuoğlu ÖE, Abdallah A. Pediatric Spinal Ependymomas. Medical science monitor: international medical journal of experimental and clinical research. 2018;24:7072.</ref>
 
==== Anaplastic ependymoma (WHO grade III) ====
This tumour is characterised by hypercellularity, cellular and nuclear pleomorphism, frequent mitosis, pseudopalisading necrosis and endothelial proliferation. The latter two criteria do not appear to be independently related to prognosis [15]. Perivascular rosettes are a histological hallmark.<ref>Reni, M., Gatta, G., Mazza, E. and Vecht, C. (2007). Ependymoma. ''Critical Reviews in Oncology/Hematology'', 63(1), pp.81-89.
</ref>
 
== Management ==
add text here relating to management approaches to the condition<br>
 
== Differential Diagnosis<br>  ==
 
add text here relating to the differential diagnosis of this condition<br>  


== Key Evidence ==
== Diagnosis ==
To get an accurate diagnosis, a tumor biopsy is performed a ie piece of tumor tissue will be removed during surgery, if possible. A neuropathologist should then review the tumor tissue.<ref name=":2">NIH Ependymoma Available:https://www.cancer.gov/rare-brain-spine-tumor/tumors/ependymoma (accessed 11.5.2022)</ref>


add text here relating to key evidence with regards to any of the above headings<br>
==Ependymoma Grades==
[[File:Ependymoma2.jpg|thumb|Spinal ependymoma]]
Ependymomas are grouped in three grades based on their characteristics. Within each grade, are different ependymoma subtypes. Molecular testing is used to help identify subtypes that are related to location and disease characteristics.


== Resources <br> ==
# Grade I ependymomas: low grade tumors, cells grow slowly. The subtypes include subependymoma and myxopapillary ependymoma. Both are more common in adults than in children. Myxopapillary tumors usually occur in the spine.
# Grade II ependymomas: low grade tumors and can occur in either the brain or the spine.
# Grade III ependymomas: malignant (cancerous), fast-growing tumors.  The subtypes include anaplastic ependymomas.  These most often occur in the brain, but can also occur in the spine<ref name=":2" />.


add appropriate resources here
=== Treatment ===
Surgery: When possible, removing the tumour from the brain or spinal cord is a priority as SCI associated with spinal tumor is often managed surgically<ref>Ge L, Arul K, Mesfin A. Spinal Cord Injury From Spinal Tumors: Prevalence, Management, and Outcomes. World neurosurgery. 2019 Feb 1;122:e1551-6.</ref>. A secondary goal of surgery is obtaining a biopsy of cancerous cells for diagnosis.


== Case Studies  ==
After surgery, there is no standard treatment for ependymomas. with many people not needing other treatment after surgery. For others, treatments may include [[Radiation Side Effects and Syndromes|radiation]], [[Chemotherapy Side Effects and Syndromes|chemotherapy]] or clinical trials. Clinical trials, with new chemotherapy, targeted therapy, or [[Immunotherapy|immunotherapy drugs]], may also be available and can be a possible treatment option. Treatments are decided by the patient’s healthcare team based on the patient’s age, remaining tumor after surgery, tumor type, and tumor location<ref name=":2" />.


add links to case studies here (case studies should be added on new pages using the [[Template:Case Study|case study template]])<br>  
Palliative care may be necessary for patients at end-of-life. Those who undergo surgery may also develop a number of neurological deficits. These individuals may require physical therapy, speech therapy, and occupational therapy. In many cases, the neurological deficits are permanent<ref name=":5">Zamora EA, Alkherayf F. Ependymoma. InStatPearls [Internet] 2021 Jul 20. StatPearls Publishing.Available:https://www.ncbi.nlm.nih.gov/books/NBK538244/ (accessed 11.5.2022)</ref>.


== References ==
=== Physiotherapy ===
[[File:Pediatric polysomnogram.jpg|right|frameless]]
Patients who are long-term survivors of CNS tumors may present a wide diversity of complications. Physiotherapists may be involved with the rehabilitation for eg neurological deficits, sensorineural hearing loss, gait deficits and management of long-term complications, most commonly fatigue, numbness and tingling, pain, and disturbed sleep.<ref name=":5" />


References will automatically be added here, see [[Adding References|adding references tutorial]].  
Physiotherapists may also be involved in palliative care.  Patients should receive counseling regarding their prognosis. Those with CNS tumors at end-of-life benefiting from palliative care. Palliative care should be interprofessional to cover the wide spectrum of needs that these patients will face<ref name=":5" />. <br>


== References ==
<references />
<references />
[[Category:Oncology]]

Latest revision as of 03:06, 11 May 2022

Original Editor - George Prudden

Top Contributors - Shaimaa Eldib, Lucinda hampton, George Prudden, Kim Jackson, Vidya Acharya and Rewan Elsayed Elkanafany

Introduction[edit | edit source]

Anaplastic ependymoma in an adult patient

Ependymomas represent a broad group of glial tumours most often arising from the lining of the ventricles of the brain or the central canal of the spinal cord. They account for ~5% of all neuroepithelial neoplasms, ~10% of all paediatric brain tumours and up to 33% of brain tumours occurring in those less than 3 years of age[1].

Unlike other kinds of cancer, ependymomas usually don’t spread to other parts of the body, but can spread to more than one area of the brain or spine. In children, these tumors are likely to come back after treatment[2].

Tentorium cerebelli.jpeg

They can be divided into three groups depending on the anatomical compartment in which they are found:

  1. Posterior fossa (60%)
  2. Supratentorial (30%) ie above the tentorium cerebelli
  3. Spinal cord (10%)[1]

Clinically Relevant Anatomy[edit | edit source]

Glial cells: cell type that are found between nerve cells that share a general function of holding the CNS together. Although there are about 86-100 billion neurons in the brain, there are about the same number of glial cells in the brain.[3]

Ventricles Brain

Ventricals and the Central Canal of the Spinal Cord: fluid-filled spaces within the CNS that contain cerebrospinal fluid. Both are common locations for tumours.

Tentorium Cerebelli: extension of the dura matter that separates the cerebellum from the inferior aspect of the occipital lobes. Tumour below the tentorium are called infratentorial and those above are called supratentorial.

Pathological Process:[edit | edit source]

Ependymomas are traditionally thought to arise from oncogenetic events that transform normal ependymal cells into tumor phenotypes. The precise nature and order of these genetic events are unknown.[4]

Epidemiology[edit | edit source]

Ependymal Cells Ventricle

Ependymomas affect all age groups, with a higher frequency in children, being the third most common brain tumor in pediatric patients. As per the Central Brain Tumor Registry of the United States (CBTRUS) Statistical Report for CNS tumors from the years 2011 to 2015, ependymal tumors represent 1.7% of all brain and CNS tumors, with a median age of 44 years.

Children: It represents around 6% to 12% of children brain tumor and 2% of all childhood cancer[5]. The prognosis for pediatric ependymomas remains relatively poor when compared with other brain tumors in children,despite advances in neurosurgery, neuroimaging techniques, and postoperative adjuvant therapy.[5] The 5-year survival rate ranges from 39% to 64%.[5]

Adults: the most common primary glial neoplasm of spinal cord representing 50%–60% of all intramedullary cord neoplasms.[6][7]; Most commonly occur in the spinal cord[8]; Ependymomas are believed to be slow-growing tumors and exhibit benign pathology behavior[6].

Clinical Presentation[edit | edit source]

4th ventricular ependymoma

Brain tumor symptoms include:

  • Headache or pressure in the head
  • Nausea or vomiting
  • Blurred vision
  • Weakness or numbness and tingling

Spinal cord symptoms include:

  • Back pain
  • Weakness in the arms or legs
  • Numbness or tingling in the arms, legs or trunk
  • Problems going to the bathroom or controlling bowel or bladder function[8][9]

Diagnosis[edit | edit source]

To get an accurate diagnosis, a tumor biopsy is performed a ie piece of tumor tissue will be removed during surgery, if possible. A neuropathologist should then review the tumor tissue.[10]

Ependymoma Grades[edit | edit source]

Spinal ependymoma

Ependymomas are grouped in three grades based on their characteristics. Within each grade, are different ependymoma subtypes. Molecular testing is used to help identify subtypes that are related to location and disease characteristics.

  1. Grade I ependymomas: low grade tumors, cells grow slowly. The subtypes include subependymoma and myxopapillary ependymoma. Both are more common in adults than in children. Myxopapillary tumors usually occur in the spine.
  2. Grade II ependymomas: low grade tumors and can occur in either the brain or the spine.
  3. Grade III ependymomas: malignant (cancerous), fast-growing tumors.  The subtypes include anaplastic ependymomas.  These most often occur in the brain, but can also occur in the spine[10].

Treatment[edit | edit source]

Surgery: When possible, removing the tumour from the brain or spinal cord is a priority as SCI associated with spinal tumor is often managed surgically[11]. A secondary goal of surgery is obtaining a biopsy of cancerous cells for diagnosis.

After surgery, there is no standard treatment for ependymomas. with many people not needing other treatment after surgery. For others, treatments may include radiation, chemotherapy or clinical trials. Clinical trials, with new chemotherapy, targeted therapy, or immunotherapy drugs, may also be available and can be a possible treatment option. Treatments are decided by the patient’s healthcare team based on the patient’s age, remaining tumor after surgery, tumor type, and tumor location[10].

Palliative care may be necessary for patients at end-of-life. Those who undergo surgery may also develop a number of neurological deficits. These individuals may require physical therapy, speech therapy, and occupational therapy. In many cases, the neurological deficits are permanent[12].

Physiotherapy[edit | edit source]

Pediatric polysomnogram.jpg

Patients who are long-term survivors of CNS tumors may present a wide diversity of complications. Physiotherapists may be involved with the rehabilitation for eg neurological deficits, sensorineural hearing loss, gait deficits and management of long-term complications, most commonly fatigue, numbness and tingling, pain, and disturbed sleep.[12]

Physiotherapists may also be involved in palliative care. Patients should receive counseling regarding their prognosis. Those with CNS tumors at end-of-life benefiting from palliative care. Palliative care should be interprofessional to cover the wide spectrum of needs that these patients will face[12].

References[edit | edit source]

  1. 1.0 1.1 Radiopedia Ependymoma Available:https://radiopaedia.org/articles/ependymoma(accessed 11.5.2022)
  2. Web Md Ependymoma Available: https://www.webmd.com/cancer/brain-cancer/what-is-ependymoma (accessed 11.5.2022)
  3. Palastanga, N., Field, D. and Soames, R. (2012). Anatomy and Human Movement: Structure and Function. 6th ed. Burlington: Elsevier Science.
  4. Emedicine.medscape.com. (2017). Ependymoma: Practice Essentials, Background, Pathophysiology. [online] Available at: http://emedicine.medscape.com/article/277621-overview [Accessed 30 Aug. 2017].
  5. 5.0 5.1 5.2 Kilday JP, Rahman R, Dyer S, Ridley L, Lowe J, Coyle B, Grundy R. Pediatric ependymoma: biological perspectives. Molecular Cancer Research. 2009 Jun 1;7(6):765-86.
  6. 6.0 6.1 Helseth A, Mørk SJ. Primary intraspinal neoplasms in Norway, 1955 to 1986: a population-based survey of 467 patients. Journal of neurosurgery. 1989 Dec 1;71(6):842-5
  7. Mohammed W, Farrell M, Bolger C. Spinal cord ependymoma–Surgical management and outcome. Journal of Neurosciences in Rural Practice. 2019 Apr 1;10(2):316.
  8. 8.0 8.1 Cern-foundation.org. (2017). Ependymoma Basics | CERN Foundation. [online] Available at: http://www.cern-foundation.org/education/ependymoma-basics [Accessed 24 Aug. 2017].
  9. Sofuoğlu ÖE, Abdallah A. Pediatric Spinal Ependymomas. Medical science monitor: international medical journal of experimental and clinical research. 2018;24:7072.
  10. 10.0 10.1 10.2 NIH Ependymoma Available:https://www.cancer.gov/rare-brain-spine-tumor/tumors/ependymoma (accessed 11.5.2022)
  11. Ge L, Arul K, Mesfin A. Spinal Cord Injury From Spinal Tumors: Prevalence, Management, and Outcomes. World neurosurgery. 2019 Feb 1;122:e1551-6.
  12. 12.0 12.1 12.2 Zamora EA, Alkherayf F. Ependymoma. InStatPearls [Internet] 2021 Jul 20. StatPearls Publishing.Available:https://www.ncbi.nlm.nih.gov/books/NBK538244/ (accessed 11.5.2022)
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