Pineal gland tumor: Difference between revisions
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* Cerebellar involvement would result in motor impairment. | * Cerebellar involvement would result in motor impairment. | ||
** If the tumor of the pineal gland is present in childhood, then endocrine dysfunctions can also result such as precocious pseudopuberty, [[diabetes insipidus]], and a slowed growth rate. | ** If the tumor of the pineal gland is present in childhood, then endocrine dysfunctions can also result such as precocious pseudopuberty, [[diabetes insipidus]], and a slowed growth rate. | ||
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|Pineal choriocarcinoma | |||
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* Presence of intimately related [[Syncytiotrophoblast|syncytiotrophoblasts]] and [[Cytotrophoblast|cytotrophoblasts]] without formation of definite placental type villi. | |||
* [[Syncytiotrophoblast|Syncytiotrophoblasts]] are large multi-nucleated cells with eosinophilic cytoplasm. | |||
* They often surround the [[Cytotrophoblast|cytotrophoblasts]], reminiscent of their normal anatomical relationship in [[chorionic villi]]. | |||
* [[Cytotrophoblast|Cytotrophoblasts]] are polyhedral, mononuclear cells with hyperchromatic [[nuclei]] and a clear or pale [[cytoplasm]].<ref name="histo1pc2" /> | |||
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== Pineal choriocarcinoma == | == Pineal choriocarcinoma == | ||
*Pineal choriocarcinoma is a relatively rare, malignant, highly vascular neoplasm and accounts for a small proportion of all intracranial germ cell tumors. It is an aggressive tumor and has a propensity to metastasise systemically. Pure pineal choriocarcinoma tumors secrete [[Human chorionic gonadotropin|β-HCG]]. | *Pineal choriocarcinoma is a relatively rare, malignant, highly vascular neoplasm and accounts for a small proportion of all intracranial germ cell tumors. It is an aggressive tumor and has a propensity to metastasise systemically. Pure pineal choriocarcinoma tumors secrete [[Human chorionic gonadotropin|β-HCG]]. | ||
*On microscopic histopathological analysis, pineal choriocarcinoma is characterized by presence of intimately related [[Syncytiotrophoblast|syncytiotrophoblasts]] and [[Cytotrophoblast|cytotrophoblasts]] without formation of definite placental type villi. [[Syncytiotrophoblast|Syncytiotrophoblasts]] are large multi-nucleated cells with eosinophilic cytoplasm. They often surround the [[Cytotrophoblast|cytotrophoblasts]], reminiscent of their normal anatomical relationship in [[chorionic villi]]. [[Cytotrophoblast|Cytotrophoblasts]] are polyhedral, mononuclear cells with hyperchromatic [[nuclei]] and a clear or pale [[cytoplasm]].<ref name="histo1pc2">Pathology of choriocarcinoma. Wikipedia 2015. https://en.wikipedia.org/wiki/Choriocarcinoma. Accessed on December 7, 2015</ref> | *On microscopic histopathological analysis, pineal choriocarcinoma is characterized by presence of intimately related [[Syncytiotrophoblast|syncytiotrophoblasts]] and [[Cytotrophoblast|cytotrophoblasts]] without formation of definite placental type villi. [[Syncytiotrophoblast|Syncytiotrophoblasts]] are large multi-nucleated cells with eosinophilic cytoplasm. They often surround the [[Cytotrophoblast|cytotrophoblasts]], reminiscent of their normal anatomical relationship in [[chorionic villi]]. [[Cytotrophoblast|Cytotrophoblasts]] are polyhedral, mononuclear cells with hyperchromatic [[nuclei]] and a clear or pale [[cytoplasm]].<ref name="histo1pc2">Pathology of choriocarcinoma. Wikipedia 2015. https://en.wikipedia.org/wiki/Choriocarcinoma. Accessed on December 7, 2015</ref> | ||
*Pineal choriocarcinoma accounts for 5% of all pineal masses.<ref name="overviewpc12" /> | *Pineal choriocarcinoma accounts for 5% of all pineal masses.<ref name="overviewpc12">Intracranial choriocarcinoma. Frank Gaillard et al. Radiopaedia 2015. http://radiopaedia.org/articles/intracranial-choriocarcinoma. Accessed on December 7, 2015</ref> | ||
*The peak age at diagnosis for pineal choriocarcinoma is 20-30 years. | *The peak age at diagnosis for pineal choriocarcinoma is 20-30 years. | ||
*Common complications of pineal choriocarcinoma include:<ref name="pmid38402342">{{cite journal| author=Kida Y, Banno M, Kanzaki M, Kobayashi T, Kageyama N| title=[Pineal choriocarcinoma presenting massive ventricular hemorrhage--a case report]. | journal=No Shinkei Geka | year= 1985 | volume= 13 | issue= 6 | pages= 641-5 | pmid=3840234 | doi= | pmc= | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/istopatcite&retmode=ref&cmd=prlinks&id=3840234 }}</ref><ref name="complicationpc12">Radiographic features of intracranial choriocarcinoma. Frank Gaillard et al. Radiopaedia 2015. http://radiopaedia.org/articles/intracranial-choriocarcinoma. Accessed on December 7, 2015</ref> | *Common complications of pineal choriocarcinoma include:<ref name="pmid38402342">{{cite journal| author=Kida Y, Banno M, Kanzaki M, Kobayashi T, Kageyama N| title=[Pineal choriocarcinoma presenting massive ventricular hemorrhage--a case report]. | journal=No Shinkei Geka | year= 1985 | volume= 13 | issue= 6 | pages= 641-5 | pmid=3840234 | doi= | pmc= | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/istopatcite&retmode=ref&cmd=prlinks&id=3840234 }}</ref><ref name="complicationpc12">Radiographic features of intracranial choriocarcinoma. Frank Gaillard et al. Radiopaedia 2015. http://radiopaedia.org/articles/intracranial-choriocarcinoma. Accessed on December 7, 2015</ref> | ||
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*Laboratory findings consistent with the diagnosis of pineal choriocarcinoma include [[CSF analysis|abnormal CSF analysis]], demonstrating xanthochromia.<ref name="FujiiItakura19812" /> | *Laboratory findings consistent with the diagnosis of pineal choriocarcinoma include [[CSF analysis|abnormal CSF analysis]], demonstrating xanthochromia.<ref name="FujiiItakura19812" /> | ||
*Head CT scan and brain MRI may be helpful in the diagnosis of pineal choriocarcinoma. | *Head CT scan and brain MRI may be helpful in the diagnosis of pineal choriocarcinoma. | ||
*On head CT scan, pineal choriocarcinoma is characterized by a | *On head CT scan, pineal choriocarcinoma is characterized by a | ||
*On brain MRI, pineal choriocarcinoma is characterized by | *On brain MRI, pineal choriocarcinoma is characterized by | ||
*[[Biopsy]] is generally done to confirm the diagnosis of pineal choriocarcinoma. | *[[Biopsy]] is generally done to confirm the diagnosis of pineal choriocarcinoma. | ||
*The mainstay of therapy for pineal choriocarcinoma is [[radiotherapy]] and/or [[chemotherapy]]. Sometimes, [[surgical resection]] may be done. | *The mainstay of therapy for pineal choriocarcinoma is [[radiotherapy]] and/or [[chemotherapy]]. Sometimes, [[surgical resection]] may be done. | ||
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* Hypo- to isointense on T1-weighted images | * Hypo- to isointense on T1-weighted images | ||
* Hyperintense on T2-weighted images. | * Hyperintense on T2-weighted images. | ||
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|Pineal choriocarcinoma | |||
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* Grade IV | |||
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* Relatively rare, malignant, highly vascular neoplasm and accounts for a small proportion of all intracranial germ cell tumors. | |||
* It is an aggressive tumor and has a propensity to metastasise systemically. | |||
* Pure pineal choriocarcinoma tumors secrete [[Human chorionic gonadotropin|β-HCG]].<ref name="overviewpc12" /> | |||
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* High | |||
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* Round, calcified, homogeneous, enhancing mass in the third ventricle associated with the dilation of the lateral and third ventricles and periventricular lucency.<ref name="FujiiItakura19812" /> | |||
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* Hyperintensity on T1-weighted images and signal drop-out and blooming on T2* sequences.<ref name="mripc12">MRI brain radiographic features of intracranial choriocarcinoma. Frank Gaillard et al. Radiopaedia 2015. http://radiopaedia.org/articles/intracranial-choriocarcinoma. Accessed on December 8, 2015</ref> | |||
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|Pineal Parenchymal Tumor of Intermediate Differentiation | |Pineal Parenchymal Tumor of Intermediate Differentiation |
Revision as of 20:21, 16 May 2019
Pineal gland tumor Main page |
Differentiating features among different various Pineal Gland Tumors |
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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]Associate Editor(s)-in-Chief: Fahimeh Shojaei, M.D., Sujit Routray, M.D. [2], Aditya Ganti M.B.B.S. [3]
Synonyms and keywords: Pineal gland tumors; Pineal gland cancer; Pineal gland cancers; Pineal gland neoplasm; Pineal gland neoplasms; Neoplasm of the pineal gland; Neoplasms of the pineal gland; Cancer of the pineal gland; Cancers of the pineal gland; Astrocytoma; Meningioma; Pineal gland; Parinaud syndrome; Brain tumor
Overview
The pineal gland is an endocrine gland that is located in the posterior aspect of the cranial fossa in the brain. The pineal gland is responsible for the secretion of melatonin hormone that regulates the in the circadian cycle sleep and wakefulness. The blood supply of the pineal gland is derived from the posterior cerebral artery from its choroidal branches. The internal cerebral vein drains the blood from the epiphysis cerebri. Histologically the gland consists of cells called pinealocytes. Several different tumors can arise from the pineal gland. Primary pineal cell tumors include pineocytoma, pineoblastoma, and mixed pineal tumors. Tumors that may occur in this region but are not necessarily pineal tumors include germinoma, non-germinoma (eg, teratoma, endodermal sinus tumor, embryonal cell tumor, choriocarcinoma, and mixed tumors), meningioma, astrocytoma, ganglioglioma, and dermoid cysts. Diagnosis of the type of tumor is crucial for treatment. The primary symptom of the tumor would be hydrocephalus. If the pineal gland invades the thalamus, it can cause weakness and loss of sensation in half of the body. Invasion of the hypothalamus would disrupt sleep, impede temperature and water regulation, and cause weight gain. An MRI is important when trying to see the location and size of the tumor. A biopsy is required to determine the type of tumor. Usually, a biopsy is done via a stereotactic or endoscopic procedure. Sometimes biomarkers are used to detect the presence of the tumor, and if these are found in the CSF and blood, then a biopsy might not be needed. Some of these chemicals are beta-human chorionic gonadotropin, carcinoembryonic antigen, and a-fetoprotein.
Classification
Pineal gland tumors are broadly divided into four subcategories. The various types of pineal gland tumors include:[1]
1. Pineal parenchymal tumors: Pineal parenchymal tumors arise directly from the normal functional cells of the pineal gland, pineal parenchymal cells (pineocytes or their precursors), and they are distinct from other pineal gland neoplasms such as astrocytic and germ cell tumors. These tumors are formed after the embryological development of the pineal gland.
2. Pineal germ cell tumors: They are tumors which arise from the embryological abnormalities. They are derived from the germ cells, including sex cells, of the pineal gland during the developmental process of the pineal gland.
3. Astrocytoma of the pineal gland: They arise from the astrocytes, which are a particular kind of star-shaped, glial brain cells around the pineal gland.
4. Pineal metastasis: Pineal metastasis is a cancer that has metastasized to the pineal gland from another location in the body.
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Pathophysiology
Normal Anatomy
- The pineal gland is a small reddish-brown structure that derives its name from its pinecone-like shape.
- The pineal ranges in size from 10 to 14 mm; it is located in the midline, above the tentorium and superior colliculi and below the splenium of the corpus callosum and the vein of Galen, and is attached to the superior aspect of the posterior border of the third ventricle.
- The blood supply of the pineal gland is derived from the posterior cerebral artery from its choroidal branches.
- The internal cerebral vein drains the blood from the epiphysis cerebri.
- Histologically the gland consists of cells called pinealocytes and supporting cells.
Embryology
- Pineal gland develops as a diverticulum in the diencephalic roof of the third ventricle during the second month of gestation.
- The mature gland is suspended from the pineal stalk from the posterior roof of the third ventricle.
- The pineal secretes melatonin, which is involved in diurnal rhythms.
Pathogenesis
- Due to the pineal gland's location, any tumor or cyst formation would lead to the compression of the aqueduct of Sylvius.
- The aqueduct of Sylvius allows the cerebrospinal fluid to circulate out.
- When there is a blockage in aqueduct of Sylvius by an abnormal pineal gland, the passage of the duct is blocked, and CSF pressure builds up, leading to hydrocephalus.
- Increase in intracranial pressure can even be life-threatening, prompting emergency treatment.
- The hydrocephalus can be relieved by the placement of a VP shunt or ventriculostomy.
- Vision changes would also occur due to an involvement of the tectal region.
- The tectal region helps dictate eye movements.
- Fault in the tectal region causes double vision, an issue with focusing on objects, and eye movement impairment.
- The pineal gland can cause Parinaud syndrome due to the increasing size of the gland compressing the pretectal area and superior colliculi of the midbrain.
- Parinaud syndrome prevents a person from moving his or her eyes up and down.
- The thalamus can be affected, and if so, there can be disturbances on that side of the body which would result in weakness and loss of sensation.
- The tumor's effect on the hypothalamus will lead to weight gain, disruption of sleep, disruption of temperature control, and water regulation.
- Cerebellar involvement would result in motor impairment.
- If the tumor of the pineal gland is present in childhood, then endocrine dysfunctions can also result such as precocious pseudopuberty, diabetes insipidus, and a slowed growth rate.
Microscopic histopathological analysis | |||
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Pineal choriocarcinoma |
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Pineal choriocarcinoma
- Pineal choriocarcinoma is a relatively rare, malignant, highly vascular neoplasm and accounts for a small proportion of all intracranial germ cell tumors. It is an aggressive tumor and has a propensity to metastasise systemically. Pure pineal choriocarcinoma tumors secrete β-HCG.
- On microscopic histopathological analysis, pineal choriocarcinoma is characterized by presence of intimately related syncytiotrophoblasts and cytotrophoblasts without formation of definite placental type villi. Syncytiotrophoblasts are large multi-nucleated cells with eosinophilic cytoplasm. They often surround the cytotrophoblasts, reminiscent of their normal anatomical relationship in chorionic villi. Cytotrophoblasts are polyhedral, mononuclear cells with hyperchromatic nuclei and a clear or pale cytoplasm.[2]
- Pineal choriocarcinoma accounts for 5% of all pineal masses.[3]
- The peak age at diagnosis for pineal choriocarcinoma is 20-30 years.
- Common complications of pineal choriocarcinoma include:[4][5]
- The clinical presentation of pineal choriocarcinoma is mainly from the obstructive hydrocephalus secondary to compression of the tectum of the midbrain and obstruction of the aqueduct. Symptoms of pineal choriocarcinoma include headache, vomiting, ptosis, and weakness.[6]
- Compression of the superior colliculi can lead to a characteristic gaze palsy, known as Parinaud syndrome.
- Common physical examination findings of pineal choriocarcinoma include papilledema, signs of precocious puberty, restricted extraocular movements, sluggish pupillary light reflex, stiff neck, hemiparesis, and abducent nerve palsy.[6]
- Laboratory findings consistent with the diagnosis of pineal choriocarcinoma include abnormal CSF analysis, demonstrating xanthochromia.[6]
- Head CT scan and brain MRI may be helpful in the diagnosis of pineal choriocarcinoma.
- On head CT scan, pineal choriocarcinoma is characterized by a
- On brain MRI, pineal choriocarcinoma is characterized by
- Biopsy is generally done to confirm the diagnosis of pineal choriocarcinoma.
- The mainstay of therapy for pineal choriocarcinoma is radiotherapy and/or chemotherapy. Sometimes, surgical resection may be done.
Differentiating pineal gland tumor from Other Diseases
Pineal gland tumormust be differentiated from other diseases that cause seizure, visual disturbance, and constitutional symptoms, such as:
- Oligodendroglioma
- Meningioma
- Astrocytoma
- Pituitary adenoma
- Schwannoma
- primary CNS lymphoma
- Medulloblastoma
- Ependymoma
- Craniopharyngioma
- Hemangioblastoma
- AV malformation
- Brain aneurysm
- Bacterial brain abscess
- Tuberculosis
- Toxoplasmosis
- Hydatid cyst
- CNS cryptococcosis
- CNS aspergillosis
- Brain metastasis
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Differentiating features among different various Pineal Gland Tumors
Tumors | Grade | Pathalogic Features | 5-year survival | Cerebrospinal fluid (CSF) dissemination | Imaging | |
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Pineocytoma |
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Pineal choriocarcinoma |
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Pineal Parenchymal Tumor of Intermediate Differentiation |
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Pineoblastoma |
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Papillary Tumor of the Pineal Region |
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Germinoma |
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Teratoma |
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Pineal Cyst |
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Epidermoid and Dermoid Cysts |
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Astrocytoma |
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Lipoma |
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References
- ↑ Pineal region mass. Dr Henry Knipe and Dr Frank Gaillard et al. Radiopaedia 2015. http://radiopaedia.org/articles/pineal-region-mass. Accessed on November 18, 2015
- ↑ 2.0 2.1 Pathology of choriocarcinoma. Wikipedia 2015. https://en.wikipedia.org/wiki/Choriocarcinoma. Accessed on December 7, 2015
- ↑ 3.0 3.1 Intracranial choriocarcinoma. Frank Gaillard et al. Radiopaedia 2015. http://radiopaedia.org/articles/intracranial-choriocarcinoma. Accessed on December 7, 2015
- ↑ Kida Y, Banno M, Kanzaki M, Kobayashi T, Kageyama N (1985). "[Pineal choriocarcinoma presenting massive ventricular hemorrhage--a case report]". No Shinkei Geka. 13 (6): 641–5. PMID 3840234.
- ↑ Radiographic features of intracranial choriocarcinoma. Frank Gaillard et al. Radiopaedia 2015. http://radiopaedia.org/articles/intracranial-choriocarcinoma. Accessed on December 7, 2015
- ↑ 6.0 6.1 6.2 6.3 Fujii, Toru; Itakura, Toru; Hayashi, Seiji; Komai, Norihiko; Nakamine, Hirokazu; Saito, Koji (1981). "Primary pineal choriocarcinoma with hemorrhage monitored by computerized tomography". Journal of Neurosurgery. 55 (3): 484–487. doi:10.3171/jns.1981.55.3.0484. ISSN 0022-3085.
- ↑ MRI brain radiographic features of intracranial choriocarcinoma. Frank Gaillard et al. Radiopaedia 2015. http://radiopaedia.org/articles/intracranial-choriocarcinoma. Accessed on December 8, 2015
- ↑ See SJ, Gilbert MR (October 2004). "Anaplastic astrocytoma: diagnosis, prognosis, and management". Semin. Oncol. 31 (5): 618–34. PMID 15497115.
- ↑ Korshunov A, Golanov A, Sycheva R (July 2002). "Immunohistochemical markers for prognosis of anaplastic astrocytomas". J. Neurooncol. 58 (3): 203–15. PMID 12187956.
- ↑ Burger PC, Vogel FS, Green SB, Strike TA (September 1985). "Glioblastoma multiforme and anaplastic astrocytoma. Pathologic criteria and prognostic implications". Cancer. 56 (5): 1106–11. PMID 2990664.