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==Diffuse Midline Glioma==
{{SI}}
 
{{Infobox medical condition
[[File:Palliative_Care_Options_for_a_Young_Adult_Patient_with_a_Diffuse_Intrinsic_Pontine_Glioma_-_Fig._1_(cropped).png|thumb|right|MRI scan showing a diffuse midline glioma in the brainstem.]]
| name                    = Diffuse midline glioma
 
| image                  = [[File:Palliative_Care_Options_for_a_Young_Adult_Patient_with_a_Diffuse_Intrinsic_Pontine_Glioma_-_Fig._1_(cropped).png|250px]]
'''Diffuse midline glioma''' is a type of [[brain tumor]] that occurs primarily in children, although it can also be found in adults. These tumors are characterized by their location in the midline structures of the brain, such as the [[thalamus]], [[brainstem]], and [[spinal cord]]. They are highly aggressive and are classified as [[World Health Organization]] (WHO) grade IV tumors.
| caption                = MRI of a diffuse midline glioma
 
| field                  = [[Neuro-oncology]]
| synonyms                = Diffuse intrinsic pontine glioma (DIPG)
| symptoms                = [[Headache]], [[nausea]], [[vomiting]], [[balance disorder]], [[vision problems]], [[facial weakness]]
| onset                  = Typically in [[childhood]]
| duration                = Progressive
| causes                  = [[Genetic mutations]] (e.g., [[H3 K27M mutation]])
| risks                  = Unknown
| diagnosis              = [[Magnetic resonance imaging|MRI]], [[biopsy]]
| differential            = [[Brainstem glioma]], [[ependymoma]], [[medulloblastoma]]
| treatment              = [[Radiation therapy]], [[chemotherapy]], [[palliative care]]
| prognosis              = Poor
| frequency              = Rare
}}
{{Short description|Overview of Diffuse Midline Glioma}}
'''Diffuse midline glioma''' (DMG) is a type of [[brain tumor]] that occurs in the midline structures of the [[central nervous system]], such as the [[thalamus]], [[brainstem]], and [[spinal cord]]. These tumors are characterized by their infiltrative nature, making them difficult to surgically remove. They are most commonly diagnosed in children and are associated with a poor prognosis.
==Classification==
Diffuse midline gliomas are classified as [[high-grade gliomas]], specifically as [[World Health Organization]] (WHO) grade IV tumors. They are often associated with a specific genetic mutation in the [[H3 K27M]] gene, which is a hallmark of this tumor type. This mutation leads to changes in the [[epigenetic]] regulation of gene expression, contributing to the aggressive nature of the tumor.
==Pathophysiology==
==Pathophysiology==
 
[[File:Mutations_in_diffuse_intrinsic_pontine_glioma_samples_from_several_anatomical_locations_-_Ncomms11185-f1.jpg|thumb|left|Genetic mutations associated with diffuse intrinsic pontine glioma.]]
Diffuse midline gliomas are infiltrative tumors that spread along the white matter tracts of the brain. They are often associated with mutations in the [[H3 K27M]] gene, which is a hallmark of this tumor type. These mutations lead to changes in the chromatin structure, affecting gene expression and promoting tumor growth.
The pathophysiology of diffuse midline glioma involves the infiltration of tumor cells into the surrounding brain tissue. The H3 K27M mutation results in a global reduction of [[histone]] H3 lysine 27 trimethylation, which affects the expression of numerous genes involved in cell growth and differentiation. This mutation is thought to drive the oncogenic process in these tumors.
 
[[File:Mutations_in_diffuse_intrinsic_pontine_glioma_samples_from_several_anatomical_locations_-_Ncomms11185-f1.jpg|thumb|left|Diagram showing common mutations in diffuse intrinsic pontine glioma.]]
 
==Clinical Presentation==
==Clinical Presentation==
 
Patients with diffuse midline glioma typically present with symptoms related to the location of the tumor. For example, tumors in the [[brainstem]] may cause [[cranial nerve]] deficits, [[ataxia]], and [[dysphagia]]. Tumors in the thalamus can lead to [[hemiparesis]], [[sensory deficits]], and [[altered mental status]].
Patients with diffuse midline glioma typically present with symptoms related to the location of the tumor. For example, tumors in the brainstem may cause cranial nerve deficits, difficulty swallowing, and problems with balance and coordination. Tumors in the thalamus can lead to sensory and motor deficits, while spinal cord involvement may cause weakness and sensory changes in the limbs.
 
==Diagnosis==
==Diagnosis==
 
[[File:Integrated_Molecular_Meta-Analysis_of_1,000_Pediatric_High-Grade_and_Diffuse_Intrinsic_Pontine_Glioma_-_graphical_abstract.jpg|thumb|left|Molecular analysis of pediatric high-grade gliomas.]]
Diagnosis of diffuse midline glioma is primarily based on [[magnetic resonance imaging]] (MRI) findings. The tumors appear as poorly defined, infiltrative masses that enhance with contrast. A biopsy may be performed to confirm the diagnosis and identify specific genetic mutations.
Diagnosis of diffuse midline glioma is typically made using [[magnetic resonance imaging]] (MRI), which reveals a diffusely infiltrative lesion in the midline structures. [[Biopsy]] may be performed to confirm the diagnosis and identify the presence of the H3 K27M mutation.
 
==Treatment==
==Treatment==
 
The treatment of diffuse midline glioma is challenging due to the tumor's location and infiltrative nature. [[Radiation therapy]] is the mainstay of treatment and can provide temporary relief of symptoms. However, the tumor often recurs, and the overall prognosis remains poor. [[Chemotherapy]] has limited effectiveness, and research is ongoing to find more effective treatments.
[[File:Drug_delivery_to_diffuse_intrinsic_pontine_glioma_(DIPG)_-_Fphar-08-00495-g004.jpg|thumb|right|Illustration of drug delivery methods for treating diffuse intrinsic pontine glioma.]]
 
Treatment options for diffuse midline glioma are limited. The standard approach is [[radiation therapy]], which can provide temporary relief of symptoms and slow tumor progression. Chemotherapy has not been shown to be effective in most cases. Research is ongoing to find new treatments, including targeted therapies and immunotherapy.
 
==Prognosis==
==Prognosis==
 
The prognosis for patients with diffuse midline glioma is generally poor, with a median survival of less than one year from diagnosis. The presence of the H3 K27M mutation is associated with a particularly aggressive clinical course.
The prognosis for patients with diffuse midline glioma is poor, with a median survival of less than one year. The aggressive nature of the tumor and its location in critical areas of the brain make it difficult to treat effectively.
 
==Research Directions==
==Research Directions==
 
[[File:Palliative_Care_Options_for_a_Young_Adult_Patient_with_a_Diffuse_Intrinsic_Pontine_Glioma_-_Fig._2_(cropped).png|thumb|left|Research into palliative care options for patients with diffuse intrinsic pontine glioma.]]
Ongoing research is focused on understanding the molecular mechanisms underlying diffuse midline glioma and developing new therapeutic strategies. Studies are exploring the use of targeted therapies that specifically inhibit the pathways activated by the H3 K27M mutation.
Research into diffuse midline glioma is focused on understanding the molecular mechanisms driving tumor growth and identifying potential therapeutic targets. Novel treatment approaches, including targeted therapies and [[immunotherapy]], are being investigated in clinical trials.
 
==See also==
[[File:Integrated_Molecular_Meta-Analysis_of_1,000_Pediatric_High-Grade_and_Diffuse_Intrinsic_Pontine_Glioma_-_graphical_abstract.jpg|thumb|left|Graphical abstract of a molecular meta-analysis of pediatric high-grade gliomas.]]
* [[Glioma]]
 
* [[Brain tumor]]
==Related Pages==
* [[Pediatric oncology]]
* [[Glioblastoma]]
* [[Pediatric brain tumor]]
* [[Radiation therapy]]
* [[Radiation therapy]]
* [[Targeted therapy]]
[[Category:Brain tumors]]
[[Category:Brain tumors]]
[[Category:Pediatric cancers]]
[[Category:Pediatric cancers]]
[[Category:Neurology]]

Latest revision as of 00:41, 6 April 2025

Editor-In-Chief: Prab R Tumpati, MD
Obesity, Sleep & Internal medicine
Founder, WikiMD Wellnesspedia &
W8MD medical weight loss NYC and sleep center NYC

Diffuse midline glioma
Synonyms Diffuse intrinsic pontine glioma (DIPG)
Pronounce N/A
Specialty N/A
Symptoms Headache, nausea, vomiting, balance disorder, vision problems, facial weakness
Complications N/A
Onset Typically in childhood
Duration Progressive
Types N/A
Causes Genetic mutations (e.g., H3 K27M mutation)
Risks Unknown
Diagnosis MRI, biopsy
Differential diagnosis Brainstem glioma, ependymoma, medulloblastoma
Prevention N/A
Treatment Radiation therapy, chemotherapy, palliative care
Medication N/A
Prognosis Poor
Frequency Rare
Deaths N/A


Overview of Diffuse Midline Glioma


Diffuse midline glioma (DMG) is a type of brain tumor that occurs in the midline structures of the central nervous system, such as the thalamus, brainstem, and spinal cord. These tumors are characterized by their infiltrative nature, making them difficult to surgically remove. They are most commonly diagnosed in children and are associated with a poor prognosis.

Classification[edit]

Diffuse midline gliomas are classified as high-grade gliomas, specifically as World Health Organization (WHO) grade IV tumors. They are often associated with a specific genetic mutation in the H3 K27M gene, which is a hallmark of this tumor type. This mutation leads to changes in the epigenetic regulation of gene expression, contributing to the aggressive nature of the tumor.

Pathophysiology[edit]

Genetic mutations associated with diffuse intrinsic pontine glioma.

The pathophysiology of diffuse midline glioma involves the infiltration of tumor cells into the surrounding brain tissue. The H3 K27M mutation results in a global reduction of histone H3 lysine 27 trimethylation, which affects the expression of numerous genes involved in cell growth and differentiation. This mutation is thought to drive the oncogenic process in these tumors.

Clinical Presentation[edit]

Patients with diffuse midline glioma typically present with symptoms related to the location of the tumor. For example, tumors in the brainstem may cause cranial nerve deficits, ataxia, and dysphagia. Tumors in the thalamus can lead to hemiparesis, sensory deficits, and altered mental status.

Diagnosis[edit]

Molecular analysis of pediatric high-grade gliomas.

Diagnosis of diffuse midline glioma is typically made using magnetic resonance imaging (MRI), which reveals a diffusely infiltrative lesion in the midline structures. Biopsy may be performed to confirm the diagnosis and identify the presence of the H3 K27M mutation.

Treatment[edit]

The treatment of diffuse midline glioma is challenging due to the tumor's location and infiltrative nature. Radiation therapy is the mainstay of treatment and can provide temporary relief of symptoms. However, the tumor often recurs, and the overall prognosis remains poor. Chemotherapy has limited effectiveness, and research is ongoing to find more effective treatments.

Prognosis[edit]

The prognosis for patients with diffuse midline glioma is generally poor, with a median survival of less than one year from diagnosis. The presence of the H3 K27M mutation is associated with a particularly aggressive clinical course.

Research Directions[edit]

Research into palliative care options for patients with diffuse intrinsic pontine glioma.

Research into diffuse midline glioma is focused on understanding the molecular mechanisms driving tumor growth and identifying potential therapeutic targets. Novel treatment approaches, including targeted therapies and immunotherapy, are being investigated in clinical trials.

See also[edit]

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