Astrocytoma IDH-mutant [Neurosurgery Wiki]

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====== Astrocytoma IDH-mutant ======


{{rss>https://pubmed.ncbi.nlm.nih.gov/rss/search/1BYJ_3OKYOAbe6rQKQvE0JKh3J0UKvaVO68jUmIf9w1ErF9IgX/?limit=15&utm_campaign=pubmed-2&fc=20231107065252}}

[[Astrocytoma]], [[IDH-mutant]] tumors are [[World Health Organization grade 2]], [[World Health Organization grade 3]], and [[World Health Organization grade 4]] [[brain tumor]]s found in [[adult]]s. They are [[diffuse]] infiltrating [[astrocytic tumor]]s where there is no identifiable border between the tumor and normal [[brain tissue]], even though the borders may appear relatively well-marginated on imaging.

===== General information =====

A [[diffuse astrocytoma]] with a [[mutation]] in either the [[IDH1]] or [[IDH2]] gene. Use of the former term “[[low-grade glioma]]” is discouraged.

Since most diffuse astrocytomas carry the [[IDH]] mutation, historical data (pre-IDH era) regarding what was formerly called [[low-grade astrocytoma]]s (WHO grade II) is reflective of the current category to a limited extent.

These tumors tend to occur in children and young adults. They are relatively rare, comprising only ≈ 5% of primary brain tumors, and 15% of all gliomas. Pediatric (age < 20 years) diffuse astrocytomas ([[IDH mutation]] status not determined) occur at a rate of 0.26 per 100,000, about half that for adult (0.48).

There is a predilection for temporal, posterior frontal and anterior parietal lobes. In the pediatric population, a significant number occur in the [[thalamus]], which is unusual in adults.

Characterized by slow growth. Most present with [[seizure]]s.

===== Classification =====

● [[Astrocytoma IDH-mutant Grade 2]] 

● [[Astrocytoma IDH-mutant Grade 3]] 

● [[Astrocytoma IDH-mutant Grade 4]]

Subtypes of IDH-mutant diffuse astrocytoma.

[[DNA methylation]] patterns of metabolic genes successfully distinguished the molecular subtypes of IDHmut and IDHwt gliomas. Promoter methylation of lactate dehydrogenase A negatively correlated with protein expression and was associated with IDHmut gliomas. Mitochondrial DNA copy number was increased in IDHmut tumours and did not change in recurrent tumours.Hierarchical clustering based on metabolism panel IHC revealed distinct subclasses of IDHmut and IDHwt gliomas with an impact on patient outcome. Further quantification of these markers allowed for the prediction of survival under antiangiogenic therapy.

A mitochondrial signature was associated with increased survival in all analyses, which could indicate tumour subgroups with specific metabolic vulnerabilities
((Braun Y, Filipski K, Bernatz S, Baumgarten P, Roller B, Zinke J, Zeiner PS, Ilina E, Senft C, Ronellenfitsch MW, Plate KH, Bähr O, Hattingen E, Steinbach JP, Mittelbronn M, Harter PN. Linking epigenetic signature and metabolic phenotype in IDH mutant and IDH wildtype diffuse glioma. Neuropathol Appl Neurobiol. 2020 Oct 20. doi: 10.1111/nan.12669. Epub ahead of print. PMID: 33080075.)).



[[Gemistocytic astrocytoma IDH-mutant]] (WHO grade II).

===== Clinical features =====
The most common presenting feature (~40% of cases) is a seizure. This is particularly the case in adults. Headaches are often also present. Depending on the size of the lesion and its location, other features may be present, such as hydrocephalus and focal neurological dysfunction, including personality changes.

===== Diagnosis =====
T2-[[Fluid-attenuated inversion recovery]] ([[FLAIR]]) mismatch sign is now known to be a specific yet insensitive image feature for IDH-mutant, 1p19q non-codeleted astrocytoma. The current study revealed that lesion presenting T2-FLAIR mismatch exhibited extremely long T1- and T2-relaxation time while T2-FLAIR matched lesions showed low to moderate values. On the other hand, IDH-wildtype tumors presented noticeably short T1- and T2-relaxation time. These different relaxation time characteristics seemed to render [[T2-FLAIR mismatch sign]] of becoming such a unique and specific image feature for IDH-mutant, 1p19q non-codeleted astrocytoma
((Kinoshita M, Uchikoshi M, Sakai M, Kanemura Y, Kishima H, Nakanishi K.
T(2)-FLAIR Mismatch Sign Is Caused by Long T(1) and T(2) of IDH-mutant, 1p19q
Non-codeleted Astrocytoma. Magn Reson Med Sci. 2020 Feb 27. doi:
10.2463/mrms.bc.2019-0196. [Epub ahead of print] PubMed PMID: 32101817.
)).

===== Pediatric diffuse astrocytoma =====
see [[Pediatric diffuse astrocytoma]]

===== Pathology =====

==== Histology ====
Low degrees of cellularity with highly differentiated cells and preservation of normal brain elements within the tumor. Calcifications are rare. Anaplasia and mitoses are absent (single mitosis is allowed). Blood vessels may be slightly increased in number. These tumors stain positive for GFAP.
In the absence of [[1p/19q co-deletion]], areas of cells resembling oligodendrogliomas are compatible with the diagnosis.

==== Molecular genetics ====
IDH mutation present by definition. [[ATRX]] & [[TP53 mutation]]s support the diagnosis. Prognostically distinct subgroups based on a number of [[genetic marker]]s have been tentatively identified.

IDH1 / 2 mutated well differentiated diffusely infiltrating glioma with astrocytic features without 1p / 19q codeletion and usually with p53 and / or ATRX mutations.

In the absence of 1p / 19q codeletion, a component morphologically resembling oligodendroglioma is compatible with this diagnosis.

Intrinsic capacity for malignant progression to IDH-mutant anaplastic astrocytoma and eventually to [[IDH-mutant glioblastoma]] (Glia 1995;15:211)
Accounts for approximately 11 - 15% of all astrocytic brain tumors

===== Neuroradiology =====

Usually [[hypodense]] on [[CT]]. Most are [[hypointense]] on [[T1WI]] MRI, and show high-intensity changes on [[T2 weighted image]] that extend beyond the tumor volume.

Most do not enhance on CT or MRI (although up to 40% do, and these may have a worse prognosis).

===== Differential diagnosis =====

Possible imaging differential considerations include:

glioblastoma

may be indistinguishable from grade 4 astrocytoma, IDH-mutant

tends to be in older patients

tends to have a less sizable non-enhancing component

infarction: major vascular territory

cerebritis/encephalitis: herpes simplex encephalitis, ADEM

cortical based tumors: oligodendroglioma, angiocentric glioma

===== Treatment =====

[[Astrocytoma IDH-mutant treatment]]


===== Outcome =====

[[Diffuse astrocytoma IDH Mutant outcome]].