Biomarkers for differentiating grade II meningiomas from grade I: a systematic review

Abstract: IntroductionThere are a number of prognostic markers (methylation, CDKN2A/B) described to be useful for the stratification of meningiomas. However, there are currently no clinically validated biomarkers for the preoperative prediction of meningioma grade, which is determined by the histological analysis of tissue obtained from surgery.Accurate preoperative biomarkers would inform the pre-surgical assessment of these tumours, their grade and prognosis and refine the decision-making process for treatment. This r… Show more

“…Validating clinically useful prognostic markers remains a major challenge in neuro-oncology. The availability of accurate preoperative biomarkers in MGM patients would improve the pre-surgical assessment of these tumors, their grade and clinical prognosis, and help direct treatment decisions [43]. Advances in the identification of biomarkers in liquid biopsies using samples of cerebrospinal fluid and blood should enable the development of less invasive diagnostic and prognostic methods that will also allow the monitoring of treatment efficacy during disease [83].…”

“…Many radiological, plasmatic, histological, and molecular prognostic markers have been put forward to help to stratify MGMs. However, to date there are no clinically validated biomarkers to help inform determination of tumor grade and clinical prognosis [20,43]. Investigation of gene expression features of progressing, recurrent, or grade III MGM tumors revealed that notably aggressive tumor subsets share a substantial group of differentially expressed genes, in addition to identifying genes separating non-recurring from recurrent and malignant grade I or grade II tumors.…”

“…GFAP expression correlated with the stem cell markers CD133, stage specific embryo antigen 4 (SSEA4), and vimentin in cell populations enriched in grade II/III tumors[52].Measurement of protein serum markers has revealed significant increases in amphiregulin (AREG), EGF, HB-EGF and caspase3 in patients with MGM of different grades, helping to establish an MGM protein signature in the blood[53].Epigenetic changes have been put forward as prognostic markers in MGM[2].Enhancer of Zeste homolog-2 (EZH2) and trimethyl histone-3 (H3K27me3), which mediate histone modifications related to chromatin state, have been examined. Low histological levels of H3K27me3 were found by a systematic review as a marker that may aid the differentiation between grade I and grade II tumors[43]. Immunohistochemical analysis of 149 cases of MGM tumors grade I (n = 102) or grade II (n = 47) has indicated that positivity for EZH2 and negativity for H3K27me3 are associated with higher tumor cell proliferation and significantly more common in grade II MGM compared to grade I tumors.…”

“…Also using a proteomic strategy, one group has put forward retinoblastoma associated protein-1 (RB1) as a critical marker to identify grade I MGM tumors with high risk for recurrence[48].Other studies quantifying protein content via multiple techniques have aided in the identification of possible protein MGM biomarkers. Semiquantitative analysis of nuclear expression of karyopherin a2 and chromosome region maintenance protein 1, members of the karyopherin protein family that comprises nucleocytoplasmic shuttling receptors importins and exportins, revealed that expression of these proteins correlated significantly with MGM histological grade and predicted tumor recurrence[49].Expression changes in securin (PTTG1), which prevents sister chromatid separation, and leptin receptor (LEPR) were associated with MGM malignancy[43]. The somatostatin receptor 2A (SST2A) has been proposed as a good immunostain target due to its high sensitivity[50].…”

Receptor Tyrosine Kinases as Candidate Prognostic Biomarkers in Meningioma

“…Validating clinically useful prognostic markers remains a major challenge in neuro-oncology. The availability of accurate preoperative biomarkers in MGM patients would improve the pre-surgical assessment of these tumors, their grade and clinical prognosis, and help direct treatment decisions [43]. Advances in the identification of biomarkers in liquid biopsies using samples of cerebrospinal fluid and blood should enable the development of less invasive diagnostic and prognostic methods that will also allow the monitoring of treatment efficacy during disease [83].…”

“…Many radiological, plasmatic, histological, and molecular prognostic markers have been put forward to help to stratify MGMs. However, to date there are no clinically validated biomarkers to help inform determination of tumor grade and clinical prognosis [20,43]. Investigation of gene expression features of progressing, recurrent, or grade III MGM tumors revealed that notably aggressive tumor subsets share a substantial group of differentially expressed genes, in addition to identifying genes separating non-recurring from recurrent and malignant grade I or grade II tumors.…”

“…GFAP expression correlated with the stem cell markers CD133, stage specific embryo antigen 4 (SSEA4), and vimentin in cell populations enriched in grade II/III tumors[52].Measurement of protein serum markers has revealed significant increases in amphiregulin (AREG), EGF, HB-EGF and caspase3 in patients with MGM of different grades, helping to establish an MGM protein signature in the blood[53].Epigenetic changes have been put forward as prognostic markers in MGM[2].Enhancer of Zeste homolog-2 (EZH2) and trimethyl histone-3 (H3K27me3), which mediate histone modifications related to chromatin state, have been examined. Low histological levels of H3K27me3 were found by a systematic review as a marker that may aid the differentiation between grade I and grade II tumors[43]. Immunohistochemical analysis of 149 cases of MGM tumors grade I (n = 102) or grade II (n = 47) has indicated that positivity for EZH2 and negativity for H3K27me3 are associated with higher tumor cell proliferation and significantly more common in grade II MGM compared to grade I tumors.…”

“…Also using a proteomic strategy, one group has put forward retinoblastoma associated protein-1 (RB1) as a critical marker to identify grade I MGM tumors with high risk for recurrence[48].Other studies quantifying protein content via multiple techniques have aided in the identification of possible protein MGM biomarkers. Semiquantitative analysis of nuclear expression of karyopherin a2 and chromosome region maintenance protein 1, members of the karyopherin protein family that comprises nucleocytoplasmic shuttling receptors importins and exportins, revealed that expression of these proteins correlated significantly with MGM histological grade and predicted tumor recurrence[49].Expression changes in securin (PTTG1), which prevents sister chromatid separation, and leptin receptor (LEPR) were associated with MGM malignancy[43]. The somatostatin receptor 2A (SST2A) has been proposed as a good immunostain target due to its high sensitivity[50].…”

Receptor Tyrosine Kinases as Candidate Prognostic Biomarkers in Meningioma

“…Many radiological, plasmatic, histological, and molecular prognostic markers have been put forward to help to stratify MGMs. However, to date there are no clinically validated biomarkers to help inform the determination of tumor grade and clinical prognosis [ 21 , 44 ]. Investigation of gene expression features of progressing, recurrent, or grade III MGM tumors revealed that notably aggressive tumor subsets share a substantial group of differentially expressed genes, in addition to identifying genes separating non-recurring from recurrent and malignant grade I or grade II tumors.…”

Receptor Tyrosine Kinases as Candidate Prognostic Biomarkers and Therapeutic Targets in Meningioma

Impact on natural history of atypical meningioma after changes in 2016 edition of the world health organization (WHO) classification of central nervous system tumors: a literature review