DNA methylation alterations in grade II- and anaplastic pleomorphic xanthoastrocytoma.

BACKGROUND: Pleomorphic xanthoastrocytoma (PXA) is a rare WHO grade II tumor accounting for less than 1% of all astrocytomas. Malignant transformation into PXA with anaplastic features, is unusual and correlates with poorer outcome of the patients.
METHODS: Using a DNA methylation custom array, we have quantified the DNA methylation level on the promoter sequence of 807 cancer-related genes of WHO grade II (n = 11) and III PXA (n = 2) and compared to normal brain tissue (n = 10) and glioblastoma (n = 87) samples. DNA methylation levels were further confirmed on independent samples by pyrosequencing of the promoter sequences.
RESULTS: Increasing DNA promoter hypermethylation events were observed in anaplastic PXA as compared with grade II samples. We further validated differential hypermethylation of CD81, HCK, HOXA5, ASCL2 and TES on anaplastic PXA and grade II tumors. Moreover, these epigenetic alterations overlap those described in glioblastoma patients, suggesting common mechanisms of tumorigenesis.
CONCLUSIONS: Even taking into consideration the small size of our patient populations, our data strongly suggest that epigenome-wide profiling of PXA is a valuable tool to identify methylated genes, which may play a role in the malignant progression of PXA. These methylation alterations may provide useful biomarkers for decision-making in those patients with low-grade PXA displaying a high risk of malignant transformation.

Background

Pleomorphic xanthoastrocytoma (PXA) is a rare WHO grade II tumor accounting for less than 1% of all astrocytomas. They are usually hemispheric, and often they affect children and young adults (median age 26 years) with a frequent history of chronic epilepsy at presentation [1-3]. The majority of the tumors occur in the supratentorial compartment, mostly in the temporal lobe [1,4]; rarely, they were observed in thalamus, cerebellum, sellar region and spinal cord [1,5-7].

Histologically, PXA shows a pleomorphic appearance, an intense reticulin network and lipid deposits within ovoid and spindled tumor cells. Giant tumor cells, eosinophilic granular bodies and lymphocytic infiltrates are also observed. Immunopositivity for glial fibrillary acidic protein (GFAP) is virtually always encountered. The mitotic activity is absent or very low and MIB-1 labeling index is frequently <1%.

The biological behavior is usually benign with a 10-years survival rate of 70% and a recurrence-free lapse of 61% [8]. Nevertheless, gradeII PXA may undergo malignant transformation in up to 15-20% [8]. Thus, PXA with elevated mitotic activity (≥ 5 mitoses per 10 high-power fields) and/ or presence of necrosis has been classified as “PXA with anaplastic features” [1,8]. In these cases, the rate of recurrence has been observed to be much higher and the survival time clearly shorter [8]. These malignant forms are largely responsible for the mortality rate from the disease at 10 years. This aspect is particularly relevant considering that PXA is often encountered in children and young adults.

Epigenetic alterations are able to modulate gene activity without affecting their nucleotide sequence. Aberrant methylation has been recognized as a hallmark of human cancer, and DNA methylation patterns are altered in all types of cancers analyzed, affecting virtually all cellular pathways trough methylation-mediated silencing of regulator genes such as VHL, p16, E-cadherin, hMLH1, BRCA1 and LKB1, and many others [9,10]. In cancer cells a wide-ranging process leading to global changes in DNA methylation patterns takes place. Specifically, a global hypomethylation process happening mainly at intergenic regions and repetitive sequences, as well as local promoter DNA hypermethylation that affects usually unmethylated CpG-rich DNA sequences mapping to tumor-suppressor genes. Thus, their activity is abrogated by means of transcriptional repression [11,12].

Although an increasing interest about aberrant DNA methylation in gliomas exists, the epigenetic profile of astrocytic tumors remains only partially devised, which is especially true for PXA. Widespread hypomethylation [13] might play a role in the pathogenesis of gliomas through activation of oncogenes, loss of imprinting, or the promotion of genomic instability which, in turn exacerbates the tumorigenic phenotype of the cell. Moreover, the importance of aberrant DNA methylation of CpG island promoter regions in the pathogenesis of gliomas, oligodendrogliomas, ependymomas and pituitary adenomas is highlighted by the observation of hypermethylation of a wide variety of genes associated with tumor suppression (RB1, VHL, EMP3, RASSF1A, CITED4, BLU), cell cycle regulation (p16, p15), DNA repair (MGMT, hMLH1), and tumor invasion and apoptosis (DAPK, TIMP3, CDH1, SOCS3) [13-24]. MGMT is another good example of a DNA repair gene undergoing methylation-mediated inactivation in human cancer [25], including GBM [26].

It has recently become evident that the methylation signature of astrocytic tumors appears to be class-specific. Analyzing a panel of 7 genes (CDKN2B, PTGS2, CALCA, MYOD1, THBS1, TIMP3 and CDH1) Uhlman and colleagues observed differences in the methylation status in astrocytomas WHO grades II, III and IV [27]. Concerning PXA there is almost no data available from the literature reporting on epigenetic signatures and only a specific report focusing on MGMT[28] methylation status has been published so far.

In the present study we have analyzed the DNA methylation profiles of PXA WHO grade II (n = 9) and PXA with anaplastic features (n = 2). Brain tissue obtained by epilepsy neurosurgical procedures in patients without brain tumors (n = 10) and GBM consecutive samples (n = 87, previously analyzed [29]) were included in the DNA methylation analysis. For this purpose, we have investigated the DNA methylation alterations following a microarray-based DNA methylation approach as well as pyrosequencing of selected genes for further validation.

Methods

Patient samples and controls

The study was approved by the Ethics Committee of the School of Medicine, University of Göttingen (project number 11/8/13), and patients provided written informed consent to participate on the study, as well as for publishing the images and clinical information. All PXA (n = 13 tumors, 12 patients) and GBM patients (n = 87) had undergone surgery with the goal of maximal possible tumor resection. One anaplastic PXA (PXA-5) was the local relapse of a grade II PXA (PXA-4), one year after complete tumor resection (Table 1). All patient IDs have been appropriately codified to ensure privacy protection. Normal human adult brain (NB, n = 10) tissue obtained from epilepsy neurosurgical procedures, and post-mortem from healthy individuals was included in the study as normal control. Tumor samples were frozen in liquid nitrogen and stored at –80°C. Tumor tissue was evaluated by experienced neuropathologists according to the 2007 WHO classification criteria. DNA from tumor specimens was isolated applying the QIAamp® DNA Mini Kit (Qiagen, Hilden, Germany). Informed consent for samples and data analysis was obtained from each patient or the patient’s carer. The design of this analysis conforms to standards currently applied in Germany. Survival times were collected for all cases and were calculated from the time of diagnosis to death, or last contact in the case of living patients.

Table 1

Histopathological characterization of PXA patients

PXA patients	Diagnosis	Gender, age	ICH features	Brain localization
			BRAF V600E negative (no mutation)
			CD34 positive.
PXA-1	PXA WHO grade II	18y., female	GFAP positive.	right frontal
			MIB-1:1%
			IDH1 R132H negative (no mutation).
			GFAP positive.
PXA-2	PXA WHO grade II	17y., female	MIB-1: 1%.	right temporal
			No tumor tissue available for BRAF/CD34 characterization
			BRAF V600E positive (mutated)
			CD34 focal positive
PXA-3	PXA WHO grade II	34y., female	GFAP. Positive.	left temporal
			MIB-1: <1%.
			IDH1 R132H negative (no mutation)
			BRAF V600E negative (no mutation)
			CD34 positive
			Mitotic index <5 mitoses/10 HPF
PXA-4 precursor of PXA-5	PXA WHO grade II	59y., male	Immunopositivity for GFAP, S100, MAP2,	right parietal
			vimentin and EMA
			MIB-1: 5-10%
			IDH1 R132H negative (no mutation)
			BRAF V600E negative (no mutation)
			CD34 positive
			Mitotic index >5mitoses/10 HPF
PXA-5	PXA with anaplastic features	59y., male	Immunopositivity for GFAP, S100, MAP2,	right parietal
			vimentin and EMA
			MIB-1: 10-15%
			IDH1 R132H negative (no mutation)
			BRAF V600 E negative (no mutation)
			CD34 positive
PXA-6	PXA with anaplastic features	22y., male	GFAP positive	right temporal
			MIB-1: 5%.
			IDH1 R132H negative (no mutation)
			BRAF V600 E negative (no mutation)
			CD34 positive
PXA-7	PXA WHO grade II	44y., female	Immunopositivity for GFAP	right temporal
			MIB-1: 1%.
			IDH1 R132H negative (no mutation)
			BRAF V600 E negative (no mutation)
			CD34 positive
PXA-8	PXA WHO grade II	20y., male	Immunopositivity for GFAP.	right parieto-occipital
			MIB-1: <1%.
			IDH1 R132H negative (no mutation)
			BRAF V600 E negative (no mutation)
			CD34 positive
PXA-9	PXA WHO grade II	78y., female	Immunopositivity for GFAP.	right temporo-parietal
			MIB-1: <1%.
			IDH1 R132H negative (no mutation)
PXA-10	PXA WHO grade II	15y., female	BRAFV600E negative (no mutation)	right occipital
			CD34 positive
			Immunopositivity for GFAP.
			MIB-1: 1%.
PXA-11	PXA WHO grade II	52y., male	BRAFV600E negative (no mutation)	left occipital
			CD34 positive
			Immunopositivity for GFAP.
			MIB-1: < 1%.
PXA-12	PXA WHO grade II	17 y., male	BRAFV600E positive (mutated)	left parietal
			CD34 negative
			Immunopositivity for GFAP.
			MIB-1: 1%.
PXA-13	PXA WHO grade II	37 y., female	BRAFV600E positive (mutated)	right parietal
			CD34 focal positive
			Immunopositivity for GFAP
			MIB-1: < 1%

Patients undergoing surgical resection of diagnosed pleomorphic xanthoastrocytoma of diverse grade were investigated for specific features characteristic of this tumor type.

DNA methylation profiling using universal BeadArrays

DNA methylation profiling was performed with the GoldenGate Methylation Cancer Panel I assay (Illumina Inc., San Diego CA) on a total of 8 WHO grade II PXA, 2 anaplastic PXA, 87 GBM samples and 10 normal brain tissue samples as control. The panel was developed to assay 1,505 CpG sites selected from 807 cancer-related genes, including oncogenes and tumor suppressor genes, imprinted genes, genes involved in various signaling pathways, and those responsible for DNA repair, cell cycle control, metastasis, cell migration and invasion, differentiation and apoptosis.

Methylation assay was performed following manufacturer’s instructions. Briefly, bisulphite conversion of DNA samples was carried out using the EZ DNA methylation kit (Zymo Research, Orange, CA). After bisulphite treatment, the remaining assay steps were performed using Illumina-supplied reagents and conditions. We excluded 84 CpGs mapping to X chromosome to avoid gender-specific bias. Additionally, we evaluated the detection probabilities (comparing signal intensities against background noise) for all CpGs and excluded those probes with values of P > 0.01 in more than 10% of cases. In the final analysis, 1,390 CpGs mapping to 762 genes were used in the subsequent statistical analyses.

Data analysis and definition of DNA methylation patterns

For further analyses, only the 1,390 autosomal CpGs that met our quality criteria were used. In order to distinguish groups of patients according to their DNA methylation patterns, we selected only the informative probes, that is, considering those probes with SD > 0.05 between patients. We sought to identify genes affected by DNA hypermethylation in the precursor grade II PXA (PXA-4) that are further maintained in the anaplastic relapsed tumor (PXA-5) and in the analyzed glioblastoma samples, in comparison with the average values of grade II PXA cases and normal brain. The glioblastoma patients used in this study for comparison purposes were described in detail elsewhere [29]. To this aim, we set up a threshold increment of 30% in methylation, as has been previously reported to result in expression differences [30], when comparing the averaged anaplastic and precursor PXA samples (PXA-4 and PXA-5), the averaged grade II PXA cases (PXA1-3) and the GBM patients. Candidates that exhibit (i) an unmethylated status in normal brain (β ≤ 0.2, SD < 0.1), (ii) a difference in DNA methylation (DM) between averaged grade II and anaplastic cases higher than DM > 30%, and (iii) are also methylated in the averaged GBM group (β > 0.4, SD < 0.1), were selected for validation. Furthermore, we investigated DNA hypermethylation events specific for precursor (PXA-4) and anaplastic (PXA-5) PXA cases that retained normal levels in the rest of the samples, including GBM, and therefore represent specific DNA hypermethylation events of this tumor entity.

Pyrosequencing and bisulfite genomic sequencing

In order to validate the results obtained from the DNA methylation array, pyrosequencing was performed on selected candidate genes as has been previously described, on grade II PXA samples, anaplastic PXA samples (PXA 4-6), as well as in glioblastoma and normal brain samples.

Genomic DNA was converted using the EZ DNA Methylation Gold kit (Zymo Research, Orange, CA, USA). DNA methylation in clinical samples was studied by pyrosequencing, which was performed on bisulphite-treated DNA extracted from formalin-fixed paraffin-embedded (FFPE) samples. Specific primers were designed using the PyroMark Assay Design Software (QIAGEN-version 2.0.01.15) for to examine the methylation status of particular CG sites covering the candidate genes promoter regions (Additional file 1: Table S1). Pyrosequencing primer sequences were designed to hybridize with CpG-free sites to ensure methylation-independent amplification. PCR was performed with primers biotinylated to convert the PCR product to single-stranded DNA templates. We used the Vacuum Prep Tool (Biotage) to prepare single-stranded PCR products according to the manufacturer’s instructions. Pyrosequencing reactions and quantification of DNA methylation were performed in a PyroMark Q96 System version 2.0.6 (QIAGEN) including appropriate controls. For bisulfite genomic sequencing of MGMT promoter sequence, specific sets of primers were designed using the Methyl Primer Express software (Applied Biosystems) (Fwd: GGTAAATTAAGGTATAGAGTTTTAGG; Rev: ACCCAAACACTCACCAAAT), and a minimum of eight clones were sequenced. It allows a positive display of 5- methyl cytosines in the gene promoter after bisulfite modification as unmethylated cytosines appear as thymines, while 5-methylcytosines appear as cytosines in the final sequence.

Statistical analysis and Gene ontology analysis of differentially methylated genes

In order to define DNA methylation patterns between and inside groups of samples, statistical comparisons were performed. Mann-Whitney U-test (False Discovery Rate, FDR < 0.05) and Fisher’s exact test were performed to compare differences between groups of glioblastoma and normal brain sample sets, depending on the data types of the variables being examined. DNA methylation values of glioblastoma and normal brain samples were averaged for comparative purposes. Furthermore, the genes found differentially methylated on anaplastic PXA cases exhibited a SD < 0.1 in the GBM cohort, and were all detected as significantly hypermethylated in a large series study [29]. Due to sample size, average values and standard deviation of PXA were compared to the values of DNA methylation patterns of glioblastoma and normal brain samples sets. Analyses were performed with SPSS (version 11.5, SPSS Inc., Chicago, IL., USA). GO enrichments for biological process ontology were calculated using the GOStats package under R statistical software. Those terms below an adjusted (Benjamini-Hochberg correction) p-value below 0.01 were selected and considered significant.

Results

Clinical, histological and genetic characterization of patient samples

In PXA patients, the male: female ratio was 1:0.8, in GBM patients was 1:0.7, and in control cases 1:1.3. The median age at diagnosis was in PXA patients 26 years (Table 1), in GBM patients 60.6 years, and in control cases 52.1 years. All PXA patients presented with a 4-8-week history of epileptic seizures, dizziness and headache, after that MRI diagnosis (Figure 1) was performed and the tumors were diagnosed. All PXA patients underwent complete surgical resection. The one patient diagnosed with a PXA with anaplastic features (PXA-5) was the local relapse of one of the grade II PXA (PXA-4), one year after complete tumor resection. Albeit being an outlier for the median age at diagnosis, cases of PXA diagnosed in adults and elderly patients have been documented previously as well [31,32]. After resection of the anaplastic PXA, adjuvant fractionated radiotherapy (59Gy) and chemotherapy with temozolomide were performed. All analyzed PXA show the typical characteristic of this type of lesion (Table 1). Figure 1 shows comparative immunohistochemical investigations with hematoxylin & eosin (HE), glial fibrillary acidic protein (GFAP) and MIB-1 in the cases of grade II PXA and associated anaplastic PXA, and illustrative examples of histological assessment of BRAF V600E mutation (PXA-3) and CD34 immunoreactivity (PXA-1) are included on Additional file 2: Figure S1. Patients with glioblastoma had undergone standard therapy with gross-total surgical resection followed by adjuvant fractionated radiotherapy (median 59 Gy) and chemotherapy with temozolomide (Stupp regime).

Figure 1

Immunohistochemical characterization of grade II PXA and associated anaplastic PXA. Upper row: T1-weighted, gadolinium-enhanced axial MRI showing the right parietal PXA at presentation (A), after surgical resection (B) and at the time of local relapse (C). Lower row: Photomicrographs showing histological and immunohistochemical features of the grade II PXA and grade III PXA with anaplastic features (HE, GFAP and MIB-1. The last one showed a higher positivity of 20% in the anaplastic PXA, whereas it was 10% in the grade II PXA).

Detection of candidate-genes differentially methylated in malignant PXA

Aiming to recognize changes attributable to malignant transformation of PXA into GBM, we sought to identify specific changes between grade II and anaplastic PXA cases. To this end, we explored the DNA methylation profiles in PXA patients, restricting the analysis to genes being unmethylated (β < 0.2, SD < 0.1) in NB and methylated in GBM (β > 0.4, SD < 0.1) in any of the probes. As a result, a pattern of progressive hypermethylation was recognized, allowing the categorization of the analyzed cases in three groups: (1) grade II PXA samples without further recurrence; (2) anaplastic PXA cases and the corresponding grade II PXA precursor tumor; and (3) GBM (Figure 2). PXA samples showed a progressive increase in the frequency of hypermethylated CpGs correlating with the presence of malignant features (>5 mitoses pro high-power field and/or necrosis). A considerable number of hypermethylated genes stand out the anaplastic PXA cases and the one grade II PXA precursor tumor (PXA-4), whereas no hypomethylation events were detected. Interestingly, we found a series of genes showing DNA hypermethylation (DM > 30%) at gene promoters restricted to the malignant PXAs (Figure 2) as compared with grade II samples. Specifically, this set of genes (CD81, HCK, HOXA5, ASCL2, TES, AHR, DIO3, FZD9 and MOS) exhibited large DNA methylation increments when comparing grade II PXAs and grade II PXA-4 case precursor of the anaplastic PXA-5; were consistently methylated in anaplastic PXA and in GBM patients as well (β > 0.4) but unmethylated (β < 0.2) in normal brain, thus indicating an association between increasing rate of hypermethylation events and the presence of histological malignant features.

Figure 2

DNA methylation alterations on grade II and malignant PXA samples. Based on methylation frequencies, tumor samples can be categorized on three groups: (1) grade II PXA (PXA 1-3); (2) precursor and anaplastic PXA (PXA 4-5) and (3) GBM. PXA-4 and PXA-5 samples show increased DNA methylation when compared with grade II PXA. A set of genes was observed to be commonly hypermethylated in anaplastic PXA, its grade II PXA precursor and GBM, whereas being unmethylated in all other grade II PXA and normal brain (squared in blue). Color scale shows methylated (red) and unmethylated (green) status of the probes.

Pyrosequencing validation of the investigated genes

DNA methylation values obtained from the GoldenGate methylation assay were validated by pyrosequencing in those samples used for the discovery phase (PXA 4, 5), as well as on an independent set of validation samples (PXA 6-11). Specifically, we carried out validation of the candidate genes differentiating grade II PXA cases and anaplastic PXAs (including the one corresponding precursor grade II PXA), which were hypermethylated in GBM cases as well. For technical limitations, from the nine genes identified, pyrosequencing could be performed for five of them (CD81, TES, HOXA5, ASCL2, HCK). The results obtained on the GoldenGate assay (Figure 3A) were highly consistent with those obtained by pyrosequencing on the discovery and validation samples (Figure 3B). The five genes exhibited comparable DNA hypermethylation gains in the anaplastic PXA cases and were unmethylated in normal brain and grade II PXA cases (Figure 3B). In addition, analysis of MGMT promoter hypermethylation was also performed, and comparable promoter DNA hypermethylation was found in the anaplastic PXA samples as well as in the one grade II tumor further relapsing as an anaplastic PXA (Additional file 3: Figure S2).

Figure 3

Validation of DNA hypermethylation events in malignant transformation of PXA. Representation of DNA methylation levels exhiited by the five selected markers on the GoldenGate DNA methylation assay (a) and validated by pyrosequencing on an independent set of samples (b).

Gene ontology (GO) analysis of genes differentially methylated in malignant PXA

In order to gain insights into the impact of DNA hypermethylation on each of the established categories, we extracted the specific DNA methylation increases for each sample set, taking the DNA methylation profile of normal brain (NB) as a reference. By comparing normal brain and malignant PXA cases, we identified 140 probes mapping to 116 unique genes gaining methylation (β > 30%; NB < 20%) in the malignant PXA and precursor lesion (Additional file 4: Table S2), and 49 probes (42 unique genes) showed hypermethylation specifically in the anaplastic PXA cases. These genes retained an unmethylated status in GBM and grade II PXA, indicating that these DNA hypermethylation changes are inherent to these tumor samples. As genes studied with the methylation-specific BeadArray were selected for their involvement in cancer, by definition they will be enriched for functions deregulated in cancer. Even taking this limitation into consideration, gene ontology analyses of the changes identified between malignant PXA and normal brain, were observed to be preferentially affecting genes involved in neuronal regulation, including response to stimulus or protein phosphorilation; in addition to pathways related with oncogenic progression, including cell motility and cell adhesion -cadherin and integrin signaling pathways-, cell proliferation -Wnt signaling components-, and angiogenesis among the affected signaling circuits (Figure 4). These pathways were considerably overlapping with those affected by DNA hypermethylation in GBM patients, as has been previously described [29]. When focusing on changes affecting grade II PXA, only 23 probes mapping to 19 unique genes where found differentially methylated in comparison with NB (Additional file 5: Table S3) and no enrichment in biological functions resulted, confirming their benign nature.

Figure 4

Gene ontology analysis of the genes hypermethylated in anaplastic PXA. When comparing the precursor grade II (PXA-4) and anaplastic grade III (PXA-5) PXA tumors with average methylation observed in normal brain, specific gains of methylation involve specific nervous system pathways, as well as other related with oncogenic potential such as cell proliferation, motility and differentiation. Scale bar at the bottom indicates number of genes involved on each biological process. Annotated biological processes were selected among the statistically significant GO-terms resulting from the analysis (BH-adjusted p value < 0.01).

Discussion

In the present study, we sought to explore the epigenetic alterations associated to grade II PXA and those occurring associated with the acquisition of histological malignant features, such as mitoses (as above mentioned) and/or necrosis. PXA WHO grade II is a slow-growing astrocytic tumor, which is considered benign and presents a 10-years survival rate of 70% and a recurrence-free lapse of 61% [8,33]. However, up to 20% PXA will develop anaplastic features and may further progress to secondary glioblastoma, exhibiting much more aggressive phenotype and dropping significantly survival rates with a median survival time of 15 months [8].

DNA methylation changes, and moreover those associated to malignant transformation of grade II PXA, had not been investigated previously. In the present study, we analyzed DNA hypermethylation on the promoter sequences of a panel of cancer-related genes in order to investigate epigenetic alterations associated to this process. To our knowledge, only MGMT methylation status has been previously studied in PXA [28], while the data on the epigenetic regulation of CD81, HCK, TES, HOXA5 and ASCL2 in PXA patient have not been documented before. Despite the low cohort size, we observed comparable increases on the DNA methylation levels in independent samples used for validation. Interestingly, when analyzing differences in DNA methylation affecting each sample type, we found a much higher number of changes occurring in anaplastic PXA and the grade II precursor tumor (116 genes) as compared with fewer occurring in all other grade II PXA (19 genes) samples (Additional file 4: Table S2 and Additional file 5: Table S3). Accumulation of genetic alterations has been found associated to the pathogenesis and progression of astrocytic tumours [34], and concomitantly, accumulation of epigenetic lesions is present as well. Among the changes identified, we observed a set of DNA hypermethylation events in anaplastic PXA, its corresponding precursor grade II tumor, overlapping with DNA methylation alterations also found in GBM (Figure 3). Several studies have previously reported frequent epigenetic disruption of CD81 in glioblastoma [29,35], supporting its tumor-suppressor roles in this cancer type. Moreover, promoter hypermethylation of the gene coding for Testin (TES) was also reported by us [29] and others [36,37]. Its role acting as a negative regulator of cell growth supports a role for tumor-suppression, as has been proposed in diverse cancer types including ovarian cancer [38] and acute lymphocytic leukemia [39]. DNA hypermethylation of the transcription factor ASCL2 has been identified in other cancers [40] and is involved in the regulation of gene expression in the central and peripheral nervous system [41]. Additionally, the pathways deregulated by DNA methylation changes (Figure 4) showed great consistency with those targeted in GBM, and are concordant with previous observations reported by us and others [29,37]. This data suggest that malignant progression of grade II PXA towards anaplastic relapses could be triggered by molecular mechanisms also involved in GBM. This change of methylation status during malignant progression could be also confirmed at the end-point of anaplastic PXA cases (Additional file 4: Table S2). The subset of genes validated in our study (CD81, TES, HOXA5, ASCL2, and HCK) were not affected by DNA hypermethylation in the grade II patients analyzed, and therefore could be specifically associated to the progression of the disease in this patient (Figure 2 and 3). On the other hand, we cannot rule out that the epigenetic alterations observed could be attributable to individual-specific DNA methylation phenomena; however, methylation of these genes has also been found in GBM in larger population studies [29,35-37,42], thus indicating that they are most probably involved in the pathogenesis and malignant progression of astrocytic tumors.

Of note, considerable promoter hypermethylation was found in MGMT promoter region, both in the precursor and the anaplastic tumors (Additional file 3: Figure S2). A recent report analyzing the methylation status of MGMT in 11 grade II PXA concluded that this event was infrequent in PXA [28]. Albeit this finding needs to be assessed in larger population studies, the extensive promoter hypermethylation we found in the anaplastic PXA patient supported the indication of chemotherapy with temozolomide in a similar pattern as it is in other malignant tumors of astrocytic lineage [40].

The pathogenesis of PXA is largely unknown. Nevertheless, a series of molecular studies have described genomic alterations in PXA patients [28,42-48] Chromosomal gains and losses have been associated with PXA pathogenesis, although prevalent losses -frequently involving chromosomes 7 and 9- were observed in grade II astrocytomas of poor prognosis [28,42-44], accounting for a potential inactivating mechanism of tumor suppressor genes. Further genetic studies have also unveiled the high frequency of BRAF V600E mutations in WHO grade II PXAs and PXAs with anaplastic features (65 and 66% of cases, respectively) [48], as well as homozygous deletion of CDKN2A/p14(ARF)/CDKN2B in six out of ten tumors analyzed in a different cohort [46]. DNA methylation alterations have been scarcely analyzed in PXA. Marucci and colleagues examined MGMT promoter methylation in 11 grade II PXA [28], but, to our knowledge, no additional studies have been done to examine epigenetic alterations in this setting. Methylation markers in a variety of human cancers have proved trustworthy in clinical trials for diagnostic and prognostic purposes. In other solid tumors, DNA methylation markers have shown their relevance in early diagnosis, prognosis of tumor progression, or response to therapy and chemo-resistance [49,50]. For instance, DNA methylation profiles were shown to correlate with clinical parameters; specifically hypermethylation of GATA6 transcription factor was found associated with poor survival in GBM patients [35], or hypermethylation of the pro-apoptotic CASP8 is a differential feature of GBM relapses [51]. Though limited by the size of the populations analyzed, our study suggests that DNA hypermethylation mediated silencing of tumor suppressor genes in PXA could be a relevant event contributing to malignant progression, as also defined by other diffuse astrocytic tumors. The diagnosis of grade II PXA at a high risk to recur as a malignant tumor widens the therapeutic window for intervention, in the form of early onset of adjuvant chemotherapy, even at a grade II tumor stage. Thus, in order to depict biomarkers with prognostic value on PXA patients, broader studies should be undertaken in this and further low-grade astrocytic tumors with risk to undergo malignant transformation.

Conclusions

In the present study, though limited by sample constraints, we have identified promoter hypermethylation of CD81, HCK, HOXA5, ASCL2 and TES genes in anaplastic cases compared to grade II PXA. These events could potentially contribute to malignant progression of PXA, since similar methylation increases were not observed in grade II cases. Moreover, hypermethylation of these genes were observed in GBM as well, suggesting widespread epigenetic mechanisms of malignancy. This study should be further confirmed in larger population series aiming to identify clinically relevant biomarkers for the management of the disease.

Competing interests

The authors declare that they have no competing interests.

Authors’ contributions

RM and FJC designed the study, performed DNA methylation analyses, coordinated tissue sampling and wrote the manuscript. MV and SR carried out pyrosequencing experiments. AG carried out bioinformatic analyses. VR and ME participated in the design of the study and helped drafting the manuscript. MK and GS coordinated tissue sampling and analyzed clinical data. WP and AB performed the neuropathological characterization of the samples and the IHC of the tissues. All authors read and approved the manuscript as submitted.

Pre-publication history

The pre-publication history for this paper can be accessed here:

http://www.biomedcentral.com/1471-2407/14/213/prepub

Additional file 1: Table S1

Pyrosequencing primers used for the validation of selected candidates.

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Additional file 2: Figure S1

BRAF V600E positivity observed in patient PXA-3 (left image); and CD34 positivity detected in patient PXA-1 (right image).

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Additional file 3: Figure S2

Bisulphite genomic sequencing of MGMT promoter sequence in the precursor (PXA-4) and anaplastic (PXA-5) samples. Squares represent CpG sites along the promoter sequence, displaying methylated (black) or unmethylated (white) status.

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Additional file 4: Table S2

List of hypermethylated genes in the anaplastic PXA cases.

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Additional file 5: Table S3

List of hypermethylated genes in benign PXA cases.

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