Skip to main content
Advertisement
Browse Subject Areas
?

Click through the PLOS taxonomy to find articles in your field.

For more information about PLOS Subject Areas, click here.

  • Loading metrics

Prevalence of c-KIT Mutations in Gonadoblastoma and Dysgerminomas of Patients with Disorders of Sex Development (DSD) and Ovarian Dysgerminomas

  • Remko Hersmus,

    Affiliation Department of Pathology, Erasmus MC - University Medical Center Rotterdam, Josephine Nefkens Institute, Daniel den Hoed Cancer Center, Rotterdam, The Netherlands

  • Hans Stoop,

    Affiliation Department of Pathology, Erasmus MC - University Medical Center Rotterdam, Josephine Nefkens Institute, Daniel den Hoed Cancer Center, Rotterdam, The Netherlands

  • Gert Jan van de Geijn,

    Affiliation Department of Pathology, Erasmus MC - University Medical Center Rotterdam, Josephine Nefkens Institute, Daniel den Hoed Cancer Center, Rotterdam, The Netherlands

  • Ronak Eini,

    Affiliation Department of Pathology, Erasmus MC - University Medical Center Rotterdam, Josephine Nefkens Institute, Daniel den Hoed Cancer Center, Rotterdam, The Netherlands

  • Katharina Biermann,

    Affiliation Department of Pathology, Erasmus MC - University Medical Center Rotterdam, Josephine Nefkens Institute, Daniel den Hoed Cancer Center, Rotterdam, The Netherlands

  • J. Wolter Oosterhuis,

    Affiliation Department of Pathology, Erasmus MC - University Medical Center Rotterdam, Josephine Nefkens Institute, Daniel den Hoed Cancer Center, Rotterdam, The Netherlands

  • Catharina DHooge,

    Affiliation Department of Pediatrics, Division of Pediatric Hemato-Oncology, University Hospital Ghent, Ghent, Belgium

  • Dominik T. Schneider,

    Affiliation Clinic of Pediatrics, Municipal Hospital Dortmund, Dortmund, Germany

  • Isabelle C. Meijssen,

    Affiliation Molecular Diagnostics, Department of Pathology, Erasmus MC - University Medical Center Rotterdam, Josephine Nefkens Institute, Rotterdam, The Netherlands

  • Winand N. M. Dinjens,

    Affiliation Molecular Diagnostics, Department of Pathology, Erasmus MC - University Medical Center Rotterdam, Josephine Nefkens Institute, Rotterdam, The Netherlands

  • Hendrikus Jan Dubbink,

    Affiliation Molecular Diagnostics, Department of Pathology, Erasmus MC - University Medical Center Rotterdam, Josephine Nefkens Institute, Rotterdam, The Netherlands

  • Stenvert L. S. Drop,

    Affiliation Department of Pediatric Endocrinology, Erasmus MC - University Medical Center Rotterdam, Sophia Children’s Hospital, Rotterdam, The Netherlands

  • Leendert H. J. Looijenga

    l.looijenga@erasmusmc.nl

    Affiliation Department of Pathology, Erasmus MC - University Medical Center Rotterdam, Josephine Nefkens Institute, Daniel den Hoed Cancer Center, Rotterdam, The Netherlands

Abstract

Activating c-KIT mutations (exons 11 and 17) are found in 10–40% of testicular seminomas, the majority being missense point mutations (codon 816). Malignant ovarian dysgerminomas represent ∼3% of all ovarian cancers in Western countries, resembling testicular seminomas, regarding chromosomal aberrations and c-KIT mutations. DSD patients with specific Y-sequences have an increased risk for Type II Germ Cell Tumor/Cancer, with gonadoblastoma as precursor progressing to dysgerminoma. Here we present analysis of c-KIT exon 8, 9, 11, 13 and 17, and PDGFRA exon 12, 14 and 18 by conventional sequencing together with mutational analysis of c-KIT codon 816 by a sensitive and specific LightCycler melting curve analysis, confirmed by sequencing. The results are combined with data on TSPY and OCT3/4 expression in a series of 16 DSD patients presenting with gonadoblastoma and dysgerminoma and 15 patients presenting pure ovarian dysgerminomas without DSD. c-KIT codon 816 mutations were detected in five out of the total of 31 cases (all found in pure ovarian dysgerminomas). A synonymous SNP (rs 5578615) was detected in two patients, one DSD patient (with bilateral disease) and one patient with dysgerminoma. Next to these, three codon N822K mutations were detected in the group of 15 pure ovarian dysgerminomas. In total activating c-KIT mutations were found in 53% of ovarian dysgerminomas without DSD. In the group of 16 DSD cases a N505I and D820E mutation was found in a single tumor of a patient with gonadoblastoma and dysgerminoma. No PDGFRA mutations were found. Positive OCT3/4 staining was present in all gonadoblastomas and dysgerminomas investigated, TSPY expression was only seen in the gonadoblastoma/dysgerminoma lesions of the 16 DSD patients. This data supports the existence of two distinct but parallel pathways in the development of dysgerminoma, in which mutational status of c-KIT might parallel the presence of TSPY.

Introduction

c-KIT belongs to the Type III tyrosine kinase receptor family, which also includes the platelet-derived growth factor receptor (PDGFR) and macrophage-colony stimulating receptor (M-CSFR). The ligand for c-KIT is the stem cell factor (SCF, KITLG) and the SCF-KIT pathway regulates the differentiation of melanocytes, red blood cells, mast cells, interstitial cells of Cajal, and germ cells [1], [2], [3]. Moreover, this pathway is important in the survival of primordial germ cells (PGCs) [4], [5]. Expression of c-KIT and gain-of-function mutations in c-KIT has been found in mastocytosis, leukemia and gastro-intestinal stromal tumors (GIST) [6], [7], [8]. In GIST activating mutations in c-KIT exons 8, 9, 11, 13 and 17 are found in 75–80% of cases, mutations in PDGFRA exons 12, 14 and 18 in 5–8%, and they are mutually exclusive (for review [9]).

Activating c-KIT mutations have also been found in human germ cell tumors/cancers (GCC), and 10–40% of testicular seminomas harbor activating mutations in exons 11 and 17. About two thirds are missense point mutations at codon 816 [2], [10], [11], [12], which are also found in almost all mast cell tumors [13]. Noteworthy is that activating c-KIT mutations have been found in a subset of tumors showing the same histology as testicular seminoma, namely; mediastinal seminomas, intracranial germinomas and ovarian dysgerminomas [14], [15], [16]. Next to mutations in c-KIT, amplification of chromosome 4q12, harboring the c-KIT gene, has been described in testicular GCC, likely related to the progression to seminoma [10]. Malignant ovarian dysgerminomas represent approximately 3% of all ovarian cancers in Western countries, and share a morphological resemblance, and show a similar pattern of chromosomal aberrations [17] with testicular GCC. Families with both ovarian and testicular GCC have been reported, suggestive of a common etiology [18].

Disorders of Sex Development (DSD), previously referred to as intersex, are a congenital condition in which there is an atypical development of the chromosomal, gonadal or anatomical sex [19]. DSD patients with gonadal dysgenesis or hypovirilization harboring Y-chromosomal material in their karyotype have an increased risk of developing GCC (for review [20], [21]). The precursor lesion in the dysgenetic gonads of these patients is the gonadoblastoma (GB), or carcinoma in situ (CIS), depending on the level of gonadal testicularization [22]. The invasive component is the dysgerminoma in most cases (genetically the counterpart of the seminoma of the testis). For the development of GB the presence of the GonadoBlastoma locus on the Y-chromosome (GBY) is imperative, with the testis specific protein, Y-linked (TSPY) gene being the most likely candidate in this region. TSPY expression is linked to the proliferation and survival of germ cells, and expression is increased in CIS, GB and sometimes seminoma [23]. The octamer-binding protein 3 (OCT3/4, POU5F1) is specifically expressed in all GCC with pluripotent potential, as well as in the neoplastic precursor lesions CIS and GB [24], [25]. Germ cells residing in an unfavorable environment, as is the case in DSD, might escape cell death by prolonged expression of both OCT3/4 and TSPY. If mutations in c-KIT or PDGFRA play a significant role in the development of GB and the development of dysgerminoma in DSD patients is not clear so far because of the lack of multiple studies.

Here we report the analysis of activating mutations in codon 816 of c-KIT in 31 patients with a GB and/or dysgerminoma by LightCycler analysis, together with conventional sequence analysis of c-KIT exons 8, 9, 11, 13 and 17, and PDGFRA exons 12, 14 and 18, mutations in which are frequently found in GIST. These results are linked with karyotype, histology of the gonads, expression of TSPY in the tumors and putative role of the mutations found in the etiology of the disease.

Materials and Methods

Tissue Samples and Immunohistochemistry

In total 31 cases, consisting of eleven cases of GB, fifteen cases of DG and eight cases of GB with DG were retrieved from the archives (Table 1). Collected tissue samples were diagnosed according to WHO standards [26] by an experienced pathologist (JWO). Use of tissue samples for scientific reasons was approved by the Medical Ethical Committee ErasmusMC (MEC 02.981 and CCR2041). Patients gave their verbal consent that left over material, after a diagnostic procedure, can be used for scientific purposes. This agreement is not documented, as agreed upon by the MEC. If patients chose to not consent, it is specifically indicated in the clinical files, and samples were excluded. This consent procedure was used according to the “Code for Proper Secondary Use of Human Tissue in the Netherlands.”

thumbnail
Table 1. Overview mutations found and immunohistochemistry.

https://doi.org/10.1371/journal.pone.0043952.t001

Immunohistochemistry was performed on paraffin-embedded tissue sections of 3-µm thickness. After deparaffinization and 5 min. incubation in 3% H2O2 to inactivate endogenous peroxidase activity, antigen retrieval was carried out by heating under pressure of up to 1.2 bar in an appropriate buffer; 0.01 M sodium citrate (pH 6) or 0.01 M EGTA, 0.01 M TRIS (pH 9). After blocking endogenous biotin using the avidin/biotin blocking kit (SP-2001, Vector Laboratories, Burlingame, CA, USA), the sections were incubated for either 2 hrs at room-temperature (OCT3/4, c-KIT (CD117) or overnight at 4°C (TSPY). Appropriate biotinylated secondary antibodies were used for detection and were visualized using the avidin-biotin detection and substrate kits (Vector Laboratories). The antibodies used directed against OCT3/4, TSPY and c-KIT have been described before [27], [28], [29].

DNA Isolation and c-KIT Codon 816 Mutational Screen

DNA was isolated from formalin-fixed-paraffin-embedded material using a standard protocol, percentage of tumor present in each sample was over 50% unless indicated otherwise (Table 1). In brief, 10 slices of 10-µm thickness were cut and incubated three times with xylene for at least 30 min at RT, after which the pellet was washed each time with ethanol. Lysisbuffer consisting of 10 mM TRIS, 100 mM NaCl, 5 mM EDTA, 1% SDS and 1 mM CaCl2 together with 10 mg/ml proteinase-K was added, and the sample was incubated for 16 hrs at 50°C, while shaking at 1200 rpm. DNA was subsequently extracted by standard phenol/chloroform extraction and ethanol precipitation. DNA was dissolved in 10 mM TRIS with 1 mM EDTA. DNA quality and concentration was checked on the Nanodrop 1000 (ThermoScientific, Wilmington, DE, USA).

50 ng of DNA from each sample was screened for c-KIT D816V, D816H, D816Y mutations using a melting-curve based LightCycler assay (Roche Diagnostics, Mannheim, Germany) with forward primer KIT816For, CAGCCAGAAATATCCTCCTTACT; or KIT816 ForA, CTTTTCTCCTCCAACCTAATAG; reverse primer KIT816Rev, TTGCAGGACTGTCAAGCAGAG; and hybridization probes c-KIT-anchor, LC640-ATGTGGTTAAAGGAAACGTGAGTACCCA–PH; c-KIT-sensor VAL, AGCCAGAGTCATCAAGAATGATTCTA–FL; c-KIT-sensor TYR, AGCCAGACACATCAAGAATGATTCTA–FL; c-KIT-sensor HIS, AGCCAGATACATCAAGAATGATTCTA. To suppress wild type sequences, all reactions were performed with and without addition of a locked nucleic acid (LNA), c-KIT probe GCCAGAGACATCAAGAATG (all primers produced by TIB molbiol, Berlin, Germany). Mixing experiments showed that with the addition of LNA to block wild type sequence, the lower limit of detection was 20 fg of mutant DNA in 50 ng of wild type DNA, and routinely 20 pg of mutant DNA could be detected (data not shown). As a control, samples containing the c.816 mutation under investigation were included in each experiment and were analyzed with and without LNA, together with the experimental samples. The PCR reaction was carried out in a 20 µL volume with 0.5 µM each of forward, reverse, anchor and appropriate sensor probe, 0.01 µM of LNA, 3 mM MgCl2 and 2 µL LightCycler Fast-Start DNA Master HybProbe mix. Reactions were run on a LightCycler Instrument (Roche Diagnostics, Almere, The Netherlands). Amplification was performed with 45 cycles using 60°C annealing temperature. Final melting curve analysis was started at 40°C up to 95°C with a slope of 0.2°C /second and continuous detection with channel F2/F1. Lightcycler data was analyzed using the LightCycler 3.0 software (Roche Diagnostics). Samples showing an aberrant melting curve were run at least in duplicate.

Sequence Analysis

All cases found to be positive in the c-KIT c.816 screen were confirmed by sequence analysis. Approximately 100 ng of PCR product was treated with ExoSAP-IT (GE Healthcare Life Sciences, Piscataway, NJ, USA) following manufacturers instructions, and directly sequenced with 3.3 pmol of each forward and reverse primer using the Big Dye terminator Cycle Sequencing Kit (Applera, Darmstadt, Germany). After initial denaturation at 95°C for 5 min, 25 cycles at 94°C for 15 seconds and 60°C for 4 minutes were performed. Sequence analysis was performed on an ABI 3100 Genetic Analyzer (Applied Biosystems, Foster City, CA, USA).

In addition to screening for activating mutations of c.816, in all samples c-KIT exon 8, 9, 11, 13, en 17 and PDGFRA exon 12, 14 and 18 were analyzed by conventional bidirectional cycle sequencing of PCR-amplified fragments. Amplification of 50 ng genomic DNA of each sample was performed with M13-tailed primers (Table S1). After initial denaturation at 95°C for 3 min, 35 cycles of 95°C for 30 seconds, 60°C for 45 seconds, and 72°C for 45 seconds were performed, followed by 10 min at 72°C. Subsequent sequence analyses of the PCR products was carried out with M13 forward and reverse primers, essentially as described above.

Results

The mean age of diagnosis of the GB and/or DG was 15 years (range, 3 months-36 years, see Table 1). The mean age of diagnosis between the group of patients with DSD (cases 1–16), being 16 (3 months-36 years) and the group with ovarian dysgerminoma (cases 17–31), being 14 (6–19 years) did not differ significantly. Within the group of DSD patients the mean age of diagnosis did differ between patients showing GB, being 13 and patients who had a dysgerminoma with GB, being 21 years. In total, twenty-two cases showed a dysgerminoma component; thirteen patients had pure dysgerminoma, three patients had non-dysgerminoma components (yolk sac tumor and (immature) teratoma) next to the dysgerminoma component, and six patients showed GB next to dysgerminoma. One patient showed teratoma and yolk sac tumor next to GB. Eight patients did not have an invasive component; seven showed GB (one bilaterally) and one patient had GB next to CIS and intratubular seminoma. Five cases presented with bilateral disease; one case showing GB in both gonads, one patient having GB in one gonad and GB together with dysgerminoma in the other, one case with GB in one gonad and GB next to dysgerminoma, yolk sac tumor and immature teratoma in the other, and from two cases only material from one of the gonads was available, showing GB, CIS, and dysgerminoma in one patient and GB, teratoma and yolk sac tumor in the other patient (cases 1–5, Table 1).

LightCycler analysis detected variants in exon 17 of c-KIT in five out of the total group of 31 patients (19%). Four were found in the group of ovarian dysgerminomas (27%: four out of fifteen cases), consisting of two D816V, one D816H and one D816Y mutation (cases 17, 19, 22 and 25, Table 1). All mutations at codon 816 were detected in the LightCycler assay, in analyses with and without LNA added, showing a shift in melting curves which were compared with control samples (Figure S1). One variant in c-KIT exon 17 was found in the group of DSD patients, which changed the codon 178 sequence from ATC to ATT (I798I), which encodes a known synonymous SNP (rs. 55789615) (case 4, Table 1). This variation shifted the melting curve to a position different from that of any of the control mutation samples included (data not shown). Two other samples produced an aberrant melting curve (case 1 and 2, Table 1), but no mutation was detected in subsequent sequencing, despite analyzing the samples in triplicate for all three c.816 variants on two independent DNA isolations (data not shown). All mutations found were verified by sequencing the LightCycler products from reactions with and without LNA (Figure S1). All other samples tested showed melting curves identical to non-mutated Asp 816 (data not shown).

Next to the c.816 LightCycler analysis, conventional Sanger sequencing of c-KIT exons 8, 9, 11, 13, and 17 was performed on the DNA samples in a diagnostic setting. This confirmed the presence of the four c.816 mutations found by the LightCycler analysis (cases 17, 19, 22 and 25, Table 1), but also revealed an additional D816V mutation (case 31, Table 1). Furthermore, in three ovarian dysgerminoma cases a N822K mutation was found (cases 21, 24 and 27 Table 1). In total, in eight out of fifteen ovarian dysgerminoma cases (53%) an exon 17 mutation was found. One patient (case 28, Table 1), showed a heterozygous synonymous SNP (rs. 55789615). In case 16 a D820E mutation in exon 17, next to a N505I mutation in exon 9 was found, being the only DSD case showing mutations in c-KIT (6%, 1 out of 16). No mutations in any of the other exons analyzed were found. Sequence analysis of PDGFRA exon 12, 14 and 18 did not reveal any mutations, only a homozygous synonymous SNP in exon 12 (rs. 1873778) was detected in all samples analyzed.

Immunohistochemical analysis of c-KIT showed no correlation between the presence of c-KIT activating mutations and protein expression in the tumor. In four cases c-KIT immunohistochemistry was not investigated (case 23, 25, 29 and 31), as no additional material was available (Table 1). Staining for c-KIT was variable in the whole series analyzed, ranging from absent through intermediate to strong staining and no clear difference between the DSD and ovarian dysgerminoma subgroups could be seen. As expected, staining for OCT3/4 was positive in the GB, and dysgerminoma components in all cases analyzed, with the exception of case 7. TSPY staining correlated with the two subgroups of patients analyzed, being positive in the DSD group (cases 1–16), with the exception of cases 7 and 13, which showed no staining, and negative in the ovarian dysgerminomas (cases 17–31) (p-value 3.6×10−8).

Discussion

c-KIT expression has been demonstrated in a wide variety of human tumors, although in most types expression is variable. The highest percentages are seen in gastro-intestinal tumors, seminomas, adenoid-cystic carcinomas and malignant melanomas, and amplification and enhanced expression is associated with seminoma progression [10], [30]. The presence of activating mutations of c-KIT in testicular seminomas is well known. Although ovarian dysgerminomas resemble seminomas in morphology and chromosomal aberrations [31], expression of c-KIT is not extensively explored. Here we analyzed fifteen cases of pure ovarian dysgerminomas and found that c-KIT is expressed, although variable, in all but two of the cases analyzed. Mutations in c-KIT codon 816 were found in 5 (33%) and mutations in codon 822 in 3 (20%) out of the 15 pure ovarian dysgerminoma cases (case 17, 19, 22, 25, 31 and 21, 24, 27 respectively, Table 1), accounting for 53% of cases analyzed. No mutations were detected in c-KIT exon 8, 9, 11, and 13. Although most ovarian dysgerminomas express c-KIT, we could not find a correlation between expression and c-KIT exon 17 mutations. It is known that in GIST in addition to mutations in c-KIT, also mutations in PDGFRA exon 12, 14 and 18 play a role and that these are mutually exclusive [9]. Sequencing PDGFRA did not reveal mutations in any of the dysgerminoma DNA samples analyzed, only a variation in exon 12 was found in almost all cases (homozygous synonymous SNP, rs. 1873778, Table 1). This indicates that mutations in PDGFRA do not play a major role in the development of (ovarian) dysgerminomas or GB. The results shown here extend those of Cheng et al. and Hoei-Hansen et al. [16], [32]. Cheng et al. [32] analyzed 22 cases of dysgerminoma and found a c-KIT codon 816 mutation in 27% of cases, and KIT expression in 87%. Hoei-Hansen et al. found c-KIT codon 816 mutations in five out of seventeen dysgerminoma cases (29%) with 80% expressing c-KIT [16]. Furthermore, also in gastro-intestinal tumors KIT mutation rate is lower than the expression rate of KIT [33], [34]. The results presented here suggest that in about half of ovarian dysgerminomas activating mutations in c-KIT play a role, with about a third consisting of codon 816 mutations, as has been reported by others [16], [32], while the remaining 20% consisted of N822K mutations. Indeed, c-KIT N822K mutations have also been found in testicular GCC [10], [35], [36], indicating a role for this mutation in the development of GCC, independent of the origin in the testis or ovary. Next to these mutations a known synonymous SNP (rs55789615) was detected in exon 17 of case 28, which has been described before in a patient having a N822K mutation in the GCC of the contralateral testis [36]. Besides these, no other aberrations in the exons analyzed could be found in the group of ovarian dysgerminomas. Patients showing expression of c-KIT might benefit from targeted therapy with imatinib mesylate, as has been shown for patients with GIST [37], and also in a patient with metastatic seminoma [38]. This might therefore also be of interest to treat ovarian dysgerminoma.

DSD patients with gonadal dysgenesis or hypovirilization have an increased risk of developing GCC, with GB as the precursor lesion, linked to the presence of (part of) the Y-chromosome. Y-chromosomal material is detected in 90% of patients with dysgenetic gonads, with the TSPY gene being seen as the candidate gene in the GonadoBlastoma on the Y-chromosome (GBY) region [39]. Interestingly, the role of TSPY has been suggested to be a repressor of androgen signaling by trapping AR in the cytoplasm, even in presence of the ligand [40]. It is therefore possible that the relative high levels of TSPY protein found in CIS and GB creates a local androgen –insensitivity environment, in which these cells are not able to respond to the presence of ligand. This is of particular interest during the window of so-called mini-puberty, whereby the affected germ cells remain in an embryonic state (positive for OCT3/4 amongst others). During puberty these cells might become sensitive to prolonged and increased levels of androgens and subsequently become invasive (associated by loss of TSPY expression). Here we show that in 89% of cases (17 out of 19 analyzed) where GB was present, either with or without dysgerminoma, positive staining of the TSPY protein could be seen in the neoplastic cells. It is possible that in the two TSPY negative cases (7 and 13) the staining was sub-optimal due to poor tissue fixation, as other markers tested showed unexpected (negative) results (data not shown). In contrast, all cases with ovarian dysgerminoma in a 46,XX (normal female) genetic background were negative for TSPY. The results underline the importance of presence of (part of) the Y-chromosome in the development of GB and point to the fact that in the case of DSD and ovarian dysgerminomas the pathways leading to the tumors are distinct. This is in line with, and extends the results reported by Hoei-Hansen [16], who showed TSPY in five out of seven cases with GB, the precursor lesion of dysgerminoma in DSD patients, and no TSPY protein expression in eleven pure dysgerminoma cases. Presence of the TSPY gene in malignant ovarian germ cell tumors has also been studied by Shahsiah et al. [41], showing positivity of the gene in 6 out of 47 (12.7%) cases, two patients showed GB and in one patient presence of the Y chromosome was confirmed cytogenetically. However, no c-KIT mutation analysis was performed.

Next to the presence of TSPY, also presence of OCT3/4 was investigated in this series. OCT3/4 is one of the key regulators of self renewal and pluripotency of embryonic stem cells, and in normal development this protein is only present in primordial germ cells/gonocytes and oogonia [28], [42]. In the testis expression is only seen in GCC (i.e. seminoma and embryonal carcinoma) and its precursor lesion CIS [25], [43]. In DSD patients OCT3/4 expression is present in GB and dysgerminoma [44], [45]. OCT3/4 was present in all but one GB analyzed in this study, and also a positive staining was found in all dysgerminomas, in line with previous studies [16], [44]. Case 7 which did not show a positive OCT3/4 staining of the GB, also gave mixed results using other markers (negative TSPY staining amongst others), indicating possible poor quality of the material.

Analyzing the presence of c-KIT activating - and PDGFRA mutations, either by LightCycler melting curve analysis or conventional sequencing, in the group of sixteen DSD cases showing GB, with or without an invasive tumor, showed that in the majority of cases no mutations could be detected (15 out of 16 cases, 94%). It must be mentioned however, that in a number of cases the percentage of tumor present in the sample was low, possibly leading to false negative results. In three patients a shift in melting curve not corresponding to one of the c-KIT c.816 mutations investigated was found, and subsequent sequencing of the LightCycler products revealed a wild type exon 17 sequence in case 1 and 2, and a known synonymous SNP (rs 55789615) in case 4 (I798I), although this latter finding was not confirmed by conventional sequencing of the original DNA sample. Strikingly, these three patients all have bilateral disease. The I798I variant was also detected in a patient with ovarian dysgerminoma (case 28, see above). In one patient (case 16) showing GB and mainly dysgerminoma, missense mutations in c-KIT were found in exon 9 and 17, resulting in N505I and D820E respectively, which were not present in normal adjacent adnexal material. In this case, which was also positive for TSPY, presence of the Y-chromosome was confirmed with fluorescent in-situ hybridization on paraffin embedded material of the dysgerminoma lesion using a Y-centromeric probe (data not shown), confirming a 46,XY-DSD diagnosis. A mutation in c-KIT codon 816 in a DSD patient presenting with GB and dysgerminoma has also been reported previously [16], indicating that in rare cases these mutations can be found in DSD patients. Interestingly, the phenotypically male patient described here presented with a unilateral cryptorchid testis, which was removed during orchidopexy. He has two sons, who both presented with bilateral cryptorchid testis, which is one of the major risk factors for testicular GCC [46]. If the mutations found are also present in the sons cannot be ascertained as no material is available for analysis. To our knowledge this is the first time a N505I mutation in exon 9 of c-KIT has been found. c-KIT mutations in exon 9 have been described in GIST [47], and it is thought that these mutations mimic the conformational change that the extracellular KIT receptor undergoes when SCF is bound [48]. The activating c-KIT D820E mutation has been described together with mutations in exon 9, related to sunitinib resistance in GIST [49]. If the mutations found are located on the same or different alleles cannot be determined, as only paraffin embedded material was available for analysis. Besides the specific c-KIT c.816 mutations investigated here, other mutations in exon 17 have been reported in GCC; c-KIT gain-of-function D820G and Y823D [2], [10], [35], [36] have been found, next to S821F, C809S, Y823N and D816E together with D820H [12], [36] amongst others, which are not present in the cases analyzed here, and thus do not seem to be involved in ovarian dysgerminomas or DSD. Interestingly, recently genome-wide association studies of have identified SNPs within KITLG (SCF) as having the strongest association with an increased risk of developing a testicular GCC, pointing to the importance of the SCF-cKIT pathway in this disease [50], [51], [52].

Taken together, c-KIT mutations occur in approximately half of pure ovarian dysgerminoma cases, all residing in exon 17, indicating a role in the etiology of the disease. The activated c-KIT, together with prolonged expression of OCT3/4 may allow increased survival and proliferation of undifferentiated gonocytes/oogonia, leading to the development of dysgerminoma. In DSD, presence of Y-chromosomal material leads to the gonadal dysgenesis, in which the germ cells survive because of prolonged expression of both OCT3/4 and TSPY, setting the stage for GB and subsequent dysgerminoma development; although in a minority of cases mutations in c-KIT might play a role.

Supporting Information

Figure S1.

Detection of c-KIT c.816 mutations in patient samples by melting curve analysis. The y-axis represents fluorescence intensity and the x-axis represents temperature. Mutations lead to different melting temperatures of the hybridization probes from the amplification product. A, B) Melting curves of sample 19 and 22 with and without the addition of LNA are shown together with a positive control harboring the D816V mutation. C) Melting curves of sample 17 with and without the addition of LNA are shown together with a positive control harboring the D816H mutation. D) Melting curves of sample 25 with and without the addition of LNA are shown together with a positive control harboring the D816Y mutation. E, F) Electropherogram showing the A to T mutation in codon 816 in LightCycler products with and without LNA added of sample 19 and 22 respectively. G) Electropherogram showing the G to C mutation in LightCycler products with and without LNA added of codon 816 in sample 17. H) Electropherogram showing the G to T mutation in LightCycler products with and without LNA added of codon 816 in sample 25. Note the suppression of wild type c-KIT and the enrichment of the mutant amplification product in the + LNA samples. pc: positive control, Val: valine mutation, His: histidine mutation, Tyr: tyrosine mutation, LNA: locked nucleic acid.

https://doi.org/10.1371/journal.pone.0043952.s001

(TIF)

Author Contributions

Conceived and designed the experiments: RH SLSD LHJL. Performed the experiments: RH HS GJG ICM. Analyzed the data: RH HS KB JWO WNMD HJD LHJL. Contributed reagents/materials/analysis tools: GJG RE CD DTS. Wrote the paper: RH LHJL.

References

  1. 1. Heinrich MC, Blanke CD, Druker BJ, Corless CL (2002) Inhibition of KIT tyrosine kinase activity: a novel molecular approach to the treatment of KIT-positive malignancies. J Clin Oncol 20: 1692–1703.
  2. 2. Kemmer K, Corless CL, Fletcher JA, McGreevey L, Haley A, et al. (2004) KIT Mutations Are Common in Testicular Seminomas. Am J Pathol 164: 305–313.
  3. 3. Robinson TL, Sircar K, Hewlett BR, Chorneyko K, Riddell RH, et al. (2000) Gastrointestinal stromal tumors may originate from a subset of CD34-positive interstitial cells of Cajal. Am J Pathol 156: 1157–1163.
  4. 4. Runyan C, Schaible K, Molyneaux K, Wang Z, Levin L, et al. (2006) Steel factor controls midline cell death of primordial germ cells and is essential for their normal proliferation and migration. Development 133: 4861–4869.
  5. 5. Tu J, Fan L, Tao K, Zhu W, Li J, et al. (2007) Stem cell factor affects fate determination of human gonocytes in vitro. Reproduction 134: 757–765.
  6. 6. Verzijl A, Heide R, Oranje AP, van Schaik RH (2007) C-kit Asp-816-Val mutation analysis in patients with mastocytosis. Dermatology 214: 15–20.
  7. 7. Corless CL, Fletcher JA, Heinrich MC (2004) Biology of gastrointestinal stromal tumors. J Clin Oncol 22: 3813–3825.
  8. 8. Reilly JT (2002) Class III receptor tyrosine kinases: role in leukaemogenesis. Br J Haematol 116: 744–757.
  9. 9. Corless CL, Barnett CM, Heinrich MC (2011) Gastrointestinal stromal tumours: origin and molecular oncology. Nat Rev Cancer 11: 865–878.
  10. 10. McIntyre A, Summersgill B, Grygalewicz B, Gillis AJ, Stoop J, et al. (2005) Amplification and overexpression of the KIT gene is associated with progression in the seminoma subtype of testicular germ cell tumors of adolescents and adults. Cancer Res 65: 8085–8089.
  11. 11. Nakai Y, Nonomura N, Oka D, Shiba M, Arai Y, et al. (2005) KIT (c-kit oncogene product) pathway is constitutively activated in human testicular germ cell tumors. Biochem Biophys Res Commun 337: 289–296.
  12. 12. Willmore-Payne C, Holden JA, Chadwick BE, Layfield LJ (2006) Detection of c-kit exons 11- and 17-activating mutations in testicular seminomas by high-resolution melting amplicon analysis. Mod Pathol.
  13. 13. Kitamura Y, Hirota S, Nishida T (2001) A loss-of-function mutation of c-kit results in depletion of mast cells and interstitial cells of Cajal, while its gain-of-function mutation results in their oncogenesis. Mutat Res 477: 165–171.
  14. 14. Przygodzki RM, Hubbs AE, Zhao FQ, O’Leary TJ (2002) Primary Mediastinal Seminomas: Evidence of Single and Multiple KIT Mutations. Lab Invest 82: 1369–1375.
  15. 15. Sakuma Y, Sakurai S, Oguni S, Satoh M, Hironaka M, et al. (2004) c-kit gene mutations in intracranial germinomas. Cancer Science 95: 716–720.
  16. 16. Hoei-Hansen CE, Kraggerud SM, Abeler VM, Kaern J, Rajpert-De Meyts E, et al. (2007) Ovarian dysgerminomas are characterised by frequent KIT mutations and abundant expression of pluripotency markers. Mol Cancer 6: 12.
  17. 17. Kraggerud SM, Szymanska J, Abeler VM, Kaern J, Eknaes M, et al. (2000) DNA copy number changes in malignant ovarian germ cell tumors. Cancer Res 60: 3025–3030.
  18. 18. Galani E, Alamanis C, Dimopoulos MA (2005) Familial female and male germ cell cancer. A new syndrome? Gynecol Oncol 96: 254–255.
  19. 19. Hughes IA, Houk C, Ahmed SF, Lee PA (2006) Group LC, et al (2006) Consensus statement on management of intersex disorders. Arch Dis Child 91: 554–563.
  20. 20. Cools M, Drop SL, Wolffenbuttel KP, Oosterhuis JW, Looijenga LH (2006) Germ cell tumors in the intersex gonad: Old paths, new directions, moving frontiers. Endocr Rev 27: 468–484.
  21. 21. Hersmus R, de Leeuw BH, Wolffenbuttel KP, Drop SL, Oosterhuis JW, et al. (2008) New insights into type II germ cell tumor pathogenesis based on studies of patients with various forms of disorders of sex development (DSD). Mol Cell Endocrinol 291: 1–10.
  22. 22. Hersmus R, Kalfa N, de Leeuw B, Stoop H, Oosterhuis JW, et al. (2008) FOXL2 and SOX9 as parameters of female and male gonadal differentiation in patients with various forms of disorders of sex development (DSD). J Pathol 215: 31–38.
  23. 23. Lau Y, Chou P, Iezzoni J, Alonzo J, Komuves L (2000) Expression of a candidate gene for the gonadoblastoma locus in gonadoblastoma and testicular seminoma. Cytogenet Cell Genet 91: 160–164.
  24. 24. de Jong J, Stoop H, Dohle GR, Bangma CH, Kliffen M, et al. (2005) Diagnostic value of OCT3/4 for pre-invasive and invasive testicular germ cell tumours. J Pathol 206: 242–249.
  25. 25. Looijenga LH, Stoop H, de Leeuw HP, de Gouveia Brazao CA, Gillis AJ, et al. (2003) POU5F1 (OCT3/4) identifies cells with pluripotent potential in human germ cell tumors. Cancer Res 63: 2244–2250.
  26. 26. Woodward PJ, Heidenreich A, Looijenga LHJ, et al. (2004) Testicular germ cell tumors. In: Eble JN, Sauter G, Epstein JI, Sesterhann IA, editors. World Health Organization Classification of Tumours Pathology and Genetics of the Urinary System and Male Genital Organs. Lyon: IARC Press. 217–278.
  27. 27. Honecker F, Stoop H, de Krijger RR, Chris Lau YF, Bokemeyer C, et al. (2004) Pathobiological implications of the expression of markers of testicular carcinoma in situ by fetal germ cells. J Pathol 203: 849–857.
  28. 28. Stoop H, Honecker F, Cools M, de Krijger R, Bokemeyer C, et al. (2005) Differentiation and development of human female germ cells during prenatal gonadogenesis: an immunohistochemical study. Hum Reprod 20: 1466–1476.
  29. 29. Kido T, Lau YF (2005) A Cre gene directed by a human TSPY promoter is specific for germ cells and neurons. Genesis 42: 263–275.
  30. 30. Went PT, Dirnhofer S, Bundi M, Mirlacher M, Schraml P, et al. (2004) Prevalence of KIT expression in human tumors. J Clin Oncol 22: 4514–4522.
  31. 31. Looijenga LH, Hersmus R, Gillis AJ, Pfundt R, Stoop HJ, et al. (2006) Genomic and expression profiling of human spermatocytic seminomas: primary spermatocyte as tumorigenic precursor and DMRT1 as candidate chromosome 9 gene. Cancer Res 66: 290–302.
  32. 32. Cheng L, Roth LM, Zhang S, Wang M, Morton MJ, et al. (2011) KIT gene mutation and amplification in dysgerminoma of the ovary. Cancer 117: 2096–2103.
  33. 33. Feng F, Liu XH, Xie Q, Liu WQ, Bai CG, et al. (2003) Expression and mutation of c-kit gene in gastrointestinal stromal tumors. World J Gastroenterol 9: 2548–2551.
  34. 34. Willmore C, Holden JA, Zhou L, Tripp S, Wittwer CT, et al. (2004) Detection of c-kit-activating mutations in gastrointestinal stromal tumors by high-resolution amplicon melting analysis. Am J Clin Pathol 122: 206–216.
  35. 35. Rapley EA, Hockley S, Warren W, Johnson L, Huddart R, et al. (2004) Somatic mutations of KIT in familial testicular germ cell tumours. Br J Cancer 90: 2397–2401.
  36. 36. Biermann K, Göke F, Nettersheim D, Eckert D, Zhou H, et al. (2007) c-KIT is frequently mutated in bilateral germ cell tumours and down-regulated during progression from intratubular germ cell neoplasia to seminoma. The Journal of Pathology 213: 311–318.
  37. 37. Joensuu H, Fletcher C, Dimitrijevic S, Silberman S, Roberts P, et al. (2002) Management of malignant gastrointestinal stromal tumours. Lancet Oncol 3: 655–664.
  38. 38. Pedersini R, Vattemi E, Mazzoleni G, Graiff C (2007) Complete response after treatment with imatinib in pretreated disseminated testicular seminoma with overexpression of c-KIT. Lancet Oncol 8: 1039–1040.
  39. 39. Lau YF, Li Y, Kido T (2009) Gonadoblastoma locus and the TSPY gene on the human Y chromosome. Birth Defects Res C Embryo Today 87: 114–122.
  40. 40. Akimoto C, Ueda T, Inoue K, Yamaoka I, Sakari M, et al. (2010) Testis-specific protein on Y chromosome (TSPY) represses the activity of the androgen receptor in androgen-dependent testicular germ-cell tumors. Proc Natl Acad Sci U S A 107: 19891–19896.
  41. 41. Shahsiah R, Jahanbin B, Rabiei R, Ardalan FA, Sarhadi B, et al. (2011) Malignant ovarian germ cell tumours in gonadal Y chromosome mosaicism. J Clin Pathol 64: 973–976.
  42. 42. Rosner MH, Vigano MA, Ozato K, Timmons PM, Poirier F, et al. (1990) A POU-domain transcription factor in early stem cells and germ cells of the mammalian embryo. Nature 345: 686–692.
  43. 43. Rajpert-De Meyts E, Hanstein R, Jorgensen N, Graem N, Vogt PH, et al. (2004) Developmental expression of POU5F1 (OCT-3/4) in normal and dysgenetic human gonads. Hum Reprod 19: 1338–1344.
  44. 44. Cheng L, Thomas A, Roth LM, Zheng W, Michael H, et al. (2004) OCT4: A Novel Biomarker for Dysgerminoma of the Ovary. Am J Surg Pathol 28: 1341–1346.
  45. 45. Cools M, Stoop H, Kersemaekers AM, Drop SL, Wolffenbuttel KP, et al. (2006) Gonadoblastoma arising in undifferentiated gonadal tissue within dysgenetic gonads. J Clin Endocrinol Metab 91: 2404–2413.
  46. 46. UKTesticular Cancer Study Group (1994) Aetiology of testicular cancer: Association with congenital abnormalities, age at puberty, infertility, and exercise. BMJ 308: 1393–1399.
  47. 47. Lux ML, Rubin BP, Biase TL, Chen CJ, Maclure T, et al. (2000) KIT extracellular and kinase domain mutations in gastrointestinal stromal tumors. Am J Pathol 156: 791–795.
  48. 48. Yuzawa S, Opatowsky Y, Zhang Z, Mandiyan V, Lax I, et al. (2007) Structural basis for activation of the receptor tyrosine kinase KIT by stem cell factor. Cell 130: 323–334.
  49. 49. Guo T, Hajdu M, Agaram NP, Shinoda H, Veach D, et al. (2009) Mechanisms of sunitinib resistance in gastrointestinal stromal tumors harboring KITAY502-3ins mutation: an in vitro mutagenesis screen for drug resistance. Clin Cancer Res 15: 6862–6870.
  50. 50. Kanetsky PA, Mitra N, Vardhanabhuti S, Li M, Vaughn DJ, et al. (2009) Common variation in KITLG and at 5q31.3 predisposes to testicular germ cell cancer. Nat Genet 41: 811–815.
  51. 51. Rapley EA, Turnbull C, Al Olama AA, Dermitzakis ET, Linger R, et al. (2009) A genome-wide association study of testicular germ cell tumor. Nat Genet 41: 807–810.
  52. 52. Dalgaard MD, Weinhold N, Edsgard D, Silver JD, Pers TH, et al. (2012) A genome-wide association study of men with symptoms of testicular dysgenesis syndrome and its network biology interpretation. J Med Genet 49: 58–65.