Abstract 512P
Background
Central nervous system germ cell tumors (CNS GCTs) are a group of rare heterogeneous CNS tumors. CNS GCTs are usually in midline location and mainly affect children and adolescents. The incidence of CNS GCTs is higher in Asia (11%) than that in Western Europe (4%) with a male predominance. The different tumor distribution demographically and high incidence in East Asia suggests a probable genetic background.
Methods
We collected samples including tissue and blood leukocyte control from 17 patients with CNS GCTs. All samples were tested using a 551-cancer related gene profiling, and somatic mutations, TMB, MSI and germline mutations were analyzed. The pathogenicity of germline mutations was categorized based on American College of Medical Genetics and Genomics guidelines. We screened out the pathogenic and likely pathogenic (P/LP) mutations of germline mutations and calculated the relative risk (RR) in our cohort compared to that in a control population (gnomAD). Then the relationship between mutation characteristics and clinical features were further analyzed, as well as the correlation with patient prognosis.
Results
In 17 patients with CNS GCTs, 4 patients (4/17) were found harboring germline pathogenic or likely-pathogenic mutations, respectively, in FANCA, FANCD2, FANCE, SDHA. All the four genes are Fanconi anemia (FA)-related genes. The RR of total FA mutations in patients with CNS GCTs was 21.589 (95% CI, 28.934-257.728; P value, 3.22E-07) compared to gnomAD controls. Then the 17 patients were divided into two groups, the FA group (with FA-related gene heterozygous germline P/LP mutations) and the non-FA group (without P/LP mutation). The results showed that pathological classification (P=0.00588) and site of lesion (P=0.00714) were significantly different in the two groups. There was no significant difference in gender, age and TMB between the two groups. The 4 recurrent patients were all in the non-FA group, but there was no statistical difference in prognosis between the two groups.
Conclusions
FA-related gene germline P/LP mutations increase the susceptibility to CNS GCTs. Moreover, the germline FA mutation may be related to the pathological subtype, site of lesion and prognosis, which needs to be verified with a large sample.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
35P - SAT-122: A potential first-in-class, potent, small-molecule disruptor of RAD51-BRCA2, attenuates RAD51 foci formation and tumor progression in preclinical models
Presenter: Sukanya Patra
Session: Poster session 09
36P - Molecular assessment of clinical antitumour therapeutics utilising established pancreatic ductal adenocarcinoma patient-derived models
Presenter: Young-Ah Suh
Session: Poster session 09
37P - Nischarin can be a target for stromal normalisation in pancreatic ductal adenocarcinoma
Presenter: Jelena Grahovac
Session: Poster session 09
38P - Effects of antiemetics on zolbetuximab-induced gastric injury and emesis frequency in ferrets
Presenter: Jane Weng
Session: Poster session 09
39P - Casein kinase 2 modulates epithelial–mesenchymal transition through helicobacter pylori CagA-dependent pathway in gastric cancer cells
Presenter: SODAM LEE
Session: Poster session 09
40P - Bioinformatic evaluation of the transcriptomic and immunologic profile of prostate tumors with high expression of kallikrein-2
Presenter: Irene Moreno
Session: Poster session 09
42P - Developing a photodynamic therapy strategy targeted to endometrial cancer stem cells
Presenter: Beatriz Serambeque
Session: Poster session 09
43P - Looking for therapeutic targets on the proteome profile of endometrial cancer stem cells
Presenter: Mafalda Laranjo
Session: Poster session 09
44P - PAUF as a target for treatment of high PAUF-expressing ovarian cancer
Presenter: Junghyun Cho
Session: Poster session 09