Abstract 547P
Background
To analyze clinicopathological features of ETMRs.
Methods
A total of 14 cases of ETMRs from 2016 to 2021 in Xuanwu Hospital of Capital Medical University were retrospectively summarized. The clinical and imaging characteristics, pathological and molecular characteristics were analyzed, and the related literature was reviewed.
Results
All 14 patients (6 males and 8 females) aged from 9 months old to 3 years old (mean 2 years) mainly had a history of headache or/and vomiting. Twelve tumors were supratentorial and two infratentorial, seven of which occurred in the frontal lobe. The MRI findings showed that the lesions were located in the third ventricle, and the enhanced MRI showed abnormal enhancement signals. The MRI enhancement all showed an abnormal enhancement signal. Pathological finding showed that 12 cases had displaying the morphological characteristics of ETMR. The distribution of tumor cells is sparse and uneven, and some cells arrange in multiple layers and grow around blood vessels, partially forming a "Homm-rett group" structure, island-like structure can be seen. IHC showed Syn and Lin28a were immunopositive in all 14 cases (14/14). GFAP and Olig-2 were partially immunopositive in 3 cases (3/14). EMA was dot-and/or-ring immunopositivity in 2 cases (90%, 2/14). At the same time, there was a case immunopositive for H3K27M, with the loss of H3K27me3. 12 ETMRs were available to detect C19MC and Dicer1 gene mutation. 11 in 12 (88.9%) were found to have C19MC amplification, and one have Dicer1 mutation as well as H3K27M mutation. Among the 14 patients after surgery, All 10 patients received adjuvant radiotherapy/chemotherapy,Progression-free survival was 6.2 months, and overall survival was 11 months.
Conclusions
ETMRs have relatively distinguishing clinical and histopathological features. C19MC alteration and Dicer1 gene mutation, can be considered as useful biomarkers for the diagnosis and differential diagnosis, and provide a direction for targeted therapy in the future.
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
571P - Artificial intelligence-powered analysis of tumor lymphocytes infiltration: A translational analysis of AtezoTRIBE trial
Presenter: Martina Carullo
Session: Poster session 10
572P - Neoantigen heterogeneity among subtypes in colorectal cancer
Presenter: Fuqiang Li
Session: Poster session 10
574P - Comparative analysis of the tumor immune microenvironment (TIME) in primary and metastatic sites of microsatellite stable (MSS) and microsatellite instability-high (MSI) colorectal cancer
Presenter: Marwan Fakih
Session: Poster session 10
575P - Impact of immunological alterations and post-operative biomarkers on long-term outcomes in patients with locally advanced rectal cancer: Results from the STAR-01 study cohort
Presenter: Francesca Negri
Session: Poster session 10
576P - Prognostic values of a modified diagnostic biopsy-adapted immunoscore based on double immunohistochemical staining in patients with locally advanced rectal cancer
Presenter: Qiang Zeng
Session: Poster session 10
577P - Systematically assessing the intratissue microbiota in 937 patients with colorectal cancer
Presenter: Huanzi Zhong
Session: Poster session 10
578P - Tissue-resident microbiota characterization in colorectal cancer metastases
Presenter: Philippe Stevens
Session: Poster session 10
579P - A clinico-imaging predictive artificial intelligence model of relapse in colon cancer using baseline CT scans
Presenter: América Bueno Gómez
Session: Poster session 10
580P - Prognosis in stage II colorectal cancer: The effect of the primary tumor location and biomarkers
Presenter: Vincent Liégeois
Session: Poster session 10