Abstract 1972P
Background
Osteosarcoma (OS) is a common primary bone malignancy in children and adolescents, with most patients diagnosed with Enneking stage IIB. However, the prognosis for these patients is inconsistent, with over half experiencing recurrence or metastasis under standard treatment. The Enneking staging system alone cannot accurately distinguish the risk group for recurrence and metastasis, highlighting the need for further research into the molecular mechanisms.
Methods
74 Chinese patients with Enneking stage IIB OS under standard treatment were included, followed up for over two years. Targeted deep sequencing was performed by YUANSU panel (OrigiMed, Shanghai, China) with 706 cancer-related genes and the Kaplan-Meier method was used to calculate survival curves.
Results
The cohort included 74 patients, 50 males and 24 females, with 40 experiencing recurrence or metastasis and 34 not. The high frequency mutated genes in IIB primary OS were found to be TP53 (33%) FLCN (29%) GID4 (29%) NCOR1 (28%) VEGFA (24%) CCND3 (21%). The group with recurrence or metastasis had significantly higher TMB than the group without (p<0.05). Survival analysis revealed that genetic mutations in MCL1, MYC, TFEB, CCND3, AURKB, ALOX12B, and VEGFA increase the likelihood of recurrence and metastasis in IIB OS patients. (MCL1/MYC/TFEB/CCND3/AURKB/ALOX12B, p<0.05; VEGFA, p=0.065); Abnormalities in the MYC, WNT, and Cell cycle pathways are associated with a worse prognosis (MYC/WNT, p<0.05; Cell cycle, p=0.057). These results indicate that genetic variants and pathway abnormalities are significant risk factors for IIB OS.
Conclusions
Our study represents the largest cohort investigating the molecular mechanisms of Chinese IIB OS. Mutations of MCL1/MYC/TFEB/CCND3/AURKB/ALOX12B/VEGFA genes and MYC/WNT/cell-cycle pathways are high-risk factors for recurrence/metastasis. Given the high mutation frequency and poor prognosis of patients with VEGFA and cell cycle signaling pathway abnormalities, anti-angiogenic agents and cell cycle inhibitors may be more effective treatment options compared with standard therapy. Further studies are needed to confirm their efficacy.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The First Affiliated Hospital of Sun Yat-sen University.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
1939P - phase I clinical results of SQ3370, a doxorubicin-based click chemistry therapeutic in advanced solid tumor patients
Presenter: Sant Chawla
Session: Poster session 15
1940P - Deep molecular profiling of advanced synovial sarcoma as a basis for interventional clinical trials
Presenter: Richard Schlenk
Session: Poster session 15
1941P - Preliminary efficacy and safety of SHR-2554 in advanced epithelioid sarcoma: A phase II trial
Presenter: Haiyan Hu
Session: Poster session 15
1942P - Non-metastatic malignant phyllodes tumors of the breast (B-MPT): A retrospective analysis from a referral center
Presenter: Carmine Valenza
Session: Poster session 15
1944P - MAGE-A4 and NY-ESO-1 expression analysed in a synovial sarcoma tissue micro-array
Presenter: Lore De Cock
Session: Poster session 15
1945P - Diagnostic and therapeutic impact of liquid biopsy in soft tissue sarcomas: A case series
Presenter: Tarek Assi
Session: Poster session 15
1946P - Bladder primary sarcomas (BSar): A genomic landscape and clinical outcomes study
Presenter: ALINA BASNET
Session: Poster session 15
1947P - Predictors and outcomes of recurrent retroperitoneal liposarcoma: New insights into its recurrence patterns
Presenter: Huan Deng
Session: Poster session 15
1948P - Concordance of the pathological diagnosis between local institutional and central judgment in high-grade non-round-cell sarcomas: A supplementary analysis of JCOG1306
Presenter: Eisuke Kobayashi
Session: Poster session 15