[Objective] To explore the prognostic model of IncRNA for osteosarcoma (OS), and create competing endogenouse RNA (ceRNA) regulatory networks. [Methods] High- throughput sequencing data and corresponding clinical data were downloaded from the TARGET database after R software was used to filter low-abundance genes and collate corresponding clinical information, sequencing data of 85 cases were obtained, and lncRNA and FRGs were extracted. Gene Ontology (GO) function and Kyoto Encyclopedia of Genes and Ge- nomes (KEGG) pathway enrichment analysis were conducted and the lncRNA, miRNA and FRGs genes were finally screened by Spearman correlation analysis. [Results] A total of 7 658 lncRNA and 175 FRGs were extracted from the TARGET-OS database and 1 158 lncRNAs were significantly associated with ferroptosis. GO analysis showed that CC mainly involved extracellular matrix, osteogenesis, cell-matrix adhesion and receptor-mediated endocytosis, while BP mainly involved cell-base junction, adhesion plaque, extracellular matrix contain- ing collagen, cell contact front and free ribosome. lncRNA PVT1 was found to have certain binding targets with miRNA (hsa-miR-106a5p, hsa-miR-17-5p, hsa-miR-20a-5p). Further analysis showed that lncRNA PVT1 gene was associated with OS immunity (R=-0.27, P= 0.014). The expressions of PDCD1LG2 and CD27 in high-risk group were lower than those in low-risk group (T-test, P＜0.05). [Conclu- sion] The prognosis model of lncRNA related to ferroptosis has good predictive ability, which provides a basis for optimizing the manage- ment of OS. lncRNA ceRNA networks related to ferroptosis may provide valuable data support for the molecular mechanism of OS occur- rence and development.