What does this research mean for the field?

True osteosarcoma can co-occur with genetically confirmed IFITM5-related osteogenesis imperfecta, requiring careful multidisciplinary evaluation to distinguish the malignancy from benign OI-related skeletal changes. Novelty: ClaimNovelty.NOVEL_FINDING. Consensus alignment: ConsensusAlignment.NEUTRAL.

What question did this study set out to answer?

To highlight the novel association between IFITM5-related osteogenesis imperfecta and osteosarcoma, improving diagnostic recognition.

June 1, 2026Open Access

Osteosarcoma in the Setting of Genetically Confirmed IFITM5- Related Osteogenesis Imperfecta

Key Points

To highlight the novel association between IFITM5-related osteogenesis imperfecta and osteosarcoma, improving diagnostic recognition.
Presented a case of a 23-year-old female with genetically confirmed IFITM5-related OI.
Conducted molecular testing indicating heterozygosity for IFITM5 mutation c.119C>T (p.Ser40Leu).
Utilized the MISER chemotherapy protocol followed by surgical resection for the patient.
The patient was diagnosed with a nondisplaced pelvic fracture and potential concomitant osteosarcoma.
This case represents the first documented instance of true osteosarcoma in a patient with IFITM5-related OI.
Emphasized the importance of distinguishing between OI-related skeletal changes and malignant bone tumors.

Abstract

Background Osteogenesis imperfecta (OI) is a group of skeletal dysplasias characterized by recurrent fractures and fragile bones. Two pathogenic variants in the IFITM5 gene cause distinct forms of OI: The recurrent c.–14C>T variant causes OI type V (MIM #610967), characterized by hyperplastic callus formation and interosseous membrane ossification, while the rare c.119C>T (p.Ser40Leu) variant causes a phenotypically distinct, severe form of IFITM5 ‐related OI without these hallmark features. Radiographically, OI‐related skeletal lesions may resemble malignant bone tumors such as osteosarcoma, leading to diagnostic challenges. Although the co‐occurrence of OI and osteosarcoma has been reported, with approximately nine documented cases, all involved other OI subtypes. No case of true osteosarcoma arising in a patient with genetically confirmed IFITM5 ‐related OI has been previously described. We present this case to highlight the novelty of this association, improve recognition of the distinguishing features, and prevent future misdiagnosis. Case Presentation A 23‐year‐old female with IFITM5 ‐related OI, confirmed by molecular testing showing heterozygosity for a pathogenic IFITM5 mutation (c.119C>T, p.Ser40Leu; parental testing to determine inheritance was not performed) presented to our Comprehensive Cancer Center in May 2025 with localized groin pain, later diagnosed as a nondisplaced pelvic fracture. Although initial clinical and radiographic findings were consistent with the patient′s underlying OI, further evaluation revealed features concerning for concomitant osteosarcoma. The patient was treated with the MISER chemotherapy protocol with subsequent surgical resection. Conclusion Distinguishing OI‐related skeletal changes from malignant bone tumors requires integration of clinical history, genetic testing, and careful pathologic evaluation via a multidisciplinary approach. While prior reports of concomitant osteosarcoma and OI have involved other subtypes, this case represents the first documented true co‐occurrence in a patient with IFITM5 ‐related OI and underscores the importance of recognizing the overlapping and divergent features of these conditions when rendering a diagnosis and initiating treatment protocols.

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