骨巨细胞瘤的恶性转化及其与Denosumab治疗的关系:放射学和病理学的观点。

Q2 Medicine Sarcoma Pub Date : 2022-06-17 eCollection Date: 2022-01-01 DOI:10.1155/2022/3425221
K van Langevelde, A H G Cleven, A Navas Cañete, L van der Heijden, M A J van de Sande, H Gelderblom, J V M G Bovée
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引用次数: 2

摘要

目的:骨巨细胞瘤(mGCTB)的恶性分为原发性(合并常规巨细胞瘤)和继发性(经放疗或其他治疗后)。Denosumab治疗已被认为在继发性mGCTB的病因学中发挥作用。在这个来自三级转诊肉瘤中心的病例系列中,我们旨在发现不同成像方式下GCTB恶性转化的独特特征。此外,我们评估了地诺单抗治疗的持续时间和恶性肿瘤发展的滞后时间。方法:从组织病理学数据库检索,6例患者病理证实为最初的常规GCTB,随后继发性mGCTB。结果:mGCTB确诊时,单纯地诺单抗治疗2例,单纯地诺单抗联合手术治疗2例,多次刮痧联合放疗1例,单纯手术治疗1例。在4例denosumab治疗的患者中,到恶性转化的平均滞后时间为7个月(范围2-11个月)。影像学表现怀疑与denosumab治疗相关的恶性转化是CT上没有纤维骨基质形成和没有新皮质形成,软组织成分稳定甚至增大。结论:在4例接受denosumab治疗的患者中,继发性mGCTB在开始治疗后的一年内发生。放疗相关的mGCTB比denosumab相关的mGCTB有更长的延迟时间。在denosumab治疗的头几个月密切的临床和影像学随访是关键,因为mGCTB倾向于具有快速的侵袭行为,类似于其他高级别肉瘤。无应答者应(重新)评估其对常规GCTB的初步诊断。
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Malignant Transformation of Giant Cell Tumor of Bone and the Association with Denosumab Treatment: A Radiology and Pathology Perspective.

Objective: Malignancy in giant cell tumor of bone (mGCTB) is categorized as primary (concomitantly with conventional GCTB) or secondary (after radiotherapy or other treatment). Denosumab therapy has been suggested to play a role in the etiology of secondary mGCTB. In this case series from a tertiary referral sarcoma center, we aimed to find distinctive features for malignant transformation in GCTB on different imaging modalities. Furthermore, we assessed the duration of denosumab treatment and lag time to the development of malignancy.

Methods: From a histopathology database search, 6 patients were pathologically confirmed as having initial conventional GCTB and subsequently with secondary mGCTB.

Results: At the time of mGCTB diagnosis, 2 cases were treated with denosumab only, 2 with denosumab and surgery, 1 with multiple curettages and radiotherapy, and 1 with surgery only. In the 4 denosumab treated patients, the mean lag time to malignant transformation was 7 months (range 2-11 months). Imaging findings suspicious of malignant transformation related to denosumab therapy are the absence of fibro-osseous matrix formation and absent neocortex formation on CT, and stable or even increased size of the soft tissue component.

Conclusion: In 4 patients treated with denosumab, secondary mGCTB occurred within the first year after initiation of treatment. Radiotherapy-associated mGCTB has a longer lag time than denosumab-associated mGCTB. Close clinical and imaging follow-up during the first months of denosumab therapy is key, as mGCTB tends to have rapid aggressive behavior, similar to other high-grade sarcomas. Nonresponders should be (re) evaluated for their primary diagnosis of conventional GCTB.

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来源期刊
Sarcoma
Sarcoma Medicine-Radiology, Nuclear Medicine and Imaging
CiteScore
5.00
自引率
0.00%
发文量
15
审稿时长
14 weeks
期刊介绍: Sarcoma is dedicated to publishing papers covering all aspects of connective tissue oncology research. It brings together work from scientists and clinicians carrying out a broad range of research in this field, including the basic sciences, molecular biology and pathology and the clinical sciences of epidemiology, surgery, radiotherapy and chemotherapy. High-quality papers concerning the entire range of bone and soft tissue sarcomas in both adults and children, including Kaposi"s sarcoma, are published as well as preclinical and animal studies. This journal provides a central forum for the description of advances in diagnosis, assessment and treatment of this rarely seen, but often mismanaged, group of patients.
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