对比增强型感性加权成像(CE-SWI)用于描述肌肉骨骼肿瘤病理学:一家癌症机构最初五年经验的图解文章

Valenzuela Raul F, Duran-Sierra E, Canjirathinkal Ma, Amini B, Ma J, Hwang Kp, Stafford Rj, Torres Keila E, Zarzour Ma, Livingston Ja, Madewell Je, Murphy Wa, Costelloe Cm
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引用次数: 0

摘要

磁感应强度加权成像(SWI)基于三维高空间分辨率、速度校正梯度回波磁共振成像序列,使用幅度和滤波相位信息来创建图像。SWI 利用组织的磁感应强度差异产生信号对比度,这种对比度可能来自顺磁性(血色素)、二磁性(矿物质和钙化)和铁磁性(金属)分子。通过滤波相位图像可区分钙化和血液产物,有助于观察成骨细胞和溶骨性骨转移瘤,或显示脂肪肉瘤和骨肉瘤中的钙化和类骨生成。如果结合注射外源性造影剂进行采集,造影剂增强 SWI(CE-SWI)可同时检测 T2* 感度效应、T2 信号差、造影剂引起的 T1 缩短以及相外脂肪和水的化学位移效应。骨骼和软组织病变的 SWI 特征已被描述,包括骨骼中的巨细胞瘤和软组织中的滑膜肉瘤。我们将进一步探讨良性软组织病变的外观,如血管瘤、神经纤维瘤、色素性绒毛滑膜炎、脓肿和血肿。大多数肌样肉瘤在基线时没有或仅有低度瘤内出血。CE-SWI能很好地区分脱模性纤维瘤中成熟的纤维化T2*深色成分和活跃的增强T1缩短成分。SWI 在肿瘤 MSK 成像中越来越受欢迎,因为它能灵敏地显示软组织病变中的出血,从而帮助区分良性和恶性软组织肿瘤。将软组织肉瘤有活力、增强的部分与出血/坏死的部分分开显示的能力也表明它可作为肿瘤治疗反应的生物标记物。了解和认识高级别肉瘤的自发性出血模式与有反应的肿瘤在治疗诱导坏死过程中出现的出血模式之间的差异至关重要。在治疗成功的肉瘤中可观察到环状血色素 SWI 模式。CE-SWI 在区分健康的铁负荷骨髓的 T2* 增厚和被肿瘤移位的骨髓的 T1 缩短增强方面也显示出早期的良好效果。MSK 肿瘤学中的 SWI 和 CE-SWI 学习目标:SWI 和 CE-SWI 可用于识别 MRI 上的钙化。某些 SWI 和 CE-SWI 模式与肿瘤组织学类型相关。CE-SWI可鉴别脱模瘤的成熟和未成熟成分。CE-SWI 模式有助于评估软组织肉瘤的治疗反应。了解手术后变化的CE-SWI模式还有助于区分具有重叠成像特征的残留肿瘤和复发肿瘤。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Contrast-enhanced Susceptibility Weighted Imaging (CE-SWI) for the Characterization of Musculoskeletal Oncologic Pathology: A Pictorial Essay on the Initial Five-year Experience at a Cancer Institution
Susceptibility-weighted imaging (SWI) is based on a 3D high-spatial-resolution, velocity-corrected gradient-echo MRI sequence that uses magnitude and filtered-phase information to create images. It SWI uses tissue magnetic susceptibility differences to generate signal contrast that may arise from paramagnetic (hemosiderin), diamagnetic (minerals and calcifications) and ferromagnetic (metal) molecules. Distinguishing between calcification and blood products is possible through the filtered phase images, helping to visualize osteoblastic and osteolytic bone metastases or demonstrating calcifications and osteoid production in liposarcoma and osteosarcoma. When acquired in combination with the injection of an exogenous contrast agent, contrast-enhanced SWI (CE-SWI) can simultaneously detect the T2* susceptibility effect, T2 signal difference, contrast-induced T1 shortening, and out-of-phase fat and water chemical shift effect. Bone and soft tissue lesion SWI features have been described, including giant cell tumors in bone and synovial sarcomas in soft tissues. We expand on the appearance of benign soft-tissue lesions such as hemangioma, neurofibroma, pigmented villonodular synovitis, abscess, and hematoma. Most myxoid sarcomas demonstrate absent or just low-grade intra-tumoral hemorrhage at the baseline. CE-SWI shows superior differentiation between mature fibrotic T2* dark components and active enhancing T1 shortening components in desmoid fibromatosis. SWI has gained popularity in oncologic MSK imaging because of its sensitivity for displaying hemorrhage in soft tissue lesions, thereby helping to differentiate benign versus malignant soft tissue tumors. The ability to show the viable, enhancing portions of a soft tissue sarcoma separately from hemorrhagic/necrotic components also suggests its utility as a biomarker of tumor treatment response. It is essential to understand and appreciate the differences between spontaneous hemorrhage patterns in high-grade sarcomas and those occurring in the therapy-induced necrosis process in responding tumors. Ring-like hemosiderin SWI pattern is observed in successfully treated sarcomas. CE-SWI also demonstrates early promising results in separating the T2* blooming of healthy iron-loaded bone marrow from the T1-shortened enhancement in bone marrow that is displaced by the tumor. SWI and CE-SWI in MSK oncology learning objectives: SWI and CE-SWI can be used to identify calcifications on MRI. Certain SWI and CE-SWI patterns can correlate with tumor histologic type. CE-SWI can discriminate mature from immature components of desmoid tumors. CE-SWI patterns can help to assess treatment response in soft tissue sarcomas. Understanding CE-SWI patterns in post-surgical changes can also be useful in discriminating between residual and recurrent tumors with overlapping imaging features.
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