用于胶质母细胞瘤放疗靶点划定的酰胺质子转移加权CEST磁共振成像:一项前瞻性试验研究。

IF 3.7 Q1 RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING European Radiology Experimental Pub Date : 2024-10-30 DOI:10.1186/s41747-024-00523-4
Patrick L Y Tang, Alejandra Méndez Romero, Remi A Nout, Caroline van Rij, Cleo Slagter, Annemarie T Swaak-Kragten, Marion Smits, Esther A H Warnert
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引用次数: 0

摘要

背景:胶质母细胞瘤的广泛浸润要求在肿瘤总体积(GTV)周围留出15毫米的余量,以确定放疗的临床靶体积(CTV)。酰胺质子转移(APT)加权成像可实现肿瘤浸润的可视化,从而更准确地划分 GTV。我们量化了将 APT 加权成像整合到胶质母细胞瘤 GTV 划分中的影响,并比较了两种 APT 加权量化方法--磁化传递比不对称(MTRasym)和洛伦兹差分(LD)分析--对目标划定的影响:九名胶质母细胞瘤患者在放疗前接受了扩展成像方案,获得了APT加权MTRasym和LD图。根据这两张图生成生物肿瘤体积(BTVMTRasym 和 BTVLD),并与常规 GTV 相加生成生物 GTV(GTVbio,MTRasym 和 GTVbio,LD)。比较结果采用 Wilcoxon 符号秩检验:GTVbio,MTRasym和GTVbio,LD明显大于常规GTV(P≤0.022),体积增加的中位数分别为9.3%和2.1%。GTVbio,MTRasym和GTVbio,LD明显小于CTV(p = 0.004),体积减少的中位数分别为72.1%和70.9%。BTVMTRasym 和 BTVLD 的体积差异不大(p = 0.074)。在三名患者中,BTVMTRasym的划定受到了残留运动伪影导致的大脑外围信号升高的影响;而在APT加权LD图上则没有这种升高:结论:与传统 GTV 相比,更大的生物 GTV 凸显了 APT 加权成像在胶质母细胞瘤放疗靶区划分方面的潜力。APT加权低密度成像在靶点划分方面可能更具优势,因为它对运动伪影的抵抗力更强:APT 加权成像的引入最终可能会增强肿瘤浸润的可视化,并使胶质母细胞瘤的靶区划分不再需要 15 毫米的安全裕度。这可以在有效照射肿瘤的同时降低辐射毒性风险:试验注册:NCT05970757(ClinicalTrials.gov):要点:将APT加权成像整合到放射治疗的靶区划分中是可行的。在胶质母细胞瘤中整合 APT 加权成像可获得更大的 GTV。与 APT 加权 MTRasym 相比,APT 加权 LD 映射对运动伪影的抗干扰能力更强。
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Amide proton transfer-weighted CEST MRI for radiotherapy target delineation of glioblastoma: a prospective pilot study.

Background: Extensive glioblastoma infiltration justifies a 15-mm margin around the gross tumor volume (GTV) to define the radiotherapy clinical target volume (CTV). Amide proton transfer (APT)-weighted imaging could enable visualization of tumor infiltration, allowing more accurate GTV delineation. We quantified the impact of integrating APT-weighted imaging into GTV delineation of glioblastoma and compared two APT-weighted quantification methods-magnetization transfer ratio asymmetry (MTRasym) and Lorentzian difference (LD) analysis-for target delineation.

Methods: Nine glioblastoma patients underwent an extended imaging protocol prior to radiotherapy, yielding APT-weighted MTRasym and LD maps. From both maps, biological tumor volumes were generated (BTVMTRasym and BTVLD) and added to the conventional GTV to generate biological GTVs (GTVbio,MTRasym and GTVbio,LD). Wilcoxon signed-rank tests were performed for comparisons.

Results: The GTVbio,MTRasym and GTVbio,LD were significantly larger than the conventional GTV (p ≤ 0.022), with a median volume increase of 9.3% and 2.1%, respectively. The GTVbio,MTRasym and GTVbio,LD were significantly smaller than the CTV (p = 0.004), with a median volume reduction of 72.1% and 70.9%, respectively. There was no significant volume difference between the BTVMTRasym and BTVLD (p = 0.074). In three patients, BTVMTRasym delineation was affected by elevated signals at the brain periphery due to residual motion artifacts; this elevation was absent on the APT-weighted LD maps.

Conclusion: Larger biological GTVs compared to the conventional GTV highlight the potential of APT-weighted imaging for radiotherapy target delineation of glioblastoma. APT-weighted LD mapping may be advantageous for target delineation as it may be more robust against motion artifacts.

Relevance statement: The introduction of APT-weighted imaging may, ultimately, enhance visualization of tumor infiltration and eliminate the need for the substantial 15-mm safety margin for target delineation of glioblastoma. This could reduce the risk of radiation toxicity while still effectively irradiating the tumor.

Trial registration: NCT05970757 (ClinicalTrials.gov).

Key points: Integration of APT-weighted imaging into target delineation for radiotherapy is feasible. The integration of APT-weighted imaging yields larger GTVs in glioblastoma. APT-weighted LD mapping may be more robust against motion artifacts than APT-weighted MTRasym.

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来源期刊
European Radiology Experimental
European Radiology Experimental Medicine-Radiology, Nuclear Medicine and Imaging
CiteScore
6.70
自引率
2.60%
发文量
56
审稿时长
18 weeks
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