创伤性微出血附近的水肿进展：连续MRI上细胞毒性和血管源性水肿的演变

Edema progression in proximity to traumatic microbleeds: evolution of cytotoxic and vasogenic edema on serial MRI.

作者信息

Lee Jacquie, Baniewicz Emily, Peterkin Nicole L, Greenman Danielle, Griffin Allison D, Jikaria Neekita, Turtzo L Christine, Luby Marie, Latour Lawrence L

机构信息

Acute Cerebrovascular Diagnostics Unit, National Institute of Neurological Disorders and Stroke, Bethesda (MD), United States.

American University, Washington (DC), United States.

出版信息

Neuroimage Rep. 2024 Mar;4(1). doi: 10.1016/j.ynirp.2024.100199. Epub 2024 Mar 11.

DOI:10.1016/j.ynirp.2024.100199

PMID:38558768

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10976922/

Abstract

INTRODUCTION

Although cerebral edema is common following traumatic brain injury (TBI), its formation and progression are poorly understood. This is especially true for the mild TBI population, who rarely undergo magnetic resonance imaging (MRI) studies, which can pick up subtle structural details not visualized on computed tomography, in the first few days after injury. This study aimed to visually classify and quantitatively measure edema progression in relation to traumatic microbleeds (TMBs) in a cohort of primarily mild TBI patients up to 30 days after injury. Researchers hypothesized that hypointense lesions on Apparent Diffusion Coefficient (ADC) detected acutely after injury would evolve into hyperintense Fluid Attenuated Inversion Recover (FLAIR) lesions.

METHODS

This study analyzed the progression of cerebral edema after acute injury using multimodal MRI to classify TMBs as potential edema-related biomarkers. ADC and FLAIR MRI were utilized for edema classification at three different timepoints: ≤48 hours, ~1 week, and 30 days after injury. Hypointense lesions on ADC (ADC+) suggested the presence of cytotoxic edema while hyperintense lesions on FLAIR (FLAIR+) suggested vasogenic edema. Signal intensity Ratio (SIR) calculations were made using ADC and FLAIR to quantitatively confirm edema progression.

RESULTS

Our results indicated the presence of ADC+ lesions ≤48 hours and ~1 week were associated with FLAIR+ lesions at ~1 week and 30 days, respectively, suggesting some progression of cytotoxic edema to vasogenic edema over time. Ten out of 15 FLAIR+ lesions at 30 days (67%) were ADC+ ≤48 hours. However, ADC+ lesions ≤48 hours were not associated with FLAIR+ lesions at 30 days; 10 out of 25 (40%) ADC+ lesions ≤48 hours were FLAIR+ at 30 days, which could indicate that some lesions resolved or were not visualized due to associated atrophy or tissue necrosis. Quantitative analysis confirmed the visual progression of some TMB lesions from ADC+ to FLAIR+. FLAIR SIRs at ~1 week were significantly higher when lesions were ADC+ ≤48 hours (1.22 [1.08-1.32] vs 1.03 [0.97-1.11], p=0.002).

CONCLUSION

Awareness of how cerebral edema can evolve in proximity to TMBs acutely after injury may facilitate identification and monitoring of patients with traumatic cerebrovascular injury and assist in development of novel therapeutic strategies.

摘要

引言

尽管创伤性脑损伤（TBI）后常出现脑水肿，但其形成和进展仍知之甚少。对于轻度TBI患者群体而言尤其如此，他们在受伤后的头几天很少接受磁共振成像（MRI）检查，而MRI能够发现计算机断层扫描无法显示的细微结构细节。本研究旨在对一组主要为轻度TBI的患者在受伤后30天内的脑水肿进展与创伤性微出血（TMBs）进行视觉分类和定量测量。研究人员推测，受伤后急性期检测到的表观扩散系数（ADC）低信号病变会演变为液体衰减反转恢复（FLAIR）高信号病变。

方法

本研究使用多模态MRI分析急性损伤后脑水肿的进展情况，将TMBs分类为潜在的与水肿相关的生物标志物。在三个不同时间点使用ADC和FLAIR MRI进行水肿分类：受伤后≤48小时、约1周和30天。ADC上的低信号病变（ADC+）提示存在细胞毒性水肿，而FLAIR上的高信号病变（FLAIR+）提示血管源性水肿。使用ADC和FLAIR进行信号强度比（SIR）计算以定量确认水肿进展。

结果

我们的结果表明，受伤后≤48小时和约1周时存在的ADC+病变分别与约1周和30天时的FLAIR+病变相关，提示随着时间推移细胞毒性水肿有一定程度进展为血管源性水肿。30天时15个FLAIR+病变中有10个（67%）在≤48小时时为ADC+。然而，受伤后≤48小时的ADC+病变与30天时的FLAIR+病变无关；25个≤48小时的ADC+病变中有10个（40%）在30天时为FLAIR+，这可能表明一些病变已消退或由于相关萎缩或组织坏死而未显示出来。定量分析证实了一些TMB病变从ADC+到FLAIR+ 的视觉进展。当病变在≤48小时时为ADC+时，约1周时的FLAIR SIRs显著更高（1.22 [1.08 - 1.32] 对比1.03 [0.97 - 1.11]，p = 0.002）。