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Detection and appearance of intraparenchymal haematomas of the brain at 1.5 T with spin-echo, FLAIR and GE sequences: poor relationship to the age of the haematoma

机译:自旋回波,FLAIR和GE序列在1.5 T时检测和检测脑实质内血肿:与血肿年龄的关系较差

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The specific appearance of blood related to time at T1- and T2-weighted spin-echo (SE) sequences is generally accepted; thus, these sequences are classically used for estimating the age of haematomas. Magnetic resonance imaging at 1.5 T, including T1- and T2-weighted SE fluid-attenuated inversion recovery (FLAIR) and T2*-weighted gradient-echo (GE) sequences, was performed on 82 intraparenchymal haematomas (IPHs) and 15 haemorrhagic infarcts (HIs) in order to analyse the appearance at different stages and with different sequences, and to investigate how reliably the age of hematomas can be estimated. The IPHs had been previously detected by CT, were spontaneous (n=72) or traumatic (n=10) in origin and were of different sizes (2 mm to 7 cm) and ages (from 7.5 h to 4 years after acute haemorrhagic event). The age of the lesion was calculated from the moment when clinical symptoms started or the traumatic event occurred. The 15 patients with HIs were patients with ischaemic stroke in whom there was either a suspicion of haemorrhagic transformation on CT, or haemorrhage was detected as an additional finding on MR performed for other indications. Patients with conditions that could affect the SI of blood, such as anticoagulant therapy or severe anaemia, were excluded. The signal intensity pattern of the lesions was analysed and related to their ages without prior knowledge of the clinical data. All lesions were detected with T2*-weighted GE. T1-weighted SE missed 13 haematomas and T2-weighted SE and FLAIR sequences missed five. Haemorrhagic transformation was missed in three infarcts by T1-, T2-weighted SE and FLAIR. The signal pattern on FLAIR was identical to that on T2-weighted SE. For all sequences, a wide variety of signal patterns, without a clear relationship to the age of the haematomas, was observed. There was a poor relationship between the real MR appearance of IPHs and the theoretical appearance on SE sequences. T2*-weighted GE was effective for detecting small bleedings but was not useful for estimating the age of a lesion. The FLAIR does not provide any more information than T2-weighted SE.
机译:在T1和T2加权自旋回波(SE)序列上,与时间有关的血液的特定外观通常被接受。因此,这些序列通常用于估计血肿的年龄。在1.5 T时进行了磁共振成像,其中包括82例实质性内壁血肿(IPH)和15例出血性梗死(包括T1和T2加权的SE液衰减反转恢复(FLAIR)和T2 *加权的梯度回波(GE)序列)( HIs)是为了分析不同阶段和不同顺序的出现,并调查血肿年龄的可靠程度。 IPHs先前已经通过CT进行了检测,起源是自发的(n = 72)或外伤的(n = 10),大小不同(2 mm至7 cm),年龄不同(急性出血事件后7.5 h至4年) )。从临床症状开始或发生创伤事件的那一刻起计算病变的年龄。 15例HIs患者是缺血性中风患者,他们怀疑CT上有出血性转变,或者在其他适应症的MR上发现了出血。排除可能影响血液SI的疾病(例如抗凝治疗或严重贫血)的患者。在没有临床数据先验知识的情况下,分析了病变的信号强度模式并将其与年龄相关。所有病变均用T2 *加权GE检出。 T1加权的SE错过了13个血肿,T2加权的SE和FLAIR序列错过了5个。 T1,T2加权的SE和FLAIR在三个梗塞中错过了出血性转化。 FLAIR上的信号模式与T2加权SE上的信号模式相同。对于所有序列,观察到各种各样的信号模式,与血肿的年龄没有明显的关系。 IPH的真实MR外观与SE序列的理论外观之间的关系不佳。 T2 *加权GE可有效检测少量出血,但不能用于估计病变年龄。 FLAIR除了提供T2加权SE之外,没有提供更多信息。

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