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T1 映射作为 T2* 的补充工具在无创性心脏铁过载评估中的作用。

Role of T1 mapping as a complementary tool to T2* for non-invasive cardiac iron overload assessment.

作者信息

Torlasco Camilla, Cassinerio Elena, Roghi Alberto, Faini Andrea, Capecchi Marco, Abdel-Gadir Amna, Giannattasio Cristina, Parati Gianfranco, Moon James C, Cappellini Maria D, Pedrotti Patrizia

机构信息

Department of Cardiovascular, Neural and Metabolic Sciences, San Luca Hospital, Istituto Auxologico Italiano, Milan, Italy.

Rare Diseases Centre, Department of Medicine and Medical Specialities, "Ca' Granda" Foundation IRCCS, Milan, Italy.

出版信息

PLoS One. 2018 Feb 21;13(2):e0192890. doi: 10.1371/journal.pone.0192890. eCollection 2018.

Abstract

BACKGROUND

Iron overload-related heart failure is the principal cause of death in transfusion dependent patients, including those with Thalassemia Major. Linking cardiac siderosis measured by T2* to therapy improves outcomes. T1 mapping can also measure iron; preliminary data suggests it may have higher sensitivity for iron, particularly for early overload (the conventional cut-point for no iron by T2* is 20ms, but this is believed insensitive). We compared T1 mapping to T2* in cardiac iron overload.

METHODS

In a prospectively large single centre study of 138 Thalassemia Major patients and 32 healthy controls, we compared T1 mapping to dark blood and bright blood T2* acquired at 1.5T. Linear regression analysis was used to assess the association of T2* and T1. A "moving window" approach was taken to understand the strength of the association at different levels of iron overload.

RESULTS

The relationship between T2* (here dark blood) and T1 is described by a log-log linear regression, which can be split in three different slopes: 1) T2* low, <20ms, r2 = 0.92; 2) T2* = 20-30ms, r2 = 0.48; 3) T2*>30ms, weak relationship. All subjects with T2*<20ms had low T1; among those with T2*>20ms, 38% had low T1 with most of the subjects in the T2* range 20-30ms having a low T1.

CONCLUSIONS

In established cardiac iron overload, T1 and T2* are concordant. However, in the 20-30ms T2* range, T1 mapping appears to detect iron. These data support previous suggestions that T1 detects missed iron in 1 out of 3 subjects with normal T2*, and that T1 mapping is complementary to T2*. The clinical significance of a low T1 with normal T2* should be further investigated.

摘要

背景

铁过载相关的心力衰竭是依赖输血患者(包括重型地中海贫血患者)的主要死亡原因。将通过T2测量的心脏铁沉积与治疗相联系可改善预后。T1映射也可测量铁;初步数据表明其对铁可能具有更高的敏感性,尤其是对于早期铁过载(T2判断无铁的传统阈值为20毫秒,但人们认为该阈值不敏感)。我们比较了心脏铁过载时T1映射与T2*的情况。

方法

在一项对138例重型地中海贫血患者和32名健康对照者进行的前瞻性大型单中心研究中,我们将T1映射与在1.5T下采集的黑血和亮血T2进行了比较。采用线性回归分析评估T2与T1的相关性。采用“移动窗口”方法来了解不同铁过载水平下的相关强度。

结果

T2*(此处指黑血)与T1之间的关系由对数-对数线性回归描述,该回归可分为三个不同斜率:1)T2低,<20毫秒,r2 = 0.92;2)T2* = 20 - 30毫秒,r2 = 0.48;3)T2*>30毫秒,关系较弱。所有T2<20毫秒的受试者T1均较低;在T2*>20毫秒的受试者中,38%的人T1较低,T2*范围在20 - 30毫秒的大多数受试者T1较低。

结论

在已确诊的心脏铁过载中,T1和T2是一致的。然而,在T2为20 - 30毫秒的范围内,T1映射似乎能检测到铁。这些数据支持了之前的观点,即T1能在三分之一T2正常的受试者中检测到遗漏的铁,且T1映射是T2的补充。T2*正常但T1较低的临床意义应进一步研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4d17/5821344/118be133de9c/pone.0192890.g001.jpg

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