Department of Inherited Metabolic Disorders, Queen Elizabeth Hospital Birmingham, Birmingham, UK.
Institute of Cardiovascular Science, University of Birmingham, Birmingham, UK.
Orphanet J Rare Dis. 2020 Jun 5;15(1):139. doi: 10.1186/s13023-020-01426-4.
Alström syndrome (ALMS) is a rare ciliopathy characterised by early onset insulin resistance, obesity, and dyslipidaemia and is a model for diseases that have huge social, health and economic impact. Cardiomyopathy develops in the majority, with high rates of morbidity and mortality, the definitive features of which are coarse replacement fibrosis and diffuse myocardial fibrosis (DIF). The pathogenesis of heart failure is thought to involve fibroblast accumulation and expansion of the extracellular matrix with excess protein deposition, leading to distorted organ architecture and impaired contractile function. Consecutive adults with genetically proven ALMS attending the National Centre for Rare Disease in Birmingham, England were studied. All patients underwent serial CMR, echocardiography and venous blood sampling, with computed tomography coronary angiography (CTCA) performed to assess severity of CAD. The aims of this study were: 1) to evaluate changes over time in DIF by cardiovascular magnetic resonance tissue characterization in ALMS; 2) to examine whether changes in DIF are associated with alteration in systolic or diastolic function; and 3) to evaluate the frequency and severity of coronary artery disease as a confounder for progression of ischaemic versus non-ischaemic fibrosis.
In total, 30/32 adults (63% male; 67% White British) participated. The median age at first scan was 21.3 years (interquartile range: 19.0-32.6) and participants were followed for a maximum of 67 months. Only 4 patients had significant coronary artery stenosis on post-mortem, invasive coronary angiography or CTCA. Mid short axis myocardial T1 times, myocardial extracellular volume, and left ventricular mass increased significantly over time, by an average of 21.8 ms (95% CI 17.4-26.1; p < 0.001), 1.1 percentage points (0.6-1.6, p < 0.001), and 2.8 g/m (1.9-3.7; p < 0.001) per year, respectively. These changes were not associated with significant deterioration in myocardial structure or function.
This is the first comprehensive prospective study demonstrating progression of DIF in ALMS over time, although no structural or functional consequences were noted within a median three and a half years' follow up. Further study is warranted to define whether DIF is a by-stander or the driver to impaired contractile function, heart failure and death.
Alström 综合征(ALMS)是一种罕见的纤毛病,其特征为早期发生胰岛素抵抗、肥胖和血脂异常,是一种具有巨大社会、健康和经济影响的疾病模型。大多数患者会发生心肌病,发病率和死亡率都很高,其明确特征为粗糙的替代纤维化和弥漫性心肌纤维化(DIF)。心力衰竭的发病机制被认为涉及成纤维细胞的积累和细胞外基质的扩张,伴有过量的蛋白沉积,导致器官结构扭曲和收缩功能受损。本研究纳入了连续就诊于英国伯明翰国家罕见疾病中心的、经基因证实的 ALMS 成年患者。所有患者均接受了连续心脏磁共振成像(CMR)、超声心动图和静脉血样采集,还进行了计算机断层扫描冠状动脉造影(CTCA)以评估 CAD 的严重程度。本研究的目的为:1)通过 ALMS 的心血管磁共振组织特征评估 DIF 随时间的变化;2)检测 DIF 的变化是否与收缩或舒张功能的改变相关;3)评估冠状动脉疾病的发生频率和严重程度是否会影响缺血性或非缺血性纤维化的进展。
共纳入 32 名成年人(63%为男性;67%为白种英国人)。首次扫描时的中位年龄为 21.3 岁(四分位间距:19.0-32.6),随访时间最长为 67 个月。尸检、有创冠状动脉造影或 CTCA 仅显示 4 例患者存在显著的冠状动脉狭窄。平均随访 21.8 毫秒(95%置信区间:17.4-26.1;p<0.001)、1.1 个百分点(0.6-1.6,p<0.001)和 2.8 克/米(1.9-3.7;p<0.001)后,心肌短轴 T1 时间、心肌细胞外容积和左心室质量呈显著增加趋势。每年分别为 21.8ms(95% CI 17.4-26.1;p < 0.001)、1.1 个百分点(0.6-1.6,p < 0.001)和 2.8 克/米(1.9-3.7;p < 0.001)。这些变化与心肌结构或功能的显著恶化无关。
这是首次全面的前瞻性研究,证明了 ALMS 中的 DIF 随时间的进展,尽管在中位 3 年半的随访中未发现结构或功能方面的不良后果。需要进一步的研究来明确 DIF 是收缩功能障碍、心力衰竭和死亡的旁观者还是驱动因素。
