Ophthalmology department, Saint Martin hospital, Ramsay Générale de Santé, 18 rue des Roquemonts, 14000 Caen, France; Clinical Investigation Center 1423, Quinze-Vingts hospital, INSERM-DHOS, Paris F-75012, France.
Nephrology department, Saint Martin hospital, Ramsay Générale de Santé, 18 rue des Roquemonts, 14000 Caen, France.
Microvasc Res. 2023 Jan;145:104450. doi: 10.1016/j.mvr.2022.104450. Epub 2022 Nov 11.
Mutations of the COL4A1 gene, a major structural protein of vessels, may cause hereditary angiopathy with nephropathy, aneurysms and muscle cramps (HANAC) syndrome. The vascular structure and function of patients with HANAC is poorly known. Here, we report a family with HANAC syndrome associated to a previously unreported mutation in COL4A1. The structure and function of retinal vessels were detailed by adaptive optics ophthalmoscopy (AOO) and optical coherence tomography (OCT) angiography.
Clinical data from six affected individuals (43 to 72 years old) from a single family comprising two generations were collected. Imaging charts including conventional fundus imaging, OCT-angiography and AOO in static and dynamic (flicker) mode were reviewed. DNA sequencing was done in the proband.
DNA sequencing of the proband revealed a heterozygous deletion of COL4A1 (NM_001845) at position 1120 in the intron 20 resulting in the loss of splicing donor site for exon 20 (c.1120 + 2_1120 + 8del heterozygote). Four patients had arterial hypertension, and three had kidney dysfunction, one of which under dialysis. By fundus examination, five had typical retinal arteriolar tortuosity with arteriolar loops. Wall-to-lumen ratio of arteries was within normal limits, that is, lower than expected for hypertensive patients. Several foci of arteriolar irregularities were noted in the two oldest patients. In three affected subjects, evaluation of the neurovascular coupling showed a higher flicker-induced vasodilation than a control population (6 % to 11 %; n < 5 %).
Structural and dynamic analysis of retinal vessels in a HANAC family bearing a previously unreported intronic COL4 mutation was done. In addition to arteriolar tortuosity, we found reduced wall-to-lumen ratio, arteriolar irregularity and increased vasodilatory response to flicker light. These abnormalities were more marked in the oldest subjects. This abnormal flicker response affected also non-tortuous arteries, suggesting that microvascular dysfunction extends beyond tortuosity. Such explorations may help to better vascular dysfunction related to HANAC and hence better understand the mechanisms of end-organ damage.
COL4A1 基因突变可能导致伴有肾病、动脉瘤和肌肉痉挛的遗传性血管病(HANAC)综合征。HANAC 患者的血管结构和功能知之甚少。在这里,我们报告了一个家族性 HANAC 综合征病例,该家族与 COL4A1 中一个以前未报道的突变有关。通过自适应光学检眼镜(AOO)和光相干断层扫描血管造影术(OCTA)详细研究了视网膜血管的结构和功能。
收集了一个由两代人组成的单一家族的 6 名受影响个体(43 至 72 岁)的临床数据。回顾了包括常规眼底成像、OCTA 和 AOO 在内的成像图表,包括静态和动态(闪烁)模式。对先证者进行 DNA 测序。
对先证者的 DNA 测序显示 COL4A1(NM_001845)第 20 内含子 1120 位的杂合缺失导致外显子 20 的剪接供体位点缺失(c.1120+2_1120+8del 杂合子)。4 名患者患有动脉高血压,3 名患者肾功能不全,其中 1 名患者正在接受透析。眼底检查发现,5 名患者有典型的视网膜小动脉迂曲伴小动脉环。动脉的管壁腔比在正常范围内,即低于高血压患者的预期值。在两名最年长的患者中,发现了几个小动脉不规则的病灶。在 3 名受影响的受试者中,神经血管耦合的评估显示闪烁诱导的血管扩张高于对照组(6%至 11%;n<5)。
对携带以前未报道的内含子 COL4 突变的 HANAC 家族的视网膜血管进行了结构和动态分析。除了小动脉迂曲外,我们还发现管壁腔比降低、小动脉不规则和闪烁光诱导的血管舒张反应增加。这些异常在最年长的受试者中更为明显。这种异常的闪烁反应也影响了非迂曲的动脉,表明微血管功能障碍不仅限于迂曲。这种探索可能有助于更好地了解与 HANAC 相关的血管功能障碍,并更好地理解终末器官损伤的机制。
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