PRKG1 突变 c.530G>A(p.Arg177Gln)患者的 B 型主动脉夹层的自然病史。
The natural history of type B aortic dissection in patients with PRKG1 mutation c.530G>A (p.Arg177Gln).
机构信息
Division of Vascular Surgery, Department of Surgery, University of Washington School of Medicine, Seattle, Wash.
Division of Medical Genetics, Department of Internal Medicine, The University of Texas Health Science Center at Houston, Houston, Tex.
出版信息
J Vasc Surg. 2019 Sep;70(3):718-723. doi: 10.1016/j.jvs.2018.12.032. Epub 2019 Mar 11.
OBJECTIVE
The c.530G>A (p.Arg177Gln) mutation in PRKG1 has been shown to be associated with thoracic aortic aneurysms and dissections. This rare mutation accounts for an estimated 1% of nonsyndromic heritable thoracic aortic disease. We sought to describe the clinical presentation of type B aortic dissection (TBAD), management, and outcomes in patients with this mutation.
METHODS
This is a descriptive multi-institutional retrospective study of patients from six families with the PRKG1 mutation. Patients with TBAD were selected for analysis. Demographics, family histories, TBAD management, and outcomes were reviewed.
RESULTS
Of the 29 individuals diagnosed with the PRKG1 mutation, 12 (41.3%) had TBAD (50% male, TBAD median age: 31 years [range, 16-58 years], median follow-up: 6 years [range, 3-15 years] after TBAD). All had a family history of aortic dissections and none had features of Marfan syndrome. The median size of the descending thoracic aorta (DTA) at TBAD was 4.1 cm (range, 3.8-5 cm). Most cases (9 acute TBAD, 1 incidental TBAD diagnosis during screening) were managed medically. One case had open DTA repair the acute phase. Repair for dissection-related aneurysmal degeneration was performed in seven cases (58.3%) in the chronic phase at a median of 2 years (range, 1-8 years) after TBAD. In four cases (33.3%), the DTA remained stable in size over a range of 1 to 7 years after TBAD. Type A aortic dissection subsequent to TBAD occurred in three cases (25%). There were four (33.3%) deaths in the series, all aortic related at a median age of 24 years (range, 19-43 years).
CONCLUSIONS
The PRKG1 (p.Arg177Gln) mutation although rare is associated with nonsyndromic TBAD in young and middle-aged patients. Workup for this gene mutation should be included as part of the workup for TBAD etiology in relatively young patients and those with familial history of aortic dissections. Once diagnosed, testing of first-degree family members is warranted. In all individuals with a PRKG1 mutation, close follow-up for aortic root dilatation and hypertension control is essential to reduce the risk of type A or type B aortic dissection, and in cases of TBAD, to decrease the risk of dissection-related aneurysmal degeneration.
目的
PRKG1 中的 c.530G>A(p.Arg177Gln)突变与胸主动脉瘤和夹层有关。这种罕见的突变约占非综合征遗传性胸主动脉疾病的 1%。我们旨在描述携带该突变患者的 B 型主动脉夹层(TBAD)的临床表现、治疗方法和结局。
方法
这是一项来自六个 PRKG1 突变家族的患者的多机构回顾性描述性研究。选择 TBAD 患者进行分析。回顾了人口统计学、家族史、TBAD 治疗方法和结局。
结果
在诊断为 PRKG1 突变的 29 人中,有 12 人(41.3%)患有 TBAD(50%为男性,TBAD 中位年龄:31 岁[范围,16-58 岁],TBAD 后中位随访时间:6 年[范围,3-15 年])。所有人都有主动脉夹层的家族史,且均无马凡综合征的特征。TBAD 时降主动脉(DTA)的中位大小为 4.1cm(范围,3.8-5cm)。大多数病例(9 例急性 TBAD,1 例在筛查期间偶然诊断为 TBAD)采用药物治疗。1 例在急性期行开放 DTA 修复。TBAD 后 2 年(范围,1-8 年)的慢性期,有 7 例(58.3%)因夹层相关动脉瘤样变行修复治疗。4 例(33.3%)在 TBAD 后 1 至 7 年内 DTA 大小保持稳定。3 例(25%)在 TBAD 后发生 A 型主动脉夹层。该系列中共有 4 例(33.3%)死亡,均与主动脉相关,中位年龄为 24 岁(范围,19-43 岁)。
结论
尽管 PRKG1(p.Arg177Gln)突变罕见,但它与年轻和中年患者的非综合征性 TBAD 有关。对于相对年轻的患者和有主动脉夹层家族史的患者,应将该基因突变的筛查作为 TBAD 病因学检查的一部分。一旦确诊,应进行一级亲属的检测。对于所有携带 PRKG1 突变的患者,应密切随访主动脉根部扩张和高血压控制情况,以降低发生 A 型或 B 型主动脉夹层的风险,对于 TBAD 患者,降低夹层相关动脉瘤样变的风险。
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