甲基化精氨酸代谢产物作为Fontan循环患者临床状态及对5型磷酸二酯酶抑制反应的生物标志物
Methylated Arginine Metabolites as Biomarkers for Clinical Status and Response to Type 5 Phosphodiesterase Inhibition in Patients With Fontan Circulation.
作者信息
Cedars Ari, Manlhiot Cedric, Chinni Bhargava Kumar, Opotowsky Alexander R, Becker Kristian, Le Anne, Khare Pratik, Love Ko Jong, Everett Allen, Kutty Shelby, Russell Mark W, Payne R Mark, Atz Andrew M, McCrindle Brian W, Rathod Rahul H, Lewis Matthew, Goldberg David, Hill Kevin, Ploutz Michelle, Detterich Jon, Schumacher Kurt, Whitehill Robert, Penny Daniel J, Cartoski Mark, Sullivan Rachel, Files Matthew, Garg Ruchira, Wagner Jonathan, Jacobsen Roni, Nowlen Todd, Fletcher Scott, Conway Jennifer, Kim Gi Boem, Wu Fred, Zak Victor
机构信息
Johns Hopkins University Baltimore MD USA.
Cincinnati Children's Hospital University of Cincinnati College of Medicine Cincinnati OH USA.
出版信息
J Am Heart Assoc. 2025 Apr;14(7):e038061. doi: 10.1161/JAHA.124.038061. Epub 2025 Mar 26.
BACKGROUND
There is significant interest in NO pathway modulators, specifically type 5 phosphodiesterase inhibitors (PDE5is), to treat patients with a Fontan circulation. Trials, however, have had mixed results. The relationship between the NO pathway and clinical status in patients with Fontan circulation is a significant knowledge gap.
METHODS AND RESULTS
We performed targeted metabolomic analysis using liquid chromatography coupled to mass spectrometry to quantify plasma NO pathway metabolite concentrations from 2 well-characterized populations of patients with Fontan circulation: the Boston Adult Congenital Heart Disease Biobank and Fontan Udenafil Exercise Longitudinal studies. We investigated associations between NO metabolite concentrations and clinical outcomes, exercise capacity, and response to PDE5is. Increased plasma concentration of asymmetric dimethyl arginine (ADMA), an inhibitor of NO production, was associated with risk for hospitalization or death. Increased ADMA and symmetric dimethyl arginine (another inhibitor of NO production) concentrations were associated with decreased baseline exercise capacity among patients with Fontan circulation with <90% predicted peak oxygen uptake, and change in ADMA and symmetric dimethyl arginine concentrations were predictive of change in exercise capacity over time. Treatment with the PDE5i udenafil uncoupled this association. Finally, baseline ADMA and symmetric dimethyl arginine concentrations predicted response to PDE5is among patients with subnormal peak oxygen uptake.
CONCLUSIONS
Plasma concentrations of metabolites that inhibit NO flux are associated with negative clinical outcomes and worse exercise capacity. Moreover, metabolite shifts over time associated with increased NO flux are associated with improved exercise capacity. In patients with a Fontan circulation, the NO pathway modulators ADMA and symmetric dimethyl arginine may be useful as biomarkers of clinical status and predictive of response to PDE5is.
背景
一氧化氮(NO)通路调节剂,特别是5型磷酸二酯酶抑制剂(PDE5is),在治疗接受Fontan循环手术的患者方面备受关注。然而,相关试验结果不一。Fontan循环患者中NO通路与临床状况之间的关系存在重大知识空白。
方法与结果
我们采用液相色谱-质谱联用技术进行靶向代谢组学分析,以量化来自两个特征明确的Fontan循环患者群体(波士顿成人先天性心脏病生物样本库和Fontan伐地那非运动纵向研究)的血浆NO通路代谢物浓度。我们研究了NO代谢物浓度与临床结局、运动能力以及对PDE5is反应之间的关联。作为NO生成抑制剂的不对称二甲基精氨酸(ADMA)血浆浓度升高与住院或死亡风险相关。ADMA和对称二甲基精氨酸(另一种NO生成抑制剂)浓度升高与预测峰值摄氧量<90%的Fontan循环患者的基线运动能力下降相关,且ADMA和对称二甲基精氨酸浓度的变化可预测运动能力随时间的变化。使用PDE5i伐地那非治疗可消除这种关联。最后,基线ADMA和对称二甲基精氨酸浓度可预测峰值摄氧量未达正常水平的患者对PDE5is的反应。
结论
抑制NO通量的代谢物血浆浓度与不良临床结局和较差的运动能力相关。此外,随着时间推移与NO通量增加相关的代谢物变化与运动能力改善相关。在Fontan循环患者中,NO通路调节剂ADMA和对称二甲基精氨酸可能作为临床状况的生物标志物,并可预测对PDE5is的反应。
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