Skoro-Sajer N, Bonderman D, Wiesbauer F, Harja E, Jakowitsch J, Klepetko W, Kneussl M P, Lang I M
Division of Cardiology, Vienna General Hospital, Medical University of Vienna, Vienna, Austria.
J Thromb Haemost. 2007 Mar;5(3):483-9. doi: 10.1111/j.1538-7836.2007.02394.x.
Chronic thromboembolic pulmonary hypertension (CTEPH) results from non-resolving pulmonary thromboemboli that are resistant to plasmatic anticoagulation. Because of a secondary pulmonary arteriopathy accompanying major vessel obstruction, the disorder may be a target for vasodilator therapy.
In an open-label uncontrolled study, we investigated the prostacyclin analog treprostinil given s.c. in patients with severe inoperable CTEPH.
Between September 1999 and September 2005, 25 patients were included if their World Health Organization (WHO) functional class was III or IV, if their six-minute walking distance (6-MWD) <or= 380 m, and if they had undergone at least one hospitalization for right heart decompensation within the prior six months, albeit not within one month before treatment start. Right heart catheterization was performed at baseline and after a minimum of 12 months (range: 12-33 months) of treatment. Treprostinil plasma concentrations were determined after at least six months of treatment. A historical group of 31 patients at our center with inoperable CTEPH matched for disease severity was used for comparative analyses.
Treprostinil-treated patients demonstrated significant improvements in 6-MWD (P = 0.01), WHO functional class (P = 0.001), B-type brain natriuretic peptide plasma levels (P = 0.02), cardiac outputs (P = 0.007) and pulmonary vascular resistances (P = 0.01) after 19 +/- 6.3 months. Treprostinil plasma concentrations correlated with drug dose (P < 0.001), indicating stable absorption over time. Long-term survival was significantly better than in controls.
Treprostinil improves exercise capacity, hemodynamics and survival in patients with severe inoperable CTEPH. We speculate that the effects may be explained by a combined vasodilatory, platelet-antagonistic and potential antiproliferative action of the drug.
慢性血栓栓塞性肺动脉高压(CTEPH)由对血浆抗凝有抵抗性的未溶解肺血栓栓子引起。由于伴有大血管阻塞的继发性肺动脉病变,该疾病可能是血管扩张剂治疗的靶点。
在一项开放标签的非对照研究中,我们调查了皮下注射前列环素类似物曲前列尼尔对重度无法手术的CTEPH患者的疗效。
1999年9月至2005年9月期间,纳入25例患者,要求其世界卫生组织(WHO)功能分级为III级或IV级,6分钟步行距离(6-MWD)≤380 m,且在之前6个月内至少因右心失代偿住院1次,但在治疗开始前1个月内未住院。在基线时以及至少治疗12个月(范围:12 - 33个月)后进行右心导管检查。在至少治疗6个月后测定曲前列尼尔血浆浓度。使用本中心31例病情严重程度匹配的无法手术的CTEPH患者的历史队列进行比较分析。
曲前列尼尔治疗的患者在19±6.3个月后,6-MWD(P = 0.01)、WHO功能分级(P = 0.001)、B型脑钠肽血浆水平(P = 0.02)、心输出量(P = 0.007)和肺血管阻力(P = 0.01)均有显著改善。曲前列尼尔血浆浓度与药物剂量相关(P < 0.001),表明随着时间推移吸收稳定。长期生存率显著优于对照组。
曲前列尼尔可改善重度无法手术的CTEPH患者的运动能力、血流动力学和生存率。我们推测这些作用可能由该药物的血管舒张、血小板拮抗和潜在的抗增殖联合作用来解释。
