Department of Cardiovascular Science, Child and Family Research Institute, University of British Columbia, Vancouver, British Columbia, Canada.
J Thorac Cardiovasc Surg. 2010 Aug;140(2):305-312.e2. doi: 10.1016/j.jtcvs.2009.10.039. Epub 2010 Feb 26.
Losartan potassium (INN losartan), an antihypertensive drug, has been shown to prevent thoracic aortic aneurysm in Marfan syndrome through the inhibition of transforming growth factor beta. Recently we reported that doxycycline, a nonspecific inhibitor of matrix metalloproteinases 2 and 9, normalized aortic vasomotor function and suppressed aneurysm growth. We hypothesized that a combination of losartan potassium and doxycycline would offer better secondary prevention treatment than would single-drug therapy to manage thoracic aortic aneurysm.
A well-characterized mouse model of Marfan syndrome (Fbn1(C1039G/+)) was used. At 4 months of age, when aneurysm had established, mice (n = 15/group) were given doxycycline alone (0.24 g/L), losartan potassium alone (0.6 g/L), or combined (0.12-g/L doxycycline and 0.3-g/L losartan potassium) in drinking water. Littermate Fbn1(+/+) mice served as control. Thoracic aortas at 6 and 9 months were studied.
At 9 months, aortic diameter in untreated group was increased by 40% relative to control. Losartan potassium or doxycycline reduced aortic diameter by 10% to 16% versus untreated aortas. Losartan potassium and doxycycline combined completely prevented thoracic aortic aneurysm and improved elastic fiber organization, also downregulating matrix metalloproteinases 2 and 9 and transforming growth factor beta and normalizing aortic contractile and relaxation functions to control values.
Neither losartan potassium nor doxycycline alone completely restored vascular integrity and cell function when given during delayed treatment, indicating the importance of timed pharmacologic intervention. Combined, however, they synergistically offered better aneurysm-suppressing effects than did single-drug medication in the secondary prevention of thoracic aortic aneurysm.
血管紧张素 II 受体拮抗剂(氯沙坦钾,INN 氯沙坦)通过抑制转化生长因子-β已被证实可预防马凡综合征的胸主动脉瘤。最近我们报道,多西环素,基质金属蛋白酶 2 和 9 的非特异性抑制剂,可使主动脉血管舒缩功能正常化并抑制动脉瘤生长。我们假设氯沙坦钾和多西环素联合治疗比单一药物治疗更能为胸主动脉瘤的二级预防提供更好的治疗效果。
使用一种已被充分证实的马凡综合征(Fbn1(C1039G/+)) 小鼠模型。在 4 个月龄时,当动脉瘤已经形成时,将小鼠(每组 15 只)给予单独的多西环素(0.24 g/L)、氯沙坦钾(0.6 g/L)或联合用药(0.12g/L 多西环素和 0.3g/L 氯沙坦钾)饮用水。同窝 Fbn1(+/+) 小鼠作为对照。在 6 个月和 9 个月时研究胸主动脉。
未经治疗组的主动脉直径在 9 个月时相对于对照组增加了 40%。氯沙坦钾或多西环素使未经治疗的主动脉直径减少了 10%至 16%。氯沙坦钾和多西环素联合治疗完全预防了胸主动脉瘤,并改善了弹性纤维组织,还下调了基质金属蛋白酶 2 和 9 以及转化生长因子-β,使主动脉收缩和舒张功能恢复到对照值。
当在延迟治疗期间给予时,氯沙坦钾或多西环素单独治疗均不能完全恢复血管完整性和细胞功能,这表明及时进行药物干预的重要性。然而,联合使用时,它们在胸主动脉瘤的二级预防中比单一药物治疗具有更好的协同抑制动脉瘤作用。
