MMP-2/TIMP-2/TIMP-4 与 MMP-9/TIMP-3 在从代偿性肥大和血管生成向失代偿性心力衰竭的转变中的作用。
MMP-2/TIMP-2/TIMP-4 versus MMP-9/TIMP-3 in transition from compensatory hypertrophy and angiogenesis to decompensatory heart failure.
机构信息
Department of Physiology and Biophysics, University of Louisville School of Medicine, 500 South Preston Street, Louisville, KY 40202, USA.
出版信息
Arch Physiol Biochem. 2010 May;116(2):63-72. doi: 10.3109/13813451003652997.
Although matrix metalloproteinase (MMPs) and tissue inhibitor of metalloproteinase (TIMPs) play a vital role in tumour angiogenesis and TIMP-3 caused apoptosis, their role in cardiac angiogenesis is unknown. Interestingly, a disruption of co-ordinated cardiac hypertrophy and angiogenesis contributed to the transition to heart failure, however, the proteolytic and anti-angiogenic mechanisms of transition from compensatory hypertrophy to decompensatory heart failure were unclear. We hypothesized that after an aortic stenosis MMP-2 released angiogenic factors during compensatory hypertrophy and MMP-9/TIMP-3 released anti-angiogenic factors causing decompensatory heart failure. To verify this hypothesis, wild type (WT) mice were studied 3 and 8 weeks after aortic stenosis, created by banding the ascending aorta in WT and MMP-9-/- (MMP-9KO) mice. Cardiac function (echo, PV loops) was decreased at 8 weeks after stenosis. The levels of MMP-2 (western blot) increased at 3 weeks and returned to control level at 8 weeks, MMP-9 increased only at 8 weeks. TIMP-2 and -4 decreased at 3 and even more at 8 weeks. The angiogenic VEGF increased at 3 weeks and decreased at 8 weeks, the anti-angiogenic endostatin and angiostatin increased only at 8 weeks. CD-31 positive endothelial cells were more intensely labelled at 3 weeks than in sham operated or in 8 weeks banded mice. Vascularization, as estimated by x-ray angiography, was increased at 3 weeks and decreased at 8 weeks post-banding. Although the vast majority of studies were performed on control WT mice only, interestingly, MMP9-KO mice seemed to have increased vascular density 8 weeks after banding. These results suggested that there was increase in MMP-2, decrease in TIMP-2 and -4, increase in angiogenic factors and vascularization in compensatory hearts. However, in decompensatory hearts there was increase in MMP-9, TIMP-3, endostatin, angiostatin and vascular rarefaction.
虽然基质金属蛋白酶 (MMPs) 和金属蛋白酶组织抑制剂 (TIMPs) 在肿瘤血管生成中发挥着重要作用,TIMP-3 引起细胞凋亡,但它们在心脏血管生成中的作用尚不清楚。有趣的是,心脏肥厚和血管生成的协调失调会导致心力衰竭的发生,然而,从代偿性肥厚到失代偿性心力衰竭的转化的蛋白水解和抗血管生成机制尚不清楚。我们假设,在主动脉瓣狭窄时,MMP-2 释放血管生成因子,导致代偿性肥厚,MMP-9/TIMP-3 释放抗血管生成因子,导致失代偿性心力衰竭。为了验证这一假设,我们在主动脉瓣狭窄后 3 周和 8 周对野生型 (WT) 小鼠和 MMP-9-/- (MMP-9KO) 小鼠进行了研究,通过在 WT 和 MMP-9KO 小鼠的升主动脉上绑扎来制造主动脉瓣狭窄。狭窄 8 周后,心脏功能(回声、PV 环)下降。MMP-2 水平(western blot)在 3 周时升高,8 周时恢复到对照水平,MMP-9 仅在 8 周时升高。TIMP-2 和 -4 在 3 周时下降,在 8 周时下降更明显。血管生成因子 VEGF 在 3 周时升高,在 8 周时下降,抗血管生成因子内皮抑素和血管生成素仅在 8 周时升高。CD-31 阳性内皮细胞在 3 周时比假手术或 8 周时绑扎的小鼠更强烈标记。血管化程度(通过 X 射线血管造影估计)在绑扎后 3 周时增加,8 周时减少。虽然绝大多数研究仅在对照 WT 小鼠上进行,但有趣的是,MMP9-KO 小鼠在绑扎后 8 周时似乎增加了血管密度。这些结果表明,在代偿性心脏中,MMP-2 增加,TIMP-2 和 -4 减少,血管生成因子和血管化增加。然而,在失代偿性心脏中,MMP-9、TIMP-3、内皮抑素、血管生成素和血管稀疏增加。
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