血流量和一氧化氮合酶表达的时间模式影响侧枝生长过程中巨噬细胞的积累和增殖。

Journal of angiogenesis research Pub Date : 2010-09-16 DOI:10.1186/2040-2384-2-18

Hendrik B Sager, Ralf Middendorff, Kim Rauche, Joachim Weil, Wolfgang Lieb, Heribert Schunkert, Wulf D Ito

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引用次数: 10

摘要

背景:侧枝血流/流体剪切应力、一氧化氮(NO)和巨噬细胞在侧枝生长(动脉发生)过程中的参与是确定的，但它们的相互作用仍然是矛盾的。方法:为了进一步阐明“流体剪应力/NO/巨噬细胞”悖论，我们研究了股动脉闭塞后生长大鼠侧支血管侧支血流(多普勒血流探针)和NOS表达(免疫组化、Western blot)的时间过程及其对巨噬细胞募集和侧支增殖的影响(免疫组化、血管造影)。结果:(数值为平均值±标准误差平均值)闭塞早期侧支血流量明显减少(闭塞前90.0±4.5 μl/min vs闭塞后62.5±5.9 μl/min;p < 0.01)，局部诱导型NOS (iNOS)和内皮型NOS (eNOS)表达下调(闭塞后12 h，未闭塞组中eNOS的表达率为49.4±11.8%，iNOS的表达率为54.5±7.9%;P < 0.03)。最初减少的侧支血流量(由外周血管扩张引起)人工升高到闭塞前水平，减少侧支巨噬细胞募集(每侧支巨噬细胞:闭塞后42.5±4.4 vs.人工闭塞前27.8±2.0;P < 0.05)和侧枝增生减少(增生指数:术后0.54±0.02 vs人工预闭塞0.19±0.04;P < 0.001)。结论:我们提出了以下“流体剪切应力/NO/巨噬细胞”悖论的解决方案:在动脉形成过程中，侧支血流量和NOS表达最初减少，从而使巨噬细胞积聚，从而增强侧支增殖。巨噬细胞归巢后(闭塞后24 h)，侧支血流量和NOS表达恢复，以加入巨噬细胞恢复血流的作用。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Temporal patterns of blood flow and nitric oxide synthase expression affect macrophage accumulation and proliferation during collateral growth.

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Temporal patterns of blood flow and nitric oxide synthase expression affect macrophage accumulation and proliferation during collateral growth.

Background: The involvement of collateral blood flow/fluid shear stress, nitric oxide (NO), and macrophages during collateral growth (arteriogenesis) is established, but their interplay remains paradoxical.

Methods: In order to further elucidate the "fluid shear stress/NO/macrophage" paradox, we investigated the time course of collateral blood flow (using a Doppler flow probe) and NOS expression (immunohistochemistry, Western blot) in growing rat collateral vessels after femoral artery occlusion and their impact on macrophage recruitment and collateral proliferation (immunohistochemistry, angiographies).

Results: (values are given as mean ± standard error of mean) Early after occlusion, collateral blood flow was significantly reduced (pre- 90.0 ± 4.5 vs. post-occlusion 62.5 ± 5.9 μl/min; p < 0.01), and local inducible NOS (iNOS) and endothelial NOS (eNOS) expression were down-regulated (expression in % of non-occluded: eNOS 49.4 ± 11.8% and iNOS 54.5 ± 7.9% vs. non-occluded at 12 h after occlusion; p < 0.03). An artificial rise (induced by a peripheral vasodilatation) of the initially decreased collateral blood flow back to pre-occlusion levels reduced collateral macrophage recruitment (macrophages per collateral section: post- 42.5 ± 4.4 vs. artificial pre-occlusion 27.8 ± 2.0; p < 0.05) and diminished collateral proliferation (proliferative index: post- 0.54 ± 0.02 vs. artificial pre-occlusion 0.19 ± 0.04; p < 0.001) significantly 72 h after femoral artery occlusion.

Conclusions: We propose the following resolution of the "fluid shear stress/NO/macrophage" paradox: Collateral blood flow and NOS expression are initially reduced during arteriogenesis allowing macrophages to accumulate and therewith enhancing collateral proliferation. After homing of macrophages (24 h after occlusion), collateral blood flow and NOS expression recover in order to join the effects of macrophages for restoring blood flow.

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Journal of angiogenesis research

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