fractalkine/CX3CR1在肝肺综合征发病机制中的作用
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孙诚谊, Email: guhuajian_wh@163.com

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Effects of fractalkine/CX3CR1 on pathogenesis of hepatopulmonary syndrome
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    摘要:

    目的:探讨趋化因子fractalkine及其受体CX3CR1在大鼠肝肺综合征(HPS)发病机制中的作用。 方法:将40只大鼠行胆总管结扎后随机均分为模型组与治疗组,5只大鼠仅游离胆总管不结扎,作为假手术组;治疗组大鼠于术后15~28 d腹腔内注射CX3CR1中和抗体,模型组组与假手术组大鼠给予等容量生理盐水代替。术后29 d检测大鼠肝功能、动脉血气,肺组织病理学、肺血管内巨噬细胞(PIM)、微血管密度(MVD)及CX3CR1的表达。 结果:与假手术组比较,模型组大鼠血清谷丙转氨酶(ALT)、碱性磷酸酶(ALP)、总胆红素(TBIL)水平均明显升高,动脉血氧分压(PaO2)下降、肺泡-动脉血氧分压差(A-aDO2)升高,肺组织出现明显的病理改变、PIM(CD68表达量)、MVD增加(CD34表达量)、CX3CR1表达水平升高;治疗组大鼠肝功能也出现明显损伤,但好于模型组(均P<0.05),肺组织未见明显病理改变,血气指标、PIM、MVD、CX3CR1表达水平均无明显变化(均P>0.05)。 结论:fractalkine/CX3CR1在肺组织中表达增加并结合是HPS肺组织巨噬细胞聚积及微血管增生的关键信号通路,阻断该信号通路可抑制HPS的发生与发展。

    Abstract:

    Objective: To investigate the action of the chemotactic factor fractalkine and its receptor CX3CR1 in the pathogenesis of hepatopulmonary syndrome (HPS) in rats. Methods: Forty rats undergoing common bile duct ligation were equally randomized into model group and therapeutic group, and 5 rats subjected to isolation of the common bile duct only were served as sham operation group. Rats in therapeutic group received intraperitoneal injection with CX3CR1-neutralizing polyclonal antibody on postoperative day (POD) 15 to 28, while rats in model group and sham operation group were given normal saline of the same volume instead. On POD 29, rats were sacrificed, their liver function and arterial blood gas were determined, and the pathological changes, accumulation of pulmonary intravascular macrophages (PIM), microvessel density (MVD) and CX3CR1 expression in the lung tissues of rats were examined. Results: Compared with sham operation group, rats in model group showed significantly increased serum levels of alanine transaminase (ALT), alkaline phosphatase (ALP) and total bilirubin (TRIL), decreased arterial partial pressure of oxygen (PaO2), increased alveolar-arterial oxygen gradient (A-aDO2), clear pathological changes, and increased levels of PIM (CD86 expression), MVD (CD34 expression) and CX3CR1 expression in the lung tissues (all P<0.05); rats in therapeutic group showed liver function impairments as well, which however were milder than those in model group (all P<0.05), while there were no significant pathological changes in the lung tissues, and no obvious changes in arterial blood gas indexes and lung PIM, MVD and CX3CR1 expression (all P>0.05). Conclusion: Increased fractalkine/CX3CR1 expression and binding is an important signaling pathway for pulmonary macrophage aggregation and microvascular proliferation in HPS, and blockage of this pathway may inhibit the occurrence and development of HPS.

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谷化剑,孙诚谊,潘耀振,冯贤松,辛小燕 . fractalkine/CX3CR1在肝肺综合征发病机制中的作用[J].中国普通外科杂志,2014,23(8):1087-1092.
DOI:10.7659/j. issn.1005-6947.2014.08.015

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  • 收稿日期:2014-03-18
  • 最后修改日期:2014-06-25
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  • 在线发布日期: 2014-08-15