阻断p-选择素可减少小鼠睾丸缺血-再灌注损伤后中性粒细胞的浸润。

M Celebi, A G A Paul
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摘要

缺血再灌注(I/R)诱导睾丸损伤后生殖细胞特异性凋亡依赖于中性粒细胞向睾丸的募集。血管内粘附分子如P-和E-选择素在这种招募中起重要作用。本研究的目的是利用功能阻断单克隆抗小鼠p -选择素抗体抑制I/R诱导的睾丸损伤中性粒细胞募集。将成年小鼠进行2小时的睾丸扭转(缺血),然后再扭转(再灌注)。再灌注开始10分钟后,小鼠接受100微克功能阻断单克隆p选择素抗体(FBMAB组)或同型匹配对照抗体(IMCA组)。各组小鼠分别采用假手术(SO组)或tnf α 500 ng (IF组)诱导炎症。再灌注24 h后处死小鼠,分离睾丸间质细胞,流式细胞术检测中性粒细胞的存在。功能阻断型单克隆p -选择素抗体显著降低I/R诱导睾丸损伤中性粒细胞募集(FBMAB组与IMCA组相比,Gr-1 + cd11b +占总白细胞的比例为26 +/- 4 vs 52 +/- 10%;P < 0.001)。因此,阻断p -选择素可能在治疗上有利于保护前列腺癌后的睾丸。
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Blockade of p-selectin reduces neutrophil infiltration into the murine testis after ischemia-reperfusion-injury.

Germ cell specific apoptosis after ischemia-reperfusion (I/R) induced testicular injury is dependent on neutrophil recruitment to the testis. Intravascular adhesion molecules like the P- and E- selectins play an important role in this recruitment.The purpose of this study was to inhibit neutrophil recruitment in I/R induced testicular injury by using a function-blocking monoclonal anti-mouse P-selectin antibody. Adult mice were subjected to a 2 h period of testicular torsion (ischemia) followed by detorsion (reperfusion).Ten minutes after the onset of reperfusion, mice received either 100 microg of a function-blocking monoclonal P-selectin antibody (FBMAB group) or isotype-matched control antibody (IMCA group). Separate groups of mice underwent sham-operation (SO group) or received 500 ng of TNFalpha (IF group) to induce inflammation. Mice were sacrificed 24 h after reperfusion and testiscular interstitial cells were isolated and analyzed for the presence of neutrophils by means of flow cytometry. The function-blocking monoclonal P-selectin antibody reduced neutrophil recruitment in I/R induced testicular injury significantly (FBMAB group as compared to the IMCA group 26 +/- 4 vs. 52 +/- 10% Gr-1 +CD11 b+ of total leucocytes; P < 0.001). Therefore, blocking P-selectin may be therapeutically beneficial to protect postischemic testis.

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