Araki Y, Andoh A, Fujiyama Y, Bamba T
Department of Internal Medicine, Shiga University of Medical Science, Otsu, Japan.
Clin Exp Immunol. 2000 Feb;119(2):264-9. doi: 10.1046/j.1365-2249.2000.01094.x.
Ws/Ws rats have a small deletion of the c-kit gene, and are deficient in both mucosal-type mast cells (MMC) and connective tissue-type mast cells (CTMC). In the present study we investigated the role of intestinal MMC in the development of dextran sulphate sodium (DSS)-induced experimental colitis using Ws/Ws rats. Ws/Ws and control (+/+) rats were given a 3% DSS aqueous solution orally for 10 days, and the subsequent mucosal damage was evaluated macroscopically and histologically. The mucosal myeloperoxidase (MPO) activities and histamine levels were also measured. (i) DSS induced severe oedema and hyperaemia with sporadic erosions in the control (+/+) rats, but these changes were significantly attenuated in the Ws/Ws rats (P < 0.01). (ii) The microscopic mucosal damage score was lower in the Ws/Ws rats than in the control (+/+) rats (P = 0.06). (iii) There were no significant differences in mucosal MPO activity between the Ws/Ws and control (+/+) rats (P = 0.46). (iv) The mucosal histamine levels in the colon were significantly reduced in the Ws/Ws rats compared with the control (+/+) rats (P < 0.05). (v) Significant positive correlations were observed between mucosal histamine levels and the degree of mucosal oedema (calculated as colonic wet weight/protein content) (r = 0.778, P < 0.01), and between histamine levels and the macroscopic damage (r = 0.623, P < 0.05), respectively. (vi) DSS induced a local recruitment of MMC in the colonic mucosa of Ws/Ws rats, and mucosal damage gradually increased in accordance with this MMC recruitment. These results indicate that MMC play an important role in the development of DSS colitis.
Ws/Ws大鼠的c-kit基因存在小片段缺失,且缺乏黏膜型肥大细胞(MMC)和结缔组织型肥大细胞(CTMC)。在本研究中,我们使用Ws/Ws大鼠研究了肠道MMC在葡聚糖硫酸钠(DSS)诱导的实验性结肠炎发展中的作用。给Ws/Ws大鼠和对照(+/+)大鼠口服3% DSS水溶液,持续10天,随后通过宏观和组织学评估黏膜损伤情况。还测量了黏膜髓过氧化物酶(MPO)活性和组胺水平。(i)DSS在对照(+/+)大鼠中诱导了严重水肿、充血并伴有散在糜烂,但这些变化在Ws/Ws大鼠中明显减轻(P < 0.01)。(ii)Ws/Ws大鼠的微观黏膜损伤评分低于对照(+/+)大鼠(P = 0.06)。(iii)Ws/Ws大鼠和对照(+/+)大鼠之间的黏膜MPO活性无显著差异(P = 0.46)。(iv)与对照(+/+)大鼠相比,Ws/Ws大鼠结肠黏膜中的组胺水平显著降低(P < 0.05)。(v)分别观察到黏膜组胺水平与黏膜水肿程度(以结肠湿重/蛋白质含量计算)之间存在显著正相关(r = 0.778,P < 0.01),以及组胺水平与宏观损伤之间存在显著正相关(r = 0.623,P < 0.05)。(vi)DSS在Ws/Ws大鼠的结肠黏膜中诱导了MMC的局部募集,并且黏膜损伤随着这种MMC募集而逐渐增加。这些结果表明MMC在DSS结肠炎的发展中起重要作用。