大鼠硫酸葡聚糖结肠炎中通透性增加：发展的时间进程及丁酸盐的作用

Increased permeability in dextran sulphate colitis in rats: time course of development and effect of butyrate.

作者信息

Venkatraman A, Ramakrishna B S, Pulimood A B, Patra S, Murthy S

机构信息

Dept. of Gastrointestinal Sciences, Christian Medical College Hospital, Vellore, India.

出版信息

Scand J Gastroenterol. 2000 Oct;35(10):1053-9. doi: 10.1080/003655200451171.

DOI:10.1080/003655200451171

PMID:11099058

Abstract

BACKGROUND

Increased mucosal permeability is an important factor in the genesis of mucosal inflammation in inflammatory bowel disease. This study examined the time course of increased permeability and the effect of butyrate on permeability in experimental colitis in rats.

METHODS

Colitis was induced in albino rats by administration of 4% dextran sulphate sodium (DSS) orally for up to 7 days. Rats were killed sequentially after 1-7 days of DSS feeding and compared with control animals. Distal colon sheets, from normal and DSS rats, were mounted in Ussing chambers. Electric resistance and passive permeation of 14C-mannitol were measured over 90 min. In control and 5-day DSS rats additional permeability measurements were made in the presence of butyrate (25 mmol/l) in the bathing solutions. The permeability of the normal distal colon was measured after addition of DSS in vitro. Sections of colon were examined by light microscopy. The viability of colonocytes, from normal and DSS rat colon, was measured by release of lactate dehydrogenase immediately and during a 60-min incubation after isolation.

RESULTS

Focal mild inflammation and shedding of epithelium were noted after 2 days of DSS administration; crypt loss with flattened epithelium in adjacent areas after 5 days; and fibrosis after 7 days. Decreased epithelial cell survival after 60 min of incubation was noted after 1 day of DSS administration, whereas decreased viability at the time of isolation was noted after 2 days of DSS administration (viability, 72.7% +/- 1.4%; mean +/- standard error) compared with control (89.3% +/- 0.8%) (P < 0.01). Increased permeability was noted after 1 day of DSS administration. Electric resistance (mu omega/cm2/h) was significantly reduced after 1 day of DSS administration to 85.9 +/- 4.6 (mean +/- standard error) compared with control animals (117.2 +/- 2.2; P < 0.001). Serosa-mucosa flux of mannitol (micromol/cm2/h) was also significantly increased after 1 day of DSS feeding (0.169 +/- 0.01) compared with control (0.061 +/- 0.08) (P < 0.01). Electric resistance and mannitol permeability were significantly returned towards normal by the presence of butyrate. DSS added directly to the bathing solution did not significantly alter the colon permeability in vitro.

CONCLUSIONS

Increased mucosal permeability is a very early change in colitis induced by DSS, is accompanied by decreased cell survival, and precedes detectable changes in histology. Reversal of increased mucosal permeability by butyrate may explain its utility in the therapy of inflammatory disease of the colon.

摘要

背景

黏膜通透性增加是炎症性肠病黏膜炎症发生的一个重要因素。本研究检测了实验性大鼠结肠炎中通透性增加的时间进程以及丁酸盐对通透性的影响。

方法

通过口服4%硫酸葡聚糖钠（DSS）诱导白化大鼠患结肠炎，持续7天。在给予DSS喂养1 - 7天后依次处死大鼠，并与对照动物进行比较。将正常大鼠和DSS大鼠的远端结肠片安装在尤斯灌流小室中。在90分钟内测量跨上皮电阻和14C - 甘露醇的被动渗透。在对照大鼠和给予DSS 5天的大鼠中，在浴液中加入丁酸盐（25 mmol/L）后进行额外的通透性测量。在体外加入DSS后测量正常远端结肠的通透性。通过光学显微镜检查结肠切片。通过立即分离后及分离后60分钟孵育期间乳酸脱氢酶的释放来测量正常大鼠和DSS大鼠结肠中结肠上皮细胞的活力。

结果

给予DSS 2天后可见局灶性轻度炎症和上皮脱落；5天后可见隐窝缺失，相邻区域上皮扁平；7天后出现纤维化。给予DSS 1天后，孵育60分钟后上皮细胞存活率降低，而给予DSS 2天后分离时可见活力降低（活力为72.7%±1.4%；平均值±标准误），与对照（89.3%±0.8%）相比（P<0.01）。给予DSS 1天后可见通透性增加。给予DSS 1天后，跨上皮电阻（μΩ/cm²/h）显著降低至85.9±4.6（平均值±标准误），与对照动物（117.2±2.2）相比（P<0.001）。给予DSS 1天后，甘露醇的浆膜 - 黏膜通量（μmol/cm²/h）也显著增加（0.169±0.01），与对照（0.061±0.08）相比（P<0.01）。丁酸盐的存在使跨上皮电阻和甘露醇通透性显著恢复至正常。直接向浴液中加入DSS在体外并未显著改变结肠通透性。