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Gastrointestinal cell proliferation and crypt fission are separate but complementary means of increasing tissue mass following infusion of epidermal growth factor in rats

机译:胃肠道细胞增殖和隐窝裂变是单独的但是补充大鼠表皮生长因子后增加组织质量的补充手段

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BACKGROUND AND AIMS—Epidermal growth factor (EGF) is a potent mitogen for the gastrointestinal tract and also influences the number of new crypts formed by crypt fission. The time course of these events and possible linkage between these two complementary mechanisms is however poorly understood. We therefore examined the temporal relationship of proliferation and fission in rats treated with EGF.
METHODS—Osmotic minipumps were implanted subcutaneously into male Wistar rats to infuse EGF continuously (60 µg/rat/day) for periods of 1-14 days. Proliferation and crypt branching were quantified following vincristine induced metaphase arrest and morphometric assessment of microdissected tissue.
RESULTS—In the small intestine, EGF significantly increased epithelial cell proliferation and crypt and villus area after 24 hours of EGF, although maximal effects were only reached following six days of infusion. EGF also resulted in an approximate 30% reduction in crypt fission in the small bowel. In the colon, EGF caused a twofold increase in epithelial cell proliferation one day after infusion, from 15.3 (2.3) to 29.6 (3.5) metaphases per crypt (p<0.01). Maximal effects were seen in rats receiving EGF for seven days. For all time points, colonic crypt size increased in response to EGF. The amount of branching increased following one day of infusion with EGF (from 15.3 (1.9) to 32.4 (5.5)%; p<0.001) but was significantly lower (approximately 25% of control values) following longer periods of infusion. Crypt fission did not correlate with crypt area.
CONCLUSION—EGF has profound effects on cell proliferation and also altered crypt fission, with its actions on crypt fission most pronounced in the colon where it first increased and then decreased fission. EGF can thus be a potent stimulus for crypt fission during short term infusion and may reduce the number of branched crypts present in a resting or quiescent stage. Growth factors can alter cell mass by two separate but linked mechanisms, namely altered cell production and crypt fission.


>Keywords: epithelium; cell division; cell proliferation; crypt fission; crypt branching; growth control; epidermal growth factor; rat
机译:背景与目的-表皮生长因子(EGF)是胃肠道的一种有力促分裂原,它还影响由隐窝裂变形成的新隐窝的数量。然而,人们对这些事件的时程以及这两个互补机制之间可能存在的联系知之甚少。因此,我们检查了用EGF处理的大鼠中增殖与裂变的时间关系。
方法-将渗透性微型泵皮下植入雄性Wistar大鼠中,以连续(60 µg /大鼠/天)的剂量注入EGF,持续1-14天。长春新碱诱导的中期停滞和微观解剖组织的形态计量学评估后,对增殖和隐窝分支进行了量化。
结果—在小肠中,EGF显着增加了EGF 24小时后上皮细胞的增殖以及隐窝和绒毛的面积,尽管最大的作用是仅在输注六天后达到。 EGF还导致小肠隐窝裂变减少了大约30%。在结肠中,EGF输注后一天导致上皮细胞增殖增加两倍,从每个隐窝的15.3(2.3)到29.6(3.5)中期(p <0.01)。在接受EGF 7天的大鼠中看到了最大的作用。在所有时间点上,结肠隐窝的大小均响应EGF而增加。输注EGF一天后分支量增加(从15.3(1.9)增至32.4(5.5)%; p <0.001),但在较长时间输注后显着降低(约为对照值的25%)。隐窝裂变与隐窝区域不相关。
结论—EGF对细胞增殖具有深远影响,并且改变了隐窝裂变,其对隐窝裂变的作用在结肠中最明显,首先在结肠中增加然后减少。因此,EGF可能是短期输注过程中隐窝裂变的有效刺激物,并可能减少处于静止或静止阶段的分支隐窝的数量。生长因子可以通过两个独立但相互联系的机制来改变细胞质量,即改变细胞产量和隐窝裂变。


>关键词:细胞分裂;细胞增殖;隐窝裂变隐窝分支;生长控制表皮生长因子鼠

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