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X连锁基因虎斑(Ta)对新生小鼠眼睑张开和门齿萌出的影响与表皮生长因子的影响相反。

Effect of the X-linked gene Tabby (Ta) on eyelid opening and incisor eruption in neonatal mice is opposite to that of epidermal growth factor.

作者信息

Kapalanga J, Blecher S R

机构信息

School of Human Biology, University of Guelph, Ontario, Canada.

出版信息

Development. 1990 Feb;108(2):349-55. doi: 10.1242/dev.108.2.349.

Abstract

Studies on eyelid opening and incisor eruption in 216 neonatal Tabby (Ta)-bearing mice and wildtype controls (35 Ta/Y, 62 + /Y, 30 Ta/Ta, 57 Ta/+ and 32 +/+) showed that in animals hemizygous and homozygous for Ta, the timing of eyelid opening and incisor eruption was significantly delayed (P less than 0.05). It was also observed that once open, the eyes of mutant pups do not remain open for long but soon close again for several days before reopening. An iterative eyes open-eyes closed process seems to continue beyond puberty. Studies in 25 epidermal growth factor (EGF)-treated mutants and 23 saline-treated controls showed that neonatal EGF injections (4 micrograms g-1 body weight per day) reversed the delayed timing of eyelid opening and incisor eruption in hemizygote and homozygote Tabby mice. However, both mutant and wildtype EGF-treated mice also showed the eyes open-eyes closed cycle, whereas untreated nonmutant mice did not. Because Tabby appears to be genetically homologous to the gene for human X-linked hypohidrotic ectodermal dysplasia, these results may have potential clinical significance. The eyes open-eyes closed cycle may involve cycling levels of EGF receptor; since the gene for this receptor shows homology with an oncogene, this system may be useful in studies on genetic control of oncogene function.

摘要

对216只携带新生儿虎斑(Ta)基因的小鼠和野生型对照小鼠(35只Ta/Y、62只+/Y、30只Ta/Ta、57只Ta/+和32只+/+)进行的眼睑张开和门齿萌出研究表明,对于Ta基因半合子和纯合子的动物,眼睑张开和门齿萌出的时间显著延迟(P小于0.05)。还观察到,突变幼崽的眼睛一旦睁开,不会长时间保持睁开状态,而是很快再次闭合几天,然后才重新睁开。这种反复的睁眼-闭眼过程似乎会持续到青春期之后。对25只经表皮生长因子(EGF)处理的突变体和23只经生理盐水处理的对照小鼠的研究表明,新生儿期注射EGF(每天4微克/克体重)可逆转半合子和纯合子虎斑小鼠眼睑张开和门齿萌出延迟的时间。然而,经EGF处理的突变体和野生型小鼠也都表现出睁眼-闭眼周期,而未经处理的非突变小鼠则没有。由于虎斑基因似乎与人类X连锁少汗性外胚层发育不良基因在遗传上同源,这些结果可能具有潜在的临床意义。睁眼-闭眼周期可能涉及EGF受体水平的循环;由于该受体的基因与一种癌基因具有同源性,这个系统可能有助于研究癌基因功能的遗传控制。

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