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mSpry-2(果蝇Sprouty的小鼠同源物)的保守功能,其对呼吸器官发生起负向调节作用。

Conserved function of mSpry-2, a murine homolog of Drosophila sprouty, which negatively modulates respiratory organogenesis.

作者信息

Tefft J D, Lee M, Smith S, Leinwand M, Zhao J, Bringas P, Crowe D L, Warburton D

机构信息

Center for Craniofacial Molecular Biology Departments of Surgery and Pediatrics The Childrens Hospital Los Angeles Research Institute University of Southern California Schools of Dentistry and Medicine Los Angeles California 90033, USA.

出版信息

Curr Biol. 1999 Feb 25;9(4):219-22. doi: 10.1016/s0960-9822(99)80094-3.

Abstract

In Drosophila embryos, the loss of sprouty gene function enhances branching of the respiratory system. Three human sprouty homologues (h-Spry1-3) have been cloned recently, but their function is as yet unknown [1]. Here, we show that a murine sprouty gene (mSpry-2), the product of which shares 97% homology with the respective human protein, is expressed in the embryonic murine lung. We used an antisense oligonucleotide strategy to reduce expression of mSpry-2 by 96%, as measured by competitive reverse transcriptase PCR, in E11. 5 murine embryonic lungs cultured for 4 days [2]. Morphologically, the decrease in mSpry-2 expression resulted in a 72% increase in embryonic murine lung branching morphogenesis as well as a significant increase in expression of the lung epithelial marker genes SP-C, SP-B and SP-A. These results support a striking conservation of function between the Drosophila and mammalian sprouty gene families to negatively modulate respiratory organogenesis.

摘要

在果蝇胚胎中,sprouty基因功能的丧失会增强呼吸系统的分支。最近已克隆出三种人类sprouty同源物(h-Spry1 - 3),但其功能尚不清楚[1]。在此,我们表明一种鼠类sprouty基因(mSpry - 2),其产物与相应人类蛋白质具有97%的同源性,在胚胎期鼠肺中表达。我们采用反义寡核苷酸策略,通过竞争性逆转录聚合酶链反应测定,在培养4天的E11.5期鼠胚胎肺中,将mSpry - 2的表达降低了96%[2]。从形态学上看,mSpry - 2表达的降低导致胚胎期鼠肺分支形态发生增加了72%,同时肺上皮标记基因SP - C、SP - B和SP - A的表达也显著增加。这些结果支持果蝇和哺乳动物sprouty基因家族在负向调节呼吸器官发生方面功能的显著保守性。

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