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Bmp-2、Bmp-4、Msx-2在发育中小鼠心脏的心内膜垫及相邻组织中的重叠与差异定位以及细胞凋亡

Overlapping and differential localization of Bmp-2, Bmp-4, Msx-2 and apoptosis in the endocardial cushion and adjacent tissues of the developing mouse heart.

作者信息

Abdelwahid E, Rice D, Pelliniemi L J, Jokinen E

机构信息

Department of Pediatrics and MediCity Research Laboratory, University of Turku, Finland.

出版信息

Cell Tissue Res. 2001 Jul;305(1):67-78. doi: 10.1007/s004410100399.

DOI:10.1007/s004410100399
PMID:11512673
Abstract

The bone morphogenetic proteins BMP-2 and BMP-4 and the homeobox gene MSX-2 are required for normal development of many embryonic tissues. To elucidate their possible roles during the remodeling of the tubular heart into a fully septated four-chambered heart, we have localized the mRNA of Bmp-2, Bmp-4, Msx-2 and apoptotic cells in the developing mouse heart from embryonic day (E)11 to E17. mRNA was localized by in situ hybridization, and apoptotic cells by TUNEL (TDT-mediated dUTP-biotin nick end-labeling) as well as by transmission electron microscopy. By analyzing adjacent serial sections, we demonstrated that the expression of Msx-2 and Bmp-2 strikingly overlapped in the atrioventricular canal myocardium, in the atrioventricular junctional myocardium, and in the maturing myocardium of the atrioventricular valves. Bmp-4 was expressed in the outflow tract myocardium and in the endocardial cushion of the outflow tract ridges from E12 to E14. Msx-2 appeared in the mesenchyme of the atrioventricular endocardial cushion from E11 to E14, while Bmp-2 and Bmp-4 were detected between E11 and E14. Apoptotic cells were also detected in the mesenchyme of the endocardial cushion between E12 and E14. Our results suggest that BMP-2 and MSX-2 are tightly linked to the formation of the atrioventricular junction and valves and that BMP-4 is involved in the development of the outflow tract myocardium and of the endocardial cushion. In addition, BMP-2, BMP-4 and MSX-2 and apoptosis seem to be associated with differentiation of the endocardial cushion.

摘要

骨形态发生蛋白BMP - 2和BMP - 4以及同源框基因MSX - 2是许多胚胎组织正常发育所必需的。为了阐明它们在管状心脏重塑为完全分隔的四腔心脏过程中可能发挥的作用,我们定位了从胚胎第(E)11天到E17天发育中的小鼠心脏中Bmp - 2、Bmp - 4、Msx - 2的mRNA以及凋亡细胞。通过原位杂交定位mRNA,通过TUNEL(末端脱氧核苷酸转移酶介导的dUTP - 生物素缺口末端标记)以及透射电子显微镜定位凋亡细胞。通过分析相邻的连续切片,我们证明Msx - 2和Bmp - 2的表达在房室管心肌、房室交界心肌以及房室瓣成熟心肌中显著重叠。Bmp - 4在E12至E14期间在流出道心肌和流出道嵴的心内膜垫中表达。Msx - 2在E11至E14期间出现在房室心内膜垫的间充质中,而Bmp - 2和Bmp - 4在E11至E14期间被检测到。在E12至E14期间,在心内膜垫的间充质中也检测到了凋亡细胞。我们的结果表明,BMP - 2和MSX - 2与房室交界和瓣膜的形成紧密相关,并且BMP - 4参与流出道心肌和心内膜垫的发育。此外,BMP - 2、BMP - 4和MSX - 2以及细胞凋亡似乎与心内膜垫的分化有关。

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