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血管紧张素转换酶2主要存在于上皮细胞中,且在小鼠肺中受发育调控。

Angiotensin converting enzyme 2 is primarily epithelial and is developmentally regulated in the mouse lung.

作者信息

Wiener Renda Soylemez, Cao Yu Xia, Hinds Anne, Ramirez Maria I, Williams Mary C

机构信息

The Pulmonary Center, Department of Medicine, Boston University School of Medicine, Boston, Massachusetts 02118, USA.

出版信息

J Cell Biochem. 2007 Aug 1;101(5):1278-91. doi: 10.1002/jcb.21248.

Abstract

Angiotensin converting enzyme (ACE) 2 is a carboxypeptidase that shares 42% amino acid homology with ACE. Little is known about the regulation or pattern of expression of ACE2 in the mouse lung, including its definitive cellular distribution or developmental changes. Based on Northern blot and RT-PCR data, we report two distinct transcripts of ACE2 in the mouse lung and kidney and describe a 5' exon 1a previously unidentified in the mouse. Western blots show multiple isoforms of ACE2, with predominance of a 75-80 kDa protein in the mouse lung versus a 120 kDa form in the mouse kidney. Immunohistochemistry localizes ACE2 protein to Clara cells, type II cells, and endothelium and smooth muscle of small and medium vessels in the mouse lung. ACE2 mRNA levels peak at embryonic day 18.5 in the mouse lung, and immunostaining demonstrates protein primarily in the bronchiolar epithelium at that developmental time point. In murine cell lines ACE2 is strongly expressed in the Clara cell line mtCC, as opposed to the low mRNA expression detected in E10 (type I-like alveolar epithelial cell line), MLE-15 (type II alveolar epithelial cell line), MFLM-4 (fetal pulmonary vasculature cell line), and BUMPT-7 (renal proximal tubule cell line). In summary, murine pulmonary ACE2 appears to be primarily epithelial, is developmentally regulated, and has two transcripts that include a previously undescribed exon.

摘要

血管紧张素转换酶(ACE)2是一种羧肽酶,与ACE有42%的氨基酸同源性。关于小鼠肺中ACE2的调控或表达模式,包括其确切的细胞分布或发育变化,我们所知甚少。基于Northern印迹和RT-PCR数据,我们报道了小鼠肺和肾中ACE2的两种不同转录本,并描述了小鼠中先前未鉴定的5'外显子1a。蛋白质印迹显示ACE2有多种同工型,在小鼠肺中以75 - 80 kDa的蛋白质为主,而在小鼠肾中以120 kDa的形式为主。免疫组织化学将ACE2蛋白定位到小鼠肺中的克拉拉细胞、II型细胞以及中小血管的内皮和平滑肌。ACE2 mRNA水平在小鼠肺胚胎第18.5天达到峰值,免疫染色显示在该发育时间点蛋白质主要存在于细支气管上皮中。在鼠细胞系中,ACE2在克拉拉细胞系mtCC中强烈表达,而在E10(I型样肺泡上皮细胞系)、MLE - 15(II型肺泡上皮细胞系)、MFLM - 4(胎儿肺血管细胞系)和BUMPT - 7(肾近端小管细胞系)中检测到的mRNA表达较低。总之,小鼠肺中的ACE2似乎主要是上皮性的,受发育调控,并且有两种转录本,其中包括一个先前未描述的外显子。

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