abnormal notochord branching is associated with foregut malformations in the adriamycin treated mouse model脊索异常分支与前肠畸形的阿霉素治疗小鼠模型.pdfVIP
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abnormal notochord branching is associated with foregut malformations in the adriamycin treated mouse model脊索异常分支与前肠畸形的阿霉素治疗小鼠模型
Abnormal Notochord Branching Is Associated with
Foregut Malformations in the Adriamycin Treated Mouse
Model
1,2 1,2 2 1
Piotr Hajduk , Hideaki Sato , Prem Puri , Paula Murphy *
1 Zoology Department, School of Natural Sciences, University of Dublin, Trinity College, Dublin, Ireland, 2 National Children’s Research Centre, Our Lady’s Children’s
Hospital, Crumlin, Dublin, Ireland
Abstract
Oesophageal atresia (OA) and tracheooesophageal fistula (TOF) are relatively common human congenital malformations of
the foregut where the oesophagus does not connect with the stomach and there is an abnormal connection between the
stomach and the respiratory tract. They require immediate corrective surgery and have an impact on the future health of
the individual. These abnormalities are mimicked by exposure of rat and mouse embryos in utero to the drug adriamycin.
The causes of OA/TOF during human development are not known, however a number of mouse mutants where different
signalling pathways are directly affected, show similar abnormalities, implicating multiple and complex signalling
mechanisms. The similarities in developmental outcome seen in human infants and in the adriamycin treated mouse model
underline the potential of this model to unravel the early embryological events and further our understanding of the
processes disturbed, leading to such abnormalities. Here we report a systematic study of the foregut and adjacent tissues in
embryos treated with adriamycin at E7 and E8 and analysed between E9 and E12, comparing morphology in 3D in 149
specimens. We describe a spectrum of 8 defects, the most common of which is ventral displacement and branching of the
notochord (in 94% of embryos at E10) and a close spatial correspo
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