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HippoTAZ信号通路对细生长调控的研究
复旦大学博士毕业论文Abstract
复旦大学博士毕业论文
Abstract
The Hippo Pathway was first identified as a novel organ size control apparatus during Drosophila development by coordination cell proliferation and apoptosis.The core components function as a kinase cascade.phosphorylates Yorkie.down-regulates its transcription activation,and then denne cell number and organ size.Dysfunction of Hippo pathway leads to organ hypertrophy and tissue cancerous growth.In mammalian cells,the components of Hippo pathway are highly conserved;most of them have been characterized as tumor suppressor genes which often found silencing or loss of function in human cancer tissue. TAZ is a transcription CO.activator,one of Yorkie orthologs in mammalian cell. Our study has demonstrated that TAZ functions as the downstream factor of
Hippo pathway.Wb found four conserved HⅪ阳ⅨS motif in TAZ;Lats2,a
kinase homolog of Wts in Drosophila,phosphorylates the serine residue of the
motif and creates a 14.3-3 binding sites.which results in TAZ cytoplasmic retention.Disruption the phosphorylation leads to constitutive activation of TAZ including nuclear import and transcription activation,consequently stimulates cell proliferation.induces EMT(F:,_pithelial-Mesenchymai Transition)and
promotes cell migration.Wb also defined TEAD.a family of transcription factor, mediates TAZ function in promoting cell proliferation and inducing EMT.We found the key residue for TAZ.TEAD binding,$51A mutation or TEAD silencing
leads to the block of TAz tumorigenetic function in stimulating celI proliferation, inducing EMT and promoting cell migration.Our work established the connection between TAZ and Hippo pathway.It is very meaningful to fully unde体tand the physiological function of the pathway,and the role of TA Z厂I’EAD playing in tumorigenesis and human cancer development.
Keywords
Hippo pathway,TAZ,TEAD,Phosphorylation,l们一3,Cell Proliferation,EMT,Migration
复旦大学博士毕业论文第一章引言
复旦大学博士毕业论文
第一章引言
一、研究背景
Hippo Pathway是近年来在模式生物果蝇(Fruit Fly,Dros
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