Title of article
Binding of Ras to Phosphoinositide 3-Kinase p110α Is Required for Ras- Driven Tumorigenesis in Mice
Author/Authors
Surbhi Gupta، نويسنده , , Antoine R. Ramjaun، نويسنده , , Paula Haiko، نويسنده , , Yihua Wang، نويسنده , , Patricia H. Warne، نويسنده , , Barbara Nicke، نويسنده , , Emma Nye، نويسنده , , Gordon Stamp، نويسنده , , Kari Alitalo، نويسنده , , Julian Downward، نويسنده ,
Issue Information
هفته نامه با شماره پیاپی سال 2007
Pages
12
From page
957
To page
968
Abstract
Ras proteins signal through direct interaction with a number of effector enzymes, including type I phosphoinositide (PI) 3-kinases. Although the ability of Ras to control PI 3-kinase has been well established in manipulated cell culture models, evidence for a role of the interaction of endogenous Ras with PI 3-kinase in normal and malignant cell growth in vivo has been lacking. Here we generate mice with mutations in the Pi3kca gene encoding the catalytic p110α isoform that block its interaction with Ras. Cells from these mice show proliferative defects and selective disruption of signaling from growth factors to PI 3-kinase. The mice display defective development of the lymphatic vasculature, resulting in perinatal appearance of chylous ascites. Most importantly, they are highly resistant to endogenous Ras oncogene-induced tumorigenesis. The interaction of Ras with p110α is thus required in vivo for certain normal growth factor signaling and for Ras-driven tumor formation.
Journal title
CELL
Serial Year
2007
Journal title
CELL
Record number
1018699
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