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Biochemical and functional characterization of germ line KRAS mutations.

Biochemical and functional characterization of germ line KRAS mutations. Research Abstract Details 

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  • Biochemical and functional characterization of germ line KRAS mutations. Abstract Text:

    suzanne schubbertSuzanne Schubbert,gideon bollagGideon Bollag,natalya lyubynskaNatalya Lyubynska,hoa nguyenHoa Nguyen,christian p kratzChristian P Kratz,martin zenkerMartin Zenker,charlotte m niemeyerCharlotte M Niemeyer,anders molvenAnders Molven,kevin shannonKevin Shannon,suzanne schubbertSuzanne Schubbert,gideon bollagGideon Bollag,natalya lyubynskaNatalya Lyubynska,hoa nguyenHoa Nguyen,christian p kratzChristian P Kratz,martin zenkerMartin Zenker,charlotte m niemeyerCharlotte M Niemeyer,anders molvenAnders Molven,kevin shannonKevin Shannon,

    Germ line missense mutations in HRAS and KRAS and in genes encoding molecules that function up- or downstream of Ras in cellular signaling networks cause a group of related developmental disorders that includes Costello syndrome, Noonan syndrome, and cardiofaciocutaneous syndrome. We performed detailed biochemical and functional studies of three mutant K-Ras proteins (P34R, D153V, and F156L) found in individuals with Noonan syndrome and cardiofaciocutaneous syndrome. Mutant K-Ras proteins demonstrate a range of gain-of-function effects in different cell types, and biochemical analysis supports the idea that the intrinsic Ras guanosine nucleotide triphosphatase (GTPase) activity, the responsiveness of these proteins to GTPase-activating proteins, and guanine nucleotide dissociation all regulate developmental programs in vivo.

    Biochemical and functional characterization of germ line KRAS mutations. Publishing Authors By Initials

    s schubbertS Schubbert,g bollagG Bollag,n lyubynskaN Lyubynska,h nguyenH Nguyen,cp kratzCP Kratz,m zenkerM Zenker,cm niemeyerCM Niemeyer,a molvenA Molven,k shannonK Shannon,s schubbertS Schubbert,g bollagG Bollag,n lyubynskaN Lyubynska,h nguyenH Nguyen,cp kratzCP Kratz,m zenkerM Zenker,cm niemeyerCM Niemeyer,a molvenA Molven,k shannonK Shannon,

    For similar abstracts research abstracts see: abstracts research

    PUBMED ID PMID:

    MEDLINE DATE:

    Biochemical and functional characterization of germ line KRAS mutations. Journal Published:

    PUBLICATION TYPE: Research Support, N.I.H., Extr

    Journal: Molecular and cellular biology

    VOLUME: 27

    Page Numbers: 7765-70

    Journal Abbreviation: Mol. Cell. Biol.

    ISSN: 1098-5549

    DAY: 17

    MONTH: 09

    YEAR: 2007

    Biochemical and functional characterization of germ line KRAS mutations. Information

    Number of References:

    LANGUAGE: eng

    NlmUniqueID: 8109087

    Biochemical and functional characterization of germ line KRAS mutations. Keywords Mesh Terms:

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    Grant and Affiliation Information for Biochemical and functional characterization of germ line KRAS mutations.

    AFFILIATION: Department of Pediatrics, University of California, 513 Parnassus Avenue, HSE 302, San Francisco, California 94143, USA.

    Country: United States

    United States Research PublicationUnited States Research Publication

    AGENCY: United States NCI

    GRANT: R37 CA72614

    ACRONYM: CA

    MEDLINETA: Mol Cell Biol

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