Suppressor screen in
 Mpl
 -/-
 mice:
 c-Myb
 mutation causes supraphysiological production of platelets in the absence of thrombopoietin signaling

Carpinelli, Marina R.; Hilton, Douglas J.; Metcalf, Donald; Antonchuk, Jennifer; Hyland, Craig D.; Mifsud, Sandra; Rago, Ladina Di; Hilton, Adrienne; Willson, Tracy A.; Roberts, Andrew W.; Ramsay, Robert G.; Nicola, Nicos A.; Alexander, Warren S.

doi:10.1073/pnas.0401496101

Cited by 168 publications

(168 citation statements)

References 31 publications

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“…6A). The c-Myb 3M, PLT3, and PLT4 mutants possessed comparable activities with that of the WT in contrast to lower activity from the PLT4 mutant reported by Carpinelli et al (4). Surprisingly, the double-domain mutants (3M.CT3 and 3M.L3,4P) exhibited minimal transactivation ability, which was substantially less than that of the WT and CT3 Myb forms.…”

Section: Tad Mutants and Nrd/dbd Double Mutants Lose Transactivation contrasting

confidence: 40%

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Mutations in Multiple Domains of c-Myb Disrupt Interaction with CBP/p300 and Abrogate Myeloid Transforming Ability

Pattabiraman

Sun

Dowhan

et al. 2009

Molecular Cancer Research

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The c-myb proto-oncogene is a key regulator of hematopoietic cell proliferation and differentiation. MYB mRNA is expressed at high levels in, and is required for the proliferation of, most human myeloid and acute lymphoid leukemias. Recently, chromosomal translocation and genomic duplications of c-MYB have been identified in human T-cell acute leukemia. The present work focuses on the effects of mutations in different domains of the murine c-Myb protein on its transforming ability as defined by suppression of myelomonocytic differentiation and continued proliferation. Using both a novel myeloid cell line-based assay and a primary hematopoietic cell assay, we have shown that mutation of single residues in the transactivation domain important for CBP/p300 binding leads to complete loss of transforming ability. We also simultaneously mutated residues in the DNA-binding domain and the negative regulatory domain of the protein. These double mutants, but not the corresponding single mutants, show a complete loss of transforming activity. Surprisingly, these double mutants show severely impaired transactivation and are also defective for CBP/ p300 binding. Our results imply that multiple Myb domains influence its interaction with CBP/p300, highlight the importance of this interaction for myeloid transformation, and suggest an approach for molecular targeting

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Section: Tad Mutants and Nrd/dbd Double Mutants Lose Transactivation contrasting

confidence: 40%

“…c-myb-null mice display abnormal fetal liver hematopoiesis and die by day 15 of gestation due to severe anemia (3). Moreover, ENU mutagenesis studies in mice revealed point mutations in myb that resulted in hypomorphic alleles and consequent hematopoietic irregularities (4,5).…”

Section: Introductionmentioning

confidence: 99%

Mutations in Multiple Domains of c-Myb Disrupt Interaction with CBP/p300 and Abrogate Myeloid Transforming Ability

Pattabiraman

Sun

Dowhan

et al. 2009

Molecular Cancer Research

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“…Similarly, Ski deficiency resulted in a high penetrance (83%) of exencephaly in a 129p2 background but a low penetrance (5-6%) in the C57BL6 strain (Colmenares et al, 2002). Genetic variation of NTDs in mouse likely reflects the additive effects of several mutant genes, and additional mutagenesis may be required to define factors that affect the penetrance of NTDs in the presence of defective alleles of Gcn5 (for example, see Carpinelli et al, 2004). Genetic variations also likely underlie different susceptibilities to NTDs in humans (Zohn et al, 2005).…”

Section: Discussionmentioning

confidence: 99%

Proper expression of the Gcn5 histone acetyltransferase is required for neural tube closure in mouse embryos

Lin

Zhang

Srajer

et al. 2008

Developmental Dynamics

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Histone acetyltransferases (HATs) are important to gene activation, altering chromatin structures to facilitate association of transcription proteins with gene promoters. The functions of individual HATs in mammalian developmental are not well defined. Our previous studies demonstrated that Gcn5, a prototypical HAT, is required for mesodermal maintenance in early embryos. Homozygous Gcn5 null embryos die soon after gastrulation, preventing determination of Gcn5 functions later during development. We report here the creation of a Gcn5 flox(neo) allele, which is only partially functional and gives rise to a hypomorphic phenotype. Mice homozygous for this allele had an increased risk of cranial neural tube closure defects (NTDs) and exencephaly. These defects were found at an even greater penetrance in

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“…Modifier screens have proven extremely powerful in yeast, worms, and flies to dissect complex biological questions. A dominant modifier screen in the mouse found two alleles that suppressed the lack of platelets found in Mpl homozygous deletion mice (Carpinelli et al, 2004). Modifier screens take time and careful planning, as mouse production must be ramped up so that there are enough animals available for the screening crosses.…”

Section: Perspectivementioning

confidence: 99%

Uncovering the uncharacterized and unexpected: Unbiased phenotype‐driven screens in the mouse

Caspary

Anderson

2006

Developmental Dynamics

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Phenotype-based chemical mutagenesis screens for mouse mutations have undergone a transformation in the past five years from a potential approach to a practical tool. This change has been driven by the relative ease of identifying causative mutations now that the complete genome sequence is available. These unbiased screens make it possible to identify genes, gene functions and processes that are uniquely important to mammals. In addition, because chemical mutagenesis generally induces point mutations, these alleles often uncover previously unappreciated functions of known proteins. Here we provide examples of the success stories from forward genetic screens, emphasizing the examples that illustrate the discovery of mammalian-specific processes that could not be discovered in other model organisms. As the efficiency of sequencing and mutation detection continues to improve, it is likely that forward genetic screens will provide an even more important part of the repertoire of mouse genetics in the future. Developmental Dynamics 235:2412-2423, 2006.

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Suppressor screen in Mpl ^-/- mice: c-Myb mutation causes supraphysiological production of platelets in the absence of thrombopoietin signaling

Cited by 168 publications

References 31 publications

Mutations in Multiple Domains of c-Myb Disrupt Interaction with CBP/p300 and Abrogate Myeloid Transforming Ability

Mutations in Multiple Domains of c-Myb Disrupt Interaction with CBP/p300 and Abrogate Myeloid Transforming Ability

Proper expression of the Gcn5 histone acetyltransferase is required for neural tube closure in mouse embryos

Uncovering the uncharacterized and unexpected: Unbiased phenotype‐driven screens in the mouse

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Suppressor screen in Mpl -/- mice: c-Myb mutation causes supraphysiological production of platelets in the absence of thrombopoietin signaling

Cited by 168 publications

References 31 publications

Mutations in Multiple Domains of c-Myb Disrupt Interaction with CBP/p300 and Abrogate Myeloid Transforming Ability

Mutations in Multiple Domains of c-Myb Disrupt Interaction with CBP/p300 and Abrogate Myeloid Transforming Ability

Proper expression of the Gcn5 histone acetyltransferase is required for neural tube closure in mouse embryos

Uncovering the uncharacterized and unexpected: Unbiased phenotype‐driven screens in the mouse

Contact Info

Product

Resources

About

Suppressor screen in Mpl ^-/- mice: c-Myb mutation causes supraphysiological production of platelets in the absence of thrombopoietin signaling