Gain-of-function mutations of
            <i>Ptpn11</i>
            (Shp2) cause aberrant mitosis and increase susceptibility to DNA damage-induced malignancies

Liu, Xia; Zheng, Hong; Li, Xiaobo; Wang, Siying; Meyerson, Howard; Yang, Wentian; Neel, Benjamin G.; Qu, Cheng Kui

doi:10.1073/pnas.1508535113

Cited by 43 publications

(28 citation statements)

References 39 publications

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“…Subsequent analysis of E17.5 embryos confirmed that VavCre+;PTPN11 E76K embryos were dying in utero (Fig-3D). This was in contrast to recent publications that reported this model to be viable and develop MPN (Dong et al, 2016; Liu et al, 2016). This discrepancy is likely due to the use of different VavCre strains.…”

Section: Resultscontrasting

confidence: 95%

“…In contrast, non-irradiated animals expressing PTPN11 D61Y die from MPN (Chan et al, 2009a). Our findings are consistent with other studies that showed frequent T-ALL emergence in irradiated mutant PTPN11-expressing animals due to impaired DNA repair (Liu et al, 2016). As such, our results emphasize that the same mutation may give rise to divergent disease manifestations in irradiated and non-irradiated animals.…”

Section: Discussionsupporting

confidence: 93%

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Yolk sac erythromyeloid progenitors expressing gain of function PTPN11 have functional features of JMML but are not sufficient to cause disease in mice

Tarnawsky

Yoshimoto

Deng

et al. 2017

Developmental Dynamics

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Background Accumulating evidence suggests the origin of Juvenile Myelomonocytic Leukemia (JMML) is closely associated with fetal development. Nevertheless, the contribution of embryonic progenitors to JMML pathogenesis remains unexplored. We hypothesized that expression of JMML-initiating PTPN11 mutations in HSC-independent yolk sac erythromyeloid progenitors (YS EMPs) would result in a mouse model of pediatric myeloproliferative neoplasm (MPN). Results E9.5 YS EMPs from VavCre+;PTPN11D61Y embryos demonstrated growth hypersensitivity to GM-CSF and hyperactive RAS-ERK signaling. Mutant EMPs engrafted the spleens of neonatal recipients, but did not cause disease. To assess MPN development during unperturbed hematopoiesis we generated CSF1R-MCM+;PTPN11E76K;ROSAYFP mice in which oncogene expression was restricted to EMPs. YFP+ progeny of mutant EMPs persisted in tissues one year after birth and demonstrated hyperactive RAS-ERK signaling. Nevertheless, these mice had normal survival and did not demonstrate features of MPN. Conclusions YS EMPs expressing mutant PTPN11 demonstrate functional and molecular features of JMML but do not cause disease following transplantation nor following unperturbed development.

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Section: Resultscontrasting

confidence: 95%

Section: Discussionsupporting

confidence: 93%

Yolk sac erythromyeloid progenitors expressing gain of function PTPN11 have functional features of JMML but are not sufficient to cause disease in mice

Tarnawsky

Yoshimoto

Deng

et al. 2017

Developmental Dynamics

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“…Indeed, the Shp2 enhances the Tyr phosphorylation of ER by facilitating the Src kinase activity through dephosphorylation of an inhibitory Tyr in Src kinase. Whereas the Src kinase is broadly recognized as a cytoplasmic protein, recent reports also observed the nuclear function of this kinase that was activated by Shp2 through dephosphorization of the inhibitory p-Tyr site for DNA damage response (26).…”

Section: Discussionmentioning

confidence: 99%

Nuclear Shp2 directs normal embryo implantation via facilitating the ERα tyrosine phosphorylation by the Src kinase

Hao

Kong

Zhang

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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Estrogen and progesterone coupled with locally produced signaling molecules are essential for embryo implantation. However, the hierarchical landscape of the molecular pathways that governs this process remains largely unexplored. Here we show that the protein tyrosine phosphatase Shp2, a positive transducer of RTK signaling, is predominately localized in the nuclei in the periimplantation mouse uterus. Uterine-specific deletion of Shp2 exhibits reduced progesterone receptor (PR) expression and progesterone resistance, which derails normal uterine receptivity, leading to complete implantation failure in mice. Notably, the PR expression defects are attributed to the limited estrogen receptor α (ERα) activation in uterine stroma. Further analysis reveals that nuclear Shp2, rather than cytosolic Shp2, promotes the ERα transcription activity. This function is achieved by enhancing the Src kinasemediated ERα tyrosine phosphorylation, which facilitates ERα binding to Pgr promoter in an ERK-independent manner in periimplantation uteri. Besides uncovering a regulatory mechanism, this study could be clinically relevant to dysfunctional ERα-caused endometrial disorders in women.Shp2 | ERK signaling | Src kinase | estrogen receptor | uterine receptivity S uccessful implantation requires synchronization between an implantation-competent blastocyst and a receptive uterus. In humans, natural conception per cycle is poor (∼30%), and ∼75% of failed pregnancies are considered to be due to implantation failure (1). One-third of implantation failure is attributed to the embryo itself, whereas the remaining two-thirds appear to result from inadequate uterine receptivity (2). The endometrium enters into a receptive stage for blastocyst implantation only in a restricted time period termed "implantation window," which is dominated by precisely regulated proliferation and differentiation of endometrial epithelium and stroma under the influence of progesterone and estrogen (3).Estrogen and progesterone bind to the estrogen receptor (ER) and progesterone receptor (PR), respectively, coupled with specific cofactors to endure the optimal functions. The activity of these nuclear receptors is also regulated at the posttranslational level by various modifications, such as phosphorylation, which can influence the protein stability, interaction with the cofactors and DNA binding affinity. So far, a wide range of nuclear receptor cofactors have been identified to ensure the normal ER transcriptional activation, such as the well-known steroid receptor coactivator (SRC) family members, which bind with ERα in the chromatin to recruit the histone acetyltransferase p300 (P300) for transcriptional activation (4-6). It is conceivable that ordered and combinatorial recruitment of cofactors at a specific target promoter after ERα binding to DNA sequence was essential to ensure target gene transcription. Recent evidence shows that nuclear receptor coactivator 6 is essential for embryo implantation by maintaining the appropriate level and activity of uteri...

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“…PTPN11 is frequently altered in Noonan and Leopard syndromes and cancer cells (Zhang et al, 2015). Analyses of the D61G mutation, frequent in RASopathies, showed that it is gain-function-change, activating the proto-oncogene SRC tyrosine kinase, that in turn activates the serine/threonine kinases PLK1 inducing chromosomal instability and disruption of mitosis (Liu et al, 2016). Among the 20 mutation sites in melanoma, seven are shared with Noonan and Leopard syndromes (F71L, Y279C, A461T, T468M, P491L, Q506P, Q510H).…”

Section: Comparisons Of Specific Genesmentioning

confidence: 99%

RASopathy Gene Mutations in Melanoma

Halaban

Krauthammer

2016

Journal of Investigative Dermatology

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Next-Generation sequencing (NGS) of melanomas has unraveled critical “driver” genes and genomic abnormalities, mostly defined as occurring at high frequency. In addition, less abundant mutations are present that link melanoma to a set of disorders, commonly called RASopathies. These disorders which include neurofibromatosis, Noonan and Legius syndromes, harbor germline mutations in various RAS/MAPK signaling pathway genes. We highlight shared amino acid substitutions between this set of RASopathy mutations and those observed in large-scale melanoma sequencing data, uncovering a significant overlap. We review the evidence that these mutations activate the MAPK pathway in melanoma, and are involved in melanomagenesis. Furthermore, we discuss the observations that two or more RASopathy mutations often co-occur in melanoma, and may act synergistically on activating the pathway.

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Gain-of-function mutations of Ptpn11 (Shp2) cause aberrant mitosis and increase susceptibility to DNA damage-induced malignancies

Cited by 43 publications

References 39 publications

Yolk sac erythromyeloid progenitors expressing gain of function PTPN11 have functional features of JMML but are not sufficient to cause disease in mice

Yolk sac erythromyeloid progenitors expressing gain of function PTPN11 have functional features of JMML but are not sufficient to cause disease in mice

Nuclear Shp2 directs normal embryo implantation via facilitating the ERα tyrosine phosphorylation by the Src kinase

RASopathy Gene Mutations in Melanoma

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