Diversity and Functional Consequences of Germline and Somatic PTPN11 Mutations in Human Disease

Tartaglia, Marco; Martinelli, Simone; Stella, Lorenzo; Bocchinfuso, Gianfranco; Flex, Elisabetta; Cordeddu, Viviana; Zampino, Giuseppe; Burgt, Ineke van der; Palleschi, Antonio; Petrucci, Tamara C.; Sorcini, Mariella; Schoch, Claudia; Foà, Robin; Emanuel, Peter D.; Gelb, Bruce D.

doi:10.1086/499925

Cited by 349 publications

(435 citation statements)

References 83 publications

(43 reference statements)

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“…In this phosphatase assay, the E76K mutant of SHP-2, the most common leukemia-specific mutant that causes complete relief of autoinhibition and full activation (Neel et al, 2003;Keilhack et al, 2005;Tartaglia et al, 2006), exhibited more than 100-fold activity of wild-type SHP-2. In contrast, the T507K mutant showed only twofold increase in phosphatase activity compared with that of wild-type SHP-2 ( Figure 2b).…”

Section: Resultsmentioning

confidence: 99%

Isolation of a distinct class of gain-of-function SHP-2 mutants with oncogenic RAS-like transforming activity from solid tumors

Miyamoto

Takahashi

et al. 2008

Oncogene

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Section: Resultsmentioning

confidence: 99%

Isolation of a distinct class of gain-of-function SHP-2 mutants with oncogenic RAS-like transforming activity from solid tumors

Miyamoto

Takahashi

et al. 2008

Oncogene

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“…55,56 Somatic mutations in PTPN11 represent the most frequent molecular lesion identified to date in JMML, with up to 35% of JMML cases demonstrating PTPN11 mutations, often mutually exclusive with RAS or NF1 mutations. [57][58][59][60][61] Mouse models of these genetic lesions have proven their causal role in myeloproliferative disease development as well as hyperactivation of the Ras pathway and GM-CSF hypersensitivity. [62][63][64][65][66][67] The interested reader can see one of several recent reviews for a more in-depth review of these biochemical and genetic aberrations.…”

Section: Jmmlfpathogenesismentioning

confidence: 99%

Juvenile myelomonocytic leukemia and chronic myelomonocytic leukemia

2008

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“…In NS, most of SHP-2 mutations described so far affect residues located in or close to the interaction surface between the N-SH2 and the PTP domains [7]. This is thought to disrupt the autoinhibited closed conformation of SHP-2, resulting in an increased basal PTP activity of most NS-associated SHP-2 mutants observed in vitro [8,9].…”

Section: Introductionmentioning

confidence: 99%

Reduced phosphatase activity of SHP‐2 in LEOPARD syndrome: Consequences for PI3K binding on Gab1

et al. 2006

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LEOPARD (LS) and Noonan (NS) are overlapping syndromes associated with distinct mutations of SHP-2. Whereas NS mutations enhance SHP-2 catalytic activity, we show that the activity of three representative LS mutants is undetectable when assayed using a standard protein tyrosine phosphatase (PTP) substrate. A different assay using a specific SHP-2 substrate confirms their decreased PTP activity, but also reveals a significant activity of the T468M mutant. In transfected cells stimulated with epidermal growth factor, the least active LS mutants promote Gab1/PI3K binding, validating our in vitro data. LS mutants thus display a reduced PTP activity both in vitro and in transfected cells.

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Diversity and Functional Consequences of Germline and Somatic PTPN11 Mutations in Human Disease

Cited by 349 publications

References 83 publications

Isolation of a distinct class of gain-of-function SHP-2 mutants with oncogenic RAS-like transforming activity from solid tumors

Isolation of a distinct class of gain-of-function SHP-2 mutants with oncogenic RAS-like transforming activity from solid tumors

Juvenile myelomonocytic leukemia and chronic myelomonocytic leukemia

Reduced phosphatase activity of SHP‐2 in LEOPARD syndrome: Consequences for PI3K binding on Gab1

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