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Query: UNIPROT:P04637 (
p53
)
77,613
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Neurofibromatosis type 1
(
NF1
), a common autosomal dominant neurogenetic disorder affecting 1 in 4000 individuals worldwide, results from functional inactivation of the 17q11.2-located
NF1
gene. Plexiform neurofibroma (PNF) is a congenital benign tumour present in 30-50% of
NF1
patients, which in about 10-15% of cases, can develop into a malignant peripheral nerve sheath tumour (MPNST). This study aimed to characterise the
NF1
germline and somatic mutations associated with such tumours by DNA analysis in 51 PNFs resected from 44 unrelated
NF1
patients. Germline mutations were identified in 35 patients, of which 21 were novel. Somatic
NF1
mutations were found in 29 PNF DNAs, which included 9 point mutations, 5 being novel, and 20 tumour DNA samples exhibiting, either loss of heterozygosity (LOH) of the
NF1
gene region (16 tumours), or complete or partial
NF1
gene deletions analyzed by multiplex ligation-dependent probe amplification (MPLA) analysis. The type of
NF1
germline mutations detected in patients with PNF were similar to those detected in most
NF1
patients. LOH of the
NF1
gene region, as identified by marker analysis and/or MLPA, was detected in only 20/29 (69%) PNFs, compared to the >90% LOH previously found in MPNST. This systematic analysis of the
NF1
germline and somatic mutations associated with PNF development suggest that in most such tumours neither the
NF1
somatic mutation type, nor its gene location, is influenced by the underlying
NF1
germline mutation. Evidence for LOH involving the
TP53
gene identified in the PNFs is also reported for the first time.
...
PMID:Germline and somatic NF1 gene mutations in plexiform neurofibromas. 1848 66
Malignant peripheral nerve sheath tumours (MPNSTs) are highly malignant and resistant. Transformation might implicate up regulation of epidermal growth factor receptor (EGFR). Fifty-two MPNST samples were studied for EGFR, Ki-67,
p53
, and survivin expression by immunohistochemistry and for EGFR amplification by in situ hybridization. Results were correlated with clinical data. EGFR RNA was also quantified by RT-PCR in 20 other MPNSTs and 14 dermal neurofibromas. Half of the patients had a
neurofibromatosis type 1 (NF1)
. EGFR expression, detected in 86% of MPNSTs, was more frequent in
NF1
specimens and closely associated with high-grade and
p53
-positive areas. MPNSTs expressed more EGFR transcripts than neurofibromas. No amplification of EGFR locus was observed.
NF1
status was the only prognostic factor in multivariate analysis, with median survivals of 18 and 43 months for patients with or without
NF1
. Finally, EGFR might become a new target for MPNSTs treatment, especially in
NF1
-associated MPNSTs.
...
PMID:Frequent EGFR Positivity and Overexpression in High-Grade Areas of Human MPNSTs. 1876 52
Neurofibromas are benign tumors of peripheral nerve that occur sporadically or in patients with the autosomal dominant tumor predisposition syndrome
neurofibromatosis type 1 (NF1)
. Multiple neurofibroma subtypes exist which differ in their site of occurrence, their association with
NF1
, and their tendency to undergo transformation to become malignant peripheral nerve sheath tumors (MPNSTs), the most common malignancy associated with
NF1
. Most
NF1
patients carry a constitutional mutation of the
NF1
tumor suppressor gene. Neurofibromas develop in these patients when an unknown cell type in the Schwann cell lineage loses its remaining functional
NF1
gene and initiates a complex series of interactions with other cell types; these interactions may be influenced by aberrant expression of growth factors and growth factor receptors and the action of modifier genes. Cells within certain neurofibroma subtypes subsequently accumulate additional mutations affecting the p19(ARF)-MDM2-
TP53
and p16INK4A-Rb signaling cascades, mutations of other as yet unidentified genes, and amplification of growth factor receptor genes, resulting in their transformation into MPNSTs. These observations have been validated using a variety of transgenic and knockout mouse models that recapitulate neurofibroma and MPNST pathogenesis. A new generation of mouse models is also providing important new insights into the identity of the cell type in the Schwann cell lineage that gives rise to neurofibromas. Our improving understanding of the mechanisms underlying the pathogenesis of neurofibromas and MPNSTs raises intriguing new questions about the origin and pathogenesis of these neoplasms and establishes models for the development of new therapies targeting these neoplasms.
...
PMID:How does the Schwann cell lineage form tumors in NF1? 1880 26
Malignant peripheral nerve sheath tumors (MPNSTs) arising from cranial nerves or their branches are very uncommon. The literature consists mainly of isolated case reports and small series. We identified 17 such cases in 14 males and 3 females. With one exception, the tumors affected adults (age range 5 to 69 y, mean 39, median 32). Sites of involvement included vestibular nerves (n=6), vagal nerves (n=4), facial nerves (n=3) (1 centered in the geniculate ganglion), and 2 unspecified cranial nerves in the posterior fossa. In addition, 1 tumor involved the optic chiasm (n=1). Only 1 tumor arose in brain parenchyma of (frontal lobe). All but 3 lesions were intracranial. Five tumors arose in patients who satisfied clinical criteria for
neurofibromatosis type 1 (NF1)
. One patient with a vestibular tumor and presumed NF2 had previously undergone resection of a contralateral vestibular cellular schwannoma. One posterior fossa tumor was a malignant melanotic schwannoma. Four patients had postirradiation malignant peripheral nerve sheath tumors, 2 having been treated for optic chiasm glioma, both being
NF1
affected. One patient was irradiated for hypothalamic pilocytic astrocytoma and another for cervical Hodgkin disease. Identifiable precursor lesions included schwannoma (n=4), plexiform neurofibroma (n=2), and solitary intraneural neurofibroma (n=2). All tumors were histologically high grade (6 grade III and 10 grade IV). Three tumors showed heterologous elements, 2 osseous, and 1 rhabdomyoblastic. More often scattered than diffuse, S-100 protein staining was noted in 11 of 16 tumors and variable collagen IV staining in 10 of the 16. Immunoreactivity for
p53 protein
was diffuse and strong in 7 of 11 tumors. Twelve patients died within 17 months to 3 years of diagnosis, 1 was lost to follow-up, 2 are very recent cases, and 2 patients are currently alive, 1 after 2 recurrences, and another with spinal leptomeningeal metastases. Malignant cranial nerve sheath tumors are rare and are associated with the same poor prognosis as those of spinal nerves at other sites.
...
PMID:Malignant peripheral nerve sheath tumors of cranial nerves and intracranial contents: a clinicopathologic study of 17 cases. 1906 5
The purpose of this study was to identify new prognostic biomarkers with clinical impact in malignant peripheral nerve sheath tumor (MPNST), a highly aggressive malignancy for which no consensus therapy exists besides surgery. We have used tissue microarrays (TMAs) to assess in situ expression of 14 cell-cycle-regulating proteins in 64 well-characterized MPNST patients: 36 sporadic and 28 with
neurofibromatosis type 1 (NF1)
. We developed a new software application for evaluation and logistics of the TMA images and performed a literature survey of cell cycle proteins in MPNST. For
NF1
-associated patients, there was a clear association between nuclear expression of
p53
and poor survival (p = 0.004). Among the other proteins analyzed, we also found significant associations between survival and clinical variables, but none were as strong as that for
p53
. For the total series of MPNSTs,
p53
was shown to be an independent predictor of survival, and patients without remission, with tumor size larger than 8 cm, and with positive
p53
expression had a 60 times greater risk of dying within the first 5 years compared with the remaining patients (p = 0.000002). This is the most comprehensive study of in situ protein expression in MPNST so far, and expressed
p53
was found to be a strong surrogate marker for outcome. Patients in complete remission with a primary
p53
-positive MPNST diagnosis may be considered in a high-risk subgroup and candidates for adjuvant treatment.
...
PMID:Identification of p53 as a strong predictor of survival for patients with malignant peripheral nerve sheath tumors. 1918 48
Neurofibromatosis type 1
(
NF1
) is a common inherited complex multi-system disorder associated with the growth of various benign and malignant tumors. About 40% of
NF1
patients develop spinal tumors, of whom some have familial spinal neurofibromatosis (FSNF), a variant form of
NF1
in which patients present with multiple bilateral spinal tumors but have few other clinical features of the disease. We have studied 22 spinal neurofibromas derived from 14 unrelated
NF1
patients. Seven of these patients satisfied the diagnostic criteria of
NF1
while the remaining seven had only few features of
NF1
. The latter group defined as FSNF harbored significantly higher number of missense or missense and splice-site germline mutations compared to the group with classical
NF1
. This is the first study to describe
NF1
somatic mutations in spinal neurofibromas. Loss-of-heterozygosity (LOH) was identified in 8/22 of the spinal tumors, 75% of LOH observed was found to result from mitotic recombination, suggesting that this may represent a frequent mutational mechanisms in these benign tumors. No evidence for LOH of the
TP53
gene was found in these tumors.
...
PMID:The spectrum of somatic and germline NF1 mutations in NF1 patients with spinal neurofibromas. 1922 14
We analyzed two unrelated male patients in whom
neurofibromatosis type 1 (NF1)
was not suspected until they presented with malignant peripheral nerve sheath tumours (MPNSTs) in their thirties and forties, respectively. Patient A presented with progressive peroneus paresis due to a rapidly growing MPNST in the thigh. MRI examination revealed multiple symmetrical spinal neurofibromas in this patient as well as in patient B who presented at the age of 42 with paraparesis and an MPNST at spinal level L4. Dermal features in both patients were strikingly mild, therefore both patients were considered belonging to the
NF1
-subform of spinal neurofibromatosis (SNF). The novel
NF1
mutations identified, i.e. splice mutation, c.7675+1G > A, in patient A and two alterations, p.Cys1016Arg and p.2711delVal, located in trans in patient B support the notion that the phenotype of SNF may be related to mutations with possible residual functionality. The MPNSTs of both patients showed LOH affecting chromosome 17 including the
NF1
locus. Furthermore, a truncating
TP53
mutation was identified in the tumour of patient A. Both alterations are frequent findings in
NF1
-associated MPNSTs. To our knowledge these are the first MPNST patients with the clinical phenotype of SNF. The clinical course observed in these two patients suggests that nodular plexiform neurofibromas and spinal-nerve-root neurofibromas which may be asymptomatic for a long time and, hence, unrecognized in SNF patients bear the risk for malignant transformation.
...
PMID:Two sporadic spinal neurofibromatosis patients with malignant peripheral nerve sheath tumour. 1966 63
Malignant peripheral nerve sheath tumours (MPNSTs) are aggressive soft tissue tumours that occur either sporadically or in patients with
neurofibromatosis type 1
. The malignant transformation of the benign neurofibroma to MPNST is incompletely understood at the molecular level. We have determined the gene expression signature for benign and malignant PNSTs and found that the major trend in malignant transformation from neurofibroma to MPNST consists of the loss of expression of a large number of genes, rather than widespread increase in gene expression. Relatively few genes are expressed at higher levels in MPNSTs and these include genes involved in cell proliferation and genes implicated in tumour metastasis. In addition, a gene expression signature indicating
p53
inactivation is seen in the majority of MPNSTs. Subsequent microRNA profiling of benign and malignant PNSTs indicated a relative down-regulation of miR-34a in most MPNSTs compared to neurofibromas. In vitro studies using the cell lines MPNST-14 (NF1 mutant) and MPNST-724 (from a non-NF1 individual) show that exogenous expression of
p53
or miR-34a promotes apoptotic cell death. In addition, exogenous expression of
p53
in MPNST cells induces miR-34a and other miRNAs. Our data show that
p53
inactivation and subsequent loss of expression of miR-34a may significantly contribute to the MPNST development. Collectively, our findings suggest that deregulation of miRNAs has a potential role in the malignant transformation process in peripheral nerve sheath tumours.
...
PMID:Genome-wide transcriptome analyses reveal p53 inactivation mediated loss of miR-34a expression in malignant peripheral nerve sheath tumours. 1989 Aug 83
Mutations in
TP53
underlie the development of malignant peripheral nerve sheath tumors (MPNSTs) in animal models, but there is controversy regarding the extent of
TP53
mutations in human MPNSTs. We assessed the
TP53
mutation frequency in 145 consecutive cases from our department over 36 years; 88 cases were histologically confirmed as MPNSTs, and corresponding clinical data were reviewed. Mutation analysis of
TP53
Exons 4 to 9 on DNA from formalin-fixed, paraffin-embedded specimens was performed by bidirectional DNA sequencing. Tumors were localized in the extremities (n = 34), trunk (n = 34), or head and neck (n = 20). A minority of patients (n = 26, 30%) had
neurofibromatosis type 1 (NF1)
; in these patients, the diagnosis of MPNST was made at younger ages (33 [SD, 3.6] years vs 49 [SD, 2.9] years in
NF1
vs non-
NF1
; p = 0.003). High
p53 protein
expression was detected in 18 (21%) of 86 cases by immunohistochemistry.
TP53
mutations were detected in 17 (24%) of 72 evaluable tumors, of which 36% were from
NF1
patients.
TP53
mutation and strong
p53
immunostaining were positively correlated (p = 0.002); high proliferation indices correlated with cellular epithelioid and storiform growth patterns. These results indicate that
TP53
mutations are relatively rare in human MPNST and that they are not positively correlated with the presence of
NF1
.
...
PMID:TP53 mutation analysis of malignant peripheral nerve sheath tumors. 2001 Mar 6
Neurofibromatosis Type 1
(
NF1
) is a common autosomal dominant disease characterized by complex and multicellular neurofibroma tumors, and less frequently by malignant peripheral nerve sheath tumors (MPNSTs) and optic nerve gliomas. Significant advances have been made in elucidating the cellular, genetic, and molecular biology involved in tumor formation in
NF1
.
Neurofibromatosis Type 1
is caused by germline mutations of the
NF1
tumor suppressor gene, which generally result in decreased intracellular neurofibromin protein levels, leading to increased cascade Ras signaling to its downstream effectors. Multiple key pathways are involved with the development of tumors in
NF1
, including Ras/mitogen-activated protein kinase (MAPK) and Akt/mammalian target of rapamycin (mTOR). Interestingly, recent studies demonstrate that multiple other developmental syndromes (in addition to
NF1
) share phenotypic features resulting from germline mutations in genes responsible for components of the Ras/MAPK pathway. In general, a somatic loss of the second
NF1
allele, also referred to as loss of heterozygosity, in the progenitor cell, either the Schwann cell or its precursor, combined with haploinsufficiency in multiple supporting cells is required for tumor formation. Importantly, a complex series of interactions with these other cell types in neurofibroma tumorigenesis is mediated by abnormal expression of growth factors and their receptors and modification of gene expression, a key example of which is the process of recruitment and involvement of the
NF1
(+/-) heterozygous mast cell. In general, for malignant transformation to occur, there must be accumulation of additional mutations of multiple genes including INK4A/ARF and
P53
, with resulting abnormalities of their respective signal cascades. Further, abnormalities of the
NF1
gene and molecular cascade described above have been implicated in the tumorigenesis of
NF1
and some sporadically occurring gliomas, and thus, these treatment options may have wider applicability. Finally, increased knowledge of molecular and cellular mechanisms involved with
NF1
tumorigenesis has led to multiple preclinical and clinical studies of targeted therapy, including the mTOR inhibitor rapamycin, which is demonstrating promising preclinical results for treatment of MPNSTs and gliomas.
...
PMID:Neurofibromatosis Type 1 and tumorigenesis: molecular mechanisms and therapeutic implications. 2004 23
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