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Interview with Paolo Antonelli##Mutant Materials
Year: 1996

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Article
Abnormal fear response and aggressive behavior in mutant mice deficient for alfa--calcium-calmodulin kinase II.
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Year: 1994

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Article
Behavioral phenotyping enhanced - beyond (environmental) standardization.
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Year: 2002

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Book
Human Tumor-Derived p53 Mutants: A Growing Family of Oncoproteins
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Year: 2016 Publisher: Frontiers Media SA

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TP53 gene mutations are present in more than half of all human cancers. The resulting proteins are mostly full-length with a single amino acid change and are abundantly expressed in cancer cells. Some of the mutant p53 proteins gain oncogenic functions (GOF) through which it actively contribute to the aberrant cell proliferation, increased resistance to apoptotic stimuli and ability to metastasize. Gain of function mutant p53 proteins can transcriptionally regulate the expression of a large plethora of target genes. This mainly occurs through the formation of oncogenic transcriptional competent complexes that include mutant p53 protein, known transcription factors, posttranslational modifiers and scaffold proteins. Mutant p53 protein can also transcriptionally regulate the expression of microRNAs, small non-coding RNAs that regulate gene expression at the posttranscriptional level. Each microRNA can putatively target the expression of hundred mRNAs and consequently impact on many cellular functions. Thus, gain of function mutant p53 proteins can exert their oncogenic activities through the modulation of both non-coding and coding regions of human genome. Over the past 3 decades, the regulation of p53 has been extensively studied. However, the regulation of mutant p53 remained largely unexplored. This snapshot focuses on recent discovery of mutant p53 GOF and regulation.


Book
Genetics and biotechnology of Bacilli : Proceedings of the Fourth International Conference on Bacilli held at San Diego, California, June 21-24, 1987.
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ISBN: 0122741617 0323138713 Year: 1988 Publisher: San Diego : Academic Press,

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The Scid mouse : characterization and potential uses : EMBO workshop held at the Basel Institute for Immunology, Basel, Switzerland, February 20-22, 1989
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ISBN: 3540515127 0387515127 3642749763 3642749747 9780387515120 9783540515128 Year: 1989 Volume: 152 Publisher: Berlin ; New York, NY : Springer-Verlag,

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Dissertation
Brain maps and patterns of sensory organs : a genetical and experimental analysis of the whisker-to-barrel pathway in mice (Mus musculus).
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Year: 1985 Publisher: Lausanne : Magnenat,

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Stress-induced hyperthermia and anxiety: pharmacological validation.

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Book
Human Tumor-Derived p53 Mutants: A Growing Family of Oncoproteins
Authors: ---
Year: 2016 Publisher: Frontiers Media SA

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Abstract

TP53 gene mutations are present in more than half of all human cancers. The resulting proteins are mostly full-length with a single amino acid change and are abundantly expressed in cancer cells. Some of the mutant p53 proteins gain oncogenic functions (GOF) through which it actively contribute to the aberrant cell proliferation, increased resistance to apoptotic stimuli and ability to metastasize. Gain of function mutant p53 proteins can transcriptionally regulate the expression of a large plethora of target genes. This mainly occurs through the formation of oncogenic transcriptional competent complexes that include mutant p53 protein, known transcription factors, posttranslational modifiers and scaffold proteins. Mutant p53 protein can also transcriptionally regulate the expression of microRNAs, small non-coding RNAs that regulate gene expression at the posttranscriptional level. Each microRNA can putatively target the expression of hundred mRNAs and consequently impact on many cellular functions. Thus, gain of function mutant p53 proteins can exert their oncogenic activities through the modulation of both non-coding and coding regions of human genome. Over the past 3 decades, the regulation of p53 has been extensively studied. However, the regulation of mutant p53 remained largely unexplored. This snapshot focuses on recent discovery of mutant p53 GOF and regulation.


Book
Human Tumor-Derived p53 Mutants: A Growing Family of Oncoproteins
Authors: ---
Year: 2016 Publisher: Frontiers Media SA

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Abstract

TP53 gene mutations are present in more than half of all human cancers. The resulting proteins are mostly full-length with a single amino acid change and are abundantly expressed in cancer cells. Some of the mutant p53 proteins gain oncogenic functions (GOF) through which it actively contribute to the aberrant cell proliferation, increased resistance to apoptotic stimuli and ability to metastasize. Gain of function mutant p53 proteins can transcriptionally regulate the expression of a large plethora of target genes. This mainly occurs through the formation of oncogenic transcriptional competent complexes that include mutant p53 protein, known transcription factors, posttranslational modifiers and scaffold proteins. Mutant p53 protein can also transcriptionally regulate the expression of microRNAs, small non-coding RNAs that regulate gene expression at the posttranscriptional level. Each microRNA can putatively target the expression of hundred mRNAs and consequently impact on many cellular functions. Thus, gain of function mutant p53 proteins can exert their oncogenic activities through the modulation of both non-coding and coding regions of human genome. Over the past 3 decades, the regulation of p53 has been extensively studied. However, the regulation of mutant p53 remained largely unexplored. This snapshot focuses on recent discovery of mutant p53 GOF and regulation.

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