Mice Expressing a Mammary Gland–Specific R270H Mutation in the <i>p53</i> Tumor Suppressor Gene Mimic Human Breast Cancer Development

Wijnhoven, Susan; Zwart, Edwin; Speksnijder, Ewoud N.; Beems, Rudolf B.; Olive, Kenneth P.; Tuveson, David A.; Jonkers, Jos; Schaap, Mirjam M.; Berg, Jolanda van den; Jacks, Tyler; Steeg, Harry van; Vries, Annemieke de

doi:10.1158/0008-5472.can-05-1650

Cited by 62 publications

(73 citation statements)

References 35 publications

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“…It is possible that disruption of p53 protein expression might not be an early step in tumor initiation in this model, although some sort of interference with p53 function may be a necessary step for eventual tumor promotion (as this is a commonly observed event in tumorigenesis; refs. 21,41). Expression of p53 protein in all tissues is typically low, with an increase observed in response to cellular stress or damage (41).…”

Section: Discussionmentioning

confidence: 99%

“…At the developmental stages of puberty [postnatal day (PND) 30] and young adulthood (PND 60), mammary glands from mice reared in each of these environmental conditions were examined for mRNA and protein levels of both estrogen receptor α (ERα) and tumor-suppressor p53. These factors were chosen as they are considered to play important roles in normal and malignant mammary gland growth (16,21,22). Changes in the molecular profiles of mammary epithelial cells may influence the morphology of the mammary gland, which can also be used to infer cancer risk.…”

Section: Introductionmentioning

confidence: 99%

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Neonatal Experiences Differentially Influence Mammary Gland Morphology, Estrogen Receptor α Protein Levels, and Carcinogenesis in BALB/c Mice

Boyd

Salleh

Humber

et al. 2010

Cancer Prevention Research

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Prevention of breast cancer can be achieved with a better understanding of the factors contributing to normal breast development. Because the breast develops postnatally, alterations in the development and lifetime activity of the neuroendocrine system may set up an environment that increases cancer risk. The present study examined how two neonatal experiences over the first 3 weeks of life influence normal and malignant mammary gland development in female BALB/c mice. Following puberty, both brief (15 minutes) and prolonged (4 hours) daily maternal separations of newborn mice accelerated mammary gland development relative to nonseparated mice. Despite similar mammary gland morphologies between mice exposed to these two neonatal separation experiences, only mice exposed to prolonged maternal separation bouts showed a higher incidence and faster onset of mammary tumorigenesis following adulthood carcinogen [7,12-dimethylbenz(a)anthracene] administration. Molecular analysis of estrogen receptor α (ERα) and p53, two proteins that have been implicated in breast cancer, revealed that for mice exposed to prolonged neonatal maternal separation bouts, mammary gland ERα protein levels were upregulated in a transcription-independent manner. On the other hand, p53 expression in mammary glands of adult mice was not differentially influenced by neonatal experiences. Our findings show that chronic, moderate psychosocial stress during the neonatal period increases the expression of ERα protein and promotes mammary tumorigenesis in adulthood. Cancer Prev Res; 3(11); 1398-408. ©2010 AACR.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Neonatal Experiences Differentially Influence Mammary Gland Morphology, Estrogen Receptor α Protein Levels, and Carcinogenesis in BALB/c Mice

Boyd

Salleh

Humber

et al. 2010

Cancer Prevention Research

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“…There is also difficulty in controlling the level of oncogene overexpression, which is often activated constitutively throughout development, not likely representing the physiologic situation in human breast cancer. The third, and most recent, generation of mouse breast cancer models involves mammary gland-specific gene deletion and activation by use of technology such as the Cre-lox system and tetracycline-responsive transactivation to induce tissue-specific gene mutations in adult somatic tissue and, as such, provides the opportunity to more authentically model human cancer (Furth, 1997;Liu et al, 2007;Moody et al, 2002;Wijnhoven et al, 2005).…”

Section: Introductionmentioning

confidence: 99%

Chapter 4 A Mouse Mammary Epithelial Cell Model to Identify Molecular Mechanisms Regulating Breast Cancer Progression

Karantza‐Wadsworth

White

2008

Methods in Enzymology

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Breast cancer, like any other human cancer, results from the accumulation of mutations that deregulate critical cellular processes, such as cell proliferation and death. Activation of oncogenes and inactivation of tumor suppressor genes are common events during cancer initiation and progression and often determine treatment responsiveness. Thus, recapitulating these events in mouse cancer models is critical for unraveling the molecular mechanisms involved in tumorigenesis and for interrogating their possible impact on response to anticancer drugs. We have developed a novel mouse mammary epithelial cell model, which replicates the steps of epithelial tumor progression and takes advantage of the power of mouse genetics and the ability to assess three-dimensional morphogenesis in the presence of extracellular matrix to model human breast cancer.

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“…The targeting vectors (Figure 3 and Supplementary Figure 1) were constructed by cloning the mutated fragment into flanking genomic p53 fragments comprising intron 4-3 0 end of the gene (Wijnhoven et al, 2005) together with the transcriptional stop cassette described by Olive et al (2004). This stop cassette contains a puromycin selection marker flanked by LoxP sites.…”

Section: Methodsmentioning

confidence: 99%

“…Several isoforms of p53 have been identified (Courtois et al, 2002;Candeias et al, 2006;Grover et al, 2009;Marcel and Hainaut, 2009), and point mutations influencing the functionality of p53 were elucidated and mimicked in vivo (de Vries et al, 2002;Wijnhoven et al, 2005;Hoogervorst et al, 2005a;Iwakuma and Lozano, 2007;Heinlein et al, 2008). The p53 gene is the most frequently mutated gene in cancer and analysis of many different human tumor types have shown a high prevalence of missense mutations located primarily in the central DNA-binding domain (Levine, 1997).…”

Section: Introductionmentioning

confidence: 99%

Genotoxic exposure: novel cause of selection for a functional ΔN-p53 isoform

Melis¹,

Hoogervorst²,

Oostrom³

et al. 2010

Oncogene

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The p53 gene is frequently mutated in cancers and it is vital for cell cycle control, homeostasis and carcinogenesis. We describe a novel p53 mutational spectrum, different to those generally observed in human and murine tumors. Our study shows a high prevalence of nonsense mutations in the p53 N terminus of 2-acetylaminofluorene (2-AAF)-induced urinary bladder tumors. These nonsense mutations forced downstream translation initiation at codon 41 of Trp53, resulting in the aberrant expression of the p53 isoform DN-p53 (or p44). We propose a novel mechanism for the origination and the selection for this isoform. We show that chemical exposure can act as a novel cause of selection for this truncated protein. In addition, our data suggest that the occurrence of DN-p53 accounts, at least in mice, for a cancer phenotype. We also show that gene expression profiles of embryonic stem (ES) cells carrying the DN-p53 isoform in a p53-null background are divergent from p53 knockout ES cells, and therefore postulate that DN-p53 itself has functional transcriptional properties.

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Mice Expressing a Mammary Gland–Specific R270H Mutation in the p53 Tumor Suppressor Gene Mimic Human Breast Cancer Development

Cited by 62 publications

References 35 publications

Neonatal Experiences Differentially Influence Mammary Gland Morphology, Estrogen Receptor α Protein Levels, and Carcinogenesis in BALB/c Mice

Neonatal Experiences Differentially Influence Mammary Gland Morphology, Estrogen Receptor α Protein Levels, and Carcinogenesis in BALB/c Mice

Chapter 4 A Mouse Mammary Epithelial Cell Model to Identify Molecular Mechanisms Regulating Breast Cancer Progression

Genotoxic exposure: novel cause of selection for a functional ΔN-p53 isoform

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