Dysregulated PTEN‐PKB and negative receptor status in human breast cancer

Shi, Wei; Zhang, Xinghe; Pintilie, Melania; Ma, Nancy; Miller, Naomi; Banerjee, Diponkar; Tsao, Ming‐Sound; Mak, Tak W.; Fyles, Anthony; Liu, Fei‐Fei

doi:10.1002/ijc.10909

Cited by 79 publications

(71 citation statements)

References 56 publications

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“…Furthermore, ER and PR were still expressed in four of the five tumors that had lost the wild-type Pten allele (Figure 3a and b). These results suggest that loss of Pten does not prevent ER expression in mammary cancers, consistent with another study examining ER expression in mammary lesions in Pten þ /À mice that do not carry a transgene (Shi et al, 2003). Neu (HER2, ErbB2) is a member of the epidermal growth factor receptor (EGFR) family of transmembrane tyrosine kinases (Olayioye et al, 2000).…”

Section: Resultssupporting

confidence: 85%

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Estrogen receptor positivity in mammary tumors of Wnt-1 transgenic mice is influenced by collaborating oncogenic mutations

et al. 2005

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The majority (75%) of human breast cancers express estrogen receptor (ER). Although ER-positive tumors usually respond to antiestrogen therapies, 30% of them do not. It is not known what controls the ER status of breast cancers or their responsiveness to antihormone interventions. In this report, we document that transgenic (TG) expression of Wnt-1 in mice induces ER-positive tumors. Loss of Pten or gain of Ras mutations during the evolution of tumors in Wnt-1 TG mice has no effect on the expression of ER, but overexpression of Neu or loss of p53 leads to ER-negative tumors. Thus, our results provide compelling evidence that expression of ER in breast cancer may be influenced by specific genetic changes that promote cancer progression. These findings constitute a first step to explore the molecular mechanisms leading to ER-positive or ER-negative mammary tumors. In addition, we find that ER-positive tumors arising in Wnt-1 TG mice are refractory to both ovariectomy and the ER antagonist tamoxifen, but lose ER expression with tamoxifen, suggesting that antiestrogen selects for ERnegative tumor cells and that the ER-positive cell fraction is dispensable for growth of these tumors. This is a first report of a mouse model of antiestrogen-resistant ERpositive breast cancers, and could provide a powerful tool to study the molecular mechanisms that control antiestrogen resistance.

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Section: Resultssupporting

confidence: 85%

“…Loss of Pten is usually associated with ER À human breast cancers (Garcia et al, 1999;Perren et al, 1999;Shi et al, 2003). We have previously reported that inactivation of one allele of Pten accelerates mammary tumorigenesis in MMTV-Wnt-1 TG mice, and 70% of the resulting tumors have lost the wild-type allele of Pten (Li et al, 2001).…”

Section: Resultsmentioning

confidence: 99%

Estrogen receptor positivity in mammary tumors of Wnt-1 transgenic mice is influenced by collaborating oncogenic mutations

et al. 2005

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“…PTEN (phosphatase and tensin homologue deleted on chromosome 10) inhibits PKB activation by virtue of its dephosphorylating role in reverting PIP 3 to PIP 2 . We and others have documented that PTEN is underexpressed in approximately 30% of human breast cancers, 27,28 resulting in upregulation of PKB activity, which in turn is associated with reduced patient survival. 29 Hyperthermia has been demonstrated in Phase III randomized trials to benefit patients with both improved local control 1,4,5 and survival.…”

Section: Discussionmentioning

confidence: 90%

“…One possible explanation might be related to the endogenous PTEN-PKB pathway whereby we have previously documented that the more sensitive MDA-MB-468 cells lack PTEN and have increased P-PKB expression. 27 In contrast, the MCF-7 cells have preserved PTEN expression, and undetectable phospho-PKB (in the unstimulated state). Hence, potentially, the MDA-MB-468 cells may be dependent upon activated PKB for their continued proliferation and survival.…”

Section: Discussionmentioning

confidence: 99%

“…In addition, the PTEN-PKB pathway is relevant in human breast cancer in that dysregulation of this pathway, as indicated by immunohistochemistry studies of patients' surgical samples, was associated with negative ER/PR status. 27 Hence, a logical extension of our research was to evaluate the potential efficacy of combining HT with a method to neutralize the PKB survival pathway.…”

Section: Discussionmentioning

confidence: 99%

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Kinase-dead PKB gene therapy combined with hyperthermia for human breast cancer

Szmitko

Brade

et al. 2003

Cancer Gene Ther

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We have previously demonstrated that protein kinase B (PKB) is a mediator of heat-induced apoptosis for human breast cancer cells. To investigate the therapeutic potential of abrogating the function of this important survival protein, a novel replication-deficient adenovirus was constructed, wherein a mutant, kinase-inactive PKB gene (AAA) was inserted downstream of the CMV promoter. Two human breast cancer cell lines, MCF-7 and MDA-468, were treated, along with the MCF-10 serving as a ''normal'' mammary epithelial comparator. Apoptosis was increased with adv.AAA (25 PFU/cell) infection alone, but was significantly enhanced with the addition of heat exposure. Differential survival was observed with the MDA-468 cancer cells being more sensitive than the MCF-7 cells. The MCF-10 cells, in contrast, were most resistant to these treatments. Results from the clonogenic assay reflected the apoptosis data, with an apparent additive interaction between adv.AAA and hyperthermia treatments, again with greater differential sensitivity of the malignant, compared to the ''normal'' mammary epithelial cells. Heat or adv.b-gal treatments led to phosphorylation of PKB and Forkhead, but this phosphorylation was reduced with adv.AAA therapy. In parallel, the combination of adv.AAA and heat treatment reduced PKB kinase activity more so than with either heat or adv.b-gal alone. In conclusion, our results demonstrate that inhibition of the PKB-dependent survival pathway will promote apoptosis and thermosensitization in malignant breast cancer cells, with relative sparing of their normal counterpart, suggesting that a therapeutic gain could be achievable using this therapeutic strategy.

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Cranial Pair II: The Optic Nerves

Herrera

Agudo‐Barriuso²,

Murcia‐Belmonte

2018

The Anatomical Record

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The optic nerves (ONs), one of the 12 pairs of cranial nerves (Pair II), together with the olfactory and the cochlear nerves, are devoted to transmit sensory inputs. In particular, ONs convey visual information from the retina to the brain. In mammals, the ONs are bilateral structures that extend from the optic disc to the optic chiasm containing glial cells and retinal ganglion cells (RGCs) axons. RGCs are the only retinal neurons able to collect visual information and transmit it to the visual centers in the brain for its processing and integration with the rest of sensory inputs. During embryonic development, RGCs born in the retina extend their axons to exit the eye and follow a stereotypic path outlined by the transient expression of a wide set of guidance molecules. As the rest of central nervous system structures, the ONs are covered with myelin produced by oligodendrocytes and wrapped by the meninges. ON injuries or RGCs degenerative conditions may provoke partial or complete blindness because they are incapable of spontaneous regeneration. Here, we first review major advances on the current knowledge about the mechanisms underlying the formation of the ONs in mammals. Then, we discuss some of the human disorders and pathologies affecting the development and function of the ONs and finally we comment on the existing view about ON regeneration possibilities. Anat Rec, 302:428-445, 2019.

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Dysregulated PTEN‐PKB and negative receptor status in human breast cancer

Cited by 79 publications

References 56 publications

Estrogen receptor positivity in mammary tumors of Wnt-1 transgenic mice is influenced by collaborating oncogenic mutations

Estrogen receptor positivity in mammary tumors of Wnt-1 transgenic mice is influenced by collaborating oncogenic mutations

Kinase-dead PKB gene therapy combined with hyperthermia for human breast cancer

Cranial Pair II: The Optic Nerves

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