PTEN activation contributes to tumor inhibition by trastuzumab, and loss of PTEN predicts trastuzumab resistance in patients

Nagata, Yoichi; Lan, Keng Hsueh; Zhou, Xiaoyan; Tan, Ming; Esteva, Francisco J.; Şahin, Ayşegül; Klos, Kristine S.; Li, Ping; Monia, Brett P.; Nguyen, Nina; Hortobágyi, Gabriel N.; Hung, Mien‐Chie; Yu, Dihua

doi:10.1016/j.ccr.2004.06.022

Cited by 1,609 publications

(1,399 citation statements)

References 51 publications

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“…It is not clear whether or not targeting single PI3K isoforms will be successful in cancer therapy, and whether PI3K inhibitors will be effective as single agents. Collective data indicate that they will be of value in combination therapy: PI3K inhibitors have been shown to reverse resistance to trastuzumab (herceptin, a monoclonal antibody directed against ERBB2), which was caused by the loss of PTEN 123 .…”

Section: Therapeutic Opportunitiesmentioning

confidence: 99%

Lipid signalling in disease

Wymann

Schneiter

2008

Nat Rev Mol Cell Biol

1,124

906

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Section: Therapeutic Opportunitiesmentioning

confidence: 99%

Lipid signalling in disease

Wymann

Schneiter

2008

Nat Rev Mol Cell Biol

1,124

906

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“…To elucidate the ErbB2 downstream signals that contribute to ErbB2-mediated breast cancer metastasis, we previously established in ErbB2-low-expressing MDA-MB-435 human breast cancer cells stable transfectants expressing either two ErbB2 mutants (V659E, a constitutive active form of ErbB2; K753M, a kinasedefective mutant), a wild-type ErbB2 or a control pcDNA3 vector ( Figure 1a and Nagata et al, 2004;Tan et al, 2005). We showed that the wild-type ErbB2-overexpressing 435.eB cells, ErbB2-activated V659E cells had increased tyrosine phosphorylation levels and kinase activities, and were more invasive in vitro and more metastatic in an animal model than the ErbB2 low-expressing parental MDA-MB-435 cells, control 435.neo cells and ErbB2 kinase-defective K753M cells (Tan et al, 2005).…”

Section: Upregulation and Activation Of Pkca By Erbb2mentioning

confidence: 99%

“…Reverse immunoprecipitation (IP) with an Src antibody (Figure 3b) also showed increased Src and PKCa association in ErbB2-activated cells. To test whether ErbB2 activates PKCa through Src, the 435.neo and 435.eB cells were treated with 5 or 10 mM PP2, an Src-specific inhibitor that has been shown to effectively block Src activation in these cells (Nagata et al, 2004;Tan et al, 2005). The results showed that PP2 inhibited the expression of PKCa and reduced PKCa phosphorylation in ErbB2-overexpressing cells to levels similar to that in the 435.neo cells, whereas PP2 only inhibited PKCa phosphorylation to a lesser degree in 435.neo cells (Figure 4a).…”

Section: Erbb2 Activates Pkca Through Src Kinasementioning

confidence: 99%

“…Activation of Src has been linked to the development of many human neoplasias, especially those of the colon, breast, lung and pancreas (Summy and Gallick, 2003). Src binds to ErbB2 and is activated in ErbB2-overexpressing cancer cells (Muthuswamy and Muller, 1995;Nagata et al, 2004;Tan et al, 2005). We recently showed that activation of ErbB2 can lead to increased Src protein synthesis and decreased Src protein degradation, resulting in Src protein upregulation and activation, which play critical roles in ErbB2-mediated breast cancer invasion and metastasis (Tan et al, 2005).…”

Section: Introductionmentioning

confidence: 99%

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Upregulation and activation of PKCα by ErbB2 through Src promotes breast cancer cell invasion that can be blocked by combined treatment with PKCα and Src inhibitors

Tan

Sun

et al. 2006

Oncogene

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Although ErbB2 is known to enhance breast cancer metastasis, the signaling events responsible for this remain elusive. a-Isozyme of protein kinase C (PKCa), which is involved in cancer development and progression, has been suggested to be activated by ErbB2 without direct evidence. In addition, the roles of PKCa in ErbB2-mediated cancer cell malignancy have not been clearly identified. In this study, we investigated whether ErbB2 can activate PKCa and determined what role PKCa plays in ErbB2-mediated breast cancer cell invasion. We expressed wild-type and mutant ErbB2 with altered signaling capacities in MDA-MB-435 breast cancer cells and revealed that overexpression or activation of ErbB2 in MDA-MB-435 cells upregulated and activated PKCa and that downregulation of ErbB2 by small-interfering RNA decreased the expression and activity of PKCa in BT474 breast cancer cells. These in vitro results were supported by data from breast cancer patient samples. In 150 breast cancer tumor samples, ErbB2-overexpressing tumors showed significantly higher positive rates of PKCa membrane immunohistochemistry staining than that of ErbB2-low-expressing tumors. Mechanistically, we found that PKCa is co-immunoprecipitated with Src and PKCa expression and activity can be decreased by Src inhibitor PP2 and by the expression of a dominantnegative mutant of Src. Moreover, ErbB2-mediated upregulation of urokinase-type plasminogen activator receptor (uPAR) is reduced by either the PKCa inhibitor Go6976 or the Src inhibitor PP2, and the combination of Go6976 with PP2 is superior to either agent alone in suppressing uPAR expression and cell invasion. These results demonstrate that PKCa is critical for ErbB2-mediated cancer cell invasion and provide valuable insights for current and future PKCa and Src inhibitor clinical trials.

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“…Akt regulates diverse cellular processes such as apoptosis, cell proliferation, differentiation, migration and angiogenesis. Furthermore, a number of studies have shown that overexpression and/or activation of Akt renders tumour cells resistant to chemotherapeutic drugs and signalling pathway inhibitors such as Gleevec, Iressa and Herceptin [21]. siRNA-mediated knockdown of Akt significantly reduces tumor growth and invasiveness and induces apoptosis [23].…”

mentioning

confidence: 99%

Opposing roles of the oncogene Akt isoforms in tumour progression: is there a dark side to Akt pathway inhibition?

Veeriah

2012

J Chem Biol

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PTEN activation contributes to tumor inhibition by trastuzumab, and loss of PTEN predicts trastuzumab resistance in patients

Cited by 1,609 publications

References 51 publications

Lipid signalling in disease

Lipid signalling in disease

Upregulation and activation of PKCα by ErbB2 through Src promotes breast cancer cell invasion that can be blocked by combined treatment with PKCα and Src inhibitors

Opposing roles of the oncogene Akt isoforms in tumour progression: is there a dark side to Akt pathway inhibition?

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