Src Kinase and Mitogen-Activated Protein Kinases in the Progression from Normal to Malignant Endometrium

Desouki, Mohamed Mokhtar; Rowan, Brian G.

doi:10.1158/1078-0432.ccr-0661-03

Cited by 17 publications

(17 citation statements)

References 35 publications

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“…Consistent with our results, active, phospho-JNK levels coincided with a decrease in estrogen and progesterone levels, which induced apoptosis in cultured endometrial cells [42,43]. Endometrial adenocarcinomas exhibited increased JNK expression relative to benign endometrium but no significant increase in JNK phosphorylation/activation was detected in tumors of increasing grade [12], suggesting that JNK does not exhibit oncogenic activity associated with progression to malignancy. However, JNK may also function as a tumor suppressor, regulating apoptosis and response to chemotherapy [7,8,11] and, prior to this study, the role of JNK in apoptotic responses in endometrial cancer cells had not been addressed.…”

Section: Discussionsupporting

confidence: 89%

“…However, since our data show that JNK can be activated independently of PKCd and higher-grade tumors retain JNK expression and activity [12], JNK activation, by PKCd-independent pathways, may mediate apoptotic responses to DNA damage in endometrial adenocarcinoma, despite a reduction in PKCd expression.…”

Section: Discussionmentioning

confidence: 65%

“…Expression of JNK is elevated in endometrial carcinomas relative to benign endometrium [12], but its role as a promoter or suppressor of tumorigenesis is not understood. Apoptosis is a critical component of normal endometrial physiology and its aberrant regulation is a hallmark of progression to malignancy [13][14][15].…”

Section: Introductionmentioning

confidence: 99%

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c-Jun N-terminal kinase regulates apoptosis in endometrial cancer cells

et al. 2009

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Section: Discussionsupporting

confidence: 89%

Section: Discussionmentioning

confidence: 65%

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c-Jun N-terminal kinase regulates apoptosis in endometrial cancer cells

et al. 2009

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“…3a). Elevated levels of phosphorylated JNK have been found in breast tumors [41]. JNK activation has been shown to mediate the invasive activity of breast cancer cells [42][43][44].…”

Section: Resultsmentioning

confidence: 99%

Leptin utilizes Jun N-terminal kinases to stimulate the invasion of MCF-7 breast cancer cells

McMurtry

Simeone

Nieves-Alicea

et al. 2008

Clin Exp Metastasis

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In breast tumors, high levels of leptin have been associated with increased incidence of breast cancer metastasis. Breast cancer metastasis is directly associated with breast cancer cell invasion. However, whether leptin could augment breast cancer cell invasion is not known. Here we showed that leptin increased the invasiveness and the matrix metallo-proteinase-2 (MMP-2) activity of the MCF-7 breast cancer cell line. Leptin stimulated the phosphorylation of extracellular signals regulated kinases, signal transducers and activators of transcription 3 and Jun N-terminal kinases (JNK); however, only inhibition of JNK decreased leptin-mediated activation of MMP-2. Furthermore, inhibition of JNK suppressed leptin-mediated breast cancer cell invasion. Here we report the novel findings that leptin increased invasion of breast cancer cells by activating JNK, resulting in increased MMP-2 activity.

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“…Previous studies from this laboratory demonstrated that active kinases are elevated in benign when compared to cancerous endometrium raising the possibility that elevation of active kinases in benign endometrium could contribute to the endometrial oncogenic transformation [10]. Additional work demonstrated that c-Src promoted tamoxifen agonist activity in Ishikawa endometrial cells [11].…”

Section: Introductionmentioning

confidence: 92%

KX-01, a novel Src kinase inhibitor directed toward the peptide substrate site, synergizes with tamoxifen in estrogen receptor α positive breast cancer

Anbalagan

Carrier

Glodowski

et al. 2011

Breast Cancer Res Treat

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KX-01 is the first clinical Src inhibitor of the novel peptidomimetic class that targets the peptide substrate site of Src providing more specificity toward Src kinase. The present study was designed to evaluate the effects of KX-01 as a single agent and in combination with tamoxifen (TAM) on cell growth and apoptosis of ERα positive breast cancer in vitro and in vivo. Flow cytometry demonstrated that KX-01 induced cell cycle arrest in G2/M phase. Immunofluorescent staining for mitotic phase markers and TUNEL staining indicated that cells had arrested in the mitotic phase and mitotic arrested cells were undergoing apoptosis. KX-01 induced nuclear accumulation of cyclin B1, and activation of CDK1, MPM2, and Cdc25C that is required for progression past the G2/M checkpoint. Apoptosis resulted from activation of caspases 6, 7, 8, and 9. Combinational index analysis revealed that combinations of KX-01 with TAM resulted in synergistic growth inhibition of breast cancer cell lines. KX-01 combined with TAM resulted in decreased ERα phosphorylation at Src-regulated phosphorylation sites serines 118 and 167 that were associated with reduced ERα transcriptional activity. Orally administered KX-01 resulted in a dose dependent growth inhibition of MCF-7 tumor xenografts, and in combination with TAM exhibited synergistic growth inhibition. Immunohistochemical analysis revealed that combinational treatment reduced angiogenesis, and ERα signaling in tumors compared to either drug alone that may underlie the synergistic tumor growth inhibition. Combinations of KX-01 with endocrine therapy present a promising new strategy for clinical management of ERα positive breast cancer.

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Src Kinase and Mitogen-Activated Protein Kinases in the Progression from Normal to Malignant Endometrium

Cited by 17 publications

References 35 publications

c-Jun N-terminal kinase regulates apoptosis in endometrial cancer cells

c-Jun N-terminal kinase regulates apoptosis in endometrial cancer cells

Leptin utilizes Jun N-terminal kinases to stimulate the invasion of MCF-7 breast cancer cells

KX-01, a novel Src kinase inhibitor directed toward the peptide substrate site, synergizes with tamoxifen in estrogen receptor α positive breast cancer

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