Phase II studies of two different schedules of dasatinib in bone metastasis predominant metastatic breast cancer: SWOG S0622

Schott, Anne F.; Barlow, William E.; Poznak, Catherine Van; Hayes, Daniel F.; Moinpour, Carol M.; Lew, Danika; Dy, Philip A.; Keller, Evan T.; Keller, Jill M.; Hortobágyi, Gabriel N.

doi:10.1007/s10549-016-3911-z

Cited by 35 publications

(27 citation statements)

References 32 publications

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“…Patients in the advanced stage in various solid tumors show resistance to treatment, and a number of studies have investigated novel antitumor agents, with a particular focus on molecularly targeted drugs. In recent years, Src inhibitors have been studied extensively ( 8 – 17 ).…”

Section: Discussionmentioning

confidence: 99%

“…Clinical trials have revealed no effect of dasatinib alone on breast, pancreatic, colorectal and ovarian tumor progression, overall survival or progression-free survival ( 8 , 12 , 13 , 15 ). This may be due to the activation of other signaling molecules, such as the Src family kinases Janus kinase and FGR ( 14 ).…”

Section: Discussionmentioning

confidence: 99%

“…It was originally approved as a drug for the treatment of chronic myeloid leukemia and Philadelphia chromosome-positive acute lymphoblastic leukemia ( 4 , 5 ). Clinical trials have been conducted using dasatinib in combination with anticancer drugs for the treatment of breast, colon, prostate and other cancers ( 8 – 17 ). Single-agent dasatinib has not exhibited any clinical activity in breast, pancreatic, colorectal and ovarian carcinoma ( 8 , 12 , 13 , 15 ).…”

Section: Introductionmentioning

confidence: 99%

“…Clinical trials have been conducted using dasatinib in combination with anticancer drugs for the treatment of breast, colon, prostate and other cancers ( 8 – 17 ). Single-agent dasatinib has not exhibited any clinical activity in breast, pancreatic, colorectal and ovarian carcinoma ( 8 , 12 , 13 , 15 ). However, combination therapy with dasatinib and anticancer drugs has been demonstrated to be clinically effective in the treatment of breast, prostate, ovarian and pancreatic cancers ( 9 – 11 , 14 , 16 , 17 ).…”

Section: Introductionmentioning

confidence: 99%

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Growth inhibitory effect of the Src inhibitor dasatinib in combination with anticancer agents on uterine cervical adenocarcinoma cells

et al. 2017

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Uterine cervical adenocarcinoma has a poor clinical prognosis when compared with squamous cell carcinoma. Therefore, the development of new treatment strategies for uterine cervical adenocarcinoma is necessary. Src is a proto-oncogene that is important in cancer progression. Dasatinib is a Src inhibitor that has been reported to be effective when used in combination with anticancer drugs. The present study aimed to confirm Src expression in human cervical adenocarcinoma cell lines and to determine the mechanism underlying the inhibitory effect of dasatinib on Src signaling in vitro. Western blot analysis was performed to investigate Src expression in cervical adenocarcinoma cell lines (HeLa and TCO-2 cells). The cells were cultured for 48 h with the addition of different concentrations of anticancer drugs (paclitaxel or oxaliplatin). Viable cell count was measured using a colorimetric (WST-1) assay. The concentrations of anticancer agents were fixed according to the results obtained, and the same experiments were performed using the drugs in combination with dasatinib at various concentrations to determine the concentrations that significantly affected the number of viable cells. The presence or absence of apoptosis was investigated using a caspase-3/7 assay. Signal transduction in each cell line was examined using western blotting. Src was activated in the two cell lines, and cell proliferation was significantly suppressed by each anticancer drug in combination with 10 µM dasatinib. Caspase-3/7 activity was also increased and Src signaling was suppressed by each anticancer drug in combination with dasatinib. In conclusion, Src is overexpressed in cervical adenocarcinoma cell lines, and dasatinib inhibits intracellular Src signaling and causes apoptosis. The results of the present study suggest that Src may be targeted in novel therapeutic strategies for cervical adenocarcinoma.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Growth inhibitory effect of the Src inhibitor dasatinib in combination with anticancer agents on uterine cervical adenocarcinoma cells

et al. 2017

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“…This results in the release of matrix-derived growth factors, such as transforming growth factor-β1 (TGF-β1), which further stimulate tumor growth [6,7]. Although novel therapeutic options and targets are emerging (e.g., tyrosine kinase inhibitors, microRNAs [8][9][10][11]), the disease remains incurable once osteolytic lesions have developed.…”

Section: Introductionmentioning

confidence: 99%

Breast cancer bone metastases are attenuated in a Tgif1-deficient bone microenvironment

et al. 2020

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Background: Osteoclast activation is a hallmark of breast cancer-induced bone disease while little is known about the role of osteoblasts in this process. Recently, we identified the homeodomain protein TG-interacting factor-1 (Tgif1) as a crucial regulator of osteoblast function. In this study, we demonstrate that lack of Tgif1 also restricts the progression of breast cancer bone metastases. Methods: Transwell migration assays were used to investigate the osteoblast-breast cancer cell interaction in vitro. Molecular analyses included RNA sequencing, immunoblotting, and qRT-PCR. To determine the role of Tgif1 in metastatic bone disease, 4T1 breast cancer cells were injected intracardially into mice with a germ line deletion of Tgif1 (Tgif1 −/−) or control littermates (Tgif1 +/+). Progression of bone metastases and alterations in the bone microenvironment were assessed using bioluminescence imaging, immunofluorescence staining, confocal microscopy, and histomorphometry. Results: Medium conditioned by osteoblasts stimulated breast cancer cell migration, indicating a potential role of osteoblasts during bone metastasis progression. Tgif1 expression was strongly increased in osteoblasts upon stimulation by breast cancer cells, demonstrating the implication of Tgif1 in the osteoblast-breast cancer cell interaction. Indeed, conditioned medium from osteoblasts of Tgif1 −/− mice failed to induce breast cancer cell migration compared to control, suggesting that Tgif1 in osteoblasts augments cancer cell motility. Semaphorin 3E (Sema3E), which is abundantly secreted by Tgif1 −/− osteoblasts, dose-dependently reduced breast cancer cell migration while silencing of Sema3E expression in Tgif1 −/− osteoblasts partially restored the impaired migration. In vivo, we observed a decreased number of breast cancer bone metastases in Tgif1 −/− mice compared to control littermates. Consistently, the presence of single breast cancer cells or micro-metastases in the tibiae was reduced in Tgif1 −/− mice. Breast cancer cells localized in close proximity to Endomucin-positive vascular cells as well as to osteoblasts. Although Tgif1 deficiency did not affect the bone marrow vasculature, the number and activity of osteoblasts were reduced compared to control. This suggests that the protective effect on bone metastases might

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Breast Cancer Metastasis to Bone: Look into the Future

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Scioli

Bonfiglio

et al. 2023

Interdisciplinary Cancer Research

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Phase II studies of two different schedules of dasatinib in bone metastasis predominant metastatic breast cancer: SWOG S0622

Cited by 35 publications

References 32 publications

Growth inhibitory effect of the Src inhibitor dasatinib in combination with anticancer agents on uterine cervical adenocarcinoma cells

Growth inhibitory effect of the Src inhibitor dasatinib in combination with anticancer agents on uterine cervical adenocarcinoma cells

Breast cancer bone metastases are attenuated in a Tgif1-deficient bone microenvironment

Breast Cancer Metastasis to Bone: Look into the Future

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