<i>Retracted</i>: Effects of RNA interference‐mediated silencing of toll‐like receptor 4 gene on proliferation and apoptosis of human breast cancer MCF‐7 and MDA‐MB‐231 cells: An in vitro study

Gao, Xiaoling; Yang, Jiaojiao; Wang, Shujuan; Chen, Yan; Wang, Bei; Cheng, Er-Jing; Gong, Jiannan; Dong, Yanting; Dai, Li‐Xin; Xiang-li, Wang; Huang, Yongye; An, Dong-Dong

doi:10.1002/jcp.26573

Cited by 4 publications

(1 citation statement)

References 27 publications

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“…Several immune-related molecules have been found to be important for breast cancer progression-related mechanisms. Among them is the TLR4/myD88 pathway, which is expressed in tumor cells and has been linked to axillary lymph node metastasis and histological grade [ 8 ], while the inhibition of TLR4 expression impedes proliferation and promotes apoptosis of breast cancer cells [ 9 ]. Furthermore, activation of nuclear factor-kappaB (NFκB) is also common in breast cancer and has been associated with resistance to therapy and is present in more aggressive tumors.…”

Section: Introductionmentioning

confidence: 99%

ERα36–GPER1 Collaboration Inhibits TLR4/NFκB-Induced Pro-Inflammatory Activity in Breast Cancer Cells

Notas

Panagiotopoulos

Vamvoukaki

et al. 2021

IJMS

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Inflammation is important for the initiation and progression of breast cancer. We have previously reported that in monocytes, estrogen regulates TLR4/NFκB-mediated inflammation via the interaction of the Erα isoform ERα36 with GPER1. We therefore investigated whether a similar mechanism is present in breast cancer epithelial cells, and the effect of ERα36 expression on the classic 66 kD ERα isoform (ERα66) functions. We report that estrogen inhibits LPS-induced NFκB activity and the expression of downstream molecules TNFα and IL-6. In the absence of ERα66, ERα36 and GPER1 are both indispensable for this effect. In the presence of ERα66, ERα36 or GPER1 knock-down partially inhibits NFκB-mediated inflammation. In both cases, ERα36 overexpression enhances the inhibitory effect of estrogen on inflammation. We also verify that ERα36 and GPER1 physically interact, especially after LPS treatment, and that GPER1 interacts directly with NFκB. When both ERα66 and ERα36 are expressed, the latter acts as an inhibitor of ERα66 via its binding to estrogen response elements. We also report that the activation of ERα36 leads to the inhibition of breast cancer cell proliferation. Our data support that ERα36 is an inhibitory estrogen receptor that, in collaboration with GPER1, inhibits NFκB-mediated inflammation and ERα66 actions in breast cancer cells.

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Section: Introductionmentioning

confidence: 99%

ERα36–GPER1 Collaboration Inhibits TLR4/NFκB-Induced Pro-Inflammatory Activity in Breast Cancer Cells

Notas

Panagiotopoulos

Vamvoukaki

et al. 2021

IJMS

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Sodium arsenite-mediated upregulation of circDHX34 promotes apoptosis in hormone-independent breast cancer cells by regulating apoptotic genes

Jiang

Tan

et al. 2021

Environ Sci Pollut Res

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Targeting Toll like Receptors in Cancer: Role of TLR Natural and Synthetic Modulators

Narayanankutty¹,

Sasidharan

Job³

2020

CPD

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Background: Toll like receptors (TLRs) are a group of transmembrane receptors belonging to the broad class pattern recognition receptors (PRR), involved in the recognition of Pathogen Associated Molecular Patterns (PAMPs) and thereby inducing an immune response. Apart from these exogenous PAMPs, numerous endogenous PAMPs are also ligands for various TLRs thereby activating the TLR dependent immune response, subsequently leading to the onset of an inflammatory response. Prolonged activation of TLR by these endogenous PAMPs leads to chronic inflammatory insults to the body and which in turn alters the proliferative patterns of the cells, which ultimately leads to the development of cancer. Objectives: The present review aims to provide a detailed outline of the differential roles of various TLRs in cancer and the possible use of them as a therapeutic target. Methods: Data were collected from PubMed/Sciencedirect/Web of Science database and sorted; the latest literature on TLRs was incorporated in the review. Results: Among the different TLRs, few are reported to be anti-neoplastic, which controls the cell growth and multiplication in response to the endogenous signals. On the contrary, numerous studies have reported the pro-carcinogenic potentials of TLRs. Hence, TLRs has emerged as a potential target for the prevention and treatment of various types of cancers. Several molecules such as monoclonal antibodies, small molecule inhibitors and natural products have shown promising anticancer potential by effectively modulating the TLR signalling. Conclusion: Toll like receptors play vital roles in the process of carcinogenesis, hence TLR targeting is a promising approach for cancer prevention.

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Retracted: Effects of RNA interference‐mediated silencing of toll‐like receptor 4 gene on proliferation and apoptosis of human breast cancer MCF‐7 and MDA‐MB‐231 cells: An in vitro study

Cited by 4 publications

References 27 publications

ERα36–GPER1 Collaboration Inhibits TLR4/NFκB-Induced Pro-Inflammatory Activity in Breast Cancer Cells

ERα36–GPER1 Collaboration Inhibits TLR4/NFκB-Induced Pro-Inflammatory Activity in Breast Cancer Cells

Sodium arsenite-mediated upregulation of circDHX34 promotes apoptosis in hormone-independent breast cancer cells by regulating apoptotic genes

Targeting Toll like Receptors in Cancer: Role of TLR Natural and Synthetic Modulators

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