Epithelial–mesenchymal transition: The history, regulatory mechanism, and cancer therapeutic opportunities

Huang, Zhao; Zhang, Zhe; Zhou, Chengwei; Liu, Lin; Huang, Canhua

doi:10.1002/mco2.144

Cited by 50 publications

(40 citation statements)

References 549 publications

(1,151 reference statements)

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“…One of the conceivable effector mechanisms is the induction of epithelial-mesenchymal transformation (EMT), characterized by invasion and enhanced motility. 52 Indeed, abemaciclib triggered vimentin and N-cadherin expression, especially in Mlh1 −/− mice, but effectively suppressed Fpr2 , which is also involved in invasion and metastasis. 53 , 54 We, therefore, conclude a compensatory mechanism to counteract abemaciclib-driven EMT.…”

Section: Discussionmentioning

confidence: 96%

CDK4/6 blockade provides an alternative approach for treatment of mismatch-repair deficient tumors

et al. 2022

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Mismatch repair-deficient (dMMR) tumors show a good response toward immune checkpoint inhibitors (ICI), but developing resistance impairs patients’ outcomes. Here, we compared the therapeutic potential of an α-PD-L1 antibody with the CDK4/6 inhibitor abemaciclib in two preclinical mouse models of dMMR cancer, focusing on immune-modulatory effects of either treatment. Abemaciclib monotherapy significantly prolonged overall survival of Mlh1 −/− and Msh2 loxP/loxP;TgTg(Vil1- cre) mice (Mlh1 −/− : 14.5 wks vs . 9.0 wks (α-PD-L1), and 3.5 wks (control); Msh2 loxP/loxP;TgTg(Vil1- cre) : 11.7 wks vs . 9.6 wks (α-PD-L1), and 2.0 wks (control)). The combination was not superior to either monotherapy. PET/CT imaging revealed individual response profiles, with best clinical responses seen with abemaciclib mono- and combination therapy. Therapeutic effects were accompanied by increasing numbers of tumor-infiltrating CD4 + /CD8 + T-cells and lower numbers of M2-macrophages. Levels of T cell exhaustion markers and regulatory T cell counts declined. Expression analysis identified higher numbers of dendritic cells and neutrophils within tumors together with high expression of DNA damage repair genes as part of the global stress response. In Mlh1 −/− tumors, abemaciclib suppressed the PI3K/Akt pathway and led to induction of Mxd4 / Myc . The immune-modulatory potential of abemaciclib renders this compound ideal for dMMR patients not eligible for ICI treatment.

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Section: Discussionmentioning

confidence: 96%

CDK4/6 blockade provides an alternative approach for treatment of mismatch-repair deficient tumors

et al. 2022

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“…However, radioresistance is one of the main challenges for the applications of radiotherapy. At present, a series of studies have pointed out that radioresistance is related to DNA repair capacity, reduced apoptosis, cell cycle status, EMT and other factors, among which EMT is one of the most important factors affecting the sensitivity of cancer cells to ionizing radiation (IR) [39][40][41]. Studies have shown that IR-induced EMT accelerates the invasion, migration, and radioresistance of various tumor cell lines, including lung, liver, and breast cancer, after radiotherapy.…”

Section: Discussionmentioning

confidence: 99%

LPAR5 confers radioresistance to cancer cells associated with EMT activation via the ERK/Snail pathway

Sun

Xie

et al. 2022

J Transl Med

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Background Epithelial-to-mesenchymal transition (EMT) is a critical event contributing to more aggressive phenotypes in cancer cells. EMT is frequently activated in radiation-targeted cells during the course of radiotherapy, which often endows cancers with acquired radioresistance. However, the upstream molecules driving the signaling pathways of radiation-induced EMT have not been fully delineated. Methods In this study, RNA-seq-based transcriptome analysis was performed to identify the early responsive genes of HeLa cells to γ-ray irradiation. EMT-associated genes were knocked down by siRNA technology or overexpressed in HeLa cells and A549 cells, and the resulting changes in phenotypes of EMT and radiosensitivity were assessed using qPCR and Western blotting analyses, migration assays, colony-forming ability and apoptosis of flow cytometer assays. Results Through RNA-seq-based transcriptome analysis, we found that LPAR5 is downregulated in the early response of HeLa cells to γ-ray irradiation. Radiation-induced alterations in LPAR5 expression were further revealed to be a bidirectional dynamic process in HeLa and A549 cells, i.e., the early downregulating phase at 2 ~ 4 h and the late upregulating phase at 24 h post-irradiation. Overexpression of LPAR5 prompts EMT programing and migration of cancer cells. Moreover, increased expression of LPAR5 is significantly associated with IR-induced EMT and confers radioresistance to cancer cells. Knockdown of LPAR5 suppressed IR-induced EMT by attenuating the activation of ERK signaling and downstream Snail, MMP1, and MMP9 expression. Conclusions LPAR5 is an important upstream regulator of IR-induced EMT that modulates the ERK/Snail pathway. This study provides further insights into understanding the mechanism of radiation-induced EMT and identifies promising targets for improving the effectiveness of cancer radiation therapy.

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“…However, radioresistance is one of the main challenges for the applications of radiotherapy. At present, a series of studies have pointed out that radioresistance is related to DNA repair capacity, reduced apoptosis, cell cycle status, EMT and other factors, among which EMT is one of the most important factors affecting the sensitivity of cancer cells to ionizing radiation (IR) [40][41][42]. Studies have shown that IR-induced EMT accelerates the invasion, migration, and radioresistance of various tumor cell lines including lung, liver, and breast cancer after radiotherapy.…”

Section: Discussionmentioning

confidence: 99%

LPAR5 confers cancer cells radioresistance associated with EMT activation via ERK/ Snail pathway

Sun

li²,

Xie

et al. 2022

Preprint

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Epithelial-to-mesenchymal transition (EMT) is a critical event contributing cancer cells more aggressive phenotypes. EMT programs are frequently activated in radiation-targeted cells during the course of radiotherapy, and which often endows cancers the acquired radioresistance. Through RNA-seq based transcriptome analysis, here we found that LPAR5 is downregulated in the early response of HeLa cells to γ-rays irradiation. Radiation-induced alterations of LPAR5 expression were further revealed to be a bidirectional dynamic process in HeLa and A549 cells, i.e., early downregulating phase at 2 ~ 4h and late upregulating phase at 24h post-irradiation. Overexpression of LPAR5 prompts EMT programing and migration of cancer cells. Moreover, increased expression of LPAR5 is significantly associated with IR-induced EMT and confers cancer cells radioresistance. Knockdown of LPAR5 suppressed IR-induced EMT by attenuating the activation of ERK signaling and downstream Snail, MMP1, and MMP9 expressions. In conclusion, LPAR5 is an important upstream regulator of IR-induced EMT through modulating ERK/Snail pathway. This study provides further insights into understanding the mechanism of radiation-induced EMT and promising target for improving the effectiveness of cancer radiation therapy.

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Epithelial–mesenchymal transition: The history, regulatory mechanism, and cancer therapeutic opportunities

Cited by 50 publications

References 549 publications

CDK4/6 blockade provides an alternative approach for treatment of mismatch-repair deficient tumors

CDK4/6 blockade provides an alternative approach for treatment of mismatch-repair deficient tumors

LPAR5 confers radioresistance to cancer cells associated with EMT activation via the ERK/Snail pathway

LPAR5 confers cancer cells radioresistance associated with EMT activation via ERK/ Snail pathway

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