A positive feedback loop: RAD18-YAP-TGF-β between triple-negative breast cancer and macrophages regulates cancer stemness and progression

Yan, Xinmin; He, Yunjie; Yang, Shuguang; Zeng, Tianyu; Hua, Yijia; Bao, Shengnan; Yang, Fan; Duan, Ningjun; Sun, Chunxiao; Liang, Yan; Fu, Ziyi; Huang, Xing‐Huai; Li, Wei; Yin, Yongmei

doi:10.1038/s41420-022-00968-9

Cited by 12 publications

(10 citation statements)

References 54 publications

(55 reference statements)

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“…Our results displayed a connection between the nuclear YAP and the upregulation of TGF‐β1, which were in correspondence with previously published studies that knocked out of LATS1/2 could lead to decreased expression of phosphorylated YAP, which could cause increased expression of TGF‐β in mouse neuroepithelium and liver cells 49,50 . Other studies also showed that when the activity of YAP was inhibited with Verteporfin, the TGF‐β pathway was hindered in fibroblast, 51 and the secretion of TGF‐β by macrophages was diminished 52 . These results suggest a possible crosstalk between Hippo and TGF‐β pathways where dephosphorylated YAP could translocate into the nucleus to activate the TGF‐β signaling pathway.…”

Section: Discussionsupporting

confidence: 88%

Matrix stiffness‐induced α‐tubulin acetylation is required for skin fibrosis formation through activation of Yes‐associated protein

Wen

Gao

Liu

et al. 2023

MedComm

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Skin fibrosis, a pathological process featured by fibroblast activation and extracellular matrix (ECM) deposition, makes a significant contribution to morbidity. Studies have identified biomechanics as the central element in the complex network of fibrogenesis that drives the profibrotic feedback loop. In this study, we found that the acetylation of α‐tubulin at lysine 40 (K40) was augmented in fibrotic skin tissues. Further analysis showed that α‐tubulin acetylation is required for fibroblast activation, including contraction, migration, and ECM deposition. More importantly, we revealed that biomechanics‐induced upregulation of K40 acetylation promotes fibrosis by mediating mechanosensitive Yes‐associated protein S127 dephosphorylation and its cytoplasm nucleus shuttle. Furthermore, we demonstrated that the knockdown of α‐tubulin acetyltransferase 1 could rescue the K40 acetylation upregulation caused by increased matrix rigidity and ameliorate skin fibrosis both in vivo and in vitro. Herein, we highlight the critical role of α‐tubulin acetylation in matrix stiffness‐induced skin fibrosis and clarify a possible molecular mechanism. Our research suggests α‐tubulin acetylation as a potential target for drug design and therapeutic intervention.

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Section: Discussionsupporting

confidence: 88%

Matrix stiffness‐induced α‐tubulin acetylation is required for skin fibrosis formation through activation of Yes‐associated protein

Wen

Gao

Liu

et al. 2023

MedComm

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“…JH-RE-06 also suppresses growth of A549 and H1299 lung cancer cells grown as xenografts in vivo ( 155 ). Further consistent with a role for TLS in sustaining tumors, RAD18 overexpression elevates colonization of esophageal cancer cells in the mice lung ( 156 ), while RAD18-deficient TNBC xenografts show reduced tumor volume ( 157 ). Taken together, these studies suggest that TLS is a cancer-dependency at least under select conditions.…”

Section: Evidence That Tls Polymerases Contribute To Cancermentioning

confidence: 59%

“…Implanting cancer cells orthotopically in mice provides a convenient approach to study tumor growth in a physiologically relevant environment. Orthotopic injection of esophageal cancer cells overexpressing RAD18 increases colonization ( 156 ), while RAD18-deficient TNBC cell xenografts show reduced tumor growth ( 157 ). TLS inhibition by the REV1 inhibitor JH-RE-06 decreases colonization of lung cancer cells in mice ( 155 ).…”

Section: Evidence That Tls Polymerases Contribute To Cancermentioning

confidence: 99%

Roles of trans-lesion synthesis (TLS) DNA polymerases in tumorigenesis and cancer therapy

et al. 2023

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DNA damage tolerance and mutagenesis are hallmarks and enabling characteristics of neoplastic cells that drive tumorigenesis and allow cancer cells to resist therapy. The ‘Y-family’ trans-lesion synthesis (TLS) DNA polymerases enable cells to replicate damaged genomes, thereby conferring DNA damage tolerance. Moreover, Y-family DNA polymerases are inherently error-prone and cause mutations. Therefore, TLS DNA polymerases are potential mediators of important tumorigenic phenotypes. The skin cancer-propensity syndrome xeroderma pigmentosum-variant (XPV) results from defects in the Y-family DNA Polymerase Pol eta (Polη) and compensatory deployment of alternative inappropriate DNA polymerases. However, the extent to which dysregulated TLS contributes to the underlying etiology of other human cancers is unclear. Here we consider the broad impact of TLS polymerases on tumorigenesis and cancer therapy. We survey the ways in which TLS DNA polymerases are pathologically altered in cancer. We summarize evidence that TLS polymerases shape cancer genomes, and review studies implicating dysregulated TLS as a driver of carcinogenesis. Because many cancer treatment regimens comprise DNA-damaging agents, pharmacological inhibition of TLS is an attractive strategy for sensitizing tumors to genotoxic therapies. Therefore, we discuss the pharmacological tractability of the TLS pathway and summarize recent progress on development of TLS inhibitors for therapeutic purposes.

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“…Moreover, BA dose-dependently inhibited the GRP78-mediated secretion of TGF-β, thereby suppressing macrophage polarization, IL-6 secretion, and IL-6-mediated gastric cancer stemness ( Figure 6 ). In a previous study, TGF-β signaling was reported to involve a positive feedback loop in the regulation of triple-negative breast cancer and macrophage-mediated cancer stemness and progression [ 41 ]. The results also indicated that BA-induced downregulation of TGF-β through the GRP78-mediated pathway may inhibit the positive feedback loop between gastric cancer cells and macrophage-mediated cancer stemness and tumor progression.…”

Section: Discussionmentioning

confidence: 99%

Betulinic Acid Inhibits the Stemness of Gastric Cancer Cells by Regulating the GRP78-TGF-β1 Signaling Pathway and Macrophage Polarization

et al. 2023

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Cancer stemness is the process by which cancer cells acquire chemoresistance and self-renewal in the tumor microenvironment. Glucose-regulated protein 78 (GRP78) is a biomarker for gastric cancer and is involved in cancer stemness. By inducing cancer stemness in various types of cancer, the polarization of macrophages into tumor-associated macrophages (TAMs) controls tumor progression. Betulinic acid (BA) is a bioactive natural compound with anticancer properties. However, whether GRP78 regulates TAM-mediated cancer stemness in the tumor microenvironment and whether BA inhibits GRP78-mediated cancer stemness in gastric cancer remain unknown. In this study, we investigated the role of GRP78 in gastric cancer stemness in a tumor microenvironment regulated by BA. The results indicated that BA inhibited not only GRP78-mediated stemness-related protein expression and GRP78-TGF-β-mediated macrophage polarization into TAMs, but also TAM-mediated cancer stemness. Therefore, BA is a promising candidate for clinical application in combination-chemotherapy targeting cancer stemness.

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A positive feedback loop: RAD18-YAP-TGF-β between triple-negative breast cancer and macrophages regulates cancer stemness and progression

Cited by 12 publications

References 54 publications

Matrix stiffness‐induced α‐tubulin acetylation is required for skin fibrosis formation through activation of Yes‐associated protein

Matrix stiffness‐induced α‐tubulin acetylation is required for skin fibrosis formation through activation of Yes‐associated protein

Roles of trans-lesion synthesis (TLS) DNA polymerases in tumorigenesis and cancer therapy

Betulinic Acid Inhibits the Stemness of Gastric Cancer Cells by Regulating the GRP78-TGF-β1 Signaling Pathway and Macrophage Polarization

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