Distinct expression profiles and functions of Kindlins in breast cancer

Azorin, Paula; Bonin, Florian; Moukachar, Ahmad; Ponceau, Aurélie; Vacher, Sophie; Bièche, Ivan; Marangoni, Elisabetta; Fuhrmann, Laetitia; Vincent‐Salomon, Anne; Lidereau, Rosette; Driouch, Keltouma

doi:10.1186/s13046-018-0955-4

Cited by 18 publications

(24 citation statements)

References 58 publications

(69 reference statements)

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“…Conversely, this gene is also found to enhance breast cancer progression and metastasis by activating Twistmediated angiogenesis (72). Moreover, FERMT3 expressed in the TME is correlated with a poor prognosis of breast cancer patients (73), which is inconsistent with our finding that FERMT3 could serve as a protective prognostic factor in TNBC. These results highlight the complex role of FERMT3 which could exhibit dual effects, so the prognostic value of this gene in breast cancer deserve more attention.…”

Section: Discussioncontrasting

confidence: 83%

High Throughput Transcriptome Data Analysis and Computational Verification Reveal Immunotherapy Biomarkers of Compound Kushen Injection for Treating Triple-Negative Breast Cancer

Liu

Zhang³

et al. 2021

Front. Oncol.

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BackgroundAlthough notable therapeutic and prognostic benefits of compound kushen injection (CKI) have been found when it was used alone or in combination with chemotherapy or radiotherapy for triple-negative breast cancer (TNBC) treatment, the effects of CKI on TNBC microenvironment remain largely unclear. This study aims to construct and validate a predictive immunotherapy signature of CKI on TNBC.MethodsThe UPLC-Q-TOF-MS technology was firstly used to investigate major constituents of CKI. RNA sequencing data of CKI-perturbed TNBC cells were analyzed to detect differential expression genes (DEGs), and the GSVA algorithm was applied to explore significantly changed pathways regulated by CKI. Additionally, the ssGSEA algorithm was used to quantify immune cell abundance in TNBC patients, and these patients were classified into distinct immune infiltration subgroups by unsupervised clustering. Then, prognosis-related genes were screened from DEGs among these subgroups and were further overlapped with the DEGs regulated by CKI. Finally, a predictive immunotherapy signature of CKI on TNBC was constructed based on the LASSO regression algorithm to predict mortality risks of TNBC patients, and the signature was also validated in another TNBC cohort.ResultsTwenty-three chemical components in CKI were identified by UPLC-Q-TOF-MS analysis. A total of 3692 DEGs were detected in CKI-treated versus control groups, and CKI significantly activated biological processes associated with activation of T, natural killer and natural killer T cells. Three immune cell infiltration subgroups with 1593 DEGs were identified in TNBC patients. Then, two genes that can be down-regulated by CKI with hazard ratio (HR) > 1 and 26 genes that can be up-regulated by CKI with HR < 1 were selected as key immune- and prognosis-related genes regulated by CKI. Lastly, a five-gene prognostic signature comprising two risky genes (MARVELD2 and DYNC2I2) that can be down-regulated by CKI and three protective genes (RASSF2, FERMT3 and RASSF5) that can be up-regulated by CKI was developed, and it showed a good performance in both training and test sets.ConclusionsThis study proposes a predictive immunotherapy signature of CKI on TNBC, which would provide more evidence for survival prediction and treatment guidance in TNBC as well as a paradigm for exploring immunotherapy biomarkers in compound medicines.

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Section: Discussioncontrasting

confidence: 83%

High Throughput Transcriptome Data Analysis and Computational Verification Reveal Immunotherapy Biomarkers of Compound Kushen Injection for Treating Triple-Negative Breast Cancer

Liu

Zhang³

et al. 2021

Front. Oncol.

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“…Kindlin-3 overexpression in a BC cell line increased primary tumor growth and lung metastasis and mechanistically, kindlin-3overexpressing cells displayed a marked increase in VEGF secretion, which was dependent upon enhanced expression of the Twist transcription factor (Sossey-Alaoui et al, 2014) and enhanced β 1 integrin activation. The association of kindlin-3 with BC has been corroborated by some studies (Djaafri et al, 2014), although not all other studies (Azorin et al, 2018). In the present work, we establish that kindlin-3 phosphorylation is crucial for kindlin-3 function in BC cells and other cell types, including platelets, megakaryocytes, and human erythroleukemia (HEL) megakaryocytic-like cells.…”

Section: Introductionsupporting

confidence: 85%

Site-specific phosphorylation regulates the functions of kindlin-3 in a variety of cells

et al. 2019

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Studies of isolated cells, mice, and humans have demonstrated the vital role of the FERM domain protein kindlin-3 in integrin activation in certain hematopoietic and non-hematopoietic cells, consequent to binding to integrin β-subunits. To explore regulatory mechanisms, we developed a monoclonal antibody that selectively recognizes the phosphorylated form of Ser484 (pS484) in kindlin-3. Activation of platelets, HEL megakaryocytic-like cells and BT549 breast cancer cells led to enhanced expression of pS484 as assessed by immunofluorescence or Western blotting. In platelets, pS484 rose rapidly and transiently upon stimulation. When a mutant form of kindlin-3, T482S484/AA kindlin-3, was transduced into mouse megakaryocytes, it failed to support activation of integrin αIIbβ3, whereas wild-type kindlin-3 did. In MDA-MB231 breast cancer cells, expression of T482S484/AA kindlin-3 suppressed cell spreading, migration, invasion, and VEGF production. Wild-type kindlin-3 expressing cells markedly increased tumor growth in vivo, whereas T482S484/AA kindlin-3 significantly blunted tumor progression. Thus, our data establish that a unique phosphorylation event in kindlin-3 regulates its cellular functions.

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“…kindlin-2 and kindlin-3 can self-associate roles of kindlin-3 self-association in hematopoietic cells, endothelial cells, and breast cancer cells that express endogenous kindlin-3 (36)(37)(38). In light of our findings that kindlin self-association inversely correlates with integrin binding, it will be important to test the consequences of selectively modulating kindlin-3 selfassociation on cell adhesion and spreading and integrin activation and signaling in these cells.…”

Section: Discussionmentioning

confidence: 88%

Differences in self-association between kindlin-2 and kindlin-3 are associated with differential integrin binding

Kadry

Maisuria

Huet-Calderwood

et al. 2020

Journal of Biological Chemistry

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The integrin family of transmembrane adhesion receptors coordinate complex signaling networks that control the ability of cells to sense and communicate with the extracellular environment. Kindlin proteins are a central cytoplasmic component of these networks, directly binding integrin cytoplasmic domains and mediating interactions with cytoskeletal and signaling proteins. The physiological importance of kindlins is well established, but how the scaffolding functions of kindlins are regulated at the molecular level is still unclear. Here, using a combination of GFP nanotrap association assays, pulldown and integrin-binding assays, and live-cell imaging, we demonstrate that full-length kindlins can oligomerize (self-associate) in mammalian cells, and we propose that this self-association inhibits integrin binding and kindlin localization to focal adhesions. We show that both kindlin-2 and kindlin-3 can self-associate and that kindlin-3 self-association is more robust. Using chimeric mapping, we demonstrate that the F2PH and F3 subdomains are important for kindlin self-association. Through comparative sequence analysis of kindlin-2 and kindlin-3, we identify kindlin-3 point mutations that decrease self-association and enhance integrin binding, affording mutant kindlin-3 the ability to localize to focal adhesions. Our results support the notion that kindlin self-association negatively regulates integrin binding.

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Distinct expression profiles and functions of Kindlins in breast cancer

Cited by 18 publications

References 58 publications

High Throughput Transcriptome Data Analysis and Computational Verification Reveal Immunotherapy Biomarkers of Compound Kushen Injection for Treating Triple-Negative Breast Cancer

High Throughput Transcriptome Data Analysis and Computational Verification Reveal Immunotherapy Biomarkers of Compound Kushen Injection for Treating Triple-Negative Breast Cancer

Site-specific phosphorylation regulates the functions of kindlin-3 in a variety of cells

Differences in self-association between kindlin-2 and kindlin-3 are associated with differential integrin binding

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