The complementary roles of STAT3 and STAT1 in cancer biology: insights into tumor pathogenesis and therapeutic strategies

Wang, Weiyuan; Lopez McDonald, Melanie Cristina; Kim, Christine; Ma, Mirielle; Pan, Zetao (Tommy); Kaufmann, Charlotte; Frank, David A.

doi:10.3389/fimmu.2023.1265818

Cited by 8 publications

(5 citation statements)

References 111 publications

(40 reference statements)

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“…8 F). These results were consistent with previous reports showing that YTHDF1 gene deletion reduced STAT3 protein levels and phosphorylation, disrupted the STAT3-STAT1 balance in macrophages, promoted STAT1 expression and phosphorylation, and induced an anti-tumor polarization of macrophages [ 36 , 48 ]. Thus, our study provides valuable insights into the molecular mechanisms underlying the combination therapy and highlights its potential to enhance the efficacy of existing immunotherapies.…”

Section: Resultssupporting

confidence: 93%

“…Reduction of STAT3 through pharmacological or genetic methods in many systems enhances STAT1 activation. This is because both STAT1 and STAT3 bind to the same phosphorylated tyrosine residues in signaling proteins such as gp130, leading to increased phosphorylation of STAT1 protein due to reduced competition at these sites [ 36 ]. MeRIP-qPCR analysis showed that STAT3 mRNA has significantly higher m6A enrichment levels in M2 macrophages compared to M1, indicating the regulatory role of YTHDF1 in the methylation of STAT3 mRNA and its impact on STAT3 protein translation (Fig.…”

Section: Resultsmentioning

confidence: 99%

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Photosensitive and dual-targeted chromium nanoparticle delivering small interfering RNA YTHDF1 for molecular-targeted immunotherapy in liver cancer

Chen,

He,

Huang

et al. 2024

J Nanobiotechnol

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Tumor-associated macrophages (TAMs) are a promising target for cancer immunotherapy, but delivering therapeutic agents to TAMs within the tumor microenvironment (TME) is challenging. In this study, a photosensitive, dual-targeting nanoparticle system (M.RGD@Cr-CTS-siYTHDF1 NPs) was developed. The structure includes a shell of DSPE-modified RGD peptides targeting integrin receptors on tumor cells and carboxymethyl mannose targeting CD206 receptors on macrophages, with a core of chitosan adsorbing m6A reading protein YTHDF1 siRNA and chromium nanoparticles (Cr NPs). The approach is specifically designed to target TAM and cancer cells, utilizing the photothermal effect of Cr NPs to disrupt the TME and deliver siYTHDF1 to TAM. In experiments with tumor-bearing mice, M.RGD@Cr-CTS-siYTHDF1 NPs, when exposed to laser irradiation, effectively killed tumor cells, disrupted the TME, delivered siYTHDF1 to TAMs, silenced the YTHDF1 gene, and shifted the STAT3-STAT1 equilibrium by reducing STAT3 and enhancing STAT1 expression. This reprogramming of TAMs towards an anti-tumor phenotype led to a pro-immunogenic TME state. The strategy also suppressed immunosuppressive IL-10 production, increased expression of immunostimulatory factors (IL-12 and IFN-γ), boosted CD8 + T cell infiltration and M1-type TAMs, and reduced Tregs and M2-type TAMs within the TME. In conclusion, the dual-targeting M.RGD@Cr-CTS-siYTHDF1 NPs, integrating dual-targeting capabilities with photothermal therapy (PTT) and RNA interference, offer a promising approach for molecular targeted cancer immunotherapy with potential for clinical application. Graphical Abstract

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Section: Resultssupporting

confidence: 93%

Section: Resultsmentioning

confidence: 99%

Photosensitive and dual-targeted chromium nanoparticle delivering small interfering RNA YTHDF1 for molecular-targeted immunotherapy in liver cancer

Chen,

He,

Huang

et al. 2024

J Nanobiotechnol

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“…As noted earlier, STAT1 mediates the effects of IFNs and is a key component of the innate immune system response to viral infections and other pathogens [217]. Activated STAT1 can promote cell cycle arrest, apoptosis, differentiation, and enhanced immune recognition [6]. It can also mediate antiangiogenic effects [218].…”

Section: Chemical Biology Approachesmentioning

confidence: 92%

“…A key mediator of this effect, both in making tumor cells more visible to immune cells and activating immune cell function, are IFNs [185,186]. JAK inhibitors will generally suppress IFN signaling (which also uses JAK1, JAK2, and TYK2) and thus suppress critical immune effects [6]. This has also limited the clinical applicability of JAK inhibitors in cancer therapy.…”

Section: Targeting Upstream Kinases: Stat Phosphorylation As a Biomar...mentioning

confidence: 99%

“…STAT tyrosine phosphorylation and nuclear translocation occur within seconds of cytokine stimulation. Reflecting the critical functions of target genes regulated by STATs, they are also inactivated very rapidly by a number of mechanisms, including protein tyrosine phosphatases (PTPs), protein inhibitors of activated STAT (PIAS), and suppressors of cytokine signaling proteins (SOCS) [6]. Nuclear PTPs can dephosphorylate STAT proteins, which leads to their inactivation and subsequent transport out of the nucleus [7].…”

Section: Introduction: Stat Transcription Factorsmentioning

confidence: 99%

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Oncogenic STAT Transcription Factors as Targets for Cancer Therapy: Innovative Strategies and Clinical Translation

Wang,

Lopez McDonald,

Hariprasad

et al. 2024

Cancers

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Despite advances in our understanding of molecular aspects of oncogenesis, cancer remains a leading cause of death. The malignant behavior of a cancer cell is driven by the inappropriate activation of transcription factors. In particular, signal transducers and activators of transcription (STATs), which regulate many critical cellular processes such as proliferation, apoptosis, and differentiation, are frequently activated inappropriately in a wide spectrum of human cancers. Multiple signaling pathways converge on the STATs, highlighting their importance in the development and progression of oncogenic diseases. STAT3 and STAT5 are two members of the STAT protein family that are the most frequently activated in cancers and can drive cancer pathogenesis directly. The development of inhibitors targeting STAT3 and STAT5 has been the subject of intense investigations in the last decade, although effective treatment options remain limited. In this review, we investigate the specific roles of STAT3 and STAT5 in normal physiology and cancer biology, discuss the opportunities and challenges in pharmacologically targeting STAT proteins and their upstream activators, and offer insights into novel therapeutic strategies to identify STAT inhibitors as cancer therapeutics.

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The co‐location of CD14+APOE+ cells and MMP7+ tumour cells contributed to worse immunotherapy response in non‐small cell lung cancer

Fan,

Xie,

Tang

et al. 2024

Clinical & Translational Med

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Intra‐tumour immune infiltration is a crucial determinant affecting immunotherapy response in non‐small cell lung cancer (NSCLC). However, its phenotype and related spatial structure have remained elusive. To overcome these restrictions, we undertook a comprehensive study comprising spatial transcriptomic (ST) data (28 712 spots from six samples). We identified two distinct intra‐tumour infiltration patterns: immune exclusion (characterised by myeloid cells) and immune activation (characterised by plasma cells). The immune exclusion and immune activation signatures showed adverse and favourable roles in NSCLC patients' survival, respectively. Notably, CD14+APOE+ cells were recognised as the main cell type in immune exclusion samples, with increased epithelial‒mesenchymal transition and decreased immune activities. The co‐location of CD14+APOE+ cells and MMP7+ tumour cells was observed in both ST and bulk transcriptomics data, validated by multiplex immunofluorescence performed on 20 NSCLC samples. The co‐location area exhibited the upregulation of proliferation‐related pathways and hypoxia activities. This co‐localisation inhibited T‐cell infiltration and the formation of tertiary lymphoid structures. Both CD14+APOE+ cells and MMP7+ tumour cells were associated with worse survival. In an immunotherapy cohort from the ORIENT‐3 clinical trial, NSCLC patients who responded unfavourably exhibited higher infiltration of CD14+APOE+ cells and MMP7+ tumour cells. Within the co‐location area, the MK, SEMA3 and Macrophage migration inhibitory factor (MIF) signalling pathway was most active in cell‒cell communication. This study identified immune exclusion and activation patterns in NSCLC and the co‐location of CD14+APOE+ cells and MMP7+ tumour cells as contributors to immune resistance.

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The complementary roles of STAT3 and STAT1 in cancer biology: insights into tumor pathogenesis and therapeutic strategies

Cited by 8 publications

References 111 publications

Photosensitive and dual-targeted chromium nanoparticle delivering small interfering RNA YTHDF1 for molecular-targeted immunotherapy in liver cancer

Photosensitive and dual-targeted chromium nanoparticle delivering small interfering RNA YTHDF1 for molecular-targeted immunotherapy in liver cancer

Oncogenic STAT Transcription Factors as Targets for Cancer Therapy: Innovative Strategies and Clinical Translation

The co‐location of CD14+APOE+ cells and MMP7+ tumour cells contributed to worse immunotherapy response in non‐small cell lung cancer

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