Liver cancer heterogeneity modeled by in situ genome editing of hepatocytes

Tang, Mei; Zhao, Yang; Zhao, Jianhui; Wei, Shumei; Liu, Mingwei; Zheng, Nairen; Geng, Didi; Han, Shixun; Zhang, Yuchao; Zhong, Guoxuan; Li, Shuaifeng; Zhang, Xiuming; Wang, Chenliang; Yan, Huan; Cao, Xiaolei; Li, Li; Bai, Xueli; Ji, Junfang; Feng, Xin‐Hua; Qin, Jun; Liang, Tingbo; Zhao, Bin

doi:10.1126/sciadv.abn5683

Cited by 28 publications

(29 citation statements)

References 81 publications

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“…The concept of tumor heterogeneity leading to a low immune response to tumors is important in clinical evaluation [ 259 ]. Intertumor or intratumor heterogeneity is thought to be an impediment to tumor targeted therapy [ 260 ]. Tumor heterogeneity and cancer stem cell plasticity are linked, and it is thought to be an emerging marker related to cancer invasion [ 261 ].…”

Section: Immune Checkpoint-targeted Immunotherapy For Cscsmentioning

confidence: 99%

Cross-talk between cancer stem cells and immune cells: potential therapeutic targets in the tumor immune microenvironment

Xiang

Jiang

et al. 2023

Mol Cancer

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Ongoing research has revealed that the existence of cancer stem cells (CSCs) is one of the biggest obstacles in the current cancer therapy. CSCs make an influential function in tumor progression, recurrence and chemoresistance due to their typical stemness characteristics. CSCs are preferentially distributed in niches, and those niche sites exhibit characteristics typical of the tumor microenvironment (TME). The complex interactions between CSCs and TME illustrate these synergistic effects. The phenotypic heterogeneity within CSCs and the spatial interactions with the surrounding tumor microenvironment led to increased therapeutic challenges. CSCs interact with immune cells to protect themselves against immune clearance by exploiting the immunosuppressive function of multiple immune checkpoint molecules. CSCs also can protect themselves against immune surveillance by excreting extracellular vesicles (EVs), growth factors, metabolites and cytokines into the TME, thereby modulating the composition of the TME. Therefore, these interactions are also being considered for the therapeutic development of anti-tumor agents. We discuss here the immune molecular mechanisms of CSCs and comprehensively review the interplay between CSCs and the immune system. Thus, studies on this topic seem to provide novel ideas for reinvigorating therapeutic approaches to cancer.

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Section: Immune Checkpoint-targeted Immunotherapy For Cscsmentioning

confidence: 99%

Cross-talk between cancer stem cells and immune cells: potential therapeutic targets in the tumor immune microenvironment

Xiang

Jiang

et al. 2023

Mol Cancer

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“…Hepatocellular carcinoma (HCC) and intrahepatic cholangiocarcinoma (ICC) are the two major subtypes of primary liver cancers (PLCs) [ 1 ]. The HCC accounts for up to 85%, while the ICC accounts for 10 to 15% of all PLC cases [ 2 ]. Although some early-stage PLC patients can benefit from surgical treatment and systematic anti-tumor therapies, including target therapy and immunotherapy, those with advanced stage can only receive limited benefits from few multi-kinase inhibitors [ 2 , 3 ].…”

Section: Introductionmentioning

confidence: 99%

“…The HCC accounts for up to 85%, while the ICC accounts for 10 to 15% of all PLC cases [ 2 ]. Although some early-stage PLC patients can benefit from surgical treatment and systematic anti-tumor therapies, including target therapy and immunotherapy, those with advanced stage can only receive limited benefits from few multi-kinase inhibitors [ 2 , 3 ]. Currently, immunotherapeutic strategies, such as tumor vaccines, adoptive T-cell transfer therapy, immune-checkpoint inhibitors, and even immunotherapeutic strategies combined with conventional strategies, have been increasingly investigated in managing HCC and ICC.…”

Section: Introductionmentioning

confidence: 99%

Prognostic values of tissue-resident CD8+T cells in human hepatocellular carcinoma and intrahepatic cholangiocarcinoma

Chen

Huang

et al. 2023

World J Surg Onc

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Background Tissue-resident CD8+T cells (CD103+CD8+T cells) are the essential effector cell population of anti-tumor immune response in tissue regional immunity. And we have reported that IL-33 can promote the proliferation and effector function of tissue-resident CD103+CD8+T cells. As of now, the immunolocalization and the prognostic values of tissue-resident CD8+T cells in human hepatocellular carcinoma (HCC) and intrahepatic cholangiocarcinoma (ICC) still remain to be illustrated. Methods In our present study, we used the tissue microarrays of HCC and ICC, the multicolor immunohistochemistry (mIHC), and imaging analysis to characterize the tissue-resident CD8+T cells in HCC and ICC tissues. The prognostic values and clinical associations were also analyzed. We also studied the biological functions and the cell–cell communication between tumor-infiltrating CD103+CD8+T cells and other cell types in HCC and ICC based on the published single-cell RNA sequencing (scRNA-seq) data. Results Our work unveiled the expressions of CD8 and CD103 and immunolocalization of tissue-resident CD8+T cells in human HCC and ICC. Elevated CD8+T cells indicated a better overall survival (OS) rate, implying that tumor-infiltrating CD8+T cells in HCC and ICC could serve as an independent prognostic factor. Moreover, the number of CD103+CD8+T cells was increased in HCC and ICC tissues compared with adjacent normal tissues. HCC patients defined as CD8highCD103high had a better OS, and the CD8lowCD103low group tended to have a poorer prognosis in ICC. Evaluation of the CD103+CD8+T-cell ratio in CD8+T cells could also be a prognostic predictor for HCC and ICC patients. A higher ratio of CD103+CD8+T cells over total CD8+T cells in HCC tissues was negatively and significantly associated with the advanced pathological stage. The percentage of higher numbers of CD103+CD8+T cells in ICC tissues was negatively and significantly associated with the advanced pathological stage. In contrast, the higher ratio of CD103+CD8+T cells over total CD8+T cells in ICC tissues was negatively and significantly associated with the advanced pathological stage. In addition, single-cell transcriptomics revealed that CD103+CD8+T cells were enriched in genes associated with T-cell activation, proliferation, cytokine function, and T-cell exhaustion. Conclusion The CD103+ tumor-specific T cells signified an important prognostic marker with improved OS, and the evaluation of the tissue-resident CD103+CD8+T cells might be helpful in assessing the on-treatment response of liver cancer.

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“…[ 3,8–14 ] Owing to the low κ of organic TE materials and the difficulty to measure correctly, the power factor (PF = α 2 σ) is often used to evaluate their TE performance. [ 9,15–18 ] Recently, extensive studies on TE material design, fundamentals in charge generation/transport, and optimization of device architectures have been performed, successfully demonstrating a record high ZT up to 0.75 for poly(3,4‐ethylenedioxythiophene):polystyrene sulfonate (PEDOT:PSS)/ionic liquid (IL) heterostructures. [ 19 ] The enhancement of ZT is attributed to only a slight drop in σ and a significant rise in α due to ion accumulation of IL on the polymer surface which can scatter the low energy charge carriers and thus increase the mean energy of the holes at the cold side of the PEDOT:PSS films.…”

Section: Introductionmentioning

confidence: 99%

Remarkably High Conductivity and Power Factor in D–D′‐type Thermoelectric Polymers Based on Indacenodithiophene

Tripathi

Seo

Kim

et al. 2022

Adv Elect Materials

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Three p‐type thermoelectric (TE) polymers based on the indacenodithiophene moiety substituted with bis(alkylsulfanyl)methylene side‐chains (IDTS) are synthesized. The TE characteristics of IDTS‐based donor–donor’ (D–D′) type PIDTSDTTT and donor–acceptor (D–A) type polymers, PIDTSBT and PIDTS2FBT are investigated. Remarkably higher electrical conductivity (σ = ≈1000 S cm−1) and power factor (PF = ≈120 μW m−1 K−2) by doping with AuCl3 are measured for PIDTSDTTT compared to D–A type polymers. The higher σ of PIDTSDTTT originates from its higher carrier concentration compared to those of PIDTSBT and PIDTS2FBT. Moreover, the facile polaron‐to‐bipolaron transition is measured, and the charge carriers are calculated to be more stable with extended delocalization in PIDTSDTTT compared to D–A polymers. The significantly higher doping stability in PIDTSDTTT can be explained in terms of the higher conduction band of bipolarons than the valence band of O2 and H2O, which blocks the facile reduction of bipolarons in air. The energetic structures of doped polaron and bipolaron states, as well as pristine TE polymers, must be carefully considered to realize efficient and stable p‐type thermoelectric polymers, where a D–D′ type structure with further enhanced carrier mobility can be considered as a potential molecular framework.

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Liver cancer heterogeneity modeled by in situ genome editing of hepatocytes

Cited by 28 publications

References 81 publications

Cross-talk between cancer stem cells and immune cells: potential therapeutic targets in the tumor immune microenvironment

Cross-talk between cancer stem cells and immune cells: potential therapeutic targets in the tumor immune microenvironment

Prognostic values of tissue-resident CD8+T cells in human hepatocellular carcinoma and intrahepatic cholangiocarcinoma

Remarkably High Conductivity and Power Factor in D–D′‐type Thermoelectric Polymers Based on Indacenodithiophene

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