Remodeling the hepatic fibrotic microenvironment with emerging nanotherapeutics: a comprehensive review

Zhao, Xingtao; Amevor, Felix Kwame; Xue, Xinyan; Wang, Cheng; Cui, Zhifu; Dai, Shu-Ho; Peng, Cheng; Li, Yunxia

doi:10.1186/s12951-023-01876-5

Cited by 12 publications

(5 citation statements)

References 180 publications

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“…Flow cytometry analysis results of the sorted liver cells displayed that the percentage of nonparenchymal cells (mainly Kupffer cells) that internalized with siApoB (Cy5) was much higher than that of hepatocytes (6.13 vs 1.12%) (Figure D). Hepatocytes accounting for 60–70% of the total liver cells and Kupffer cells accounting for 10–15% of the total liver cells , are the major cells for the internalization of nanoparticles. , This indicates that approximately half of the BCP- siApoB can be taken up by hepatocytes and the other half by Kupffer cells. Besides, to study the distribution of BCP- siApoB (Cy5) in the liver, the tissue slices were stained with fluorescent dyes.…”

Section: Resultsmentioning

confidence: 99%

Bioresponsive Chimaeric Polymersomes Mediate Sustained and Liver-Specific siRNA Transfection In Vivo

Huang,

Wang,

et al. 2023

Biomacromolecules

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The silencing of disease-causing genes with small interfering RNA (siRNA) offers a particularly effective therapeutic strategy for different disorders; however, its clinical efficacy relies on the development of nontoxic and tissue-specific delivery vehicles. Herein, we report that bioresponsive chimaeric polymersomes (BCP) with short poly(ethylenimine) as inner shell mediate highly efficacious, sustained, and liver-specific siRNA transfection in vivo. BCP exhibited remarkable encapsulation efficiencies of siRNA (95–100%) at siRNA-feeding contents of 15–25 wt %, to afford stable, small-sized (55–64 nm), and neutral-charged BCP-siRNA. siApoB-Loaded BCP (BCP-siApoB) outperformed lipofectamine counterparts and silenced 93% of ApoB mRNA in HepG2 cells at 50 nM siApoB without inducing cytotoxicity. Intriguingly, the in vivo studies using wild-type C57BL/6 mice revealed that BCP-siApoB preferentially accumulated in the liver, and a single dose of 4.5 mg/kg achieved over 90% downregulation of ApoB mRNA for at least 10 days. The systemic administration of BCP-siApoB at 4.5 mg/kg every 2 weeks or 1.5 mg/kg weekly in diet-induced obese mice could also achieve up to 80% silencing of ApoB mRNA. The liver specificity and silencing efficacy of BCP-siApoB could further be improved by decorating it with the trivalent N-acetylgalactosamine (TriGalNAc) ligand. These bioresponsive and liver-specific chimaeric polymersomes provide an enabling technology for siRNA therapy of various liver-related diseases.

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Section: Resultsmentioning

confidence: 99%

Bioresponsive Chimaeric Polymersomes Mediate Sustained and Liver-Specific siRNA Transfection In Vivo

Huang,

Wang,

et al. 2023

Biomacromolecules

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“…They are irregular in shape and often extend several stellate processes around the hepatic sinusoids. HSCs can secrete chemokines, cytokines, growth factors, or proteases, which promote tumor growth, metastasis, angiogenesis, and immune escape, and are considered liver-specific pericytes (69)(70)(71)(72). Ming Qi et al found that in the CRCLM models of bevacizumab resistance, the HSCs around the co-option vessels had a high expression of fibroblast activation protein a (FAPa).…”

Section: Hepatic Stellate Cellsmentioning

confidence: 99%

Vessel co-option: a unique vascular-immune niche in liver cancer

Yang,

Dang,

Wang

et al. 2024

Front. Oncol.

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Tumor vasculature is pivotal in regulating tumor perfusion, immune cell infiltration, metastasis, and invasion. The vascular status of the tumor is intricately linked to its immune landscape and response to immunotherapy. Vessel co-option means that tumor tissue adeptly exploits pre-existing blood vessels in the para-carcinoma region to foster its growth rather than inducing angiogenesis. It emerges as a significant mechanism contributing to anti-angiogenic therapy resistance. Different from angiogenic tumors, vessel co-option presents a distinctive vascular-immune niche characterized by varying states and distribution of immune cells, including T-cells, tumor-associated macrophages, neutrophils, and hepatic stellate cells. This unique composition contributes to an immunosuppressive tumor microenvironment that is crucial in modulating the response to cancer immunotherapy. In this review, we systematically reviewed the evidence and molecular mechanisms of vessel co-option in liver cancer, while also exploring its implications for anti-angiogenic drug resistance and the immune microenvironment, to provide new ideas and clues for screening patients with liver cancer who are effective in immunotherapy.

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“…It highlights these cytokines as potential therapeutic targets for mitigating ballooning and its detrimental consequences. Understanding these inflammatory mediators and their interconnected pathways is crucial for unraveling the complexities of NASH and advancing targeted treatment strategies [ 44 ].…”

Section: Reviewmentioning

confidence: 99%

Hepatocytic Ballooning in Non-alcoholic Steatohepatitis: Bridging the Knowledge Gap and Charting Future Avenues

Singla,

Muneshwar,

Pathade

et al. 2023

Cureus

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Non-alcoholic steatohepatitis (NASH) is emerging as a significant global health concern, characterized by hepatic lipid accumulation, inflammation, and hepatocellular injury. Hepatocytic ballooning, a histological feature of NASH, has gained prominence for its role in disease progression and potential as a therapeutic target. This review provides an overview of the current knowledge regarding hepatocytic ballooning in NASH, highlighting the key molecular and cellular mechanisms implicated in its development. We delve into the intricate interplay of metabolic dysregulation, oxidative stress, and lipid toxicity as drivers of hepatocytic ballooning, shedding light on the pathways responsible for its initiation and perpetuation. Furthermore, we explore the diagnostic challenges associated with hepatocytic ballooning and its significance as a prognostic indicator in NASH patients. While hepatocytic ballooning holds promise as a therapeutic target, this abstract discusses the various experimental and clinical approaches to ameliorate this histological hallmark. Potential interventions, including lifestyle modifications, pharmacological agents, and emerging therapies, are evaluated in terms of their efficacy and safety profiles. In conclusion, this review underscores the need to bridge the knowledge gap surrounding hepatocytic ballooning in NASH and emphasizes its importance in understanding disease pathogenesis and progression. By charting future research avenues and clinical strategies, we aspire to advance our comprehension of NASH and ultimately improve patient outcomes in this rapidly evolving field of hepatology.

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Remodeling the hepatic fibrotic microenvironment with emerging nanotherapeutics: a comprehensive review

Cited by 12 publications

References 180 publications

Bioresponsive Chimaeric Polymersomes Mediate Sustained and Liver-Specific siRNA Transfection In Vivo

Bioresponsive Chimaeric Polymersomes Mediate Sustained and Liver-Specific siRNA Transfection In Vivo

Vessel co-option: a unique vascular-immune niche in liver cancer

Hepatocytic Ballooning in Non-alcoholic Steatohepatitis: Bridging the Knowledge Gap and Charting Future Avenues

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