Your search keyword '"drug delivery"' showing total 4,296 results

1. Dual immunostimulatory CD73 antibody-polymeric cytotoxic drug complex for triple negative breast cancer therapy.

Author

Xie, Xiao, Yang, Ming, Wei, Xue, Chu, Hongyu, Zhao, Weidong, and Shen, Na

Abstract

Treatment of triple-negative breast cancer (TNBC) poses significant challenges due to its propensity for metastasis. A key impediment lies in the suppressive immune microenvironment, which fosters tumor progression. This study introduces an approach employing a dual immune-stimulatory CD73 antibody-polymeric cytotoxic drug complex (αCD73-PLG-MMAE). This complex is designed for targeted eradication of TNBC while modulating tumor immunity through mechanisms such as immunogenic cell death (ICD) and interference with the adenosine signaling pathway. By enhancing antitumor immune responses, this strategy offers a highly effective means of treating TNBC and mitigating metastasis. The complex is synthesized by combining αCD73 with poly(L -glutamic acid) (PLG) grafted Fc binding peptides (Fc-III-4C) and Val-Cit-PAB-monomethyl auristatin E (MMAE), exploiting the affinity between αCD73 and Fc-III-4C. αCD73 selectively targets CD73 molecules on both tumor and immune suppressive cells, thereby inhibiting the adenosine pathway. Meanwhile, Val-Cit-PAB-MMAE, activated by cathepsin B, triggers selective release of MMAE, inducing ICD in tumor cells. In a 4T1 tumor model, αCD73-PLG-MMAE significantly enhances drug accumulation in tumors by 4.13-fold compared to IgG-PLG-MMAE, leading to suppression of tumor growth and metastasis. Furthermore, it synergistically augments the antitumor effects of αPD-1, resulting in a tumor inhibition rate of 92 % as compared to 21 % with αPD-1 alone. This study thus presents a pioneering therapeutic strategy for TNBC, emphasizing the potential of targeted immunomodulation in cancer treatment. Antibody-drug conjugate (ADC) therapy holds promise for treating triple-negative breast cancer (TNBC). However, the current ADC, sacituzumab govitecan, fails to overcome the crucial role of adenosine in the suppressive immune microenvironment characteristic of this "cold tumor". Here, we present a dual immune-stimulatory complex, αCD73-PLG-MMAE, which targets TNBC specifically and modulates tumor immunity through mechanisms such as immunogenic cell death (ICD) and interference with the adenosine signaling pathway. Thus, it kills tumor cells with cytotoxic drugs, comprehensively regulates immunosuppression, and restores a durable immune response. This study proposes an antibody-polymeric drug complex with immunomodulatory and immunoagonist roles, offering new insights into TNBC treatment. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

2. Synthesis, characterization, and surface modification of degradable polar hydrophobic ionic polyurethane nanoparticles for the delivery of therapeutics to vascular tissue.

Author

Trepanier, Chantal M., Rubianto, Jonathan, Burke-Kleinman, Jonah, Appings, Ryan, Bendeck, Michelle P., and Santerre, J. Paul

Subjects

TRANSLUMINAL angioplasty, NANOPARTICLES, DRUG stability, PEPTIDES, SURFACE charges

Abstract

Degradable polar hydrophobic ionic polyurethanes (D-PHI) are an emerging class of biomaterials with particular significance for blood-contacting applications due to their immunomodulatory effects and highly customizable block chemistry. In this manuscript, D-PHI polymer was formulated as a nanoparticle excipient for the first time by inverse emulsion polymerization. The nanoparticles were optimized with consideration of diameter, surface charge, size variability, and yield as a delivery vehicle for a custom vascular therapeutic peptide. A layer-by-layer (LBL) surface modification technique using poly-L-lysine was integrated within the nanoparticle design to optimize therapeutic loading efficiency. Solvent pH played a pivotal role in emulsion micelle formation, LBL polymer secondary structure, and the polymer functional group interactions critical for high therapeutic loading. The resulting nanoparticle platform met target size (200 ± 20 nm), polydispersity (<0.07), and storage stability standards, was nontoxic, and did not affect therapeutic peptide bioactivity in vitro. Surface-modified D-PHI nanoparticles can be reproducibly manufactured at low cost, generating a highly customizable excipient platform suitable for delivery of biomolecular therapeutics. These nanoparticles have potential applications in vascular drug delivery via localized infusion, drug eluting stents, and drug-coated angioplasty balloons. Nanoscale excipients have become critical in the delivery of many therapeutics to enhance drug stability and targeted biodistribution through careful design of nanoparticle composition, surface chemistry, and size. This manuscript describes the development of a nanoparticle excipient derived from an immunomodulatory degradable polar hydrophobic ionic polyurethane, in combination with a layer-by-layer surface modification approach utilizing poly-L-lysine, to transport a mimetic peptide targeting smooth muscle cell migration in vascular disease. The nanoparticle platform draws on the effect of pH to maximize drug loading and tailor particle properties. The low cost and easily reproducible system presents a highly customizable platform that can be adapted for therapeutic delivery across a wide range of clinical indications. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

3. Mussel-inspired adhesive drug-loaded hydrogels for oral ulcers treatment.

Author

Wang, Zhongchao, Han, Xiao, Xiao, Weiwei, Wang, Pin, Wang, Jinghan, Zou, Dan, Luo, Xiao, Shi, Liang, Wu, Jiaqi, Guo, Ling, Mu, Yandong, Lu, Bingyang, and Fan, Liyuan

Subjects

DRUG bioavailability, DRUG accessibility, CHLORHEXIDINE, TREATMENT effectiveness, CANKER sores

Abstract

Oral aphthous ulcers are common mucosal lesions that cause pain and discomfort. There are diverse biomaterials and drug treatments for oral ulcers used in both research and clinical settings. However, the complex oral environment often results in low adhesion and short drug retention times, which lead to poor drug availability and treatment outcomes. In this study, a mussel-inspired adhesive hydrogel was developed by grafting catechol onto hyaluronic acid (C-HA), and dopamine was added for oxidative pre-polymerization to form modified hyaluronic acid (M-HA), which remarkably increased the adhesion of the hydrogels. Then, M-HA was interpenetrated into the gelatin methacryloyl (GelMA) network. Chlorhexidine gluconate (CHG) was then incorporated into the hydrogel to enhance its availability and therapeutic effect through its sustained-release capability. The GelMA/M-HA hydrogel demonstrated strong adhesion to wet tissues, antibacterial and anti-inflammatory properties, and good biocompatibility. In both rat oral ulcers and infected wounds, the adhesive hydrogel significantly accelerated the healing of the ulcers and infected wounds. These results indicated that this adhesive hydrogel offers a promising new strategy for the treatment of oral ulcers in clinical practice. Oral ulcers are a common and high-incidence mucosal condition that seriously affect people's daily lives, often making it difficult for patients to chew and speak. However, a dynamic oral environment with various types of bacteria influences drug availability and treatment effects in clinical settings. To address this challenge, an adhesive, mussel-inspired, drug-loaded hydrogel was constructed using natural macromolecules (hyaluronic acid and gelatin) with good biocompatibility. Chlorhexidine gluconate (CHG), with its broad-spectrum antibacterial activity, has been incorporated to synergistically promote oral ulcer healing. The splendid adhesion, antibacterial, and therapeutic effects of this hydrogel demonstrated a new strategy for treating oral ulcers. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

4. Collagen patches releasing phosphatidylserine liposomes guide M1-to-M2 macrophage polarization and accelerate simultaneous bone and muscle healing.

Author

Toita, Riki, Shimizu, Yuki, Shimizu, Eiko, Deguchi, Tomonori, Tsuchiya, Akira, Kang, Jeong-Hun, Kitamura, Masahiro, Kato, Atsushi, Yamada, Hideto, Yamaguchi, Shogo, and Kasahara, Shinjiro

Subjects

TYPE I interferons, PHOSPHATIDYLSERINES, MUSCULOSKELETAL system injuries, NUCLEOTIDE sequencing, PHENOTYPIC plasticity

Abstract

Bilateral communication between bones and muscles is essential for healing composite bone–muscle injuries from orthopedic surgeries and trauma. However, these injuries are often characterized by exaggerated inflammation, which can disrupt bone–muscle crosstalk, thereby seriously delaying the healing of either tissue. Existing approaches are largely effective at healing single tissues. However, simultaneous healing of multiple tissues remains challenging, with little research conducted to date. Here we introduce collagen patches that overcome this overlooked issue by harnessing the plasticity of macrophage phenotypes. Phosphatidylserine liposomes (PSLs) capable of shifting the macrophage phenotype from inflammatory M1 into anti-inflammatory/prohealing M2 were coated on collagen patches via a layer-by-layer method. Original collagen patches failed to improve tissue healing under inflammatory conditions coordinated by M1 macrophages. In contrast, PSL-coated collagen patches succeeded in accelerating bone and muscle healing by inducing a microenvironment dominated by M2 macrophages. In cell experiments, differentiation of preosteoblasts and myoblasts was completely inhibited by secretions of M1 macrophages but unaffected by those of M2 macrophages. RNA-seq analysis revealed that type I interferon and interleukin-6 signaling pathways were commonly upregulated in preosteoblasts and myoblasts upon stimulation with M1 macrophage secretions, thereby compromising their differentiation. This study demonstrates the benefit of PSL-mediated M1-to-M2 macrophage polarization for simultaneous bone and muscle healing, offering a potential strategy toward simultaneous regeneration of multiple tissues. Existing approaches for tissue regeneration, which primarily utilize growth factors, have been largely effective at healing single tissues. However, simultaneous healing of multiple tissues remains challenging and has been little studied. Here we demonstrate that collagen patches releasing phosphatidylserine liposomes (PSLs) promote M1-to-M2 macrophage polarization and are effective for simultaneous healing of bone and muscle. Transcriptome analysis using next-generation sequencing reveals that differentiation of preosteoblasts and myoblasts is inhibited by the secretions of M1 macrophages but promoted by those of M2 macrophages, highlighting the importance of timely regulation of M1-to-M2 polarization in tissue regeneration. These findings provide new insight to tissue healing of multiple tissues. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

5. A comprehensive review on modeling aspects of infusion-based drug delivery in the brain.

Author

Yuan, Tian, Zhan, Wenbo, Terzano, Michele, Holzapfel, Gerhard A., and Dini, Daniele

Subjects

SOLID mechanics, FINITE element method, FLUID mechanics, BRAIN diseases, DRUG interactions, BIOMATERIALS

Abstract

[Display omitted] Brain disorders represent an ever-increasing health challenge worldwide. While conventional drug therapies are less effective due to the presence of the blood-brain barrier, infusion-based methods of drug delivery to the brain represent a promising option. Since these methods are mechanically controlled and involve multiple physical phases ranging from the neural and molecular scales to the brain scale, highly efficient and precise delivery procedures can significantly benefit from a comprehensive understanding of drug-brain and device-brain interactions. Behind these interactions are principles of biophysics and biomechanics that can be described and captured using mathematical models. Although biomechanics and biophysics have received considerable attention, a comprehensive mechanistic model for modeling infusion-based drug delivery in the brain has yet to be developed. Therefore, this article reviews the state-of-the-art mechanistic studies that can support the development of next-generation models for infusion-based brain drug delivery from the perspective of fluid mechanics, solid mechanics, and mathematical modeling. The supporting techniques and database are also summarized to provide further insights. Finally, the challenges are highlighted and perspectives on future research directions are provided. Despite the immense potential of infusion-based drug delivery methods for bypassing the blood-brain barrier and efficiently delivering drugs to the brain, achieving optimal drug distribution remains a significant challenge. This is primarily due to our limited understanding of the complex interactions between drugs and the brain that are governed by principles of biophysics and biomechanics, and can be described using mathematical models. This article provides a comprehensive review of state-of-the-art mechanistic studies that can help to unravel the mechanism of drug transport in the brain across the scales, which underpins the development of next-generation models for infusion-based brain drug delivery. More broadly, this review will serve as a starting point for developing more effective treatments for brain diseases and mechanistic models that can be used to study other soft tissue and biomaterials. [ABSTRACT FROM AUTHOR]

Published

2024

6. Green fabrication techniques for graphene and graphene nanocomposites—state-of-the-art and modern prospects.

Author

Kausar, Ayesha and Ahmad, Ishaq

Abstract

Graphene is a unique nanocarbon nanostructure which is commonly used to form the nanocomposites. Green strategies (chemical vapour deposition with green catalysts, mechanical exfoliation, sonication) and sustainable carbon sources (plant extracts and recycled polymers) have been applied to synthesise graphene and graphene derivatives. For the formation of graphene nanocomposites, green fabrication methods (sonication, solution route, electrostatic, in situ polymerisation, printing, hydrothermal, etc.) involving green matrices, nanofillers, solvents, and reagents, have also been investigated. Thus, this state-of-the-art overview highlights essential green methods for the formation of graphene and nanomaterials. The resulting green graphene nanocomposites have numerous superior structural and physical properties such as morphology, electrical conductivity, thermal conductivity, thermal stability, and mechanical stability. Subsequently, the green synthesised graphene and graphene nanocomposites have been explored for important high performance technical applications including the energy storage, packaging, antibacterial, bioimaging, and drug delivery applications. Future research on the development of advanced synthesis methods may overcome the design and performance challenges of the green graphene nanocomposites. [ABSTRACT FROM AUTHOR]

Published

2024

7. Albuterol Delivery via In-Line Intrapulmonary Percussive Ventilation Superimposed on Invasive Ventilation in an Adult Lung Model.

Author

Takashi Karashima, Yuka Mimura-Kimura, and Yusuke Mimura

Subjects

BIOLOGICAL models, CONTINUING education units, DATA analysis, RESEARCH funding, POSITIVE pressure ventilation, DRUG delivery systems, TREATMENT effectiveness, DESCRIPTIVE statistics, ARTIFICIAL respiration, NEBULIZERS & vaporizers, ONE-way analysis of variance, STATISTICS, ALBUTEROL, DATA analysis software, MECHANICAL ventilators, SPECTROPHOTOMETRY, ADULTS

Abstract

BACKGROUND: Intrapulmonary percussive ventilation (IPV) is frequently used for airway clearance, together with delivery of aerosolized medications. Drug delivery via IPV alone increases with decreasing percussion frequency and correlates with tidal volume (VT), whereas drug delivery via IPV during invasive ventilation is not well characterized. We hypothesized that drug delivery via IPV-invasive ventilation would differ from IPV alone due to control of ventilation by invasive ventilation. METHODS: An adult ventilator circuit was used for IPV-invasive ventilation. A normal or a diseased lung model was configured to airway resistance of 5 cm H2O/L/s and lung compliance of 100 mL/cm H2O or to airway resistance of 20 cm H2O/L/s and lung compliance of 50 mL/cm H2O, respectively. The ventilator settings were the following: pressure control continuous mandatory ventilation mode, 10 breaths/min; PEEP, 5 cm H2O; ..., 0.21; inspiratory time, 1 s; no bias flow; and inspiratory pressure, 10 or 15 cm H2O for the normal or the diseased lung model, respectively, to reach VT 500 mL with IPV off. Albuterol nebulized from an IPV device was captured in a filter placed before the lung model and quantitated by spectrophotometry. RESULTS: The maximum efficiency of albuterol delivery via IPV-invasive ventilation was not different from that via IPV alone (mean ± SD of loading dose, 3.7 ± 0.2% vs 4.2 ± 0.3%, respectively; P = .12). The mean ± SD albuterol delivery efficiency with IPV-invasive ventilation was lower for the diseased lung model versus the normal model (1.6 ± 0.3% vs 3.2 ± 0.5%; P < .001), which increased with decreasing percussion frequency. In contrast, the mean ± SD was lower for the normal lung model versus the diseased model (401 ± 14 mL vs 470 ± 11 mL; P < .001). CONCLUSIONS: Albuterol delivery via IPV-invasive ventilation was modulated by percussion frequency but was not increased with increasing VT. The delivery efficiency was not sufficiently high for clinical use, in part due to nebulizer retention and extrapulmonary deposition. [ABSTRACT FROM AUTHOR]

Published

2024

8. A matrix metalloproteinase-responsive hydrogel system controls angiogenic peptide release for repair of cerebral ischemia/reperfusion injury.

Author

Qi Liu, Jianye Xie, Runxue Zhou, Jin Deng, Weihong Nie, Shuwei Sun, Haiping Wang, and Chunying Shi

Published

2025

9. Characterization of cellular uptake, anti-colorectal cancer effects and pharmacokinetics of curcumin-loaded polypropylene/rice husk composites filled with nano-SiO2.

Author

Yu, Miao, Li, Quanhui, and Yu, Hualong

Subjects

HEAT release rates, COLON cancer, ORAL drug administration, FLEXURAL modulus, RICE hulls, CURCUMIN

Abstract

Curcumin-loaded polypropylene/rice husk/SiO 2 composites were fabricated with tunable nano-SiO 2 filler loadings (0–10 wt%) via melt-blending and injection molding. XRD analysis revealed effective intercalation of nanoparticles and interaction with the polymer chains up to 6 wt% loading. Incorporation of SiO 2 fillers significantly enhanced mechanical strength with 6 % nano-SiO 2 formulation demonstrating 27 % higher tensile strength, 52 % increased flexural modulus and 51 % greater impact resistance. The silica nanoparticles also reduced heat release rate through protective charring and decreased moisture absorption by over 8 % due to hydrophilic surface groups. In vitro studies showed that curcumin nano-composites with 6 % nano-SiO 2 exhibited maximal cytotoxicity against HT-29 and HCT-116 colon cancer cells with CC50 values of 12.4±1.1 μg/ml and 10.3±0.9 μg/ml respectively, attributed to optimal drug release profile. The formulation arrested 22.1% cells in sub-G1 phase inducing apoptosis. Oral administration in tumor-bearing mice led to 3-fold increase in plasma exposure (Cmax 186±14 ng/ml) and relative bioavailability versus free curcumin, indicating capacity to evade presystemic clearance. The composites also enabled 3 times higher tumor accumulation highlighting potential for targeted colorectal cancer therapy via improved pharmacokinetics and site-specific action. Overall, precise tuning of nanostructured fillers augments mechanical and transport properties while potentiating anticancer performance. [ABSTRACT FROM AUTHOR]

Published

2024

10. Engineered nanoparticles for precise targeted drug delivery and enhanced therapeutic efficacy in cancer immunotherapy.

Author

Peng, Xueqiang, Fang, Jianjun, Lou, Chuyuan, Yang, Liang, Shan, Shaobo, Wang, Zixian, Chen, Yutong, Li, Hangyu, and Li, Xuexin

Subjects

DRUG delivery systems, TARGETED drug delivery, TREATMENT effectiveness, IMMUNE response, CANCER cells

Abstract

The advent of cancer immunotherapy has imparted a transformative impact on cancer treatment paradigms by harnessing the power of the immune system. However, the challenge of practical and precise targeting of malignant cells persists. To address this, engineered nanoparticles (NPs) have emerged as a promising solution for enhancing targeted drug delivery in immunotherapeutic interventions, owing to their small size, low immunogenicity, and ease of surface modification. This comprehensive review delves into contemporary research at the nexus of NP engineering and immunotherapy, encompassing an extensive spectrum of NP morphologies and strategies tailored toward optimizing tumor targeting and augmenting therapeutic effectiveness. Moreover, it underscores the mechanisms that NPs leverage to bypass the numerous obstacles encountered in immunotherapeutic regimens and probes into the combined potential of NPs when co-administered with both established and novel immunotherapeutic modalities. Finally, the review evaluates the existing limitations of NPs as drug delivery platforms in immunotherapy, which could shape the path for future advancements in this promising field. This paper reviews recent advances in various nanoparticle-enhanced tumor immunotherapy strategies as delivery vehicles for immune agents. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

11. External Jet Nebulization and Measured Ventilator Performance.

Author

Jayakumaran, Jeyanthan, Smaldone, Gerald C., and Cuccia, Ann D.

Subjects

ARTIFICIAL respiration equipment, RESPIRATORY muscle physiology, CONTINUING education units, PRODUCT design, RESPIRATION, BIOSENSORS, DESCRIPTIVE statistics, SIMULATION methods in education, NEBULIZERS & vaporizers, RESPIRATORY measurements, PATIENT monitoring, MECHANICAL ventilators, RESPIRATORY mechanics

Abstract

BACKGROUND: During invasive ventilation, external flow jet nebulization results in increases in displayed exhaled tidal volumes (VT). We hypothesized that the magnitude of the increase is inaccurate. An ASL 5000 simulator measured ventilatory parameters over a wide range of adult settings: actual VT, peak inspiratory pressure (PIP), and time to minimum pressure. METHODS: Ventilators with internal and external flow sensors were tested by using a variety of volume and pressure control modes (the target VT was 420 mL). Patient conditions (normal, COPD, ARDS) defined on the ASL 5000 were assessed at baseline and with 3.5 or 8 L/min of added external flow. Patient-triggering was assessed by reducing muscle effort to the level that resulted in backup ventilation and by changing ventilator sensitivity to the point of auto-triggering. RESULTS: Results are reported as percentage change from baseline after addition of 3.5 or 8 L/min external flow. For ventilators with internal flow sensors, changes in displayed exhaled VT ranged from 10% to 118%, however, when using volume control, actual increases in actual VT and PIP were only 4%-21% (P = .063, .031) and 6%-24% (P = .25, .031), respectively. Changes in actual correlated closely with changes in PIP (P < .001; R² = 0.68). For pressure control, actual decreased by 3%-5% (P = .031) and 4%-9% (P = .031) with 3.5 and 8 L/min respectively, PIP was unchanged. With external flow sensors at the distal Y-piece junction, volume and pressure changes were statistically insignificant. The time to minimum pressure increased at most by 8% (P = .02) across all modes and ventilators. The effects on muscle pressure were minimal (-1 cm H2O), and ventilator sensitivity effects were nearly undetectable. CONCLUSIONS: External flow jet nebulization resulted in much smaller changes in volume than indicated by the ventilator display. Statistically significant effects were confined primarily to machines with internal flow sensors. Differences approached the manufacturer-reported variation in ventilator baseline performance. During nebulizer therapy, effects on VT can be estimated at the bedside by monitoring PIP. [ABSTRACT FROM AUTHOR]

Published

2024

12. Complications and comorbidities associated with antineoplastic chemotherapy: Rethinking drug design and delivery for anticancer therapy.

Author

Mao, Xiaoman, Wu, Shuang, Huang, Dandan, and Li, Chong

Subjects

DRUG design, CANCER chemotherapy, COMORBIDITY, OLDER people, TARGETED drug delivery, ANIMAL models in research, XENOGRAFTS

Abstract

Despite the considerable advancements in chemotherapy as a cornerstone modality in cancer treatment, the prevalence of complications and pre-existing diseases is on the rise among cancer patients along with prolonged survival and aging population. The relationships between these disorders and cancer are intricate, bearing significant influence on the survival and quality of life of individuals with cancer and presenting challenges for the prognosis and outcomes of malignancies. Herein, we review the prevailing complications and comorbidities that often accompany chemotherapy and summarize the lessons to learn from inadequate research and management of this scenario, with an emphasis on possible strategies for reducing potential complications and alleviating comorbidities, as well as an overview of current preclinical cancer models and practical advice for establishing bio-faithful preclinical models in such complex context. The prevailing complications and comorbidities associated with chemotherapy are overviewed in this work, with an emphasis on crucial lessons to learn for improved management of both conditions. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

13. Beta cyclodextrin conjugated Au[sbnd]Fe3O4 Janus nanoparticles with enhanced chemo-photothermal therapy performance.

Author

Park, Sumin, Choi, Jaeyeop, Ko, Namsuk, Mondal, Sudip, Pal, Umapada, Lee, Byeong-Il, and Oh, Junghwan

Subjects

JANUS particles, REACTIVE oxygen species, IRON oxides, CYCLODEXTRINS, TREATMENT effectiveness, PHOTOTHERMAL conversion, IRON oxide nanoparticles, SELF-healing materials

Abstract

The strategic integration of multi-functionalities within a singular nanoplatform has received growing attention for enhancing treatment efficacy, particularly in chemo-photothermal therapy. This study introduces a comprehensive concept of Janus nanoparticles (JNPs) composed of Au and Fe 3 O 4 nanostructures intricately bonded with β-cyclodextrins (β-CD) to encapsulate 5-Fluorouracil (5-FU) and Ibuprofen (IBU). This strategic structure is engineered to exploit the synergistic effects of chemo-photothermal therapy, underscored by their exceptional biocompatibility and photothermal conversion efficiency (∼32.88 %). Furthermore, these β-CD-conjugated JNPs enhance photodynamic therapy by generating singlet oxygen (1O 2) species, offering a multi-modality approach to cancer eradication. Computer simulation results were in good agreement with in vitro and in vivo assays. Through these studies, we were able to prove the improved tumor ablation ability of the drug-loaded β-CD-conjugated JNPs, without inducing adverse effects in tumor-bearing nude mice. The findings underscore a formidable tumor ablation potency of β-CD-conjugated Au-Fe 3 O 4 JNPs, heralding a new era in achieving nuanced, highly effective, and side-effect-free cancer treatment modalities. The emergence of multifunctional nanoparticles marks a pivotal stride in cancer therapy research. This investigation unveils Janus nanoparticles (JNPs) amalgamating gold (Au), iron oxide (Fe 3 O 4), and β-cyclodextrins (β-CD), encapsulating 5-Fluorouracil (5-FU) and Ibuprofen (IBU) for synergistic chemo-photothermal therapy. Demonstrating both biocompatibility and potent photothermal properties (∼32.88 %), these JNPs present a promising avenue for cancer treatment. Noteworthy is their heightened photodynamic efficiency and remarkable tumor ablation capabilities observed in vitro and in vivo , devoid of adverse effects. Furthermore, computational simulations validate their interactions with cancer cells, bolstering their utility as an emerging therapeutic modality. This endeavor pioneers a secure and efficacious strategy for cancer therapy, underscoring the significance of β-CD-conjugated Au-Fe 3 O 4 JNPs as innovative nanoplatforms with profound implications for the advancement of cancer therapy. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

14. Suppressing Wnt signaling of the blood‒tumor barrier to intensify drug delivery and inhibit lipogenesis of brain metastases.

Author

Tong, Yang, An, Pei, Tang, Puxian, Mu, Rui, Zeng, Yuteng, Sun, Hang, Zhao, Mei, Lv, Ziyan, Wang, Pan, Han, Wanjun, Gui, Chunshan, Zhen, Xuechu, and Han, Liang

Subjects

WNT signal transduction, FATTY acid synthases, LIPID synthesis, CEREBRAL edema, LIPASE inhibitors

Abstract

Lipogenesis is often highly upregulated in breast cancer brain metastases to adapt to intracranial low lipid microenvironments. Lipase inhibitors hold therapeutic potential but their intra-tumoral distribution is often blocked by the blood‒tumor barrier (BTB). BTB activates its Wnt signaling to maintain barrier properties, e.g. , Mfsd2a-mediated BTB low transcytosis. Here, we reported VCAM-1-targeting nano-wogonin (W@V-NPs) as an adjuvant of nano-orlistat (O@V-NPs) to intensify drug delivery and inhibit lipogenesis of brain metastases. W@V-NPs were proven to be able to inactivate BTB Wnt signaling, downregulate BTB Mfsd2a, accelerate BTB vesicular transport, and enhance tumor accumulation of O@V-NPs. With the ability to specifically kill cancer cells in a lipid-deprived environment with IC 50 at 48 ng/mL, W@V-NPs plus O@V-NPs inhibited the progression of brain metastases with prolonged survival of model mice. The combination did not induce brain edema, cognitive impairment, and systemic toxicity in healthy mice. Targeting Wnt signaling could safely modulate the BTB to improve drug delivery and metabolic therapy against brain metastases. An innovative strategy is proposed to boost the efficacy of drug delivery and anti-lipogenesis therapy for brain metastases by targeting the blood-tumor barrier (BTB), inhibiting endothelial Wnt signaling, and suppressing the activation of fatty acid synthase. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

15. Engineering nanomedicines for immunogenic eradication of cancer cells: Recent trends and synergistic approaches.

Author

Elzoghby, Ahmed O., Samir, Omar, Emam, Hagar E., Soliman, Ahmed, Abdelgalil, Riham M., Elmorshedy, Yomna M., Elkhodairy, Kadria A., and Nasr, Mahmoud L.

Subjects

CANCER cells, NANOMEDICINE, CLINICAL medicine, IMMUNE response, REACTIVE oxygen species

Abstract

Resistance to cancer immunotherapy is mainly attributed to poor tumor immunogenicity as well as the immunosuppressive tumor microenvironment (TME) leading to failure of immune response. Numerous therapeutic strategies including chemotherapy, radiotherapy, photodynamic, photothermal, magnetic, chemodynamic, sonodynamic and oncolytic therapy, have been developed to induce immunogenic cell death (ICD) of cancer cells and thereby elicit immunogenicity and boost the antitumor immune response. However, many challenges hamper the clinical application of ICD inducers resulting in modest immunogenic response. Here, we outline the current state of using nanomedicines for boosting ICD of cancer cells. Moreover, synergistic approaches used in combination with ICD inducing nanomedicines for remodeling the TME via targeting immune checkpoints, phagocytosis, macrophage polarization, tumor hypoxia, autophagy and stromal modulation to enhance immunogenicity of dying cancer cells were analyzed. We further highlight the emerging trends of using nanomaterials for triggering amplified ICD-mediated antitumor immune responses. Endoplasmic reticulum localized ICD, focused ultrasound hyperthermia, cell membrane camouflaged nanomedicines, amplified reactive oxygen species (ROS) generation, metallo-immunotherapy, ion modulators and engineered bacteria are among the most innovative approaches. Various challenges, merits and demerits of ICD inducer nanomedicines were also discussed with shedding light on the future role of this technology in improving the outcomes of cancer immunotherapy. Immunogenic cell death (ICD) inducer nanomedicines enhance tumor immunogenicity by stimulating the release of DAMPs, promoting antigen presentation, and activating dendritic cells, ultimately eliciting a robust and lasting antitumor immune response. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

16. A strong, silk protein-inspired tissue adhesive with an enhanced drug release mechanism for transdermal drug delivery.

Author

Song, Haoyuan, Wang, Liuyang, Wu, Jiaxu, Liu, Jie, Liu, Chao, Guo, Jianpeng, and Fang, Liang

Subjects

TRANSDERMAL medication, SKIN permeability, PRESSURE-sensitive adhesives, DRUG delivery systems, POLYETHYLENE glycol, MOLECULAR dynamics

Abstract

In transdermal drug delivery system (TDDS) patches, achieving prolonged adhesion, high drug loading, and rapid drug release simultaneously presented a significant challenge. In this study, a PHT-SP-Cu2+ adhesive was synthesized using polyethylene glycol (PEG), hexamethylene diisocyanate (HDI), trimethylolpropane (TMP), and silk protein (SP) as functional monomers which were combined with Cu2+ to improve the adhesion, drug loading, and drug release of the patch. The structure of the adhesion chains and the formation of Cu2+-p-π conjugated network in PHT-SP-Cu2+ were characterized and elucidated using different characterization methods including FT-IR, 13C NMR, XPS, SEM imaging and thermodynamic evaluation. The formulation of pressure-sensitive adhesive (PSA) was optimized through comprehensive research on adhesion, mechanics, rheology, and surface energy. The formulation of 3 wt.% SP and 3 wt.% Cu2+ provided superior adhesion properties compared to commercial standards. Subsequently, the peel strength of PHT-SP-Cu2+ was 7.6 times higher than that of the commercially available adhesive DURO-TAK® 87–4098 in the porcine skin peel test. The adhesion test on human skin confirmed that PHT-SP-Cu2+ could adhere to the human body for more than six days. Moreover, the drug loading, in vitro release test and skin permeation test were investigated using ketoprofen as a model drug, and the results showed that PHT-SP-Cu2+ had the efficacy of improving drug compatibility, promoting drug release and enhancing skin permeation as a TDDS. Among them, the drug loading of PHT-SP-Cu2+ was increased by 6.25-fold compared with PHT, and in the in vivo pharmacokinetic analysis, the AUC was similarly increased by 19.22-fold. The mechanism of α-helix facilitated drug release was demonstrated by Flori-Hawkins interaction parameters, molecular dynamics simulations and FT-IR. Biosafety evaluations highlighted the superior skin cytocompatibility and safety of PHT-SP-Cu2+ for transdermal applications. These results would contribute to the development of TDDS patch adhesives with outstanding adhesion, drug loading and release efficiency. A new adhesive, PHT-SP-Cu2+, was created for transdermal drug delivery patches. Polyethylene glycol, hexamethylene diisocyanate, trimethylolpropane, silk protein, and Cu2+ were used in synthesis. Characterization techniques confirmed the structure and Cu2+-p-π conjugated networks. Optimal formulation included 3 wt.% SP and 3 wt.% Cu2+, exhibiting superior adhesion. PHT-SP-Cu2+ showed 7.6 times higher peel strength than DURO-TAK® 87–4098 on porcine skin and adhered to human skin for over six days. It demonstrated a 6.25-fold increase in drug loading compared to PHT, with 19.22-fold higher AUC in vivo studies. α-helix facilitated drug release, proven by various analyses. PHT-SP-Cu2+ showed excellent cytocompatibility and safety for transdermal applications. This study contributes to developing efficient TDDS patches. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

17. A facile one-step self-assembly strategy for constructing biocompatible and pH-sensitive polyphenol-based nanoparticles for high-efficiency tumor therapy.

Author

Dong, Yuman, Li, Jieru, Wang, Tao, Dai, Yiwei, Guo, Shimeng, Zhao, Liangtao, and Du, Pengcheng

Subjects

NANOPARTICLES, DRUG delivery systems, TANNINS, HYDROGEN bonding interactions, BIOLOGICAL systems, CYTOTOXINS

Abstract

[Display omitted] • A simple and efficient strategy for biocompatible and pH-sensitive polyphenol-based nanoparticles. • Highly biocompatible, satisfactory safety and commercially materials are used. • DOX@F127-TA nanoparticles possess advantages of a high drug content, pH-sensitive and small size. • It exhibits efficient endocytosis, successful organoid delivery, and remarkable anti-tumor effects. Self-assembled supramolecular nanoparticles possess several advantages, including convenient preparation process, high controllability, stability, and multifunctionality, which make them highly beneficial as drug-carriers in field of drug delivery. Size of nano-carriers plays a crucial role in their performance, affecting their ability for long-term circulation and deep penetration into tumor tissues within biological systems. In this study, we present a simple one-step self-assembly strategy for constructing biocompatible and pH-sensitive polyphenol-based nanoparticles for high-efficiency tumor therapy. The self-assembled DOX@F127-TA nanoparticles are achieved through a combination of hydrogen bonding and hydrophobic interactions. The Pluronic F127 (F127) and tannic acid (TA) endow high biocompatibility and satisfactory safety to nano-drug carriers. By adjusting DOX content, DOX@F127-TA nanoparticles are successfully prepared with advantages of high drug content, pH-sensitive, high stability and small size. Additionally, the nanoparticles exhibit low hemolysis performance and electronegativity, which contribute to their long-term circulation stability in vivo. Furthermore, in vitro cytotoxicity, cellular uptake and patient-derived organoids were utilized to evaluate the efficacy of the DOX@F127-TA. The results demonstrate efficient endocytosis, successful organoid drug delivery, and remarkable anti-tumor effects, while exhibiting minimal toxicity to normal cells. Overall, DOX@F127-TA nanoparticles demonstrate great potential as a promising drug delivery platform for high-efficient cancer therapy and practical application. [ABSTRACT FROM AUTHOR]

Published

2024

18. Microfluidic strategies for engineering oxygen-releasing biomaterials.

Author

Zhu, Zhiqiang, Chen, Tianao, Wu, Yongqi, Wu, Xizhi, Lang, Zhongliang, Huang, Fangsheng, Zhu, Pingan, Si, Ting, and Xu, Ronald X.

Subjects

BIOMATERIALS, TISSUE engineering, OXYGEN carriers, MICROFLUIDIC analytical techniques, SMART materials, ENGINEERING, SCIENTIFIC community

Abstract

In the field of tissue engineering, local hypoxia in large-cell structures (larger than 1 mm3) poses a significant challenge. Oxygen-releasing biomaterials supply an innovative solution through oxygen ⁠ delivery in a sustained and controlled manner. Compared to traditional methods such as emulsion, sonication, and agitation, microfluidic technology offers distinct benefits for oxygen-releasing material production, including controllability, flexibility, and applicability. It holds enormous potential in the production of smart oxygen-releasing materials. This review comprehensively covers the fabrication and application of microfluidic-enabled oxygen-releasing biomaterials. To begin with, the physical mechanism of various microfluidic technologies and their differences in oxygen carrier preparation are explained. Then, the distinctions among diverse oxygen-releasing components in regards for oxygen-releasing mechanism, oxygen-carrying capacity, and duration of oxygen release are presented. Finally, the present obstacles and anticipated development trends are examined together with the application outcomes of oxygen-releasing biomaterials based on microfluidic technology in the biomedical area. Oxygen is essential for sustaining life, and hypoxia (a condition of low oxygen) is a significant challenge in various diseases. Microfluidic-based oxygen-releasing biomaterials offer precise control and outstanding performance, providing unique advantages over traditional approaches for tissue engineering. However, comprehensive reviews on this topic are currently lacking. In this review, we provide a comprehensive analysis of various microfluidic technologies and their applications for developing oxygen-releasing biomaterials. We compare the characteristics of organic and inorganic oxygen-releasing biomaterials and highlight the latest advancements in microfluidic-enabled oxygen-releasing biomaterials for tissue engineering, wound healing, and drug delivery. This review may hold the potential to make a significant contribution to the field, with a profound impact on the scientific community. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

19. An insight into the dual role of MoS2-based nanocarriers in anticancer drug delivery and therapy.

Author

Ghosh, Sandip and Lai, Jui-Yang

Subjects

NANOCARRIERS, DRUG therapy, ANTINEOPLASTIC agents, MEDICAL sciences, TARGETED drug delivery, SCIENTIFIC community

Abstract

Over the years, nanomaterials have been exploited as drug delivery systems and therapeutic agents in cancer treatment. Special emphasis has been placed on structure and shape-mediated drug loading and release. Functional materials, including molybdenum disulfide (MoS 2), have shown promising results because of their tunable structure and unmatched physicochemical properties. Specifically, easy surface functionalization and high drug adsorption ability make them ideal candidates. Although the large surface area of nanosheets/nanoflakes may result in high drug loading, the encapsulation efficiency is better for MoS 2 nanoflower structures. Due to its high targeting abilities, the loading of chemotherapeutic drugs onto MoS 2 may minimize nonspecific cellular death and undesired side effects. Furthermore, due to their strong light-absorption ability, MoS 2 nanostructures have been widely exploited as photothermal and photodynamic therapeutic agents. The unexplored dimensions of cancer therapy, including chemodynamic (Fenton-like reaction) and piezo-catalytic (ultrasound-mediated reactive oxygen generation), have been recently unlocked, in which the catalytic properties of MoS 2 are utilized to generate toxic free radicals to eliminate cancer. Intriguingly, combining these therapeutic modalities often results in high therapeutic efficacy at low doses and minimizes side effects. With a plethora of recent studies, a thorough analysis of current findings is crucial. Therefore, this review discusses the major advances in this field of research. A brief commentary on the limitations/future outlook/ethical issues of the clinical translation of MoS 2 -mediated cancer treatments is also deliberated. Overall, in our observations, the MoS 2 -based nanoformulations hold great potential for future cancer therapy applications. Development of nanomedicines based on MoS 2 has opened new avenues in cancer treatment. The MoS 2 with different morphologies (nanosheet/nanoflower/QDs) has shown promising results in controlled and targeted drug delivery, leading to minimized side effects and increased therapeutic efficacy. While existing reviews have primarily focused on the optical/thermal properties utilized in photodynamic/photothermal therapy, the outstanding catalytic properties of MoS 2 utilized in cancer therapies (chemodynamic/piezo-catalytic) are often overlooked. This review critically highlights and praises/criticizes individual articles reporting the MoS 2 -based nanoplatforms for cancer therapy applications. Additionally, MoS 2 -based combined therapies for synergistic effects are discussed. Furthermore, a brief commentary on the future prospects for clinical translations is also deliberated, which is appealing to various research communities engaged in cancer theranostics and biomedical sciences research. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

20. Nano-formulated delivery of active ingredients from traditional Chinese herbal medicines for cancer immunotherapy.

Author

Shang, Qi, Liu, Wandong, Leslie, Faith, Yang, Jiapei, Guo, Mingmei, Sun, Mingjiao, Zhang, Guangji, Zhang, Qiang, and Wang, Feihu

Subjects

CHINESE medicine, HERBAL medicine, IMMUNOTHERAPY, IMMUNE system, IMMUNE response

Abstract

Cancer immunotherapy has garnered promise in tumor progression, invasion, and metastasis through establishing durable and memorable immunological activity. However, low response rates, adverse side effects, and high costs compromise the additional benefits for patients treated with current chemical and biological agents. Chinese herbal medicines (CHMs) are a potential treasure trove of natural medicines and are gaining momentum in cancer immunomodulation with multi-component, multi-target, and multi-pathway characteristics. The active ingredient extracted from CHMs benefit generalized patients through modulating immune response mechanisms. Additionally, the introduction of nanotechnology has greatly improved the pharmacological qualities of active ingredients through increasing the hydrophilicity, stability, permeability, and targeting characteristics, further enhancing anti-cancer immunity. In this review, we summarize the mechanism of active ingredients for cancer immunomodulation, highlight nano-formulated deliveries of active ingredients for cancer immunotherapy, and provide insights into the future applications in the emerging field of nano-formulated active ingredients of CHMs. Nano-formulated active ingredients from Chinese herbal medicines demonstrate cancer immunomodulation through interacting with the innate and adaptive immune systems and modulating the microenvironment signal molecules. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

21. Microfluidics-derived hierarchical microparticles for the delivery of dienogest for localized endometriosis therapy.

Author

Wu, Meiling, Zhang, Qingfei, Shang, Luoran, and Duan, Ping

Subjects

ENDOMETRIUM, ENDOMETRIOSIS, NANOGELS, FEMALE reproductive organ diseases, GENITALIA, DRUG carriers, SERUM albumin

Abstract

Drug therapy is one of the most important strategies for treating gynecological diseases. Local drug delivery is promising for achieving optimal regional drug exposure, considering the complex anatomy and dynamic environment of the upper genital tract. Here, we present microparticle-based microcarriers with a hierarchical structure for localized dienogest (DNG) delivery and endometriosis treatment. The microparticles were fabricated by microfluidics and consisted of photo-crosslinked bovine serum albumin hydrogel particles (D@P-B MPs) encapsulating DNG-loaded PLGA (poly lactic-co-glycolic acid) microspheres. Such design enables the microparticles to have sustained release capacity and cell adhesion ability. Based on this, the microparticles were applied for the treatment of peritoneal endometriosis through intraperitoneal injection. The performance of the microparticles in inhibiting the growth of ectopic lesions as well as their anti-inflammatory, anti-angiogenesis, and pelvic pain-relieving effects are well demonstrated in vivo. These findings indicate that the present hierarchical microparticles are good candidates for localized treatment of endometriosis and are promising for the management of gynecological diseases. We prepared photo-crosslinked bovine serum albumin hydrogel particles (D@P-B MPs) encapsulating DNG-loaded PLGA microspheres using microfluidic electrospray. Such hierarchical structure provided multiple functions of the particles as drug carriers. The hierarchical microparticles not only supported the sustained release of drugs but also provided adhesion to human ectopic endometrial stromal cells. The hierarchical microparticles represented a localized treatment method for endometriosis and is promising for the management of gynecological diseases. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

22. Genome editing of PAR2 through targeted delivery of CRISPR-Cas9 system for alleviating acute lung inflammation via ERK/NLRP3/IL-1β and NO/iNOS signalling.

Author

Zhuo, Xin, Wu, Yue, Fu, Xiujuan, Li, Jianbin, Xiang, Yuxin, Liang, Xiaoyu, Mao, Canquan, and Jiang, Yuhong

Subjects

PNEUMONIA, GENOME editing, CRISPRS, PROTEASE-activated receptors, GENE targeting, LUNG diseases

Abstract

Excessive and uncontrollable inflammatory responses in alveoli can dramatically exacerbate pulmonary disease progressions through vigorous cytokine releases, immune cell infiltration and protease-driven tissue damages. It is an urgent need to explore potential drug strategies for mitigating lung inflammation. Protease-activated receptor 2 (PAR2) as a vital molecular target principally participates in various inflammatory diseases via intracellular signal transduction. However, it has been rarely reported about the role of PAR2 in lung inflammation. This study applied CRISPR-Cas9 system encoding Cas9 and sgRNA (pCas9-PAR2) for PAR2 knockout and fabricated an anionic human serum albumin-based nanoparticles to deliver pCas9-PAR2 with superior inflammation-targeting efficiency and stability (TAP /pCas9-PAR2). TAP /pCas9-PAR2 robustly facilitated pCas9-PAR2 to enter and transfect inflammatory cells, eliciting precise gene editing of PAR2 in vitro and in vivo. Importantly, PAR2 deficiency by TAP /pCas9-PAR2 effectively and safely promoted macrophage polarization, suppressed pro-inflammatory cytokine releases and alleviated acute lung inflammation, uncovering a novel value of PAR2. It also revealed that PAR2-mediated pulmonary inflammation prevented by TAP /pCas9-PAR2 was mainly dependent on ERK-mediated NLRP3/IL-1 β and NO/iNOS signalling. Therefore, this work indicated PAR2 as a novel target for lung inflammation and provided a potential nanodrug strategy for PAR2 deficiency in treating inflammatory diseases. TAP/ pCas9-PAR2 alleviated acute lung inflammation through ERK/NLRP3/IL-1 β and NO/iNOS signalling via genome editing of PAR2. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

23. The involvement of the mitochondrial membrane in drug delivery.

Author

Huang, Yinghui, Ji, Wenhui, Zhang, Jiaxin, Huang, Ze, Ding, Aixiang, Bai, Hua, Peng, Bo, Huang, Kai, Du, Wei, Zhao, Tingting, and Li, Lin

Subjects

MITOCHONDRIAL membranes, CELLULAR control mechanisms, THERAPEUTICS, TARGETED drug delivery, COMPREHENSION in children, TREATMENT effectiveness, NANOMEDICINE

Abstract

Treatment effectiveness and biosafety are critical for disease therapy. Bio-membrane modification facilitates the homologous targeting of drugs in vivo by exploiting unique antibodies or antigens, thereby enhancing therapeutic efficacy while ensuring biosafety. To further enhance the precision of disease treatment, future research should shift focus from targeted cellular delivery to targeted subcellular delivery. As the cellular powerhouses, mitochondria play an indispensable role in cell growth and regulation and are closely involved in many diseases (e.g. , cancer, cardiovascular, and neurodegenerative diseases). The double-layer membrane wrapped on the surface of mitochondria not only maintains the stability of their internal environment but also plays a crucial role in fundamental biological processes, such as energy generation, metabolite transport, and information communication. A growing body of evidence suggests that various diseases are tightly related to mitochondrial imbalance. Moreover, mitochondria-targeted strategies hold great potential to decrease therapeutic threshold dosage, minimize side effects, and promote the development of precision medicine. Herein, we introduce the structure and function of mitochondrial membranes, summarize and discuss the important role of mitochondrial membrane-targeting materials in disease diagnosis/treatment, and expound the advantages of mitochondrial membrane-assisted drug delivery for disease diagnosis, treatment, and biosafety. This review helps readers understand mitochondria-targeted therapies and promotes the application of mitochondrial membranes in drug delivery. Bio-membrane modification facilitates the homologous targeting of drugs in vivo by exploiting unique antibodies or antigens, thereby enhancing therapeutic efficacy while ensuring biosafety. Compared to cell-targeted treatment, targeting of mitochondria for drug delivery offers higher efficiency and improved biosafety and will promote the development of precision medicine. As a natural material, the mitochondrial membrane exhibits excellent biocompatibility and can serve as a carrier for mitochondria-targeted delivery. This review provides an overview of the structure and function of mitochondrial membranes and explores the potential benefits of utilizing mitochondrial membrane-assisted drug delivery for disease treatment and biosafety. The aim of this review is to enhance readers' comprehension of mitochondrial targeted therapy and to advance the utilization of mitochondrial membrane in drug delivery. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

24. Nanoparticle-integrated dissolving microneedles for the co-delivery of R848/aPD-1 to synergistically reverse the immunosuppressive microenvironment of triple-negative breast cancer.

Author

Huang, Sicong, Wen, Ting, Wang, Jiachen, Wei, Huiye, Xiao, Zecong, Li, Bo, and Shuai, Xintao

Subjects

TRIPLE-negative breast cancer, T cells, IMMUNE checkpoint inhibitors, TRANSDERMAL medication, DRUG delivery systems, IMMUNE checkpoint proteins

Abstract

Nowadays, effective immunotherapy against triple-negative breast cancer (TNBC) remains challenging due to the immunosuppressive tumor microenvironment. Immune checkpoint inhibitor is mostly employed to restore the activity of tumor-specific immune cells, which however brings little therapeutic outcome owing to the limited number of tumor-infiltrating CD8+ T cells and the inefficient delivery of immune drugs to the tumor tissue. Aiming to solve these problems, we herein constructed a tailor-made dissolving microneedle co-encapsulating the TLR7/8 agonist R848 and the immune checkpoint inhibitor aPD-1, termed αNP-RNP@DMN, and fabricated it as a transdermal drug delivery system. This well-designed microneedle patch, endowed with efficient tumor drug delivery ability, was able to mature tumor-infiltrating dendritic cells (TIDCs) and further promote the infiltration of CD8+ T cells into the tumor tissue with the aid of R848. Moreover, the introduction of aPD-1 blocked the programmed cell death protein 1/programmed cell death ligand 1(PD-1/PD-L1) immune checkpoints, synergistically reversing the immunosuppressive microenvironment of TNBC. In vivo therapeutic results demonstrated that αNP-RNP@DMN not only significantly prolonged the survival time of 4T1 tumor-bearing mice, but also inhibited tumor recurrence and lung metastasis after surgery, implying the great potential of this effective drug delivery system for enhanced immunotherapy of superficial tumors. The limited number of tumor-infiltrating CD8+ T cells and the inefficient delivery of immune drugs to the tumor tissue hinder the effective immunotherapy of triple-negative breast cancer (TNBC). Herein, a dissolving microneedle co-encapsulating TLR7/8 agonist R848 and immune checkpoint inhibitor aPD-1 was developed and fabricated as a transdermal drug delivery system. This tailor-made microneedle patch not only promoted drug accumulation in tumor sites in a safe and painless manner, but also lifted the immune-suppressive state of tumor-infiltrating dendritic cells (TIDCs). The activated TIDCs further enhanced T-cell infiltration into the tumor tissue, thus successfully boosting the therapeutic efficacy of aPD-1. This study demonstrated that this well-designed microneedle patch could be served as an effective drug delivery system for enhanced immunotherapy of TNBC. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

25. DNA origami nanodevice with spatial regulation of CD95 signaling for rheumatoid arthritis treatment.

Author

Mao, Miao, Pu, Zhe, and Zhang, Yuanqing

Subjects

DNA folding, RHEUMATOID arthritis, CELL communication

Published

2024

26. In-situ synthesis of copper-gallic acid metal–organic framework into the gentamicin-loaded chitosan hydrogel bead: A synergistic enhancement of antibacterial properties.

Author

Hamedi, Hanieh, Javanbakht, Siamak, and Mohammadi, Reza

Subjects

GALLIC acid, METAL-organic frameworks, HYDROGELS, DRUG efficacy, CHITOSAN, CYTOTOXINS, HISTORY of medicine

Abstract

[Display omitted] • GA-MOF was successfully in-situ synthesized in the CS matrix. • GM-CS/GA-MOF nanocomposite hydrogel beads was prepared via a simple approach. • GM-CS/GA-MOF displayed controlled release with a minor initial burst release. • GM-CS/GA-MOF showed notable antibacterial activity. • GM-CS/GA-MOF exhibited a cytocompatibility nature toward HFF2 cells. In the history of modern medicine, there has been a serious risk of antibacterial drugs as losing their effectiveness against bacteria. In this regard, nanocomposite hydrogel beads based on biopolymers such as chitosan (CS) have been recently developed as antibacterial platform. In this work, antibacterial copper-gallic acid metal–organic framework (GA-MOF) were developed to increase the biological efficiency of CS hydrogel beads. To end this, in-situ synthesis method was used to grow different concentration of GA-MOF into the hydrogel matrix. Also, gentamicin (GM) as the antibacterial drug was preloaded in the preparation of CS hydrogel beads to further enhance the antibacterial properties. Various analysis techniques were utilized for the validation of successful nanocomposites construction. In-vitro GA and GM release in the simulated physiological environmental (PBS, pH 7.4) were considered, revealing a controlled and sustained release profile during 72 h. Antibacterial studies showed inhibition zone of 26 ± 0.5 and 18 ± 0.5 mm for the Staphylococcus aureus and Escherichia coli bacteria, respectively. In addition, the MTT assay demonstrated good cytotoxicity (over 70 % cell viability after 48 h) for the human skin fibroblast HFF-2 cells. According to the results, the prepared nanocomposites have a good potential for use as an antibacterial bioplatform. [ABSTRACT FROM AUTHOR]

Published

2024

27. Collagenase Type I and Probucol-Loaded Nanoparticles Penetrate the Extracellular Matrix to Target Hepatic Stellate Cells for Hepatic Fibrosis Therapy.

Author

Wang, Xiaowei, Zhang, Wenjun, Zeng, Sheng, Wang, Liudi, and Wang, Bin

Subjects

HEPATIC fibrosis, LIVER cells, EXTRACELLULAR matrix, COLLAGENASES, CARRIER proteins

Abstract

Hepatic fibrosis is a common pathological process in chronic liver diseases, characterized by excessive reactive oxygen species (ROS), activated hepatic stellate cells (HSCs), and massive synthesis of extracellular matrix (ECM), which are important factors in the development of liver cirrhosis, liver failure, and liver cancer. During the development of hepatic fibrosis, ECM collagen produced by activated HSCs significantly hinders medication delivery to targeted cells and reduces the efficiency of pharmacological therapy. In this study, we designed a multifunctional hyaluronic acid polymeric nanoparticle (HA@PRB/COL NPs) based on autophagy inhibitor probucol (PRB) and collagenase type I (COL) modification, which could enhance ECM degradation and accurately target HSCs through specificity binding CD44 receptor in hepatic fibrosis therapy. Upon encountering excessive collagen I-deposition formed barrier, HA@PRB/COL NPs performed the nanodrill-like function to effectively degrade pericellular collagen I, leading to greater ECM penetration and prominent HSCs internalization capacity of delivered PRB. In mouse hepatic fibrosis model, HA@PRB/COL NPs were efficiently delivered to HSCs through binding CD44 receptor to achieve efficient accumulation in fibrotic liver. Further, we showed that HA@PRB/COL NPs executed the optimal anti-fibrotic activity by inhibiting autophagy and activation of HSCs. In conclusion, our novel dual-functional co-delivery system with degrading fibrotic ECM collagen and targeting activated HSCs exhibits great potentials in the treatment of hepatic fibrosis in clinic. The excess release of extracellular matrix (ECM) such as collagen in hepatic fibrosis hinders medication delivery and decreases the efficiency of pharmacological drugs. We aimed to develop a nano-delivery carrier system with protein hydrolyzed surfaces and further encapsulated an autophagy inhibitor (PRB) to enhance fibrosis-related ECM degradation-penetration and hepatic stellate cells (HSCs) targeting in hepatic fibrosis niche (HA@PRB/COL NPs). The COL of HA@PRB/COL NPs successfully worked as a scavenger to promote the digestion of the ECM collagen I barrier for deeper penetration into fibroid liver tissue. It also accurately targeted HSCs through specifically binding to the CD44 receptor and subsequently released PRB to inhibit autolysosome and ROS generation, thus preventing HSCs activation. Our HA@PRB/COL NPs system provided a promising therapeutic strategy for hepatic fibrosis in a clinic setting. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

28. Suicide gene delivery by morphology-adaptable enantiomeric peptide assemblies for combined ovarian cancer therapy.

Author

Song, Na, Sun, Zhe, Wang, Bo, Liu, Xin, Hu, Binbin, Chen, Ninglin, Zhang, Sihe, and Yu, Zhilin

Subjects

PEPTIDES, OVARIAN cancer, CANCER treatment, CANCER genes, PACLITAXEL, GENE therapy, SUICIDE

Abstract

Suicide gene therapy is a promising therapeutic model for ovarian cancer (OC), while suffering from poor gene delivery and limited therapeutic efficacy. To address this concern, here we reported the GSH-responsive morphology-transformable enantiomeric peptide assemblies as delivering vehicles for suicide genes and co-delivery of paclitaxel (PTX). Connecting a lipid-like amphiphile and a hydrophilic arginine segment through disulfide bonds led to the enantiomeric peptides. The enantiomeric peptide assemblies are able to simultaneously uptake plasmid DNA (pDNA) and PTX based on electrostatic and hydrophobic interactions. The resulting co-assemblies underwent GSH-responsive disulfide cleavage and thereby promoting their assembly from nanoparticles to nanofibers, leading to the co-release of pDNA and PTX. Cellular and animal studies confirmed the co-delivery of pDNA and PTX into OC cells and the cell apoptosis by the enantiomeric peptides. In addition, in vitro and in vivo experiments supported the advanced uptake and cytotoxicity for L-type peptide vehicles by OC cells, and their great potential for OC-imaging, growth-inhibition and apoptosis-induction compared to D-counterpart. Our results demonstrate that the GSH-responsive morphology-transformable chiral peptide assemblies accurately and simultaneously release suicide genes and chemodrugs at tumor sites, thus providing a new strategy for the development of delivering vehicles for suicide gene and establishment of new therapeutic models for ovarian cancer. Appropriate delivery carriers are essential for the clinical translation of cancer gene therapy, including the emerging suicide gene therapy. By combining the advantages of morphological transformable vehicles with the chirality peptides towards their bioactivity, we developed the GSH-responsive morphology-transformable enantiomeric peptide assemblies as delivering vehicles for suicide genes and co-delivery of paclitaxel. The GSH-responsive assembly of the enantiomeric peptides allows for precise release of plasmid DNA and paclitaxel in cancer cells, and promotes the formation of nanofibrils that facilitate gene entering nuclei for transfection. The enantiomeric peptide-based vehicles show the chirality-dependent capability for inducing cell apoptosis and inhibiting tumor growth. Our findings demonstrate a new strategy for developing therapeutic models for ovarian cancer. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

29. Release mechanism and pharmacodynamics of entecavir micro spheres.

Author

Chunyan Zhang, Liuxiang Chu, Keke Li, and Maocai Yan

Abstract

Entecavir, an effective anti-hepatitis B drug with low resistance rate, was designed as sustained-release micro spheres in our previous study. Here, we aimed to reveal the drug-release mechanism by observing the drug distribution and degradation behavior of poly (lactic-co-glycolic acid) and to investigate the pharmacodynamics of entecavir micro spheres. Raman spectroscopy was used to analyze the distribution of active pharmaceutical ingredients in the micro spheres. The results showed that there was little entecavir near the micro sphere surface. With increasing micro sphere depth, the drug distribution gradually increased and larger-size entecavir crystals were mainly distributed near the spherical center. The degradation behavior of poly (lactic-co-glycolic acid) was investigated using gel permeation chromatography. Changes in poly (lactic-co-glycolic acid) molecular weights during micro sphere degradation revealed that dissolution dominated the release process, which proved our previous research results. Pharmacodynamics studies on transgenic mice indicated that the anti-hepatitis B virus replication effect was maintained for 42 days after a single injection of entecavir micro spheres, similar to the effect of daily oral administration of entecavir tablets for 28 days. The entecavir micro spheres prepared in this study had a good anti-hepatitis B virus replication effect and it is expected to be used in anti hepatitis B virus treatment against hepatitis B virus. [ABSTRACT FROM AUTHOR]

Published

2024

30. Biomaterials-based anti-inflammatory treatment strategies for Alzheimer's disease.

Author

Jianjian Chu, Weicong Zhang, Yan Liu, Baofeng Gong, Wenbo Ji, Tong Yin, Chao Gao, Danqi Liangwen, Mengqi Hao, Cuimin Chen, Jianhua Zhuang, Jie Gao, and You Yin

Published

2024

31. Plant-derived nanovesicles as an emerging platform for cancer therapy.

Author

Liu, Hanzhe, Luo, Guo-Feng, and Shang, Zhengjun

Subjects

CANCER treatment, GREEN products, NATURAL products, NUCLEIC acids, CARCINOGENESIS

Abstract

Plant-derived nanovesicles (PDNVs) derived from natural green products have emerged as an attractive nanoplatform in biomedical application. They are usually characterized by unique structural and biological functions, such as the bioactive lipids/proteins/nucleic acids as therapeutics and targeting groups, immune-modulation, and long-term circulation. With the rapid development of nanotechnology, materials, and synthetic chemistry, PDNVs can be engineered with multiple functions for efficient drug delivery and specific killing of diseased cells, which represent an innovative biomaterial with high biocompatibility for fighting against cancer. In this review, we provide an overview of the state-of-the-art studies concerning the development of PDNVs for cancer therapy. The original sources, methods for obtaining PDNVs, composition and structure are introduced systematically. With an emphasis on the featured application, the inherent anticancer properties of PDNVs as well as the strategies in constructing multifunctional PDNVs-based nanomaterials will be discussed in detail. Finally, some scientific issues and technical challenges of PDNVs as promising options in improving anticancer therapy will be discussed, which are expected to promote the further development of PDNVs in clinical translation. An overview of the state-of-the-art studies concerning the development of plant-derived nanovesicles for cancer therapy was summarized systematically, including the original sources, isolation methods, composition/structure, and their applications in anti-tumor study. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

32. Development of exosome membrane materials-fused microbubbles for enhanced stability and efficient drug delivery of ultrasound contrast agent.

Author

Jang, Yongho, Park, Jeehun, Kim, Pilsu, Park, Eun-Joo, Sun, Hyungjin, Baek, Yujin, Jung, Jaehun, Song, Tai-kyong, Doh, Junsang, and Kim, Hyuncheol

Subjects

ULTRASOUND contrast media, MICROBUBBLES, DRUG stability, DRUG delivery systems, EXOSOMES

Abstract

Lipid-coated microbubbles are widely used as an ultrasound contrast agent, as well as drug delivery carriers. However, the two main limitations in ultrasound diagnosis and drug delivery using microbubbles are the short half-life in the blood system, and the difficulty of surface modification of microbubbles for active targeting. The exosome, a type of extracellular vesicle, has a preferentially targeting ability for its original cell. In this study, exosome-fused microbubbles (Exo-MBs) were developed by embedding the exosome membrane proteins into microbubbles. As a result, the stability of Exo-MBs is improved over the conventional microbubbles. On the same principle that under the exposure of ultrasound, microbubbles are cavitated and self-assembled into nano-sized particles, and Exo-MBs are self-assembled into exosome membrane proteins-embedded nanoparticles (Exo-NPs). The Exo-NPs showed favorable targeting properties to their original cells. A photosensitizer, chlorin e6, was loaded into Exo-MBs to evaluate therapeutic efficacy as a drug carrier. Much higher therapeutic efficacy of photodynamic therapy was confirmed, followed by cancer immunotherapy from immunogenic cell death. We have therefore developed a novel ultrasound image-guided drug delivery platform that overcomes the shortcomings of the conventional ultrasound contrast agent and is capable of simultaneous photodynamic therapy and cancer immunotherapy. Exosome-fused microbubbles (Exo-MBs) were developed and self-assembled into exosome membrane proteins-embedded nanoparticles (Exo-NPs), which became a novel ultrasound image-guided drug delivery platform in simultaneous photodynamic therapy and cancer immunotherapy. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

33. Purpurolide C-based microneedle promotes macrophage-mediated diabetic wound healing via inhibiting TLR4-MD2 dimerization and MYD88 phosphorylation.

Author

Liu, Yitong, Xia, Guiyang, Chen, Yingyi, Xia, Huan, Xu, Junji, Guo, Lijia, Lin, Sheng, and Liu, Yi

Subjects

WOUND healing, MYELOID differentiation factor 88, SURFACE plasmon resonance, DIMERIZATION, SKIN permeability

Abstract

Delayed wound healing in diabetes is a global challenge, and the development of related drugs is a clinical problem to be solved. In this study, purpurolide C (PC), a small-molecule secondary metabolite of the endophytic fungus Penicillium purpurogenum , was found to promote diabetic wound healing. To investigate the key regulation targets of PC, in vitro RNA-seq, molecular docking calculations, TLR4-MD2 dimerization SDS-PAGE detection, and surface plasmon resonance (SPR) were performed, indicating that PC inhibited inflammatory macrophage activation by inhibiting both TLR4-MD2 dimerization and MYD88 phosphorylation. Tlr4 knockout in vivo attenuated the promotion effect of PC on wound healing. Furthermore, a delivery system consisting of macrophage liposome and GelMA-based microneedle patches combined with PC (PC@MLIP MN) was developed, which overcame the poor water solubility and weak skin permeability of PC, so that successfully punctured the skin and delivered PC to local tissues, and accurately regulated macrophage polarization in diabetic wound management. Overall, PC is an anti-inflammatory small molecule compound with a well-defined structure and dual-target regulation, and the PC@MLIP MN is a promising novel biomaterial for the management of diabetic wound. Purpurolide C (PC), a small-molecule secondary metabolite of the endophytic fungus Penicillium purpurogenum , was found to promote diabetic wound healing. Schematic illustration of targeted and long-acting regulation mechanism of PC@MLIP MN in T2DM wound healing promotion. PC loaded with macrophage-liposome (MLIP) achieved an accurate regulation on local macrophages, and Gelatin methacryloyl (GelMA)-based microneedles (MNs) promote its skin permeability, which successfully achieved the effect of diabetic wound healing promotion in T2DM mouse models. Figure created with BioRender.com. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

34. Development of hyaluronic acid-silica composites via in situ precipitation for improved penetration efficiency in fast-dissolving microneedle systems.

Author

Tay, Jie Hao, Lim, Yu Han, Zheng, Mengjia, Zhao, Yakai, Tan, Wen See, Xu, Chenjie, Ramamurty, Upadrasta, and Song, Juha

Subjects

TRANSDERMAL medication, SILICA nanoparticles, PATIENT compliance, HYALURONIC acid

Abstract

Fast-dissolving microneedles (DMNs) hold significant promise for transdermal drug delivery, offering improved patient compliance, biocompatibility, and functional adaptability for various therapeutic purposes. However, the mechanical strength of the biodegradable polymers used in DMNs often proves insufficient for effective penetration into human skin, especially under high humidity conditions. While many composite strategies have been developed to reinforce polymer-based DMNs, simple mixing of the reinforcements with polymers often results in ineffective penetration due to inhomogeneous dispersion of the reinforcements and the formation of undesired micropores. In response to this challenge, this study aimed to enhance the mechanical performance of hyaluronic acid (HA)-based microneedles (MNs), one of the most commonly used DMN systems. We introduced in situ precipitation of silica nanoparticles (Si) into the HA matrix in conjunction with conventional micromolding. The precipitated silica nanoparticles were uniformly distributed, forming an interconnected network within the HA matrix. Experimental results demonstrated that the mechanical properties of the HA–Si composite MNs with up to 20 vol% Si significantly improved, leading to higher penetration efficiency compared to pure HA MNs, while maintaining structural integrity without any critical defects. The composite MNs also showed reduced degradation rates and preserved their drug delivery capabilities and biocompatibility. Thus, the developed HA–Si composite MNs present a promising solution for efficient transdermal drug delivery and address the mechanical limitations inherent in DMN systems. HA–Si composite dissolving microneedle (DMN) systems were successfully fabricated through in situ precipitation and conventional micromolding processes. The precipitated silica nanoparticles formed an interconnected network within the HA matrix, ranging in size from 25 to 230 nm. The optimal silica content for HA–Si composite MN systems should be up to 20 % by volume to maintain structural integrity and mechanical properties. HA–Si composite MNs with up to 20 % Si showed improved penetration efficiency and reduced degradation rates compared to pure HA MNs, thereby expanding the operational window. The HA–Si composite MNs retained good drug delivery capabilities and biocompatibility. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

35. Synthesis and characterization of pH-triggered doxorubicin-conjugated polydopamine-coated cobalt ferrite nanoparticles for in-vitro/in-vivo studies in liver cancer therapy.

Author

Septian Dwitya, Sat, Lin, Kuen-Song, Weng, Meng-Tzu, Vukile Mdlovu, Ndumiso, Tsai, Wei-Chin, and Wu, Chun-Ming

Subjects

DOXORUBICIN, LIVER cancer, SMALL-angle X-ray scattering, CANCER treatment, FICK'S laws of diffusion, FERRITES, MATERIAL erosion

Abstract

[Display omitted] • The PDA-coated CF NPs for drug delivery in cancer therapy were successfully synthesized; • The SAXS of PDA-coated CF NPs have been characterized by BioXTAS RAW analyses; • Drug release behavior represents a Fickian diffusion mechanism at sustained release phase; • A pH sensitive drug delivery system was successfully prepared; • In vitro and in vivo studies indicated higher antitumor efficiency on liver cancer of mice. Polydopamine-coated cobalt ferrite nanoparticles (PDA-coated CF-NPs) were synthesized and characterized for their potential in drug delivery evaluation. Small-angle X-ray scattering (SAXS) showed post-coating spherical shape of magnetic PDA NPs. The scattering intensity at zero angle (I(0)) of PDA-coated CF (0.01) had higher scattering intensity than CF-NPs (0.49 × 10-3). PDA increased the flexibility degree of unfolding on Kratky plot shifting from 1.05 to 1.87 at same qR g values. The pair-distance distribution function (P(r)) of PDA-coated CF-NPs indicated a more homogeneous and compact scattering structure. GNOM indicated larger size for CF, while PDA-coated CF (a narrower and taller peak) displayed a more compact and uniform scattering profile. PDA reduced crystallinity size to 2.51 nm with amorphous peaks at 38.12°, 44.28°, and 64.43° degree and infrared spectrum confirmed PDA incorporation onto CF-NPs. PDA-coated CF had 1.5-fold larger pore size and enhanced surface area. CF and PDA-coated CF exhibited "S" shape behavior in Langevin function without hysteresis. The kinetic models suggested Fickian diffusion and sustainable release for the erosion-dominated release of the PDA-coated CF. In vitro , doxorubicin (DOX)-carried PDA-coated CF (D-P@CF) showed low toxicity to HepG2 cells; in vivo , liver tumor inhibition indicated medication delivery potential for cancer treatment. [ABSTRACT FROM AUTHOR]

Published

2024

36. Extracellular Vesicles for Drug Delivery in Cancer Treatment.

Author

Wang, Li, Yu, Xin, Zhou, Juan, and Su, Chunxia

Subjects

EXTRACELLULAR vesicles, CANCER treatment, DRUG carriers, CELL communication, ANTINEOPLASTIC agents

Abstract

Extracellular vesicles (EVs) are nanoscale vesicles derived from cells that mediate intercellular communication by transporting bioactive molecules. They play significant roles in various physiological and pathological conditions. EVs hold great potential as novel biomarkers of diseases, therapeutic agents, and drug delivery vehicles. Furthermore, EVs as novel drug delivery vehicles have demonstrated significant advantages in preclinical settings. In this review, we discussed the biogenesis and characteristics of EVs and their functions in cancer. We summarize the therapeutic applications of EVs as a natural delivery vehicles in cancer therapy. We highlight the existing challenges, illuminate vital questions, and propose recommendations to effectively address them effectively. [ABSTRACT FROM AUTHOR]

Published

2023

37. Biomimetic nanomedicines for precise atherosclerosis theranostics.

Author

Tao, Ying, Lan, Xinmiao, Zhang, Yang, Fu, Chenxing, Liu, Lu, Cao, Feng, and Guo, Weisheng

Subjects

NANOMEDICINE, COMPANION diagnostics, DRUG delivery systems, ATHEROSCLEROSIS, CARDIOVASCULAR diseases, SYSTEMS design

Abstract

Atherosclerosis (AS) is a leading cause of the life-threatening cardiovascular disease (CVD), creating an urgent need for efficient, biocompatible therapeutics for diagnosis and treatment. Biomimetic nanomedicines (bNMs) are moving closer to fulfilling this need, pushing back the frontier of nano-based drug delivery systems design. This review seeks to outline how these nanomedicines (NMs) might work to diagnose and treat atherosclerosis, to trace the trajectory of their development to date and in the coming years, and to provide a foundation for further discussion about atherosclerotic theranostics. This review summerize various biomimetic nanomedicines for precise atherosclerosis diagnosis and treatment, which is vital for the development of atherosclerotic theranostic agents. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

38. Current research trends of nanomedicines.

Author

Liu, Qiuyue, Zou, Jiahui, Chen, Zhongjian, He, Wei, and Wu, Wei

Subjects

NANOMEDICINE, NANOCARRIERS, TREATMENT effectiveness

Abstract

Owing to the inherent shortcomings of traditional therapeutic drugs in terms of inadequate therapeutic efficacy and toxicity in clinical treatment, nanomedicine designs have received widespread attention with significantly improved efficacy and reduced non-target side effects. Nanomedicines hold tremendous theranostic potential for treating, monitoring, diagnosing, and controlling various diseases and are attracting an unfathomable amount of input of research resources. Against the backdrop of an exponentially growing number of publications, it is imperative to help the audience get a panorama image of the research activities in the field of nanomedicines. Herein, this review elaborates on the development trends of nanomedicines, emerging nanocarriers, in vivo fate and safety of nanomedicines, and their extensive applications. Moreover, the potential challenges and the obstacles hindering the clinical translation of nanomedicines are also discussed. The elaboration on various aspects of the research trends of nanomedicines may help enlighten the readers and set the route for future endeavors. This review elaborates on the development trends of nanomedicines, emerging nanocarriers, in vivo fate and safety of nanomedicines, and their extensive applications. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

39. Adaptable polymerization platform for therapeutics with tunable biodegradability.

Author

Hrochová, M., Kotrchová, L., Frejková, M., Konefał, R., Gao, S., Fang, J., Kostka, L., and Etrych, T.

Subjects

POLYMERS, BLOCK copolymers, DRUG side effects, LIVING polymerization, POLYMER degradation, POLYMERIZATION, BLOOD circulation

Abstract

Biodegradable polymer-based therapeutics have recently become essential drug delivery biomaterials for various bioactive compounds. Biodegradable and biocompatible polymer-based biomaterials fulfill the requirements of these therapeutics because they enable to obtain polymer biomaterials with optimized blood circulation, pharmacokinetics, biodegradability, and renal excretion. Herein, we describe an adaptable polymerization platform employed for the synthesis of long-circulating, stimulus-sensitive and biodegradable biomaterials, therapeutics, or theranostics. Four chain transfer agents (CTA) were designed and successfully synthesized for the reversible addition-fragmentation chain transfer polymerization, allowing the straightforward synthesis of hydrolytically biodegradable structures of block copolymers-based biomaterials. The controlled polymerization using the CTAs enables controlling the half-life of the hydrolytic degradation of polymer precursors in a wide range from 5 h to 21 days. Moreover, the antitumor drug pirarubicin (THP) was successfully conjugated to the polymer biomaterials via a pH-sensitive hydrazone bond for in vitro and in vivo experiments. Polymer conjugates demonstrated superior antitumor efficacy compared to basic linear polymer-based conjugates. Notably, the biodegradable systems, even though those with degradation in the order of hours were selected, increased the half-life of THP in the bloodstream almost two-fold. Indeed, the presented platform design enables the main chain-end specific attachment of targeting ligands or diagnostic molecules. The adaptable polymerization platform design allows tuning of the biodegradability rate, stimuli-sensitive drug bonding, and optimized pharmacokinetics to increase the therapy outcome and system targeting, thus allowing the preparation of targeted or theranostic polymer conjugates. Biodegradable and biocompatible polymer-based biomaterials are recognized as potential future bioactive nanomedicines. To advance the development of such biomaterials, we developed polymerization platforms utilizing tailored chain transfer agents allowing the straightforward synthesis of hydrolytically degradable polymer biomaterials with tuned biodegradability from hours to several days. The platform allows for the synthesis of long-circulating, stimulus-sensitive and biodegradable biomaterial serving as drug carriers or theranostics. The therapeutic potential was validated by preparation of polymer biomaterials containing pirarubicin, anticancer drug, bound via pH sensitive bond and by showing prolonged blood circulation and increased antitumor activity while keeping the drug side effects low. This work paves the way for future development of biodegradable polymer biomaterials with advanced properties in drug delivery. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

40. High-precision targeting and destruction of cancer-associated PDGFR-β+ stromal fibroblasts through self-assembling, protein-only nanoparticles.

Author

Voltà-Durán, Eric, Alba-Castellón, Lorena, Serna, Naroa, Casanova, Isolda, López-Laguna, Hèctor, Gallardo, Alberto, Sánchez-Chardi, Alejandro, Villaverde, Antonio, Unzueta, Ugutz, Vázquez, Esther, and Mangues, Ramón

Subjects

NANOMEDICINE, BREAST, PLATELET-derived growth factor, CELL receptors, TARGETED drug delivery, MICROBIAL toxins, FIBROBLASTS, TOXINS

Abstract

The need for more effective and precision medicines for cancer has pushed the exploration of new materials appropriate for drug delivery and imaging, and alternative receptors for targeting. Among the most promising strategies, finding suitable cell surface receptors and targeting agents for cancer-associated platelet derived growth factor receptor β (PDGFR-β)+ stromal fibroblasts is highly appealing. As a neglected target, this cell type mechanically and biologically supports the growth, progression, and infiltration of solid tumors in non-small cell lung, breast, pancreatic, and colorectal cancers. We have developed a family of PDGFR-β-targeted nanoparticles based on biofabricated, self-assembling proteins, upon hierarchical and iterative selective processes starting from four initial candidates. The modular protein PDGFD-GFP-H6 is well produced in recombinant bacteria, resulting in structurally robust oligomeric particles that selectively penetrates into PDGFR-β+ stromal fibroblasts in a dose-dependent manner, by means of the PDGFR-β ligand PDGFD. Upon in vivo administration, these GFP-carrying protein nanoparticles precisely accumulate in tumor tissues and enlighten them for IVIS observation. When GFP is replaced by a microbial toxin, selective tumor tissue destruction is observed associated with a significant reduction in tumor volume growth. The presented data validate the PDGFR-β/PDGFD pair as a promising toolbox for targeted drug delivery in the tumor microenvironment and oligomeric protein nanoparticles as a powerful instrument to mediate highly selective biosafe targeting in cancer through non-cancer cells. We have developed a transversal platform for nanoparticle-based drug delivery into cancer-associated fibroblasts. This is based on the engineered modular protein PDGFD-GFP-H6 that spontaneously self-assemble and selectively penetrates into PDGFR-β+ stromal fibroblasts in a dose-dependent manner, by means of the PDGFR-β ligand PDGFD. In vivo , these protein nanoparticles accumulate in tumor and when incorporating a microbial toxin, they destroy tumor tissues with a significant reduction in tumor volume, in absence of side toxicities. The data presented here validate the PDGFR-β/PDGFD pair as a fully versatile toolbox for targeted drug delivery in the tumor microenvironment intended as a synergistic treatment. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

41. The effect of electrostatic high pressure nebulization on the stability, activity and ex vivo distribution of ionic self-assembled nanomedicines.

Author

Braet, Helena, Andretto, Valentina, Mariën, Remco, Yücesan, Beyza, van der Vegte, Stefan, Haegebaert, Ragna, Lollo, Giovanna, De Smedt, Stefaan C., and Remaut, Katrien

Subjects

SPRAY nozzles, NANOMEDICINE, PERITONEAL cancer, ELECTROSTATIC precipitation, DRUG carriers, PERITONEUM, ELECTROSTATIC interaction

Abstract

Pressurized intraperitoneal aerosol chemotherapy (PIPAC) is applied to treat unresectable peritoneal metastasis (PM), an advanced, end-stage disease with a poor prognosis. Electrostatic precipitation of the aerosol (ePIPAC) is aimed at improving the intraperitoneal (IP) drug distribution and tumor penetration. Also, the combination of nanoparticles (NPs) as drug delivery vehicles and IP aerosolization as administration method has been proposed as a promising tool to treat PM. There is currently limited knowledge on how electrostatic precipitation (ePIPAC) and high pressure nebulization (PIPAC) affects the performance of electrostatically formed complexes. Therefore, the stability, in vitro activity and ex vivo distribution and tissue penetration of negatively charged cisPt-pArg-HA NPs and positively charged siRNA-RNAiMAX NPs was evaluated following PIPAC and ePIPAC. Additionally, a multidirectional Medspray® nozzle was developed and compared with the currently used Capnopen® nozzle. For both NP types, PIPAC and ePIPAC did not negatively influence the in vitro activity, although limited aggregation of siRNA-RNAiMAX NPs was observed following nebulization with the Capnopen®. Importantly, ePIPAC was linked to a more uniform distribution and higher tissue penetration of the NPs aerosolized by both nozzles, independent on the NPs charge. Finally, compared to the Capnopen®, an increased NP deposition was observed at the top of the ex vivo model following aerosolization with the Medspray® nozzle, which indicates that this device possesses great potential for IP drug delivery purposes. Aerosolized drug delivery in the peritoneal cavity holds great promise to treat peritoneal cancer. In addition, electrostatic precipitation of the aerosol to the peritoneal tissue is aimed at improving the drug distribution and tumor penetration. The combination of nanoparticles (NPs), which are nano-sized drug delivery vehicles, and aerosolization has been proposed as a promising tool to treat peritoneal cancer. However, there is currently limited knowledge on how electrostatic precipitation and aerosolization affect the performance of electrostatically formed NPs. Therefore, the stability, activity, distribution and penetration of negatively and positively charged NPs was evaluated after aerosolization and electrostatic precipitation. Additionally, to further optimize the local drug distribution, a multidirectional spray nozzle was developed and compared with the currently used nozzle. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

42. Lipid carriers for mRNA delivery.

Author

Zhang, Wanting, Jiang, Yuxin, He, Yonglong, Boucetta, Hamza, Wu, Jun, Chen, Zhongjian, and He, Wei

Subjects

MESSENGER RNA, LIPIDS, PROTEIN synthesis, COVID-19 pandemic, VIRUS diseases

Abstract

Messenger RNA (mRNA) is the template for protein biosynthesis and is emerging as an essential active molecule to combat various diseases, including viral infection and cancer. Especially, mRNA-based vaccines, as a new type of vaccine, have played a leading role in fighting against the current global pandemic of COVID-19. However, the inherent drawbacks, including large size, negative charge, and instability, hinder its use as a therapeutic agent. Lipid carriers are distinguishable and promising vehicles for mRNA delivery, owning the capacity to encapsulate and deliver negatively charged drugs to the targeted tissues and release cargoes at the desired time. Here, we first summarized the structure and properties of different lipid carriers, such as liposomes, liposome-like nanoparticles, solid lipid nanoparticles, lipid-polymer hybrid nanoparticles, nanoemulsions, exosomes and lipoprotein particles, and their applications in delivering mRNA. Then, the development of lipid-based formulations as vaccine delivery systems was discussed and highlighted. Recent advancements in the mRNA vaccine of COVID-19 were emphasized. Finally, we described our future vision and perspectives in this field. Lipid carriers with high biocompatibility have excellent mRNA encapsulation and delivery efficacy. Meanwhile, the emergence of lipid carriers provides an effective solution for delivering mRNA vaccines. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

43. Interplay between G protein-coupled receptors and nanotechnology.

Author

Jiang, Yuhong, Li, Yuke, Fu, Xiujuan, Wu, Yue, Wang, Rujing, Zhao, Mengnan, Mao, Canquan, and Shi, Sanjun

Subjects

NANOMEDICINE, NANOTECHNOLOGY, DRUG target, CELL membranes, DRUG efficacy, CELLULAR signal transduction, G protein coupled receptors

Abstract

G protein-coupled receptors (GPCRs), as the largest family of membrane receptors, actively modulate plasma membrane and endosomal signalling. Importantly, GPCRs are naturally nanosized, and spontaneously formed nanoaggregates of GPCRs (natural nano-GPCRs) may enhance GPCR-related signalling and functions. Although GPCRs are the molecular targets of the majority of marketed drugs, the poor pharmacokinetics and physicochemical properties of GPCR ligands greatly limit their clinical applicability. Nanotechnology, as versatile techniques, can encapsulate GPCR ligands to assemble synthetic nano-GPCRs to overcome their obstacles, robustly elevating drug efficacy and safety. Moreover, endosomal delivery of GPCR ligands by nanoparticles can precisely initiate sustained endosomal signal transduction, while nanotechnology has been widely utilized for isolation, diagnosis, and detection of GPCRs. In turn, due to overexpression of GPCRs on the surface of various types of cells, GPCR ligands can endow nanoparticles with active targeting capacity for specific cells via ligand-receptor binding and mediate receptor-dependent endocytosis of nanoparticles. This significantly enhances the potency of nanoparticle delivery systems. Therefore, emerging evidence has revealed the interplay between GPCRs and nanoparticles, although investigations into their relationship have been inadequate. This review aims to summarize the interaction between GPCRs and nanotechnology for understanding their mutual influences and utilizing their interplay for biomedical applications. It will provide a fundamental platform for developing powerful and safe GPCR-targeted drugs and nanoparticle systems. GPCRs as molecular targets for the majority of marketed drugs are naturally nanosized, and even spontaneously form nano aggregations (nano-GPCRs). Nanotechnology has also been applied to construct synthetic nano-GPCRs or detect GPCRs, while endosomal delivery of GPCR ligands by nanoparticles can magnify endosomal signalling. Meanwhile, molecular engineering of nanoparticles with GPCRs or their ligands can modulate membrane binding and endocytosis, powerfully improving the efficacy of nanoparticle system. However, there are rare summaries on the interaction between GPCRs and nanoparticles. This review will not only provide a versatile platform for utilizing nanoparticles to modulate or detect GPCRs, but also facilitate better understanding of the designated value of GPCRs for molecular engineering of biomaterials with GPCRs in therapeutical application. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

44. Self-assembly of CXCR4 antagonist peptide–docetaxel conjugates for breast tumor multi-organ metastasis inhibition.

Author

Li, Chen, Lang, Jiayan, Wang, Yazhou, Cheng, Zhaoxia, Zu, Mali, Li, Fenfen, Sun, Jingyi, Deng, Yating, Ji, Tianjiao, Nie, Guangjun, and Zhao, Ying

Subjects

CXCR4 receptors, METASTASIS, TRIPLE-negative breast cancer, BREAST tumors, PEPTIDES, ABIRATERONE acetate

Abstract

As a representative chemotherapeutic drug, docetaxel (DTX) has been used for breast cancer treatment for decades. However, the poor solubility of DTX limits its efficacy, and the DTX based therapy increases the metastasis risk due to the upregulation of C–X–C chemokine receptor type 4 (CXCR4) expression during the treatment. Herein, we conjugated CXCR4 antagonist peptide (CTCE) with DTX (termed CTCE–DTX) as an anti-metastasis agent to treat breast cancer. CTCE–DTX could self-assemble to nanoparticles, targeting CXCR4-upregulated metastatic tumor cells and enhancing the DTX efficacy. Thus, the CTCE–DTX NPs achieved promising efficacy on inhibiting both bone-specific metastasis and lung metastasis of triple-negative breast cancer. Our work provided a rational strategy on designing peptide–drug conjugates with synergistic anti-tumor efficacy. The peptide–drug conjugate (CTCE‒DTX) was developed for anti-metastasis of breast cancer in two ways: 1) blocking CXCL12–CXCR4 binding and interaction to restrain cell invasion; 2) enhancing chemo-sensitivity to obtain direct cytotoxicity. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

45. A bioresponsive diselenide-functionalized hydrogel with cascade catalytic activities for enhanced local starvation- and hypoxia-activated melanoma therapy.

Author

Ding, Xiaoran, Zang, Mingsong, Zhang, Yujie, Chen, Yongchen, Du, Jingjing, Yan, An, Gu, Jiamei, Li, Yuqi, Wei, Shu, Xu, Jiayun, Sun, Hongcheng, Liu, Junqiu, and Yu, Shuangjiang

Subjects

CATALYTIC activity, DACARBAZINE, GLUCOSE oxidase, DEXTRAN, HYDROGELS, GLUTATHIONE peroxidase, ANTINEOPLASTIC agents, MELANOMA

Abstract

Glutathione (GSH) consumption-enhanced cancer therapies represent important potential cancer treatment strategies. Herein, we developed a new multifunctional diselenide-crosslinked hydrogel with glutathione peroxidase (GPx)-like catalytic activity for GSH depletion-enhanced glucose oxidase (GOx)-mediated tumor starvation and hypoxia-activated chemotherapy. By increasing acid and H 2 O 2 during GOx-induced tumor starvation, the degradation of the multiresponsive scaffold could be promoted, which led to accelerated release of the loaded drugs. Meanwhile, the overproduced H 2 O 2 led to accelerated intracellular GSH consumption under the cascade catalysis of small molecular selenides released from the degraded hydrogel, further enhancing the curative effect of in situ H 2 O 2 and subsequent multimodal cancer treatment. Following the GOx-induced amplification of hypoxia, tirapazamine (TPZ) was transformed into the highly toxic benzotriazinyl radical (BTZ·), exhibiting enhanced antitumor activity. This GSH depletion-augmented cancer treatment strategy effectively boosted GOx-mediated tumor starvation and activated the hypoxia drug, leading to significantly enhanced local anticancer efficacy. There has been a growing interest in depleting intracellular GSH as a potential strategy for improving ROS-based cancer therapy. Herein, a bioresponsive diselenide-functionalized dextran-based hydrogel with GPx-like catalytic activity was developed for GSH consumption-enhanced local starvation- and hypoxia-activated melanoma therapy. Results showed that the overproduced H 2 O 2 led to accelerated intracellular GSH consumption under the cascade catalysis of small molecular selenides released from the degraded hydrogel, further enhancing the curative effect of in situ H 2 O 2 and subsequent multimodal cancer treatment. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

46. Stimuli-responsive cancer nanomedicines inhibit glycolysis and impair redox homeostasis.

Author

Meng, Xuan, Wang, Lin, Zhao, Ning, Zhao, Delong, Shen, Yongli, Yao, Yuan, Jing, Wenjie, Man, Shuli, Dai, Yujie, and Zhao, Yanjun

Subjects

OXYGEN consumption, GLYCOLYSIS, HOMEOSTASIS, REACTIVE oxygen species, NANOMEDICINE, OXIDATION-reduction reaction

Abstract

The solid tumors are characterized with oxidative stress and metabolic reprogramming, which has been independently used for targeted tumor monotherapy. However, the potential of targeting metabolism-redox circuit in tumor therapy has long been neglected. Herein, we report a hybrid nanocarrier for concurrent targeting of glycolysis and redox balance in the current work. The nanocarriers are made of pH- and ATP-responsive zeolitic imidazolate framework (ZIF-8) as the porous core that was further coated with poloxamer 407 as the steric stabilizer. Two active cargos, glucose oxidase (GOx) and 3-bromopyruvate (3-BrPA) were co-loaded in the core of nanocarrier. GOx is well-known for its ability of producing hydrogen peroxide at the expense of glucose and oxygen. 3-BrPA can reduce oxygen and glucose consumption through glycolysis, which sensitized cancer cells to GOx-induced apoptosis. At the cellular level, the hybrid nanocarrier significantly impaired the redox balance in the liver hepatocellular carcinoma cell line (HepG2), as evidenced by the depletion of glutathione and boost of reactive oxygen species. The potency of hybrid nanocarrier in terms of suppressing HepG2 cell energy metabolism was proven by the exhaustion of ATP. As a consequence, cell viability was greatly reduced. The in vivo efficacy of hybrid nanocarriers was demonstrated in HepG2 tumor-bearing mice. The current work presents an approach of targeting metabolism-redox circuit for tumor treatment, which may enrich the available anti-tumor strategies. Metabolic alterations and elevated reactive oxygen species (ROS) are two characteristics of cancer. The metabolic patterns of cancer cells are elaborately reprogrammed to enable the rapid propagation of cancer cells. However, the potential of targeting the metabolism-redox circuit in anti-tumor therapy has long been neglected. As a proof-of-concept, we report an engineered stimuli-responsive nanomedicine that can eradicate cancer cells via cooperative glycolysis inhibition and redox impairment. The current work presents an approach of targeting the metabolism-redox circuit for tumor treatment, which may enrich the available anti-tumor strategies. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

47. Three generations of thiolated cyclodextrins: A direct comparison of their mucus permeating and mucoadhesive properties.

Author

Haddadzadegan, Soheil, Knoll, Patrick, Wibel, Richard, Kali, Gergely, and Bernkop-Schnürch, Andreas

Subjects

MUCUS, SULFHYDRYL group, CYCLODEXTRINS, FREE groups, POLYETHYLENE glycol, HYDROXYL group, THIOLS, THIOUREA

Abstract

This study aims to compare the mucus permeating and mucoadhesive properties of three generations of thiolated cyclodextrins (CDs). Free thiol groups of thiolated γ-CDs (CD-SH) were S-protected with 2-mercaptonicotinic acid (MNA), leading to a second generation of thiolated CDs (CD-SS-MNA) and with 2 kDa polyethylene glycol (PEG) bearing a terminal thiol group leading to a third generation of thiolated CDs (CD-SS-PEG). The structure of these thiolated CDs was confirmed and characterized by FT-IR, 1H NMR and colorimetric assays. Thiolated CDs were evaluated regarding viscosity, mucus diffusion, and mucoadhesion. The viscosity of the mixture of CD-SH, CD-SS-MNA, or CD-SS-PEG with mucus increased up to 11-, 16-, and 14.1-fold compared to unmodified CD within 3 hours, respectively. Mucus diffusion increased in the following rank order: unprotected CD-SH < CD-SS-MNA < CD-SS-PEG. The residence time of CD-SH, CD-SS-MNA, and CD-SS-PEG on porcine intestine was up to 9.6-, 12.55-, and 11.2-fold prolonged compared to native CD, respectively. According to these results, S-protection of thiolated CDs can be a promising approach to improve their mucus permeating and mucoadhesive properties. Three generations of thiolated cyclodextrins (CDs) with different types of thiol ligands have been synthesized to improve mucus interaction. 1st generation of thiolated CDs was synthesized by converting hydroxyl groups into thiols by reaction with Thiourea. For 2nd generation, free thiol groups were S-protected by reaction with 2-mercaptonicotinic acid (MNA), resulting in high reactive disulfide bonds. For 3rd generation, terminally thiolated short PEG chains (2 kDa) were used for S-protection of thiolated CDs. Mucus penetrating properties were found to be increased as follows: 1st generation < 2nd generation < 3rd generation. Furthermore, mucoadhesive properties were improved in the following rank order: 1st generation < 3rd generation < 2nd generation. This study suggests that the S-protection of thiolated CDs can enhance mucus penetrating and mucoadhesive properties. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

48. Targeted long-term noninvasive treatment of choroidal neovascularization by biodegradable nanoparticles.

Author

Yao, Hao, Xu, Huan, Wu, Mingxing, Lei, Wulong, Li, Lanjiao, Liu, Danning, Wang, Zhigang, Ran, Haitao, Ma, Huafeng, and Zhou, Xiyuan

Subjects

BIODEGRADABLE nanoparticles, MACULAR degeneration, NANOMEDICINE, NEOVASCULARIZATION, VASCULAR endothelial cells, INTRAVITREAL injections, LOW vision

Abstract

Choroidal neovascularization (CNV) is the main cause of vision loss in patients with wet age-related macular degeneration (AMD). Currently, treatment of these conditions requires repeated intravitreal injections, which may lead to complications such as infection and hemorrhage. So, we have developed a noninvasive method for treating CNV with nanoparticles, namely, Angiopoietin1-anti CD105-PLGA nanoparticles (AAP NPs), which targets the CNV to enhance drug accumulation at the site. These nanoparticles, with PLGA as a carrier, can slowly release encapsulated Angiopoietin 1 (Ang 1) and target the choroidal neovascularization marker CD105 to enhance drug accumulation, increases vascular endothelial cadherin (VE-cadherin) expression between vascular endothelial cells, effectively reduce neovascularization leakage and inhibit Angiopoietin 2(Ang 2) secretion by endothelial cells. In a rat model of laser-induced CNV, intravenous injection of AAP NPs exerted a good therapeutic effect in reducing CNV leakage and area. In short, these synthetic AAP NPs provide an effective alternative treatment for AMD and meet the urgent need for noninvasive treatment in neovascular ophthalmopathy. This work describes the synthesis, injection-mediated delivery, in vitro and in vivo efficacy of targeted nanoparticles with encapsulated Ang1; via these nanoparticles, the drug can be targeted to choroidal neovascularization lesions for continuous treatment. The release of Ang1 can effectively reduce neovascularization leakage, maintain vascular stability, and inhibit Ang2 secretion and inflammation. This study provides a new approach for the treatment of wet age-related macular degeneration. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

49. Antibacterial, anti-inflammatory and wet-adhesive poly(ionic liquid)-based oral patch for the treatment of oral ulcers with bacterial infection.

Author

Zhang, Zijun, Zhang, Qiuyang, Gao, Shuna, Xu, Hui, Guo, Jiangna, and Yan, Feng

Subjects

ORAL drug administration, BACTERIAL diseases, CANKER sores, IONIC liquids, STAPHYLOCOCCUS aureus infections

Abstract

Oral aphthous ulcers are a common inflammatory efflorescence of oral mucosa, presenting as inflammation and oral mucosal damage and manifesting as pain. The moist and highly dynamic environment of the oral cavity makes the local treatment of oral aphthous ulcers challenging. Herein, a poly(ionic liquid)-based diclofenac sodium (DS)-loaded (PIL-DS) buccal tissue adhesive patch fabricated with intrinsically antimicrobial, highly wet environment adhesive properties and anti-inflammatory activities to treat oral aphthous ulcers was developed. The PIL-DS patch was prepared via polymerization of a catechol-containing ionic liquid, acrylic acid, and butyl acrylate, followed by anion exchange with DS−. The PIL-DS can adhere to wet tissues, including mucosa muscles and organs, and efficiently deliver the carried DS− at wound sites, exerting remarkable synergistic antimicrobial (bacteria and fungi) properties. Accordingly, the PIL-DS elicited dual therapeutic effects on oral aphthous ulcers with Staphylococcus aureus infection through antibacterial and anti-inflammatory activities, significantly accelerating oral aphthous ulcer healing as an oral mucosa patch. The results indicated that the PIL-DS patch, with inherently antimicrobial and wet adhesion properties, is promising for treating oral aphthous ulcers in clinical practice. Oral aphthous ulcers are a common oral mucosal disease, which could lead to bacterial infection and inflammation in severe cases, especially for people with large ulcers or low immunity. However, moist oral mucosa and highly dynamic oral environment make it challenging to maintain therapeutic agents and physical barriers at the wound surface. Therefore, an innovative drug carrier with wet adhesion is urgently needed. Herein, a poly(ionic liquid)-based diclofenac sodium (DS)-loaded (PIL-DS) buccal tissue adhesive patch was developed to treat oral aphthous ulcers showing intrinsically antimicrobial and highly wet environment adhesive properties due to the presence of catechol-containing ionic liquid monomer. Additionally, the PIL-DS showed significantly therapeutic effects on oral aphthous ulcers with S. aureus infection through antibacterial and anti-inflammatory activities. We expect that our work can provide inspiration for the development of treatment for microbially infected oral ulcers. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

50. Development and evaluation of sustained release matrix tablets of pregabalin: A case study based on quality by design to analyze the impact of variables.

Author

Yonghua Yu, Penghe Xu, Tingting Lou, Benkai Qin, and Huina Zhang

Abstract

The current research work describes systematic development of sustained release matrix tablets of a hydrophilic drug, pregabalin, using employing rational blend of hydrophilic polymers such as polyoxyethylene and carbomer as the release controlling polymers. As per the QbD-based approach, the patient-centric quality target product profile was defined and critical quality attributes were earmarked. Preliminary studies were conducted for screening the formulation and process variables. Systematic optimization of the highly critical and influential formulation variables were optimized with the help of an orthogonal experimental design. The impact of independent factors such as the amount of polyvinyl pyrrolidone, polyethylene oxide and carbomer 971P was optimized on in vitro drug release parameters at different time points as the dependent factors. The optimized tablet formulation was subjected to film coating with opadry color concentrate with the help of standard pan coating process. Further, the process optimization was performed for evaluating the impact of key process parameters on the quality attributes of the drug product. Overall, the study indicated successful development of the sustained release tablet formulation of pregabalin using hydrophilic polymers, where experimental design use provides significantly benefit in the product and process understanding. [ABSTRACT FROM AUTHOR]

Published

2023