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1. Enhancing antitumor efficacy of CLDN18.2-directed antibody-drug conjugates through autophagy inhibition in gastric cancer

Author

Wenjing Xue, Caili Xu, Kaiqi Zhang, Lu Cui, Xiting Huang, Yanyang Nan, Dianwen Ju, Xusheng Chang, and Xuyao Zhang

Subjects
Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Cytology, QH573-671
Abstract

Abstract Claudin18.2 (CLDN18.2) is overexpressed in cancers of the digestive system, rendering it an ideal drug target for antibody-drug conjugates (ADCs). Despite many CLDN18.2-directed ADCs undergoing clinical trials, the inconclusive underlying mechanisms pose a hurdle to extending the utility of these agents. In our study, αCLDN18.2-MMAE, an ADC composed of an anti-CLDN18.2 monoclonal antibody and the tubulin inhibitor MMAE, induced a dose-dependent apoptosis via the cleavage of caspase-9/PARP proteins in CLDN18.2-positive gastric cancer cells. It was worth noting that autophagy was remarkably activated during the αCLDN18.2-MMAE treatment, which was characterized by the accumulation of autophagosomes, the conversion of autophagy marker LC3 from its form I to II, and the complete autophagic flux. Inhibiting autophagy by autophagy inhibitor LY294002 remarkably enhanced αCLDN18.2-MMAE-induced cytotoxicity and caspase-mediated apoptosis, indicating the cytoprotective role of autophagy in CLDN18.2-directed ADC-treated gastric cancer cells. Combination with an autophagy inhibitor significantly potentiated the in vivo antitumoral efficacy of αCLDN18.2-MMAE. Besides, the Akt/mTOR pathway inactivation was demonstrated to be implicated in the autophagy initiation in αCLDN18.2-MMAE-treated gastric cancer cells. In conclusion, our study highlighted a groundbreaking investigation into the mechanism of the CLDN18.2-directed ADC, focusing on the crucial role of autophagy, providing a novel insight to treat gastric cancer by the combination of CLDN18.2-directed ADC and autophagy inhibitor.

Published
2024
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2. Modulating autophagy to boost the antitumor efficacy of TROP2-directed antibody-drug conjugate in pancreatic cancer

Author

Caili Xu, Xiting Huang, Qinchao Hu, Wenjing Xue, Kaicheng Zhou, Xingxiu Li, Yanyang Nan, Dianwen Ju, Ziyu Wang, and Xuyao Zhang

Subjects
TROP2, Antibody-drug conjugate, Autophagy, Apoptosis, Pancreatic cancer, Therapeutics. Pharmacology, RM1-950
Abstract

Pancreatic cancer, characterized by a dismal prognosis and limited treatment options, persists as a formidable challenge in oncology. Trophoblast cell surface antigen 2 (TROP2)-directed antibody-drug conjugates have achieved great success in solid tumors such as breast cancer and uroepithelial carcinoma. However, their efficacy against pancreatic cancer was insufficient in clinical trials, necessitating an imperative exploration of underlying mechanisms and new therapeutic strategies. In this study, we indicated that αTROP2-MMAE, an antibody-drug conjugate targeting TROP2, induced apoptosis through the caspase-9/PARP pathway and exerted potent antitumor effects against TROP2-positive pancreatic cancer. Simultaneously, RNA sequencing suggested significant changes in autophagy after αTROP2-MMAE treatment. The formation of autophagosomes and activation of autophagic flux were markedly induced through mechanisms associated with suppressing the activation of the Akt/mTOR pathway. The addition of pharmacological inhibitors of autophagy enhanced the cytotoxicity and apoptosis caused by αTROP2-MMAE, revealing the cytoprotective role of autophagy in TROP2-positive pancreatic cancer. In the subcutaneous xenograft model using BxPC3 cells, the combined administration of αTROP2-MMAE and an autophagy inhibitor elevated the tumor inhibition rate of αTROP2-MMAE from 71.6 % to 99.0 %, resulting in the eradication of tumors in half of the mice. Collectively, our research demonstrated for the first time the cytoprotective role of autophagy in TROP2-targeted antibody-drug conjugate therapy for pancreatic cancer, providing new perspectives for mechanistic exploration and therapeutic strategies in the treatment of pancreatic cancer.

Published
2024
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3. Targeting IL-33 reprograms the tumor microenvironment and potentiates antitumor response to anti-PD-L1 immunotherapy

Author

Yu Bai, Tao Wu, Jun Lin, Shuwen Xu, Xian Zeng, Xuyao Zhang, Jiajun Fan, Dianwen Ju, Mengyang Li, Yanyang Nan, Xiaozhi Hu, Kaicheng Zhou, An Zhu, Zihan Dou, Zhonglian Cao, Xumeng Zhang, Yuanzhen Zhang, and Xuebin Wang

Subjects
Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Background The main challenge against patients with cancer to derive benefits from immune checkpoint inhibitors targeting PD-1/PD-L1 appears to be the immunosuppressive tumor microenvironment (TME), in which IL-33/ST2 signal fulfills critical functions. However, whether IL-33 limits the therapeutic efficacy of anti-PD-L1 remains uncertain.Methods Molecular mechanisms of IL-33/ST2 signal on anti-PD-L1 treatment lewis lung carcinoma tumor model were assessed by RNA-seq, ELISA, WB and immunofluorescence (IF). A sST2-Fc fusion protein was constructed for targeting IL-33 and combined with anti-PD-L1 antibody for immunotherapy in colon and lung tumor models. On this basis, bifunctional fusion proteins were generated for PD-L1-targeted blocking of IL-33 in tumors. The underlying mechanisms of dual targeting of IL-33 and PD-L1 revealed by RNA-seq, scRNA-seq, FACS, IF and WB.Results After anti-PD-L1 administration, tumor-infiltrating ST2+ regulatory T cells (Tregs) were elevated. Blocking IL-33/ST2 signal with sST2-Fc fusion protein potentiated antitumor efficacy of PD-L1 antibody by enhancing T cell responses in tumor models. Bifunctional fusion protein anti-PD-L1-sST2 exhibited enhanced antitumor efficacy compared with combination therapy, not only inhibited tumor progression and extended the survival, but also provided long-term protective antitumor immunity. Mechanistically, the superior antitumor activity of targeting IL-33 and PD-L1 originated from reducing immunosuppressive factors, such as Tregs and exhausted CD8+ T cells while increasing tumor-infiltrating cytotoxic T lymphocyte cells.Conclusions In this study, we demonstrated that IL-33/ST2 was involved in the immunosuppression mechanism of PD-L1 antibody therapy, and blockade by sST2-Fc or anti-PD-L1-sST2 could remodel the inflammatory TME and induce potent antitumor effect, highlighting the potential therapeutic strategies for the tumor treatment by simultaneously targeting IL-33 and PD-L1.

Published
2024
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4. A potential strategy for bladder cancer treatment: inhibiting autophagy to enhance antitumor effects of Nectin-4-MMAE

Author

Yichen Wang, Yanyang Nan, Chunguang Ma, Xiaolin Lu, Qian Wang, Xiting Huang, Wenjing Xue, Jiajun Fan, Dianwen Ju, Dingwei Ye, and Xuyao Zhang

Subjects
Cytology, QH573-671
Abstract

Abstract Research and development on Nectin-4 antibody-drug conjugates (ADC) have been greatly accelerated since the approval of enfortumab vedotin to treat uroepithelial cancer. During the course of this study, we identified that autophagy serves as a cytoprotective mechanism during Nectin-4-MMAE treatment and proposed a strategy to enhance the antitumor effects of Nectin-4-MMAE in bladder cancer. Nectin-4-MMAE rapidly internalized into bladder cancer cells in 30 minutes and released MMAE, inducing the onset of caspase-mediated apoptosis and leading to the inhibition of tumor cell growth. Transcriptomics showed significant alterations in autophagy-associated genes in bladder cancer cells treated with Nectin-4-MMAE, which suggested autophagy was activated by Nectin-4-MMAE. Furthermore, autophagy activation was characterized by ultrastructural analysis of autophagosome accumulation, immunofluorescence of autophagic flux, and immunoblotting autophagy marker proteins SQSTM1 and LC3 I/II. Importantly, inhibiting autophagy by LY294002 and chloroquine significantly enhances the cytotoxicity effects of Nectin-4-MMAE in bladder cancer cells. Additionally, we detected the participation of the AKT/mTOR signaling cascade in the induction of autophagy by Nectin-4-MMAE. The combination of Nectin-4-MMAE and an autophagy inhibitor demonstrated enhanced antitumor effects in the HT1376 xenograft tumor model. After receiving a single dose of Nectin-4-MMAE, the group that received the combination treatment showed a significant decrease in tumor size compared to the group that received only one type of treatment. Notably, one mouse in the combination treatment group achieved complete remission of the tumor. The combination group exhibited a notable rise in apoptosis and necrosis, as indicated by H&E staining and immunohistochemistry (cleaved caspase-3, ki67). These findings demonstrated the cytoprotective role of autophagy during Nectin-4-MMAE treatment and highlighted the potential of combining Nectin-4-MMAE with autophagy inhibitors for bladder cancer treatment.

Published
2024
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5. Novel nitroxoline derivative combating resistant bacterial infections through outer membrane disruption and competitive NDM-1 inhibition

Author

Peng He, Sijing Huang, Rui Wang, Yunkai Yang, Shangye Yang, Yue Wang, Mengya Qi, Jiyang Li, Xiaofen Liu, Xuyao Zhang, and Meiqing Feng

Subjects
Nitroxoline, ASN-1733, NDM-1, inhibitor, antibiotic resistance, Infectious and parasitic diseases, RC109-216, Microbiology, QR1-502
Abstract

ABSTRACTNew Delhi metallo-β-lactamase-1 (NDM-1) has rapidly disseminated worldwide, leading to multidrug resistance and worse clinical prognosis. Designing and developing effective NDM-1 inhibitors is a critical and urgent challenge. In this study, we constructed a library of long-lasting nitroxoline derivatives and identified ASN-1733 as a promising dual-functional antibiotic. ASN-1733 can effectively compete for Ca2+ on the bacterial surface, causing the detachment of lipopolysaccharides (LPS), thereby compromising the outer membrane integrity and permeability and exhibiting broad-spectrum bactericidal activity. Moreover, ASN-1733 demonstrated wider therapeutic applications than nitroxoline in mouse sepsis, thigh and mild abdominal infections. Furthermore, ASN-1733 can effectively inhibit the hydrolytic capability of NDM-1 and exhibits synergistic killing effects in combination with meropenem against NDM-1 positive bacteria. Mechanistic studies using enzymatic experiments and computer simulations revealed that ASN-1733 can bind to key residues on Loop10 of NDM-1, hindering substrate entry into the enzyme's active site and achieving potent inhibitory activity (Ki = 0.22 µM), even in the presence of excessive Zn2+. These findings elucidate the antibacterial mechanism of nitroxoline and its derivatives, expand their potential application in the field of antibacterial agents and provide new insights into the development of novel NDM-1 inhibitors.

Published
2024
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6. Targeting CD47 and Angiogenesis Demonstrates Effective Anti-Tumor Effect in Bladder Cancer

Author

Xiting Huang, Qian Wang, Yanyang Nan, Xuyao Zhang, Ke Xu, Dianwen Ju, and Weihong Ding

Subjects
bladder cancer, CD47 blockade therapy, innate immunity, angiogenesis, combinational therapy, Biology (General), QH301-705.5
Abstract

Background: Although immunotherapy has shown potential in cancer treatment, current immunotherapeutics for bladder cancer are limited by a low response rate. Therefore, it is necessary to investigate other suitable immunotherapeutic targets and strategies for bladder cancer. Methods: To evaluate whether CD47 could be a suitable target for bladder cancer immunotherapy, CD47 protein expression levels in 116 bladder cancer tissue samples were assessed by IHC staining. In vitro anti-tumor effect of blocking CD47 was examined by phagocytosis assays. In vivo anti-tumor effects of targeting CD47 and angiogenesis were experimented in the HSPCs-CDX model. Results: We find that CD47 is highly expressed in bladder cancer samples and is associated with poor prognosis. Blocking CD47 could enhance the human PBMC-derived macrophages’ phagocytosis of T24 (from 10.40% to 29.70%) and 5637 (from 5.31% to 33.52%) human bladder cancer cells, as well as demonstrate anti-tumor effects in the HSPCs-CDX model (tumor growth inhibition rate, TGI: 33.05%). During CD47 treatment, we observed that the level of angiogenesis increased after CD47 blockade, and it might undermine the effect of CD47 immunotherapy. We then combined CD47 blockade with anti-angiogenic drugs to treat bladder cancer and discovered that inhibiting angiogenesis could further improve the anti-tumor effect of CD47 blockade (TGI: 76.39%). Finally, we tested the anti-tumor effect of co-targeting CD47 and angiogenesis using a bispecific fusion protein, SIRPα-VEGFR1, which successfully inhibited tumor growth to a similar extent as a combination therapy. Conclusions: Our study suggests that targeting CD47 could inhibit the growth of bladder cancer by promoting macrophage-mediated anti-tumor immunity. Moreover, blocking CD47 and angiogenesis could achieve a potent anti-tumor effect and could be an effective immunotherapy strategy for bladder cancer.

Published
2024
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7. TROP2-directed nanobody-drug conjugate elicited potent antitumor effect in pancreatic cancer

Author

Caili Xu, Min Zhu, Qian Wang, Jiajun Cui, Yuping Huang, Xiting Huang, Jing Huang, Junwei Gai, Guanghui Li, Peng Qiao, Xian Zeng, Dianwen Ju, Yakun Wan, and Xuyao Zhang

Subjects
TROP2, Nanobody-drug conjugate, Pancreatic cancer, Mechanisms of action, Antitumor effect, Biotechnology, TP248.13-248.65, Medical technology, R855-855.5
Abstract

Abstract Background Pancreatic cancer is a highly aggressive malignancy with limited treatment options and a poor prognosis. Trophoblast cell surface antigen 2 (TROP2), a cell surface antigen overexpressed in the tumors of more than half of pancreatic cancer patients, has been identified as a potential target for antibody–drug conjugates (ADCs). Almost all reported TROP2-targeted ADCs are of the IgG type and have been poorly studied in pancreatic cancer. Here, we aimed to develop a novel nanobody-drug conjugate (NDC) targeting TROP2 for the treatment of pancreatic cancer. Results In this study, we developed a novel TROP2-targeted NDC, HuNbTROP2-HSA-MMAE, for the treatment of TROP2-positive pancreatic cancer. HuNbTROP2-HSA-MMAE is characterized by the use of nanobodies against TROP2 and human serum albumin (HSA) and has a drug-antibody ratio of 1. HuNbTROP2-HSA-MMAE exhibited specific binding to TROP2 and was internalized into tumor cells with high endocytosis efficiency within 5 h, followed by intracellular translocation to lysosomes and release of MMAE to induce cell apoptosis in TROP2-positive pancreatic cancer cells through the caspase-3/9 pathway. In a xenograft model of pancreatic cancer, doses of 0.2 mg/kg and 1 mg/kg HuNbTROP2-HSA-MMAE demonstrated significant antitumor effects, and a dose of 5 mg/kg even eradicated the tumor. Conclusion HuNbTROP2-HSA-MMAE has desirable affinity, internalization efficiency and antitumor activity. It holds significant promise as a potential therapeutic option for the treatment of TROP2-positive pancreatic cancer. Graphical Abstract

Published
2023
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8. Time-course RNA-sequencing and Co-expression Modules Revealed a Critical Salt Response Regulatory Network in Apple

Author

Xin Huang, Meiling Zhang, Liping Wang, Xuyao Zhang, Ruigang Wu, and Fei Shen

Subjects
gene expression, malus domestica, regulatory network, salt stress, transcriptome sequencing, Plant culture, SB1-1110
Abstract

As one of the most important fruit tree crops, apple (Malus ×domestica), is faced with the serious impact of soil salinization. However, the underlying genetic and regulatory network remains elusive. Here, we adopted time-course RNA sequencing to decipher the genetic basis and regulatory module of apple in response to salt stress. Among a series of intense changes in genes at each time point, the critical genes in the mitogen-activated protein kinase signaling pathway were highly consistent with the duration of the stress treatment. Moreover, Salt Overly Sensitive 1 (SOS1) genes were identified and predicted to play important roles in the response process. We constructed coexpression modules and explored modules significantly associated with stress. SOS genes were identified in the hub genes, suggesting a critical role. Interestingly, transcription factors were also identified and predicted to cointeract with SOS genes in the hub genes of the coexpression module [e.g., HB7 (MD01G1226600), WRKY33 (MD12G1181000), and ERF106 (MD07G1248700)]. Collectively, our exploration and findings provide a reference and data resource for the study of genetic and salt regulatory networks in apple.

Published
2023
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11. Spin-Hall Effect of Cylindrical Vector Vortex Beams

Author

Xuyao Zhang, Shuo Wang, Jinhong Liu, Jinze Wu, and Jinhong Li

Subjects
Spin-Hall effect of light, cylindrical vector vortex beams, Imbert–Fedorov shift, weak measurement, Applied optics. Photonics, TA1501-1820
Abstract

Spin-Hall effect (SHE) of light is one of the main manifestations of the spin-orbit interaction of photons, and has been extensively studied for optical beams with homogeneous polarization. Here, we present a theoretical study of the SHE of cylindrical vector vortex beams (CVVBs) possessing inhomogeneous polarization. We derive the analytical expressions of the SHE of CVVBs reflected and refracted at a dielectric interface with radial and azimuthal polarization of incidence. The spin-dependent shifts of the SHE of light linearly depend on the topological charge of the CVVBs. In contrast to the conventional SHE of horizontally or vertically polarized beams, the SHE shifts of the CVVBs are asymmetrical when the topological charge is nonzero. This asymmetry results in the transverse Imbert–Fedorov (IF) shifts that are proportional to the topological charge. Furthermore, based on weak measurement, we propose an experimental scheme to enhance the SHE and related IF shifts with proper pre- and post-selection polarization states. Our results advance the study of the SHE of structured light and may find applications in SHE-based techniques such as precision measurement.

Published
2023
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12. Characterization and functional analysis of AhGPAT9 gene involved in lipid synthesis in peanut (Arachis hypogaea L.)

Author

Yue Shen, Yi Shen, Yonghui Liu, Yang Bai, Man Liang, Xuyao Zhang, and Zhide Chen

Subjects
Arachis hypogaea, AhGPAT9, evolution analysis, triacylglycerol, oil content, fatty acid, Plant culture, SB1-1110
Abstract

GPAT enzymes (glycerol-3-phosphate 1-O-acyltransferase, EC 2.3.1.15) catalyze the initial and rate-limiting step of plant glycerolipid biosynthesis for membrane homeostasis and lipid accumulation, yet little research has been done on peanuts. By reverse genetics and bioinformatics analyses, we have characterized an AhGPAT9 isozyme, of which the homologous product is isolated from cultivated peanut. QRT-PCR assay revealed a spatio-temporal expression pattern that the transcripts of AhGPAT9 accumulating in various peanut tissues are highly expressed during seed development, followed by leaves. Green fluorescent protein tagging of AhGPAT9 confirmed its subcellular accumulation in the endoplasmic reticulum. Compared with the wild type control, overexpressed AhGPAT9 delayed the bolting stage of transgenic Arabidopsis, reduced the number of siliques, and increased the seed weight as well as seed area, suggesting the possibility of participating in plant growth and development. Meanwhile, the mean seed oil content from five overexpression lines increased by about 18.73%. The two lines with the largest increases in seed oil content showed a decrease in palmitic acid (C16:0) and eicosenic acid (C20:1) by 17.35% and 8.33%, respectively, and an increase in linolenic acid (C18:3) and eicosatrienoic acid (C20:3) by 14.91% and 15.94%, respectively. In addition, overexpressed AhGPAT9 had no significant effect on leaf lipid content of transgenic plants. Taken together, these results suggest that AhGPAT9 is critical for the biosynthesis of storage lipids, which contributes to the goal of modifying peanut seeds for improved oil content and fatty acid composition.

Published
2023
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13. Targeting 4-1BB and PD-L1 induces potent and durable antitumor immunity in B-cell lymphoma

Author

Yichen Wang, Xuyao Zhang, Caili Xu, Yanyang Nan, Jiajun Fan, Xian Zeng, Byoung S. Kwon, and Dianwen Ju

Subjects
B-cell lymphoma, anti-PD-L1 ICI, 4-1BB agonist, CD8+ T cells, combination therapy, Immunologic diseases. Allergy, RC581-607
Abstract

IntroductionAlthough PD-1/L1 mAb has demonstrated clinical benefits in certain cancer types, low response rate and resistance remain the main challenges for the application of these immune checkpoint inhibitors (ICIs). 4-1BB is a co-stimulator molecule expressed in T cells, which could enhance T cell proliferation and activation. Herein, the synergetic antitumor effect and underlying mechanism of 4-1BB agonist combined with PD-1/PD-L1 blockade were determined in B-cell lymphoma (BCL).MethodsSubcutaneous transplantation BCL tumor models and metastasis models were established to evaluate the therapeutic effect of PD-L1 antibody and/or 4-1BB agonist in vivo. For the mechanistic study, RNA-seq was applied to analyze the tumor microenvironment and immune-related signal pathway after combination treatment. The level of IFN-γ, perforin, and granzyme B were determined by ELISA and Real-time PCR assays, while tumor-infiltrating T cells were measured by flow cytometry and immunohistochemical analysis. CD4/CD8 specific antibodies were employed to deplete the related T cells to investigate the role CD4+ and CD8+ T cells played in combination treatment.ResultsOur results showed that combining anti-PD-L1 ICI and 4-1BB agonists elicited regression of BCL and significantly extended the survival of mice compared to either monotherapy. Co-targeting PD-L1 and 4-1BB preferentially promoted intratumoral cytotoxic lymphocyte infiltration and remodeled their function. RNA-sequence analysis uncovered a series of up-regulated genes related to the activation and proliferation of cytotoxic T lymphocytes, further characterized by increased cytokines including IFN-γ, granzyme B, and perforin. Furthermore, depleting CD8+ T cells not CD4+ T cells totally abrogated the antitumor efficacy, indicating the crucial function of the CD8+ T cell subset in the combination therapy.DiscussionIn summary, our findings demonstrated that 4-1BB agonistic antibody intensified the antitumor immunity of anti-PD-1/PD-L1 ICI via promoting CD8+ T cell infiltration and activation, providing a novel therapeutic strategy to BCL.

Published
2022
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14. Assessing the eco-efficiency of complex forestry enterprises using LCA/time-series DEA methodology

Author

Xuyao Zhang and Dayu Xu

Subjects
Eco-efficiency, Complex forestry enterprise, LCA, Time-series DEA, Case study, Ecology, QH540-549.5
Abstract

Complex forestry enterprises have the potential to lead the current industrial upgrade under the strategy of carbon neutrality and carbon peaking. This paper aims to investigate the inputs and outputs influencing the eco-efficiency of complex forestry enterprises through a case study. A hybrid ensemble approach of life cycle assessment (LCA) and time-series data envelopment analysis (time-series DEA) was proposed to evaluate the case enterprise's eco-efficiency. It is found that, from the perspective of the average intensity of key input and output factors, environmental impact in efficient years is 45.25% of that in inefficient ones, and when it comes to the fiber consumption and the energy consumption, this percentage turns into 65.53% and 77.66%. With the findings, we provide guidelines for complex forestry enterprises to enhance the eco-efficiency in improving environmental impact and in giving full play to the advantages of forestry industrial chain resources. Our findings also contribute to the existent literature by providing a systematic study based on a corporate time-series dataset.

Published
2022
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15. Innate Immunity in Cancer Biology and Therapy

Author

Yuxia Zhang, Wenjing Xue, Caili Xu, Yanyang Nan, Shuang Mei, Dianwen Ju, Shaofei Wang, and Xuyao Zhang

Subjects
innate immunity, cancer therapy, immune checkpoint inhibitors, chimeric antigen receptors, cytokines, Biology (General), QH301-705.5, Chemistry, QD1-999
Abstract

Immunotherapies including adaptive immune checkpoint inhibitors (ICIs) and chimeric antigen receptor (CAR) T cells, have developed the treatment of cancer in clinic, and most of them focus on activating T cell immunity. Although these strategies have obtained unprecedented clinical responses, only limited subsets of cancer patients could receive long-term benefits, highlighting the demand for identifying novel targets for the new era of tumor immunotherapy. Innate immunity has been demonstrated to play a determinative role in the tumor microenvironment (TME) and influence the clinical outcomes of tumor patients. A thorough comprehension of the innate immune cells that infiltrate tumors would allow for the development of new therapeutics. In this review, we outline the role and mechanism of innate immunity in TME. Moreover, we discuss innate immunity-based cancer immunotherapy in basic and clinical studies. Finally, we summarize the challenges in sufficiently motivating innate immune responses and the corresponding strategies and measures to improve anti-tumor efficacy. This review could aid the comprehension of innate immunity and inspire the creation of brand-new immunotherapies for the treatment of cancer.

Published
2023
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16. Computational Study of Stiffness-Tuning Strategies in Anguilliform Fish

Author

Zuo Cui and Xuyao Zhang

Subjects
anguilliform fish, planar serial-parallel mechanism, stiffness-tuning strategies, swimming speed, Technology
Abstract

Biological evidence demonstrates that fish can tune their body stiffness to improve thrust and efficiency during swimming locomotion. However, the stiffness-tuning strategies that maximize swimming speed or efficiency are still unclear. In the present study, a musculo-skeletal model of anguilliform fish is developed to study the properties of variable stiffness, in which the planar serial-parallel mechanism is used to model the body structure. The calcium ion model is adopted to simulate muscular activities and generate muscle force. Further, the relations among the forward speed, the swimming efficiency, and Young’s modulus of the fish body are investigated. The results show that for certain body stiffness, the swimming speed and efficiency are increased with the tail-beat frequency until reaching the maximum value and then decreased. The peak speed and efficiency are also increased with the amplitude of muscle actuation. Anguilliform fish tend to vary their body stiffness to improve the swimming speed and efficiency at a high tail-beat frequency or small amplitude of muscle actuation. Furthermore, the midline motions of anguilliform fish are analyzed by the complex orthogonal decomposition (COD) method, and the discussions of fish motions associated with the variable body stiffness and the tail-beat frequency are also presented. Overall, the optimal swimming performance of anguilliform fish benefits from the matching relationships among the muscle actuation, the body stiffness, and the tail-beat frequency.

Published
2023
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17. Inhibition of PCSK9 enhances the antitumor effect of PD-1 inhibitor in colorectal cancer by promoting the infiltration of CD8+ T cells and the exclusion of Treg cells

Author

Rui Wang, Hongchuan Liu, Peng He, Duopeng An, Xiaohan Guo, Xuyao Zhang, and Meiqing Feng

Subjects
PD-1, CD8+ T cells, regulatory T cells, tumor microenvironment, PCSK9, Immunologic diseases. Allergy, RC581-607
Abstract

Immunotherapy especially immune checkpoint inhibitors (ICIs) has brought favorable clinical results for numerous cancer patients. However, the efficacy of ICIs in colorectal cancer (CRC) is still unsatisfactory due to the poor median progression-free survival and overall survival. Here, based on the CRC models, we tried to elucidate novel relapse mechanisms during anti-PD-1 therapy. We found that PD-1 blockade elicited a mild antitumor effect in these tumor models with both increased CD8+ T cells and Treg cells. Gene mapping analysis indicated that proprotein convertase subtilisin/kexin type 9 (PCSK9), low-density lipoprotein receptor, transforming growth factor-β (TGF-β), and CD36 were unexpectedly upregulated during PD-1 blockade. To investigate the critical role of these proteins especially PCSK9 in tumor growth, anti-PCSK9 antibody in combination with anti-PD-1 antibody was employed to block PCSK9 and PD-1 simultaneously in CRC. Data showed that neutralizing PCSK9 during anti-PD-1 therapy elicited a synergetic antitumor effect with increased CD8+ T-cell infiltration and inflammatory cytokine releases. Moreover, the proportion of Treg cells was significantly reduced by co-inhibiting PCSK9 and PD-1. Overall, inhibiting PCSK9 can further enhance the antitumor effect of anti-PD-1 therapy in CRC, indicating that targeting PCSK9 could be a promising approach to potentiate ICI efficacy.

Published
2022
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18. Cell Membrane-Derived Vesicle: A Novel Vehicle for Cancer Immunotherapy

Author

Caili Xu, Dianwen Ju, and Xuyao Zhang

Subjects
cellular vesicle, drug delivery vehicle, cancer immunotherapy, combination therapy, membrane hybridization, drug encapsulation, Immunologic diseases. Allergy, RC581-607
Abstract

As nano-sized materials prepared by isolating, disrupting and extruding cell membranes, cellular vesicles are emerging as a novel vehicle for immunotherapeutic drugs to activate antitumor immunity. Cell membrane-derived vesicles inherit the surface characteristics and functional properties of parental cells, thus having superior biocompatibility, low immunogenicity and long circulation. Moreover, the potent antitumor effect of cellular vesicles can be achieved through surface modification, genetic engineering, hybridization, drug encapsulation, and exogenous stimulation. The capacity of cellular vesicles to combine drugs of different compositions and functions in physical space provides a promising vehicle for combinational immunotherapy of cancer. In this review, the latest advances in cellular vesicles as vehicles for combinational cancer immunotherapy are systematically summarized with focuses on manufacturing processes, cell sources, therapeutic strategies and applications, providing an insight into the potential and existing challenges of using cellular vesicles for cancer immunotherapy.

Published
2022
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19. A SIRPαFc Fusion Protein Conjugated With the Collagen-Binding Domain for Targeted Immunotherapy of Non-Small Cell Lung Cancer

Author

Jiayang Liu, Zhefeng Meng, Tongyang Xu, Kudelaidi Kuerban, Songna Wang, Xuyao Zhang, Jiajun Fan, Dianwen Ju, Wenzhi Tian, Xuan Huang, Xiting Huang, Danjie Pan, Huaning Chen, Weili Zhao, and Li Ye

Subjects
SIRPαFc fusion protein, collagen, macrophage, conjugate, cancer immunotherapy, Immunologic diseases. Allergy, RC581-607
Abstract

The SIRPαFc fusion protein can block the immunosuppressive CD47-SIRPα signal between macrophages and tumor cells as a decoy receptor and has demonstrated its immunotherapeutic efficacy in various tumors. However, its clinical application was limited because of the potential hematologic toxicity. The heptapeptide “TKKTLRT” is a collagen-binding domain (CBD) which can bind collagen specifically. Herein, we aim to improve the tumor targeting of SIRPαFc and therefore avoid its unnecessary exposure to normal cells through synthesizing a TKKTLRT–SIRPαFc conjugate. Experiments at molecular and cellular levels indicate that the TKKTLRT–SIRPαFc conjugate-derived collagen-binding affinity and the introduction of CBD did not impact the CD47-binding affinity as well as its phagocytosis-promoting effect on NSCLC cells. In vivo distribution experiments showed that CBD–SIRPαFc accumulated in tumor tissue more effectively compared to unmodified SIRPαFc, probably due to the exposed collagen in the tumor vascular endothelium and stroma resulting from the abnormal vessel structure. On an A549 NSCLC nude mouse xenograft model, CBD–SIRPαFc presented more stable and effective antitumor efficacy than SIRPαFc, along with significantly increased CD11b+F4/80+ macrophages especially MHC II+ M1 macrophages within tumors. All of these results revealed that CBD brought a tumor-targeting ability to the SIRPαFc fusion protein, which contributed to the enhanced antitumor immune response. Altogether, the CBD–SIRPαFc conjugate may have the potential to be an effective tumor immunotherapy with improved antitumor efficacy but less non-tumor-targeted side effect.

Published
2022
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20. Blocking CD47 efficiently potentiated therapeutic effects of anti-angiogenic therapy in non-small cell lung cancer

Author

Xuyao Zhang, Yichen Wang, Jiajun Fan, Wei Chen, Jingyun Luan, Xiaobin Mei, Shaofei Wang, Yubin Li, Li Ye, Song Li, Wenzhi Tian, Kai Yin, and Dianwen Ju

Subjects
Anti-angiogenesis, VEGF, CD47, Immunotherapy, Bispecific therapy, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Abstract Background Inhibitors targeting VEGF and VEGFR are commonly used in the clinic, but only a subset of patients could benefit from these inhibitors and the efficacy was limited by multiple relapse mechanisms. In this work, we aimed to investigate the role of innate immune response in anti-angiogenic therapy and explore efficient therapeutic strategies to enhance efficacy of anti-angiogenic therapy against non-small cell lung cancer (NSCLC). Methods Three NSCLC tumor models with responses to VEGF inhibitors were designed to determine innate immune-related underpinnings of resistance to anti-angiogenic therapy. Immunofluorescence staining, fluorescence-activated cell sorting and immunoblot analysis were employed to reveal the expression of immune checkpoint regulator CD47 in refractory NSCLC. Metastatic xenograft models and VEGFR1-SIRPα fusion protein were applied to evaluate the therapeutic effect of simultaneous disruption of angiogenetic axis and CD47-SIRPα axis. Results Up-regulation of an innate immunosuppressive pathway, CD47, the ligand of the negative immune checkpoint regulator SIRPα (signal regulatory protein alpha), was observed in NSCLC tumors during anti-angiogenic therapy. Further studies revealed that CD47 upregulation in refractory lung tumor models was mediated by TNF-α/NF-κB1 signal pathway. Targeting CD47 could trigger macrophage-mediated elimination of the relapsed NSCLC cells, eliciting synergistic anti-tumor effect. Moreover, simultaneously targeting VEGF and CD47 by VEGFR1-SIRPα fusion protein induced macrophages infiltration and sensitized NSCLC to angiogenesis inhibitors and CD47 blockade. Conclusions Our research provided evidence that CD47 blockade could sensitize NSCLC to anti-angiogenic therapy and potentiate its anti-tumor effects by enhancing macrophage infiltration and tumor cell destruction, providing novel therapeutics for NSCLC by disrupting CD47/SIRPα interaction and angiogenetic axis.

Published
2019
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21. Identification of Peanut AhMYB44 Transcription Factors and Their Multiple Roles in Drought Stress Responses

Author

Yonghui Liu, Yue Shen, Man Liang, Xuyao Zhang, Jianwen Xu, Yi Shen, and Zhide Chen

Subjects
peanut, R2R3-MYB TF, AhMYB44 overexpression, drought stress, transgenic plant, Botany, QK1-989
Abstract

MYB transcription factors (TFs) comprise a large gene family that plays an important role in plant growth, development, stress responses, and defense regulation. However, their functions in peanut remain to be further elucidated. Here, we identified six AhMYB44 genes (AhMYB44-01/11, AhMYB44-05/15, and AhMYB44-06/16) in cultivated peanut. They are typical R2R3-MYB TFs and have many similarities but different expression patterns in response to drought stress, suggesting different functions under drought stress. Homologous genes with higher expression in each pair were selected for further study. All of them were nuclear proteins and had no self-transactivation activity. In addition, we compared the performances of different lines at germination, seedling, and adult stages under drought stress. After drought treatment, the overexpression of AhMYB44-11 transgenic plants resulted in the longest root length at the seedling stage. Levels of proline, soluble sugar and chlorophyll, and expression levels of stress-related genes, including P5CS1, RD29A, CBF1, and COR15A, were higher than those of the wild type (WT) at the adult stage. While the overexpression of AhMYB44-16 significantly increased the drought sensitivity of plants at all stages, with differential ABA content, the expression levels of the ABA-related genes PP2CA and ABI1 were significantly upregulated and those of ABA1 and ABA2 were significantly downregulated compared with the WT. AhMYB44-05 showed similar downregulated expression as AhMYB44-16 under drought stress, but its overexpression in Arabidopsis did not significantly affect the drought resistance of transgenic plants. Based on the results, we propose that AhMYB44-11 plays a role as a positive factor in drought tolerance by increasing the transcription abundance of stress-related genes and the accumulation of osmolytes, while AhMYB44-16 negatively regulates drought tolerance through its involvement in ABA-dependent stress response pathways.

Published
2022
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22. Association and Occurrence of Bifidobacterial Phylotypes Between Breast Milk and Fecal Microbiomes in Mother–Infant Dyads During the First 2 Years of Life

Author

Wenli Yan, Baolong Luo, Xuyao Zhang, Yongqing Ni, and Fengwei Tian

Subjects
human breast milk, mother–infant dyads, microbiome, Bifidobacterium, association, Microbiology, QR1-502
Abstract

Breast milk acts as an intermediary for the transfer of functionally important commensal bacteria from mother to infant, especially for Bifidobacterium that can colonize the infant gut. However, the vast majority of rRNA amplicon-based studies reported the conspicuous intercohort and interindividual variation for the prevalence of Bifidobacterium in breast milk. In order to elucidate whether Bifidobacterium phylotypes persistently co-occured at the species or strain level in mother–breast milk–infant triads, we analyzed collectively the next-generation sequencing (NGS) datasets of bacterial 16S rRNA gene and the Bifidobacterium-specific groEL gene from maternal feces, breast milk, and infant feces in a small yet very homogeneous cohort of 25 healthy Uyghur mother–infant pairs (lactation for 7–720 days) in Kashgar, Xinjiang, China. Overall, 16S rRNA gene analysis showed that microbiome in the newborn gut was closer to that of breast milk in the first 4 months of lactation, and subsequently showed an obvious trend of adulthood at 6–12 months. Based on the BLAST accurate taxonomic result of the representative sequences of all ASVs (amplicon sequencing variants), only three sets of ASVs could be clearly assigned into Bifidobacterium species, whereas the remaining eight sets of ASVs corresponded to four indefinite Bifidobacterium species group. By contrast, the groEL gene dataset was partitioned into 376 ASVs, at least belonging to 13 well-known Bifidobacterium species or subspecies, of which 15 ASVs, annotated to seven well-known Bifidobacterium species or subspecies, showed triadic synchronism in most 23 mother–infant pairs tested. However, several other rare bifidobacterial phylotypes, which were frequently encountered in animals, were found to display no correspondence of the presence between the three ecosystems of mother–infant pairs. Our test results were obviously to support the hypothesis that breast milk acts as an intermediary for the transfer of probiotic commensal bacteria from mother to infant, especially for endosymbiotic Bifidobacterium that can colonize the infant gut. Some oxygen-insensitive exogenous Bifidobacterium phylotypes with a cosmopolitan lifestyle may be indirectly transferred to breast milk and the infant’s intestinal tract through environmental contamination. Thus, the groEL gene proved to be a very effective target for the depth resolution of Bifidobacterium community by high-throughput sequencing technologies.

Published
2021
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23. Influence of Low-Level Jet intensity on aerodynamic loads of horizontal axis wind turbine rotor

Author

Xuyao Zhang, Congxin Yang, and Shoutu Li

Subjects
low-level jet, horizontal axis wind turbine, fast, aerodynamic loads, Engineering (General). Civil engineering (General), TA1-2040
Abstract

High wind speeds associated with Low-Level Jet (LLJ) make wind resources more favorable for wind energy production. However, the aerodynamic loads of large-scale horizontal axis wind turbine (HAWT) rotor under different LLJ inflow conditions have not been thoroughly studied. To gain insight into the aerodynamic loads of rotor under LLJ inflow conditions with different LLJ intensities, a method to establish an engineering LLJ inflow model was proposed according to the plane wall jet theory and Von Karman spectra model with user-defined scaling. The parameters in the engineering LLJ inflow model were determined by comparing the wind speed distribution obtained from the GP_LLJ spectral model, which was summarized from field measurements in the real atmosphere. The LLJ fluctuating wind fields with different intensities generated by the engineering LLJ inflow model were used as the inflow conditions of Fatigue, Aerodynamics, Structures, and Turbulence (FAST) open source code to calculate and analyze the aerodynamic loads of the HAWT. It was found that the engineering LLJ inflow model can be used to establish the LLJ inflow condition of HAWT. When the LLJ height is located at the hub height and LLJ intensity increases from 8 to 16 m/s, the RMS rotor unbalanced aerodynamic load coefficients, including ones of lateral force, longitudinal force, tilt moment and yaw moment are increased by 2.2, 2.13, 1.02 and 0.95 times, respectively.

Published
2019
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24. IL‐22‐mediated renal metabolic reprogramming via PFKFB3 to treat kidney injury

Author

Wei Chen, Yilan Shen, Jiajun Fan, Xian Zeng, Xuyao Zhang, Jingyun Luan, Yichen Wang, Jinghui Zhang, Si Fang, Xiaobin Mei, Zhen Zhao, and Dianwen Ju

Subjects
interleukin‐22, kidney injury, metabolic reprogramming, mitochondrial dysfunction, Medicine (General), R5-920
Abstract

Abstract Kidney damage initiates the deteriorating metabolic states in tubule cells that lead to the development of end‐stage renal disease (ESTD). Interleukin‐22 (IL‐22) is an effective therapeutic antidote for kidney injury via promoting kidney recovery, but little is known about the underlying molecular mechanisms. Here, we first provide evidence that IL‐22 attenuates kidney injury via metabolic reprogramming of renal tubular epithelial cells (TECs). Specifically, our data suggest that IL‐22 regulates mitochondrial function and glycolysis in damaged TECs. Further observations indicate that IL‐22 alleviates the accumulation of mitochondrial reactive oxygen species (ROS) and dysfunctional mitochondria via the induction of AMPK/AKT signaling and PFBFK3 activities. In mice, amelioration of kidney injury and necrosis and improvement of kidney functions via regulation of these metabolism relevant signaling and mitochondrial fitness of recombinant IL‐22 are certificated in cisplatin‐induced kidney damage and diabetic nephropathy (DN) animal models. Taken together, our findings unravel new mechanistic insights into protective effects of IL‐22 on kidneys and highlight the therapeutic opportunities of IL‐22 and the involved metabolic regulators in various kidney diseases.

Published
2021
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25. The Composition and Concordance of Lactobacillus Populations of Infant Gut and the Corresponding Breast-Milk and Maternal Gut

Author

Xuyao Zhang, Saiyidan Mushajiang, Baolong Luo, Fengwei Tian, Yongqing Ni, and Wenli Yan

Subjects
Lactobacillus populations, mother-breast milk-infant “triad, ” composition and concordance, selective media, molecular methods, Microbiology, QR1-502
Abstract

The maternal gut is the principal source of commensal bacteria in the infant gut during the lactation stage, where breast milk acts as an intermediary for the transfer of potential probiotic bacteria consortia, including Lactobacillus. This study aimed to characterize the bacterial communities in human milk, maternal, and infant feces in a small yet very homogeneous cohort of 25 healthy mother–infant pairs in northwestern China (n = 25, infant age from 7 days to 2 years), with special emphasis on the cooccurrence and vertical transfer of Lactobacillus phylotypes at the species or strain level in mother-breast milk-infant triads. Accurate sequencing analysis revealed that among 73 Lactobacillus zero-radius operational classification units (ZOTUs) identified, 58 belonging to 18 recognized species or species groups were distributed in all three types of samples. Lactobacillus ruminis, L. mucosae and L. gasseri-johnsonii as true residents were the most represented in all three ecosystems, whereas the content of Lactobacillus phylotypes commonly developed as probiotics was not dominant. While the numbers of Lactobacillus species in breast milk and infant feces were greater than that in maternal feces, principal coordinates analysis (PCoA) based on beta diversity, coupled with the frequency of isolates determined by culture methods, showed that the Lactobacillus community in the infant gut was more similar to that in the maternal gut than to that in breast milk, suggesting that the gut is niche selective for Lactobacillus populations. In addition, identical strains of L. ruminis, L. paracasei, L. mucosae and L. salivarius were isolated from multiple mother–infant pairs, supporting the hypothesis that vertical transfer of bacteria via breastfeeding contributes to the initial establishment of the microbiota in the developing infant intestine.

Published
2020
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26. An Ecological Development Level Evaluation of the Forestry Industry in China Based on a Hybrid Ensemble Approach

Author

Dayu Xu, Chunping Lu, and Xuyao Zhang

Subjects
ecological development, forestry industry, synthetic evaluation, system coordination degree, Plant ecology, QK900-989
Abstract

The straits of ecological development in the forestry industry and the problems existing in the industrial forestry system are currently the main focus of policy-making research in China, to alleviate the contradiction between forestry economic development and the ecological environment, as well as evaluate the level and trend of the ecological development in China’s forestry industry. This paper analyzed the status of ecological development in China’s forestry industry via public data, constructed a novel evaluation index system for forestry industrial ecological development, and proposed a hybrid ensemble approach combined with principal component analysis, entropy weights, and fuzzy-DEMATEL to synthetically evaluate the ecological development level and system coordination of the forestry industry in each province of China. The experimental results show that technological innovation ability is the most significant restriction for the ecological development of China’s forestry industry. Obvious regional differences in the promotion degree of ecological development and the coordination of various elements throughout the country has also been confirmed. Findings of our research could be used for promoting the green transformation and upgrading of the forestry industry, and providing targeted practical countermeasures according to local conditions for governments at all levels.

Published
2021
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27. Interleukin-22 Attenuated Renal Tubular Injury in Aristolochic Acid Nephropathy via Suppressing Activation of NLRP3 Inflammasome

Author

Shaofei Wang, Jiajun Fan, Xiaobin Mei, Jingyun Luan, Yubin Li, Xuyao Zhang, Wei Chen, Yichen Wang, Guangxun Meng, and Dianwen Ju

Subjects
IL-22, aristolochic acid nephropathy, NLRP3 inflammasome, tubular injury, renal function, Immunologic diseases. Allergy, RC581-607
Abstract

Aristolochic acid nephropathy (AAN), as a rapidly progressive interstitial nephropathy due to excessive ingestion of aristolochia herbal medications, has recently raised considerable concerns among clinicians and researchers as its underlying pathogenic mechanisms are largely unclear. In the current study, we identified NLRP3 inflammasome activation as a novel pathological mechanism of AAN. We found that NLRP3 inflammasome was aberrantly activated both in vivo and in vitro after AA exposure. Blockade of IL-1β and NLRP3 inflammasome activation by IL-1Ra significantly attenuated renal tubular injury and function loss in AA-induced nephropathy. Moreover, NLRP3 or Caspase-1 deficiency protected against renal injury in the mouse model of acute AAN, suggesting that the NLRP3 signaling pathway was probably involved in the pathogenesis of AAN. We also found that administration of IL-22 could markedly attenuate renal tubular injury in AAN. Notably, IL-22 intervention significantly alleviated renal fibrosis and dysfunction in AA-induced nephropathy. Furthermore, IL-22 largely inhibited renal activation of NLRP3 inflammasome in AA-induced nephropathy. These results indicated that IL-22 ameliorated renal tubular injury in AAN through suppression of NLRP3 inflammasome activation. In summary, this study identified renal activation of NLRP3 inflammasome as a novel mechanism underlying the pathogenesis of AAN, thus providing a potential therapeutic strategy for AAN based on suppression of NLRP3 inflammasome activation.

Published
2019
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28. Activating Autophagy Enhanced the Antitumor Effect of Antibody Drug Conjugates Rituximab-Monomethyl Auristatin E

Author

Yichen Wang, Xuyao Zhang, Jiajun Fan, Wei Chen, Jingyun Luan, Yanyang Nan, Shaofei Wang, Qicheng Chen, Yujie Zhang, Youling Wu, and Dianwen Ju

Subjects
non-Hodgkin lymphoma, antibody drug conjugates, autophagy, apoptosis, combination therapy, Immunologic diseases. Allergy, RC581-607
Abstract

BackgroundAntibody drug conjugate (ADC) showed potent therapeutic efficacy in several types of cancers. The role of autophagy in antitumor effects of ADC remains unclear.MethodsIn this study, the ADC, Rituximab-monomethyl auristatin E (MMAE) with a Valine–Citrulline cleavable linker, was designed to investigate its therapeutic efficacy against non-Hodgkin lymphoma (NHL) as well as the underlying mechanisms. Methylthiazolyldiphenyl-tetrazolium bromide (MTT) was used to detect growth inhibition in B-cell lymphoma cell lines, Ramos and Daudi cells, which were treated by Rituximab-MMAE alone or combined with autophagy conditioner. Apoptosis was detected by flow cytometry and immunohistochemistry, and apoptosis inhibitor was employed to discover the relationship between autophagy and apoptosis during the Rituximab-MMAE treatment. Autophagy was determined by three standard techniques which included confocal microscope, transmission electron microscope, and western blots. Ramos xenograft tumors in BALB/c nude mice were established to investigate the antitumor effect of combination use of Rituximab-MMAE and autophagy conditioner in B-NHL therapy.ResultsOur results showed that Rituximab-MMAE elicited caspase-3-dependent apoptosis in NHL cells and exhibited potent therapeutic efficacy in vivo. Autophagy, which was characterized by upregulated light chain 3-II expression, and accumulation of autophagosomes, was triggered during the Rituximab-MMAE treatment. Meanwhile, inactivation of Akt/mTOR pathway was shown to be involved in the autophagy triggered by Rituximab-MMAE, indicating a probable mechanism of the ADC-initiated autophagy. Importantly, inhibition of autophagy by chloroquine suppressed the Rituximab-MMAE-induced apoptosis, while activating autophagy by rapamycin significantly enhanced the therapeutic effect of Rituximab-MMAE both in vitro and in vivo.ConclusionOur data elucidated the critical relationship between autophagy and apoptosis in Rituximab-MMAE-based therapy and highlighted the potential approach for NHL therapy by combined administration of the ADC and autophagy activator.

Published
2018
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29. NOD-Like Receptor Protein 3 Inflammasome-Dependent IL-1β Accelerated ConA-Induced Hepatitis

Author

Jingyun Luan, Xuyao Zhang, Shaofei Wang, Yubin Li, Jiajun Fan, Wei Chen, Wenjing Zai, Sijia Wang, Yichen Wang, Mingkuan Chen, Guangxun Meng, and Dianwen Ju

Subjects
NOD-like receptor protein 3 inflammasome, IL-1β, caspase-1, pyroptosis, autoimmune hepatitis, Immunologic diseases. Allergy, RC581-607
Abstract

Autoimmune hepatitis (AIH) is a progressive inflammatory disorders of unknown etiology, characterized by immune-mediated destruction of hepatocytes and massive production of cytokines. Interleukin-1β is a pleiotropic proinflammatory cytokine and well known to be critical in a variety of autoimmune diseases. However, the role of interleukin-1β (IL-1β) in AIH is still indistinct. Here, we first investigated the significance of NOD-like receptor protein 3 (NLRP3) inflammasome-dependent IL-1β in the pathogenesis of AIH with a murine model of immune-mediated hepatitis induced by Concanavalin A (ConA). In ConA-treated mice, pathogenic elevated NLRP3, Cleaved caspase-1 and IL-1β levels, as well as an inflammatory cell death known as pyroptosis predominantly occurred in the livers. Strikingly, NLRP3−/− and caspase-1−/− mice were broadly protected from hepatitis as determined by decreased histological liver injury, serum aminotransferase (ALT)/aspartate transaminase levels, and pyroptosis. In vivo intervention with recombinant human interleukin-1 receptor antagonist (rhIL-1Ra) strongly suppressed ConA-induced hepatitis by decreasing tumor necrosis factor-alpha (TNF-α) and interleukin-17 (IL-17) secretion, and inflammatory cell infiltration into livers. Additionally, rhIL-1Ra-pretreated mice developed significantly reduced NLRP3 inflammasome activation and reactive oxygen species (ROS) generation. Scavenging of ROS by N-acetyl-cysteine also attenuated NLRP3 inflammasome activation and liver inflammation, indicating that the essential role of ROS in mediating NLRP3 inflammasome activation in ConA-induced hepatitis. In conclusion, our results demonstrated that NLRP3 inflammasome-dependent IL-1β production was crucial in the pathogenesis of ConA-induced hepatitis, which shed light on the development of promising therapeutic strategies for AIH by blocking NLRP3 inflammasome and IL-1β.

Published
2018
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30. Influence of the Heights of Low-Level Jets on Power and Aerodynamic Loads of a Horizontal Axis Wind Turbine Rotor

Author

Xuyao Zhang, Congxin Yang, and Shoutu Li

Subjects
low-level jet, horizontal axis wind turbine, FAST, rotor power, aerodynamic load, Meteorology. Climatology, QC851-999
Abstract

The influence of the heights of low-level jets (LLJs) on the rotor power and aerodynamic loads of a horizontal axis wind turbine were investigated using the fatigue, aerodynamics, structures, and turbulence code. The LLJ and shear inflow wind fields were generated using an existing wind speed spectral model. We found that the rotor power predicted by the average wind speed of the hub height is higher than the actual power in relatively weak and shallow LLJ inflow conditions, especially when the LLJ height is located inside the rotor-swept area. In terms of aerodynamic loads, when the LLJ height is located inside the rotor-swept area, the root mean square (RMS) rotor thrust coefficient and torque coefficient increase, while the RMS rotor unbalanced aerodynamic load coefficients, including lateral force, longitudinal force, tilt moment, and yaw moment, decreased. This means that the presence of both positive and negative wind shear in the rotor-swept area not only increases the rotor power but also reduces the unbalanced aerodynamic loads, which is beneficial to the operation of wind turbine. Power spectrum analysis shows no obvious difference in the power spectrum characteristics of the rotor torque and thrust in LLJ inflow conditions with different heights.

Published
2019
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33. Design and Testing of a LUT Airfoil for Straight-Bladed Vertical Axis Wind Turbines

Author

Shoutu Li, Ye Li, Congxin Yang, Xuyao Zhang, Qing Wang, Deshun Li, Wei Zhong, and Tongguang Wang

Subjects
airfoil design, aerodynamic, wind tunnel experiment, VAWTs (Vertical axis wind turbines), Technology, Engineering (General). Civil engineering (General), TA1-2040, Biology (General), QH301-705.5, Physics, QC1-999, Chemistry, QD1-999
Abstract

The airfoil plays an important role in improving the performance of wind turbines. However, there is less research dedicated to the airfoils for Vertical Axis Wind Turbines (VAWTs) compared to the research on Horizontal Axis Wind Turbines (HAWTs). With the objective of maximizing the aerodynamic performance of the airfoil by optimizing its geometrical parameters and by considering the law of motion of VAWTs, a new airfoil, designated the LUT airfoil (Lanzhou University of Technology), was designed for lift-driven VAWTs by employing the sequential quadratic programming optimization method. Afterwards, the pressure on the surface of the airfoil and the flow velocity were measured in steady conditions by employing wind tunnel experiments and particle image velocimetry technology. Then, the distribution of the pressure coefficient and aerodynamic loads were analyzed for the LUT airfoil under free transition. The results show that the LUT airfoil has a moderate thickness (20.77%) and moderate camber (1.11%). Moreover, compared to the airfoils commonly used for VAWTs, the LUT airfoil, with a wide drag bucket and gentle stall performance, achieves a higher maximum lift coefficient and lift⁻drag ratios at the Reynolds numbers 3 × 105 and 5 × 105.

Published
2018
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34. Research on Fatigue Damage Behavior of Main Beam Sub-Structure of Composite Wind Turbine Blade.

Author

Haixia Kou, Bowen Yang, Xuyao Zhang, Xiaobo Yang, and Haibo Zhao

Subjects
WIND turbine blades, LAMINATED materials, THREE-dimensional imaging, DEAD loads (Mechanics), COMPUTER simulation
Abstract

Given the difficulty in accurately evaluating the fatigue performance of large composite wind turbine blades (referred to as blades), this paper takes the main beam structure of the blade with a rectangular cross-section as the simulation object and establishes a composite laminate rectangular beam structure that simultaneously includes the flange, web, and adhesive layer, referred to as the blade main beam sub-structure specimen, through the definition of blade sub-structures. This paper examines the progressive damage evolution law of the composite laminate rectangular beam utilizing an improved 3D Hashin failure criterion, cohesive zone model, B-K failure criterion, and computer simulation technology. Under static loading, the layup angle of the anti-shear web has a close relationship with the static load-carrying capacity of the composite laminate rectangular beam; under fatigue loading, the fatigue damage will first occur in the lower flange adhesive area of the whole composite laminate rectangular beam and ultimately result in the fracture failure of the entire structure. These results provide a theoretical reference and foundation for evaluating and predicting the fatigue performance of the blade main beam structure and even the full-size blade. [ABSTRACT FROM AUTHOR]

Published
2024
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35. Predicting Multidimensional Environmental Factor Trends in Greenhouse Microclimates Using a Hybrid Ensemble Approach

Author

Dayu Xu, Lei Ren, and Xuyao Zhang

Subjects
Article Subject, Control and Systems Engineering, Electrical and Electronic Engineering, Instrumentation
Abstract

Trend prediction of greenhouse microclimate is crucial, as greenhouse crops are vulnerable to potential losses resulting from dramatic changes in greenhouse microclimate. Consequently, a precise greenhouse microclimate predictive model is required that can predict trends in greenhouse microclimates several weeks in advance to avoid financial losses. In the present study, we proposed a hybrid ensemble approach to predict greenhouse microclimate based on an Informer model that is optimized using improved empirical mode decomposition (IEMD). The dataset was decomposed using IEMD, and then all the decomposed datasets were predicted using the Informer model. Afterward, the predictions were combined. In the present study, five different environmental factor datasets of CO2 concentration, atmospheric pressure, light intensity, temperature, and humidity were predicted. The performance of the IEMD-Informer model was compared with other modeling approaches. The results demonstrate that the proposed method has outstanding performance and can predict the greenhouse microclimate environmental factors more accurately.

Published
2023

36. NPASS database update 2023: quantitative natural product activity and species source database for biomedical research

Author

Hui Zhao, Yuan Yang, Shuaiqi Wang, Xue Yang, Kaicheng Zhou, Caili Xu, Xuyao Zhang, Jiajun Fan, Dongyue Hou, Xingxiu Li, Hanbo Lin, Ying Tan, Shanshan Wang, Xin-Yi Chu, Dongzhi Zhuoma, Fengying Zhang, Dianwen Ju, Xian Zeng, and Yu Zong Chen

Subjects
Genetics
Abstract

Quantitative activity and species source data of natural products (NPs) are important for drug discovery, medicinal plant research, and microbial investigations. Activity values of NPs against specific targets are useful for discovering targeted therapeutic agents and investigating the mechanism of medicinal plants. Composition/concentration values of NPs in individual species facilitate the assessments and investigations of the therapeutic quality of herbs and phenotypes of microbes. Here, we describe an update of the NPASS natural product activity and species source database previously featured in NAR. This update includes: (i) new data of ∼95 000 records of the composition/concentration values of ∼1 490 NPs/NP clusters in ∼390 species, (ii) extended data of activity values of ∼43 200 NPs against ∼7 700 targets (∼40% and ∼32% increase, respectively), (iii) extended data of ∼31 600 species sources of ∼94 400 NPs (∼26% and ∼32% increase, respectively), (iv) new species types of ∼440 co-cultured microbes and ∼420 engineered microbes, (v) new data of ∼66 600 NPs without experimental activity values but with estimated activity profiles from the established chemical similarity tool Chemical Checker, (vi) new data of the computed drug-likeness properties and the absorption, distribution, metabolism, excretion and toxicity (ADMET) properties for all NPs. NPASS update version is freely accessible at http://bidd.group/NPASS.

Published
2022

39. Improved Data Stream Clustering Method: Incorporating KD-Tree for Typicality and Eccentricity-Based Approach.

Author

Dayu Xu, Jiaming Lü, Xuyao Zhang, and Hongtao Zhang

Subjects
SEARCH algorithms, DATA analysis, SCAPEGOAT
Abstract

Data stream clustering is integral to contemporary big data applications. However, addressing the ongoing influx of data streams efficiently and accurately remains a primary challenge in current research. This paper aims to elevate the efficiency and precision of data stream clustering, leveraging the TEDA (Typicality and Eccentricity Data Analysis) algorithm as a foundation, we introduce improvements by integrating a nearest neighbor search algorithm to enhance both the efficiency and accuracy of the algorithm. The original TEDA algorithm, grounded in the concept of "Typicality and Eccentricity Data Analytics", represents an evolving and recursive method that requires no prior knowledge. While the algorithm autonomously creates and merges clusters as new data arrives, its efficiency is significantly hindered by the need to traverse all existing clusters upon the arrival of further data. This work presents the NS-TEDA (Neighbor Search Based Typicality and Eccentricity Data Analysis) algorithm by incorporating a KD-Tree (K-Dimensional Tree) algorithm integrated with the Scapegoat Tree. Upon arrival, this ensures that new data points interact solely with clusters in very close proximity. This significantly enhances algorithmefficiencywhile preventing a single data point fromjoining too many clusters andmitigating the merging of clusters with high overlap to some extent. We apply the NS-TEDA algorithm to several well-known datasets, comparing its performance with other data stream clustering algorithms and the original TEDA algorithm. The results demonstrate that the proposed algorithm achieves higher accuracy, and its runtime exhibits almost linear dependence on the volume of data, making it more suitable for large-scale data stream analysis research. [ABSTRACT FROM AUTHOR]

Published
2024
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45. Introduction

Author

Paul Cheung, Ammu George, and Xuyao Zhang

Published
2023

47. Data from Protein Kinase C Alpha is a Central Node for Tumorigenic Transcriptional Networks in Human Prostate Cancer

Author

Marcelo G. Kazanietz, Martin C. Abba, Michael D. Feldman, Reba E. Daniel, Priti Lal, Evgeniy Eruslanov, Suli Zhang, Xuyao Zhang, and Mariana Cooke

Abstract

Aberrant expression of protein kinase C (PKC) isozymes is a hallmark of cancer. The different members of the PKC family control cellular events associated with cancer development and progression. Whereas the classical/conventional PKCα isozyme has been linked to tumor suppression in most cancer types, here we demonstrate that this kinase is required for the mitogenic activity of aggressive human prostate cancer cells displaying aberrantly high PKCα expression. IHC analysis showed abnormal upregulation of PKCα in human primary prostate tumors. Interestingly, silencing PKCα expression from aggressive prostate cancer cells impairs cell-cycle progression, proliferation, and invasion, as well as their tumorigenic activity in a mouse xenograft model. Mechanistic analysis revealed that PKCα exerts a profound control of gene expression, particularly over genes and transcriptional networks associated with cell-cycle progression and E2F transcription factors. PKCα RNAi depletion from PC3 prostate cancer cells led to a reduction in the expression of proinflammatory cytokine and epithelial-to-mesenchymal transition (EMT) genes, as well as a prominent downregulation of the immune checkpoint ligand PD-L1. This PKCα-dependent gene expression profile was corroborated in silico using human prostate cancer databases. Our studies established PKCα as a multifunctional kinase that plays pleiotropic roles in prostate cancer, particularly by controlling genetic networks associated with tumor growth and progression. The identification of PKCα as a protumorigenic kinase in human prostate cancer provides strong rationale for the development of therapeutic approaches toward targeting PKCα or its effectors.Significance:PKCα was found to be aberrantly expressed in human prostate cancer. Silencing the expression of this kinase from aggressive prostate cancer cell lines reduces their proliferative, tumorigenic, and invasive properties. In addition, our findings implicate PKCα as a major node for transcriptional regulation of tumorigenic, inflammatory, and EMT networks in prostate cancer, highlighting its potential relevance as a therapeutic target.

Published
2023

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