Your search keyword '"Qinhuai Lai"' showing total 20 results

1. FTL004, an anti-CD38 mAb with negligible RBC binding and enhanced pro-apoptotic activity, is a novel candidate for treatments of multiple myeloma and non-Hodgkin lymphoma

Author

Guangbing Zhang, Cuiyu Guo, Yan Wang, Xianda Zhang, Shuang Liu, Wen Qu, Chunxia Chen, Lingli Yan, Zhouning Yang, Zhixiong Zhang, Xiaohua Jiang, Xiaofeng Chen, Hong Liu, Qinhuai Lai, Xian Wei, Ying Lu, Shengyan Zhao, Han Deng, Yuxi Wang, Lin Yu, Hongbin Yu, Yu Wu, Zhaoming Su, Pengyu Chen, Ziqing Ren, Meng Yu, Feng Qu, Yong Luo, Lantu Gou, Qing Li, Ying Huang, Fanxin Ma, and Jinliang Yang

Subjects

Multiple myeloma, Monoclonal antibodies, CD38, Red blood cells, Direct apoptosis, Diseases of the blood and blood-forming organs, RC633-647.5, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Anti-CD38 monoclonal antibodies (mAbs), daratumumab, and isatuximab have represented a breakthrough in the treatment of multiple myeloma (MM). Recently, CD38-based mAbs were expected to achieve increasing potential beyond MM, which encouraged us to develop new anti-CD38 mAbs to meet clinical needs. In this study, we developed a novel humanized anti-CD38 antibody, FTL004, which exhibited enhanced pro-apoptotic ability and negligible binding to red blood cells (RBCs). FTL004 presented a better ability to induce direct apoptosis independent of Fc-mediated cross-linking against lymphoma and MM cell lines as well as primary myeloma cells derived from MM patients. For instance, FTL004 induced RPMI 8226 cells with 55% early apoptosis cells compared with 20% in the isatuximab-treated group. Of interest, FTL004 showed ignorable binding to CD38 on human RBCs in contrast to tumor cells, even at concentrations up to 30 μg/mL. Furthermore, with an engineered Fc domain, FTL004 displayed stronger antibody-dependent cellular cytotoxicity (ADCC) against CD38+ malignant cells. In vivo MM and non-Hodgkin lymphoma tumor xenograft models showed that FTL004 possessed an effective anti-tumor effect. Cryo-electron microscopy structure resolved two epitope centers of FTL004 on CD38: one of which was unique while the other partly overlapped with that of isatuximab. Taken together, FTL004 distinguishes it from other CD38 targeting mAbs and represents a potential candidate for the treatment of MM and non-Hodgkin lymphoma.

Published

2022

2. Combination Foretinib and Anti-PD-1 Antibody Immunotherapy for Colorectal Carcinoma

Author

Yuyin Fu, Yujia Peng, Shengyan Zhao, Jun Mou, Lishi Zeng, Xiaohua Jiang, Chengli Yang, Cheng Huang, Yuyan Li, Yin Lu, Mengdan Wu, Yanfang Yang, Ting Kong, Qinhuai Lai, Yangping Wu, Yuqin Yao, Yuxi Wang, Lantu Gou, and Jinliang Yang

Subjects

foretinib, anti-PD-1, combination therapy, immunotherapy, tumor microenvironment, colon cancer, Biology (General), QH301-705.5

Abstract

Immune checkpoint inhibitors have achieved unprecedented success in cancer immunotherapy. However, the overall response rate to immune checkpoint inhibitor therapy for many cancers is only between 20 and 40%, and even less for colorectal cancer (CRC) patients. Thus, there is an urgent need to develop an efficient immunotherapeutic strategy for CRC. Here, we developed a novel CRC combination therapy consisting of a multiple receptor tyrosine kinase inhibitor (Foretinib) and anti-PD-1 antibody. The combination therapy significantly inhibited tumor growth in mice, led to improved tumor regression without relapse (83% for CT26 tumors and 50% for MC38 tumors) and prolonged overall survival. Mechanistically, Foretinib caused increased levels of PD-L1 via activating the JAK2-STAT1 pathway, which could improve the effectiveness of the immune checkpoint inhibitor. Moreover, the combination therapy remodeled the tumor microenvironment and enhanced anti-tumor immunity by further increasing the infiltration and improving the function of T cells, decreasing the percentage of tumor-associated macrophages (TAMs) and inhibiting their polarization toward the M2 phenotype. Furthermore, the combination therapy inhibited the metastasis of CT26-Luc tumors to the lung in BALB/c mouse by reducing proportions of regulatory T-cells, TAMs and M2 phenotype TAMs in their lungs. This study suggests that a novel combination therapy utilizing both Foretinib and anti-PD-1 antibody could be an effective combination strategy for CRC immunotherapy.

Published

2021

3. Targeting of DDR1 with antibody‐drug conjugates has antitumor effects in a mouse model of colon carcinoma

Author

Yiran Tao, Ruixue Wang, Qinhuai Lai, Mengdan Wu, Yuxi Wang, Xiaohua Jiang, Lishi Zeng, Shijie Zhou, Zhongping Li, Tinghan Yang, Yuqin Yao, Yangping Wu, Lin Yu, Yuyin Fu, Weirong Lai, Yujia Peng, Ying Lu, Zhixiong Zhang, Cuiyu Guo, Guangbing Zhang, Lantu Gou, and Jinliang Yang

Subjects

antibody‐drug conjugate, colon cancer, receptor tyrosine kinase, resistance, xenograft tumor model, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

DDR1 has been identified as a cancer‐associated receptor tyrosine kinase that is highly expressed in several malignancies relative to normal tissues. Clinically approved multi‐kinase inhibitors, such as nilotinib, inhibit DDR1‐mediated tumor growth in xenograft models, suggesting DDR1 might be a potential target for cancer treatments. Here, we employed an antibody‐based strategy with a novel anti‐DDR1 antibody‐drug conjugate (ADC) for colon carcinoma treatment. We developed T4H11‐DM4, an ADC targeting DDR1 which carries the tubulin inhibitor payload DM4. Immunohistochemical analysis of a tissue microarray containing 100 colon cancer specimens revealed that DDR1 was highly expressed in 81% of tumor tissues. Meanwhile, high expression of DDR1 was associated with poor survival in patients. In vitro, T4H11‐DM4 exhibited potent anti‐proliferative activity with half maximal inhibitory concentration (IC50) values in the nanomolar range in a panel of colon cancer cell lines. In vivo, the antitumor efficacy of T4H11‐DM4 was evaluated in three colon cancer cell lines expressing different levels of DDR1. T4H11‐DM4 achieved complete tumor regression at doses of 5 and 10 mg·kg−1 in HT‐29 and HCT116 tumor models. Moreover, a correlation between in vivo efficacy of T4H11‐DM4 and the levels of DDR1 expression on the cell surface was observed. Tumor cell proliferation was caused by the induction of mitotic arrest, indicating that the antitumor effect in vivo was mediated by DM4. In addition, T4H11‐DM4 was efficacious in oxaliplatin‐resistant colon cancer models. In exploratory safety studies, T4H11‐DM4 exhibited no overt toxicities when multi‐doses were administered at 10 mg·kg−1 into BALB/c nude mice or when a single dose up to 50 mg·kg−1 was administered into BALB/c mice. Overall, our findings highlight the potential of DDR1‐targeted ADC and may facilitate the development of a new effective therapeutic strategy for colon cancer.

Published

2019

4. Serum Metabolic Profiling Analysis of Chronic Gastritis and Gastric Cancer by Untargeted Metabolomics

Author

Lin Yu, Qinhuai Lai, Qian Feng, Yuanmeng Li, Jiafu Feng, and Bei Xu

Subjects

chronic gastritis, gastric cancer, untargeted metabolomics, lipid metabolism, candidate biomarkers, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

PurposeGastric cancer is a common tumor of the digestive system. Identification of potential molecules associated with gastric cancer progression and validation of potential biomarkers for gastric cancer diagnosis are very important. Thus, the aim of our study was to determine the serum metabolic characteristics of the serum of patients with chronic gastritis (CG) or gastric cancer (GC) and validate candidate biomarkers for disease diagnosis.Experimental DesignA total of 123 human serum samples from patients with CG or GC were collected for untargeted metabolomic analysis via UHPLC-Q-TOF/MS to determine characteristics of the serum. Principal component analysis (PCA), partial least squares discriminant analysis (PLS-DA), and heat map were used for multivariate analysis. In addition, commercial databases were used to identify the pathways of metabolites. Differential metabolites were identified based on a heat map with a t-test threshold (p < 0.05), fold-change threshold (FC > 1.5 or FC < 2/3) and variable importance in the projection (VIP >1). Then, differential metabolites were analyzed by receiver operating characteristic (ROC) curve to determine candidate biomarkers. All samples were analyzed for fasting lipid profiles.ResultsAnalysis of serum metabolomic profiles indicated that most of the altered metabolic pathways in the three groups were associated with lipid metabolism (p < 0.05) and lipids and lipid-like molecules were the predominating metabolites within the top 100 differential metabolites (p < 0.05, FC > 1.5 or FC < 2/3, and VIP >1). Moreover, differential metabolites, including hexadecasphinganine, linoleamide, and N-Hydroxy arachidonoyl amine had high diagnostic performance according to PLS-DA. In addition, fasting lipid profile analysis showed the serum levels of total cholesterol (TC), high-density lipoprotein cholesterol (HDL-C) and apolipoprotein A1 (Apo-A1) were decreased concomitant to the progression of the progression of the disease compared with those in the control group (p < 0.05).ConclusionsThus, this study demonstrated that lipid metabolism may influence the development of CG to GC. Hexadecasphinganine, linoleamide, and N-Hydroxy arachidonoyl amine were selected as candidate diagnostic markers for CG and GC.

Published

2021

5. Comparative RNA-sequencing profiled the differential gene expression of liver in response to acetyl-CoA carboxylase inhibitor GS-0976 in a mouse model of NASH

Author

Ying Lu, Xiaolan Su, Manyu Zhao, Qianru Zhang, Chuang Liu, Qinhuai Lai, Sijia Wu, Aiping Fang, Jinliang Yang, Xiaoxin Chen, and Yuqin Yao

Subjects

Transcriptome, RNA-Seq, Non-alcoholic steatohepatitis, Acetyl-CoA carboxylase inhibitor, Medicine, Biology (General), QH301-705.5

Abstract

Background Non-alcoholic steatohepatitis (NASH) is a progressive liver disease characterized by hepatic steatosis, lobular inflammation and fibrosis. Acetyl-CoA carboxylase (ACC) isoform 1 and 2 involved in de novo lipogenesis (DNL) and fatty acid oxidation have been identified as a therapeutic target in NASH. GS-0976, the inhibitor of ACC1 and ACC2, has achieved favorable therapeutic effects in clinical trials with NASH. The purpose of this study was to explore the transcriptional alterations regulated by GS-0976 in NASH. Methods C57BL/6 mice were fed on a choline-deficient, L-amino acid-defined, high-fat diet (CDAHFD) or normal diet for 12 weeks. Mice were treated with or without GS-0976 (3 mg/kg per day) in the last 8 weeks. Oil Red O, Haematoxylin-eosin (H & E), and Sirius Red were used to evaluate hepatic steatosis, inflammation and fibrosis. The comparative RNA-sequencing was conducted to analyse the hepatic gene expression profiles in mice. Reverse transcription–polymerase chain reaction analysis was performed to validate the differential expression of representative genes. Results GS-0976 attenuated the steatosis, inflammation, and fibrosis of NASH in CDAHFD mouse model. High-throughput sequencing and differential gene expression analysis showed that there were 516 up-regulated genes and 525 down-regulated genes after GS-0976 treatment. Genes involved in the metabolic process, extracellular matrix formation, immune response, and angiogenesis were significantly enriched. The “Metabolic pathways” and “ECM-receptor interaction” pathways were the most significantly enriched KEGG pathways in the up-regulated and down-regulated differentially expressed genes (DEGs), respectively. Conclusions Transcriptome analysis showed that GS-0976 could regulate the expression of genes related to metabolism, inflammation and fibrosis in NASH. The global transcriptomic changes in gene expression promote the further understanding for the inhibition mechanisms of GS-0976 in NASH.

Published

2019

6. Filamin A is overexpressed in non-alcoholic steatohepatitis and contributes to the progression of inflammation and fibrosis

Author

Ying Lu, Mengzhu Wang, Manyu Zhao, Qianru Zhang, Rui Qian, Zan Hu, Qi Ke, Lin Yu, Liqun Wang, Qinhuai Lai, Zhenmi Liu, Xia Jiang, Ben Zhang, Jinliang Yang, and Yuqin Yao

Subjects

Biophysics, Cell Biology, Molecular Biology, Biochemistry

Published

2023

7. Design, Synthesis, and Bioevaluation of a Novel Hybrid Molecular Pyrrolobenzodiazepine-Anthracenecarboxyimide as a Payload for Antibody-Drug Conjugate

Author

Weirong Lai, Shengyan Zhao, Qinhuai Lai, Wei Zhou, Mengdan Wu, Xiaohua Jiang, Xin Wang, Yujia Peng, Xian Wei, Liang Ouyang, Lantu Gou, Hao Chen, Yuxi Wang, and Jinliang Yang

Subjects

Benzodiazepines, Mice, Immunoconjugates, Receptor, ErbB-2, Cell Line, Tumor, Drug Discovery, Molecular Medicine, Animals, Humans, Pyrroles, Trastuzumab, Xenograft Model Antitumor Assays

Abstract

A novel series of hybrid molecules combining pyrrolobenzodiazepine (PBD) and anthracenecarboxyimide pharmacophores were designed, synthesized, and tested for

Published

2022

8. Chemokine Ligand 13 Expression is Abundant in the Tumor Microenvironment and Indicates Poor Prognosis of Kidney Clear Cell Carcinoma

Author

Zhixiong Zhang, Shengyan Zhao, Mengyao Sun, Jinliang Yang, Yuyin Fu, Weirong Lai, Yin Lu, Shijie Zhou, Mengdan Wu, Yuyan Li, Qinhuai Lai, Yujia Peng, Fan Qiao, Gou Lantu, Xiaofeng Chen, Lishi Zeng, and Yiwen Zhang

Subjects

Chemokine, Poor prognosis, Tumor microenvironment, biology, biology.protein, Cancer research, Kidney Clear Cell Carcinoma, General Medicine, Ligand (biochemistry)

Published

2021

9. Opportunities and obstacles of targeted therapy and immunotherapy in small cell lung cancer

Author

Lantu Gou, Jiafu Feng, Qinhuai Lai, Lin Yu, and Jinliang Yang

Subjects

Oncology, medicine.medical_specialty, Lung Neoplasms, Combination therapy, medicine.medical_treatment, Pharmaceutical Science, 02 engineering and technology, Drug resistance, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, Molecular Targeted Therapy, Lung cancer, Adverse effect, Immune Checkpoint Inhibitors, neoplasms, Clinical Trials as Topic, Chemotherapy, business.industry, Therapeutic effect, Immunotherapy, 021001 nanoscience & nanotechnology, medicine.disease, Small Cell Lung Carcinoma, humanities, respiratory tract diseases, 030220 oncology & carcinogenesis, 0210 nano-technology, business

Abstract

Small cell lung cancer (SCLC) is an aggressive malignant tumour which accounts for approximately 13-15% of all newly diagnosed lung cancer cases. To date, platinum-based chemotherapy are still the first-line treatments for SCLC. However, chemotherapy resistance and systemic toxicity limit the long-term clinical outcome of first-line treatment in SCLC. Recent years, targeted therapy and immunotherapy have made great breakthrough in cancer therapy, and researchers aim to exploit both as a single agent or in combination with chemotherapy to improve the survival of SCLC patients, but limited effectiveness and the adverse events remain the major obstacles in the treatment of SCLC. To overcome these challenges for SCLC therapies, prevention and early diagnosis for this refractory disease is very important. At the same time, we should reveal more information about the pathogenesis of SCLC and the mechanism of drug resistance. Finally, new treatment strategies should also be taken into considerations, such as repurposing drug, optimising of targets, combination therapy strategies or prognostic biomarkers to enhance therapeutic effects and decrease the adverse events rates in SCLC patients. This article will review the molecular biology characteristics of SCLC and discuss the opportunities and obstacles of the current therapy for SCLC patients.

Published

2020

10. Combination Foretinib and Anti-PD-1 Antibody Immunotherapy for Colorectal Carcinoma

Author

Yanfang Yang, Chengli Yang, Mengdan Wu, Yuxi Wang, Shengyan Zhao, Lishi Zeng, Xiaohua Jiang, Yin Lu, Qinhuai Lai, Cheng Huang, Yangping Wu, Jinliang Yang, Lantu Gou, Ting Kong, Jun Mou, Yuqin Yao, Yujia Peng, Yuyan Li, and Yuyin Fu

Subjects

0301 basic medicine, Combination therapy, foretinib, Colorectal cancer, QH301-705.5, medicine.medical_treatment, Metastasis, combination therapy, Cell and Developmental Biology, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cancer immunotherapy, medicine, tumor microenvironment, Biology (General), Original Research, Tumor microenvironment, biology, business.industry, Foretinib, Cell Biology, Immunotherapy, medicine.disease, 030104 developmental biology, chemistry, colon cancer, 030220 oncology & carcinogenesis, biology.protein, Cancer research, anti-PD-1, immunotherapy, Antibody, business, Developmental Biology

Abstract

Immune checkpoint inhibitors have achieved unprecedented success in cancer immunotherapy. However, the overall response rate to immune checkpoint inhibitor therapy for many cancers is only between 20 and 40%, and even less for colorectal cancer (CRC) patients. Thus, there is an urgent need to develop an efficient immunotherapeutic strategy for CRC. Here, we developed a novel CRC combination therapy consisting of a multiple receptor tyrosine kinase inhibitor (Foretinib) and anti-PD-1 antibody. The combination therapy significantly inhibited tumor growth in mice, led to improved tumor regression without relapse (83% for CT26 tumors and 50% for MC38 tumors) and prolonged overall survival. Mechanistically, Foretinib caused increased levels of PD-L1 via activating the JAK2-STAT1 pathway, which could improve the effectiveness of the immune checkpoint inhibitor. Moreover, the combination therapy remodeled the tumor microenvironment and enhanced anti-tumor immunity by further increasing the infiltration and improving the function of T cells, decreasing the percentage of tumor-associated macrophages (TAMs) and inhibiting their polarization toward the M2 phenotype. Furthermore, the combination therapy inhibited the metastasis of CT26-Luc tumors to the lung in BALB/c mouse by reducing proportions of regulatory T-cells, TAMs and M2 phenotype TAMs in their lungs. This study suggests that a novel combination therapy utilizing both Foretinib and anti-PD-1 antibody could be an effective combination strategy for CRC immunotherapy.

Published

2021

11. Targeting of DDR1 with antibody‐drug conjugates has antitumor effects in a mouse model of colon carcinoma

Author

Shijie Zhou, Mengdan Wu, Yujia Peng, Lin Yu, Cuiyu Guo, Ruixue Wang, Lantu Gou, Weirong Lai, Ying Lu, Jinliang Yang, Tinghan Yang, Xiaohua Jiang, Yiran Tao, Guangbing Zhang, Yuxi Wang, Lishi Zeng, Yangping Wu, Qinhuai Lai, Zhongping Li, Zhixiong Zhang, Yuqin Yao, and Yuyin Fu

Subjects

0301 basic medicine, Cancer Research, Immunoconjugates, Colorectal cancer, Cell, Receptor tyrosine kinase, Mice, Antineoplastic Agents, Immunological, Drug Delivery Systems, 0302 clinical medicine, Research Articles, Mice, Inbred BALB C, Tissue microarray, biology, General Medicine, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Neoplasm Proteins, medicine.anatomical_structure, colon cancer, Oncology, 030220 oncology & carcinogenesis, Molecular Medicine, HT29 Cells, Research Article, antibody‐drug conjugate, medicine.drug, Antibody-drug conjugate, Mice, Nude, lcsh:RC254-282, resistance, 03 medical and health sciences, Discoidin Domain Receptor 1, In vivo, Genetics, medicine, Animals, Humans, business.industry, Cancer, Neoplasms, Experimental, HCT116 Cells, medicine.disease, Xenograft Model Antitumor Assays, 030104 developmental biology, Nilotinib, receptor tyrosine kinase, Cancer research, biology.protein, Caco-2 Cells, business, xenograft tumor model

Abstract

DDR1 has been identified as a cancer-associated receptor tyrosine kinase that is highly expressed in several malignancies relative to normal tissues. Clinically approved multi-kinase inhibitors, such as nilotinib, inhibit DDR1-mediated tumor growth in xenograft models, suggesting DDR1 might be a potential target for cancer treatments. Here, we employed an antibody-based strategy with a novel anti-DDR1 antibody-drug conjugate (ADC) for colon carcinoma treatment. We developed T4 H11 -DM4, an ADC targeting DDR1 which carries the tubulin inhibitor payload DM4. Immunohistochemical analysis of a tissue microarray containing 100 colon cancer specimens revealed that DDR1 was highly expressed in 81% of tumor tissues. Meanwhile, high expression of DDR1 was associated with poor survival in patients. In vitro, T4 H11 -DM4 exhibited potent anti-proliferative activity with half maximal inhibitory concentration (IC50 ) values in the nanomolar range in a panel of colon cancer cell lines. In vivo, the antitumor efficacy of T4 H11 -DM4 was evaluated in three colon cancer cell lines expressing different levels of DDR1. T4 H11 -DM4 achieved complete tumor regression at doses of 5 and 10 mg·kg-1 in HT-29 and HCT116 tumor models. Moreover, a correlation between in vivo efficacy of T4 H11 -DM4 and the levels of DDR1 expression on the cell surface was observed. Tumor cell proliferation was caused by the induction of mitotic arrest, indicating that the antitumor effect in vivo was mediated by DM4. In addition, T4 H11 -DM4 was efficacious in oxaliplatin-resistant colon cancer models. In exploratory safety studies, T4 H11 -DM4 exhibited no overt toxicities when multi-doses were administered at 10 mg·kg-1 into BALB/c nude mice or when a single dose up to 50 mg·kg-1 was administered into BALB/c mice. Overall, our findings highlight the potential of DDR1-targeted ADC and may facilitate the development of a new effective therapeutic strategy for colon cancer.

Published

2019

12. Expression of 5T4 extracellular domain fusion protein and preparation of anti-5T4 monoclonal antibody with high affinity and internalization efficiency

Author

Qinhuai Lai, Lin Yu, Jinliang Yang, Yu Liu, Ruirui Zhang, Yuqin Yao, Lantu Gou, Ying Lu, Xiaohua Jiang, Ruixue Wang, Yiran Tao, Yuxi Wang, Yan Zhou, and Liangze Tang

Subjects

medicine.drug_class, Recombinant Fusion Proteins, media_common.quotation_subject, Antibody Affinity, CHO Cells, Monoclonal antibody, law.invention, Flow cytometry, Antibodies, Monoclonal, Murine-Derived, Mice, Antineoplastic Agents, Immunological, Cricetulus, Protein Domains, Antigen, law, medicine, Animals, Humans, Internalization, media_common, Mice, Inbred BALB C, Membrane Glycoproteins, biology, medicine.diagnostic_test, Chemistry, Molecular biology, Fusion protein, Immunoglobulin Fc Fragments, biology.protein, Recombinant DNA, Immunohistochemistry, Female, Antibody, Biotechnology

Abstract

5T4, a membrane protein, is overexpressed in many tumor tissues but rarely expressed in normal tissues. Here, CHO-5T4+ cells were generated and served as the antigen to immunize mice. Hybridoma techniques were employed to produce monoclonal antibodies (mAbs). The recombinant protein of human IgG Fc-fused extracellular domain of 5T4 (5T4 ECD-Fc) was obtained from transient expression in HEK293F cells. The fusion protein 5T4 ECD-Fc and CHO-5T4+ cells were respectively utilized to screen anti-5T4 antibodies that could bind to the native antigen. In preliminary screening, three hundred and fifty mAbs were obtained. Via surface plasmon resonance and flow cytometry screening, seven anti-5T4 mAbs stood out. Among them, H6 showed a high affinity (KD = 1.6 × 10−11 M) and internalization percentage (36% for 1 h and 80% for 4 h). The molecular weight and isoelectric point of H6 were determined by LC-MS and iCIEF. Moreover, the specific reactivity of H6 was demonstrated by western blotting, flow cytometry, and immunohistochemistry, respectively. In conclusion, we produced human recombinant protein of 5T4 extracellular domain and developed high-affinity internalizing monoclonal antibodies which may be applied in the 5T4-targeting ADC therapy and basic research.

Published

2019

13. Effective antitumor activity of 5T4-specific CAR-T cells against ovarian cancer cells in vitro and xenotransplanted tumors in vivo

Author

Weirong Lai, Jamel Ali, Yiran Tao, Hanshuo Yang, Yuyin Fu, Yuqin Yao, E Dong, Ying Lu, Mengdan Wu, Jinliang Yang, Zhixiong Zhang, Lantu Gou, Guangbing Zhang, Yujia Peng, Cuiyu Guo, Qinhuai Lai, Shijie Zhou, Fanxin Ma, and Xiaozhu Yue

Subjects

Adoptive cell transfer, CAR‐T cell immunotherapy, chimeric antigen receptor, business.industry, medicine.medical_treatment, 5T4, Immunotherapy, Original Articles, medicine.disease, Chimeric antigen receptor, Metastasis, ovarian cancer, Antigen, Tumor progression, medicine, Cancer research, Cytotoxic T cell, Original Article, Ovarian cancer, business

Abstract

Ovarian cancer is considered to be the most lethal gynecologic malignancy, and despite the development of conventional therapies and new therapeutic approaches, the patient's survival time remains short because of tumor recurrence and metastasis. Therefore, effective methods to control tumor progression are urgently needed. The oncofetal tumor‐associated antigen 5T4 (trophoblast glycoprotein, TPBG) represents an appealing target for adoptive T‐cell immunotherapy as it is highly expressed on the surface of various tumor cells, has very limited expression in normal tissues, and spreads widely in malignant tumors throughout their development. In this study, we generated second‐generation human chimeric antigen receptor (CAR) T cells with redirected specificity to 5T4 (5T4 CAR‐T) and demonstrated that these CAR‐T cells can elicit lytic cytotoxicity in targeted tumor cells, in addition to the secretion of cytotoxic cytokines, including IFN‐γ, IL‐2, and GM‐CSF. Furthermore, adoptive transfer of 5T4 CAR‐T cells significantly delayed tumor formation in xenografts of peritoneal and subcutaneous animal models. These results demonstrate the potential efficacy and feasibility of 5T4 CAR‐T cell immunotherapy and provide a theoretical basis for the clinical study of future immunotherapies targeting 5T4 for ovarian cancer., We generated a second‐generation CAR‐T cell targeting 5T4 with the costimulatory molecule of 4‐1BB. 5T4 CAR‐T cells had specific cytotoxicity against ovarian cancer cells and secreted cytotoxic cytokines, including IFN‐γ, IL‐2 and GM‐CSF in vitro. 5T4 CAR‐T cells could eradicate peritoneal and subcutaneous tumor models in vivo completely in a short time without recurrence.

Published

2020

14. Cryptophycin-55/52 based antibody-drug conjugates: Synthesis, efficacy, and mode of action studies

Author

Tai-Ran Kang, Weirong Lai, Xin Wang, Lantu Gou, Yiran Tao, Yuxi Wang, Lin Yu, Wei Liao, Qinhuai Lai, Ruixue Wang, Ruirui Zhang, Mengdan Wu, Jinliang Yang, Yiwen Zhang, Ying Lu, Zhixiong Zhang, Xiaohua Jiang, Hao Chen, Yujia Peng, Cuiyu Guo, Yuyin Fu, and Yuqin Yao

Subjects

Drug, Immunoconjugates, Lactams, media_common.quotation_subject, Mice, Nude, Antineoplastic Agents, Apoptosis, Pharmacology, 01 natural sciences, 03 medical and health sciences, Lactones, Mice, Structure-Activity Relationship, Trastuzumab, Depsipeptides, Drug Discovery, medicine, Tumor Cells, Cultured, Animals, Humans, Cytotoxicity, Mode of action, 030304 developmental biology, media_common, Cell Proliferation, 0303 health sciences, Mice, Inbred BALB C, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Chemistry, Organic Chemistry, Cancer, General Medicine, Cell Cycle Checkpoints, Neoplasms, Experimental, Prodrug, medicine.disease, 0104 chemical sciences, Cryptophycin, Female, Drug Screening Assays, Antitumor, Ovarian cancer, medicine.drug

Abstract

Cryptophycin-52 (CR52), a tubulin inhibitor, exhibits promising antitumor activity in vitro (picomolar level) and in mouse xenograft models. However, the narrow therapeutic window in clinical trials limits its further development. Antibody-drug conjugate (ADC), formed by coupling cytotoxic compound (payload) to an antibody via a linker, can deliver drug to tumor locations in a targeted manner by antibody, enhancing the therapeutic effects and reducing toxic and side effects. In this study, we aim to explore the possibility of CR52-based ADC for tumor targeted therapy. Due to the lack of a coupling site in CR52, its prodrug cryptophycin-55 (CR55) containing a free hydroxyl was synthesized and conjugated to the model antibody trastuzumab (anti-HER2 antibody drug approved by FDA for breast cancer therapy) via the linkers based on Mc-NHS and Mc-Val-Cit-PAB-PNP. The average drug-to-antibody ratios (DARs) of trastuzumab-CR55 conjugates (named T-L1-CR55, T-L2-CR55, and T-L3-CR55) were 3.50, 3.29, and 3.35, respectively. These conjugates exhibited potent cytotoxicity in HER2-positive tumor cell lines with IC50 values at low nanomolar levels (0.58–1.19 nM). Further, they displayed significant antitumor activities at the doses of 10 mg/kg in established ovarian cancer (SKOV3) and gastric cancer (NCI–N87) xenograft models without overt toxicities. Finally, the drug releases were analyzed and the results indicated that T-L3-CR55 was able to effectively release CR55 and further epoxidized to CR52, which may be responsible for its best performance in antitumor activities. In conclusion, our results demonstrated that these conjugates have the potential for tumor targeted therapy, which provides insights to further research the CR55/CR52-based ADC for tumor therapy.

Published

2019

15. Promiximab-duocarmycin, a new CD56 antibody-drug conjugates, is highly efficacious in small cell lung cancer xenograft models

Author

Ruixue Wang, Yiran Tao, Shuli Yi, Yu Liu, Yuyin Fu, Ruirui Zhang, Ying Lu, Yuqin Yao, Jinliang Yang, Wenting Li, Lin Yu, Qinhuai Lai, Lantu Gou, Ligong Chen, and Yuxi Wang

Subjects

0301 basic medicine, medicine.medical_treatment, Cell, antibody-drug conjugates, Spleen, duocarmycins, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, In vivo, medicine, Duocarmycin, biology, Immunotherapy, In vitro, respiratory tract diseases, 030104 developmental biology, medicine.anatomical_structure, Oncology, chemistry, Cell culture, 030220 oncology & carcinogenesis, biology.protein, Cancer research, CD56, small cell lung cancer, Antibody, Research Paper

Abstract

Small cell lung cancer (SCLC) is of a highly invasive and metastatic lung cancer subtype and there had not been effective targeted therapies. CD56, a cell surface marker highly expressed on most SCLC, is a promising therapeutic target for treatment of this aggressive cancer. In this study, we generated a novel anti-CD56 antibody named promiximab, characterized by high affinity, internalization and tumor specificity. Then, the promiximab was conjugated with a potent DNA alkylating agent duocarmycin via reduced interchain disulfides to yield the promiximab-Duocarmycin (promiximab-DUBA) conjugates. Mass spectrometry analysis showed promiximab-DUBA had an average DAR (Drug-to-Antibody Ratio) of about 2.04. In vitro, promiximab-DUBA exerted strong inhibitory effects on SCLC cell lines NCI-H526, NCI-H524 and NCI-H69, with IC50 values of 0.07 nmol/L, 0.18 nmol/L and 0.29 nmol/L, respectively. In vivo antitumor activity, promiximab-DUBA at the dose of 5 mg/kg and 10 mg/kg every three days with a total of three times were sufficient to induce sustained regression of NCI-H526 tumors over control treatment with promiximab. Mostly, no recurrence was observed until 65 days post treatment with promiximab-DUBA. In the NCI-H69 subcutaneous xenograft model, significant inhibition of tumor growth was also observed following administration of promiximab-DUBA at the dose of 5 mg/kg or 10 mg/kg. Moreover, body weight and histopathology of major organs (liver, spleen, heart, lung and kidney) showed no significant changes after treatment of promiximab-DUBA. In conclusion, promiximab-DUBA is highly efficacious in small cell lung cancer xenograft models, and provides a new immunotherapy approach for SCLC.

Published

2017

16. Comparative RNA-sequencing profiled the differential gene expression of liver in response to acetyl-CoA carboxylase inhibitor GS-0976 in a mouse model of NASH

Author

Xiaolan Su, Qianru Zhang, Manyu Zhao, Ying Lu, Sijia Wu, Aiping Fang, Jinliang Yang, Yuqin Yao, Qinhuai Lai, Chuang Liu, and Xiaoxin Chen

Subjects

Normal diet, Bioinformatics, Metabolic Sciences, lcsh:Medicine, Acetyl-CoA carboxylase inhibitor, Biology, General Biochemistry, Genetics and Molecular Biology, Transcriptome, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Fibrosis, Gene expression, medicine, RNA-Seq, Molecular Biology, Sirius Red, Non-alcoholic steatohepatitis, 030304 developmental biology, 0303 health sciences, General Neuroscience, lcsh:R, General Medicine, medicine.disease, Molecular biology, chemistry, Lipogenesis, 030211 gastroenterology & hepatology, Steatosis, Steatohepatitis, General Agricultural and Biological Sciences

Abstract

Background Non-alcoholic steatohepatitis (NASH) is a progressive liver disease characterized by hepatic steatosis, lobular inflammation and fibrosis. Acetyl-CoA carboxylase (ACC) isoform 1 and 2 involved in de novo lipogenesis (DNL) and fatty acid oxidation have been identified as a therapeutic target in NASH. GS-0976, the inhibitor of ACC1 and ACC2, has achieved favorable therapeutic effects in clinical trials with NASH. The purpose of this study was to explore the transcriptional alterations regulated by GS-0976 in NASH. Methods C57BL/6 mice were fed on a choline-deficient, L-amino acid-defined, high-fat diet (CDAHFD) or normal diet for 12 weeks. Mice were treated with or without GS-0976 (3 mg/kg per day) in the last 8 weeks. Oil Red O, Haematoxylin-eosin (H & E), and Sirius Red were used to evaluate hepatic steatosis, inflammation and fibrosis. The comparative RNA-sequencing was conducted to analyse the hepatic gene expression profiles in mice. Reverse transcription–polymerase chain reaction analysis was performed to validate the differential expression of representative genes. Results GS-0976 attenuated the steatosis, inflammation, and fibrosis of NASH in CDAHFD mouse model. High-throughput sequencing and differential gene expression analysis showed that there were 516 up-regulated genes and 525 down-regulated genes after GS-0976 treatment. Genes involved in the metabolic process, extracellular matrix formation, immune response, and angiogenesis were significantly enriched. The “Metabolic pathways” and “ECM-receptor interaction” pathways were the most significantly enriched KEGG pathways in the up-regulated and down-regulated differentially expressed genes (DEGs), respectively. Conclusions Transcriptome analysis showed that GS-0976 could regulate the expression of genes related to metabolism, inflammation and fibrosis in NASH. The global transcriptomic changes in gene expression promote the further understanding for the inhibition mechanisms of GS-0976 in NASH.

Published

2019

17. Preparation and anti-cancer evaluation of promiximab-MMAE, an anti-CD56 antibody drug conjugate, in small cell lung cancer cell line xenograft models

Author

Ruixue Wang, Yu Liu, Lin Yu, Yuqin Yao, Jinliang Yang, Qinhuai Lai, Xiaoxin Chen, Ying Lu, Chuang Liu, Lantu Gou, Yuxi Wang, Shijie Zhou, Ruirui Zhang, Qiang Chen, and Yamei Yu

Subjects

0301 basic medicine, Antibody-drug conjugate, Immunoconjugates, Lung Neoplasms, Pharmaceutical Science, 03 medical and health sciences, Mice, 0302 clinical medicine, Tandem Mass Spectrometry, Cell Line, Tumor, medicine, Animals, Humans, Cell adhesion molecule, Chemistry, Gene Expression Profiling, Cancer, medicine.disease, Small Cell Lung Carcinoma, Xenograft Model Antitumor Assays, CD56 Antigen, body regions, 030104 developmental biology, Cell culture, 030220 oncology & carcinogenesis, Cancer research, Non small cell, Oligopeptides, Conjugate, Chromatography, Liquid

Abstract

Antibody-drug conjugates (ADCs) have been successfully applied clinically as target drugs for cancer. In this study, anti-neural cell adhesion molecule also called CD56 antibody-monomethyl auristatin E (MMAE) conjugate named Promiximab-MMAE was prepared by conjugation of microtubule inhibitor MMAE with Promiximab. The average drug-to-antibody ratio (DAR) of Promiximab-MMAE was 3.13 as analysed by liquid chromatography-mass spectrometry/ mass spectrometry (LC-MS/MS). The targeting capacity and affinity kinetics of Promiximab-MMAE were similar to that of Promiximab after being conjugated with MMAE as tested by flow cytometry and biolayer interferometry analysis. Promiximab-MMAE showed effective anti-proliferation on CD56-positive cell lines (NCI-H524, NCI-H526, and NCI-H69), with the half maximal inhibitory concentration (IC50) values of 19.24, 5.23, and 0.32 nmol/L in vitro, respectively. Promiximab-MMAE of 10 mg/kg every three days with a total of three times was administered in vivo. Results showed that the tumour regression was not recrudesced in NCI-H69 and NCI-H526 xenograft mice models till 52 and 56 days. Moreover, body weight and histopathology of the major organs (liver, spleen, heart, lung, and kidney) showed no significant changes after treatment with Promiximab-MMAE. In conclusion, Promiximab-MMAE is a potential candidate for the treatment of CD56 positive small cell lung cancer.

Published

2018

18. Design, synthesis and biological evaluation of a novel tubulin inhibitor 7a3 targeting the colchicine binding site

Author

Yuqin Yao, Qinhuai Lai, Yuxi Wang, Ruixue Wang, Ruirui Zhang, Shaoxue Zeng, Liangze Tang, Jinliang Yang, Yiran Tao, Lantu Gou, Hao Chen, Luyi Huang, Haotian Xiang, Yu Liu, and Weirong Lai

Subjects

0301 basic medicine, Models, Molecular, Protein Data Bank (RCSB PDB), Antineoplastic Agents, Crystallography, X-Ray, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Nude mouse, Cell Movement, Tubulin, Cell Line, Tumor, Drug Discovery, medicine, Colchicine, Animals, Humans, Cell Proliferation, Pharmacology, Combretastatin A-4, Combretastatin, Ovarian Neoplasms, Binding Sites, biology, Organic Chemistry, General Medicine, Cell cycle, biology.organism_classification, Tubulin Modulators, Mice, Inbred C57BL, Molecular Docking Simulation, 030104 developmental biology, Biochemistry, chemistry, Mechanism of action, 030220 oncology & carcinogenesis, Drug Design, biology.protein, Pyrazoles, Female, medicine.symptom, Drug Screening Assays, Antitumor

Abstract

Tubulin inhibitors that target the colchicine binding site continue to emerge as promising anticancer agents. In this study, based on the anti-proliferative activities, a novel tubulin inhibitor 7a3 targeting the colchicine binding site was designed, synthesized, and optimized from a series of novel cis-restricted pyrazole analogues of combretastatin A-4. The structure-activity relationships (SARs) of these newly synthesized compounds are summarized indicating that the methyl substituent at the N1 position and deamination were significantly important for the anti-proliferative efficacy. The optimized compound 7a3 exhibited the ability to arrest the cell cycle in the G2/M phase, induce cell apoptosis, and inhibit cell migration in tumour cells. The results of the immunofluorescence analysis using confocal microscopy and the tubulin polymerization assay revealed that tubulin assembly was disrupted by 7a3 in vitro. Furthermore, the targeting identification of 7a3 was illuminated by solving the crystal structure of 7a3 in complex with tubulin at a resolution of 3.2 A (PDB code 5Z4U ), which confirmed the result of molecular docking and further demonstrated that 7a3 binds to the site of colchicine. Moreover, the pharmacokinetic analysis in mouse plasma showed that 7a3 rapidly reached a peak concentration at 0.25 h after intraperitoneal administration, and the T1/2, Cmax, and AUC0-inf were 1.67 ± 0.28 h, 882 ± 71 ng mL-1, and 1166 ± 129 h ng·mL-1, respectively, after a single-dose administration analysed by liquid chromatography-tandem mass spectrometry (LC/MS/MS). In addition, the in vivo study indicated that 7a3 significantly inhibited the tumour growth of the SK-OV-3 xenograft in a nude mouse model. In conclusion, our study proved 7a3 to be a potential microtubule-targeting drug for cancer therapy. The SARs and mechanism of action studies of 7a3 based on the X-ray co-crystal structure provided insights into the next-generation tubulin inhibitors for cancer therapy.

Published

2018

19. Therapeutic potential of an anti-HER2 single chain antibody–DM1 conjugates for the treatment of HER2-positive cancer

Author

Ruixue Wang, Weirong Lai, Wenting Li, Xiangzheng Chen, Yuxi Wang, Yuyin Fu, Hang Zhang, Yu-Huan Kang, Lantu Gou, Yuqin Yao, Yiran Tao, Ying Lu, Xiaohua Jiang, Yangping Wu, Yujia Peng, Lin Yu, Jinliang Yang, Min Wu, Shuli Yi, and Qinhuai Lai

Subjects

0301 basic medicine, Cancer Research, biology, medicine.drug_class, Chemistry, Single chain, Monoclonal antibody, medicine.disease, Article, In vitro, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Trastuzumab, 030220 oncology & carcinogenesis, Genetics, medicine, biology.protein, Cancer research, Cytotoxic T cell, Antibody, Ovarian cancer, medicine.drug, Conjugate

Abstract

Antibody–drug conjugates (ADCs) take the advantage of monoclonal antibodies to selectively deliver highly potent cytotoxic drugs to tumor cells, which have become a powerful measure for cancer treatment in recent years. To develop a more effective therapy for human epidermal growth factor receptor 2 (HER2)-positive cancer, we explored a novel ADCs composed of anti-HER2 scFv–HSA fusion antibodies conjugates with a potent cytotoxic drug DM1. The resulting ADCs, T-SA1–DM1 and T-SA2–DM1 (drug-to-antibody ratio in the range of 3.2–3.5) displayed efficient inhibition in the growth of HER2-positive tumor cell lines and the half-maximal inhibitory concentration on SKBR-3 and SKOV3 cells were both at the nanomolar levels in vitro. In HER2-positive human ovarian cancer xenograft models, T-SA1–DM1 and T-SA2–DM1 also showed remarkable antitumor activity. Importantly, three out of six mice exhibited complete remission without regrowth in the high-dose group of T-SA1–DM1. On the basis of the analysis of luminescence imaging, anti-HER2 scFv–HSA fusion antibodies, especially T-SA1, showed strong and rapid tumor tissue penetrability and distribution compared with trastuzumab. Collectively, the novel type of ADCs is effective and selective targeting to HER2-positive cancer, and may be a promising antitumor drug candidate for further studies.

Published

2017

20. Structures of a diverse set of colchicine binding site inhibitors in complex with tubulin provide a rationale for drug discovery

Author

Qinhuai Lai, Yangping Wu, Jinliang Yang, Qiang Chen, Xiangzheng Chen, Yuxi Wang, Hang Zhang, Yamei Yu, Zhaoya Yang, Benoît Gigant, State Key Laboratory of Biotherapy and Cancer Center, Sichuan University [Chengdu] (SCU), Biochimie Structurale des Microtubules, des Kinésines et de leurs Cargos (MIKICA), Département Biochimie, Biophysique et Biologie Structurale (B3S), Institut de Biologie Intégrative de la Cellule (I2BC), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS)-Institut de Biologie Intégrative de la Cellule (I2BC), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS), West China School of Pharmacy, Sichuan University, Biochimie Structurale des Microtubules, des Kinésines et de leurs Cargos ( MIKICA ), Département Biochimie, Biophysique et Biologie Structurale ( B3S ), Institut de Biologie Intégrative de la Cellule ( I2BC ), Université Paris-Saclay-Centre National de la Recherche Scientifique ( CNRS ) -Commissariat à l'énergie atomique et aux énergies alternatives ( CEA ) -Université Paris-Sud - Paris 11 ( UP11 ) -Université Paris-Saclay-Centre National de la Recherche Scientifique ( CNRS ) -Commissariat à l'énergie atomique et aux énergies alternatives ( CEA ) -Université Paris-Sud - Paris 11 ( UP11 ) -Institut de Biologie Intégrative de la Cellule ( I2BC ), Université Paris-Saclay-Centre National de la Recherche Scientifique ( CNRS ) -Commissariat à l'énergie atomique et aux énergies alternatives ( CEA ) -Université Paris-Sud - Paris 11 ( UP11 ) -Université Paris-Saclay-Centre National de la Recherche Scientifique ( CNRS ) -Commissariat à l'énergie atomique et aux énergies alternatives ( CEA ) -Université Paris-Sud - Paris 11 ( UP11 ), and Université Paris-Saclay-Centre National de la Recherche Scientifique ( CNRS ) -Commissariat à l'énergie atomique et aux énergies alternatives ( CEA ) -Université Paris-Sud - Paris 11 ( UP11 )

Subjects

0301 basic medicine, Models, Molecular, crystal structure, Swine, drug design, [SDV]Life Sciences [q-bio], Antineoplastic Agents, Diketopiperazines, Biology, Ligands, Biochemistry, Microtubules, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, Microtubule, Tubulin, Drug Discovery, Animals, Tivantinib, tubulin inhibitor, Molecular Biology, Protein Kinase Inhibitors, Binding Sites, [ SDV ] Life Sciences [q-bio], Molecular Structure, pharmacophore, Tubulin Modulators, Nocodazole, Cell Biology, Pyrrolidinones, 3. Good health, 030104 developmental biology, chemistry, Docking (molecular), colchicine binding domain, biology.protein, Quinolines, Pharmacophore, Colchicine, Protein Kinases, Plinabulin

Abstract

International audience; Microtubules are dynamic assemblies of αβ-tubulin heterodimers and have been recognized as highly attractive targets for cancer chemotherapy. A broad range of agents bind to tubulin and interfere with microtubule assembly. Despite having a long history of characterization, colchicine binding site inhibitors (CBSIs) have not yet reached the commercial phase as anti-cancer drugs to date. We determined the structures of tubulin complexed with a set of structurally diverse CBSIs (lexibulin, nocodazole, plinabulin and tivantinib), among which nocodazole and tivantinib are both binary-function inhibitors targeting cancer-related kinases and microtubules simultaneously. High resolution structures revealed the detailed interactions between these ligands and tubulin. Our results showed that the binding modes of the CBSIs were different from previous docking models, highlighting the importance of crystal structure information in structure-based drug design. A real structure-based pharmacophore was proposed to rationalize key common interactions of the CBSIs at the colchicine domain. Our studies provide a solid structural basis for developing new anti-cancer agents for the colchicine binding site.; The atomic coordinates and structure factors for tubulin complexed with lexibulin, nocodazole, plinabulin and tivantinib have been deposited in the Protein Data Bank under accession codes 5CA0, 5CA1, 5C8Y and 5CB4, respectively.

Published

2016