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The ABC of ADCs (Antibody-Drug Conjugates): A Comprehensive Review of Technical, Regulatory, and Clinical Challenges
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作者 Kishore Kumar Hotha 《Advances in Chemical Engineering and Science》 2023年第4期363-381,共19页
Over the past several decades, there has been a significant surge in the development of Antibody-Drug Conjugates (ADCs). Designing an ideal ADC presents a multifaceted challenge, requiring the precise orchestration of... Over the past several decades, there has been a significant surge in the development of Antibody-Drug Conjugates (ADCs). Designing an ideal ADC presents a multifaceted challenge, requiring the precise orchestration of various elements such as antigens, antibodies, linkers, and payloads. While ADCs aim to target tumor cells specifically, several antigens can also be found in regular tissues, potentially compromising the specificity of ADCs in therapeutic applications. The complexity extends to antibody selection, necessitating effective targeting of the desired antigen and ensuring compatibility with linkers for effective payload delivery. Additionally, the linker and payload combination are critical for the ADC’s therapeutic efficiency, balancing stability in circulation and timely payload release upon target binding. ADC doses must be safe for normal tissues while ensuring the released payloads are effective. The success of ADCs is attributed to their unmatched efficacy compared to traditional chemotherapy agents. The current research article aims to provide a technical review of Antibody-Drug Conjugates (ADCs) for cancer therapies. A brief discussion on the basics of ADCs, regulatory approach, overview, and technical complexities for quantification is presented. This review also summarizes recently approved ADCs and introduces the concepts of antibodies, linkers, and payloads. The article also outlines cancer-specific ADCs currently in late-stage clinical trials for cancer treatment. 展开更多
关键词 antibody-drug conjugates Cancer Therapy PAYLOAD LINKER conjugation Chemistry ANTIBODY Analytical Development Manufacturing of adcs
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Antibody-Drug Conjugates (ADCs): Navigating Four Pillars of Safety, Development, Supply Chain and Manufacturing Excellence
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作者 Kishore Kumar Hotha 《Advances in Chemical Engineering and Science》 2023年第4期351-362,共12页
Antibody-drug conjugates (ADCs) are pioneering biologics that merge antibodies’ specificity with small molecules’ potency. With a handful of FDA-approved ADCs in the market and many under development, ADCs are poise... Antibody-drug conjugates (ADCs) are pioneering biologics that merge antibodies’ specificity with small molecules’ potency. With a handful of FDA-approved ADCs in the market and many under development, ADCs are poised to revolutionize therapeutics. This paper examines the complexities of ADC production, emphasizing the importance of process characterization and the pivotal role of supply chain characteristics, safety requirements, and Contract Manufacturing Organizations (CMOs) with proficiency. The swift transition of antibody-drug conjugate (ADC) programs from early to advanced clinical stages underscores the urgency for quick and efficient commercial launch preparation. This article delves into strategies to hasten commercial readiness, supply chain strategy, the significance of partnering with adept contract development and manufacturing organizations (CDMOs), and the challenges of ADC production. 展开更多
关键词 Antibody Drug conjugates adc’s Payload LINKER Antibody HPAPI SAFETY Technology Transfer CDMO CMO
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Current LC-MS-based strategies for characterization and quantification of antibody-drug conjugates 被引量:1
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作者 Xiaoyu Zhu Shihan Huo +2 位作者 Chao Xue Bo An Jun Qu 《Journal of Pharmaceutical Analysis》 SCIE CAS CSCD 2020年第3期209-220,共12页
The past few years have witnessed enormous progresses in the development of antibody-drug conjugates(ADCs).Consequently,comprehensive analysis of ADCs in biological systems is critical in supporting discovery,developm... The past few years have witnessed enormous progresses in the development of antibody-drug conjugates(ADCs).Consequently,comprehensive analysis of ADCs in biological systems is critical in supporting discovery,development and evaluation of these agents.Liquid chromatography-mass spectrometry(LC-MS)has eme rged as a promising and versatile tool for ADC analysis across a wide range of scenarios,owing to its multiplexing ability,rapid method development,as well as the capability of analyzing a variety of targets ranging from small-molecule payloads to the intact protein with a high,molecular resolution.However,despite this tremendous potential,challenges persist due to the high complexity in both the ADC molecules and the related biological systems.This review summarizes the up-to-date LC-MS-based strategies in ADC analysis and discusses the challenges and opportunities in this rapidly-evolving field. 展开更多
关键词 antibody-drug conjugate(adc) Liquid chromatography-mass spectrometry(LCMS) Drug-to-antibody ratio(DAR)
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TCR-mimic antibody-drug conjugates targeting intracellular tumor-specific mutant antigen KRAS G12V mutation 被引量:4
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作者 Ying Shen Xiaoyue Wei +6 位作者 Shijie Jin Yue Wu Wenbin Zhao Yingchun Xu Liqiang Pan Zhan Zhou Shuqing Chen 《Asian Journal of Pharmaceutical Sciences》 SCIE CAS 2020年第6期777-785,共9页
Limited clinical application of antibody-drug conjugates(ADCs)targeting tumor associated antigens(TAAs)is usually caused by on-target off-tumor side effect.Tumor-specific mutant antigens(TSMAs)only expressed in tumor ... Limited clinical application of antibody-drug conjugates(ADCs)targeting tumor associated antigens(TAAs)is usually caused by on-target off-tumor side effect.Tumor-specific mutant antigens(TSMAs)only expressed in tumor cells which are ideal targets for ADCs.In addition,intracellular somatic mutant proteins can be presented on the cell surface by human leukocyte antigen class I(HLA I)molecules forming tumor-specific peptide/HLA I complexes.KRAS G12 V mutation frequently occurred in varied cancer and was verified as a promising target for cancer therapy.In this study,we generated two TCR-mimic antibodydrug conjugates(TCRm-ADCs),2E8-MMAE and 2 A5-MMAE,targeting KRAS G12 V/HLAA*0201 complex,which mediated specific antitumor activity in vitro and in vivo without obvious toxicity.Our findings are the first time validate the strategy of TCRm-ADCs targeting intracellular TSMAs,which improves the safety of antibody-based drugs and provides novel strategy for precision medicine in cancer therapy. 展开更多
关键词 TCR-mimic antibody-drug conjugates Tumor-specific mutant antigens KRAS G12V Human leukocyte antigen classⅠ
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Enzyme-linked immunosorbent assays for quantification of MMAE-conjugated ADCs and total antibodies in cynomolgus monkey sera
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作者 Min Pei Tingting Liu +17 位作者 Lu Ouyang Jianhua Sun Xiaojie Deng Xiaomin Sun Wei Wu Peng Huang Yi-Li Chen Xiaorong Tan Xiaoyue Liu Peng Zhu Yongzhen Liu Deheng Wang Junliang Wu Qi Wang Guifeng Wang Likun Gong Qiuping Qin Chunhe Wang 《Journal of Pharmaceutical Analysis》 SCIE CAS CSCD 2022年第4期645-652,共8页
Antibody-drug conjugates(ADCs)are commonly heterogeneous and require extensive assessment of exposure-efficacy and exposure-safety relationships in preclinical and clinical studies.In this study,we report the generati... Antibody-drug conjugates(ADCs)are commonly heterogeneous and require extensive assessment of exposure-efficacy and exposure-safety relationships in preclinical and clinical studies.In this study,we report the generation of a monoclonal antibody against monomethyl auristatin E(MMAE)and the development,validation,and application of sensitive and high-throughput enzyme-linked immunosorbent assays(ELISA)to measure the concentrations of MMAE-conjugated ADCs and total antibodies(tAb,antibodies in ADC plus unconjugated antibodies)in cynomolgus monkey sera.These assays were successfully applied to in vitro plasma stability and pharmacokinetic(PK)studies of SMADC001,an MMAE-conjugated ADC against trophoblast cell surface antigen 2(TROP-2).The plasma stability of SMADC001 was better than that of similar ADCs coupled with PEG4-Val-Cit,Lys(m-dPEG24)-Cit,and Val-Cit linkers.The developed ELISA methods for the calibration standards of ADC and tAb revealed a correlation between serum concentrations and the OD450 values,with R2 at 1.000,and the dynamic range was 0.3-35.0 ng/mL and 0.2-22.0 ng/mL,respectively;the intra-and inter-assay accuracy bias%ranged from -12.2% to -5.2%,precision ranged from -12.4% to -1.4%,and the relative standard deviation(RSD)was less than 6.6% and 8.7%,respectively.The total error was less than 20.4%.The development and validation steps of these two assays met the acceptance criteria for all addressed validation parameters,which suggested that these can be applied to quantify MMAE-conjugated ADCs,as well as in PK studies.Furthermore,these assays can be easily adopted for development of other similar immunoassays. 展开更多
关键词 Monomethyl auristatin E antibody-drug conjugates PHARMACOKINETICS Trophoblast cell surface antigen 2
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2024年欧洲肿瘤内科学会乳腺癌年会研究进展
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作者 吕文杰 吴萍 《中国肿瘤临床》 CAS CSCD 北大核心 2024年第11期572-579,共8页
2024年5月举行的欧洲肿瘤内科学会乳腺癌年会(European Society for Medical Oncology Breast Cance,ESMO BC)在德国柏林召开。本次年会展示了一系列针对乳腺癌治疗的最新进展,包括创新疗法和诊治策略。特别值得关注的是,细胞周期蛋白... 2024年5月举行的欧洲肿瘤内科学会乳腺癌年会(European Society for Medical Oncology Breast Cance,ESMO BC)在德国柏林召开。本次年会展示了一系列针对乳腺癌治疗的最新进展,包括创新疗法和诊治策略。特别值得关注的是,细胞周期蛋白依赖性激酶4和6(cyclin-dependent kinases 4 and 6,CDK4/6)抑制剂联合内分泌治疗(endocrine therapy,ET)在早期乳腺癌新辅助治疗中的研究尚未达到主要终点,而探索性分析结果表明,该领域仍有待进一步研究。CDK4/6抑制剂联合ET继续作为高危患者辅助治疗的标准。同时,阿贝西利在携带BRCA1/2突变的患者亚组中显示出初步的一致性获益。瑞波西利虽然不良反应可控,但仍需进行密切监测。新型CDK4选择性抑制剂、AKT抑制剂、抗体药物偶联物(antibody-drug conjugates,ADC)以及免疫治疗为晚期乳腺癌患者提供了新的治疗选项。本次年会所展现的研究成果,不仅代表了乳腺癌治疗领域的进步,也为未来的研究方向和患者治疗策略提供了新的视野。本文就此次年会上重点的研究进展进行综述。 展开更多
关键词 乳腺癌 研究进展 免疫治疗 CDK4/6抑制剂 抗体药物偶联物
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乳腺癌受体阳转阴的发生机理与治疗进展
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作者 韩颖 邸立军 《现代肿瘤医学》 CAS 2024年第14期2652-2656,共5页
乳腺癌因其高度异质性,给乳腺癌精准治疗带来挑战。雌激素受体(estrogen receptor, ER)、孕激素受体(progesterone receptor, PR)和人表皮生长因子受体-2(human epidermal growth factor receptor-2, HER2)状态是乳腺癌精准诊疗的重要... 乳腺癌因其高度异质性,给乳腺癌精准治疗带来挑战。雌激素受体(estrogen receptor, ER)、孕激素受体(progesterone receptor, PR)和人表皮生长因子受体-2(human epidermal growth factor receptor-2, HER2)状态是乳腺癌精准诊疗的重要依据。对于复发或转移性乳腺癌患者,既往治疗主要基于原发病灶受体状态。但研究发现部分患者复发/转移灶受体表达与原发病灶不同,推测可能与肿瘤异质性和治疗后的克隆选择效应相关。相较于受体表达“阴转阳”,受体“阳转阴”的发生率更高,且受体表达的缺失可能导致对原有疗法耐药且预后不良。重新评估乳腺癌复发/转移灶受体状态对调整治疗策略和判断预后具有显著临床意义,但能否基于受体变化情况指导临床决策,在临床研究或实践层面仍存在较大争议。随着靶向药物、免疫疗法及抗体偶联药物(antibody-drug conjugates, ADC)等新型抗肿瘤药物的应用,如何优化受体“阳转阴”乳腺癌患者的治疗方案以提高疗效成为未解决的临床需求。该文旨在深入探讨乳腺癌受体“阳转阴”的机理、预后影响以及治疗现状,为这类患者的治疗提供理论支持和实践指导。 展开更多
关键词 乳腺癌 雌激素受体 孕激素受体 HER2受体 受体阳转阴 adc药物
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抗体偶联药物在晚期胃癌治疗中的研究进展
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作者 吴雨微 阎金杉 赵明芳 《实用药物与临床》 CAS 2024年第6期449-456,共8页
胃癌发生隐匿,恶性程度较高,对传统放化疗不敏感,预后差,因此,研发新型抗胃癌药物迫在眉睫。抗体偶联药物(Antibody-drug conjugate,ADC)是由单克隆抗体经特定的连接子与细胞毒药物连接而成的一类靶向生物制剂,具有高效、靶向、精准、... 胃癌发生隐匿,恶性程度较高,对传统放化疗不敏感,预后差,因此,研发新型抗胃癌药物迫在眉睫。抗体偶联药物(Antibody-drug conjugate,ADC)是由单克隆抗体经特定的连接子与细胞毒药物连接而成的一类靶向生物制剂,具有高效、靶向、精准、低毒等优势。目前,ADC已广泛用于治疗血液系统肿瘤及实体肿瘤,并在晚期胃癌的治疗中展现出良好疗效,具有广阔的应用前景。 展开更多
关键词 抗体偶联药物 胃癌 靶向治疗
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Resistance to antibody-drug conjugates in breast cancer:mechanisms and solutions 被引量:5
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作者 Yu-Fei Chen Ying-ying Xu +1 位作者 Zhi-Ming Shao Ke-Da Yu 《Cancer Communications》 SCIE 2023年第3期297-337,共41页
Antibody-drug conjugates(ADCs)are a rapidly developing therapeutic approach in cancer treatment that has shown remarkable activity in breast cancer.Currently,there are two ADCs approved for the treatment of human epid... Antibody-drug conjugates(ADCs)are a rapidly developing therapeutic approach in cancer treatment that has shown remarkable activity in breast cancer.Currently,there are two ADCs approved for the treatment of human epidermal growth factor receptor 2-positive breast cancer,one for triple-negative breast cancer,and multiple investigational ADCs in clinical trials.However,drug resistance has been noticed in clinical use,especially in trastuzumab emtansine.Here,the mechanisms of ADC resistance are summarized into four categories:antibodymediated resistance,impaired drug trafficking,disrupted lysosomal function,and payload-related resistance.To overcome or prevent resistance to ADCs,innovative development strategies and combination therapy options are being investigated.Analyzing predictive biomarkers for optimal therapy selection may also help to prevent drug resistance. 展开更多
关键词 antibody-drug conjugate breast cancer drug resistance combination therapy predictive biomarker
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Disitamab vedotin,a HER2-directed antibody-drug conjugate,in patients with HER2-overexpression and HER2-low advanced breast cancer:a phase I/Ib study
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作者 Jiayu Wang Yunjiang Liu +6 位作者 Qingyuan Zhang Wei Li Jifeng Feng XiaojiaWang Jianmin Fang Yiqun Han Binghe Xu 《Cancer Communications》 SCIE 2024年第7期833-851,共19页
Background:Disitamab vedotin(DV;RC48-ADC)is an antibody-drug conjugate comprising a human epidermal growth factor receptor 2(HER2)-directed antibody,linker and monomethyl auristatin E.Preclinical studies have shown th... Background:Disitamab vedotin(DV;RC48-ADC)is an antibody-drug conjugate comprising a human epidermal growth factor receptor 2(HER2)-directed antibody,linker and monomethyl auristatin E.Preclinical studies have shown that DV demonstrated potent antitumor activity in preclinical models of breast,gastric,and ovarian cancers with different levels of HER2 expression.In this pooled analysis,we report the safety and efficacy of DV in patients with HER2-overexpression and HER2-low advanced breast cancer(ABC).Methods:In the phase I dose-escalation study(C001 CANCER),HER2-overexpression ABC patients received DV at doses of 0.5-2.5 mg/kg once every two weeks(Q2W)until unacceptable toxicity or progressive disease.The dose range,safety,and pharmacokinetics(PK)were determined.The phase Ib dose-range and expansion study(C003 CANCER)enrolled two cohorts:HER2-overexpression ABC patients receiving DV at doses of 1.5-2.5 mg/kg Q2W,with the recommended phase 2 dose(RP2D)determined,andHER2-lowABC patients receiving DV at doses of 2.0 mg/kg Q2W to explore the efficacy and safety of DV in HER2-low ABC.Results:Twenty-four patients with HER2-overexpression ABC in C001 CANCER,46 patients with HER2-overexpressionABCand 66 patients with HER2-low ABC in C003 CANCER were enrolled.At 2.0 mg/kg RP2D Q2W,the confirmed objective response rates were 42.9%(9/21;95%confidence interval[CI]:21.8%-66.0%)and 33.3%(22/66;95%CI:22.2%-46.0%),with median progression-free survival(PFS)of 5.7 months(95%CI:5.3-8.4 months)and 5.1 months(95%CI:4.1-6.6 months)for HER2-overexpression and HER2-low ABC,respectively.Common(≥5%)grade 3 or higher treatment-emergent adverse events included neutrophil count decreased(17.6%),gamma-glutamyl transferase increased(13.2%),asthenia(11.0%),white blood cell count decreased(9.6%),peripheral neuropathy such as hypoesthesia(5.9%)and neurotoxicity(0.7%),and pain(5.9%).Conclusion:DV demonstrated promising efficacy in HER2-overexpression and HER2-low ABC,with a favorable safety profile at 2.0 mg/kg Q2W. 展开更多
关键词 antibody-drug conjugate breast cancer clinical trials disitamab vedotin HER2-low HER2-overexpression
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抗体偶联药物诱导的间质性肺病的发病机制
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作者 赵翠翠 张传桂 《中国肿瘤临床》 CAS CSCD 北大核心 2024年第15期775-779,共5页
药物性间质性肺病(drug-induced interstitial lung disease,DI-ILD)是药物所致肺部不良事件的最常见形式,其最常见原因是抗癌药物。DI-ILD首次被确定为一种需要特别关注的不良事件是因抗体偶联药物(antibody-drug conjugates,ADC)。随... 药物性间质性肺病(drug-induced interstitial lung disease,DI-ILD)是药物所致肺部不良事件的最常见形式,其最常见原因是抗癌药物。DI-ILD首次被确定为一种需要特别关注的不良事件是因抗体偶联药物(antibody-drug conjugates,ADC)。随着研发药物数量和种类的增多、多款ADC药物被批准或即将被批准用于临床治疗,DI-ILD引发了越来越多的关注。然而,ADC药物引发DI-ILD的机制尚未明确,本文就目前常见且应用广泛的抗人表皮生长因子受体2(human epidermal growth factor receptor 2,HER2)ADC药物DI-ILD的发生机制进行综述。 展开更多
关键词 药物性间质性肺病 间质性肺病 抗癌药物 抗体偶联药物 人表皮生长因子受体2
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HER3-targeted therapeutic antibodies and antibody-drug conjugates in non-small cell lung cancer refractory to EGFR-tyrosine kinase inhibitors
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作者 Margaret E.Larsen Hui Lyu Bolin Liu 《Chinese Medical Journal Pulmonary and Critical Care Medicine》 2023年第1期11-17,共7页
Human epidermal growth factor receptor 3(HER3)is a unique member of the human epidermal growth factor receptor(HER/EGFR)family,since it has negligible kinase activity.Therefore,HER3 must interact with a kinase-profici... Human epidermal growth factor receptor 3(HER3)is a unique member of the human epidermal growth factor receptor(HER/EGFR)family,since it has negligible kinase activity.Therefore,HER3 must interact with a kinase-proficient receptor to form a heterodimer,leading to the activation of signaling cascades.Overexpression of HER3 is observed in various human cancers,including non-small cell lung cancer(NSCLC),and correlates with poor clinical outcomes in patients.Studies on the underlying mechanism demonstrate that HER3-initiated signaling promotes tumor metastasis and causes treatment failure in human cancers.Upregulation of HER3 is frequently observed in EGFR-mutant NSCLC treated with EGFR-tyrosine kinase inhibitors(TKIs).Increased expression of HER3 triggers the so-called EGFR-independent mechanism via interactions with other receptors to activate“by-pass signaling pathways”,thereby resulting in resistance to EGFR-TKIs.To date,no HER3-targeted therapy has been approved for cancer treatment.In both preclinical and clinical studies,targeting HER3 with a blocking an-tibody(Ab)is the only strategy being examined.Recent evaluations of an anti-HER3 Ab-drug conjugate(ADC)show promising results in patients with EGFR-TKI-resistant NSCLC.Herein,we summarize our understanding of the unique biology of HER3 in NSCLC refractory to EGFR-TKIs,with a focus on its dimerization partners and subsequent activation of signaling pathways.We also discuss the latest development of the therapeutic Abs and ADCs targeting HER3 to abrogate EGFR-TKI resistance in NSCLC. 展开更多
关键词 Human epidermal growth factor receptor 3(HER3) Epidermal growth factor receptor-tyrosine kinase inhibitors(EGFR-TKI) Resistance ANTIBODY antibody-drug conjugate(adc) Non-small cell lung cancer(NSCLC)
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A mild phenoxysilyl linker for self-immolative release of antibody-drug conjugates
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作者 Ding Wei Yurong Mao +5 位作者 Huihui Wang Siqi Qu Jiakang Chen Jiusheng Li Biao Jiang Hongli Chen 《Chinese Chemical Letters》 SCIE CAS CSCD 2023年第5期494-498,共5页
Self-immolative linkers have been widely used to construct prodrugs to improve their efficacy and safety.In this study,we report the use of phenoxysilyl linker as a self-immolative unit to prepare antibody-drug conjug... Self-immolative linkers have been widely used to construct prodrugs to improve their efficacy and safety.In this study,we report the use of phenoxysilyl linker as a self-immolative unit to prepare antibody-drug conjugates(ADCs).Phenoxysily based ADC Ate-PPS-CA4 was prepared and its release was systematically investigated by mass spectrometry.Biological evaluation showed that Ate-PPS-CA4 displayed the ability to target delivery and self-immolative release the active payload CA4 on PD-L1 positive cells MDA-MB-231.As the same with its payload CA4,it could arrest the cell cycle to the G2/M phase and induced changes in cell morphology at the dose of its IC_(50).The development of this linker with novel drug release mechanisms will expand the methodology to construct ADCs,especially for non-internalizing ADCs by extracellular cleavage. 展开更多
关键词 antibody-drug conjugates Self-immolative release Phenoxysilyl linker Combretastatin A4(CA4)
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Trastuzumab-Doxorubicin Conjugate Provides Enhanced Anti-Cancer Potency and Reduced Cardiotoxicity
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作者 Ningyan Zhang Melvin E. Klegerman +3 位作者 Hui Deng Yun Shi Eva Golunski Zhiqiang An 《Journal of Cancer Therapy》 2013年第1期308-322,共15页
Since trastuzumab monotherapy for treatment of breast cancer with HER2/ErbB2 over-expression has been shown to have limited efficacy, combined treatment of trastuzumab with chemotherapy is widely practiced in clinic. ... Since trastuzumab monotherapy for treatment of breast cancer with HER2/ErbB2 over-expression has been shown to have limited efficacy, combined treatment of trastuzumab with chemotherapy is widely practiced in clinic. However, certain combination treatments of trastuzumab and chemotherapy (i.e. doxorubicin) are not recommended due to high risk of cardiotoxicity. Antibody-drug conjugates (ADCs) offer selective delivery of cytotoxic agents into targeted cancer cells, thereby allowing for reduced general cellular cytotoxicity caused by chemotherapeutic agents through antibody mediated specific recognition of tumor antigens. In this study, we constructed a trastuzumab-doxorubicin conjugate (T-Dox) using a thioether linkage and characterized both biophysical stability and anti-cancer potency of the T-Dox using a panel of HER2 expressing cancer cell lines. The T-Dox conjugate showed significantly improved anti-cancer potency in comparison with trastuzumab. The results demonstrated for the first time that there were significant differences in the uptake of T-Dox among high HER2 expression cancer cells and higher T-Dox uptake also showed stronger anti-cancer potency. Similar to trastuzumab, T-Dox selectively bound to HER2 overexpressing cancer cells and low HER2 expression cells had no detectable uptake of T-Dox. Consistent to the uptake data, human cardiomyocyte cells had no detectable HER2 expression and T-Dox showed minimal cytotoxic effects. On the contrary, a treatment with combination of trastuzumab and doxorubicin showed severe cytotoxicity to human cardiomyocytes (>90% cell death after 3 day exposure). This study demonstrated that trastuzumab conjugated with doxorubicin (T-Dox) can provide valuable alternative to the combination treatment with doxorubicin and trastuzumab for high HER2 expressing cancer patients. 展开更多
关键词 Antibody Drug conjugATE adc TRASTUZUMAB DOXORUBICIN CARDIOTOXICITY HER2/ErbB2 INTERNALIZATION
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靶向Trop2的抗体偶联药物治疗三阴性乳腺癌的研究进展 被引量:1
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作者 林云 张妍(综述) 陈曦(审校) 《中国肿瘤临床》 CAS CSCD 北大核心 2023年第18期946-950,共5页
乳腺癌是目前全球发病率最高的恶性肿瘤之一,其中三阴性乳腺癌(triple-negative breast cancer,TNBC)占浸润性乳腺癌的10%~20%。TNBC是一种高度异质性和侵袭性的恶性肿瘤,与其他乳腺癌亚型相比,TNBC治疗手段相对匮乏,预后较差,临床上亟... 乳腺癌是目前全球发病率最高的恶性肿瘤之一,其中三阴性乳腺癌(triple-negative breast cancer,TNBC)占浸润性乳腺癌的10%~20%。TNBC是一种高度异质性和侵袭性的恶性肿瘤,与其他乳腺癌亚型相比,TNBC治疗手段相对匮乏,预后较差,临床上亟待寻找可用于精准治疗及提高预后的新靶点。人滋养层细胞表面抗原2(trophoblast cell surface antigen 2,Trop2)在三阴性乳腺癌及多种恶性肿瘤中高表达,其通过细胞表面受体信号在肿瘤细胞的增殖、黏附、侵袭、转移中发挥重要作用,以其为靶点的抗体偶联药物(antibody-drug conjugate,ADC)在临床上中具有广阔的应用前景。本文对靶向Trop2的ADC治疗TNBC的临床研究进展予以综述,为靶向Trop2的ADC在TNBC治疗中的临床应用和提高患者生存预后方面提供参考。 展开更多
关键词 三阴性乳腺癌 滋养层细胞表面抗原2 抗体偶联药物 研究进展
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Bispecific antibodies targeting immunomodulatory checkpoints for cancer therapy 被引量:3
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作者 Tiancheng Zhang Youpei Lin Qiang Gao 《Cancer Biology & Medicine》 SCIE CAS CSCD 2023年第3期181-195,共15页
Advances in antibody engineering have led to the generation of more innovative antibody drugs,such as bispecific antibodies(bs Abs).Following the success associated with blinatumomab,bs Abs have attracted enormous int... Advances in antibody engineering have led to the generation of more innovative antibody drugs,such as bispecific antibodies(bs Abs).Following the success associated with blinatumomab,bs Abs have attracted enormous interest in the field of cancer immunotherapy.By specifically targeting two different antigens,bs Abs reduce the distance between tumor and immune cells,thereby enhancing tumor killing directly.There are several mechanisms of action upon which bs Abs have been exploited.Accumulating experience on checkpoint-based therapy has promoted the clinical transformation of bs Abs targeting immunomodulatory checkpoints.Cadonilimab(PD-1×CTLA-4)is the first approved bs Ab targeting dual inhibitory checkpoints,which confirms the feasibility of bs Abs in immunotherapy.In this review we analyzed the mechanisms by which bs Abs targeting immunomodulatory checkpoints and their emerging applications in cancer immunotherapy. 展开更多
关键词 antibody-drug conjugate bispecific antibody IMMUNOTHERAPY tumor microenvironment clinical trials
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Targeting triple-negative breast cancer:A clinical perspective 被引量:3
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作者 LAZAR S.POPOVIC GORANA MATOVINA-BRKO +3 位作者 MAJA POPOVIC KEVIN PUNIE ANA CVETANOVIC MATTEO LAMBERTINI 《Oncology Research》 SCIE 2023年第3期221-238,共18页
Triple-negative breast cancer(TNBC)is a disease with often an aggressive course and a poor prognosis compared to other subtypes of breast cancer.TNBC accounts for approximately 10%–15%of all diagnosed breast cancer c... Triple-negative breast cancer(TNBC)is a disease with often an aggressive course and a poor prognosis compared to other subtypes of breast cancer.TNBC accounts for approximately 10%–15%of all diagnosed breast cancer cases and represents a high unmet need in the field.Up to just a few years ago,chemotherapy was the only systemic treatment option for this subtype(1).To date,TNBC is considered a heterogeneous disease.One of the existing classifications is based on the analysis of mRNA expression in 587 TNBC cases,in which Lehman et al.proposed six subtypes of TNBC as follows:two basal-like(BL1 and BL2)subtypes,a mesenchymal(M)subtype,a mesenchymal stem-like(MSL)subtype,an immunomodulatory(IM)subtype,and a luminal androgen receptor(LAR)subtype(2).Later studies have demonstrated that the IM and MSL subtypes do not correlate with independent subtypes but reflect background expression by dense infiltration of tumor-infiltrating lymphocytes(TILs)or stromal cells.According to this finding,the classification of TNBC has been revised into the following four subtypes:basal 1,basal 2,LAR,and mesenchymal subtypes(3).Over the last years,several new strategies have been investigated for the treatment of patients with TNBC.Among them,immunotherapy,antibody drug conjugates,new chemotherapy agents,and targeted therapy have been and are currently being developed.The present article aims to provide an updated overview on the different treatment options that are now available or are still under investigation for patients with TNBC. 展开更多
关键词 Triple-negative breast cancer IMMUNOTHERAPY antibody-drug conjugates Target therapy
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Antibody-drug conjugates: recent advances in conjugation and linker chemistries 被引量:52
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作者 Kyoji Tsuchikama Zhiqiang An 《Protein & Cell》 SCIE CAS CSCD 2018年第1期33-46,共14页
The antibody-drug conjugate (ADC), a humanized or human monoclonal antibody conjugated with highly cytotoxic small molecules (payloads) through chemical linkers, is a novel therapeutic format and has great potenti... The antibody-drug conjugate (ADC), a humanized or human monoclonal antibody conjugated with highly cytotoxic small molecules (payloads) through chemical linkers, is a novel therapeutic format and has great potential to make a paradigm shift in cancer chemother- apy. This new antibody-based molecular platform enables selective delivery of a potent cytotoxic payload to target cancer cells, resulting in improved efficacy, reduced systemic toxicity, and preferable pharmacokinetics (PK)I pharmacodynamics (PD) and biodistribution compared to traditional chemotherapy. Boosted by the successes of FDA-approved Adcetris~ and Kadcyla~, this drug class has been rapidly growing along with about 60 ADCs cur- rently in clinical trials. In this article, we briefly review molecular aspects of each component (the antibody, payload, and linker) of ADCs, and then mainly discuss traditional and new technologies of the conjugation and linker chemistries for successful construction of clini- cally effective ADCs. Current efforts in the conjugation and linker chemistries will provide greater insights into molecular design and strategies for clinically effective ADCs from medicinal chemistry and pharmacology standpoints. The development of site-specific conjuga- tion methodologies for constructing homogeneous ADCs is an especially promising path to improving ADC design, which will open the way for novel cancer therapeutics. 展开更多
关键词 antibody-drug conjugates cancer chemotherapy conjugATION LINKER site-specific conjugation
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Antibody-drug conjugates:Recent advances in linker chemistry 被引量:14
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作者 Zheng Su Dian Xiao +5 位作者 Fei Xie Lianqi Liu Yanming Wang Shiyong Fan Xinbo Zhou Song Li 《Acta Pharmaceutica Sinica B》 SCIE CAS CSCD 2021年第12期3889-3907,共19页
Antibody-drug conjugates(ADCs)are gradually revolutionizing clinical cancer therapy.The antibody-drug conjugate linker molecule determines both the efficacy and the adverse effects,and so has a major influence on the ... Antibody-drug conjugates(ADCs)are gradually revolutionizing clinical cancer therapy.The antibody-drug conjugate linker molecule determines both the efficacy and the adverse effects,and so has a major influence on the fate of ADCs.An ideal linker should be stable in the circulatory system and release the cytotoxic payload specifically in the tumor.However,existing linkers often release payloads nonspecifically and inevitably lead to off-target toxicity.This defect is becoming an increasingly important factor that restricts the development of ADCs.The pursuit of ADCs with optimal therapeutic windows has resulted in remarkable progress in the discovery and development of novel linkers.The present review summarizes the advance of the chemical trigger,linker-antibody attachment and linker-payload attachment over the last 5 years,and describes the ADMET properties of ADCs.This work also helps clarify future developmental directions for the linkers. 展开更多
关键词 antibody-drug conjugate LINKER Chemical trigger Linker-antibody attachment Linker-payload attachment
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晚期胆道癌抗HER-2治疗临床研究进展 被引量:1
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作者 杨帆 秦叔逵 《临床肿瘤学杂志》 CAS 2023年第9期842-848,共7页
胆道癌(BTC)是起源于胆管上皮的一组恶性肿瘤,异质性高,治疗棘手,预后差,生存期短。晚期BTC的治疗既往主要依赖于化疗,新近免疫联合化疗一线治疗已获得成功;同时,随着对胆道肿瘤的基因组和蛋白组特征认识的不断加深,业已明确其分子分型... 胆道癌(BTC)是起源于胆管上皮的一组恶性肿瘤,异质性高,治疗棘手,预后差,生存期短。晚期BTC的治疗既往主要依赖于化疗,新近免疫联合化疗一线治疗已获得成功;同时,随着对胆道肿瘤的基因组和蛋白组特征认识的不断加深,业已明确其分子分型,且发现了若干分子生物标志物,因此靶向药物在二线治疗BTC的研究如火如荼,正在改变BTC的治疗格局和结局。抗人表皮生长因子受体-2(HER-2)治疗,已在乳腺癌和胃癌等多种肿瘤的治疗中显著改善患者预后,现正在积极探索用于治疗BTC,初步显示了可期的美好前景。本文简要综述了抗HER-2治疗BTC的临床研究进展,提出需要进一步开展基于分子生物标志物HER-2驱动的随机对照、大规模的多中心Ⅲ期研究。 展开更多
关键词 胆道癌 靶向治疗 抗HER-2单抗 酪氨酸激酶抑制剂(TKI) 抗体偶联药物(adc)
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