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Recent progress in targeting the sialylated glycan-SIGLEC axis in cancer immunotherapy 被引量:3
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作者 Yingyan Yu Wenjie Peng 《Cancer Biology & Medicine》 SCIE CAS CSCD 2023年第5期369-384,共16页
Malignant tumors are complex structures composed of cancer cells and tumor microenvironmental cells.In this complex structure,cells cross-talk and interact,thus jointly promoting cancer development and metastasis.Rece... Malignant tumors are complex structures composed of cancer cells and tumor microenvironmental cells.In this complex structure,cells cross-talk and interact,thus jointly promoting cancer development and metastasis.Recently,immunoregulatory molecule-based cancer immunotherapy has greatly improved treatment efficacy for solid cancers,thus enabling some patients to achieve persistent responses or cure.However,owing to the development of drug-resistance and the low response rate,immunotherapy against the available targets PD-1/PD-L1 or CTLA-4 has limited benefits.Although combination therapies have been proposed to enhance the response rate,severe adverse effects are observed.Thus,alternative immune checkpoints must be identified.The SIGLECs are a family of immunoregulatory receptors(known as glyco-immune checkpoints)discovered in recent years.This review systematically describes the molecular characteristics of the SIGLECs,and discusses recent progress in areas including synthetic ligands,monoclonal antibody inhibitors,and Chimeric antigen receptor T(CAR-T)cells,with a focus on available strategies for blocking the sialylated glycan-SIGLEC axis.Targeting glyco-immune checkpoints can expand the scope of immune checkpoints and provide multiple options for new drug development. 展开更多
关键词 SIGLEC sialylated glycan glyco-immune checkpoint high affinity SIGLEC-ligands anti-SIGLEC antibodies
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Fragmentation stability and retention time-shift obtained by LC-MS/MS to distinguish sialylated N-glycan linkage isomers in therapeutic glycoproteins
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作者 Chi Soo Park Minju Kang +7 位作者 Ahyeon Kim Chulmin Moon Mirae Kim Jieun Kim Subin Yang Leeseul Jang Ji Yeon Jang Ha Hyung Kim 《Journal of Pharmaceutical Analysis》 SCIE CAS CSCD 2023年第3期305-314,共10页
Sialylated N-glycan isomers withα2-3 orα2-6 linkage(s)have distinctive roles in glycoproteins,but are difficult to distinguish.Wild-type(WT)and glycoengineered(mutant)therapeutic glycoproteins,cytotoxic T lymphocyte... Sialylated N-glycan isomers withα2-3 orα2-6 linkage(s)have distinctive roles in glycoproteins,but are difficult to distinguish.Wild-type(WT)and glycoengineered(mutant)therapeutic glycoproteins,cytotoxic T lymphocyte-associated antigen-4-immunoglobulin(CTLA4-Ig),were produced in Chinese hamster ovary cell lines;however,their linkage isomers have not been reported.In this study,N-glycans of CTLA4-Igs were released,labeled with procainamide,and analyzed by liquid chromatography-tandem mass spectrometry(MS/MS)to identify and quantify sialylated N-glycan linkage isomers.The linkage isomers were distinguished by comparison of 1)intensity of the N-acetylglucosamine ion to the sialic acid ion(Ln/Nn)using different fragmentation stability in MS/MS spectra and 2)retention time-shift for a selective m/z value in the extracted ion chromatogram.Each isomer was distinctively identified,and each quantity(>0.1%)was obtained relative to the total N-glycans(100%)for all observed ionization states.Twenty sialylated N-glycan isomers with onlyα2-3 linkage(s)in WT were identified,and each isomer's sum of quantities was 50.4%.Furthermore,39 sialylated N-glycan isomers(58.8%)in mono-(3 N-glycans;0.9%),bi-(18;48.3%),tri-(14;8.9%),and tetra-(4;0.7%)antennary structures of mutant were obtained,which comprised mono-(15 N-glycans;25.4%),di-(15;28.4%),tri-(8;4.8%),and tetra-(1;0.2%)sialylation,respectively,with onlyα2-3(10 N-glycans;4.8%),bothα2-3 andα2-6(14;18.4%),and onlyα2-6(15;35.6%)linkage(s).These results are consistent with those forα2-3 neuraminidase-treated N-glycans.This study generated a novel plot of Ln/Nn versus retention time to distinguish sialylated N-glycan linkage isomers in glycoprotein. 展开更多
关键词 Therapeutic glycoprotein SIALYLATION Linkage isomer LC-MS/MS
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Tandem Mass Spectrometric Characterization of Fetuin Sialylated Glycopeptides Enriched by Ti02 Microcolumn 被引量:1
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作者 王文静 刘辉 李智立 《Chinese Journal of Chemistry》 SCIE CAS CSCD 2011年第11期2229-2235,共7页
Sialylation of glycoproteins is vital for the function or physicochemical properties of a protein. It becomes more and more important to develop approaches that can be used to efficiently isolate and identify sialylat... Sialylation of glycoproteins is vital for the function or physicochemical properties of a protein. It becomes more and more important to develop approaches that can be used to efficiently isolate and identify sialylated glycopep- tides or glycoproteins for monitoring changes in glycoproteome. In the present study, we analyze intact structures of the enriched sialylated glycopeptides of bovine fetuin by matrix-assisted laser desorption/ionization-tandem mass spectrometry (MALDI-MS/MS), without any chemical derivation. The experimental data show that the optimal loading buffer for TiO2 as matrix is 80% acetonitrile/2% TFA (trifluoroacetic acid)/100 mg/mL DHB (2,5-dihydroxybenzoic acid) which is also compatible with MALDI-mass spectrometric analysis. This study indi- cates that the improved enrichment approach combined with MALDI-MS/MS may be a powerful tool to analyze intact structures and components of the sialylated glycopeptides from complex peptide mixture. 展开更多
关键词 sialylated glycopeptide titanium dioxide sialylated glycan structure MALDI-MS/MS
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Chemoenzymatic synthesis of α2–3-sialylated carbohydrate epitopes
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作者 HUANG ShengShu YU Hai CHEN Xi 《Science China Chemistry》 SCIE EI CAS 2011年第1期117-128,共12页
Sialic acids are common terminal carbohydrates on cell surface.Together with internal carbohydrate structures,they play important roles in many physiological and pathological processes.In order to obtain α2–3-sialyl... Sialic acids are common terminal carbohydrates on cell surface.Together with internal carbohydrate structures,they play important roles in many physiological and pathological processes.In order to obtain α2–3-sialylated oligosaccharides,a highly efficient one-pot three-enzyme synthetic approach was applied.The P.multocida α2–3-sialyltransferase (PmST1) involved in the synthesis was a multifunctional enzyme with extremely flexible donor and acceptor substrate specificities.Sialyltransferase acceptors,including type 1 structure (Galβ1–3GlcNAcβProN3),type 2 structures (Galβ1–4GlcNAcβProN3 and 6-sulfo-Galβ1– 4GlcNAcβProN3),type 4 structure (Galβ1–3GalNAcβProN3),type 3 or core 1 structure (Galβ1–3GalNAcβProN3) and human milk oligoscaccharide or lipooligosaccharide lacto-N-tetraose (LNT) (Galβ1–3GlcNAcβ1–3Galβ1–4GlcβProN3),were chemically synthesized.They were then used in one-pot three-enzyme reactions with sialic acid precursor ManNAc or ManNGc,to synthesize a library of naturally occurring β2–3-linked sialosides with different internal sugar structures.The sialylated oligosaccharides obtained are valuable probes for their biological studies. 展开更多
关键词 CARBOHYDRATE chemoenzymatic synthesis sialic acid SIALYLATION SIALYLTRANSFERASE
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Insights on the molecular mechanism of neuroprotection exerted by edible bird’s nest and its bioactive constituents
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作者 Weiyi Chu Chia Wei Phan +1 位作者 Seng Joe Lim Abdul Salam Babji 《Food Science and Human Wellness》 SCIE CSCD 2023年第4期1008-1019,共12页
Neurodegenerative diseases are often associated with the accumulation of oxidative stress and neuroinflammation.Edible bird’s nest(EBN)is a glycoprotein(sialylated mucin glycopeptides)found to be beneficial against n... Neurodegenerative diseases are often associated with the accumulation of oxidative stress and neuroinflammation.Edible bird’s nest(EBN)is a glycoprotein(sialylated mucin glycopeptides)found to be beneficial against neurodegenerative diseases.Antioxidative,anti-inflammatory,and anti-apoptotic properties of EBN in preserving neuronal cells were widely researched using in vitro and in vivo models.Functional effects of EBN are often linked to its great number of antioxidants and anti-inflammatory glycopeptides.Bioactive compounds in EBN,especially sialic acid,add value to neurotrophic potential of EBN and contribute to neuronal repair and protection.Various studies reporting the neuroprotective effects of EBN,their molecular mechanisms,and neuroactive composition were gathered in this review to provide better insights on the neuroprotective effects of EBN. 展开更多
关键词 Antioxidant Composition Edible bird nest Neurodegenerative disease NEUROPROTECTION sialylated mucin glycopeptide
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体外评价携Sialyl Lewis^x和抗ICAM-1单抗双配体超声微泡的靶向黏附性能 被引量:6
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作者 李美瑜 肖云彬 +6 位作者 宾建国 吴爵非 杨莉 胡广全 刘莹 黄瑞珠 宾建平 《中国医学影像技术》 CSCD 北大核心 2010年第7期1209-1213,共5页
目的构建携Sialyl Lewisx和抗ICAM-1单抗双配体和同型对照单配体靶向超声微泡,体外对比评价其靶向黏附性能。方法采用"亲和素-生物素"桥接法构建携Sialyl Lewisx与抗ICAM-1单抗双配体(MB-D)、携Sialyl Lewisx(MB-S)和携抗ICA... 目的构建携Sialyl Lewisx和抗ICAM-1单抗双配体和同型对照单配体靶向超声微泡,体外对比评价其靶向黏附性能。方法采用"亲和素-生物素"桥接法构建携Sialyl Lewisx与抗ICAM-1单抗双配体(MB-D)、携Sialyl Lewisx(MB-S)和携抗ICAM-1单抗(MB-I)三种靶向超声微泡,以流式细胞术定量分析其配体结合率,并利用平行板流动腔分别在0.5、2.0和4.0dyn/cm2三种剪切应力下的不同时间点观察微泡的结合及解离情况。结果 MB-D、MB-S和MB-I的配体结合率均达85%以上,各组间无统计学差异(P>0.05)。在三种剪切应力下,MB-D和MB-S集中于前3~5min高效结合,在5min后两者的结合率均呈平台状态,而MB-I全程结合率(1~6min)均呈低水平状态;MB-D的平均结合率和全程结合数目均明显高于MB-S和MB-I(P<0.05),而半数解离剪切应力则按MB-I、MB-D和MB-S顺序依次递减(P<0.05)。结论相同条件下,MB-S表现为早期快速、不稳定的黏附,MB-I为缓慢、牢固的结合,而MB-D呈早期高效、相对牢固的结合。MB-D有可能用于高流速的动脉超声分子成像。 展开更多
关键词 微泡 造影剂 平行板流动腔 SIALYL Lewis^x 细胞间黏附分子-1
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Sialyl Lewis-X抗原在大肠癌肝转移中的作用研究及临床意义 被引量:6
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作者 李小卫 刘平 丁彦青 《临床肿瘤学杂志》 CAS 2006年第4期269-273,共5页
目的探讨SialylLewis-X(SLeX)抗原在大肠癌肝转移中的作用及临床意义。方法采用大肠癌Lovo、HT29细胞与人脐静脉血管内皮及内皮细胞的粘附试验,分别用扫描电镜及透射电镜观察Lovo、HT29细胞与脐静脉血管内皮及内皮细胞的粘附性及SLeX单... 目的探讨SialylLewis-X(SLeX)抗原在大肠癌肝转移中的作用及临床意义。方法采用大肠癌Lovo、HT29细胞与人脐静脉血管内皮及内皮细胞的粘附试验,分别用扫描电镜及透射电镜观察Lovo、HT29细胞与脐静脉血管内皮及内皮细胞的粘附性及SLeX单抗封闭大肠癌细胞后,这种粘附性的改变;采用实验性裸鼠大肠癌肝转移模型分别观察SLeX单抗封闭Lovo、HT29细胞前后对实验性裸鼠大肠癌肝转移的影响。结果高表达SLeX抗原的Lovo细胞与脐静脉血管内皮的粘附性较低表达SLeX抗原的HT29细胞强,Lovo细胞与脐静脉血管内皮细胞的连接方式与HT29细胞明显不同;高表达SLeX抗原的Lovo细胞引起裸鼠肝转移率高于低表达SLeX抗原的HT29细胞。结论大肠癌细胞表面SLeX抗原在大肠癌细胞与脐静脉血管内皮细胞的粘附及实验性裸鼠肝转移中起重要作用,SLeX单抗能有效地抑制肿瘤细胞与脐静脉血管内皮细胞的粘附,并能降低实验性裸鼠肝转移的形成。 展开更多
关键词 SIALYL LEWIS-X 大肠癌 肝转移
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Sialyl Lewis-X抗原在大肠癌LoVo、HT29细胞系及大肠癌肝转移组织中表达的临床意义 被引量:3
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作者 李小卫 刘平 丁彦青 《临床肿瘤学杂志》 CAS 2010年第6期526-528,共3页
目的探讨具有高低转移潜能的大肠癌LoVo细胞、HT29细胞和大肠癌肝转移组织Sialyl Lewis-X(SLeX)抗原表达的临床意义。方法采用免疫组化方法检测LoVo细胞、HT29细胞和原发性大肠癌、大肠癌肝转移组织SLeX抗原表达情况。结果具有高转移潜... 目的探讨具有高低转移潜能的大肠癌LoVo细胞、HT29细胞和大肠癌肝转移组织Sialyl Lewis-X(SLeX)抗原表达的临床意义。方法采用免疫组化方法检测LoVo细胞、HT29细胞和原发性大肠癌、大肠癌肝转移组织SLeX抗原表达情况。结果具有高转移潜能的LoVo细胞SLeX抗原表达强于HT29细胞(P<0.05)。原发性大肠癌高、中分化腺癌之间,高、低分化腺癌之间,中、低分化腺癌之间SLeX抗原表达均有显著性差异(P<0.05)。转移灶中SLeX抗原表达强于原发灶SLeX抗原表达(P<0.01)。结论检测SLeX抗原对判断大肠癌肝转移及评估预后有重要意义。 展开更多
关键词 SIALYL Lewis-X/SleX LoVo细胞 HT29细胞 大肠癌 肝转移
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携Sialyl Lewis^X与携抗P-选择素单抗靶向超声微泡粘附性的对比研究 被引量:5
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作者 李军华 吴爵非 +5 位作者 杨莉 刘俭 谢佳佳 纪丽景 燕翼 宾建平 《临床超声医学杂志》 2009年第3期145-148,共4页
目的对比评价携sialylLewis。与携抗P-选择素单抗靶向超声微泡粘附特性。方法采用“亲和素-生物素”桥接法构建携Sialyl Lewis、(MB-S)、携抗P-选择素单抗靶向超声微泡(MB-P)及携同型抗体微泡(MB-C)。MB-S、MB-P及MB-C以相同流速... 目的对比评价携sialylLewis。与携抗P-选择素单抗靶向超声微泡粘附特性。方法采用“亲和素-生物素”桥接法构建携Sialyl Lewis、(MB-S)、携抗P-选择素单抗靶向超声微泡(MB-P)及携同型抗体微泡(MB-C)。MB-S、MB-P及MB-C以相同流速通过相应小鼠P-选择素Fc段包被培养皿时,利用平行板流动腔在不同时间点测定相应的MB-S、MB-P及MB-C(对照组)的结合数目、滚动数目以及解离时达到半数解离的剪切应力。结果MB-S结合数量前3min快速增加,其后随时间增加无明显变化,而MB-P结合数量与时间呈正相关(P〈0.05),且MB-S结合数目是MB-P的2~4倍;对照组MB-C未见明显结合(P〈0.05)。MB-S滚动数目大于MB-P(P〈0.05);MB-S半数解离时剪切力小于MB-P(P〈0.05)。结论靶向超声微泡MB-S表现为早期、快速、不稳定的结合及滚动,MB-P表现为缓慢牢固结合。 展开更多
关键词 超声检查 微气泡 靶向 平行板流动腔 P-选择素单克隆抗体 SIALYL Lewis^X
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食管鳞癌选择素P及其配体sialyl lewis A、sialyl lewis X的表达 被引量:2
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作者 付茂勇 粱敏 +2 位作者 张霖 赵永生 贾维坤 《肿瘤预防与治疗》 2010年第1期5-9,共5页
目的:了解P-选择素及其配体sLeA、sLeX在食管癌组织及区域淋巴结中的表达,探讨其与食管癌侵袭转移的关系。方法:应用组织芯片技术结合免疫组化检测食管鳞癌86例及其淋巴结P-选择素和sialy lewis A(sLeA)、sialylewis X(sLe X)的表达情况... 目的:了解P-选择素及其配体sLeA、sLeX在食管癌组织及区域淋巴结中的表达,探讨其与食管癌侵袭转移的关系。方法:应用组织芯片技术结合免疫组化检测食管鳞癌86例及其淋巴结P-选择素和sialy lewis A(sLeA)、sialylewis X(sLe X)的表达情况,并与16例正常食管鳞状上皮对照。结果:P-选择素在食管癌组织、正常食管鳞状上皮表达率分别为59.3%、12.5%(P<0.05),在转移淋巴结、非转移淋巴结中表达率分别为92.9%、31.3%(P<0.05)。sLeA在食管癌组织,正常食管组织中表达率分别为77.9%、6.25%(P<0.05),在转移淋巴结和非转移淋巴结中表达率分别为97.6%、20.3%(P<0.05)。sLe X食管癌组织、正常食管组织中表达率分别为15.1%、6.25%(P>0.05)。P-选择素和配体sLeA过度表达与食管鳞癌病理分级,TNM分期及淋巴结转移成显著相关性;而配体sLeX在食管癌组织中无过度表达。结论:P-选择素和配体sLeA在食管鳞癌组织、转移淋巴结中表达率明显升高,其与食管癌的侵袭转移有一定关系;配体sLeX与食管癌侵袭转移无关。 展开更多
关键词 食管鳞癌 P-选择素 SIALYL LEWIS A SIALYL LEWIS X
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携Sialyl Lewis^x多聚体微泡超声造影评价小鼠腹主动脉的炎症反应
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作者 伍巍兰 李美瑜 +5 位作者 滕中华 袁野 李莹 赵宗磊 廖禹林 宾建平 《中国介入影像与治疗学》 CSCD 2012年第4期295-299,共5页
目的探讨采用携Sialyl Lewisx多聚体(PSLex)微泡靶向CEUS评价动脉系统血管炎症反应的可行性。方法构建分别携P-Sialyl Lewisx(MB-S)、抗P-选择素单抗(MB-P)和同型对照单抗(MB-C)的3种微泡,应用流式细胞仪分析其配体结合率,利用平行板流... 目的探讨采用携Sialyl Lewisx多聚体(PSLex)微泡靶向CEUS评价动脉系统血管炎症反应的可行性。方法构建分别携P-Sialyl Lewisx(MB-S)、抗P-选择素单抗(MB-P)和同型对照单抗(MB-C)的3种微泡,应用流式细胞仪分析其配体结合率,利用平行板流动腔和Image-Pro Plus图像分析软件,分析3种微泡在0.5、2.0和4.0dyn/cm2剪切应力下的靶向结合数目。对急性腹主动脉炎症模型(炎症组)和假手术模型(对照组)小鼠各9只,采用弹丸式注入以上微泡,6min后行CEUS检查,测量腹主动脉显影的声强度(VI)。结果 MB-P、MB-S的配体结合率比较差异无统计学意义(P>0.05)。在3种剪切应力下,MB-S和MB-P的全程(6min)结合数目均高于MB-C(P均<0.05);在0.5dyn/cm2时,MB-S的全程结合数目与MB-P的差异无统计学意义(P>0.05),而在2.0和4.0dyn/cm2时,MB-S的全程结合数目明显多于MB-P(P均<0.05);各种微泡的全程结合数目均随剪切应力提高而减少(P均<0.05)。在炎症组中,MB-S、MB-P和MB-C的VI值依次降低(P均<0.05);除MB-C外,MB-S和MB-P在炎症组的VI值均分别高于对照组(P均<0.05)。结论在高剪切应力下MB-S的结合能力明显优于MB-P,可用于评价动脉血管内皮炎症反应。 展开更多
关键词 SIALYL Lewisx多聚体 靶向微泡 对比超声 腹主动脉炎症反应
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大肠癌组织黏蛋白MUC2和sialyl lewis X联合表达的临床意义
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作者 于秀文 吴甜 王俊苹 《中国现代医学杂志》 CAS CSCD 北大核心 2013年第25期20-23,共4页
目的探讨大肠腺癌组织粘蛋白MUC2和sialyl lewis X(sLex)的分型与临床各个病理参数之间的关系。方法应用免疫组织化学双染法对34例远切端大肠黏膜、18例大肠腺瘤及55例大肠腺癌组织进行粘蛋白MUC2、sLex检测。结果远切端大肠黏膜、大肠... 目的探讨大肠腺癌组织粘蛋白MUC2和sialyl lewis X(sLex)的分型与临床各个病理参数之间的关系。方法应用免疫组织化学双染法对34例远切端大肠黏膜、18例大肠腺瘤及55例大肠腺癌组织进行粘蛋白MUC2、sLex检测。结果远切端大肠黏膜、大肠腺瘤及大肠腺癌中,黏蛋白MUC2阳性表达率分别为100%、94.4%和58.2%(P<0.01);sLex阳性表达率分别为5.9%、50.0%和80.0%(P<0.05)。根据MUC2和sLex在大肠腺癌中的表达把大肠腺癌分为四型:MUC2+/sLex+、MUC2+/sLex-、MUC2-/sLex+、MUC2-/sLex-。MUC2+/sLex+型与患者的性别具有相关性;MUC2+/sLex-型与淋巴结转移、Duke’s分期具有相关性;MUC2-/sLex+型与发生部位、分化程度具有相关性;MUC2-/sLex-型与大肠腺癌临床病理参数均不具有相关性。结论 MUC2的下调表达或sLex的上调表达可能参与了大肠肿瘤的发生及恶性转化,各型大肠腺癌不同程度与其分化、生物学行为相关,对临床上判断预后具有较大的意义。 展开更多
关键词 大肠腺癌 MUC2 SIALYL LEWIS X
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流式细胞术检测结肠癌细胞表面sialyl-LewisA/X的样品制备方法探讨
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作者 张春 牛英才 +1 位作者 周丽 刘吉成 《医学研究杂志》 2009年第4期28-30,共3页
目的探讨不同样品制备方法对结肠癌细胞表面sialyl LewisA/X抗原的影响。方法应用EDTA、胰酶、细胞刮、胰酶-EDTA、胰酶联用细胞刮刀组制备培养人结肠癌细胞单细胞悬液。采用流式细胞仪检测人结肠癌细胞表面sialyl LewisA/X的表达和细... 目的探讨不同样品制备方法对结肠癌细胞表面sialyl LewisA/X抗原的影响。方法应用EDTA、胰酶、细胞刮、胰酶-EDTA、胰酶联用细胞刮刀组制备培养人结肠癌细胞单细胞悬液。采用流式细胞仪检测人结肠癌细胞表面sialyl LewisA/X的表达和细胞数。结果单用EDTA或细胞刮制备的细胞悬液中细胞产量低,胰酶或胰酶联用细胞刮刀组制备的细胞悬液中细胞产量高。胰酶组细胞表面sialyl LewisA/X的荧光强度明显降低。EDTA组、细胞刮组、胰酶联合细胞刮组间sialyl LewisA/X的荧光强度表达差异无统计学意义。结论胰酶联用细胞刮法是贴壁培养细胞制备单细胞悬液的一种好方法。 展开更多
关键词 流式细胞术 结肠癌 SIALYL LewisA/X
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应用组织芯片研究sialyl Lewis^x和CD44v6在结肠癌中的表达及意义
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作者 孙守毅 胡小云 +3 位作者 张文昌 李里香 雷英 李从于 《江西医学院学报》 CAS 2009年第5期25-28,140,共5页
目的应用组织芯片研究sialyl Lewisx和CD44v6在结肠癌中的表达及意义。方法应用组织芯片技术和免疫组化技术,检测103例结肠癌组织中sialyl Lewisx和CD44v6的表达,并结合肿瘤的病理学指标和临床随访资料进行分析。结果结肠癌中sialyl Lew... 目的应用组织芯片研究sialyl Lewisx和CD44v6在结肠癌中的表达及意义。方法应用组织芯片技术和免疫组化技术,检测103例结肠癌组织中sialyl Lewisx和CD44v6的表达,并结合肿瘤的病理学指标和临床随访资料进行分析。结果结肠癌中sialyl Lewisx和CD44v6阳性表达率分别为83.5%和82.5%,且晚期结肠癌明显高于早、中期结肠癌(P<0.05);sialyl Lewisx和CD44v6表达具有一致性,且与结肠癌的临床分期、浸润程度、淋巴结及远处转移和预后有关(P<0.05)。结论sialyl Lewisx和CD44v6的表达与结肠癌转移和患者生存期密切相关,联合检测sialyl Lewisx和CD44v6在结肠癌中的表达对于判断其恶性程度、预测生物学行为和评估患者预后具有重要意义。 展开更多
关键词 组织芯片 SIALYL LEWISX CD44V6 结肠癌
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Expression of sialyl Lewis^a relates to poor prognosis in cholangiocarcinoma 被引量:3
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作者 Apa Juntavee Banchob Sripa +2 位作者 Ake Pugkhem Narong Khuntikeo Sopit Wongkham 《World Journal of Gastroenterology》 SCIE CAS CSCD 2005年第2期249-254,共6页
AIM: High levels of serum sialyl Lewisa (sLea) are frequently found in cholangiocarcinoma (CCA) patients and have been suggested to be a serum marker for CCA. However, the significance of this antigen in CCA is unknow... AIM: High levels of serum sialyl Lewisa (sLea) are frequently found in cholangiocarcinoma (CCA) patients and have been suggested to be a serum marker for CCA. However, the significance of this antigen in CCA is unknown. In this study, the clinical significance of sLea expression in CCA tissues and the possible role of sLea in vascular invasion in vitro were elucidated. METHODS: Expression of sLea in tumor tissues of 77 patients with mass-forming CCA and 33 with periductal infiltrating CCA was determined using immunohistochemistry. The in vitro assays on adhesion and transmigration of CCA cells to human umbilical vein endothelial cells were compared between CCA cell lines with and without sLea expression. RESULTS: sLea was aberrantly expressed in 60% of CCA tumor tissues. A significant relationship was found between the frequency of sLea expression and the mass-forming type CCA (P= 0.041), well differentiated histological grading (P=0.029), and vascular invasion (P=0.030). Patients with positive sLea expression had a significantly poorer prognosis (21.28 wk, 95% CI=16.75-25.81 wk) than those negative for sLea (37.30 wk, 95% CI=27.03-47.57 wk) (P<0.001). Multivariate analysis with adjustment for all covariates showed that patients positive for sLea possessed a 2.3-fold higher risk of death than patients negative for sLea (P<0.001). The role of sLea in vascular invasion was demonstrated using in vitro adhesion and transmigration assays. KKU-M213, a human CCA cell-line with a high expression of sLea, adhered and transmigrated to IL-1β-activated endothelial cells of the human umbilical vein more than KKU-100, the line without sLea expression (P<0.001). These processes were significantly diminished when the antibodies specific to either sLea or E-selectin were added to the assays (P<0.001) CONCLUSION: This study demonstrates the clinical significance of sLea expression in vascular invasion, and an unfavorable outcome in CCA. The role of sLea in vascular invasion which may lead to poor prognosis is supported by the in vitro adhesion and transmigration studies. 展开更多
关键词 CHOLANGIOCARCINOMA Sialyl Lewis Poor prognosis
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Inhibition of Adhesion and Metastasis of HepG2 Hepatocellular Carcinoma Cells In Vitro by DNA Aptamer against Sialyl Lewis X 被引量:1
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作者 王小康 彭艳 +9 位作者 陶浩冉 周芬芳 张弛 苏飞 王诗培 刘庆 徐利华 潘雪凯 谢伟 冯茂辉 《Journal of Huazhong University of Science and Technology(Medical Sciences)》 SCIE CAS 2017年第3期343-347,共5页
The sialyl Lewis X(SLe;) antigen encoded by the FUT7 gene is the ligand of endotheliam-selectin(E-selectin). The combination of SLe;antigen and E-selectin represents an important way for malignant tumor metastasis... The sialyl Lewis X(SLe;) antigen encoded by the FUT7 gene is the ligand of endotheliam-selectin(E-selectin). The combination of SLe;antigen and E-selectin represents an important way for malignant tumor metastasis. In the present study, the effect of the SLe;-binding DNA aptamer on the adhesion and metastasis of hepatocellular carcinoma HepG2 cells in vitro was investigated. Reverse transcription-polymerase chain reaction(RT-PCR) and immunofluorescence staining were conducted to detect the expression of FUT7 at both transcriptional and translational levels. The SLe;expression in HepG2 cells treated with different concentrations of SLe;-binding DNA aptamer was detected by flow cytometry. Besides, the adhesion, migration, and invasion of HepG2 cells were measured by cell adhesion assay, and the Transwell migration and invasion assay. The results showed that the FUT7 expression was up-regulated at both mR NA and protein levels in HepG2 cells. SLe;-binding DNA aptamer could significantly decrease the expression of SLe;in HepG2 cells. The cell adhesion assay revealed that the SLe;-binding DNA aptamer could effectively inhibit the interactions between E-selectin and SLe;in the HepG2 cells. Additionally, SLe;-binding DNA aptamers at 20 nmol/L were found to have the similar effect to the monoclonal antibody CSLEX-1. The Transwell migration and invasion assay revealed that the number of penetrating cells on the down-side of Transwell membrane was significantly less in cells treated with 5, 10, 20 nmol/L SLe;-binding DNA aptamer than those in the negative control group(P<0.01). Our study demonstrated that the SLe;-binding DNA aptamer could significantly inhibit the in vitro adhesion, migration, and invasion of HepG2 cells, suggesting that the SLe;-binding DNA aptamer may be used as a potential molecular targeted drug against metastatic hepatocellular carcinoma. 展开更多
关键词 sialyl Lewis X DNA aptamer hepatocellular carcinoma METASTASIS
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Enzymatic Synthesis of Sialyl Lactosamine Grafted Chitooligosaccharides 被引量:1
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作者 Jun Yan Jianghua Li +7 位作者 Zhifei Hu Xiaoyao Ma Yun Li Xihuan Hu Jinfeng Ye Wei Wang Renzhong Wan Hongzhi Cao 《Chinese Journal of Chemistry》 SCIE CAS CSCD 2023年第11期1299-1304,共6页
An efficient enzymatic assembly strategy was developed for the concise synthesis of structurally well-defined sialylated chitooligosaccharides.Two enzyme modules for theβ-1,3-N-acetyl-glucosaminylation andβ-1,4-gala... An efficient enzymatic assembly strategy was developed for the concise synthesis of structurally well-defined sialylated chitooligosaccharides.Two enzyme modules for theβ-1,3-N-acetyl-glucosaminylation andβ-1,4-galactosylation were applied for the grafting N-acetyl lactosamine(LacNAc)unit(s)onto the chitooligosaccharides.The LacNAc grafted chitooligosaccharides were further modified withα-2,3-orα-2,6-sialylation by two enzymatic sialylation modules to generate a total of 20 sialylated chitooligosaccharides.The inhibition study of influenza virus-induced cytopathy with synthetic sialylated chitooligosaccharides indicated that the sialic acid linkage and chain length both contribute to the binding preference and inhibition potency. 展开更多
关键词 CHITOOLIGOSACCHARIDES Sialylation Influenza virus GLYCOSYLATION Biocatalysis Structure-activity relationships
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Sialylation is involved in cell fate decision during development, reprogramming and cancer progression 被引量:5
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作者 Fenjie Li Junjun Ding 《Protein & Cell》 SCIE CAS CSCD 2019年第8期550-565,共16页
Sialylation, or the covalent addition of sialic acid to the terminal end of glycoproteins, is a biologically important modification that is involved in embryonic development, neurodevelopment, reprogramming, oncogenes... Sialylation, or the covalent addition of sialic acid to the terminal end of glycoproteins, is a biologically important modification that is involved in embryonic development, neurodevelopment, reprogramming, oncogenesis and immune responses. In this review, we have given a comprehensive overview of the current literature on the involvement of sialylation in cell fate decision during development, reprogramming and cancer progressionSialylation is essential for early embryonic development and the deletion of UDP-GIcNAc 2-epimerase, a rate-limiting enzyme in sialic acid biosynthesis, is embryonically lethal. Furthermore, the sialyltransferase ST6GAL1 is required for somatic cell reprogramming, and its downregulation is associated with decreased reprogramming efficiency. In addition, sialylation levels and patterns are altered during cancer progression, indicating the potential of sialylated molecules as cancer biomarkers. Taken together, the current evidences demonstrate that sialylation is involved in crucial cell fate decision. 展开更多
关键词 SIALYLATION cell FATE DEVELOPMENT REPROGRAMMING cancer
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E-selectin ligand complexes adopt an extended high-affinity conformation
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作者 Roland C.Preston Roman P.Jakob +3 位作者 Florian P.C.Binder Christoph P.Sager Beat Ernst Timm Maier 《Journal of Molecular Cell Biology》 SCIE CAS CSCD 2016年第1期62-72,共11页
E-selectin is a cell-adhesion molecule of the vascular endothelium that promotes essential leukocyte rolling in the early inflammatory response by binding to glycoproteins containing the tetrasaccharide sialyl Lewisx(... E-selectin is a cell-adhesion molecule of the vascular endothelium that promotes essential leukocyte rolling in the early inflammatory response by binding to glycoproteins containing the tetrasaccharide sialyl Lewisx(sLex).Efficient leukocyte recruitment under vascular flow conditions depends on an increased lifetime of E-selectin/ligand complexes under tensile force in a so-called catch-bond binding mode.Co-crystal structures of a representative fragment of the extracellular E-selectin region with sLex and a glycomimetic antagonist thereof reveal an extended E-selectin conformation,which is identified as a high-affinity binding state of E-selectin by molecular dynamics simulations.Small-angle X-ray scattering experiments demonstrate a direct link between ligand binding and E-selectin conformational transition under static conditions in solution.This permits tracing a series of concerted structural changes connecting ligand binding to conformational stretching as the structural basis of E-selectin catch-bond-mediated leukocyte recruitment.The detailed molecular view of the binding site paves the way for the design of a new generation of selectin antagonists.This is of special interest,since their therapeutic potentialwas recently demonstrated with the pan-selectin antagonists GMI-1070(Rivipansel). 展开更多
关键词 inflammation leukocyte adhesion E-SELECTIN glycomimetic antagonist sialyl Lewisx conformational change
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