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一种溶酶体靶向的原位自组装短肽设计及抗肿瘤活性研究

Design of a Lysosome Targeting in situ Self-assembly Peptide and Its Antitumor Activity
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摘要 肿瘤已成为威胁人类生命的一大杀手,目前主要采用手术和放、化疗等手段进行治疗,但由于放、化疗的细胞选择性差、毒副作用明显且易引起肿瘤细胞产生耐受(/药)性,不利于肿瘤的持续治疗,因此亟待研发具有定向定位优势、毒副作用低的新型靶向药物.原位自组装多肽能识别肿瘤部位的特异性高表达物质,在肿瘤部位靶向性聚集形成稳定的纳米结构,实现精准和高效治疗,有望成为一种新型的抗肿瘤药物.本研究基于多肽原位自组装的设计理念,利用溶酶体内组织蛋白酶L的催化活性,设计了靶向溶酶体且能够原位自组装的多肽分子Fmoc-FFRIKFERQ-OH,研究了该分子的自组装特性及抗肿瘤活性.结果显示,在体外酸性条件下,组织蛋白酶L能精准切割Fmoc-FFRIKFERQ-OH分子,其酶切产物FmocFFR-OH自组装形成长纳米纤维结构,对肿瘤细胞A375和SH-SY5Y均具有较好的杀伤作用.该分子通过靶向溶酶体杀伤肿瘤细胞且对正常细胞的毒性较低,有望成为一种新型的抗肿瘤药物. Tumor has greatly threatened to human life.Now the main means of tumor treatment are surgery and(/or)chemoradiotherapy.However,the chemoradiotherapy is usually not suitable to sustained treatment of tumors due to its poor cell selectivity,side effects and inducing tumor cells resistance.Therefore,it is urgent to develop new drugs with low toxicity and high activity at the tumor sites.In situ self-assembly peptides which can target the tumors and self-assemble into specific nanostructures induced by the specific and highly expressed substances at the tumor tissues are expected to be a new kind of anti-tumor drugs.In this study,we designed a peptide denoted as Fmoc-FFRIKFERQ-OH based on the concept of in situ self-assembly of peptides.This peptide can target lysosomes and self-assemble in situ after being degraded by cathepsin L in lysosomes.The selfassembly properties of Fmoc-FFRIKFERQ-OH and its enzymolysis products degraded by cathepsin L were oberved by AFM and MALDI-TOF-MS.The anti-tumor activity of this peptide was measured by using the MTT and flow cytometry assay.The results demonstrated that cathepsin L could precisely hydrolyze the FmocFFRIKFERQ-OH molecule under acidic conditions in vitro,and its enzymolysis product Fmoc-FFR-OH selfassembled into long nanofibers,which had high antitumor activity against both A375 and SH-SY5 Y cells.The relative survival rate was only 36.08%and 25.56%for A375 and SH-SY5 Y,respectively.Comparatively,FmocFFRIKFERQ-OH had lower toxic and side effects on normal cells L929.The self-assembled long fibers formed by Fmoc-FFR-OH can disrupt the membrane of lysosome,which can induce cell apoptosis and(/or)death.Thus,the designed Fmoc-FFRIKFERQ-OH is expected to be a new anti-tumor drug due to its high antitumor activity and low toxicity against to normal cells.
作者 陈翠霞 彭晓婷 朱钰婷 郝瑞瑞 杨柳新 王彤 牛晓雅 赵玉荣 CHEN Cui-Xia;PENG Xiao-Ting;ZHU Yu-Ting;HAO Rui-Rui;YANG Liu-Xin;WANG Tong;NIU Xiao-Ya;ZHAO Yu-Rong(Centre for Bioengineering and Biotechnology,China University of Petroleum(EastChina),Qingrdao 266580,China)
出处 《生物化学与生物物理进展》 SCIE CAS CSCD 北大核心 2021年第2期204-213,共10页 Progress In Biochemistry and Biophysics
基金 中央高校自主创新项目(18CX05012A,18CX02119A)资助。
关键词 溶酶体靶向 多肽原位自组装 酶响应性 抗肿瘤活性 lysosomal targeting self-assembly of peptides in situ enzymatic response anti-tumor activity
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  • 1Kirshke H,Barrett A J.Chemistry of Lysosomal Proteases[M] //Lysosomes:Their Role in Protein Breaks Down.London:Academic Press,1987:193-238.
  • 2Mason R W,Green G D J,Barrett A J.Human Liver Cathepsin L[J].Biochem,1985,226:233-241.
  • 3Yamashita M,Konagaya S.Purification and Characterization of Cathepsin L from the White Muscle of Chum Salmon,Oncorhynchus Keta[J].Comp Biochem Physiol,1990,96B(2):247-252.
  • 4Lee J J,Chen H C,Jiang S T.Purification and Characterization of Proteinases Identified as Cathepsins L and L-like (58 KDa) Proteinase from Mackerel[J].Biosci Biotech Biochem,1993,57(9):1470-1476.
  • 5Aranishi F,Ogata H,Hara K.Purification and Characterization of Cathepsin L from Hepatopancreas of Carp Cyprinus Carpio[J].CompBiochem Physiol,1997,118B(3):532-537.
  • 6Visessanguan W,Benjakul S,An H.Purification and Characterization of Cathepsin L in Arrowtooth Flounder (Atheresthes stomias) Muscle[J].Comp Biochem Physiol,2003,134B:477-487.
  • 7Mason R W.Species Variants of Cathepsin L and Their Immunological Identification[J].Biochem,1986,240:285-288.
  • 8Mason R W,Taylor M A,Etheringtom D J.The Purification and Properties of Cathepsin L from Rabbit Liver[J].Biochem,1984,217:209-217.
  • 9Dofour E,Obled A,Valin C,et al.Purification and Amino Acid Sequence of Chicken Liver Cathepsin L[J].Biochem,1987,26:689-5695.
  • 10Yamashita M,Konagaya S.Participation of Cathepsin L Into Extensive Softening of the Muscle of Chum Salmon Caought During Spawning Migration[J].Nippon Suisan Gakkaishi,1990,56(8):1271-1277.

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