<ce:italic>De Novo</ce:italic> Macrocyclic Peptide Inhibitors of Hepatitis B Virus Cellular Entry

Toby Passioura; Koichi Watashi; Kento Fukano; Satomi Shimura; Wakana Saso; Ryo Morishita; Yuki Ogasawara; Yasuhito Tanaka; Masashi Mizokami; Camille Sureau; Hiroaki Suga; Takaji Wakita

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De Novo Macrocyclic Peptide Inhibitors of Hepatitis B Virus Cellular Entry

机译： de novo 丙型肝炎病毒细胞入学癌肽抑制剂

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Hepatitis B virus (HBV) constitutes a significant public health burden, and currently available treatment options are not generally curative, necessitating the development of new therapeutics. Here we have applied random non-standard peptide integrated discovery (RaPID) screening to identify small macrocyclic peptide inhibitors of HBV entry that target the cell-surface receptor for HBV, sodium taurocholate cotransporting polypeptide (NTCP). In addition to their anti-HBV activity, these molecules also inhibit cellular entry by the related hepatitis D virus (HDV), and are active against diverse strains of HBV (including clinically relevant nucleos(t)ide analog-resistant and vaccine escaping strains). Importantly,?these macrocyclic peptides, in contrast to other NTCP-binding HBV entry inhibitors, exhibited no?inhibition of NTCP-mediated bile acid uptake, making them appealing candidates for therapeutic development.

机译：乙型肝炎病毒（HBV）构成了重大的公共卫生负担，目前可用的待遇方面并不是治疗，所以需要开发新的治疗方法。在这里，我们应用随机非标肽整合发现（快速）筛选，以鉴定HBV进入的小型大环肽抑制剂，其靶向HBV的细胞表面受体，牛磺酸钠COTRANSOLDINE多肽（NTCP）。除了抗HBV活性外，这些分子还通过相关的丙型肝炎病毒（HDV）抑制细胞进入，并针对不同的HBV菌株（包括临床相关核（T）IDE模拟和疫苗逃逸菌株）。。重要的是，与其他NTCP结合HBV进入抑制剂相比，这些大环肽表现出没有？抑制NTCP介导的胆酸摄取，使其具有吸引治疗发育的候选者。

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来源
《Cell chemical biology》 |2018年第7期|共10页
作者
Toby Passioura; Koichi Watashi; Kento Fukano; Satomi Shimura; Wakana Saso; Ryo Morishita; Yuki Ogasawara; Yasuhito Tanaka; Masashi Mizokami; Camille Sureau; Hiroaki Suga; Takaji Wakita;
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作者单位

Department of Chemistry Graduate School of Science The University of Tokyo;

Department of Virology II National Institute of Infectious Diseases;

Department of Virology II National Institute of Infectious Diseases;

Department of Virology II National Institute of Infectious Diseases;

Department of Virology II National Institute of Infectious Diseases;

CellFree Sciences Co. Ltd;

Department of Analytical Biochemistry Meiji Pharmaceutical University;

Department of Virology and Liver Unit Nagoya City University Graduate School of Medicinal Sciences;

Genome Medical Sciences Project National Center for Global Health and Medicine;

Laboratoire de Virologie Moléculaire Institut National de la Transfusion Sanguine;

Department of Chemistry Graduate School of Science The University of Tokyo;

Department of Virology II National Institute of Infectious Diseases;

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原文格式 PDF
正文语种 eng
中图分类普通生物学;生物化学;
关键词
macrocyclic; RaPID; HBV; inhibitor; NTCP; bile acid; transporter; entry; cyclosporin; HDV;

机译：宏细胞;快速;HBV;抑制剂;NTCP;胆汁酸;运输器;进入;环孢菌素;HDV;

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3. De Novo Macrocyclic Peptide Inhibitors of Hepatitis B Virus Cellular Entry [J] . Toby Passioura, Koichi Watashi, Kento Fukano, Cell chemical biology . 2018,第7期

机译： de novo 丙型肝炎病毒细胞入学癌肽抑制剂
4. Antimicrobial peptide repertoire of ce:italic>Thitarodes armoricanu/ce:italic>s, a host species of ce:italic>Ophiocordyceps sinensis/ce:italic>, predicted based on de novo transcriptome sequencing and analysis [J] . Infection, Genetics and Evolution: Journal of Molecular Epidemiology and Evolutionary Genetics in Infectious Diseases . 2017,第期

机译：抗微生物肽曲目的＆ Ce：斜体>灰度armoratanu＆ / ce：斜体> s，＆ ce：斜体> ophiocordyceps sinensis＆ / ce：斜体>，基于de novo转录组测序和分析预测
5. Complete ce:italic>de novo/ce:italic> sequencing of antimicrobial peptides in the venom of the scorpion ce:italic>Isometrus maculatus/ce:italic> [J] . Masahiro Miyashita, Atsushi Kitanaka, Mao Yakio, Toxicon: An International Journal Devoted to the Exchange of Knowledge on the Poisons Derived from Animals, Plants and Microorganisms . 2017,第期

机译：完整＆ ce：斜体> de novo＆ / ce：斜体>透蝎肽的序列测序蝎子的毒性肽＆ ce：斜体> isometrus maculatus＆ / ce：斜体>
6. Peptide-based protease inhibitors of the hepatitis C virus full-length NS3 protein (protease-helices/NTPase) [C] . Anja Johansson, Eva Akerblom, Gunnar Lindeberg, European Peptide Symposium . 2002

机译：基于肽的蛋白质蛋白酶抑制剂甲型肝炎病毒全长NS3蛋白（蛋白酶 - 螺旋/ NTPAse）
7. Development of HCV envelope-pseudotyped virus particles for evaluation of HCV entry inhibitors and cellular proteases involved in HCV envelope processing. [D] . Wei, Jiayi. 2013

机译：HCV包膜假型病毒颗粒的开发，用于评估HCV包膜加工中涉及的HCV进入抑制剂和细胞蛋白酶。
8. Inhibitors of signal peptide peptidase and subtilisin/kexin-isozyme 1 inhibit Ebola virus glycoprotein-driven cell entry by interfering with activity and cellular localization of endosomal cathepsins [O] . Teresa Plegge, Martin Spiegel, Nadine Krüger, 2012

机译：信号肽肽酶和枯草杆菌蛋白酶/ kexin同工酶1的抑制剂通过干扰内体组织蛋白酶的活性和细胞定位来抑制埃博拉病毒糖蛋白驱动的细胞进入
9. Mechanistic In Vivo and In Vitro Pulmonary Cellular Studies Demonstrating Biodegradability of Inhaled p -Aramid RFP [O] . 2002

机译：机械化<斜体>在体内和<斜体>在体外肺细胞研究证明了吸入的生物降解性<斜体> p -aramid RFP

De Novo Macrocyclic Peptide Inhibitors of Hepatitis B Virus Cellular Entry

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