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Determination of extended substrate specificity of the MALT1 as a strategy for the design of potent substrates and activity-based probes

机译：确定MALT1的扩展底物特异性作为设计有效底物和基于活性的探针的策略

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摘要

Mucosa-associated lymphoid tissue lymphoma translocation protein 1 (MALT1) belongs to the CD clan of cysteine proteases. MALT1 is a unique enzyme among this clan because it recognizes the basic amino acid arginine in the P1 pocket. Previous studies carried out with natural amino acids revealed the substrate specificity of the P4-P1 pockets of MALT1 but have provided only limited information about the catalytic preferences of this enzyme. In this study, we exploited Hybrid Combinatorial Substrate Library and Internally Quenched Fluorescence substrate technologies to interrogate the extended substrate specificity profile of the S5-S2’ active site pockets using unnatural amino acids. This strategy resulted in the design of a peptide-based fluorogenic substrate, which exhibited significant activity toward MALT1. Subsequently, the substrate sequence was further utilized to develop potent, irreversible activity-based probes.

机译：粘膜相关淋巴组织淋巴瘤易位蛋白1（MALT1）属于半胱氨酸蛋白酶的CD家族。 MALT1是该家族中的独特酶，因为它可以识别P1口袋中的碱性氨基酸精氨酸。以前用天然氨基酸进行的研究揭示了MALT1的P4-P1口袋的底物特异性，但仅提供了有关该酶催化偏好的有限信息。在这项研究中，我们利用杂交组合底物文库和内部淬灭荧光底物技术，使用非天然氨基酸询问S5-S2活性位点口袋的扩展底物特异性谱。该策略导致了基于肽的荧光底物的设计，其对MALT1表现出显着的活性。随后，进一步利用底物序列来开发有效的，不可逆的基于活性的探针。

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期刊名称 Scientific Reports
作者
Paulina Kasperkiewicz; Sonia Kołt; Tomasz Janiszewski; Katarzyna Groborz; Marcin Poręba; Scott J. Snipas; Guy S. Salvesen; Marcin Drąg;
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年(卷),期 -1(8),-1
年度 -1
页码 15998
总页数 10
原文格式 PDF
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1. Determination of extended substrate specificity of the MALT1 as a strategy for the design of potent substrates and activity-based probes [J] . Paulina Kasperkiewicz, Sonia Ko?t, Tomasz Janiszewski, Scientific reports. . 2018,第1期

机译：MALT1的延长底物特异性的测定作为效力底物和基于活性的探针设计的策略
2. Extended substrate specificity and first potent irreversible inhibitor/activity-based probe design for Zika virus NS2B-NS3 protease [J] . Rut Wioletta, Zhang Linlin, Kasperkiewicz Paulina, Antiviral Research . 2017,第期

机译：用于Zika病毒NS2B-NS3蛋白酶的扩展底物特异性和基于效率的不可逆抑制剂/活性的探针设计
3. Neutrophil Elastase Activity Imaging: Recent Approaches in the Design and Applications of Activity-Based Probes and Substrate-Based Probes [J] . Natacha Jugniot, Pierre Voisin, Abderrazzak Bentaher, Contrast media & molecular imaging . 2019,第1期

机译：中性粒细胞弹性蛋白酶活性成像：最近的基于活性的探头和基于基础探针的设计和应用方法
4. PROBING THE SUBSTRATE SPECIFICITY OF ENDO-α-MANNOSIDASE WITH EPIMERIC α-MAN-1,3-α-MAN/α-GLC-1,3-α-MAN CONFIGURED SUBSTRATES AND INHIBITORS [C] . Zalihe Hakki, Andrew J. Thompson, Terry Butters International Carbohydrate Symposium . 2013

机译：探讨胎族α-甘露糖苷酶的底物特异性α-MAN-1,3-α-MAN /α-GLC-1,3-α-MAN配置的基材和抑制剂
5. Methodologies for Characterizing the Extended Substrate Specificity of Proteolytic Enzymes [D] . Jabaiah, Abeer Mohamad. 2010

机译：表征蛋白水解酶扩展底物特异性的方法
6. Neutrophil Elastase Activity Imaging: Recent Approaches in the Design and Applications of Activity-Based Probes and Substrate-Based Probes [O] . Natacha Jugniot, Pierre Voisin, Abderrazzak Bentaher, 2019

机译：中性粒细胞弹性蛋白酶活性成像：基于活动的探针和基于底物的探针的设计和应用中的最新方法
7. Determination of extended substrate specificity of the MALT1 as a strategy for the design of potent substrates and activity-based probes [O] . Paulina Kasperkiewicz, Sonia Kołt, Tomasz Janiszewski, 2018

机译：MALT1的延长底物特异性的测定作为效力底物和基于活性的探针设计的策略

Determination of extended substrate specificity of the MALT1 as a strategy for the design of potent substrates and activity-based probes

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