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De novo design of protein logic gates

机译:DE Novo设计蛋白质逻辑门

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摘要

The design of modular protein logic for regulating protein function at the posttranscriptional level is a challenge for synthetic biology. Here, we describe the design of two-input AND, OR, NAND, NOR, XNOR, and NOT gates built from de novo-designed proteins. These gates regulate the association of arbitrary protein units ranging from split enzymes to transcriptional machinery in vitro, in yeast and in primary human T cells, where they control the expression of the TIM3 gene related to T cell exhaustion. Designed binding interaction cooperativity, confirmed by native mass spectrometry, makes the gates largely insensitive to stoichiometric imbalances in the inputs, and the modularity of the approach enables ready extension to three-input OR, AND, and disjunctive normal form gates. The modularity and cooperativity of the control elements, coupled with the ability to de novo design an essentially unlimited number of protein components, should enable the design of sophisticated posttranslational control logic over a wide range of biological functions.
机译:模块化蛋白质逻辑用于调节蛋白质功能在后颅面水平的挑战是合成生物学的挑战。在这里,我们描述了两输入和,或,Nand,Nor,Xnor的设计,而不是从De Novo设计的蛋白质构建的盖茨。这些门调节任意蛋白质单位的关联范围从分裂酶到体外转录机械,在酵母和原代人T细胞中,在那里他们控制与T细胞耗尽相关的TIM3基因的表达。设计的结合相互作用合作率由天然质谱进行证实,使栅极大致不敏感在输入中的化学计量的不平衡,并且该方法的模块性使得能够延伸到三输入或和,并且和脱置正常形状栅极。控制元件的模块化和合作性,与Novo设计的能力相结合,基本上无限数量的蛋白质组分,应在广泛的生物学功能上实现复杂的后期控制逻辑。

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  • 来源
    《Science》 |2020年第6486期|78-84|共7页
  • 作者单位

    Univ Washington Dept Biochem Seattle WA 98195 USA|Univ Washington Inst Prot Design Seattle WA 98195 USA|CALTECH Div Biol & Biol Engn Pasadena CA 91125 USA;

    Univ Washington Dept Biochem Seattle WA 98195 USA|Univ Washington Inst Prot Design Seattle WA 98195 USA;

    Northwestern Univ Dept Chem & Biol Engn Evanston IL 60208 USA;

    Ohio State Univ Dept Chem & Biochem Columbus OH 43210 USA|Ohio State Univ Resource Native Mass Spectrometry Guided Struct B Columbus OH 43210 USA;

    Altius Inst Biomed Sci Seattle WA 98195 USA|Lyell Immunopharma Inc Seattle WA 98109 USA;

    Ohio State Univ Dept Chem & Biochem Columbus OH 43210 USA|Ohio State Univ Resource Native Mass Spectrometry Guided Struct B Columbus OH 43210 USA;

    Ohio State Univ Dept Chem & Biochem Columbus OH 43210 USA|Ohio State Univ Resource Native Mass Spectrometry Guided Struct B Columbus OH 43210 USA;

    Univ Washington Dept Biochem Seattle WA 98195 USA|Univ Washington Inst Prot Design Seattle WA 98195 USA;

    Univ Calif San Francisco Dept Biochem & Biophys San Francisco CA 94158 USA;

    Altius Inst Biomed Sci Seattle WA 98195 USA|Lyell Immunopharma Inc Seattle WA 98109 USA;

    Altius Inst Biomed Sci Seattle WA 98195 USA;

    Altius Inst Biomed Sci Seattle WA 98195 USA;

    Altius Inst Biomed Sci Seattle WA 98195 USA;

    Univ Calif San Francisco Dept Biochem & Biophys San Francisco CA 94158 USA|Chan Zuckerberg Biohub San Francisco CA 94158 USA;

    Altius Inst Biomed Sci Seattle WA 98195 USA|Univ Washington Dept Genome Sci Seattle WA 98195 USA|Univ Washington Dept Med Div Oncol Seattle WA 98109 USA;

    Ohio State Univ Resource Native Mass Spectrometry Guided Struct B Columbus OH 43210 USA;

    Northwestern Univ Dept Chem & Biol Engn Evanston IL 60208 USA|Ohio State Univ Dept Chem & Biochem Columbus OH 43210 USA|Northwestern Univ Chem Life Proc Inst Evanston IL 60208 USA|Northwestern Univ Ctr Synthet Biol Evanston IL 60208 USA;

    Univ Washington Dept Biochem Seattle WA 98195 USA|Univ Washington Inst Prot Design Seattle WA 98195 USA|Lyell Immunopharma Inc Seattle WA 98109 USA;

    Univ Washington Dept Biochem Seattle WA 98195 USA|Univ Washington Inst Prot Design Seattle WA 98195 USA|Univ Washington Howard Hughes Med Inst Seattle WA 98195 USA;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
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  • 正文语种 eng
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