Literature DB >> 30504143

Simple yet functional phosphate-loop proteins.

Maria Luisa Romero Romero1, Fan Yang2,3, Yu-Ru Lin4, Agnes Toth-Petroczy1,5, Igor N Berezovsky6,7, Alexander Goncearenco8,9, Wen Yang2, Alon Wellner1, Fanindra Kumar-Deshmukh1, Michal Sharon1, David Baker4, Gabriele Varani2, Dan S Tawfik10.   

Abstract

Abundant and essential motifs, such as phosphate-binding loops (P-loops), are presumed to be the seeds of modern enzymes. The Walker-A P-loop is absolutely essential in modern NTPase enzymes, in mediating binding, and transfer of the terminal phosphate groups of NTPs. However, NTPase function depends on many additional active-site residues placed throughout the protein's scaffold. Can motifs such as P-loops confer function in a simpler context? We applied a phylogenetic analysis that yielded a sequence logo of the putative ancestral Walker-A P-loop element: a β-strand connected to an α-helix via the P-loop. Computational design incorporated this element into de novo designed β-α repeat proteins with relatively few sequence modifications. We obtained soluble, stable proteins that unlike modern P-loop NTPases bound ATP in a magnesium-independent manner. Foremost, these simple P-loop proteins avidly bound polynucleotides, RNA, and single-strand DNA, and mutations in the P-loop's key residues abolished binding. Binding appears to be facilitated by the structural plasticity of these proteins, including quaternary structure polymorphism that promotes a combined action of multiple P-loops. Accordingly, oligomerization enabled a 55-aa protein carrying a single P-loop to confer avid polynucleotide binding. Overall, our results show that the P-loop Walker-A motif can be implemented in small and simple β-α repeat proteins, primarily as a polynucleotide binding motif.

Entities:  

Keywords:  RNA binding protein; Walker-A; conformational diversity; de novo protein design; protein evolution

Mesh:

Substances:

Year:  2018        PMID: 30504143      PMCID: PMC6304952          DOI: 10.1073/pnas.1812400115

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


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