Molecular handcraft of a well‐folded protein chimera

Author:

Toledo‐Patiño Saacnicteh12ORCID,Goetz Sara Kathrin1,Shanmugaratnam Sooruban13,Höcker Birte13ORCID,Farías‐Rico José Arcadio14ORCID

Affiliation:

1. Max Planck Institute for Developmental Biology Tübingen Germany

2. Okinawa Institute of Science and Technology Graduate University Japan

3. Department of Biochemistry University of Bayreuth Germany

4. Synthetic Biology Program, Center for Genome Sciences National Autonomous University of Mexico Cuernavaca Mexico

Abstract

Modular assembly is a compelling pathway to create new proteins, a concept supported by protein engineering and millennia of evolution. Natural evolution provided a repository of building blocks, known as domains, which trace back to even shorter segments that underwent numerous ‘copy‐paste’ processes culminating in the scaffolds we see today. Utilizing the subdomain‐database Fuzzle, we constructed a fold‐chimera by integrating a flavodoxin‐like fragment into a periplasmic binding protein. This chimera is well‐folded and a crystal structure reveals stable interfaces between the fragments. These findings demonstrate the adaptability of α/β‐proteins and offer a stepping stone for optimization. By emphasizing the practicality of fragment databases, our work pioneers new pathways in protein engineering. Ultimately, the results substantiate the conjecture that periplasmic binding proteins originated from a flavodoxin‐like ancestor.

Funder

Deutscher Akademischer Austauschdienst

Consejo Nacional de Ciencia y Tecnología

Volkswagen Foundation

Deutsche Forschungsgemeinschaft

European Research Council

Publisher

Wiley

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