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7MGA

Concanavalin A bound to a DNA glycoconjugate, Man-AAATTT

Summary for 7MGA
Entry DOI10.2210/pdb7mga/pdb
Related7MG1 7MG2 7MG3 7MG4 7MG5 7MG6 7MG7 7MG8 7MG9
DescriptorConcanavalin-A, DNA (5'-D(P*AP*AP*AP*TP*TP*T)-3'), MANGANESE (II) ION, ... (7 entities in total)
Functional Keywordslectin, dna complex, sugar binding protein, sugar binding protein-dna complex, sugar binding protein/dna
Biological sourceCanavalia ensiformis (Jack bean, Dolichos ensiformis)
More
Total number of polymer chains4
Total formula weight56010.30
Authors
Partridge, B.E.,Winegar, P.H.,Mirkin, C.A. (deposition date: 2021-04-12, release date: 2021-06-16, Last modification date: 2023-10-18)
Primary citationPartridge, B.E.,Winegar, P.H.,Han, Z.,Mirkin, C.A.
Redefining Protein Interfaces within Protein Single Crystals with DNA.
J.Am.Chem.Soc., 143:8925-8934, 2021
Cited by
PubMed Abstract: Proteins are exquisite nanoscale building blocks: molecularly pure, chemically addressable, and inherently selective for their evolved function. The organization of proteins into single crystals with high positional, orientational, and translational order results in materials where the location of every atom can be known. However, controlling the organization of proteins is challenging due to the myriad interactions that define protein interfaces within native single crystals. Recently, we discovered that introducing a single DNA-DNA interaction between protein surfaces leads to changes in the packing of proteins within single crystals and the protein-protein interactions (PPIs) that arise. However, modifying specific PPIs to effect deliberate changes to protein packing is an unmet challenge. In this work, we hypothesized that disrupting and replacing a highly conserved PPI with a DNA-DNA interaction would enable protein packing to be modulated by exploiting the programmability of the introduced oligonucleotides. Using concanavalin A (ConA) as a model protein, we circumvent potentially deleterious mutagenesis and exploit the selective binding of ConA toward mannose to noncovalently attach DNA to the protein surface. We show that DNA association eliminates the major PPI responsible for crystallization of native ConA, thereby allowing subtle changes to DNA design (length, complementarity, and attachment position) to program distinct changes to ConA packing, including the realization of three novel crystal structures and the deliberate expansion of ConA packing along a single crystallographic axis. These findings significantly enhance our understanding of how DNA can supersede native PPIs to program protein packing within ordered materials.
PubMed: 34096291
DOI: 10.1021/jacs.1c04191
PDB entries with the same primary citation
Experimental method
X-RAY DIFFRACTION (2 Å)
Structure validation

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