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Hydration-coupled allosteric locking of a phenol- and zinc-free bioactive insulin analog

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Matsuura, Hiroaki
Kawano, Yoshiaki
Abhari, Zain
Kepceoglu, Abdullah
Tosha, Takehiko

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Modern insulin still depends on phenol and zinc to keep the hormone stable in vials and pumps, yet both additives slow absorption and raise safety concerns. We therefore asked a simple, clinically driven question: Can we stabilize the fast-acting T-state of insulin without phenol/zinc by exploiting pH-dependent water and anion binding? Using high-resolution synchrotron crystallography (1.4-1.76 angstrom), we solved novel designer and acid-stable cubic insulin structures from pH 2 to 6 in citrate-sulfate buffers and mapped solvent/anion contacts onto computational analyses. Across the acidic range, we uncovered a conserved 'water-anion clamp' centered on the Phe1B-Asn3B pocket that locks insulin in its bioactive T-conformation while neutralizing the protein's positive charge. This clamp: (i) removes the need for phenolic ligands, and (ii) keeps monomers soluble at high concentration. The structural blueprint we provide can guide formulation of phenol- and zinc-free, ultra-rapid insulin for subcutaneous pumps and high-strength cartridges, addressing unmet needs in intensive diabetes management. By clarifying how simple buffer anions and structured water can replace traditional preservatives, our work may link atomic-level detail to a practical therapeutic goal: faster, safer insulin delivery.

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Wiley

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Biochemistry & Molecular Biology

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FEBS Journal

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10.1111/febs.70283

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CC BY-NC-ND (Attribution-NonCommercial-NoDerivs)

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Except where otherwised noted, this item's license is described as CC BY-NC-ND (Attribution-NonCommercial-NoDerivs)

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