1g7b Citations

Phase changes in T(3)R(3)(f) human insulin: temperature or pressure induced?

Smith GD, Pangborn WA, Blessing RH
Acta Crystallogr D Biol Crystallogr 57 1091-100 (2001)
Cited: 14 times
EuropePMC logo PMID: 11468392

Abstract

The structure of T(3)R(3) hexameric human insulin has been determined at 100 K from two different crystals at 1.2 and 1.3 A resolution and refined to residuals of 0.169 and 0.176, respectively. Owing to a phase change, the c axis is double its room-temperature value and the asymmetric unit contains two independent TR(f) insulin dimers. Compared with the orientation in the room-temperature structure, one dimer undergoes a rotation about the c axis of -5 degrees, while the second is rotated +4 degrees. A superposition of the backbone atoms of the two independent dimers shows that the C(alpha) atoms of five residues within the R(f)-state monomers are displaced by more than 1.0 A; smaller displacements are observed for the T-state monomers. Four zinc ions lie on the crystallographic threefold axis and each forms bonds to three symmetry-related HisB10 N(varepsilon2) atoms from the T- and R(f)-state trimers. While three of the zinc ions are tetrahedrally coordinated with a chloride ion completing the coordination sphere, mixed tetrahedral/octahedral coordination is observed for one of the T-state zinc ions. The three symmetry-related "phenolic binding sites" in one hexamer contain water molecules and a glycerol molecule, but the same sites in the second hexamer are occupied by a zinc ion coordinated to an alternate conformation of HisB10, a symmetry-related HisB5 and two chloride ions. Two additional and partially occupied zinc ion sites are observed at the interface between the two independent dimers. One zinc ion is coordinated by a T-state HisB5 of one dimer, an R-state HisB5 of the second dimer and two water molecules; the second zinc ion is coordinated by an alternate side-chain conformation of the T-state HisB5 and three water molecules. The carboxyl group of one GluB13 side chain, which exists in two discrete conformations, appears to be protonated, because short contacts exist to a second carboxyl group or to a carbonyl O atom.

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  1. Hypervalent nonbonded interactions of a divalent sulfur atom. Implications in protein architecture and the functions. Iwaoka M, Isozumi N. Molecules 17 7266-7283 (2012)

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  1. Generation of Marker- and/or Backbone-Free Transgenic Wheat Plants via Agrobacterium-Mediated Transformation. Wang GP, Yu XD, Sun YW, Jones HD, Xia LQ. Front Plant Sci 7 1324 (2016)
  2. Insulin in motion: The A6-A11 disulfide bond allosterically modulates structural transitions required for insulin activity. van Lierop B, Ong SC, Belgi A, Delaine C, Andrikopoulos S, Haworth NL, Menting JG, Lawrence MC, Robinson AJ, Forbes BE. Sci Rep 7 17239 (2017)
  3. Predicting binding sites from unbound versus bound protein structures. Clark JJ, Orban ZJ, Carlson HA. Sci Rep 10 15856 (2020)


Reviews citing this publication (1)

  1. In Quest for Improved Drugs against Diabetes: The Added Value of X-ray Powder Diffraction Methods. Karavassili F, Valmas A, Fili S, Georgiou CD, Margiolaki I. Biomolecules 7 E63 (2017)

Articles citing this publication (9)

  1. Structure determination from powder diffraction data. David WI, Shankland K. Acta Crystallogr A 64 52-64 (2008)
  2. Computational and structural evidence for neurotransmitter-mediated modulation of the oligomeric states of human insulin in storage granules. Palivec V, Viola CM, Kozak M, Ganderton TR, Křížková K, Turkenburg JP, Haluŝková P, Žáková L, Jiráĉek J, Jungwirth P, Brzozowski AM. J Biol Chem 292 8342-8355 (2017)
  3. Insulin fibrillation: The influence and coordination of Zn2. Frankær CG, Sønderby P, Bang MB, Mateiu RV, Groenning M, Bukrinski J, Harris P. J Struct Biol 199 27-38 (2017)
  4. Powder crystallography on macromolecules. Margiolaki I, Wright JP. Acta Crystallogr A 64 169-180 (2008)
  5. Crystallography of hydrogen-containing compounds: realizing the potential of neutron powder diffraction. Weller MT, Henry PF, Ting VP, Wilson CC. Chem Commun (Camb) 2973-2989 (2009)
  6. Effect of divalent ions on the minimal relaxase domain of MobA. Xia S, Robertus JD. Arch Biochem Biophys 488 42-47 (2009)
  7. Fine grained sampling of residue characteristics using molecular dynamics simulation. Joo H, Qu X, Swanson R, McCallum CM, Tsai J. Comput Biol Chem 34 172-183 (2010)
  8. Nucleation of glucose isomerase protein crystals in a nonclassical disguise: The role of crystalline precursors. Van Driessche AES, Ling WL, Schoehn G, Sleutel M. Proc Natl Acad Sci U S A 119 e2108674119 (2022)
  9. Performance of phased rotation, conformation and translation function: accurate protein model building with tripeptidic and tetrapeptidic fragments. Pavelcík F, Václavík J. Acta Crystallogr D Biol Crystallogr 66 1012-1023 (2010)


Related citations provided by authors (5)

  1. X-ray Crystallographic Studies on Hexameric Insulins in the Presence of Helix-Stabilizing Agents, Thiocyanate, Methylparaben, and Phenol. Whittingham JL, Chaudhuri S, Dodson EJ, Moody PCE, Dodson GG Biochemistry 34 15553-15563 (1995)
  2. Crystallographic Evidence for Dual Coordination around Zinc in the T3R3 Human Insulin Hexamer. Ciszak E, Smith GD Biochemistry 33 1512-1517 (1994)
  3. Structural stability in the 4-zinc human insulin hexamer. Smith GD, Swenson DC, Dodson EJ, Dodson GG, Reynolds CD Proc. Natl. Acad. Sci. U.S.A. 81 7093-7097 (1984)
  4. Structure of 4-zinc insulin. Bentley G, Dodson E, Dodson GG, Hodgkin D, Mercola D Nature 261 166-168 (1976)
  5. The First Protein Crystal Structure Determined from High Resolution X-Ray Powder Diffraction Data: A Variant of T3R3 Human Insulin Zinc Complex Produced by Grinding. Von Dreele RB, Stephens PW, Smith GD, Blessing RH Acta Crystallogr. D Biol. Crystallogr. 56 1549- (2000)

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