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STRUCTURAL
BIOLOGY

ISSN: 2059-7983

June 2023 issue

Cover illustration: The Collaborative Computational Project No. 4 (CCP4) suite is a collection of macromolecular crystallography software brought together by familiar execution routines, a set of common libraries, and graphical interfaces. A new article by Agirre et al. [(2023), Acta Cryst. D79, 449–461], which is intended as a general literature citation for the use of the CCP4 software suite in structure determination, gives the reader a general overview of the programs in the suite.

scientific commentaries

Unravelling the secrets of multi-domain lytic polysaccharide monooxygenases (LPMOs)

G. Vaaje-Kolstad and V. G. H. Eijsink

A new chitin-active AA10 lytic polysaccharide monooxygenase from the marine bacterium Vibrio campbellii is described in the paper by Zhou et al. [(2023), Acta Cryst. D79, 479–497].

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Continuous development in macromolecular crystallography with CCP4

M. Martinez-Ripoll and A. Albert

The evolution of the Collaborative Computational Project No. 4 (CCP4) has been described in a new article by Agirre et al. [(2023). Acta Cryst. D79, 449–461] that should provide the definitive reference for the CCP4 suite of programs.

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CCP4

The CCP4 suite: integrative software for macromolecular crystallography

J. Agirre, M. Atanasova, H. Bagdonas, C. B. Ballard, A. Baslé, J. Beilsten-Edmands, R. J. Borges, D. G. Brown, J. J. Burgos-Mármol, J. M. Berrisford, P. S. Bond, I. Caballero, L. Catapano, G. Chojnowski, A. G. Cook, K. D. Cowtan, T. I. Croll, J. É. Debreczeni, N. E. Devenish, E. J. Dodson, T. R. Drevon, P. Emsley, G. Evans, P. R. Evans, M. Fando, J. Foadi, L. Fuentes-Montero, E. F. Garman, M. Gerstel, R. J. Gildea, K. Hatti, M. L. Hekkelman, P. Heuser, S. W. Hoh, M. A. Hough, H. T. Jenkins, E. Jiménez, R. P. Joosten, R. M. Keegan, N. Keep, E. B. Krissinel, P. Kolenko, O. Kovalevskiy, V. S. Lamzin, D. M. Lawson, A. A. Lebedev, A. G. W. Leslie, B. Lohkamp, F. Long, M. Malý, A. J. McCoy, S. J. McNicholas, A. Medina, C. Millán, J. W. Murray, G. N. Murshudov, R. A. Nicholls, M. E. M. Noble, R. Oeffner, N. S. Pannu, J. M. Parkhurst, N. Pearce, J. Pereira, A. Perrakis, H. R. Powell, R. J. Read, D. J. Rigden, W. Rochira, M. Sammito, F. Sánchez Rodríguez, G. M. Sheldrick, K. L. Shelley, F. Simkovic, A. J. Simpkin, P. Skubak, E. Sobolev, R. A. Steiner, K. Stevenson, I. Tews, J. M. H. Thomas, A. Thorn, J. T. Valls, V. Uski, I. Usón, A. Vagin, S. Velankar, M. Vollmar, H. Walden, D. Waterman, K. S. Wilson, M. D. Winn, G. Winter, M. Wojdyr and K. Yamashita

This article describes the Collaborative Computational Project No. 4 (CCP4). It is intended as a general literature citation for the use of the CCP4 software suite in structure determination.

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Analysis and validation of overall N-glycan conformation in Privateer

J. S. Dialpuri, H. Bagdonas, M. Atanasova, L. C. Schofield, M. L. Hekkelman, R. P. Joosten and J. Agirre

The Privateer software allows structural biologists to evaluate and improve the atomic structures of carbohydrates, including N-glycans. This software has recently been extended to check glycan composition through the use of glycomics data, and the broadening of its scope is presented in this article.

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CCP-EM

Near-atomic resolution reconstructions from in situ revitrified cryo samples

G. Bongiovanni, O. F. Harder, J. M. Voss, M. Drabbels and U. J. Lorenz

Near-atomic resolution reconstructions can be obtained from in situ melted and revitrified cryo samples. Revitrification results in a more homogeneous angular distribution.

EMDB references: apoferritin, conventional sample, EMD-15715; revitrified sample, EMD-15721

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research papers

Structural and binding studies of a new chitin-active AA10 lytic polysaccharide monooxygenase from the marine bacterium Vibrio campbellii

Y. Zhou, S. Wannapaiboon, M. Prongjit, S. Pornsuwan, J. Sucharitakul, N. Kamonsutthipaijit, R. C. Robinson and W. Suginta

Chitin-active lytic polysaccharide monooxygenase (AA10 LPMO) is one of the key enzymes involved in the recycling of chitin biomass. A new marine chitin-active AA10 LPMO from V. campbellii could serve as a powerful biocatalyst in the bioconversion of chitin for future bioenergy production.

PDB references: VhLPMO10A, with copper(II), 8gul; apo VhLPMO10A, 8gum

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Structure of reverse gyrase with a minimal latch that supports ATP-dependent positive supercoiling without specific interactions with the topoisomerase domain

V. P. Mhaindarkar, R. Rasche, D. Kümmel, M. G. Rudolph and D. Klostermeier

The latch domain in reverse gyrases mediates the cooperation of the helicase and topoisomerase domains. In Thermotoga maritima reverse gyrase this latch can be designed into a minimal β-bulge loop that has natural precedence in Thermosipho africanus reverse gyrase. The properties and functionalities of different latch domains across reverse gyrases are discussed.

PDB references: reverse gyrase with a minimal latch, 7fse; Y851F mutant, 7fsf

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The type III secretion chaperone SctY may shield the hydrophobic export gate-binding C-terminus of its substrate SctX

D. Gilzer, J. L. Kowal, F. Flottmann and H. H. Niemann

SctX proteins are secreted substrates and are essential components of type III secretion systems. The dedicated chaperone SctY escorts SctX proteins to the secretion machinery, where the hydrophobic helix at the C-terminus of SctX mediates recognition by the export apparatus. New crystal structures suggest that in the absence of the export gate this hydrophobic helix kinks and folds back onto the chaperone, presumably to shield it from the solvent.

PDB references: AscX₃₁–YscY, 8ara; AscX₄₉–YscY, 8arb; AscX₄₉–LscY^meth, 8arc

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Cysteine synthase: multiple structures of a key enzyme in cysteine synthesis and a potential drug target for Chagas disease and leishmaniasis

K. Sowerby, S. Freitag-Pohl, A. M. Murillo, A. M. Silber and E. Pohl

Biochemical and structural analyses of cysteine synthase, the key enzyme in cysteine biosynthesis, from the protozoan pathogens Trypanosoma cruzi, T. theileri and Leishmania infantum are presented. This enzyme is a potential drug target for neglected tropical diseases such as Chagas disease and leishmaniasis.

PDB references: cysteine synthase from Leishmania infantum, 8b9m; from Trypanosoma theileri, 8b9w; from Trypanosoma cruzi, 8b9y

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Structure-based discovery of an antipsychotic drug, paliperidone, as a modulator of human superoxide dismutase 1: a potential therapeutic target in amyotrophic lateral sclerosis

S. Aouti, S. Padavattan and B. Padmanabhan

Superoxide dismutase 1 (SOD1) is a therapeutic drug target against amyotrophic lateral sclerosis. In silico and in vitro studies indicate binding of paliperidone at Trp32 of SOD1, an important site for oxidative stress-induced aggregation. Significant interactions with SOD1 and low-micromolar binding affinity make paliperidone a potential lead for the development of drug candidates that can prevent SOD1 fibrillation.

PDB reference: human superoxide dismutase, complex with paliperidone, 8gsq

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Structural and functional investigation of a fungal member of carbohydrate esterase family 15 with potential specificity for rare xylans

S. Mazurkewich, K. C. Scholzen, R. H. Brusch, J.-C.N. Poulsen, Y. Theibich, S. Hüttner, L. Olsson, J. Larsbrink and L. Lo Leggio

Structural investigation of a presumed fungal glucuronoyl esterase reveals a classical serine hydrolase active site but an unusual ligand-binding site. Functional analysis showed a lack of activity on a wide array of substrates commonly utilized by this family of enzymes. It is hypothesized that this enzyme needs complex plant cell-wall substructures for activity.

PDB reference: LfCE15C, 8b48

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June 2023 issue

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