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. 2019 Jun 4;27(6):1029-1033.e3.
doi: 10.1016/j.str.2019.03.015. Epub 2019 Apr 18.

MORC3 Is a Target of the Influenza A Viral Protein NS1

Yi Zhang  1 JaeWoo Ahn  1 Kelsie J Green  2 Kendra R Vann  1 Joshua Black  1 Christopher B Brooke  3 Tatiana G Kutateladze  4
Affiliations

MORC3 Is a Target of the Influenza A Viral Protein NS1

Yi Zhang et al. Structure. .

Abstract

Microrchidia 3 (MORC3), a human ATPase linked to several autoimmune disorders, has been characterized both as a negative and positive regulator of influenza A virus. Here, we report that the CW domain of MORC3 (MORC3-CW) is targeted by the C-terminal tail of the influenza H3N2 protein NS1. The crystal structure of the MORC3-CW:NS1 complex shows that NS1 occupies the same binding site in CW that is normally occupied by histone H3, a physiological ligand of MORC3-CW. Comparable binding affinities of MORC3-CW to H3 and NS1 peptides and to the adjacent catalytic ATPase domain suggest that the viral protein can compete with the host histone for the association with CW, releasing MORC3 autoinhibition and activating the catalytic function of MORC3. Our structural, biochemical, and cellular analyses suggest that MORC3 might affect the infectivity of influenza virus and therefore has a role in cell immune response.

Keywords: ATPase; CW; MORC3; NS1; chromatin; histone; immune; reader; structure; virus.

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Conflict of interest statement

DECLARATION OF INTERESTS

The authors declare no competing interests.

Figures

Figure 1.
Figure 1.. MORC3-CW Is a Target of NS1
(A) The amino-terminal sequence of H3 (trimethylated at lysine 4) and the C-terminal sequence of NS1 (trimethylated at lysine 229) are shown. (B) Superimposed 1H,15N HSQC spectra of 15N-labeled MORC3-CW collected upon titration with the methylated and unmodified NS1 peptides. Spectra are color coded according to the protein-to-peptide molar ratio. (C) The crystal structure of the MORC3-CW:NS1 complex. The CW domain is shown in a ribbon diagram (green), and NS1 is shown as sticks (yellow). The zinc (gray) atom is shown as a sphere. (D) Electrostatic surface potential of the MORC3-CW domain colored blue and red for positive and negative charges, respectively. The bound NS1 peptide is yellow. See also Figure S1.
Figure 2.
Figure 2.. Mechanistic Insight into H3 Mimicry by NS1
(A) Binding affinities of WT and mutated MORC3-CW to indicated peptides as measured by tryptophan fluorescence or NMR (*). The binding affinity of the CW domain to H3K4me3 peptide was determined previously (a) (Andrews et al., 2016). The experiments were carried out in triplicate (in duplicate for the CW E431A-H3K4me3 interaction). Error bars denote SD. (B) Representative binding curves used to determine the Kd values by tryptophan fluorescence in (A). (C) Superimposed 1H,15N HSQC spectra of the 15N-labeled MORC3-CW mutants collected upon titration with the NS1K229me3 peptide. Spectra are color coded according to the protein-to-peptide molar ratio. (D) Zoom-in views of the NS1 K229- and T225-binding sites of MORC3-CW. See also Figure S2.
Figure 3.
Figure 3.. Structural Similarity of the MORC3-CW Complexes
(A) Structural overlay of the MORC3-CW in complex with NS1 peptide (yellow) and H3K4me3 peptide (pink) (PDB: 5SVX). (B) The fold change in H3N2 influenza virus infectivity in a single round of infection in mCherry-MORC3-positive cells compared with mCherry-negative cells from the same sample. Infectivity measured as a percentage of cells positive of expression of the viral NP protein. The results presented are representative of two independent experiments. The experiments were carried out in triplicate (in duplicate for the D67A mutant). Data are represented as means ± SEM. The statistical significance was determined using the unpaired t test, *p < 0.05. See also Figures S3 and S4.
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References

    1. Adams PD, Afonine PV, Bunkoczi G, Chen VB, Davis IW, Echols N, Headd JJ, Hung LW, Kapral GJ, Grosse-Kunstleve RW, et al. (2010). PHENIX: a comprehensive Python-based system for macromolecular structure solution. Acta Crystallogr. D Biol. Crystallogr 66, 213–221. - PMC - PubMed
    1. Andrews FH, Tong Q, Sullivan KD, Cornett EM, Zhang Y, Ali M, Ahn J, Pandey A, Guo AH, Strahl BD, et al. (2016). Multivalent chromatin engagement and inter-domain crosstalk regulate MORC3 ATPase. Cell Rep. 16, 3195–3207. - PMC - PubMed
    1. Ali M, Yan K, Lalonde ME, Degerny C, Rothbart SB, Strahl BD, Côté J, Yang XJ, and Kutateladze TG (2012). Tandem PHD fingers of MORF/ MOZ acetyltransferases display selectivity for acetylated histone H3 and are required for the association with chromatin. J. Mol. Biol 424, 328–338. - PMC - PubMed
    1. Bortz E, Westera L, Maamary J, Steel J, Albrecht RA, Manicassamy B, Chase G, Martinez-Sobrido L, Schwemmle M, and Garcia-Sastre A (2011). Host- and strain-specific regulation of influenza virus polymerase activity by interacting cellular proteins. mBio 2, 10.1128/mBio.00151-11. - DOI - PMC - PubMed
    1. Chen VB, Arendall WB 3rd, Headd JJ, Keedy DA, Immormino RM, Kapral GJ, Murray LW, Richardson JS, and Richardson DC (2010). MolProbity: all-atom structure validation for macromolecular crystallography. Acta Crystallogr. D Biol. Crystallogr 66, 12–21. - PMC - PubMed

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