<scp>M</scp>olecular aspects of the interaction between <scp>M</scp>ason—<scp>P</scp>fizer monkey virus matrix protein and artificial phospholipid membrane

Junková, Petra; Prchal, Jan; Spiwok, Vojtěch; Pleskot, Roman; Kadlec, Jan; Krásný, Lukáš; Hynek, Radovan; Hrabal, Richard; Ruml, Tomáš

doi:10.1002/prot.25156

Cited by 3 publications

(6 citation statements)

References 56 publications

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“…The lower affinity of the M-PMV MA, a D-type retrovirus, to liposomes has previously been observed by Kroupa et al (41), where only 5% of the M-PMV MA was bound to PI4,5P 2 -containing liposomes in contrast to more than 40% of the HIV-1 MA bound to the same liposomes. In our previous study, we found that ;50% of the M-PMV MA was bound to PI4,5P 2 -containing liposomes (39). However, the concentration of the phospholipids used in the mixture of M-PMV MA and liposomes was almost five times higher than that used by Kroupa et al (41) and twice as high as in our current study to obtain a sufficient amount of protein bound to the liposomes for subsequent mapping experiments.…”

Section: Liposome Binding Of Hiv-1 and Mmtv Mascontrasting

confidence: 58%

“…Additionally, the comparison of HIV-1 and MMTV MA LBA results shows that the HIV-1 MA HBR is able to mediate stronger electrostatic interactions than the HBR of the MMTV MA because HIV-1 exhibits a higher affinity to the liposomes than the MMTV MA under the same experimental conditions. Moreover, the higher affinity of the HIV-1 MA to PI4,5P 2 -containing liposomes as compared with another B/D-type retrovirus, M-PMV, has been observed previously (39,41), although its HBR is located at the N terminus of the MA and comprises eight basic residues. Therefore, we suppose that the affinity of different MAs to PI4,5P 2 is related to the morphogenesis of particular retroviruses.…”

Section: Plasma Membrane Recruitment Of Morphogenetically Different Retrovirusesmentioning

confidence: 66%

“…This can significantly affect their tendency of myristoyl release. In our previous study, we used multiscale MD simulations to describe the MA-membrane interaction of M-PMV, which is morphogenetically similar to MMTV, and the release of myristoyl was not observed during the simulations, although the M-PMV MA stably interacted with the membrane by its HBR bound to PI4,5P 2 molecules (39). Additionally, the exposure of myristoyl was not observed in the case of HIV-2 MA under any of the conditions ensuring the exposure of the myristoyl of the HIV-1 MA (37).…”

Section: Plasma Membrane Recruitment Of Morphogenetically Different Retrovirusesmentioning

confidence: 99%

“…Although the release of virus-like HIV-2 particles is PI4,5P 2 -dependent as in HIV-1, the trimerization of the HIV-2 MA and its interaction with PI4,5P 2 does not trigger the myristoyl exposure (37). Similarly, the myristoyl exposure was not observed in the case of the M-PMV MA when it interacted with truncated PI4,5P 2 (38) or during the CG-MD simulations of the M-PMV MA interaction with the lipid bilayer (39). Nevertheless, the tendency of the nonmyristoylated M-PMV MA to form trimers in contrast to its myristoylated form suggests that the exposure of myristoyl does occur and that it induces a conformational change of M-PMV MA, which favors trimerization (40).…”

mentioning

confidence: 92%

“…We have used a combination of the MS-based protein surface mapping method and CG-MD simulations. This approach has already been utilized to describe M-PMV MA-membrane interaction (39). Additionally, we have applied surface mapping to broaden our knowledge of the HIV-1 MA interaction with the membrane.…”

mentioning

confidence: 99%

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Differences and commonalities in plasma membrane recruitment of the two morphogenetically distinct retroviruses HIV-1 and MMTV

Junková

Pleskot

Prchal

et al. 2020

Journal of Biological Chemistry

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Retroviral Gag polyproteins are targeted to the inner leaflet of the plasma membrane through their N-terminal matrix (MA) domain. Because retroviruses of different morphogenetic types assemble their immature particles in distinct regions of the host cell, the mechanism of MA-mediated plasma membrane targeting differs among distinct retroviral morphogenetic types. Here, we focused on possible mechanistic differences of the MA-mediated plasma membrane targeting of the B-type mouse mammary tumor virus (MMTV) and C-type HIV-1, which assemble in the cytoplasm and at the plasma membrane, respectively. Molecular dynamics simulations, together with surface mapping, indicated that, similarly to HIV-1, MMTV uses a myristic switch to anchor the MA to the membrane and electrostatically interacts with phosphatidylinositol 4,5-bisphosphate to stabilize MA orientation. We observed that the affinity of MMTV MA to the membrane is lower than that of HIV-1 MA, possibly related to their different topologies and the number of basic residues in the highly basic MA region. The latter probably reflects the requirement of C-type retroviruses for tighter membrane binding, essential for assembly, unlike for D/B-type retroviruses, which assemble in the cytoplasm. A comparison of the membrane topology of the HIV-1 MA, using the surface-mapping method and molecular dynamics simulations, revealed that the residues at the HIV-1 MA C terminus help stabilize protein–protein interactions within the HIV-1 MA lattice at the plasma membrane. In summary, HIV-1 and MMTV share common features such as membrane binding of the MA via hydrophobic interactions and exhibit several differences, including lower membrane affinity of MMTV MA.

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Section: Liposome Binding Of Hiv-1 and Mmtv Mascontrasting

confidence: 58%

Section: Plasma Membrane Recruitment Of Morphogenetically Different Retrovirusesmentioning

confidence: 66%

Section: Plasma Membrane Recruitment Of Morphogenetically Different Retrovirusesmentioning

confidence: 99%

mentioning

confidence: 92%

mentioning

confidence: 99%

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Differences and commonalities in plasma membrane recruitment of the two morphogenetically distinct retroviruses HIV-1 and MMTV

Junková

Pleskot

Prchal

et al. 2020

Journal of Biological Chemistry

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Membrane Interactions of the Mason-Pfizer Monkey Virus Matrix Protein and Its Budding Deficient Mutants

Kroupa

Langerová

Doležal

et al. 2016

Journal of Molecular Biology

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Interaction Interface of Mason-Pfizer Monkey Virus Matrix and Envelope Proteins

Prchal

Sýs

Junková

et al. 2020

J Virol

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Retroviral envelope glycoprotein (Env) is essential for the specific recognition of the host cell and the initial phase of infection. As reported for HIV, the recruitment of Env into a retroviral membrane envelope is mediated through its interaction with a Gag polyprotein precursor of structural proteins. This interaction, occurring between the matrix domain (MA) of Gag and the cytoplasmic tail (CT) of the transmembrane domain of Env, takes place at the host cell plasma membrane. To determine whether the MA of Mason-Pfizer monkey virus (M-PMV) also interacts directly with the CT of Env, we mimicked the in vivo conditions in an in vitro experiment by using a CT in its physiological trimeric conformation mediated by the trimerization motif of the GCN4 yeast transcription factor. The MA protein was used in the concentration shifting the equilibrium to its trimeric form. The direct interaction between MA and CT was confirmed by a pull-down assay. Through the combination of NMR spectroscopy and protein cross-linking followed by mass spectrometry analysis, the residues involved in mutual interactions were determined. NMR has shown that the C-terminus of the CT is bound to the C-terminal part of MA. In addition, protein cross-linking confirmed the close proximity of the N-terminal part of CT and the N-terminus of MA, which is enabled in vivo by their location at the membrane. These results are in agreement with the previously determined orientation of MA on the membrane and support the already observed mechanisms of M-PMV virus-like particle transport and budding. IMPORTANCE By a combination of NMR and mass spectroscopy of cross-linked peptides, we show that in contrast to HIV-1, the C-terminal residues of the unstructured cytoplasmic tail of M-PMV Env interact with MA. Based on biochemical data and molecular modeling, we propose that individual CT monomers of a trimeric complex bind MA molecules belonging to different neighboring trimers, which may stabilize the MA orientation at the membrane by the formation of a membrane-bound net of interlinked Gag and CT trimers. This also corresponds with the concept that membrane-bound MA domain of Gag recruits Env through interaction with full-length CT, while CT truncation during maturation attenuates the interaction to facilitate uncoating. We propose a model suggesting different arrangements of MA-CT complexes between a D-type and C-type retroviruses with short and long CTs, respectively

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Molecular aspects of the interaction between Mason—Pfizer monkey virus matrix protein and artificial phospholipid membrane

Cited by 3 publications

References 56 publications

Differences and commonalities in plasma membrane recruitment of the two morphogenetically distinct retroviruses HIV-1 and MMTV

Differences and commonalities in plasma membrane recruitment of the two morphogenetically distinct retroviruses HIV-1 and MMTV

Membrane Interactions of the Mason-Pfizer Monkey Virus Matrix Protein and Its Budding Deficient Mutants

Interaction Interface of Mason-Pfizer Monkey Virus Matrix and Envelope Proteins

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