Induced Maturation of Human Immunodeficiency Virus

Matteı, Simone; Anders, Maria; Konvalinka, Jan; Kräusslich, Hans‐Georg; Briggs, John; Müller, Bárbara

doi:10.1128/jvi.02271-14

Cited by 34 publications

(40 citation statements)

References 58 publications

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“…This essential process in the viral life cycle must occur in a precise order to produce infectious virus [74,75]. An inhibitor of maturation, bevirimat, was developed to target the final processing step for the Gag precursor (Figure 1).…”

Section: Inhibitors Targeting the Gag Or Gag-pol Precursorsmentioning

confidence: 99%

Highly Resistant HIV-1 Proteases and Strategies for Their Inhibition

2015

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The virally encoded protease is an important drug target for AIDS therapy. Despite the potency of the current drugs, infections with resistant viral strains limit the long-term effectiveness of therapy. Highly resistant variants of HIV protease from clinical isolates have different combinations of about 20 mutations and several orders of magnitude worse binding affinity for clinical inhibitors. Strategies are being explored to inhibit these highly resistant mutants. The existing inhibitors can be modified by introducing groups with the potential to form new interactions with conserved protease residues, and the flexible flaps. Alternative strategies are discussed, including designing inhibitors to bind to the open conformation of the protease dimer, and inhibition of the protease-catalyzed processing of the Gag-Pol precursor.

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Section: Inhibitors Targeting the Gag Or Gag-pol Precursorsmentioning

confidence: 99%

Highly Resistant HIV-1 Proteases and Strategies for Their Inhibition

2015

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“…Morphology was classified as wt (the typical conical or tubular cores found in the wt viruses), mildly aberrant (cores with a slightly deformed structure with some similarity to the conical or tubular ones), or severely aberrant (cores with a spherical or highly disordered core morphology). Core morphology data for the wt preparation were derived from the data set collected for and described by Mattei et al (28).…”

Section: Methodsmentioning

confidence: 99%

RNA and Nucleocapsid Are Dispensable for Mature HIV-1 Capsid Assembly

Matteı

Flemming

Anders-Ößwein

et al. 2015

J Virol

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Human immunodeficiency virus type 1 (HIV-1) is released from infected cells in an immature, noninfectious form in which the structural polyprotein Gag is arranged in a hexameric lattice, forming an incomplete spherical shell. Maturation to the infectious form is mediated by the viral protease, which cleaves Gag at five sites, releasing the CA (capsid) protein, which forms a conical capsid encasing the condensed RNA genome. The pathway of this structural rearrangement is currently not understood, and it is unclear how cone assembly is initiated. RNA represents an integral structural component of retroviruses, and the viral nucleoprotein core has previously been proposed to nucleate mature capsid assembly. We addressed this hypothesis by replacing the RNA-binding NC ( M orphological maturation represents a key event in the replication cycle of retroviruses. Human immunodeficiency virus type 1 (HIV-1) particles are released as immature, noninfectious virions whose main constituents are the structural polyproteins Gag and Gag-Pro-Pol. Cleavage of Gag and Gag-Pro-Pol at multiple sites by the virus genome-encoded PR (protease) releases the mature structural proteins MA (matrix), CA (capsid), and NC (nucleocapsid) as well as the functional viral enzymes PR, reverse transcriptase (RT), and IN (integrase) (1). Proteolytic processing triggers a dramatic rearrangement of the virion architecture. In immature HIV-1, an incomplete sphere made of ϳ2,500 radially arranged Gag molecules lines the viral lipid envelope. In contrast, mature, infectious particles are characterized by a cone-shaped capsid assembled from CA molecules. The capsid encases a dense ribonucleoprotein (RNP) core, in which NC condenses the viral RNA genome (2, 3).Hexagonal arrangements of the CA domain represent the basic structural element of both the immature Gag lattice and the mature capsid. However, contact surfaces involved in CA-CA interactions differ significantly between immature and mature structures, and the spacing of the immature hexagonal lattice (80 Å) is tighter than that of the mature lattice (96 Å) (2, 3). Furthermore, only about 50% of the CA molecules packaged are used for formation of the mature capsid (4). These observations led to the proposition that morphological maturation occurs via dissociation of the immature lattice, followed by new assembly of the mature cone structure. This model is supported by structural analyses of HIV-1 derivatives carrying mutations at individual PR recognition sites in Gag, in particular, those preventing the late step of CA-SP1 processing (5, 6).Whereas immature HIV-1 particles are very heterogeneous with respect to diameter and the degree of Gag shell completeness (7,8), the majority of mature particles contain a single capsid core structure and a small number of particles contain two capsid structures (9). It therefore appears to be intuitive that the process of capsid assembly from dissociated CA mono-or oligomers

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“…Molecular crowding effects are known to influence protein behaviours 29 and yet, remarkably, virion maturation consistently produces similar capsid morphologies. The relatively fast maturation process 30,31 makes in vivo study of capsid self--assembly pathways difficult. Nonetheless, Woodward et al 32 show capsid formation proceeding via a hook--shaped precursor to the broad end of the capsid, in contrast with models of capsid assembly that begin with the narrow end of the cone 33 .…”

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confidence: 99%

“Coarse-grained simulation reveals key features of HIV-1 capsid self-assembly”

Grime

Dama

Ganser‐Pornillos

et al. 2016

Preprint

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The maturation of HIV-1 viral particles is essential for viral infectivity. During maturation, many copies of the capsid protein (CA) self-assemble into a capsid shell to enclose the viral RNA. The mechanistic details of the initiation and early stages of capsid assembly remain to be delineated. We present coarse-grained simulations of capsid assembly under various conditions, considering not only capsid lattice self-assembly but also the potential disassembly of capsid upon delivery to the cytoplasm of a target cell. The effects of CA concentration, molecular crowding, and the conformational variability of CA are described, with results indicating that capsid nucleation and growth is a multi-stage process requiring well-defined metastable intermediates. Generation of the mature capsid lattice is sensitive to local conditions, with relatively subtle changes in CA concentration and molecular crowding influencing self-assembly and the ensemble of structural morphologies.

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Induced Maturation of Human Immunodeficiency Virus

Cited by 34 publications

References 58 publications

Highly Resistant HIV-1 Proteases and Strategies for Their Inhibition

Highly Resistant HIV-1 Proteases and Strategies for Their Inhibition

RNA and Nucleocapsid Are Dispensable for Mature HIV-1 Capsid Assembly

“Coarse-grained simulation reveals key features of HIV-1 capsid self-assembly”

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