Lentiviral Nef Proteins Utilize PAK2-Mediated Deregulation of Cofilin as a General Strategy To Interfere with Actin Remodeling

Stolp, Bettina; Abraham, Libin; Rudolph, Jochen M.; Fackler, Oliver T.

doi:10.1128/jvi.02467-09

Cited by 50 publications

(76 citation statements)

References 45 publications

(75 reference statements)

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“…These results were mirrored in 3D matrices where Nef specifically inhibited T-lymphocyte motility in high-density collagen, although motility at low collagen density remained unaffected by Nef expression. It thus emerges that Nef specifically interferes with cell-motility modes that rely on the generation of contractile force to overcome physical constraints of the direct environment, including T-lymphocyte chemotaxis across transwell membranes (4,5,12,14) and diapedesis (present study). This specificity would also explain why Nef-mediated inhibition is relatively moderate on T-lymphocyte homing to spleen, which does not involve the crossing of an endothelial barrier, and motility in the lymph node parenchyma, where lymphocytes are embedded in a relatively wide-spaced extracellular matrix structure (19).…”

Section: Discussionmentioning

confidence: 99%

“…How these functions individually contribute to the prominent role of Nef in AIDS pathogenesis remains to be established. Inhibition of dynamic host cell actin remodeling, mediated via association with the cellular kinase PAK2 that induces inactivation of the actin-severing factor cofilin to reduce actin turnover, represents a conserved activity of lentiviral Nef proteins (2)(3)(4)(5)(6)(7)(8). Nef-PAK2 association depends on a critical phenylalanine at position 195 of Nef (or 191 depending on the HIV-1 nef allele analyzed) that is dispensable for other Nef activities (9).…”

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HIV-1 Nef interferes with T-lymphocyte circulation through confined environments in vivo

Stolp

Imle

Coelho

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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HIV-1 negative factor (Nef) elevates virus replication and contributes to immune evasion in vivo. As one of its established in vitro activities, Nef interferes with T-lymphocyte chemotaxis by reducing host cell actin dynamics. To explore Nef’s influence on in vivo recirculation of T lymphocytes, we assessed lymph-node homing of Nef-expressing primary murine lymphocytes and found a drastic impairment in homing to peripheral lymph nodes. Intravital imaging and 3D immunofluorescence reconstruction of lymph nodes revealed that Nef potently impaired T-lymphocyte extravasation through high endothelial venules and reduced subsequent parenchymal motility. Ex vivo analyses of transendothelial migration revealed that Nef disrupted T-lymphocyte polarization and interfered with diapedesis and migration in the narrow subendothelial space. Consistently, Nef specifically affected T-lymphocyte motility modes used in dense environments that pose high physical barriers to migration. Mechanistically, inhibition of lymph node homing, subendothelial migration and cell polarization, but not diapedesis, depended on Nef’s ability to inhibit host cell actin remodeling. Nef-mediated interference with in vivo recirculation of T lymphocytes may compromise T-cell help and thus represents an important mechanism for its function as a HIV pathogenicity factor.

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Section: Discussionmentioning

confidence: 99%

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confidence: 99%

HIV-1 Nef interferes with T-lymphocyte circulation through confined environments in vivo

Stolp

Imle

Coelho

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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“…174 Furthermore, the Nef-PAK2 interaction potently inhibits motility of fibroblasts through accumulation of phosphorylated, inactive cofilin, a process that is highly conserved among different nef alleles of HIV-1, HIV-2, and SIV. 168,171,175,176 In addition, Nef has been reported to interact in a PAK2-dependent manner with components of the exocyst complex. 177 The exocyst complex is an octameric complex that tethers vesicles at the plasma membrane, regulates polarized exocytosis, and recruits membranes and proteins required for the formation of nanotubes that interconnect cells.…”

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confidence: 99%

Rho’ing in and out of cells

2014

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These authors contributed equally to this work Keywords: Rho GTPase, actin, egress, entry, gene expression, immune system, transformation, virus Rho GTPases are key regulators of actin and microtubule dynamics and organization. increasing evidence shows that many viruses have evolved diverse interactions with Rho GTPase signaling and manipulate them for their own benefit. in this review, we discuss how Rho GTPase signaling interferes with many steps in the viral replication cycle, especially entry, replication, and spread. Seen the diversity between viruses, it is not surprising that there is considerable variability in viral interactions with Rho GTPase signaling. However, several largely common effects on Rho GTPases and actin architecture and microtubule dynamics have been reported. For some of these processes, the molecular signaling and biological consequences are well documented while for others we just begin to understand them. A better knowledge and identification of common threads in the different viral interactions with Rho GTPase signaling and their ultimate consequences for virus and host may pave the way toward the development of new antiviral drugs that may target different viruses.©2014 Landes Bioscience. Do not distribute. e28318-2Small GTPases volume 5effector of ROCK, which phosphorylates and inhibits cofilin.14 Cofilin is an F-actin-severing protein. Mainly depending on the local availability of G-actin monomers, cofilin activity may lead to net actin depolymerization or increased actin polymerization and branching. Other RhoA effectors include members of the ezrin/radixin/moesin (ERM) proteins 15 . Rac1 is thought to release WAVE from an inhibited complex, thereby activating the actin-polymerizing complex Arp2/3. 16,17 Active Arp2/3 mediates branching and elongation of existing actin filaments, generating a meshwork. Cdc42 also activates Arp2/3 through a direct interaction with the Arp2/3 activators Wiskott-Aldrich syndrome protein (WASP) or N-WASP.18 Both Rac1 and Cdc42 also activate group I serine/threonine p21 activating kinases (PAK). These different signalization branches are interconnected. In general, RhoA pathway signaling counteracts the Rac1 and Cdc42 signaling axes and vice versa.Because Rho GTPase signaling is involved in a plethora of cellular processes, it is perhaps not surprising that several viral gene products have evolved to interfere with and modulate these signaling axes. Indeed, several viruses interfere with the actin cytoskeleton and Rho GTPase signaling during many steps of their replication cycle. During entry and egress, these interactions may allow or facilitate viral particle passage across the cortical actin barrier and to rearrange actin to conformations that promote virus infection and spread, while other viral processes, such as intracellular movement, gene expression and latency, but also interaction with the immune system or oncogenesis may also depend to some extent on Rho GTPase signaling and associated actin rearrangements. In this review, the current kno...

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“…Then, Nef activates Rac by binding the DOCK2-ELMO1 complex, a key activator of Rac in antigen-and chemokine-initiated signaling pathways, and this interaction is linked to the abilities of Nef to inhibit chemotaxis and promote T cell activation (Janardhan et al, 2004). Finally, Nef association with Pak2 prevents actin remodeling to impair host cell motility by disregulation of cofilin, which is an actin-depolymerizing factor that promotes actin turnover and subsequent cell motility (Stolp et al, 2010). The cytoskeleton reorganization induced by Nef is associated with an impairment of cell movements combined with induction of long filopodium-like structures in T lymphocytes (Stolp et al, 2010).…”

Section: Interference With Cell Cytoskeletonmentioning

confidence: 99%

“…Finally, Nef association with Pak2 prevents actin remodeling to impair host cell motility by disregulation of cofilin, which is an actin-depolymerizing factor that promotes actin turnover and subsequent cell motility (Stolp et al, 2010). The cytoskeleton reorganization induced by Nef is associated with an impairment of cell movements combined with induction of long filopodium-like structures in T lymphocytes (Stolp et al, 2010). In summary, Nef displays a variety of complex effects on the motility and cellular morphology of HIV-1-infectected T lymphocyte, thus resulting in a strategy to improve immune evasion and viral spread in the infected host.…”

Section: Interference With Cell Cytoskeletonmentioning

confidence: 99%

Functions of the Lentiviral Accessory Protein Nef During the Distinct Steps of HIV and SIV Replication Cycle

Costa¹,

Mendonça²,

Sampaio³

2011

HIV and AIDS - Updates on Biology, Immunology, Epidemiology and Treatment Strategies

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Lentiviral Nef Proteins Utilize PAK2-Mediated Deregulation of Cofilin as a General Strategy To Interfere with Actin Remodeling

Cited by 50 publications

References 45 publications

HIV-1 Nef interferes with T-lymphocyte circulation through confined environments in vivo

HIV-1 Nef interferes with T-lymphocyte circulation through confined environments in vivo

Rho’ing in and out of cells

Functions of the Lentiviral Accessory Protein Nef During the Distinct Steps of HIV and SIV Replication Cycle

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