Emerin Is Hyperphosphorylated and Redistributed in Herpes Simplex Virus Type 1-Infected Cells in a Manner Dependent on both UL34 and US3

Leach, Natalie; Bjerke, Susan L.; Christensen, D.; Bouchard, Jacques M.; Mou, Fan; Park, Richard; Baines, Joel D.; Haraguchi, Tokuko; Roller, Richard J.

doi:10.1128/jvi.00196-07

Cited by 104 publications

(164 citation statements)

References 68 publications

(80 reference statements)

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“…PKC and pUL97. There is accumulating evidence that the involvement of both cellular and viral protein kinases (some of which possess direct lamin-phosphorylating activity) is important for the regulation of nuclear egress of other herpesviruses as well (Klupp et al, 2001;Reynolds et al, 2002;Marschall et al, 2005;Bjerke & Roller, 2006;Park & Baines, 2006;Kato et al, 2006;Leach et al, 2007). It will be crucial to determine the exact phosphorylation target sites on lamins and lamina-associated proteins of these protein kinases for a detailed understanding of the cytomegaloviral nuclear egress.…”

Section: Conclusion: Model Of a Postulated Viral-cellular Multi-protementioning

confidence: 99%

“…Recruitment of PKC to the nuclear membrane occurs during infection with HCMV, murine cytomegalovirus (MCMV) and herpes simplex virus type-1 (HSV-1) (Muranyi et al, 2002;Park & Baines, 2006;Milbradt et al, 2007). A conserved group of herpesvirus-encoded lamina-associated proteins have been implicated in the recruitment of PKC, the rearrangement of nuclear lamina components and viral nuclear egress (Reynolds et al, 2004;Muranyi et al, 2002;Leach et al, 2007;Morris et al, 2007;Fuchs et al, 2002;Farina et al, 2005;Milbradt et al, 2007; Camozzi et al, 2008). This group comprises pUL50 and pUL53 in HCMV and their homologues in other herpesviruses.…”

Section: Introductionmentioning

confidence: 99%

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Cytomegaloviral proteins that associate with the nuclear lamina: components of a postulated nuclear egress complex

Milbradt

Auerochs

Sticht

et al. 2009

Journal of General Virology

147

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The nuclear egress of cytomegaloviral capsids traversing the nuclear envelope is dependent on a locally restricted destabilization of the rigid nuclear lamina. It has been suggested that the multicomponent nuclear egress complex (NEC) that is formed is comprised of both viral and cellular proteins which act to recruit lamin-phosphorylating protein kinases. Recently, we reported that the lamina-associated human cytomegalovirus-encoded proteins pUL50 and pUL53, conserved among herpesviruses, interact with each other and recruit protein kinase C (PKC) to the nuclear envelope in transfected cells. The multiple interactions of the transmembrane protein pUL50 with pUL53, PKC and cellular PKC-binding protein p32, appear crucial to the formation of the NEC. In this study, we mapped individual interaction sequence elements of pUL50 by coimmunoprecipitation analysis of deletion mutants and yeast two-hybrid studies. Amino acids 1-250 were shown to be responsible for interaction with pUL53, 100-280 for PKC and 100-358 for p32. Interestingly, p32 specifically interacted with multiple NEC components, including the kinases PKC and pUL97, thus possibly acting as an adaptor for protein recruitment to the lamin B receptor. Notably, p32 was the only protein that interacted with the lamin B receptor. Immunofluorescence studies visualized the colocalization of NEC components at the nuclear rim in coexpression studies. The data imply that a tight interaction between at least six viral and cellular proteins leads to the formation of a postulated multi-protein complex required for nuclear egress. INTRODUCTIONHuman cytomegalovirus (HCMV), a member of the bherpesvirus subfamily, is a ubiquitous, clinically important human pathogen that causes severe systemic disease in immunosuppressed hosts and prenatally infected children (Mocarski et al., 2007). As is characteristic for most DNA viruses, HCMV replicates its genome in the nucleus of the host cell. Thereafter, preformed viral capsids are packaged with genomic DNA and have to be transported to the cytoplasm for final maturation and viral release. Due to the large size of cytomegaloviral capsids (~130 nm; Chen et al., 1999), these cannot be transported through the nuclear pore complex (~40 nm; Panté & Kann, 2002). The most widely accepted model for nuclear egress of HCMV and other herpesviruses is based on a transient primary envelopment by budding through the inner nuclear membrane (Mettenleiter, 2004(Mettenleiter, , 2006Sanchez & Spector, 2002;Sampaio et al., 2005). However, before herpesvirusencoded capsids gain access to the inner nuclear membrane, the rigid proteinaceous network of the nuclear lamina provides a major obstacle. Thus, the locally restricted destabilization of the nuclear lamina is required during the viral replication process .A basic principle of the reorganization of the nuclear lamina is the recruitment of cellular and/or virus-encoded protein kinases to increase the site-specific phosphorylation of nuclear lamins and lamin-binding proteins (Dechat et al., 2008). Ce...

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Section: Conclusion: Model Of a Postulated Viral-cellular Multi-protementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Cytomegaloviral proteins that associate with the nuclear lamina: components of a postulated nuclear egress complex

Milbradt

Auerochs

Sticht

et al. 2009

Journal of General Virology

147

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“…Alphaherpesviruses also express a viral serine/threonine protein kinase, pUS3, that phosphorylates lamins and lamin receptor emerin, which are thought to be involved in maintaining nuclear integrity (Leach et al, 2007;Morris et al, 2007;Mou et al, 2008). In addition, both HSV-1 and PrV pUL31 and pUL34 have been shown to be phosphorylated in a pUS3-dependent manner, and all three proteins have been found to be incorporated into primary virions (Purves et al, 1991; Granzow et al, 2004;Ryckman and Roller, 2004;Kato et al, 2005;Mou et al, 2007Mou et al, , 2009.…”

Section: Primary Envelopment and Deenvelopmentmentioning

confidence: 99%

“…HSV-1 and PrV disrupt the lamina through two viral proteins, pUL31 and pUL34, which form a complex colocalized to the inner NM (Reynolds et al, 2002;Reynolds et al, 2004;Simpson-Holley et al, 2004;Simpson-Holley et al, 2005;Bjerke and Roller, 2006). Research suggested that pUL31 and pUL34 promote viral nuclear egress by several mechanisms, including (1) affecting maturation of viral replication intermediates so that capsids assemble adjacent to the nuclear envelope, making it convenient for primary egress (Simpson-Holley et al, 2004, (2) causing displacement of and conformational changes in lamins A/C and B (Reynolds et al, 2004;Simpson-Holley et al, 2004;Bjerke and Roller, 2006), and (3) mislocalizing the membrane lamin receptors, such as the lamin B receptor and emerin, which tether lamins to the inner NM (Scott and O'Hare, 2001;Leach et al, 2007;Morris et al, 2007;Mou et al, 2008). Amazingly, expression of PrV pUL31 and pUL34 in RK-13 cells resulted in formation of vesicles in the perinuclear space, indicating that they may compose the essential budding machinery (Klupp et al, 2007).…”

Section: Primary Envelopment and Deenvelopmentmentioning

confidence: 99%

“…There, the viruses encounter the nuclear lamina, a rigid network of lamin proteins lining the inner NM, which is a major obstacle for budding of the nucleocapsids. Herpesviruses disrupt the nuclear lamina in order to bud into the perinuclear space and acquire the inner NM as the envelope, the so called primary envelopment (Scott and O'Hare, 2001;Muranyi et al, 2002;Leach et al, 2007;Mou et al, 2007;Mou et al, 2008). HSV-1 and PrV disrupt the lamina through two viral proteins, pUL31 and pUL34, which form a complex colocalized to the inner NM (Reynolds et al, 2002;Reynolds et al, 2004;Simpson-Holley et al, 2004;Simpson-Holley et al, 2005;Bjerke and Roller, 2006).…”

Section: Primary Envelopment and Deenvelopmentmentioning

confidence: 99%

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Role of tegument proteins in herpesvirus assembly and egress

et al. 2010

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Morphogenesis and maturation of viral particles is an essential step of viral replication. An infectious herpesviral particle has a multilayered architecture, and contains a large DNA genome, a capsid shell, a tegument and an envelope spiked with glycoproteins. Unique to herpesviruses, tegument is a structure that occupies the space between the nucleocapsid and the envelope and contains many virus encoded proteins called tegument proteins. Historically the tegument has been described as an amorphous structure, but increasing evidence supports the notion that there is an ordered addition of tegument during virion assembly, which is consistent with the important roles of tegument proteins in the assembly and egress of herpesviral particles. In this review we first give an overview of the herpesvirus assembly and egress process. We then discuss the roles of selected tegument proteins in each step of the process, i.e., primary envelopment, deenvelopment, secondary envelopment and transport of viral particles. We also suggest key issues that should be addressed in the near future.

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Diseases of the Nucleoskeleton

Holaska

2016

Comprehensive Physiology

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The nucleus is separated from the cytosol by the nuclear envelope, which is a double lipid bilayer composed of the outer nuclear membrane and the inner nuclear membrane. The intermediate filament proteins lamin A, lamin B, and lamin C form a network underlying the inner nuclear membrane. This proteinaceous network provides the nucleus with its strength, rigidity, and elasticity. Positioned within the inner nuclear membrane are more than 150 inner nuclear membrane proteins, many of which interact directly with lamins and require lamins for their inner nuclear membrane localization. Inner nuclear membrane proteins and the nuclear lamins define the nuclear lamina. These inner nuclear membrane proteins have tissue-specific expression and diverse functions including regulating cytoskeletal organization, nuclear architecture, cell cycle dynamics, and genomic organization. Loss or mutations in lamins and inner nuclear membrane proteins cause a wide spectrum of diseases. Here, I will review the functions of the well-studied nuclear lamina proteins and the diseases associated with loss or mutations in these proteins. © 2016 American Physiological Society.

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Emerin Is Hyperphosphorylated and Redistributed in Herpes Simplex Virus Type 1-Infected Cells in a Manner Dependent on both UL34 and US3

Cited by 104 publications

References 68 publications

Cytomegaloviral proteins that associate with the nuclear lamina: components of a postulated nuclear egress complex

Cytomegaloviral proteins that associate with the nuclear lamina: components of a postulated nuclear egress complex

Role of tegument proteins in herpesvirus assembly and egress

Diseases of the Nucleoskeleton

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