Low pH-Dependent Endosomal Processing of the Incoming Parvovirus Minute Virus of Mice Virion Leads to Externalization of the VP1 N-Terminal Sequence (N-VP1), N-VP2 Cleavage, and Uncoating of the Full-Length Genome

Mani, Bernhard; Baltzer, Claudia; Valle, Noelia; Almendral, José M.; Kempf, Christoph; Ros, Carlos

doi:10.1128/jvi.80.2.1015-1024.2006

Cited by 100 publications

(127 citation statements)

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“…Thus, acidification can be essential for viruses which internalize within CCVs (Damm & Pelkmans, 2006;Marsh & Helenius, 2006;Smith & Helenius, 2004). Studies of parvovirus entry reported that minute virus of mice, adeno-associated virus and CPV internalization require endosomal acidification, and the endosomal acidic environment may induce capsid conformational changes vital for viral release from endosomes to the cytoplasm (Basak & Compans, 1989;Douar et al, 2001;Mani et al, 2006). Blocking acidification of endosomes is a way of suggesting involvement of the clathrin system in cargo entry.…”

Section: Discussionmentioning

confidence: 99%

“…Previously, reported studies have demonstrated that the clathrin-dependent endocytic pathway is the primary route for uptake for some members of the family Parvoviridae into cells (Douar et al, 2001;Mani et al, 2006;Ros et al, 2002;Vendeville et al, 2009). To determine BPV entry dependence on clathrin, CHPZ, a cationic amphiphilic drug that inhibits the formation of clathrin-coated pits at the plasma membrane was used.…”

Section: Discussionmentioning

confidence: 99%

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Bovine parvovirus uses clathrin-mediated endocytosis for cell entry

Dudleenamjil¹,

Lin²,

Dredge³

et al. 2010

Journal of General Virology

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Entry events of bovine parvovirus (BPV) were studied. Transmission electron micrographs of infected cells showed virus particles in cytoplasmic vesicles. Chemical inhibitors that block certain aspects of the cellular machinery were employed to assess viral dependency upon those cellular processes. Chlorpromazine, ammonium chloride, chloroquine and bafilamicin A1 were used to inhibit acidification of endosomes and clathrin-associated endocytosis. Nystatin was used as an inhibitor of the caveolae pathway. Cytochalasin D and ML-7 were used to inhibit actin and myosin functions, respectively. Nocodazole and colchicine were employed to inhibit microtubule activity. Virus entry was assessed by measuring viral transcription using real-time PCR, synthesis of capsid protein and assembly of infectious progeny virus in the presence of inhibitor blockage. The results indicated that BPV entry into embryonic bovine trachael cells utilizes endocytosis in clathrin-coated vesicles, is dependent upon acidification, and appears to be associated with actin and microtubule dependency. Evidence for viral entry through caveolae was not obtained. These findings provide a fuller understanding of the early cell-entry events of the replication cycle for members of the genus Bocavirus.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Bovine parvovirus uses clathrin-mediated endocytosis for cell entry

Dudleenamjil¹,

Lin²,

Dredge³

et al. 2010

Journal of General Virology

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“…The relatively rapid endocytic uptake of parvoviruses appears to be followed by slower traffic along the endocytic compartments toward the nucleus. The endosomal pathway undertaken by parvoviruses appears to be complex and depends on the virus, its concentration, and likely the cell type (Dorsch et al, 2002;Mani et al, 2006;Sonntag et al, 2006;Suikkanen et al, 2003;Yuan & Parrish, 2001). Conformational alterations in capsid structure probably occur in the endosomal compartment facilitating uncoating and transport to the nucleus.…”

Section: Engulfmentmentioning

confidence: 99%

“…It has been widely used as a probe to study acid-mediated viral trafficking using a variety of virus models. Entry pathway studies of mouse polyomavirus (Liebl et al, 2006), feline calicivirus (Stuart & Brown, 2006), bovine viral diarrhea virus (Lecot et al, 2005), AAV (Bartlett et al, 2000), MVM (Mani et al, 2006;Ros et al, 2002), mouse hepatitis virus type 2 (Pu & Zhang, 2008), poliovirus , baculovirus (Long et al, 2006), hepatitis C virus (Blanchard et al, 2006), influenza virus (Guinea & Carrasco, 1995;Sieczkarski et al, 2003), HIV-1 (Fredericksen et al, 2002), and human rhinovirus 14 (Bayer et al, 1999) have analyzed the effects of Baf A1 on virus trafficking and examined the role of endosomal acidification in a route that leads to viral replication. For studies of parvovirus entry Baf A1 may be an inhibitor preferred over chlorpromazine because chlorpromazine is not only an inhibitor of clathrin lattice processing, but is also an inhibitor of phospholipase A2.…”

Section: Engulfmentmentioning

confidence: 99%

“…Chemical inhibitors are assumed to block the entry pathway at certain specific points and incomplete virus replication in the presence of inhibitor is presumed to indicate viral penetration using the pathway blocked by the drug. Commonly used drugs are chlorpromazine (prevents assembly and disassembly of clathrin lattices at the cell surface and on endosomes by inhibiting clathrin polymerization which blocks assembly of coated pits and is also a phospholipase A2 inhibitor, Blanchard et al, 2006); bafilamycin A1 (inhibits vacuolar proton ATPases inhibiting acidification of endosomes by blocking transport of protons into the vesicle, Clague et al, 1994;Drose & Altendorf, 1997;Wassmer et al, 2005); ammonium chloride (penetrates into the endosome increasing endosomal pH, Jin et al, 2002;Liebl et al, 2006); chloroquine (blocks assembly of clathrin coated pits and raises endosomal pH, Mani et al, 2006;Ros et al, 2002). Brefeldin A has no effect on the early endosome but inhibits vesicle transport and early-to-late endosome transition (Clague et al, 1994;Nebenfuhr et al, 2002).…”

Section: Introductionmentioning

confidence: 99%

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Clathrin-Associated Endocytosis as a Route of Entry into Cells for Parvoviruses

Johnson¹,

Dudleenamjil²

2012

Molecular Regulation of Endocytosis

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Impact of the isoelectric point of model parvoviruses on viral retention in anion‐exchange chromatography

Leisi

Wolfisberg

Nowak

et al. 2020

Biotech & Bioengineering

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Anion-exchange chromatography (AEX) is used in the downstream purification of monoclonal antibodies to remove impurities and potential viral contamination based on electrostatic interactions. Although the isoelectric point (pI) of viruses is considered a key factor predicting the virus adsorption to the resin, the precise molecular mechanisms involved remain unclear. To address this question, we compared structurally homologous parvoviruses that only differ in their surface charge distribution. A single charged amino acid substitution on the capsid surface of minute virus of mice (MVM) provoked an increased apparent pI (pI app) 6.2 compared to wild-type MVM (pI app = 4.5), as determined by chromatofocusing. Despite their radically different pI app , both viruses displayed the same interaction profile in Mono Q AEX at different pH conditions. In contrast, the closely related canine parvovirus (pI app = 5.3) displayed a significantly different interaction at pH 5. The detailed structural analysis of the intricate three-dimensional structure of the capsids suggests that the charge distribution is critical, and more relevant than the pI, in controlling the interaction of a virus with the chromatographic resin. This study contributes to a better understanding of the molecular mechanisms governing virus clearance by AEX, which is crucial to enable robust process design and maximize safety. K E Y W O R D S anion-exchange chromatography, isoelectric point, parvovirus, virus clearance 1 | INTRODUCTION Recombinant proteins, such as therapeutic monoclonal antibodies (mAbs), are commonly produced in mammalian cell culture systems, which carry an inherent risk of being contaminated with viral agents. Some mammalian cell lines (e.g., Chinese hamster ovarian cells) are known to host endogenous retroviruses and to express retroviruslike particles (Dinowitz et al., 1992; Lieber, Benveniste, Livingston, & Todaro, 1973). In addition, mammalian cells can be infected by adventitious viruses, such as the minute virus of mice (MVM), which has, at very low frequency, repetitively been introduced into bioreactors through contaminated raw materials (Berting, Farcet, &

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Low pH-Dependent Endosomal Processing of the Incoming Parvovirus Minute Virus of Mice Virion Leads to Externalization of the VP1 N-Terminal Sequence (N-VP1), N-VP2 Cleavage, and Uncoating of the Full-Length Genome

Cited by 100 publications

References 56 publications

Bovine parvovirus uses clathrin-mediated endocytosis for cell entry

Bovine parvovirus uses clathrin-mediated endocytosis for cell entry

Clathrin-Associated Endocytosis as a Route of Entry into Cells for Parvoviruses

Impact of the isoelectric point of model parvoviruses on viral retention in anion‐exchange chromatography

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