Endocytosis of Chikungunya Virus into Mammalian Cells: Role of Clathrin and Early Endosomal Compartments

Bernard, Éric; Solignat, Maxime; Chazal, Nathalie; Higgs, Stephen; Devaux, Christian; Briant, Laurence

doi:10.1371/journal.pone.0011479

Cited by 150 publications

(181 citation statements)

References 56 publications

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“…4 The ribbon image showing superimposition of the modeled E2 protein (purple color) and the crystallized immature E1-E2-E3complex of Chikungunya virus [46] (PDB Id: 3n40) (green color) (color figure online) by Hunt and colleagues reported that Bafilomycin A1 was found to block the expression of a virus-encoded reporter gene of sindbis virus in both infection and transfection of the BHK cells [18]. Further, another study reported limited inhibitory effect of bafilomycin in post CHIKV infection in HEK239T cells [5]. The inhibitory effect of bafilomycin has also been reported previously for other viruses like influenza [17].…”

Section: Molecular Docking and MD Simulation Studiesmentioning

confidence: 99%

Potential entry inhibitors of the envelope protein (E2) of Chikungunya virus: in silico structural modeling, docking and molecular dynamic studies

et al. 2017

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Chikungunya fever is an arboviral infection caused by the Chikungunya virus (CHIKV) and is transmitted by Aedes mosquito. The envelope protein (E2) of Chikungunya virus is involved in attachment of virion with the host cell. The present study was conceptualized to determine the structure of E2 protein of CHIKV and to identify the potential viral entry inhibitors. The secondary and tertiary structure of E2 protein was determined using bioinformatics tools. The mutational analysis of the E2 protein suggested that mutations may stabilize or de-stabilize the structure which may affect the structure-function relationship. In silico screening of various compounds from different databases identified two lead molecules i.e. phenothiazine and bafilomycin. Molecular docking and MD simulation studies of the E2 protein and compound complexes was carried out. This analysis revealed that bafilomycin has high docking score and thus high binding affinity with E2 protein suggesting stable protein-ligand interaction. Further, MD simulations suggested that both the compounds were stabilizing E2 protein. Thus, bafilomycin and phenothiazine may be considered as the lead compounds in terms of potential entry inhibitor for CHIKV. Further, these results should be confirmed by comprehensive cell culture, cytotoxic assays and animal experiments. Certain derivatives of phenothiazines can also be explored in future studies for entry inhibitors against CHIKV. The present investigation thus provides insight into protein structural dynamics of the envelope protein of CHIKV. In addition the study also provides information on the dynamics of interaction of E2 protein with entry inhibitors that will contribute towards structure based drug design.

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Section: Molecular Docking and MD Simulation Studiesmentioning

confidence: 99%

Potential entry inhibitors of the envelope protein (E2) of Chikungunya virus: in silico structural modeling, docking and molecular dynamic studies

et al. 2017

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“…A detailed entry mechanism description is not available so far. Some authors implicate a clathrin-dependent pathway [64,66], whereas other authors have proposed that CHIKV enters by a clathrin-independent, but Eps15-dependent pathway [65]. These later authors also have found evidence that multiple pathways maybe employed by CHIKV to enter into cells, as already proposed with dengue virus (DENV) [67,68].…”

Section: Genomic Organization and Viral Replicationmentioning

confidence: 95%

“…Viral replication is initiated by attachment of viral envelope to host cell receptors [63], followed by low pH-mediated membrane fusion and delivery of the viral nucleocapsid into the cytoplasm (Fig. 1) [64,65]. A detailed entry mechanism description is not available so far.…”

Section: Genomic Organization and Viral Replicationmentioning

confidence: 99%

Chikungunya and Its Interaction With the Host Cell

et al. 2015

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Chikungunya virus (CHIKV) is a mosquitotransmitted alphavirus belonging to the Togaviridae family. It is a virus with a single-stranded, positive sense RNA genome, maintained in a sylvatic and urban cycle, involving humans and mosquitoes from Aedes species, mainly Aedes aegypti and Aedes albopictus. In less than 10 years, CHIKV has spread from the coast of Kenya throughout the Indian Ocean, Pacific Ocean, and Caribbean regions, causing millions of infections in over 50 countries. In other words, CHIKV has emerged as a true global pathogen. The clinical signs include nonspecific flu-like symptoms and a characteristic rash accompanied by joint pain that may last long time after the resolution of the infection. The molecular mechanism underlying the chronic polyarthralgia in patients is not well understood. In this review, we summarize the CHIKV genome organization, replication, epidemiology, clinical manifestations, and immunopathogenesis with particular emphasis on host-pathogen interactions.

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“…Although specific host receptors for CHIKV are still to be determined, CHIKV is believed to enter cells by receptor-mediated pathway through E2 glycoprotein (Weber et al, 2017) (Figure 4B), and it is internalized either via clathrin-mediated endocytosis or a clathrin-independent Eps-15-dependent endocytosis pathway (Hoornweg et al, 2016), like other alphaviruses. Eps-15 is a member of clathrin-coated pits (Bernard et al, 2010). With the progress of infection, the endosome become acidic, inducing the dissociation of E2-E1 heterodimer and a conformation change of E1 membrane fusion protein, allowing host cell membrane and virus envelop to fuse, followed by the release of viral nucleocapsids into the cytoplasm (Gibbons et al, 2004;Bernard et al, 2010).…”

Section: Virus Life Cyclementioning

confidence: 99%

“…Eps-15 is a member of clathrin-coated pits (Bernard et al, 2010). With the progress of infection, the endosome become acidic, inducing the dissociation of E2-E1 heterodimer and a conformation change of E1 membrane fusion protein, allowing host cell membrane and virus envelop to fuse, followed by the release of viral nucleocapsids into the cytoplasm (Gibbons et al, 2004;Bernard et al, 2010). The nucleocapsid protein will then bind to the ribosome (considered to be cellular uncoating factor) to initiate uncoating, resulting in the release of genomic RNA into the cytoplasm (Singh and Helenius, 1992).…”

Section: Virus Life Cyclementioning

confidence: 99%