Small molecule inhibitors of the host cell COX/AREG/EGFR/ERK pathway attenuate cytomegalovirus-induced pathogenesis

Melnick, Michael; Abichaker, George; Htet, Khine; Sedghizadeh, Parish P.; Jaskoll, Tina

doi:10.1016/j.yexmp.2011.04.014

Cited by 17 publications

(32 citation statements)

References 49 publications

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“…That human SG-MEC is a virally implicated pathology, is further supported by our finding that purified mouse CMV (mCMV) induces cellular pathology in an in vitro mouse SG organ model that displays a number of histologic and molecular characteristics similar to human MEC Melnick et al, 2011). Specifically, we have demonstrated that mCMV induces (1) mesenchymal-to-epithelial transformation (MET); (2) epithelial and mesenchymal hyperplasia, dysplasia and neoplasia; (3) loss of basement membrane zone components, reduced expression of epithelial-specific adherens junction proteins (E-cadherin, p120), and admixing of stromal-derived and epithelial-derived cells; (4) expression of CRTC1 protein, a protein found in SG MECs but not in normal SG tissue (Tirado et al, 2007); and (5) upregulation of the activated COX/AREG/EGFR/ERK signaling pathway.…”

Section: Introductionmentioning

confidence: 55%

“…Despite the well-documented overexpression of the EGFR → ERK signaling pathway in MEC (Akrish et al, 2009;Ito et al, 2009;Lujan et al, 2010), there has been limited to no success with inhibition of this pathway (Bell and Hanna, 2012;Gillespie et al, 2012), not unlike that seen with other malignancies (Engelman and Settleman, 2008). Using our previously described mouse model of CMV-induced SG dysplasia/neoplasia Melnick et al, 2011), we provide evidence that concurrent inhibition of ERK phosphorylation and inhibition of CMV replication obviates progressive pathogenesis and results in complete SG rescue (regression). These findings provide a mechanistic foundation for clinical trials that utilize similar concurrent treatment with extant FDA-approved drugs.…”

Section: Discussionmentioning

confidence: 90%

“…To this end, one has always to discern patterns of covarying molecular and histopathologic phenotypes, relating measurements and localization of transcripts and proteins (input) to a well-characterized pathologic phenotype (output). Here we utilize an in vitro 3D submandibular gland (SMG) organ culture strategy previously shown to induce cellular pathology resembling secretory gland neoplasia Melnick et al, 2006Melnick et al, , 2011.…”

Section: Resultsmentioning

confidence: 99%

See 2 more Smart Citations

Cytomegalovirus-induced salivary gland pathology: AREG, FGF8, TNF-α, and IL-6 signal dysregulation and neoplasia

Melnick¹,

Deluca²,

Sedghizadeh

et al. 2013

Experimental and Molecular Pathology

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Section: Introductionmentioning

confidence: 55%

Section: Discussionmentioning

confidence: 90%

Section: Resultsmentioning

confidence: 99%

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Cytomegalovirus-induced salivary gland pathology: AREG, FGF8, TNF-α, and IL-6 signal dysregulation and neoplasia

Melnick¹,

Deluca²,

Sedghizadeh

et al. 2013

Experimental and Molecular Pathology

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“…A different activity of HCMV in seropositive patients may be the explanation for the contradicting results in clinical trials, comparing seropositivity of individuals with the occurrence of restenosis or atherosclerosis. Recently Melnick et al, [30] suggested that upregulation of ERK phosphorylation is necessary for initial HCMV induced pathogenesis. The presented models are suitable for further studies on stimulatory and inhibitory effects of HCMV-infection in human coronary cells.…”

Section: Discussionmentioning

confidence: 99%

HCMV infection triggers smooth muscle cell proliferation in a 3D human coronary in vitro model

Voisard¹,

Göttling²,

Baur³

et al. 2013

Virol Discov

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Background: Although a role of the human cytomegalovirus (HCMV) in atherosclerosis and restenosis is probable, clinical studies are not conclusive. The present study investigates in a threedimensional (3D) human coronary transfilter co-culture model the effect of cell-free and cell-associated HCMV-infection. Methods: Human coronary endothelial cells (HCAEC) and HCMSMC were seeded on both sides of a polycarbonate filter membrane. HCMV-infection was carried out by HCMV-infected MO. As controls MO-attack without HCMV-infection, cell free HCMV-infection, and the transfilter co-culture model without MO-attack and without HCMV-infection (Mock) were used. Results: At day 1, day 4, day 7, and day 14 the effects of HCMV-infection on MO adhesion and chemotaxis and on reactive proliferation of HCMSMC was studied. Cell-associated HCMV infection of HCAEC and HCMSMC was less intense and postponed in comparison to cell-free HCMV infection. Endothelial adhesion of MO after cellbased HCMV infection was decreased in comparison to non-infected MO, no clear effect was found on chemotaxis. Both after cell-associated and cell-free HCMV infection proliferation of HCMSMC was significantly increased. Conclusions: In the 3D human coronary transfilter co-culture model both cell-free and cell-associated HCMV-infection significantly increased proliferation of HCMSMC. If we assume that HCMV is involved in the pathogenesis of atherosclereosis and restenosis, the effect of antiviral treatments should be studied in experimental and clinical studies.

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“…This exemplifies a sophisticated approach that poxviruses employ to differentially manipulate EGFR-triggered events for their benefit. Proper EGFR signal transduction is critical for the entry of several virus types into cells (14,36), and aberrant EGFR expression or signaling is associated with certain types of cancers (39). Thus, identifying how VACV modulates EGFR-mediated signal transduction pathways could likely yield new approaches and targets for antiviral or anticancer therapies.…”

Section: Discussionmentioning

confidence: 99%

The C11R Gene, Which Encodes the Vaccinia Virus Growth Factor, Is Partially Responsible for MVA-Induced NF-κB and ERK2 Activation

Martin

Harris

Shisler

2012

J Virol

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MVA is an attenuated strain of vaccinia virus (VACV) that is a popular vaccine vector. MVA infection activates NF-κB. For 293T cells, it is known that MVA early gene expression activates extracellular signal-regulated kinase 2 (ERK2), resulting in NF-κB activation. However, other viral and cellular mechanisms responsible for this event are ill defined. The data presented here show that the epidermal growth factor receptor (EGFR) is at least one apical trigger in this pathway: ERK2 and NF-κB activation was diminished when MVA infections occurred in cells devoid of the EGFR (CHO K1 cells) or in the presence of a drug that inhibits EGFR activation (AG1478) in 293T cells. The expression of dominant negative Ras or Raf proteins still permitted NF-κB activation, suggesting that a nonclassical EGFR-based signal transduction pathway triggered ERK2–NF-κB activation. C11R is an early gene present in MVA and other orthopoxviruses. It encodes the soluble, secreted vaccinia virus growth factor (VGF), a protein that binds to and stimulates the EGFR. Here it was observed that NF-κB was activated in 293T cells transfected with a plasmid encoding the C11R gene. Silencing by small interfering RNA (siRNA) or deletion of the C11R gene (MVAΔC11R) reduced both MVA-induced ERK2 and NF-κB activation in 293T cells or the keratinocyte line Hacat, suggesting that this mechanism of MVA-induced NF-κB activation may be common for several cell types.

show abstract

Small molecule inhibitors of the host cell COX/AREG/EGFR/ERK pathway attenuate cytomegalovirus-induced pathogenesis

Cited by 17 publications

References 49 publications

Cytomegalovirus-induced salivary gland pathology: AREG, FGF8, TNF-α, and IL-6 signal dysregulation and neoplasia

Cytomegalovirus-induced salivary gland pathology: AREG, FGF8, TNF-α, and IL-6 signal dysregulation and neoplasia

HCMV infection triggers smooth muscle cell proliferation in a 3D human coronary in vitro model

The C11R Gene, Which Encodes the Vaccinia Virus Growth Factor, Is Partially Responsible for MVA-Induced NF-κB and ERK2 Activation

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