Caveolin-1 Associated Adenovirus Entry into Human Corneal Cells

Yousuf, Mohammad; Zhou, Xiaohong; Mukherjee, Santanu; Chintakuntlawar, Ashish V.; Lee, Yoo‐Hyun; Ramke, Mirja; Chodosh, James; Rajaiya, Jaya

doi:10.1371/journal.pone.0077462

Cited by 42 publications

(65 citation statements)

References 96 publications

(121 reference statements)

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“…Because human adenoviruses do not replicate in mouse cells (Blair et al, 1989; Ginsberg et al, 1991; Silverstein and Strohl, 1986; Zucker and Flint, 1985), the mouse adenovirus keratitis model is an inflammatory rather than a replication model and bypasses the adenoviral replication-resistant mouse corneal epithelium. We have shown previously that tropism in humans is better predicted by assays of HAdV entry into human corneal epithelial cells, than by inflammatory responses upon injection of virus into the mouse corneal stroma (Yousuf et al, 2013; Zhou et al, 2012). Therefore, we tested the cellular entry of Cy3 labeled virus in Tert-immortalized human corneal epithelial (THE) cells (gift of Dr. Jerry Shay) and primary human corneal fibroblasts (HCF), with A549 cells as controls.…”

Section: Resultsmentioning

confidence: 99%

Recombination of the epsilon determinant and corneal tropism: Human adenovirus species D types 15, 29, 56, and 69

et al. 2015

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Viruses within human adenovirus species D (HAdV-D) infect epithelia at essentially every mucosal site. Hypervariable loops 1 and 2 of the hexon capsid protein contain epitopes that together form the epsilon determinant for serum neutralization. We report our analyses comparing HAdV-D15, 29, 56, and the recently identified type 69, each with highly similar hexons and the same serum neutralization profile, but otherwise disparate genomes. Of these, only HAdV-D type 56 is associated with epidemic keratoconjunctivitis (EKC), a severe infection of ocular surface epithelium and underlying corneal stroma. In the mouse adenovirus keratitis model, all four viruses induced inflammation. However, HAdV-D56 entry into human corneal epithelial cells and fibroblasts in vitro dramatically exceeded that of the other three viruses. We conclude that the hexon epsilon determinant is not a prime contributor to corneal tropism.

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Section: Resultsmentioning

confidence: 99%

Recombination of the epsilon determinant and corneal tropism: Human adenovirus species D types 15, 29, 56, and 69

et al. 2015

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“…However, it remains an open question if caveolae transcytosis plays a role in pathological BRB breakdown that deserves careful study. Finally, caveolae seem to play important roles at the ocular surface both in pathogen uptake (Mukherjee et al, 2015; Yousuf et al, 2013), corneal inflammation (Reidy et al, 2013), and wound healing (Amino et al, 1997; Rhim et al, 2010) but these areas are yet to receive further attention.…”

Section: Discussionmentioning

confidence: 99%

Section: Caveolins/caveolae In Other Ocular Cellsmentioning

confidence: 99%

“…Recent work indicates that adenoviruses utilize a caveolae-mediated pathway for entry into corneal cells (Mukherjee et al, 2015; Yousuf et al, 2013). Importantly, disruption of caveolae and cholesterol-rich membrane domains by cholesterol depletion dramatically reduced viral infection (Yousuf et al, 2013). Studies designed to examine viral-mediated gene transfer to the corneal epithelium revealed improved transduction efficiency of recombinant adenovirus to the corneal epithelium by the PDE5 inhibitor, sildenafil, which acted by redistributing caveolin-1 expression from the normal basal epithelial location to suprabasal epithelium thus facilitating viral uptake (Saghizadeh et al, 2010).…”

Section: Caveolins/caveolae In Other Ocular Cellsmentioning

confidence: 99%

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Caveolins and caveolae in ocular physiology and pathophysiology

Reagan

McClellan

et al. 2017

Progress in Retinal and Eye Research

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Caveolae are specialized, invaginated plasma membrane domains that are defined morphologically and by the expression of signature proteins called, caveolins. Caveolae and caveolins are abundant in a variety of cell types including vascular endothelium, glia, and fibroblasts where they play critical roles in transcellular transport, endocytosis, mechanotransduction, cell proliferation, membrane lipid homeostasis, and signal transduction. Given these critical cellular functions, it is surprising that ablation of the caveolae organelle does not result in lethality suggesting instead that caveolae and caveolins play modulatory roles in cellular homeostasis. Caveolar components are also expressed in ocular cell types including retinal vascular cells, Müller glia, retinal pigment epithelium (RPE), conventional aqueous humor outflow cells, the corneal epithelium and endothelium, and the lens epithelium. In the eye, studies of caveolae and other membrane microdomains (i.e., “lipid rafts”) have lagged behind what is a substantial body of literature outside vision science. However, interest in caveolae and their molecular components has increased with accumulating evidence of important roles in vision-related functions such as blood-retinal barrier homeostasis, ocular inflammatory signalling, pathogen entry at the ocular surface, and aqueous humor drainage. The recent association of CAV1/2 gene loci with primary open angle glaucoma and intraocular pressure has further enhanced the need to better understand caveolar functions in the context of ocular physiology and disease. Herein, we provide the first comprehensive review of literature on caveolae, caveolins, and other membrane domains in the context of visual system function. This review highlights the importance of caveolae domains and their components in ocular physiology and pathophysiology and emphasizes the need to better understand these important modulators of cellular function.

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“…We also previously reported that Src kinase is upregulated in the mouse adenovirus keratitis model (Yousuf et al 2013) and may play a role in CXC chemokine expression. Using chemical signaling inhibitors to study signaling and innate immunity in an animal model is a challenge, and sometimes not feasible.…”

Section: Discussionmentioning

confidence: 74%

Novel model of innate immunity in corneal infection

Rajaiya

Zhou

Barequet

et al. 2015

In Vitro Cell.Dev.Biol.-Animal

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The cornea functions as the major refractive interface for vision and protects the internal eye from insult. Current understanding of innate immune responses to corneal infection derives from a synthesis of in vitro and in vivo analyses. However, monolayer cell cultures and mouse models do not accurately duplicate all aspects of innate immunity in human patients. Here, we describe a three-dimensional culture system that incorporates human cells and extracellular matrix to more completely simulate the human cornea for studies of infection. Human corneal stromal fibroblasts were mixed with type I collagen in 3-μm pore size transwell inserts, and overlayed with Matrigel to simulate a human corneal stroma and epithelial basement membrane. These were then infected with a cornea-tropic adenovirus, and exposed on their inferior side to leukocytes derived from human peripheral blood. Subsequent analyses were performed with histology, confocal microscopy, ELISA, and fluorescence-activated cell sorting (FACS). CXCL8, a neutrophil chemokine shown previously as the first cytokine induced in infection of human corneal cells, increased upon adenovirus infection of facsimiles in a dose-responsive fashion. Myeloperoxidase-positive cells infiltrated infected corneal facsimiles in a sub-Matrigel location, possibly due to CXCL8 colocalization with heparan sulfate, a Matrigel constituent. Cellular infiltration was significantly inhibited by treatment with chemical inhibitors of p38 MAPK and Src kinase, both constituents of a signaling cascade previously suggested to regulate inflammation after adenovirus infection. FACS analysis determined that both virus and corneal fibroblasts were necessary for the induction of leukocyte migration into the facsimiles. The corneal facsimile, literally a cornea in a test tube, permits mechanistic studies on human tissue in a highly tractable system.

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Caveolin-1 Associated Adenovirus Entry into Human Corneal Cells

Cited by 42 publications

References 96 publications

Recombination of the epsilon determinant and corneal tropism: Human adenovirus species D types 15, 29, 56, and 69

Recombination of the epsilon determinant and corneal tropism: Human adenovirus species D types 15, 29, 56, and 69

Caveolins and caveolae in ocular physiology and pathophysiology

Novel model of innate immunity in corneal infection

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