An animal model of age-related macular degeneration in senescent Ccl-2- or Ccr-2-deficient mice

Ambati, Jayakrishna; Anand, Akshay; Fernandez, Stefan; Sakurai, Eiji; Lynn, Bert C.; Kuziel, William A.; Rollins, Barrett J.; Ambati, Balamurali K.

doi:10.1038/nm950

Cited by 578 publications

(545 citation statements)

References 39 publications

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“…A two-to threefold increase in the accumulation of ApoE E3 over ApoE E4 has been observed in various cell types [Ji et al, 2002]. If mechanisms for proper clearance in the retina and Bruch's membrane are not in place, this accumulation may serve as a pathogenic basis for disease development [Ambati et al, 2003;Tuo et al, 2004b]. In fact, the increased accumulation in non-E4 carriers may explain why ApoE is such a ubiquitous component of ocular drusen in AMD-afflicted eyes [Crabb et al, 2002].…”

Section: Discussionmentioning

confidence: 99%

“…Over-expression of VEGF in the RPE, even if only temporarily, is sufficient to induce choroidal neovascularization in the rat eye [Kliffen et al, 1997;Spilsbury et al, 2000]. CCL2 also has been associated with further deterioration and degeneration, especially in advanced disease stages [Ambati et al, 2003]. Considering that our data show nearly a twofold greater suppression of CCL2 mRNA and protein expression by E4 in RPE cells with similar findings for VEGF, we suggest that investigating the varied effects of the ApoE isoforms on chemokine and cytokine regulation may offer insights into the mechanisms responsible for the observed protective role of the E4 isoform.…”

Section: Discussionmentioning

confidence: 99%

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An apolipoprotein E variant may protect against age‐related macular degeneration through cytokine regulation

Bojanowski

Shen

Chew

et al. 2006

Environ and Mol Mutagen

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Age-related macular degeneration (AMD) is the leading cause of visual impairment and blindness among the elderly in Western countries. Genetic factors, age, cigarette smoking, nutrition, and exposure to light have been identified as AMD risk factors. In this study, we investigated the association between ApoE C112R/R158C single nucleotide polymorphisms (which determine the E2, E3, and E4 isoforms) and age-related macular degeneration (AMD), and the mechanism underlying the association. Genomic DNA was extracted from 133 clinically screened controls, 94 volunteers with a younger mean age, 120 patients with advanced AMD, and 40 archived ocular AMD slides for single nucleotide polymorphism typing. The effects of recombinant ApoE isoforms on CCL2 (a chemokine), CX3CR1 (a chemokine receptor), and VEGF (a cytokine) expression in cultured human retinal pigment epithelium (RPE) cells were tested and serum cholesterol profiles of the clinically screened subjects were analyzed. ApoE112R (E4) distribution differed significantly between AMD patients and controls. ApoE112R allele frequency was 10.9% in the AMD group when compared with 16.5% in the younger controls and 18.8% in the clinically screened controls. The pathologically diagnosed archived AMD cases had the lowest allele frequency of 5%. No significant differences in ApoE158C (E2) distribution were observed among the groups. A meta-analysis of 8 cohorts including 4,289 subjects showed a strong association between AMD and 112R, but not 158C. In vitro studies found that recombinant ApoE suppresses CCL2 and VEGF expression in RPE cells. However, the E4 isoform showed more suppression than E3 in both cases. These results further confirm the association between ApoE112R and a decreased risk of AMD development. The underlying mechanisms may involve differential regulation of both CCL2 and VEGF by the ApoE isoforms.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

An apolipoprotein E variant may protect against age‐related macular degeneration through cytokine regulation

Bojanowski

Shen

Chew

et al. 2006

Environ and Mol Mutagen

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“…Wild type [CCR2(+/+)] and CCR2(−/−) mice on a C57Bl/J6 background were used to explore the role of CCR2 in mediating Tat or morphine and Tat-induced increases in macrophages/microglia or astroglia, which were maintained and characterized as previously described (Ambati et al, 2003). To assess the selectivity of Tat 1-72 , the effects of intrastriatal Tat 1-72 , a minimally toxic, deletion mutant variant of Tat 1-72 (Tat Δ31-61 ), and saline injections were compared in CCR2(+/+) and CCR2(−/−) C57Bl/J6 mice.…”

Section: Methodsmentioning

confidence: 99%

CCR2 mediates increases in glial activation caused by exposure to HIV-1 Tat and opiates

El‐Hage

Ambati

et al. 2006

Journal of Neuroimmunology

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To assess the role of CCL2/MCP-1 in opiate drug abuse and HIV-1 comorbidity, the effects of systemic morphine and intrastriatal HIV-1 Tat on macrophage/microglial and astroglial activation were assessed in wild type and CCR2 null mice. Tat and/or morphine additively increased the proportion of CCL2 immunoreactive astroglia. The effects of morphine were prevented by naltrexone. Glial activation was significantly reduced in CCR2(−/−) versus wild-type mice following Tat or morphine plus Tat exposure. Thus, CCR2 contributes to local glial activation caused by Tat alone or in the presence of opiates, implicating CCR2 signaling in HIV-1 neuropathogenesis in drug abusers and non-abusers.

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“…VEGF is found in RPE in surgically excised human AMD specimens of CNV (Lopez et al, 1996;Frank et al, 1996;Grossniklaus et al, 2002). VEGF has been localized to CNV in rodent models of laserinduced CNV (Bora et al, 2005;Yi et al, 1997) and genetically modified mouse models of CNV (Ambati et al, 2003). The overexpression of VEGF in RPE caused intrachoroidal neovascularization in one model (Schwesinger et al, 2001).…”

Section: Vegf In Pathologic Neovascularization: Models Of Neovascularmentioning

confidence: 99%

“…The murine knockout model of Ccl-2, a chemokine important in inflammation and in attracting macrophages, developed drusen, VEGF immunoreactivity, and CNV late in life (Ambati et al, 2003). The investigators proposed that lack of the Ccl-2 chemokine led to reduced recruitment of phagocytosing macrophages and reduced turnover of debris in Bruch's membrane, thus leading to drusen.…”

Section: Stimuli For Neovascular Amd and Vegf Expressionmentioning

confidence: 99%

Vascular endothelial growth factor in eye disease

Penn

Madan

Caldwell

et al. 2008

Progress in Retinal and Eye Research

597

503

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Collectively, angiogenic ocular conditions represent the leading cause of irreversible vision loss in developed countries. In the U.S., for example, retinopathy of prematurity, diabetic retinopathy and age-related macular degeneration are the principal causes of blindness in the infant, working age and elderly populations, respectively. Evidence suggests that vascular endothelial growth factor (VEGF), a 40 kDa dimeric glycoprotein, promotes angiogenesis in each of these conditions, making it a highly significant therapeutic target. However, VEGF is pleiotropic, affecting a broad spectrum of endothelial, neuronal and glial behaviors, and confounding the validity of anti-VEGF strategies, particularly under chronic disease conditions. In fact, among other functions VEGF can influence cell proliferation, cell migration, proteolysis, cell survival and vessel permeability in a wide variety of biological contexts. This article will describe the roles played by VEGF in the pathogenesis of retinopathy of prematurity, diabetic retinopathy and age-related macular degeneration. The potential disadvantages of inhibiting VEGF will be discussed, as will the rationales for targeting other VEGF-related modulators of angiogenesis.

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An animal model of age-related macular degeneration in senescent Ccl-2- or Ccr-2-deficient mice

Cited by 578 publications

References 39 publications

An apolipoprotein E variant may protect against age‐related macular degeneration through cytokine regulation

An apolipoprotein E variant may protect against age‐related macular degeneration through cytokine regulation

CCR2 mediates increases in glial activation caused by exposure to HIV-1 Tat and opiates

Vascular endothelial growth factor in eye disease

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