Aldose reductase mediates endotoxin-induced production of nitric oxide and cytotoxicity in murine macrophages

Ramana, Kota V.; Reddy, Aramati B.M.; Tammali, Ravinder; Srivastava, Satish K.

doi:10.1016/j.freeradbiomed.2007.01.033

Cited by 47 publications

(41 citation statements)

References 73 publications

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“…Therefore, understanding the mechanism of RMG activation is a necessity for preventing these ocular diseases. Ramana and colleagues conducted many studies showing that AR plays a key role in modulating inflammatory responses in macrophages [30–32]. In agreement with Ramana’s group, we previously demonstrated that either genetic ablation or pharmacological inhibition of AR attenuates endotoxin-induced inflammatory responses in macrophages and primary RMG [25, 26].…”

Section: Discussionsupporting

confidence: 77%

“…Recent studies also implicate AR in the pathogenesis of uveitis [25–27] and fibrotic changes associated with posterior capsular opacification [28, 29]. Genetic or pharmacological blockade of AR successfully alleviates inflammatory responses induced by endotoxin [25, 26, 30–32] or hyperglycemia [33–35]. Our previous study showed that genetic or pharmacological downregulation of AR prevents endotoxin-induced inflammatory responses in RMG primary cell cultures [26].…”

Section: Introductionmentioning

confidence: 99%

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Aldose reductase mediates retinal microglia activation

Chang

Shieh

Petrash

2016

Biochemical and Biophysical Research Communications

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Retinal microglia (RMG) are one of the major immune cells in charge of surveillance of inflammatory responses in the eye. In the absence of an inflammatory stimulus, RMG reside predominately in the ganglion layer and inner or outer plexiform layers. However, under stress RMG become activated and migrate into the inner nuclear layer (INL) or outer nuclear layer (ONL). Activated RMG in cell culture secrete pro-inflammatory cytokines in a manner sensitive to downregulation by aldose reductase inhibitors. In this study, we utilized CX3CR1GFP mice carrying AR mutant alleles to evaluate the role of AR on RMG activation and migration in vivo. When tested on an ARWT background, IP injection of LPS induced RMG activation and migration into the INL and ONL. However, this phenomenon was largely prevented by AR inhibitors or in AR null mice, or was exacerbated in transgenic mice that over-express AR. LPS-induced increases in ocular levels of TNF-α and CX3CL-1 in WT mice were substantially lower in AR null mice or were reduced by AR inhibitor treatment. These studies demonstrate that AR expression in RMG may contribute to the proinflammatory phenotypes common to various eye diseases such as uveitis and diabetic retinopathy.

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Section: Discussionsupporting

confidence: 77%

Section: Introductionmentioning

confidence: 99%

Aldose reductase mediates retinal microglia activation

Chang

Shieh

Petrash

2016

Biochemical and Biophysical Research Communications

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“…This effect may not be peculiar to aldose reductase inhibitors but perhaps relative to the presence or absence of aldose reductase activity based on new studies using siRNA for aldose reductase. These studies show a diminished NO production and iNOS expression in LPS-treated macrophages [62].…”

Section: Limitationsmentioning

confidence: 64%

The complex role of iNOS in acutely rejecting cardiac transplants

Pieper

Roza

2008

Free Radical Biology and Medicine

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This review summarizes the evidence for a detrimental role of nitric oxide (NO) derived from inducible NO synthase (iNOS) and/or reactive nitrogen species such as peroxynitrite in acutelyrejecting cardiac transplants. In chronic cardiac transplant rejection, iNOS may have an opposing beneficial component. The purpose of this review is primarily to address issues related to acute rejection which is a recognized risk factor for chronic rejection. The evidence for a detrimental role is based upon strategies involving non-selective NOS inhibitors, NO neutralizers, selective iNOS inhibitors and iNOS gene deletion in rodent models of cardiac rejection. The review is discussed in the context of the impact on various components including graft survival, histological rejection and cardiac function which may contribute in toto to the process of graft rejection. Possible limitations of each strategy are discussed in order to understand better the variance in published findings including issues related to the potential importance of cell localization of iNOS expression. Finally, the concept of a dual role of NO and its down-stream product, peroxynitrite, in rejection vs. immune regulation is discussed.

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“…In this study, we also found that MEPA suppresses the Aktdependent activation of NF-κB, suggesting that MEPA affects the regulation of the inflammatory signal cascade. Nevertheless, further work is required to substantiate these observations in light of the study that revealed the role of the transcriptional factor AP-1 expression of proinflammatory genes [21].…”

Section: Discussionmentioning

confidence: 99%