Dynamic protein expression of NF‑κB following rat intracerebral hemorrhage and its association with apoptosis

Liu, Zongchao; Meng, Lingqiu; Song, Jinghui; Gao, Jing

doi:10.3892/etm.2018.6715

Cited by 11 publications

(8 citation statements)

References 35 publications

(30 reference statements)

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“…Secondly, as for all inducible transcription factors, NF-κB stimulation, similar as to Nrf2, may only persist for a limited amount of time, and measurements may be more time-sensitive than the resulting downstream cytokines. This was shown in a rat model of cerebral haemorrhage, where NF-κB protein expression was measured 3 h following injury (cytoplasm), identified in the nucleus at 6 h, with a peak expression of 72 h, lasting for about 5 days [ 447 ]. Finally, expression may differ between cells in the body and measuring NF-κB may require a fair amount of cells.…”

Section: Markers Of Inflammation Relation To Disease and Practicamentioning

confidence: 99%

Common and Novel Markers for Measuring Inflammation and Oxidative Stress Ex Vivo in Research and Clinical Practice—Which to Use Regarding Disease Outcomes?

Menzel¹,

Samouda

Dohet³

et al. 2021

Antioxidants

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Many chronic conditions such as cancer, chronic obstructive pulmonary disease, type-2 diabetes, obesity, peripheral/coronary artery disease and auto-immune diseases are associated with low-grade inflammation. Closely related to inflammation is oxidative stress (OS), which can be either causal or secondary to inflammation. While a low level of OS is physiological, chronically increased OS is deleterious. Therefore, valid biomarkers of these signalling pathways may enable detection and following progression of OS/inflammation as well as to evaluate treatment efficacy. Such biomarkers should be stable and obtainable through non-invasive methods and their determination should be affordable and easy. The most frequently used inflammatory markers include acute-phase proteins, essentially CRP, serum amyloid A, fibrinogen and procalcitonin, and cytokines, predominantly TNFα, interleukins 1β, 6, 8, 10 and 12 and their receptors and IFNγ. Some cytokines appear to be disease-specific. Conversely, OS—being ubiquitous—and its biomarkers appear less disease or tissue-specific. These include lipid peroxidation products, e.g., F2-isoprostanes and malondialdehyde, DNA breakdown products (e.g., 8-OH-dG), protein adducts (e.g., carbonylated proteins), or antioxidant status. More novel markers include also –omics related ones, as well as non-invasive, questionnaire-based measures, such as the dietary inflammatory-index (DII), but their link to biological responses may be variable. Nevertheless, many of these markers have been clearly related to a number of diseases. However, their use in clinical practice is often limited, due to lacking analytical or clinical validation, or technical challenges. In this review, we strive to highlight frequently employed and useful markers of inflammation-related OS, including novel promising markers.

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Section: Markers Of Inflammation Relation To Disease and Practicamentioning

confidence: 99%

Common and Novel Markers for Measuring Inflammation and Oxidative Stress Ex Vivo in Research and Clinical Practice—Which to Use Regarding Disease Outcomes?

Menzel¹,

Samouda

Dohet³

et al. 2021

Antioxidants

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show abstract

“…7 B1 ). Nf‐κb is a key nuclear transcription factor involved in apoptosis (57). Key signaling components of the NF‐κB pathway, including Tnf‐α , receptor‐interacting protein (Rip)1, RING finger domain protein Traf2/5 , and transcriptional activators P50/P65 , were up‐regulated in VEGF‐deprived retina.…”

Section: Discussionmentioning

confidence: 99%

Intraocular VEGF deprivation induces degeneration and fibrogenic response in retina

Xiao

Liu

Wang³

et al. 2019

The FASEB Journal

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VEGF is a critical driver of ocular neovascularization under disease conditions. Current therapeutic strategies rely on intraocular delivery of VEGF-antagonizing reagents, which results in sustained suppression of pathogenic vascularization. Although significant advancement has been achieved in VEGF antagonism, substantial adverse effects have been reported in retrospective clinical studies. To study mechanisms for VEGF antagonismassociated adverse effects in visual system, we intravitreally delivered recombinant adeno-associated virusmediated expression of soluble Fms-related tyrosine kinase-1 (rAAV.sFLT-1), the extracellular domain of VEGF receptor, and analyzed the morphology and functions of retinal tissue. Here, we confirmed that intraocular VEGF antagonism induced retinal degeneration and gliosis. The functional deficit in retinal response to visual stimulation was also demonstrated in rAAV.sFLT-1-treated eyes by electroretinogram. Moreover, high-throughput RNA sequencing analysis suggests that VEGF antagonism activates retinal degeneration, inflammation, and other adverse effects. Taken together, our findings have shed light on pathogenic mechanisms for VEGF antagonism-associated adverse effects and potential therapeutic targets.

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“…The NF-jB levels then peaked at 3 days and NF-jB was still present at 5 days. 44 The induction of NF-jB subsequently up-regulated the expression of several genes, including those from the matrix metalloproteinase (MMP) family, NOD-like receptor family pyrin domain containing 3 (NLRP3) inflammasome and several pro-inflammatory cytokines such as interleukin 1 beta (IL-1b) and tumor necrosis factor-alpha (TNF-⍺). Expression of these genes ultimately leads to neuroinflammation and BBB hyperpermeability.…”

Section: Inflammationmentioning

confidence: 99%

Potential therapeutic effects of Nrf2 activators on intracranial hemorrhage

Imai

Matsubara

Hara

2021

J Cereb Blood Flow Metab

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Intracranial hemorrhage (ICH) is a devastating disease which induces high mortality and poor outcomes including severe neurological dysfunctions. ICH pathology is divided into two types: primary brain injury (PBI) and secondary brain injury (SBI). Although there are numerous preclinical studies documenting neuroprotective agents in experimental ICH models, no effective drugs have been developed for clinical use due to complicated ICH pathology. Oxidative and inflammatory stresses play central roles in the onset and progression of brain injury after ICH, especially SBI. Nrf2 is a crucial transcription factor in the anti-oxidative stress defense system. Under normal conditions, Nrf2 is tightly regulated by the Keap1. Under ICH pathological conditions, such as overproduction of reactive oxygen species (ROS), Nrf2 is translocated into the nucleus where it up-regulates the expression of several anti-oxidative phase II enzymes such as heme oxygenase-1 (HO-1). Recently, many reports have suggested the therapeutic potential of Nrf2 activators (including natural or synthesized compounds) for treating neurodegenerative diseases. Moreover, several Nrf2 activators attenuate ischemic stroke-induced brain injury in several animal models. This review summarizes the efficacy of several Nrf2 activators in ICH animal models. In the future, Nrf2 activators might be approved for the treatment of ICH patients.

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Dynamic protein expression of NF‑κB following rat intracerebral hemorrhage and its association with apoptosis

Cited by 11 publications

References 35 publications

Common and Novel Markers for Measuring Inflammation and Oxidative Stress Ex Vivo in Research and Clinical Practice—Which to Use Regarding Disease Outcomes?

Common and Novel Markers for Measuring Inflammation and Oxidative Stress Ex Vivo in Research and Clinical Practice—Which to Use Regarding Disease Outcomes?

Intraocular VEGF deprivation induces degeneration and fibrogenic response in retina

Potential therapeutic effects of Nrf2 activators on intracranial hemorrhage

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