Biochemical and Biophysical Research Communications

2004

DOI: 10.1016/j.bbrc.2004.07.091

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Single injection of naked plasmid encoding α-melanocyte-stimulating hormone protects against thioacetamide-induced acute liver failure in mice

Cheng Haung Wang

¹

,

²

,

Tsung Hsing Lee

³

et al.

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Msh-α and Mch2

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Reporter Gene Immune Response1

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Cited by 28 publications

(33 citation statements)

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“…Therapeutic α-MSH-treatments have been tried in animal models of septic shock, contact dermatitis, rheumatoid arthritis, acute pancreatitis, toxin-induced liver failure, allergic airway inflammation, endotoxin induce uveitis, and experimental autoimmune uveoretinitis (Ceriani et al, 1994;Grabbe et al, 1996;Jahovic et al, 2004;Martin and Lipton, 1990;Nishida et al, 2004;Raap et al, 2003;Shiratori et al, 2004;Taylor et al, 2000;Wang et al, 2004). In addition, two other groups of researchers have attempted to use different forms of gene therapy to see if delivering α-MSH into the immune response of EAE will suppress the onset and subsequent pathology of EAE.…”

Section: Discussionmentioning

confidence: 99%

The diminishment of experimental autoimmune encephalomyelitis (EAE) by neuropeptide alpha-melanocyte stimulating hormone (α-MSH) therapy

¹

,

²

2008

Brain, Behavior, and Immunity

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The neuropeptide alpha-melanocyte stimulating hormone (α-MSH) plays an important role in immune privilege by its suppression of inflammation, and its induction of regulatory T cells. This finding led us to test the possibility that we can use α-MSH to suppress autoimmune diseases, and promote re-establishment of immune tolerance to autoantigens. To test this possibility, SJL mice with experimental autoimmune encephalomyelitis (EAE) were injected with α-MSH at the first signs of paralysis. The α-MSH-treated mice in comparison with untreated EAE mice had a profound diminishment in the severity and tempo of EAE. The spleen cells in α-MSH-treated EAE produced TGF-β in response to PLP-antigen stimulation in contrast to untreated mice spleen cells that produced IFN-γ. When the α-MSH-treated EAE mice were reimmunized there was a delay of a week before the second episode of EAE. Although this delay maybe because of the induction of TGF-β-producing spleen cells by the α-MSH-treatment, it was not adequate to suppress IFN-γ-production by PLP-antigen stimulated spleen cells from untreated mice, nor able to suppress the eventual second episode of EAE. Therefore, the injection of α-MSH at the onset of paralysis is extremely effective in diminishing the severity and tempo of EAE, and the subsequent induction of potential PLP-specific Treg cells suggests that an α-MSH therapy could be attempted as part of a therapeutic regiment to impose immunoregulation and immunosuppression on an autoimmune disease of the central nervous system.

“…Therapeutic α-MSH-treatments have been tried in animal models of septic shock, contact dermatitis, rheumatoid arthritis, acute pancreatitis, toxin-induced liver failure, allergic airway inflammation, endotoxin induce uveitis, and experimental autoimmune uveoretinitis (Ceriani et al, 1994;Grabbe et al, 1996;Jahovic et al, 2004;Martin and Lipton, 1990;Nishida et al, 2004;Raap et al, 2003;Shiratori et al, 2004;Taylor et al, 2000;Wang et al, 2004). In addition, two other groups of researchers have attempted to use different forms of gene therapy to see if delivering α-MSH into the immune response of EAE will suppress the onset and subsequent pathology of EAE.…”

Section: Discussionmentioning

confidence: 99%

The diminishment of experimental autoimmune encephalomyelitis (EAE) by neuropeptide alpha-melanocyte stimulating hormone (α-MSH) therapy

¹

,

²

2008

Brain, Behavior, and Immunity

View full text Add to dashboard Cite

The neuropeptide alpha-melanocyte stimulating hormone (α-MSH) plays an important role in immune privilege by its suppression of inflammation, and its induction of regulatory T cells. This finding led us to test the possibility that we can use α-MSH to suppress autoimmune diseases, and promote re-establishment of immune tolerance to autoantigens. To test this possibility, SJL mice with experimental autoimmune encephalomyelitis (EAE) were injected with α-MSH at the first signs of paralysis. The α-MSH-treated mice in comparison with untreated EAE mice had a profound diminishment in the severity and tempo of EAE. The spleen cells in α-MSH-treated EAE produced TGF-β in response to PLP-antigen stimulation in contrast to untreated mice spleen cells that produced IFN-γ. When the α-MSH-treated EAE mice were reimmunized there was a delay of a week before the second episode of EAE. Although this delay maybe because of the induction of TGF-β-producing spleen cells by the α-MSH-treatment, it was not adequate to suppress IFN-γ-production by PLP-antigen stimulated spleen cells from untreated mice, nor able to suppress the eventual second episode of EAE. Therefore, the injection of α-MSH at the onset of paralysis is extremely effective in diminishing the severity and tempo of EAE, and the subsequent induction of potential PLP-specific Treg cells suggests that an α-MSH therapy could be attempted as part of a therapeutic regiment to impose immunoregulation and immunosuppression on an autoimmune disease of the central nervous system.

“…Another interesting consequence of α-MSH signaling is the suppression of the collagen synthesis and deposition [83]. Furthermore, in fibrotic tissues, α-MSH treatment modulates the balance between matrix metalloproteinase (MMP)-1, MMP-8 and their inhibitors (TIMPs) [84].…”

Section: Msh-α and Mchmentioning

confidence: 99%

“…α-MSH reduces endotoxin-induced liver inflammation in the mouse model [92], protects against thioacetamide-induced acute liver failure [84] and attenuates carbon tetrachloride (CCl 4 )-induced liver fibrosis [93]. The most likely mechanisms for this protection include α-MSH-dependent inhibition of cell adhesion molecules and cyclooxygenase (COX)-2 expression, as well as the collagenolytic effects exerted through MMP and TIMP modulation [84]. Since hepatic fibrosis may progress in patients with NASH (as with patients with other chronic liver diseases), the anticollagenic effects of α-MSH may be beneficial.…”

Section: Msh-α and Mchmentioning

confidence: 99%

“…Another interesting consequence of α-MSH signaling is the suppression of the collagen synthesis and deposition [83]. Furthermore, in fibrotic tissues, α-MSH treatment modulates the balance between matrix metalloproteinase (MMP)-1, MMP-8 and their inhibitors (TIMPs) [84].In adipose tissue, α-MSH inhibits leptin secretion in differentiated rat adipocytes cultured in vitro. In turn, leptin administered to ob/ob mice increases the release of α-MSH into the circulation, suggesting a possible feedback loop between the sites of α-MSH release and the release of leptin from the adipose tissue [85,86].…”

mentioning

confidence: 99%

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Adipokines and melanocortins in the hepatic manifestation of metabolic syndrome: nonalcoholic fatty liver disease

2018

Preprint

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Metabolic syndrome is associated with nonalcoholic fatty liver disease and its more aggressive form, nonalcoholic steatohepatitis. Adipokines produced by white adipose tissue possess broad physiological activity and play an important autocrine role in obesity-associated complications, including metabolic syndrome, nonalcoholic fatty liver disease and cardiovascular disease. Various adipokines may have beneficial or harmful effects. Other tissues, particularly stomach and intestine, produce active molecules that can influence the function of adipocytes and, possibly, the levels of adipokine secretion. In some cases, the production sites of these molecules remain unknown. The review focuses on our current understanding of the disease-related effects of the adipokines and the melanocortins on various peripheral tissues, and discusses some of their potential interactions with each other. Potential therapeutic applications are also considered.Expert Rev. Mol. Diagn. 7(2), 195-205 (2007) Multiple facets of metabolic syndromeMetabolic syndrome (MS) was first introduced as a clinical entity by Reaven in 1988 [1]. MS represents a cluster of risk factors commonly associated with central obesity, insulin-resistance, hypertension and elevated triglycerides, as well as decreased high-density lipoprotein cholesterol. In turn, MS is associated with an increased risk of cardiovascular disease and is a common early abnormality in the development of Type 2 diabetes. Additionally, MS plays a well-recognized role in the development of the obstructive sleep apnea, erectile dysfunction, polycystic ovary syndrome and malignant tumors. It is noteworthy that, despite tremendous clinical impact of MS, there is no clear consensus regarding the diagnostic criteria for this important nosological entity. To date, different criteria have been proposed by the WHO, by the third report of the National Cholesterol Education Program Adult Treatment Panel III (ATPIII) on Detection, Evaluation, and Treatment of High Blood Cholesterol in Adults, International Diabetes Federation, European Group for the Study of Insulin Resistance, and American College of Endocrinology. The problem of multiple MS definitions was recently addressed in a joint statement of The American Diabetes Association and the European Association for the Study of Diabetes [2]. The statement and other publications stress the necessity of introduction of additional criteria for MS including concentrations of the proand anti-inflammatory proteins in the serum. It is most likely that the list of the etiological factors driving the development of MS includes abnormalities in visceral adipose tissue or an altered inflammatory background that, in turn, stimulate the development of the secondary complications of MS.Recently, nonalcoholic fatty liver disease (NAFLD) and its more aggressive form, nonalcoholic steatohepatitis (NASH), have come to be regarded as the hepatic manifestation of MS. In this context, insulin resistance (IR) is 196Expert Rev. Mol. Diagn. 7(2), (2007) the key eve...

“…The vectors were injected in 2 ml PBS in less than 8 s to promote hydrodynamic-based gene transfer. 39,40 Serum samples were collected 10 days later. Preimmune and immune serum samples (diluted 1:200 in PBS) were added to the wells of microtiter plates coated with 293 cells transiently transfected with pLNCX, pLNCX-DNSeB7 or pLNCX-LacZ-eB7.…”

Section: Reporter Gene Immune Responsementioning

confidence: 99%

A membrane antibody receptor for noninvasive imaging of gene expression

¹

,

Wang²,

Yu³

et al. 2005

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Monitoring gene expression is important to optimize gene therapy protocols and ensure that the proper tissue distribution is achieved in clinical practice. We developed a noninvasive imaging system based on the expression of artificial antibody receptors to trap hapten-labeled imaging probes. Functional membrane-bound anti-dansyl antibodies (DNS receptor) were stably expressed on melanoma cells in vitro and in vivo. A bivalent (DNS) 2 -diethylenetriaminepentaacetic 111 Indium probe specifically bound to cells that expressed DNS receptors but not control scFv receptors.Importantly, the 111 In probe preferentially localized to DNS receptors but not control receptors on tumors in mice as assessed by gamma camera imaging. By 48 h after intravenous injection, the uptake of the probe in tumors expressing DNS receptors was 72 times greater than the amount of probe in the blood. This targeting strategy may allow noninvasive assessment of the location, extent and persistence of gene expression in living animals and in the clinic. Gene Therapy (2006) 13, 412-420.

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