Receptor Tyrosine Kinases as Therapeutic Targets for Alcohol Use Disorder

Hamada, Kana; Lasek, Amy W.

doi:10.1007/s13311-019-00795-4

Cited by 13 publications

(5 citation statements)

References 143 publications

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“…FGF21 was shown to signal to neurons in the paraventricular nucleus to stimulate water consumption in response to alcohol (Song et al, 2018). These studies and others suggest that RTKs and FGFRs, in particular, may be viable drug targets to modify alcohol abuse behaviors (Hamada & Lasek, 2020).…”

Section: Fgf Signaling In the Brain And Sensory Organsmentioning

confidence: 91%

New developments in the biology of fibroblast growth factors

Ornitz

Itoh

2022

WIREs Mechanisms of Disease

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The fibroblast growth factor (FGF) family is composed of 18 secreted signaling proteins consisting of canonical FGFs and endocrine FGFs that activate four receptor tyrosine kinases (FGFRs 1-4) and four intracellular proteins (intracellular FGFs or iFGFs) that primarily function to regulate the activity of voltagegated sodium channels and other molecules. The canonical FGFs, endocrine FGFs, and iFGFs have been reviewed extensively by us and others. In this review, we briefly summarize past reviews and then focus on new developments in the FGF field since our last review in 2015. Some of the highlights in the past 6 years include the use of optogenetic tools, viral vectors, and inducible transgenes to experimentally modulate FGF signaling, the clinical use of small molecule FGFR inhibitors, an expanded understanding of endocrine FGF signaling, functions for FGF signaling in stem cell pluripotency and differentiation, roles for FGF signaling in tissue homeostasis and regeneration, a continuing elaboration of mechanisms of FGF signaling in development, and an expanding appreciation of roles for FGF signaling in neuropsychiatric diseases.

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Section: Fgf Signaling In the Brain And Sensory Organsmentioning

confidence: 91%

New developments in the biology of fibroblast growth factors

Ornitz

Itoh

2022

WIREs Mechanisms of Disease

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“…Pleiotrophin and MK inactivate the phosphatase activity of RPTPβ/ζ, increasing the phosphorylation levels of its substrates [12,18]. Some of these RPTPβ/ζ substrates such as ALK [19], also a proposed receptor for PTN and MK [14], and Fyn kinase [20] are known to be important regulators of alcohol behavioral effects [1,21]. Importantly, small-molecule blood-brain barrier (BBB)-permeable inhibitors of RPTPβ/ζ [22] have recently been shown to reduce alcohol-induced conditioned place preference (CPP) and alcohol consumption in mice [10,23], and to reduce alcohol consumption in an operant self-administration paradigm in rats [24].…”

Section: Extinction Of Cppmentioning

confidence: 99%

Genetic inactivation of midkine, not pleiotrophin, facilitates extinction of alcohol-induced conditioned place preference

Vicente-Rodríguez

Pérez-Garcı́a

Gramage

et al. 2021

Neuroscience Letters

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“…The pötential hepatöprötective effects öf zönisamide are drawing significant interest fröm the scientific and medical cömmunities 11 . A cömprehensive appröach, encömpassing everything fröm lifestyle mödificatiöns tö pharmacölögical interventiöns, is required tö prevent and treat alcöhöl-related liver injuries 12,13 . Understanding the röle öf zönisamide in this cöntext cöuld significantly aid in develöping effective treatment strategies and prövide new insights intö managing alcöhöl-induced liver cönditiöns 14 .…”

Section: Introductionmentioning

confidence: 99%

Investigation of the Efficacy of Zonisamide in Alcohol Induced Hepatotoxicity

Dönmezdil,

Tunik,

Aşır

et al. 2024

J. Drug Delivery Ther.

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Subject: This research aims to evaluate the histological changes in liver tissue induced by alcohol consumption and to assess the effectiveness of zonisamide in treating alcohol-related hepatotoxicity. Materials and Methods: The study utilized 40 adult Wistar albino rats, divided into four groups: a control (sham), an ethanol group, a zonisamide group, and a combination of ethanol and zonisamide (ethanol+zonisamide). Each group underwent a four-day binge drinking protocol to mimic excessive alcohol intake observed in humans. Zonisamide was administered at a dose of 100 mg/kg daily. Post-treatment, the liver tissues were collected, stained with hematoxylin and eosin, and examined for histopathological changes. Results: The control and zonisamide-only groups showed no abnormal liver or vascular alterations, indicating zonisamide's safety. In contrast, the ethanol group displayed significant liver damage, including vascular dilatation, congestion, and extensive cellular degeneration. Conversely, the ethanol+zonisamide group exhibited substantial histological improvements with noticeable reductions in vascular impairments and signs of hepatocyte regeneration, suggesting that zonisamide mitigates the detrimental effects of alcohol on the liver. Conclusion: The study concludes that zonisamide has a protective effect against alcohol-induced liver damage. It appears to preserve the structural integrity of hepatocytes and supports cellular survival, potentially through its anti-inflammatory and antioxidant properties. These promising results advocate for further exploration of zonisamide as a therapeutic option for managing liver injuries associated with alcohol abuse. This study contributes significant insights into the therapeutic potential of zonisamide, encouraging more comprehensive investigations into its clinical applications in hepatology. Keywords: Alcohol, Zonisamide, Hepatotoxicity

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Receptor Tyrosine Kinases as Therapeutic Targets for Alcohol Use Disorder

Cited by 13 publications

References 143 publications

New developments in the biology of fibroblast growth factors

New developments in the biology of fibroblast growth factors

Genetic inactivation of midkine, not pleiotrophin, facilitates extinction of alcohol-induced conditioned place preference

Investigation of the Efficacy of Zonisamide in Alcohol Induced Hepatotoxicity

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