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RETRACTED ARTICLE: Eobania vermiculata whole-body muscle extract-loaded chitosan nanoparticles enhanced skin regeneration and decreased pro-inflammatory cytokines in vivo
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Abstract
Background
Usually, wounds recover in four to six weeks. Wounds that take
longer time than this to heal are referred to as chronic wounds. Impaired
healing can be caused by several circumstances like hypoxia, microbial
colonization, deficiency of blood flow, reperfusion damage, abnormal cellular
reaction and deficiencies in collagen production. Treatment of wounds can be
enhanced through systemic injection of the antibacterial drugs and/or other
topical applications of medications. However, there are a number of
disadvantages to these techniques, including the limited or insufficient
medication penetration into the underlying skin tissue and the development of
bacterial resistance with repeated antibiotic treatment. One of the more recent
treatment options may involve using nanotherapeutics in combination with
naturally occurring biological components, such as snail extracts (SE). In this
investigation, chitosan nanoparticles (CS NPs) were loaded with an Eobania vermiculata whole-body muscle extract. The
safety of the synthesized NPs was investigated in vitro to determine if these
NPs might be utilized to treat full-skin induced wounds in vivo.
Results
SEM and TEM images showed uniformly distributed, spherical, smooth
prepared CS NPs and snail extract-loaded chitosan nanoparticles (SE-CS NPs) with
size ranges of 76–81 and 91–95 nm, respectively. The zeta
potential of the synthesized SE-CS NPs was − 24.5 mV, while that
of the CS NPs was 25 mV. SE-CS NPs showed a remarkable, in vitro, antioxidant,
anti-inflammatory and antimicrobial activities. Successfully, SE-CS NPs
(50 mg/kg) reduced the oxidative stress marker (malondialdehyde), reduced
inflammation, increased the levels of the antioxidant enzymes (superoxide
dismutase and glutathione), and assisted the healing of induced wounds. SE-CS
NPs (50 mg/kg) can be recommended to treat induced wounds safely. SE was
composed of a collection of several wound healing bioactive components [fatty
acids, amino acids, minerals and vitamins) that were loaded on CS NPs.
Conclusions
The nanostructure enabled bioactive SE components to pass through
cell membranes and exhibit their antioxidant and anti-inflammatory actions,
accelerating the healing process of wounds. Finally, it is advised to treat
rats’ wounds with SE-CS NPs.
Graphical abstract
Springer Science and Business Media LLC
Title: RETRACTED ARTICLE:
Eobania vermiculata whole-body muscle extract-loaded chitosan
nanoparticles enhanced skin regeneration and decreased pro-inflammatory cytokines in
vivo
Description:
Abstract
Background
Usually, wounds recover in four to six weeks.
Wounds that take
longer time than this to heal are referred to as chronic wounds.
Impaired
healing can be caused by several circumstances like hypoxia, microbial
colonization, deficiency of blood flow, reperfusion damage, abnormal cellular
reaction and deficiencies in collagen production.
Treatment of wounds can be
enhanced through systemic injection of the antibacterial drugs and/or other
topical applications of medications.
However, there are a number of
disadvantages to these techniques, including the limited or insufficient
medication penetration into the underlying skin tissue and the development of
bacterial resistance with repeated antibiotic treatment.
One of the more recent
treatment options may involve using nanotherapeutics in combination with
naturally occurring biological components, such as snail extracts (SE).
In this
investigation, chitosan nanoparticles (CS NPs) were loaded with an Eobania vermiculata whole-body muscle extract.
The
safety of the synthesized NPs was investigated in vitro to determine if these
NPs might be utilized to treat full-skin induced wounds in vivo.
Results
SEM and TEM images showed uniformly distributed, spherical, smooth
prepared CS NPs and snail extract-loaded chitosan nanoparticles (SE-CS NPs) with
size ranges of 76–81 and 91–95 nm, respectively.
The zeta
potential of the synthesized SE-CS NPs was − 24.
5 mV, while that
of the CS NPs was 25 mV.
SE-CS NPs showed a remarkable, in vitro, antioxidant,
anti-inflammatory and antimicrobial activities.
Successfully, SE-CS NPs
(50 mg/kg) reduced the oxidative stress marker (malondialdehyde), reduced
inflammation, increased the levels of the antioxidant enzymes (superoxide
dismutase and glutathione), and assisted the healing of induced wounds.
SE-CS
NPs (50 mg/kg) can be recommended to treat induced wounds safely.
SE was
composed of a collection of several wound healing bioactive components [fatty
acids, amino acids, minerals and vitamins) that were loaded on CS NPs.
Conclusions
The nanostructure enabled bioactive SE components to pass through
cell membranes and exhibit their antioxidant and anti-inflammatory actions,
accelerating the healing process of wounds.
Finally, it is advised to treat
rats’ wounds with SE-CS NPs.
Graphical abstract.
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