Objective
This study aims to evaluate the effects of topical hyaluronic acid (HA), hypochlorous acid (HOCl), and flurbiprofen on postoperative morbidity of palatal donor sites after free gingival graft (FGG) surgery.
Materials and methods
Sixty patients requiring FGG were randomly assigned into four groups: control, HA gel (600 mg/100 g high molecular weight hyaluronic acid), HOCl spray (170–200 ppm, ph7.1), flurbiprofen spray (0.075gr flurbiprofen). Topical agents were applied for 14 days, according to groups. Patients were followed for 28 days. Palatal healing was assessed with the Laundry wound healing index (WHI). Complete epithelization (CE) was evaluated with photographs and H
2
O
2
bubbling. Pain, burning sensation, chewing efficacy, and tissue color match (CM) were evaluated using a visual analog scale (VAS). Postoperative analgesic consumption and delayed bleeding (DB) were also recorded.
Results
HA provided better WHI values on the 7
th
, 14
th
, and 21
st
days compared to the other groups, respectively (
p
< 0.05). CE was formed on the 21
st
day in the HA group but on the 28
th
day in the other groups. HOCl and flurbiprofen groups were not different from the control group or each other in terms of WHI. HOCl had the lowest VAS scores of all time periods. DB was not observed in any group. Significantly fewer analgesics were taken in the topical agent-applied groups compared to the control group
.
Conclusions
HA exhibits a positive impact on the epithelization of palatal wound healing and color matching. HOCl and flurbiprofen provided less pain; however, they might have negative effects on palatal wound healing.
Clinical relevance
As a result of obtaining free gingival grafts from palatal tissue for mucogingival surgical procedures, secondary wound healing of the donor area occurs. This wound in the palatal region can cause discomfort and pain every time patients use their mouths. The use of HA can reduce postoperative complications by accelerating wound healing and reducing pain. The topical use of flurbiprofen and HOCl can reduce patients’ pain.
Introduction:
Favipiravir
and Vitamin C (Vit C) were used together in the treatment of the COVID-19
pandemic. However, the effects of favipiravir on the periodontium
are still unknown. Therefore, the aim of this study was to investigate
the effects of Favipiravir and Vit C treatment on alveolar bone
metabolism.
Experimental:
Fifty
healthy adult male Sprague-Dawley rats (2–3 months old) were randomly
divided into five equal groups (
n
=
10): Control, Favi 20, Favi 100, Favi 20+Vit C, Favi 100+Vit C.
Favipiravir (20 mg/kg and 100 mg/kg,
i.m.
)
and Vit C (150 mg/kg/day, oral) were administered to the rats for
14 days. Alveolar bone loss (ABL) and histopathological changes
were examined using a light microscope. Immunohistochemistry was
used to determine levels of receptor activator of nuclear factor
kappa-B ligand (RANKL), caspase-3, bone morphogenic protein 2 (BMP-2)
and alkaline phosphatase (ALP) in the bone tissues.
Results:
Favipiravir increased the
levels of RANKL and caspase-3 expression but decreased BMP-2 and ALP
levels in a dose-dependent manner. Favi 20+Vit C and Favi 100 +Vit
C groups showed decreased RANKL and caspase-3 levels in addition
to increased BMP-2 and ALP levels.
Conclusion:
Favipiravir
can cause histopathological damage to the periodontium, but administration
of favipiravir combined with Vit C can provide a protective effect
against this damage.
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