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EFFECT OF LOVASTATIN NANO DRUG DELIVERY SYSTEM ON B ONE MINERAL DENSITY (BMD) AND BIOMECHANICAL PROPERTIES OF TIBIA BONES O F WISTAR RATS

By: Kaur, Ramandeep.
Contributor(s): Ajitha, Makula.
Publisher: M P Innovare Academic Sciences Pvt Ltd 2019Edition: Vol.11(9).Description: 42-48p.Subject(s): PHARMACEUTICSOnline resources: Click here In: International journal of pharmacy and pharmaceutical scienceSummary: Objective: In the present study, transdermal nanoemulsion (NE) gel of lovastatin was investigated for its anti-os teoporosis effect on the long bones of rat i.e. tibia. Methods: Male wistar rats (n=30, weighing 180-200g) were tak en for this study and grouped as: 1) control (norma l saline daily), 2) Dex (dexamethasone sodium; 25 mg/kg subcutaneously twic e a week), 3) Dex+LNG5 (lovastatin nanoemulsion gel ; 5 mg/kg/d transdermally daily), 4) Dex+LNG10 (lovastatin nanoemulsion gel; 10 mg/kg/d transdermally daily), and 5) Dex+ALN (alendronate s odium; 0.03 mg/kg/d orally daily). All the treatments were carried out for 60 d. At the en d of the experiment, all animals were anesthetized using diethyl ether and collected blood samples from retro-orbital venous plexus of rats in dry eppendorf tubes followed by the sacrifice of a nimals by cervical dislocation method and collected tibia bones of both the legs for analysis . Results: Bone formation biomarkers (OC: osteocalcin, b-ALP: bone-specific alkaline phosphatase, PINP: N-termina l propeptides of type I procollagen) were significantly improved and resorption biomarke rs (CTx: C-terminal cross-linking telopeptides of t ype-I collagen, TRAcP5b: isoform 5b of tartarate resistant acid phosphatase) were significantly redu ced in the LNG5 (p<0.05) and LNG10 (p<0.05) treatme nt groups when compared to Dex. In vivo anti- osteoporotic results demonstrated the formation of new bone in osteoporotic rat tibias. Biomechanical strength testing demonstrated increased load- bearing capacity of rat tibias in the treated anima ls in comparison with the osteoporotic group (p<0.0 5 for LNG5 and p<0.01 for LNG10).
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Objective:
In the present study, transdermal nanoemulsion (NE)
gel of lovastatin was investigated for its anti-os
teoporosis effect on the long bones
of rat i.e. tibia.
Methods:
Male wistar rats (n=30, weighing 180-200g) were tak
en for this study and grouped as: 1) control (norma
l saline daily), 2) Dex
(dexamethasone sodium; 25 mg/kg subcutaneously twic
e a week), 3) Dex+LNG5 (lovastatin nanoemulsion gel
; 5 mg/kg/d transdermally daily), 4)
Dex+LNG10 (lovastatin nanoemulsion gel; 10 mg/kg/d
transdermally daily), and 5) Dex+ALN (alendronate s
odium; 0.03 mg/kg/d orally daily). All
the treatments were carried out for 60 d. At the en
d of the experiment, all animals were anesthetized
using diethyl ether and collected blood
samples from retro-orbital venous plexus of rats in
dry eppendorf tubes followed by the sacrifice of a
nimals by cervical dislocation method and
collected tibia bones of both the legs for analysis
.
Results:
Bone formation biomarkers (OC: osteocalcin, b-ALP:
bone-specific alkaline phosphatase, PINP: N-termina
l propeptides of type I procollagen)
were significantly improved and resorption biomarke
rs (CTx: C-terminal cross-linking telopeptides of t
ype-I collagen, TRAcP5b: isoform 5b of tartarate
resistant acid phosphatase) were significantly redu
ced in the LNG5 (p<0.05) and LNG10 (p<0.05) treatme
nt groups when compared to Dex.
In vivo
anti-
osteoporotic results demonstrated the formation of
new bone in osteoporotic rat tibias. Biomechanical
strength testing demonstrated increased load-
bearing capacity of rat tibias in the treated anima
ls in comparison with the osteoporotic group (p<0.0
5 for LNG5 and p<0.01 for LNG10).

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