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  1. Renu Agarwal, SK Gupta, Sushma Srivastava, Rohit Saxena
    MyJurnal
    Introduction: Ocimum basilicum (OB), a herb known for its antihypertensive,
    anticholinesterase and antioxidant properties was investigated for possible intraocular
    pressure (IOP) lowering effects in rabbits with ocular hypertension (OHT). Methods: The
    IOP lowering effect of a single drop of OB extract (OBE) was evaluated in oculonormotensive
    rabbits using three concentrations (0.25, 0.5 and 1% w/v). The concentration showing
    maximum IOP reduction was further evaluated in rabbits with water-loading and steroidinduced OHT. Results: IOP lowering effect of OBE 0.5% in oculonormotensive rabbit eyes
    was significantly greater compared to OBE 0.25% (p0.05) to
    OBE 1%. Therefore, 0.5% concentration was selected for further evaluation. Pretreatment
    with OBE (0.5%) caused significantly lower increase in IOP after water loading amounting to
    23.39% above baseline as compared to 54.00% in control eye, 15 minutes post water
    loading. At 60 minutes, post water loading, mean IOP rise was 95.12% and 63.58% in
    control and test eyes, respectively. Significant difference between the mean IOP of two eyes
    persisted during the 2nd hr. In rabbits with steroid induced OHT, OBE 0.5% produced a
    mean IOP reduction of 24.73% at the end of first hr and the mean peak IOP reduction of
    31.63% was observed at the end of 2 hr. A significant difference between the IOP of test and
    control eyes persisted from 1 to 6 hr. Conclusions: Ocimum basilicum seed extract showed
    significant IOP lowering effect in rabbits with water loading and steroid induced OHT,
    however, its utility as an effective antiglaucoma medication needs further investigations.
  2. Amy Suzana Abu Bakar, Norhafiza Razali, Mohammad Daniel Shafiq Hassan, Renu Agarwal
    MyJurnal
    Glaucoma is an optic neuropathy characterised by optic nerve degeneration associated with
    visual field defects. It remains the world’s number one cause of irreversible blindness and
    patients usually present at late stage of the disease since it is generally asymptomatic until
    severe. The disease is subdivided into primary and secondary with primary open-angle
    glaucoma (POAG) being the most common type. At present, lowering the intraocular pressure
    (IOP) remains the only proven efficient approach in delaying the onset or preventing the
    progression of the disease. Medical treatment with topical antiglaucoma agents is the
    treatment of choice in open angle glaucoma. The use of antiglaucoma drugs aims to reduce
    IOP by enhancing aqueous humour (AH) outflow, reducing AH production, or both. The choice
    to use any available treatment option should be carefully considered in an attempt to maximise
    benefits and reducing the risk of developing adverse drug reactions. This review highlights the
    six classes of ocular hypotensive agents currently in use for POAG treatment including
    prostaglandin analogues; -adrenergic receptor blockers; -2 adrenergic receptor stimulants;
    carbonic anhydrase inhibitors; muscarinic receptor stimulants; rho kinase inhibitors with
    regards to their mechanism/s of action and potential adverse drug reactions, and
    antiglaucoma fixed drug combinations.
  3. Norasikin Ab Azis, Mohd Saleh Ahmad Kamal, Zurain Radjeni, Ahmed Mediani, Renu Agarwal
    MyJurnal
    Introduction: This study examined the association of losartan induced changes in urinary
    metabolomic profile with the changes in blood pressure (BP) and renin-angiotensinaldosterone system (RAAS) in spontaneously hypertensive rats (SHR). Methods: Male SHR
    were administered with either 0.5 mL of distilled water (control group, n=6) or 10 mg.kg-1 of
    losartan (group 2, n=6) daily by oral gavage for 4 weeks. Body weight, BP, food and water
    intake were measured weekly. At week 4, urine was collected for urinary electrolyte analysis
    and metabolite profiling, after which the animals were euthanised by decapitation and blood
    was collected for analysis of components of RAAS and electrolyte concentrations. Urine
    metabolite profile of SHR was determined using proton nuclear magnetic resonance (
    1H-NMR)
    spectrometry combined with multivariate data analysis. Results: At week 4, losartan-treated
    SHR had significantly lower BP than non-treated SHR. There were no differences in water
    and food intake, body weight, serum and urinary electrolyte concentrations or in their urinary
    excretions between the two groups. No differences were evident in the components of RAAS
    except that the angiotensinogen level was significantly higher in losartan-treated SHR
    compared to non-treated SHR. Orthogonal partial least squares discriminant analysis (OPLSDA) showed clear separation of urinary metabolites between control and losartan-treated
    SHR. Losartan-treated SHR group was separated from the control group by changes in the
    intermediates involved in glycine, serine and threonine metabolism. Conclusion:
    Antihypertensive effect of losartan in SHR seems to be associated with changes in urinary
    metabolite profile, particularly involving the metabolism of glycine, serine and threonine.
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